Item 1.
Business.
Overview
We are a biotechnology company
with an advanced cell-based technology platform. We have developed a unique three-dimensional, or 3D, technology platform for cell expansion
with an industrial scale in-house Good Manufacturing Practice, or GMP, cell manufacturing facility. We are utilizing our technology in
the field of regenerative medicine and food tech and plan to utilize it in other industries and verticals that have a need for our mass
scale and cost-effective cell expansion platform.
We use our advanced cell-based
technology platform in the field of regenerative medicine to develop placenta-based cell therapy product candidates for the treatment
of inflammatory, muscle injuries and hematologic conditions. Our placental expanded, or PLX, cells are adherent stromal cells that are
expanded using our 3D platform. Our PLX cells can be administered to patients off-the-shelf, without blood or tissue matching or
additional manipulation prior to administration. PLX cells are believed to release a range of therapeutic proteins in response to the
patient’s condition.
Our operations are focused
on the research, development and manufacturing of cells and cell-based products, conducting clinical studies and the business development
of cell therapeutics and cell-based technologies, such as our recent collaboration with Tnuva Food Industries – Agricultural Cooperative
in Israel Ltd., through its fully owned subsidiary, Tnuva Food-Tech Incubator (2019), Limited Partnership, or Tnuva, to use our technology
to establish a cultivated food platform.
We expect to demonstrate a
real-world impact and value from our cell-based technology platform, our current PLX pipeline and from other cell-based product candidates
that may be developed based on our platform. Our business model for commercialization and revenue generation includes, but is not limited
to, licensing deals, joint ventures, partnerships, joint development agreements and direct sale of our products.
We are now completing a multinational
Phase III clinical study in muscle recovery following surgery for hip fracture, with sites in the United States, Europe and Israel. In
the last year, we have completed a Phase II clinical study in Acute Respiratory Distress Syndrome, or ARDS, associated with COVID-19 and
a Phase I clinical study for incomplete recovery following bone marrow transplantation. Additional areas of focus for clinical development
include an investigator-led Phase I/II Chronic Graft versus Host Disease, or cGVHD, study in Israel, and an Acute Radiation Syndrome,
or ARS, program under the U.S. Food and Drug Administration, or FDA, animal rule. We believe that each of these indications represents
a severe unmet medical need.
We were incorporated in Nevada
on May 11, 2001. Pluri Inc. has a wholly owned subsidiary, Pluri Biotech Ltd., or the Subsidiary, previously named Pluristem Ltd., which
is incorporated under the laws of the State of Israel. In January 2020, the Subsidiary established a wholly owned subsidiary, Pluristem
GmbH, which is incorporated under the laws of Germany. In January 2022, the Subsidiary established an additional subsidiary, Plurinuva
Ltd., or Plurinuva, which is incorporated under the laws of Israel, which followed the execution of the collaboration agreement with Tnuva
.
On July 26, 2022, we completed
our legal entity name change from Pluristem Therapeutics Inc. to Pluri Inc., by merging a wholly-owned
subsidiary with and into the Company, with us being the surviving corporation. The name change reflects a broader strategy of leveraging
our 3D cell expansion technology to develop innovative cell-based products that can be harnessed for a range of fields beyond medicine,
providing solutions for various areas of life. Effective July 26, 2022, our Nasdaq ticker symbol was changed to “PLUR.”
Scientific Background
Cell therapy is an established
field within the regenerative medicine area. The characteristics and properties of cells vary as a function of tissue source and growth
conditions. The human placenta from which our PLX cells are derived provides an uncontroversial source of non-embryonic, adult cells and
represents an innovative approach in the cell therapy field. The different factors that PLX cells release suggest that the cells can be
used therapeutically for a variety of ischemic, inflammatory, autoimmune and hematological deficiencies.
PLX cells exhibit low immunogenicity,
thus do not require tissue matching prior to administration, which allows the development of ready-to-use / “off-the-shelf”
allogeneic products.
Our Technology
Our PLX cells are adherent
stromal cells that are expanded using a proprietary three-dimensional, or 3D, process. This system utilizes a synthetic scaffold to create
an artificial 3D environment where placental-derived stromal cells can grow. Our automated proprietary 3D, cGMP approved, process enables
the large-scale monitored and controlled production of reproducible, high quality cell products and can manufacture a large number of
PLX doses. Additionally, our current manufacturing process, which has scaled up during the years, has demonstrated batch-to-batch consistency,
an important manufacturing challenge for biological products.
Our technology platform, a patented and validated
state-of-the-art 3D cell expansion system, aims to advance novel cell-based solutions for a range of initiatives, including, but not limited
to, pharmaceuticals, climate change, food security and animal welfare. Our method is uniquely accurate, scalable, cost-effective, and
consistent from batch to batch. Our technology is currently implemented in the fields of regenerative medicine and food-tech.
Product Candidates
We believe that our technology
will continue to fuel medical research and develop pharmaceuticals, while also being used to potentially create novel cell-based solutions
for other innovative initiatives—such as food-tech, agri-tech, and biologics. We aim to establish partnerships that leverage our
3D cell-based technology to additional industries that require effective, mass cell production.
Pluri Health
Our primary objective is to
be the leading provider of allogeneic placenta-based cell therapy products that are true off-the-shelf products that do not require any
matching or additional manipulation prior to administration. Currently, our PLX products are administered intramuscular, or IM, using
a standard needle and syringe.
PLX-PAD
Our first product candidate,
PLX-PAD, is composed of maternal cells originating from the placenta. PLX-PAD is used in a Phase III multinational clinical study in recovery
following surgery for hip fracture.
PLX-PAD is also under clinical
development in collaboration with Tel Aviv Sourasky Medical Center (Ichilov Hospital) through an investigator-initiated Phase I/II study
for the treatment of Steroid-Refractory cGVHD.
PLX-R18
Our second product candidate,
PLX-R18, is composed of fetal cells originating from the placenta.
We have completed our first
in human Phase I clinical study in incomplete hematopoietic recovery following hematopoietic cell transplantation, or HCT, in the United
States and Israel.
Through our collaboration
in the United States with the National Institutes of Health, or NIH, and the U.S. Department of Defense, or DoD, we are also developing
a solution for ARS following or before exposure to massive radiation via the FDA Animal Rule regulatory pathway.
Modified PLX cells
In the last decade, we developed
an allogeneic platform based on cells originated from the fetal and maternal cell from the placenta, and by using this platform we can
produce large quantities of high-quality cells in automated and robust manufacturing process suitable for cGMP environment. As a platform
technology company, we are currently developing additional product candidates, which are modified or induced PLX cells:
Induced PLX cells: we are
using cells from the placenta, induced with cytokines, to transiently alter their secretion profile.
Modified PLX cells using CRISPR,
or other gene editing technology: CRISPR is a unique technology which allows precise gene editing of cells. Using this technology, we
can initiate the next evolution in cell therapy by allowing the reprograming of cells for specific needs. Our aim is to incorporate the
genetic engineering techniques into our cell manufacturing platform in order to develop large scale allogenic engineered PLX products
designed for specific indications.
We believe that using the
placenta as a unique cell source, combined with our innovative research, development and high-quality manufacturing capabilities, will
be the “engine” that drives this platform technology towards the successful development of additional PLX cell therapy products
and indications.
Our Clinical Development Product Candidates
Orthopedic Indications.
Following FDA and European Medicine Agency, or EMA, clearance, a multinational Phase III study is currently being conducted in the United
States, Europe and Israel. The primary endpoint of this study is the Short Physical Performance Battery, or SPPB, a test for lower limb
performance and functional status. We completed enrollment of 240 patients and the study was designed
to assess the efficacy at six months and a year, as well as safety for up to two years.
On
July 13, 2022, we announced topline results from our Phase III study of muscle regeneration following hip fracture surgery. PLX-PAD
was demonstrated to be an effective accelerator of muscle strength and regeneration. A significant increase in Hip Abduction Strength
(HAS) was observed at week 26 and week 52 for patients treated with PLX-PAD (n=120), in the injured leg (p=0.047, p=0.0022) and uninjured
leg (p=0.073, p=0.0046) compared to placebo (n=120). The study did not meet the primary endpoint, which was the SPPB test at week 26.
The study will continue to follow up with patients for up to 52 weeks for safety and other efficacy measures.
Our Phase III study
protocol and design was based on our phase I/II, randomized, double-blind, placebo-controlled study (n=20) to assess the safety and efficacy
of IM injections of allogeneic PLX-PAD cells for the regeneration of injured gluteal musculature after total hip replacement had been
conducted in Germany under the approval of PEI. In this study, PLX-PAD cells or placebo were administered into the traumatized gluteal
muscle during total hip replacement surgery. The study results met its primary efficacy endpoint, change in maximal voluntary isometric
contraction force of the gluteal muscle at six months after total hip replacement. Patients treated with PLX-PAD had a significantly greater
improvement of maximal voluntary muscle contraction force than the placebo group (p=0.0067). In addition, the study demonstrated that
PLX-PAD was safe and well tolerated by patients.
COVID-19 Complicated by
ARDS. In May 2020, the FDA cleared our Investigational New Drug Application, or IND, for a Phase II study of our PLX-PAD cells for
treatment of severe COVID-19 cases complicated by ARDS and we initiated the study in June 2020. The U.S. study is a randomized, double-blind,
placebo-controlled, multicenter, parallel-group intended to evaluate the efficacy and safety of IM injections of PLX-PAD for the treatment
of severe COVID-19 cases complicated by ARDS. The primary endpoint is the number of ventilator free days, or
VFD, from day 1 through day 28 of the study. Secondary efficacy endpoints include all-cause mortality, duration of mechanical ventilation,
ICU free-days, and hospitalization free-days. Safety and survival follow-up will be conducted until week 52. In addition, the FDA has
cleared our Expanded Access Program, or EAP, for the use of our PLX-PAD cells to treat ARDS caused by COVID-19 outside of the Phase II
COVID-19 complicated by ARDS study in the United States. The EAP approval was for up to 100 patients.
In August 2020, the PEI cleared
our Phase II study in Germany titled, “A Randomized, Controlled, Multicenter, Parallel-Group Phase II Study to Evaluate the Efficacy
and Safety of Intramuscular Injections of PLX PAD for the Treatment of severe COVID-19,” relating to the treatment of patients hospitalized
with severe cases of COVID-19 complicated by ARDS. The primary efficacy endpoint of the study is the number of ventilator free days during
the 28-days from day one through day 28 of the study. Secondary efficacy endpoints include all-cause mortality, duration of mechanical
ventilation, ICU free-days, and hospitalization free-days. Safety and survival follow-up will be conducted until week 52. We enrolled
patients in Europe and Israel under this protocol.
On July 8, 2021, we announced
that we were bringing our COVID-19 complicated by ARDS Phase II studies in the United States, Europe and Israel to clinical readout. The
analysis was based on 89 patients enrolled.
On
December 27, 2021, we announced topline results for our COVID-19 studies based on 89 patients enrolled. The studies did not meet the primary
efficacy endpoint of statistically significant improvement of VFD at 28 days. Taking into consideration the baseline risk factors of the
ARDS patients, no differences in the safety profile were observed between PLX-PAD and placebo. The U.S. study was recently completed,
and the second study conducted in Europe and Israel is planned for completion during the third calendar quarter of 2022.
Recovery Following HCT.
This Phase I study of PLX-R18 in HCT was completed in the United States and Israel. The study assessed the safety of PLX-R18 by assessing
adverse events, safety labs and vital signs in patients receiving different doses of PLX-R18. One year follow up for all patients was
completed in September 2021 and the results of the study were announced on March 23, 2022. PLX-R18 was well-tolerated with a favorable
safety profile. Patients treated with PLX-R18 showed a mean increase in all three blood cell types compared to baseline with platelets
(p<0.001), hemoglobin (p=0.01) and neutrophils (p=0.15) levels increasing as early as 1 month following PLX-R18 administration and
enduring up to 12 months following treatment. Additionally, the number of transfused units decreased from a mean monthly number of 5.09
for platelets and 2.91 for red blood cells at baseline to 0.55 for platelets (p=0.045) and 0 for red blood cells (p=0.0005) at 12 months.
Peripheral and Cardiovascular
Diseases. We investigated the use of PLX-PAD cells for the treatment of peripheral arterial disease, or PAD, including IC and CLI.
We completed two Phase I safety/dose-escalating clinical studies for CLI, one in the United States and one in Germany. These CLI studies
demonstrated that no blood type or human leukocyte antigen matching is required, and that the administration of PLX-PAD cells is safe,
even if two doses are administered to a patient on two different occasions. We completed a Phase II study in IC which was conducted in
the United States, Germany, South Korea and Israel. A total of 172 patients were treated in this study. IM administration of PLX-PAD cells
was concluded to be safe and well tolerated. We completed a pivotal Phase III study of PLX-PAD cells in the treatment of CLI for
patients with minor tissue loss (Rutherford Category 5) who are unsuitable for revascularization. This multinational Phase III study was
conducted in the United States, Europe and Israel and enrolled 213 patients in total. In December 2020, the independent Data Monitoring
Committee, or DMC, issued its recommendation letter following an interim analysis relating to the CLI Phase III study. A clinical dataset
was reviewed by the independent DMC for safety and analysis of the primary endpoint of amputation-free survival, defined as time to occurrence
of major amputation of the index leg or death. Based on the review, the DMC concluded that the CLI study was unlikely to meet the primary
endpoint by the time of the final analysis. Following the DMC’s recommendation, we decided to terminate the CLI study.
ARS. We have conducted
several animal studies for the evaluation of PLX-R18 for the treatment of ARS, in collaboration with the National Institute of Allergy
and Infectious Diseases, or the NIAID. The NIH funded and conducted a pilot study in non-human primates, or NHPs, to evaluate the therapeutic
effect of PLX-R18 on hematological aspects of ARS. In 2017, we announced results of the NHPs pilot study for PLX-R18 as a treatment for
ARS. Although study size was not designed to show significance, results showed a trend toward improved survival of PLX-R18 treated animals
compared to control, placebo treated animals. The study, conducted and funded by the NIAID, was designed to assess the safety and efficacy
of PLX-R18 following IM injection into irradiated and non-irradiated NHPs. Efficacy measures included survival as well as hematological
parameters which are affected by exposure to high levels of radiation as may occur in a nuclear accident or attack. These data will help
the design of a pivotal study to fulfill the requirements for a Biologics License Application, or BLA, submission under the FDA’s
Animal Rule regulatory pathway.
We plan to continue the discussions
with the different government agencies with the goal of receiving their support for pivotal studies in NHPs as well as conducting the
safety studies required in order to file a BLA for this indication.
In October 2017, we announced
that the FDA granted us an orphan drug designation for our PLX-R18 cell therapy for the prevention and treatment of ARS.
In April 2018, we announced
that the FDA approved our IND application for PLX-R18 cell therapy in the treatment of ARS. The IND allows us to treat victims who may
have been acutely exposed to high dose radiation due to nuclear attack or accident.
In July 2019, we presented positive results from a series of studies
of our PLX-R18 cell therapy product conducted by the DoD Armed Forces Radiobiology Research Institute, part of the Uniformed Services
University of Health Sciences. The studies were designed to evaluate PLX-R18 as a potential prophylactic countermeasure against ARS administered
prior to radiation exposure. These animal studies demonstrate that PLX-R18, administered 24 hours before radiation exposure, and again
72 hours after exposure, resulted in a significant increase in survival rates, from 4% survival rate in the placebo group to 74% in the
treated group. In addition, the data show an increase in recovery of blood lineages and a favorable safety profile. Furthermore, histopathological
analysis and hematopoietic progenitor clonogenic assay of tissues collected show a significant increase in bone marrow cell numbers and
improved regenerative capability into all blood lineages.
Steroid-Refractory cGVHD.
In September 2017, we signed an agreement with Tel Aviv Sourasky Medical Center (Ichilov Hospital) to conduct a Phase I/II clinical study
of PLX-PAD cell therapy for the treatment of Steroid-Refractory cGVHD. This study is an investigator-initiated study. As such, Tel Aviv
Sourasky Medical Center supports the study and is responsible for its design and implementation. 13 patients have been treated in this
study to date.
Regulatory and Clinical Affairs Strategy
Our cell therapy development
strategy is to hold open and frequent discussions with regulators at all stages of development from preclinical studies to more advanced
regulatory stages. We utilize this strategy in working with the FDA, the EMA, Germany’s PEI as well as other European national competent
authorities, the MOH, Japan’s Pharmaceuticals and Medical Devices Agency, or PMDA, and also the Ministry of Food and Drug Safety,
or MFDS, of South Korea.
Our Activities in the Food Tech Sector
On January 5, 2022, we signed
definitive collaboration agreements with Tnuva through the Subsidiary. Under the definitive
collaboration agreements, or the Joint Venture Agreement, we established a new company, Plurinuva, with the purpose of developing cultivated
meat products of all types and kinds. Plurinuva is intended to be engaged in the development, manufacturing and commercialization of technology,
know-how and products that will be based on licensed products, or the Licensed Products, relating to the field of cultivated meat, or
the Field.
Pursuant to the Joint Venture
Agreement, Tnuva entered into a share purchase agreement, or the SPA, with Plurinuva and the Subsidiary,
pursuant to which Plurinuva issued on the closing date of the SPA, or the Closing Date, 187,500 ordinary shares, representing 15.79% of
its share capital, to Tnuva, as well as a warrant to purchase additional shares of Plurinuva, in consideration of an aggregate of $7.5
million in cash. In addition, pursuant to the SPA, in the event the Company decides to use its technology for the development of cultivated
milk or fish products, Tnuva shall also have the right, for a period of seven years following the Closing Date, to participate in the
formation of additional separate joint ventures for the development of those products.
The first warrant, or the
First Warrant, issued to Tnuva permits Tnuva to purchase up to 125,000 ordinary shares of Plurinuva at an exercise price of $40.00 per
share and has a term commencing on the Closing Date and ending at the earlier of (i) six months from the Closing Date, (ii) immediately
prior to and subject to the consummation of an initial public offering or acquisition of Plurinuva or (iii) the consummation of a financing
round with a non-affiliated investor. In addition, on the six month anniversary of the Closing Date, and provided that the First Warrant
has not expired, Plurinuva shall issue to Tnuva a second warrant, or the Second Warrant, which will permit Tnuva to purchase up to a number
of ordinary shares of Plurinuva, or the then most senior securities issued by Plurinuva, in consideration for such amount equal to 200%
of the remaining balance of the aggregate purchase price of the First Warrant, provided that Tnuva exercises at least 62,500 ordinary
shares at a price per share of $40.00, or $2,500,000 in the aggregate, of the First Warrant. The Second Warrant’s exercise price
per share equals $76.00. The Second Warrant has a term commencing on the six months anniversary of the Closing Date and ending at the
earlier of (i) six months from its issuance, (ii) immediately prior to and subject to the consummation of an initial public offering or
acquisition of Plurinuva or (iii) the consummation of a financing round with a non-affiliated investor. On August 23, 2022, the First
Warrant was extended for an additional 90-day period, so that the exercise period will end on November 22, 2022.
On
February 24, 2022, we announced the closing of the Joint Venture Agreement and the SPA, and on March 8, 2022, we announced the appointment
of Eyal Rosenthal as Chief Executive Officer of Plurinuva.
Prior to the Closing Date,
the Subsidiary and Plurinuva also executed a technology license agreement, or the License Agreement, and on the Closing Date, the Subsidiary
and Plurinuva executed a transitional services agreement, or the Services Agreement. Pursuant to the License Agreement, the Subsidiary
granted Plurinuva an exclusive, royalty bearing, perpetual and irrevocable, worldwide, non-transferable (except under specific circumstances
specified thereunder), sublicensable license to its technology for the use in the development of the Licensed Products in the Field. In
addition, Plurinuva granted the Subsidiary, pursuant to the License Agreement, an exclusive, perpetual and irrevocable, worldwide, sublicensable,
royalty-free, license to use, make, exploit and develop the improvements made by Plurinuva to the licensed technology outside of the Field.
In consideration for the license, Plurinuva agreed to pay the Subsidiary royalties from its future net sales in the mid-single digits.
Pursuant to the terms of the Services Agreement, the Subsidiary shall provide Plurinuva transitional services to support its development
efforts, for an initial term of eighteen months, subject to mutual extension for an additional six months.
Pursuant to the SPA, Tnuva
and Plurinuva agreed to enter into a commercialization agreement within twelve months pursuant to which Tnuva shall be granted exclusive
marketing, distribution and sale rights of the Licensed Products in Israel. Tnuva’s exclusivity in the region will be subject to
achieving and maintaining specific milestones. Plurinuva shall retain exclusive worldwide marketing, distribution, and sale rights for
the Licensed Products worldwide, except in Israel.
Intellectual Property
We understand that our success
will depend, in part, on maintaining our intellectual property, and therefore we are committed to protecting our technology and product
candidates with patents and other methods described below.
We are the sole owner of 137
issued patents and approximately 64 pending patent applications in the United States, Europe, China, Japan and Israel, as well as in additional
countries worldwide, including countries in the Far East and South America (in calculating the number of issued patents, each European
patent validated in multiple jurisdictions was counted as a single patent).
Based on the well-established
understanding that the characteristics and therapeutic potential of a cell product are largely determined by the source of the cells and
by the methods and conditions used during their culturing, our patent portfolio includes different types of claims that protect the various
unique aspects of our technology.
Our multi-national portfolio of patent and patent
applications includes the following claims:
| |
● |
our proprietary expansion methods for 3D stromal cells and plant cells; |
| |
● |
composition of matter claims covering the cells; |
| |
● |
the therapeutic and cosmetic use of PLX cells for the treatment of a variety of conditions; and |
| |
● |
cell-culture, harvest, thawing and formulation devices. |
Through our experience with
adherent stromal cell-based product development, we have developed expertise and know-how in this field and have established procedures
for manufacturing clinical-grade PLX cells in our facilities. Certain aspects of our manufacturing process are covered by patents and
patent applications. In addition, specific aspects of our technology are retained as know-how and trade secrets that are protected by
our confidentiality agreements with our employees, consultants, contractors, manufacturers and advisors. These agreements generally provide
for protection of confidential information, restrictions on the use of materials, and an obligation to assign to us inventions conceived
during the course of performing services for us.
The following table sets forth
our key patents and patent applications and is not intended to represent an assessment of claims, limitations or scope. In some cases,
a jurisdiction is listed as both pending and granted for a single patent family. This is due to pending continuation or divisional applications
of the granted case.
The expiration dates of these
patents, based on filing dates, range from 2027 to 2041. Actual expiration dates will be determined according to extensions received based
on the Drug Price Competition and Patent Term Restoration Act of 1984 (P.L. 98-417), commonly known as the “Hatch-Waxman”
Act, which permits extensions of pharmaceutical patents to reflect regulatory delays encountered in obtaining FDA market approval. The
Hatch-Waxman Act is based on a U.S. federal law and therefore only relevant to U.S. patents.
There is a risk that our patents
will be invalidated, and that our pending patent applications will not result in issued patents. We also cannot be certain that we will
not infringe on any patents that may be issued to others. See “Risk Factors - We must further protect and develop our technology
and products in order to become a profitable company.”
Our Patent Portfolio
| Patent
Name/ Int. App. No. |
|
Pending
Jurisdictions |
|
Granted
Jurisdictions |
|
Expiry
Date |
METHODS
FOR CELL EXPANSION AND USES OF CELLS AND CONDITIONED MEDIA PRODUCED THEREBY FOR THERAPY
PCT/IL2007/000380 |
|
China, Hong Kong |
|
Australia, Canada, China, Hong Kong, Europe, Israel,
India, Japan, South Korea, Mexico, Russia, Singapore |
|
March 23, 2027 |
ADHERENT
CELLS FROM PLACENTA TISSUE AND USE THEREOF IN THERAPY
PCT/IL2008/001185 |
|
United States, Israel |
|
Australia, Brazil, Canada, China, Europe, Hong Kong,
Israel, India, Japan, Mexico, Russia, United States, South Korea |
|
September 2, 2028 |
METHODS
OF TREATING INFLAMMATORY COLON DISEASES
PCT/IL2009/000527 |
|
|
|
United States, Israel, Russia |
|
May 26, 2029 |
METHODS
OF SELECTION OF CELLS FOR TRANSPLANTATION
PCT/IL2009/000844 |
|
|
|
Europe, Israel |
|
September 1, 2029 |
ADHERENT
CELLS FROM PLACENTA TISSUE AND USE THEREOF IN THERAPY
PCT/IL2009/000846 |
|
|
|
Australia, Canada, China, Europe, Hong Kong, Israel,
India, Mexico, Russia, Singapore, United States |
|
September 1, 2029 |
ADHERENT
CELLS FROM PLACENTA TISSUE AND USE THEREOF IN THERAPY
PCT/IL2009/000845 |
|
|
|
United States, Europe, Israel |
|
September 1, 2029 |
ADHERENT
STROMAL CELLS DERIVED FROM PLANCENTAS OF MULTIPLE DONORS AND USES THEREOF
PCT/IB2011/001413 |
|
United States |
|
Israel |
|
Israel:
April 21, 2031
U.S:
March 22, 2027 |
ADHERENT
CELLS FROM PLACENTA AND USE OF SAME IN DISEASE TREATMENT
PCT/IB2010/003219 |
|
United States, Israel |
|
Australia, Canada, China, Hong Kong, Europe, Israel,
Mexico, New Zealand, United States |
|
November 29, 2030 |
|
METHODS AND SYSTEMS FOR HARVESTING ADHERENT STROMAL CELLS
PCT/IB2012/000933 |
|
China, Israel |
|
Australia, Canada, Europe, Israel, India, South Korea, Mexico, Singapore, United States |
|
April 15, 2032 |
|
METHODS FOR TREATING RADIATION OR CHEMICAL INJURY
PCT/IB2012/000664 |
|
United States |
|
Europe, Hong Kong, Israel, Japan, South Korea, United States |
|
March 22, 2032 |
|
SKELETAL MUSCLE REGENERATION USING MESENCHYMAL STEM CELLS
PCT/EP2011/058730 |
|
|
|
United States, Europe, Israel |
|
May 27, 2031 |
|
GENE AND PROTEIN EXPRESSION PROPERTIES OF ADHERENT STROMAL CELLS
CULTURED IN 3D
PCT/IB2014/059114 |
|
|
|
Israel, United States |
|
February 20, 2034 |
|
DEVICES AND METHODS FOR CULTURE OF CELLS
PCT/IB2013/058184 |
|
|
|
United States, Israel |
|
August 31, 2033 |
|
METHODS FOR PREVENTION AND TREATMENT OF PREECLAMPSIA
PCT/IB2013/058186 |
|
|
|
China, Hong Kong, Europe, Israel, Japan, South Korea, United States |
|
August 31, 2033 |
|
METHOD AND DEVICE FOR THAWING BIOLOGICAL MATERIAL
PCT/IB2013/059808 |
|
China |
|
Australia, China, Europe, Hong Kong, Israel, India, Japan, South Korea, Russia, Singapore, United States |
|
October 31, 2033 |
|
SYSTEMS AND METHODS FOR GROWING AND HARVESTING CELLS
PCT/IB2015/051559 |
|
|
|
Israel, United States |
|
March 3, 2035 |
|
METHODS AND COMPOSITIONS FOR TREATING AND PREVENTING MUSCLE WASTING
DISORDERS
PCT/IB2015/059763 |
|
|
|
Israel, United States |
|
December 18, 2035 |
|
USE OF ADHERENT STROMAL CELLS FOR ENHANCING HEMATOPOIESIS IN A SUBJECT
IN NEED THEREOF
PCT/IB2016/051585 |
|
United States, Israel |
|
|
|
March 21, 2036 |
|
ALTERED ADHERENT STROMAL CELLS AND METHODS OF PRODUCING AND USING
SAME
PCT/IB2016/053310 |
|
Europe, China, Israel |
|
Europe, United States |
|
June 6, 2036 |
|
METHODS AND COMPOSITIONS FOR TREATING CANCERS AND NEOPLASMS
PCT/IB2017/050868 |
|
United States, Japan, Canada, Israel |
|
Europe, Japan |
|
February 16, 2037 |
|
METHODS AND COMPOSITIONS FOR TREATING NEUROLOGICAL DISORDERS
PCT/IB2018/052806 |
|
Israel, United States |
|
|
|
April 23, 2038 |
|
METHODS AND COMPOSITIONS FOR TUMOR ASSESSMENT
PCT/IB2018/050984 |
|
United States |
|
Israel |
|
February 18, 2038 |
|
METHODS AND COMPOSITIONS FOR TREATING ADDICTIONS
PCT/IB2018/055473 |
|
Israel, United States |
|
|
|
July 23, 2038 |
|
METHODS AND COMPOSITIONS FOR DETACHING ADHERENT CELLS
Germany 10 2018 115 360.0 |
|
Germany |
|
|
|
June 25-July 3, 2038 |
| DRUG CONTAINING HUMAN PLACENTA-ORIGIN MESENCHYMAL CELLS AND PROCESS FOR PRODUCING VEGF USING THE CELLS JP20030579842 |
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Japan |
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March 28, 2023 |
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METHODS AND COMPOSITIONS FOR PRODUCING CANNABINOIDS
PCT/IL2020/050477 |
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Canada, Europe, Hong Kong, Israel, Japan, United States |
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April 28, 2040 |
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METHODS FOR EXPANDING ADHERENT STROMAL CELLS AND CELLS OBTAINED
THEREBY
PCT/IB2019/052569 |
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Israel, Singapore, United States |
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March 28, 2039 |
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METHODS AND COMPOSITIONS FOR TREATING SUBJECTS EXPOSED TO VESICANTS
AND OTHER CHEMICAL AGENTS
PCT/IB2019/055074 |
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Israel, United States |
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June 18, 2039 |
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METHODS AND COMPOSITIONS FOR FORMULATING AND DISPENSING PHARMACEUTICAL
FORMULATIONS
PCT/IB2019/053115 |
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United States |
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Israel |
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United States: April 16, 2039
Israel: April 26, 2038 |
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THERAPEUTIC DOSAGE REGIMENS COMPRISING ADHERENT STROMAL CELLS
PCT/IB2019/054828 |
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Israel, United States |
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June 10, 2039 |
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MODULAR BIOREACTOR
PCT/IB2019/058429 |
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Europe, Israel, Hong Kong, South Korea, Singapore, United States |
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October 3, 2039 |
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THERAPEUTIC METHODS AND COMPOSITIONS
PCT/IB2019/059544 |
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Israel, United States |
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November 6, 2039 |
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METHODS AND COMPOSITIONS FOR TREATING VIRAL INFECTIONS AND SEQUELAE
THEREOF
PCT/IL2021/050268 |
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PCT, United States, Europe,
Israel, Mexico |
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Israel |
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First Israeli application: May 14, 2040
Other applications: March 11, 2041 |
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METHODS AND COMPOSITIONS FOR AESTHETIC AND COSMETIC TREATMENT AND
STIMULATING HAIR GROWTH
PCT/IL2020/050363 |
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United States, Europe,
Canada, China, Japan, Israel, Australia |
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March 26, 2040 |
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METHODS FOR EXPANDING ADHERENT STROMAL CELLS AND CELLS OBTAINED
THEREBY
IL277560 |
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Israel |
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September 23, 2040 |
On January 8, 2022, we entered
into a definitive license agreement with Takeda Pharmaceuticals International AG, or Takeda, a company based in Switzerland, which operates
in the field of adipose-derived cells, pursuant to which we granted Takeda a global, non-exclusive license to use several of our patents
(EP2591789, EP3103463, and 3091071), limited to adipose fat cells only, in the field of therapeutics, in exchange for Takeda ceasing its
opposition with regards to said patents and paying us a lump sum of $200,000. The license covers methods for expanding adherent stromal
cells and specified second medical uses.
On January 10, 2022, we entered
into a definitive license agreement with Novadip Biosciences, or Novadip, a company based in Belgium, which operates in the field of adipose-derived
stem cells for cell therapy and cell-free therapy in respect of medical or cosmetic conditions, under which we granted Novadip a global,
non-exclusive, royalty free license to use two of our patents (EP2591789, EP3103463), limited to non-placental cells and cell-derived
therapies, sub-licensable only to Novadip’s customers.
In April 2016, the Subsidiary
entered into a licensing agreement with TES Holdings Co., Ltd., a venture company derived from the University of Tokyo, to obtain a key
patent in Japan to cover the treatment of ischemic diseases with placental cell therapy. This license is subject to future single low-digit
royalties from sales of our product for treatment in the field of ischemic diseases in Japan, until expiry of the patent in 2023. This
license is in addition to the grant of 13 patents to us by the Japanese Patent Office, which address three dimensional methods for expanding
placental and adipose cells, and specified cell therapies produced from placental tissue using these methods and bedside thawing devices.
Research and Development
Foundational Research
Our initial technology, the
PluriX™ Bioreactor system, was invented at the Technion – Israel Institute of Technology’s Rappaport Faculty of Medicine,
in collaboration with researchers from the Weizmann Institute of Science. This technology was acquired by us and has been further significantly
developed by our research and development teams over the ensuing years.
Collaborations and Ongoing Research and Development Plans
Charité Agreement
In July 2007, we entered into
a five-year collaborative research agreement with the Berlin-Brandenburg Center for Regenerative Therapies at Charité – University
Medicine Berlin, or Charité, which was extended from time to time through June 2027. We and Charité are collaborating on
a variety of indications utilizing PLX cells. According to the agreement, we will be the exclusive owner of the technology and any products
produced as a result of the collaboration. Charité will receive between 1% to 2% royalties from net sales of new developments that
have been achieved during the joint development.
Fukushima Medical University
We signed an MOU for a collaboration with Fukushima Medical University,
Fukushima Global Medical Science Center. The purpose of the collaboration is to develop our PLX-R18 cells for the treatment of ARS, and
for morbidities following radiotherapy in cancer patients. The collaboration will proceed alongside research supported by the NIH, which
is studying PLX-R18 as a potential treatment for the hematologic component of ARS. The MOU for a collaboration with Fukushima will be
renewed automatically on a yearly basis. Each party is entitled to terminate the agreement for convenience upon providing the other party
30 days prior notice.
CHA Agreement
On June 26, 2013, we entered
into an exclusive out-licensing and commercialization agreement, or the CHA Agreement, with CHA for conducting clinical studies and commercialization
of our PLX-PAD product candidate in South Korea in connection with two indications: the treatment of CLI and IC. We will continue to retain
rights to our proprietary manufacturing technology and cell-related intellectual property.
The first clinical study that
was performed as part of the CHA Agreement was a Phase II study in IC. Upon the first regulatory approval for a PLX product in South Korea,
if granted, for the specified indications, we and CHA will establish an equally owned joint venture with the purpose of commercializing
PLX cell products in South Korea. Additionally, we will be able to use the data generated by CHA to pursue the development of PLX product
candidates outside of South Korea.
The term of the CHA Agreement
extends from June 24, 2013 until the later of the expiration, lapse, cancellation, abandonment or invalidation of the last valid patent
claim covering the development of the product indications. The CHA Agreement contains customary termination provisions, including in the
event that the parties do not reach an agreement upon a development plan for conducting the clinical studies.
Upon termination of the CHA
Agreement, the license granted thereunder will terminate, and all rights included therein will revert to us, whereupon we will be free
to enter into agreements with any other third parties for the granting of a license in or outside South Korea or to deal in any other
manner with such rights as it shall see fit in our sole discretion.
Horizon 2020
The Phase III study of PLX-PAD
in CLI was conducted as a collaborative project carried out by an international consortium led by the Berlin-Brandenburg Center for Regenerative
Therapies, together with the Company and with the participation of additional third parties.
Our Phase III study of PLX-PAD
cell therapy in the treatment of muscle recovery following surgery for hip fracture is a collaborative project carried out by an international
consortium led by Charité, together with us and with the participation of additional third parties.
In October 2017, we entered
into a collaborative project, the nTRACK, carried out by an international consortium led by Leitat. The aim of this project is to examine
gold nano particles labeling of stem cells to enable assessment of cells’ in vivo persistence and distribution in correlation to
biological efficacy. Under the project, PLX cells, labeled and non-labeled will be characterized and examined in animal models for muscle
injury.
Horizon Europe
On September 6, 2022, we announced
that a €7.5 million non-dilutive grant from the European Union’s Horizon program has been awarded to PROTO (Advanced PeRsOnalized
Therapies for Osteoarthritis), an international collaboration led by Charité Berlin Institute of Health Center for Regenerative
Therapies. The goal of the PROTO project is to utilize our PLX-PAD cells in a Phase I/IIa study for the treatment of mild to moderate
knee osteoarthritis. Final approval of the grant is subject to completion of the consortium and Horizon Europe grant agreements. The funds
from the grant are expected to be allocated between Pluri and other members of the consortium in accordance with budget and work packages
which will be determined by the consortium.
The Phase I/IIa study will
be carried out by Charité. We, together with an international consortium under the leadership of Professor Tobias Winkler, Principal
Investigator, at the Berlin Institute of Health Center of Regenerative Therapies, Julius Wolff Institute and Center for Musculoskeletal
Surgery
Indiana University
In April 2018, NIAID awarded
a $2.5 million grant to Indiana University to conduct, together with us, studies of our PLX-R18 cell therapy in the treatment of ARS.
The goal of this project is to extend the PLX-R18 ARS studies to include examination of survival in pediatric and geriatric populations
as well as the ability of PLX-R18 to alleviate delayed effects of radiation in survivors.
Chart Industries
In November 2018, we entered
into a license agreement with a subsidiary of Chart Industries, Inc., or Chart, regarding our thawing device for cell-based therapies.
Pursuant to the terms of the agreement, Chart obtained the exclusive rights to manufacture and market the thawing device in all territories
worldwide, excluding Greater China, and we are to receive royalties from sales of the product and supply of an agreed upon number of thawing
devices. Royalties shall commence on the date of Chart’s first commercial sale of the thawing device.
NASA
In February 2019, we entered
a collaboration with NASA’s Ames Research Center to evaluate the potential of our PLX cell therapies in preventing and treating
medical conditions caused during space missions.
U.S. Department of Defense
In August 2017, we announced
that a pilot study of our PLX-R18 cell therapy was initiated by the DoD. The study examined the effectiveness of PLX-R18 as a treatment
for ARS prior to, and within the first 24 hours of exposure to radiation. In July 2019, we presented positive results from a series of
studies of our PLX-R18 cell therapy product conducted by the DoD.
RESTORE
We are members of a large-scale
research initiative, the RESTORE project which has received funding of €1,000,000 (approximately $1,100,000) from the European Union’s
Horizon 2020 research and innovation program, to submit a full grant application for the development and advancement of transformative
therapeutics. Currently, due to COVID-19, there is no open call for full proposal. The members of the RESTORE project continue to collaborate
in attempt to collectively submit the grant application once such call is available.
CRISPR-IL
In June 2020, we announced that we were selected as a member of the
CRISPR-IL consortium, a group funded by the IIA. CRISPR-IL brings together the leading experts in life science and computer science from
academia, medicine, and industry, to develop Artificial Intelligence, or AI, based end-to-end genome-editing solutions. These next-generation,
multi-species genome editing products for human, plant, and animal DNA, have applications in the pharma, agriculture, and aquaculture
industries. CRISPR-IL is funded by the IIA with a total budget of approximately $10,000,000 of which, an amount of approximately $480,000
was a direct grant allocated to us, for an initial period of 18 months, with a potential for extension of an additional 18 months, or
the Second Period, with additional budget from the IIA.
In October 2021, we received
approval for an additional grant of approximately $583,000 from the IIA pursuant to the CRISPR-IL consortium program, for an additional
period of eighteen months.
The CRISPR-IL consortium program does not require
us to pay royalties to the IIA.
United Arab Emirates-based Abu Dhabi Stem Cells
Center
In August 2020, we signed
a non-binding MOU with the United Arab Emirates-based Abu Dhabi Stem Cells Center, a specialist healthcare center focused on cell therapy
and regenerative medicine. The aim of the collaboration is to capitalize on each party’s respective areas of expertise in cell therapies.
The parties have agreed to exchange research results, share samples, join usage of equipment and testing, and other essential activities
related to advancing the treatment and research of cell therapies for a broad range of medical conditions.
In-House Clinical Manufacturing
We have the in-house capability
to perform clinical cell manufacturing. Our state-of-the-art Good GMP grade manufacturing facility in Haifa has been in use since February
2013 for the main purpose of clinical grade, large-scale manufacturing. The facility’s new automated manufacturing process and products
were approved for production of PLX-PAD for clinical use by the FDA, EMA, MFDS, PMDA and the MOH. Our second product, PLX-R18, was cleared
by the FDA and the MOH for clinical use. Furthermore, the site was inspected and approved by a European Union qualified person (European
accreditation body), approving that the site and production processes meet the current GMP for the purpose of manufacturing clinical grade
products.
The site was also inspected
and approved by the MOH and we received a cGMP Certification and manufacturer-importer authorization.
We obtain the human placentas
used for our research and manufacturing activities from various hospitals in Israel after receiving a written informed consent by the
mother and pathogen clearance. Any medical waste related to the use of placentas is treated in compliance with local environmental laws
and standards.
We have developed a serum-free
formulation to support the manufacturing of cell therapy products. This serum-free formulation was developed using our deep understanding
in cell therapy industrial scale production standards, and the quality methods designed to support implementation in Phase III development
and marketing. Achieving this significant technological challenge is expected to provide us with large-scale, highly consistent production
capacity with operational independency from third party suppliers for standard serum, an expensive and quantity limited product. PLX-R18
is the first product candidate manufactured using the serum-free media.
Government Regulation
The development, manufacturing,
and future marketing of our cell therapy product candidates are subject to the laws and regulations of governmental authorities in the
United States, Europe and Israel, as well as other countries in which our products may be marketed in the future like Japan, and South
Korea. In addition, the manufacturing conditions are specifically inspected by the MOH.
The FDA and the EMA must approve
products prior to marketing. Furthermore, various governmental statutes and regulations also govern or influence testing, manufacturing,
safety, labeling, storage and record keeping related to such products and their marketing. Governments in other countries have similar
requirements for testing and marketing.
The process of obtaining these
approvals and the subsequent compliance with appropriate statutes and regulations require the expenditure of substantial time, resources
and money. There can be no assurance that our product candidates will ultimately receive marketing approval, or, if approved, will be
reimbursed by public and private health insurance.
There are several stages every drug undergoes during
its development process. Among these are:
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Performance of nonclinical laboratory and animal studies to assess a drug’s biological activity and to identify potential safety concerns, and to characterize and document the product’s chemistry, manufacturing controls, formulation, and stability. In accordance with regulatory requirements, nonclinical safety and toxicity studies are conducted under Good Laboratory Practice, requirements to ensure their quality and reliability; |
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The manufacture of the product according to GMP regulations and standards; |
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Conducting adequate and well-controlled human clinical studies in compliance with Good Clinical Practice, or GCP, to establish the safety and efficacy of the product for its intended indication; and |
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Potential post-marketing clinical testing and surveillance of the product after marketing approval, which can result in additional conditions on the approvals or suspension of clinical use. |
Approval of a drug for clinical
studies in humans and approval of marketing are sovereign decisions of states, made by national, or, in case of the European Union, international
regulatory competent authorities.
The Regulatory Process in the United States
In the United States, our
product candidates are subject to regulation as a biological product under the Public Health Service Act and the Federal Food, Drug and
Cosmetic Act. The FDA, regulating the approval of clinical studies and marketing applications in the United States, generally requires
the following steps prior to approving a new biological product for use either for clinical studies or for commercial sale:
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Submission of an IND Application, which must become effective before clinical testing in humans can begin; |
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Obtaining approval of Institutional Review Boards, or IRBs, of research institutions or other clinical sites to introduce the drug candidate into humans in clinical studies; |
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FDA may grant approval for EAP prior to the completion of clinical studies, in order to allow access for the investigational drug, for patients that are excluded from the study; |
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FDA may grant priority review status to expedite the BLA review process. Obtaining a Fast Track designation allows access for the request of priority review; |
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Submission of a BLA for marketing authorization of the product, which must include adequate results of pre-clinical testing and clinical studies; |
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Submission of BLA with a proof of efficacy that is based only on animal studies is feasible in instances where human efficacy studies cannot be conducted because the conduct of such studies is unethical and field studies after an accidental or deliberate exposure are not feasible; |
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FDA review of the BLA in order to determine, among other things, whether the product is safe and effective for its intended uses; and |
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FDA inspection and approval of the product manufacturing facility at which the product will be manufactured. |
The Regulatory Process in Europe
In the European Union, our
investigational cellular products are regulated under the Advanced Therapy Medicinal Product regulation, a regulation specific to cell
and tissue products. Additionally, as of January 31, 2022, conducting clinical studies within EMA countries is subject to clinical trials
regulation. This European Union regulation requires:
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Filing a Central Clinical Trial Application utilizing the Clinical Trials Information System (CTIS) and obtaining an assessment and approval; |
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Obtaining approval of local and central ethics committees as required to test the investigational product into humans in clinical studies; |
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Conducting adequate and well-controlled clinical studies to establish the safety and efficacy of the investigational product for its intended use; and |
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Since our investigational cellular products are regulated under the Advanced Therapy Medicinal Product regulation, the application for marketing authorization to the EMA is mandatory within the 28 member states of the European Union. The EMA is expected to review and approve the MAA. |
In May 2015, we were selected by the
EMA for development of PLX-PAD cells via the EMA Adaptive Pathways Project.
Other Regulations
In general, the approval procedure
varies among countries, and may involve additional preclinical testing and clinical studies. The requirements and time required may differ
from those required for FDA or EMA approval. Each country may impose certain procedures and requirements of its own. Most countries other
than the United States, the European Union and Japan are willing to consider requests for marketing approval only after the product had
been approved for marketing by either the FDA, the EMA or the PMDA. The decision regarding marketing approval is made following the submission
of a dossier that is thoroughly assessed and critically addressed.
In Japan, we have completed
the required regulatory interactions with the PMDA, prior to the submission of clinical study notification, in the framework of the new
regulations for regenerative therapy effective in November 2014, which promote expedited approval for regenerative therapies that are
being developed for seriously debilitating/life-threatening indications.
Clinical Studies
Typically, in the United States,
as well as in the European Union, clinical development involves a three-phase process, although the phases may overlap. Phase I,
clinical studies are conducted in a small number of healthy volunteers, or patients in cases of ethical issues with using healthy volunteers
and are designed to provide information about product safety and to evaluate the pattern of drug distribution and metabolism within the
body.
Phase II clinical studies
are conducted in a homogenous group of patients afflicted with the specific target disease, to explore preliminary efficacy, optimal dosages
and confirm the safety profile. In some cases, an initial study is conducted in patients to assess both preliminary efficacy and preliminary
safety and patterns of drug metabolism and distribution, in which case it is referred to as a Phase I/II study. Phase III clinical
studies are generally large-scale, multi-center, controlled studies conducted with a heterogeneous group of patients afflicted with the
target disease, aiming to provide statistically significant support of efficacy, as well as safety and potency. The Phase III studies
are considered confirmatory for establishing the efficacy and safety profile of the drug and are critical for approval. In some circumstances,
a regulatory agency may require Phase IV, or post-marketing studies in case additional information needs to be collected after the
drug is on the market.
During all phases of clinical
development, regulatory agencies require extensive monitoring and auditing of all clinical activities, clinical data and clinical study
sites investigators to minimize risks and ensure high quality and integrity of the collected data. The sponsor of a clinical study is
required to submit an annual safety report to the relevant regulatory agencies, in which serious adverse events are reported, and also
to submit in an expedited manner any individual serious adverse events that are suspected to be related to the tested drug and are unexpected
with its use. An agency may, at its discretion, re-evaluate, alter, suspend, or terminate the clinical study based upon the data that
have been accumulated to that point and its assessment of the risk/benefit ratio to the patient.
Employees
As of June 30, 2022, we employed
a total of 154 full-time employees and 5 part-time employees, of whom, 128 full-time employees and 5 part-time employees are engaged in
research and development, manufacturing and clinical development.
As of August 30, 2022, we
employed a total of 129 full-time employees and 6 part-time employees, of whom, 102 full-time employees and 6 part-time employees are
engaged in research and development, manufacturing and clinical development.
The reduction in the number
of our employees was part of an efficiency and cost reduction plan we initiated in June 2022.
Competition
Our legacy product candidates have focused on
the regenerative medicine field. The regenerative medicine field is characterized by intense competition, as global and local pharma
players are becoming more engaged in the cell therapy field based on the advancements made in clinical studies and due to the
favorable regenerative medicine legislation in certain regions. We face competition from both allogeneic and autologous cell therapy
companies, academic, commercial and research institutions, pharmaceutical companies, biopharmaceutical companies, and governmental
agencies. Some of the clinical indications we currently have under development are also being investigated in preclinical and
clinical programs by others.
While there are hundreds of companies in the regenerative medicine
space globally, there are multiple participants in the cell therapy field based in the United States, Europe, Japan, Korea, and Australia
such as Athersys Inc., Celularity Inc., Tigenix NV (acquired by Takeda), SanBio Inc. and Mesoblast Ltd. Among other things, we expect
to compete based upon our intellectual property portfolio, our in-house manufacturing efficiencies and capabilities, and the efficacy
of our products. Our ability to compete successfully will depend on our continued ability to attract and retain experienced and skilled
executives, scientific and clinical development personnel, to identify and develop viable cellular therapeutic candidates, and exploit
these products commercially. Given the magnitude of the potential opportunity for cell therapy, we expect competition in this area to
intensify.
More recently, through our collaboration with Tnuva and the establishment
of Plurinuva, we have begun to utilize our technology in the food tech field. Competitors in the cultivated meat domain include both producers
of consumer-end-products, as well as those developing inputs for the production process. Plurinuva competes with companies that include
Upside Foods, Future Meat, GOOD Meat, Mosa Meat, Aleph Farms, and Gourmey.
We believe that our ability to compete in the food tech field will
derive from our experienced team, our unique 3D technology platform, and our industrial scale in-house GMP, cell manufacturing facility,
together with our partner, Tnuva, which has vast experience in the food business.
Impact of COVID-19
In managing our ongoing global clinical studies, as well as our daily
operations, in the ongoing COVID-19 global pandemic, we are taking all necessary precautions for the safety and well-being of patients,
healthcare providers involved in our studies, and our employees. We are continuing our operational and manufacturing activities, subject
to the directives of the MOH, with a dedicated team on site at our facilities. In addition, the majority of our employees have been vaccinated
or recovered from COVID-19 and we are using remote work technologies that enable the mitigation of office staff while allowing other activities
to be conducted without the need for a physical presence in our facilities, if necessary. The COVID-19 global pandemic caused delays in
enrollment of some of our clinical studies. In addition, we are following the FDA and EMA guidelines regarding the management of clinical
studies during COVID-19. However, the impact of the COVID-19 global pandemic is constantly evolving, and we may experience further impacts
on our daily operations, including the need for employees to potentially self-isolate based on potential exposure to the virus, difficulties
for our employees in travelling abroad, and delays in our ongoing research work with various hospitals and academic institutions.
Available Information
Additional information about
us is contained on our Internet website at www.pluri-biotech.com. Information on our website is not incorporated by reference into this
report. Under the “SEC Filings” and “Financial Information” sections, under the “Investors & Media”
section of our website, we make available free of charge our Annual Reports on Form 10-K, Quarterly Reports on Form 10-Q, Current Reports
on Form 8-K, and amendments to those reports filed or furnished pursuant to Section 13(a) of the Securities Exchange Act of 1934, as amended,
or the Exchange Act, as soon as reasonably practicable after we electronically file such material with, or furnish it to, the SEC. Our
reports filed with the SEC are also made available on the SEC’s website at www.sec.gov. The following Corporate Governance documents
are also posted on our website: Code of Business Conduct and Ethics, Anti Bribery and Corruption and Anti Money Laundering and Terrorist
Financing Compliance Policy, Trading Policy and the Charters for each of the Committees of our Board of Directors, or the Board.
Item 1A. Risk Factors.
An investment in our securities
involves a high degree of risk. You should consider carefully the following information about these risks, together with the other information
contained in this Annual Report before making an investment decision. Our business, prospects, financial condition and results of operations
may be materially and adversely affected as a result of any of the following risks. The value of our securities could decline as a result
of any of these risks. You could lose all or part of your investment in our securities. Some of the statements in “Item 1A. Risk
Factors” are forward-looking statements. The following risk factors are not the only risk factors facing our Company. Additional
risks and uncertainties not presently known to us or that we currently deem immaterial may also affect our business, prospects, financial
condition and results of operations.
Summary of Risk Factors
Our business is subject to
a number of risks, including risks that may adversely affect our business, financial condition and results of operations. These risks
are discussed more fully below and include, but are not limited to, risks related to:
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the COVID-19 pandemic has caused interruptions and delays of our
business plan and may have a adverse effect on our business; |
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we have a history of losses and have not generated significant revenues to date. We expect to experience future losses and do not foresee generating significant or steady revenues in the immediate future; |
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we may need to raise additional capital to meet our business requirements in the future, and such capital raising may be costly or difficult to obtain and could dilute our shareholders’ ownership interests, and such offers or availability for sale of a substantial number of our common shares may cause the price of our publicly traded shares to decline; |
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we may become subject to claims by much larger and better funded competitors enforcing their intellectual property rights against us or seeking to invalidate our intellectual property or our rights thereto; |
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there are inherent risks in the manufacturing of our product candidates, including meeting relevant high regulatory standards, the failure of which could materially and adversely affect our results of operations and the value of our business; |
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if we are unable to obtain and maintain intellectual property protection covering our products and technology,
others may be able to utilize our intellectual property, which would adversely affect our business; |
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we are an international business, and we are exposed to various global and local risks that could have a material adverse effect on our financial condition and results of operations; |
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the market prices of our common shares are subject to fluctuation and have been and may continue to be volatile, which could result in substantial losses for investors; |
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we anticipate being subject to fluctuations in currency exchange rates because a significant portion of our business is conducted outside the United States and we are exposed to currency exchange fluctuations in other currencies such as the New Israeli Shekel, or NIS, and the Euro; |
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restrictions and covenants contained in the EIB Finance Agreement may restrict our ability to conduct certain strategic initiatives; |
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limitations we may face relating to the grants we have received from the IIA may impact our plans and future decisions; |
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if there are significant shifts in the political, economic and military conditions in Israel and its neighboring countries, it could have a material adverse effect on our business relationships and profitability; |
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it may be difficult for investors in the United States to enforce any judgments obtained against us or some of our directors or officers; |
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cybersecurity incidents may have an adverse impact on our business and operations; |
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recent increasing global inflation could affect our ability to
purchase materials needed for manufacturing and could increase the costs of our future product; |
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we have a limited operating history in the field of food-tech to date and our prospects will be dependent on our ability to meet a number of challenges; |
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our business and market potential in the field of food-tech are unproven, and we have limited insight into trends that may emerge and affect our business; and |
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the research and development associated with technologies for cultivated
meat manufacturing, is a lengthy and complex process. |
Risk Related to Our Business
We may need to raise additional financing
to support the research, development and manufacturing of our cell based products in the future, but we cannot be sure we will be able
to obtain additional financing on terms favorable to us when needed. If we are unable to obtain additional financing to meet our needs,
our operations may be adversely affected or terminated.
It is highly likely that we
will need to raise significant additional capital in the future. Although we were successful in raising capital in the past, our current
financial resources are limited, and may not be sufficient to finance our operations until we become profitable, if that ever happens.
It is likely that we will
need to raise additional funds in the future in order to satisfy our working capital and capital expenditure requirements. Therefore,
we are dependent on our ability to sell our common shares for funds, receive grants, enter into collaborations and licensing deals or
to otherwise raise capital. Any sale of our common shares in the future could result in dilution to existing shareholders and could adversely
affect the market price of our common shares.
Also, we may not be able to
raise additional capital in the future to support the development and commercialization of our products, which could result in the loss
of some or all of one’s investment in our common shares.
Our likelihood of profitability depends
on our ability to license and/or develop and commercialize our products based on our technology, which is currently in the development
stage. If we are unable to complete the development and commercialization of our cell-based products successfully, or are unable to obtain
the necessary regulatory approvals, our likelihood of profitability will be limited severely.
We are engaged in the business
of developing cell-based products. We have not realized a profit from our operations to date and there is little likelihood that we will
realize any profits in the short or medium term. Any profitability in the future from our business will be dependent upon successful commercialization
of our cell-based products and/or licensing of our products, which will require additional research and development.
If our cell therapy product
candidates do not prove to be safe and effective in clinical trials, we will not obtain the required regulatory approvals. If we fail
to obtain such approvals, we may not generate sufficient revenues to continue our business operations.
Even after granting regulatory
approval, the FDA, the EMA, and regulatory agencies in other countries continue to regulate marketed products, manufacturers and manufacturing
facilities, which may create additional regulatory barriers and burdens. Later discovery of previously unknown problems with a product,
manufacturer or facility, may result in restrictions on the product or manufacturer, including a withdrawal of the product from the market.
We have not generated significant or consistent
revenues to date, which raises doubts with respect to our ability to generate revenues in the future.
We have a limited operating
history in our business of commercializing cell production technology and we have not generate any material revenues to date. It is not
clear when we will generate revenues or whether we will generate revenues in the future. We cannot give assurances that we will be able
to generate any significant revenues or income in the future. There is no assurance that we will ever be profitable.
Because most of our officers and directors
are located in non-U.S. jurisdictions, you may have no effective recourse against the management for misconduct and may not be able to
enforce judgment and civil liabilities against our officers, directors, experts and agents.
Most of our directors and
officers are nationals and/or residents of countries other than the United States, and all or a substantial portion of their assets are
located outside the United States.
As a result, it may be difficult
to enforce within the United States any judgments obtained against our officers or directors, including judgments predicated upon the
civil liability provisions of the securities laws of the United States or any U.S. state.
While we may seek
partners for licensing deals, joint ventures, partnerships, and direct sale of our products in various industries, there is no guarantee
we will be successful in doing so.
To
date, we have focused our efforts primarily in the regenerative medicine field, but we may seek partners for licensing deals, joint ventures,
partnerships, and direct sale of our products or use of our technology in various industries. Licensing deals, joint ventures and partnerships
in new fields involve numerous risks, including the potential integration of our technology and products in various new ways, which may
or may not be successful. Such projects may require significant funds, time and attention of management and other key personnel. In addition,
as we do not have experience in areas outside of the regenerative medicine field, we may lack the personnel to properly lead such initiatives.
There can be no assurance that we will be successful in finding the relevant partners to fund and market the cell based products.
Risks Related to Development, Clinical studies,
and Regulatory Approval of Our Product Candidates
If we are not able to conduct our clinical
trials properly and on schedule, marketing approval by FDA, EMA, MOH and other regulatory authorities may be delayed or denied.
The completion of our future
clinical trials may be delayed or terminated for many reasons, such as:
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The FDA, the EMA or the MOH does not grant permission to proceed or
places trials on clinical hold; |
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Subjects do not enroll in our trials at the rate we expect. |
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Government actions, such as those enacted during the ongoing COVID-19 pandemic, which limit the general populations movement; |
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The regulators may ask to increase subject’s population in the clinical trials; |
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Subjects experience an unacceptable rate or severity of adverse side effects; |
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Third party clinical investigators and other related vendors may not
perform the clinical trials under the anticipated schedule or consistent with the clinical trial protocol, GCP and regulatory requirements. |
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Third party clinical investigators and other related vendors may declare bankruptcy or terminate their business unexpectedly, which most likely will result in further delays in our clinical trials’ anticipated schedule and cause additional expenditures; |
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Inspections of clinical trial sites by the FDA, EMA, MOH and other regulatory authorities find regulatory violations that require us to undertake corrective action, suspend or terminate one or more sites, or prohibit us from using some or all of the data in support of our marketing applications; or |
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One or more IRBs suspends or terminates the trial at an investigational site, precludes enrollment of additional subjects, or withdraws its approval of the trial. |
Our development costs may
increase if we have material delays in a clinical trials, or if we are required to modify, suspend, terminate or repeat a clinical trial.
If we are unable to conduct our clinical trials properly and on schedule, marketing approval may be delayed or denied by the FDA, EMA,
MOH and other regulatory authorities.
The results of our clinical trials may not
support our product candidates’ claims or any additional claims we may seek for our product candidates and our clinical trials may
result in the discovery of adverse side effects.
Even if any clinical trial
that we need to undertake is completed as planned, or if interim results from existing clinical trials are released, we cannot be certain
that such results will support our product candidates claims or any new indications that we may seek for our products or that the FDA
or foreign authorities will agree with our conclusions regarding the results of those trials. The clinical trial process may fail to demonstrate
that our products or a product candidate is safe and effective for the proposed indicated use, which could cause us to stop seeking additional
clearances or approvals for our product candidates. Any delay or termination of our clinical trials will delay the filing of our regulatory
submissions and, ultimately, our ability to commercialize a product candidate. It is also possible that patients enrolled in clinical
trials will experience adverse side effects that are not currently part of the product candidate’s profile.
Favorable results from compassionate use
treatment or initial interim results from a clinical trial do not ensure that later clinical trials will be successful and success in
early-stage clinical trials does not ensure success in later-stage clinical trials.
PLX cells have been administered
as part of compassionate use treatments, which permit the administration of the PLX cells outside of clinical trials. No assurance can
be given that any positive results are attributable to the PLX cells, or that administration of PLX cells to other patients will have
positive results. Compassionate use is a term that is used to refer to the use of an investigational drug outside of a clinical trial
to treat a patient with a serious or immediately life-threatening disease or condition who has no comparable or satisfactory alternative
treatment options. Regulators often allow compassionate use on a case-by-case basis for an individual patient or for defined groups of
patients with similar treatment needs.
Success in early clinical
trials does not ensure that later clinical trials will be successful, and initial results from a clinical trial do not necessarily predict
final results. While results from treating patients through compassionate use have in certain cases been successful, we cannot be assured
that further trials will ultimately be successful. Results of further clinical trials may be disappointing.
Even if early-stage clinical
trials are successful, we may need to conduct additional clinical trials for product candidates with patients receiving the drug for longer
periods before we are able to seek approvals to market and sell these product candidates from the FDA and regulatory authorities outside
the United States. Even if we are able to obtain approval for our product candidates through an accelerated approval review program, we
may still be required to conduct clinical trials after such an approval. If we are not successful in commercializing any of our lead product
candidates, or are significantly delayed in doing so, our business will be materially harmed.
Our product development programs are based on novel technologies
and are inherently risky.
We are subject to the risks
of failure inherent in the development of products based on new technologies. The novel nature of our therapeutics creates significant
challenges in regard to product development and optimization, manufacturing, government regulation, third party reimbursement and market
acceptance. For example, the FDA, the EMA and other countries’ regulatory authorities have relatively limited experience with cell
therapies. Very few cell therapy products have been approved by regulatory authorities to date for commercial sale, and the pathway to
regulatory approval for our cell therapy product candidates may accordingly be more complex and lengthier. As a result, the development
and commercialization pathway for our therapies may be subject to increased uncertainty, as compared to the pathway for new conventional
drugs.
Our cell therapy drug candidates represent
new classes of therapy that the marketplace may not understand or accept.
Even if we successfully develop
and obtain regulatory approval for our cell therapy candidates, the market may not understand or accept them. We are developing cell therapy
product candidates that represent novel treatments and will compete with a number of more conventional products and therapies manufactured
and marketed by others, including major pharmaceutical companies. The degree of market acceptance of any of our developed and potential
products will depend on a number of factors, including:
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the clinical safety and effectiveness of our cell therapy drug candidates and their perceived advantage over alternative treatment methods, if any; |
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adverse events involving our cell therapy product candidates or the products or product candidates of others that are cell-based; and |
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the cost of our products and the reimbursement policies of government and private third-party payers. |
If the health care community
does not accept our potential products for any of the foregoing reasons, or for any other reason, it could affect our sales, having a
material adverse effect on our business, financial condition, and results of operations.
Interim, “top-line,” and
preliminary data from our clinical trials that we announce or publish from time to time may change as more patient data become available
or as additional analyses are conducted, and as the data are subject to audit and verification procedures, which could result in material
changes in the final data.
From time to time, we may
publish interim, “top-line,” or preliminary data from our clinical studies. Interim data from clinical trials that
we may complete are subject to the risk that one or more of the clinical outcomes may materially change as patient enrollment continues
and more patient data become available. Preliminary or “top-line” data also remain subject to audit and verification
procedures that may result in the final data being materially different from the preliminary data we previously published. As a result,
interim and preliminary data should be viewed with caution until the final data are available. Material adverse changes between preliminary, “top-line,” or
interim data and final data could significantly harm our business prospects.
Risks Related to Our Food-Tech Business
Plurinuva
has a limited operating history in the field of cultivated meat to date and its prospects will be dependent on its ability to meet a number
of challenges.
Plurinuva’s
business prospects are difficult to predict due to its lack of operational history in the new and emerging food tech field, and its success
will be dependent on its ability to meet a number of challenges. Because it has a limited operating history in the field of cultivated
meat and it is in the early stages of development, Plurinuva may not be able to evaluate its future prospects accurately. Plurinuva's
prospects will be primarily dependent on its ability to successfully develop industrial scale cultivated meat technologies and processes,
and market these to its potential customers. If Plurinuva is not able to successfully meet these challenges, its prospects, business,
financial condition, and results of operations could be adversely impacted.
In
addition, Plurinuva will be subject to changing laws, rules and regulations in the Israeli, United States, Asia Pacific, the European
Union and other jurisdictions relating to the food tech industry. Such laws and regulations may negatively impact its ability to expand
its business and pursue business opportunities. Plurinuva may also incur significant expenses to comply with the laws, regulations and
other obligations that will apply to it.
Plurinuva is primarily
focused on utilizing its technology for the development of cultivated meat , and it has limited data on the performance of our and its
technologies in the field of cultivated meat to date.
Plurinuva
does not currently have any products or technologies approved for sale and it is still in the early stages of development. To date, Plurinuva
has limited data on the ability of our and its technologies to successfully manufacture cultivated meat, towards which they have devoted
substantial resources to date. Plurinuva’s current technologies are, in large part, based on our technologies and intellectual property.
We may not be successful in developing its technologies in a manner sufficient to support its expected scale-ups and future growth, or
at all. Plurinuva expects that a substantial portion of its efforts and expenditures over the next few years will be devoted to
the development of technologies designed to enable Plurinuva to market industrial-scale cultivated meat manufacturing processes.
Plurinuva cannot guarantee that it will be successful in developing these technologies, based on its current roadmap , or at all. If Plurinuva
is able to successfully develop its cultivated meat technologies, it cannot ensure that it will obtain regulatory approval or that, following
approval, upon commercialization its technologies will achieve market acceptance. Any such delay or failure could materially and
adversely affect Plurinuva's financial condition, results of operations and prospects.
Risk Related to Commercialization of Our Product
Candidates
We may not successfully establish new collaborations,
joint ventures or licensing arrangements, which could adversely affect our ability to develop and commercialize our product candidates.
One of the elements of our
business strategy is to license our technology to other companies. Our business strategy includes development and in-house manufacturing
of innovative new cell- based products and solutions powered by our 3D cell expansion technology platforms and establishing joint ventures
and partnerships that leverage our cell expansion technology and cell-based product portfolio to expand product pipelines and meet cell-based
manufacturing needs for a variety of industries. To date, we have a strategic partnership with Tnuva to use our technology to establish
a cultivated food platform ,with CHA for both the IC and CLI indications in Korea and with Chart for the thawing device. Notwithstanding,
we may not be able to further establish or maintain such licensing and collaboration arrangements necessary to develop and commercialize
our product candidates.
Even if we are able to maintain
or establish licensing or collaboration arrangements, these arrangements may not be on favorable terms and may contain provisions that
will restrict our ability to develop, test and market our product candidates. Any failure to maintain or establish licensing or collaboration
arrangements on favorable terms could adversely affect our business prospects, financial condition, or ability to develop and commercialize
our product candidates.
Our agreements with our collaborators
and licensees may have provisions that give rise to disputes regarding the rights and obligations of the parties. These and other possible
disagreements could lead to termination of the agreement or delays in collaborative research, development, supply, or commercialization
of certain product candidates, or could require or result in litigation or arbitration. Moreover, disagreements could arise with our collaborators
over rights to intellectual property or our rights to share in any of the future revenues of products developed by our collaborators.
These kinds of disagreements could result in costly and time-consuming litigation. Any such conflicts with our collaborators could reduce
our ability to obtain future collaboration agreements and could have a negative impact on our relationship with existing collaborators.
The market for our cell therapy products will be heavily dependent
on third party reimbursement policies.
Our ability to successfully
commercialize our cell therapy product candidates will depend on the extent to which government healthcare programs, as well as private
health insurers, health maintenance organizations and other third-party payers will pay for our products and related treatments.
Reimbursement by third party
payers depends on a number of factors, including the payer’s determination that use of the product is safe and effective, not experimental,
or investigational, medically necessary, appropriate for the specific patient and cost-effective. Reimbursement in the United States
or foreign countries may not be available or maintained for any of our product candidates. If we do not obtain approvals for adequate
third-party reimbursements, we may not be able to establish or maintain price levels sufficient to realize an appropriate return on our
investment in product development. Any limits on reimbursement from third party payers may reduce the demand for, or negatively affect
the price of, our products. The lack of reimbursement for these procedures by insurance payers has negatively affected the market for
our products in this indication in the past.
Managing and reducing health
care costs has been a general concern of federal and state governments in the United States and of foreign governments. In addition,
third party payers are increasingly challenging the price and cost-effectiveness of medical products and services, and many limit reimbursement
for newly approved health care products. In particular, third-party payers may limit the indications for which they will reimburse
patients who use any products that we may develop. Cost control initiatives could decrease the price for products that we may develop,
which would result in lower product revenues to us.
Risk Related to Intellectual Property
Our success depends in large part on our
ability to develop and protect our technology and our cell therapy products. If our patents and proprietary rights agreements do not provide
sufficient protection for our technology and our cell therapy products, our business and competitive position will suffer.
Our success will also depend
in part on our ability to develop our technology and commercialize cell therapy products without infringing the proprietary rights of
others. We have not conducted full freedom of use patent searches and no assurance can be given that patents do not exist or could not
be filed which would have an adverse effect on our ability to develop our technology or maintain our competitive position with respect
to our potential cell therapy products. If our technology components, devices, designs, products, processes or other subject matter are
claimed under other existing United States or foreign patents or are otherwise protected by third party proprietary rights, we may be
subject to infringement actions. In such event, we may challenge the validity of such patents or other proprietary rights, or we may be
required to obtain licenses from such companies in order to develop, manufacture or market our technology or products. There can be no
assurances that we would be able to obtain such licenses or that such licenses, if available, could be obtained on commercially reasonable
terms. Furthermore, the failure to either develop a commercially viable alternative or obtain such licenses could result in delays in
marketing our proposed products or the inability to proceed with the development, manufacture or sale of products requiring such licenses,
which could have a material adverse effect on our business, financial condition and results of operations. If we are required to defend
ourselves against charges of patent infringement or to protect our proprietary rights against third parties, substantial costs will be
incurred regardless of whether we are successful. Such proceedings are typically protracted with no certainty of success. An adverse outcome
could subject us to significant liabilities to third parties and force us to curtail or cease our development of our technology and the
commercialization our potential cell therapy products.
We have built the ability
to manufacture clinical grade adherent stromal cells in-house. Through our experience with adherent stromal cell-based product development,
we have developed expertise and know-how in this field. To protect these expertise and know-how, our policies require confidentiality
agreements with our employees, consultants, contractors, manufacturers and advisors. These agreements generally provide for protection
of confidential information, restrictions on the use of materials and assignment of inventions conceived during the course of performance
for us. These agreements might not effectively prevent disclosure of our confidential information.
Third parties may initiate legal proceedings
alleging that we are infringing their intellectual property rights, the outcome of which would be uncertain and could have a material
adverse effect on our business.
Our commercial success depends
upon our ability and the ability of our collaborators to develop, manufacture, market and sell our product candidates and use our proprietary
technologies without infringing the proprietary rights of third parties. We have yet to conduct comprehensive freedom-to-operate searches
to determine whether our proposed business activities or use of certain of the patent rights owned by us would infringe patents issued
to third parties. We may become party to, or threatened with, future adversarial proceedings or litigation regarding intellectual property
rights with respect to our products and technology, including interference proceedings before the U.S. Patent and Trademark Office. Third
parties may assert infringement claims against us based on existing patents or patents that may be granted in the future. If we are found
to infringe a third party’s intellectual property rights, we could be required to obtain a license from such third party to continue
developing and marketing our products and technology. However, we may not be able to obtain any required license on commercially reasonable
terms or at all.
Even if we were able to obtain
a license, it could be non-exclusive, thereby giving our competitors access to the same technologies licensed to us. We could be forced,
including by court order, to cease commercializing the infringing technology or product. In addition, we could be found liable for monetary
damages. A finding of infringement could prevent us from commercializing our product candidates or force us to cease some of our business
operations, which could materially harm our business. For example, we are aware of issued third party patents directed to placental stem
cells and their use for therapy and in treating various diseases. We may need to seek a license for one or more of these patents. No assurances
can be given that such a license will be available on commercially reasonable terms, if at all. Claims that we have misappropriated the
confidential information or trade secrets of third parties could have a similar negative impact on our business.
Even if resolved in our favor,
litigation or other legal proceedings relating to intellectual property claims may cause us to incur significant expenses and could distract
our technical and management personnel from their normal responsibilities. In addition, there could be public announcements of the results
of hearings, motions or other interim proceedings or developments and if securities analysts or investors perceive these results to be
negative, it could have a substantial adverse effect on the price of our common shares. Such litigation or proceedings could substantially
increase our operating losses and reduce the resources available for development activities or any future sales, marketing or distribution
activities. We may not have sufficient financial or other resources to adequately conduct such litigation or proceedings. Some of our
competitors are able to sustain the costs of such litigation or proceedings more effectively than we can because of their greater financial
resources. Uncertainties resulting from the initiation and continuation of patent litigation or other proceedings could have a material
adverse effect on our ability to compete in the marketplace.
The patent approval process is complex,
and we cannot be sure that our pending patent applications or future patent applications will be approved.
The patent position of biotechnology
and pharmaceutical companies generally is highly uncertain, involves complex legal and factual questions and has in recent years been
the subject of much litigation. As a result, the issuance, scope, validity, enforceability and commercial value of our and any future
licensors’ patent rights are highly uncertain. Our pending and future patent applications may not result in patents being issued
which protect our technology or products or which effectively prevent others from commercializing competitive technologies and products.
Changes in either the patent laws or interpretation of the patent laws in the United States and other countries may diminish the value
of our patents or narrow the scope of our patent protection. The laws of foreign countries may not protect our rights to the same extent
as the laws of the United States and we may not be able to obtain meaningful patent protection for any of our commercial products either
in or outside the United States.
No assurance can be given
that the scope of any patent protection granted will exclude competitors or provide us with competitive advantages, that any of the patents
that have been or may be issued to us will be held valid if subsequently challenged, or that other parties will not claim rights to or
ownership of our patents or other proprietary rights that we hold. Furthermore, there can be no assurance that others have not developed
or will not develop similar products, duplicate any of our technology or products or design around any patents that have been or may be
issued to us or any future licensors. Since patent applications in the United States and in Europe are not publicly disclosed until patents
are issued, there can be no assurance that others did not first file applications for products covered by our pending patent applications,
nor can we be certain that we will not infringe any patents that may be issued to others.
Risk Related to Our Common
Shares
The price of our common shares may fluctuate significantly.
The market for our common
shares may fluctuate significantly. A number of events and factors may have an adverse impact on the market price of our common shares,
such as:
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results of our clinical trials or adverse events associated with our products; |
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the amount of our cash resources and our ability to obtain additional funding; |
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changes in our revenues, expense levels or operating results; |
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entering into or terminating strategic relationships; |
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announcements of technical or product developments by us or our competitors; |
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market conditions for pharmaceutical and biotechnology shares in particular; |
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changes in laws and governmental regulations, including changes in tax, healthcare, competition and patent laws; |
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disputes concerning patents or proprietary rights; |
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new accounting pronouncements or regulatory rulings; |
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public announcements regarding medical advances in the treatment of the disease states that we are targeting; |
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patent or proprietary rights developments; |
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regulatory actions that may impact our products; |
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future sales of our common shares, or the perception of such sales; |
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disruptions in our manufacturing processes; and |
In addition, a global pandemic,
such as the COVID-19 pandemic and a market downturn in general and/or in the biopharmaceutical sector in particular, may adversely affect
the market price of our securities, which may not necessarily reflect the actual or perceived value of our Company.
We could fail to maintain the listing
of our common shares on Nasdaq, which could seriously harm the liquidity of our shares and our ability to raise capital or complete a
strategic transaction.
The Nasdaq Stock Market
has established continued listing requirements, including a requirement to maintain a minimum closing bid price of at least $1.00 per
share. If a company trades for 30 consecutive business days below such minimum closing bid price, it will receive a deficiency notice
from Nasdaq. Assuming it is in compliance with the other continued listing requirements, Nasdaq would provide such company a period of
180 calendar days in which to regain compliance by maintaining a closing bid price at least $1.00 per share for a minimum of ten consecutive
business days. If we are not able to regain compliance, there is a risk that our common shares may be delisted from Nasdaq.
As of the date of this
filing, our common shares are trading below $1.00 per share. If the closing bid price of our common shares continues trading below $1.00 per share for
an aggregate of 30 consecutive business days, we will receive a deficiency notice from Nasdaq. If, in such circumstance, we are not able
to regain compliance with the minimum bid price requirement within 180 days, our common shares will be subject to a delisting action by
Nasdaq.
A delisting from Nasdaq
would likely result in a reduction in some or all of the following, each of which could have a material adverse effect on shareholders:
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the liquidity of our common shares; |
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the market price of our common shares; |
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the availability of information concerning the trading prices and volume of our common shares; |
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our ability to obtain financing or complete a strategic transaction; |
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the number of institutional and other investors that will consider investing in our common shares; and |
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the number of market markers or broker-dealers for our common shares. |
Future sales of our common shares may cause dilution.
Future sales of our common
shares, or the perception that such sales may occur, could cause immediate dilution and adversely affect the market price of our common
shares. If we raise additional capital by issuing equity securities, the percentage ownership of our existing shareholders may be reduced,
and accordingly these shareholders may experience substantial dilution. We may also issue equity securities that provide for rights, preferences
and privileges senior to those of our common shares. Given our need for cash and that equity raising is the most common type of fundraising
for companies like ours, the risk of dilution is particularly significant for shareholders of our company.
Risks Related to Foreign Exchange Rates
We are exposed to fluctuations in currency exchange rates.
A significant portion of our
business is conducted outside the United States. Therefore, we are exposed to currency exchange fluctuations in other currencies such
as the NIS and the Euro. A significant portion of our expenses in Israel are paid in NIS, and we have also received €20 million pursuant
to the EIB Finance Agreement, that bears 4% annual interest. All of these factors subject us to the risks of foreign currency fluctuations.
Our primary expenses paid in NIS are employee salaries, and lease payments on our facilities. From time to time, we may apply a hedging
strategy by using options and forward contracts to protect ourselves against some of the risks of currency exchange fluctuations and we
are actively monitoring the exchange rate differences of the NIS, Euro and U.S. Dollar; however, we are still exposed to potential losses
from currency exchange fluctuation.
Our cash may be subject to a risk of loss,
and we may be exposed to fluctuations in interest rates.
Our assets include a significant
component of cash and cash equivalents and bank deposits. We adhere to an investment policy set by our investment committee
which aims to preserve our financial assets, maintain adequate liquidity and maximize returns. We believe that our cash is held in institutions
whose credit risk is minimal and that the value and liquidity of our deposits are accurately reflected in our consolidated financial statements
as of June 30, 2022. Currently, we hold most of our cash assets in bank deposits. However, nearly all of our cash and bank deposits are
not insured by the Federal Deposit Insurance Corporation, or the FDIC, or similar governmental deposit insurance outside the United
States. Therefore, our cash and any bank deposits that we now hold or may acquire in the future may be subject to risks, including
the risk of loss or of reduced value or liquidity, particularly in light of the increased volatility and worldwide pressures in the financial
and banking sectors.
Other Risks
The ongoing COVID-19 pandemic, or any other
pandemic, epidemic or outbreak of an infectious disease, may materially and adversely affect our business and operations.
COVID-19 has had
and continues to have a significant impact, both direct and indirect, on businesses and commerce, as worker shortages have occurred; supply
chains have been disrupted; facilities and production have been suspended; and demand for certain goods and services, such as medical
services and supplies, has spiked, while demand for other goods and services, such as travel, has fallen. We are actively monitoring any
developments regarding the pandemic, and we are taking any necessary measures to respond to the situation in cooperation with the various
stakeholders.
COVID-19 infection
of our workforce could result in a temporary disruption in our business activities, including manufacturing and other functions. Based
on guidelines provided by the Israeli Government, we have increased as much as possible the capacity and arrangement for employees to
work remotely, and although the vast majority of our employees have been vaccinated and we have adopted hybrid working models to minimize
exposure, we cannot guaranty that there will be no infection and spread of the virus among our employees and staff.
The COVID-19 pandemic
is also affecting the United States, Israel and global economies and has affected, and may continue to affect, the conduct of our clinical
trials and may in the future affect our operations and those of third parties on which we rely, including by causing disruptions in our
raw material supply. In that regard, to date we have experienced delays in enrolling patients in our various studies due to the COVID-19
pandemic.
In addition, the
COVID-19 pandemic may affect the operations of the FDA and other health authorities, which could result in delays of reviews and approvals,
including with respect to our Phase III clinical trial related to muscle recovery following surgery for hip fracture. The evolving COVID-19
pandemic has already impacted, and may continue to, directly or indirectly impact the pace of enrollment in our clinical trials as patients
may avoid or may not be able to travel to healthcare facilities and physicians’ offices unless due to a health emergency and clinical
trial staff may not be able to physically arrive to the clinical sites. Additionally, such facilities and offices have been and may continue
to be required to focus limited resources on non-clinical trial matters, including treatment of COVID-19 patients, thereby decreasing
availability, in whole or in part, for clinical trial services. Additionally, the stock market has been unusually volatile during the
COVID-19 outbreak and such volatility may continue. To date, during certain periods of the COVID-19 pandemic, our share price fluctuated
significantly, and such fluctuation may continue to occur.
The ultimate impact
of the COVID-19 pandemic is highly uncertain and subject to change. We do not yet know the full extent of potential delays or impacts
on our business, financing or clinical trial activities, or on healthcare systems or the global economy as a whole if the pandemic continues
for an extended period of time or significantly worsens. However, these effects could have a material impact on our liquidity, capital
resources, operations and business and those of the third parties on which we rely.
Since we received grants from the IIA, we are subject to on-going
restrictions.
We have received royalty-bearing
grants from the IIA, for research and development programs that meet specified criteria. The terms of the IIA’s grants limit our
ability to transfer know-how developed under an approved research and development program outside of Israel, regardless of whether the
royalties are fully paid. Any non-Israeli citizen, resident or entity that, among other things, becomes a holder of 5% or more of our
share capital or voting rights, is entitled to appoint one or more of our directors or our Chief Executive Officer, or CEO, serves as
a director of our Company or as our CEO is generally required to notify the same to the IIA and to undertake to observe the law governing
the grant programs of the IIA, the principal restrictions of which are the transferability limits described above. For more information,
see “Item 7. Management’s Discussion and Analysis of Financial Condition and Results of Operations - Liquidity and Capital
Resources.”
Recent increasing
global inflation may adversely affect our business results.
The
increasing inflation could affect our ability to purchase materials needed to support our research and operational activities, which in
turn could result in higher burn rate and a higher end price of our future products. As a result, we may not be able to effectively develop
our product candidates or cultivated meat products. If we are not able to successfully manage any increases in inflation, our prospects,
business, financial condition, and results of operations could be adversely impacted.
Since we have signed the EIB Finance Agreement,
we agreed to guaranty the loan as well as agreed to limitations that require us to notify the EIB, and in some cases obtain their approval,
before we engage with other banks for additional sources of funding or with potential partners for certain strategic activities.
The EIB Finance Agreement
contains certain limitations that we must adhere to such as the use of proceeds received from the EIB, the disposal of assets, substantive
changes in the nature of our business, our potential execution of mergers and acquisitions, changes in our holding structure, distributions
of future potential dividends and our engaging with other banks and financing entities for other loans.
Our principal research and development and
manufacturing facilities are located in Israel and the unstable military and political conditions of Israel may cause interruption or
suspension of our business operations without warning.
Our principal research and
development and manufacturing facilities are located in Israel. As a result, we are directly influenced by the political, economic and
military conditions affecting Israel. Since the establishment of the State of Israel in 1948, a number of armed conflicts have taken place
between Israel and its Arab neighbors. During June 2021, July and August 2014 and November 2012, Israel was engaged in an armed conflict
with a militia group and political party which controls the Gaza Strip, and during the summer of 2006, Israel was engaged in an armed
conflict with Hezbollah, a Lebanese Islamist Shiite militia group and political party. These conflicts involved missile strikes against
civilian targets in various parts of Israel, including areas in which our employees and some of our consultants are located, and negatively
affected business conditions in Israel. We cannot predict if or when armed conflict will take place and the duration of each conflict.
Furthermore, certain of our
employees may be obligated to perform annual reserve duty in the Israel Defense Forces and are subject to being called up for active military
duty at any time. All Israeli male citizens who have served in the army are required to perform reserve duty until they are between 40
and 49 years old, depending upon the nature of their military service.
In addition, Israeli-based
companies and companies doing business with Israel, have been the subject of an economic boycott by members of the Arab League and certain
other predominantly Muslim countries since Israel’s establishment. Although Israel has entered into various agreements with certain
Arab countries and the Palestinian Authority, and various declarations have been signed in connection with efforts to resolve some of
the economic and political problems in the Middle East, we cannot predict whether or in what manner these problems will be resolved. Wars
and acts of terrorism have resulted in significant damage to the Israeli economy, including reducing the level of foreign and local investment.
Risk Related to Our Industry
The trend towards consolidation in the pharmaceutical and biotechnology
industries may adversely affect us.
There is a trend towards consolidation
in the pharmaceutical and biotechnology industries. This consolidation trend may result in the remaining companies having greater financial
resources and technical discovery capabilities, thus intensifying competition in these industries. This trend may also result in fewer
potential collaborators or licensees for our therapeutic product candidates. Also, if a consolidating company is already doing business
with our competitors, we may lose existing licensees or collaborators as a result of such consolidation. This trend may adversely affect
our ability to enter into license agreements or agreements for the development and commercialization of our product candidates, and as
a result may materially harm our business.
If we do not keep pace with our competitors
and with technological and market changes, our technology and products may become obsolete, and our business may suffer.
The cellular therapeutics
industry, of which we are a part, is very competitive and is subject to technological changes that can be rapid and intense. We have faced,
and will continue to face, intense competition from biotechnology, pharmaceutical and biopharmaceutical companies, academic and research
institutions and governmental agencies engaged in cellular therapeutic and drug discovery activities or funding, both in the United States
and internationally. Some of these competitors are pursuing the development of cellular therapeutics, drugs and other therapies that target
the same diseases and conditions that we target in our clinical and pre-clinical programs.
Some of our competitors have
greater resources, more product candidates and have developed product candidates and processes that directly compete with our products.
Our competitors may have developed, or could develop in the future, new products that compete with our products or even render our products
obsolete.
Potential product liability claims could
adversely affect our future earnings and financial condition.
We face an inherent business
risk of exposure to product liability claims in the event that the use of our products results in adverse effects. We may not be able
to maintain adequate levels of insurance for these liabilities at reasonable cost and/or reasonable terms. Excessive insurance costs or
uninsured claims would add to our future operating expenses and adversely affect our financial condition.
Risk Related to Our Dependence on Third Parties
We are dependent upon third party suppliers
for raw materials needed to manufacture PLX; if any of these third parties fails or is unable to perform in a timely manner, our ability
to manufacture and deliver will be compromised.
In addition to the placenta
used in the clinical manufacturing process of PLX, we require certain raw materials. These items must be manufactured and supplied to
us in sufficient quantities and in compliance with current GMP. To meet these requirements, we have entered into supply agreements with
firms that manufacture these raw materials to current GMP standards. Our requirements for these items are expected to increase if and
when we transition to the manufacture of commercial quantities of our cell-based drug candidates.
In addition, as we proceed
with our clinical trial efforts, we must be able to continuously demonstrate to the FDA, EMA and other regulatory authorities that we
can manufacture our cell therapy product candidates with consistent characteristics. Accordingly, we are materially dependent on these
suppliers for supply of current GMP-grade materials of consistent quality. Our ability to complete ongoing clinical trials may be negatively
affected in the event that we are forced to seek and validate a replacement source for any of these critical materials.
We intend to decrease our
dependency in third party suppliers for raw materials. To that effect we have developed a serum-free formulation which is expected to
support the manufacturing of cell therapy products. This serum-free formulation was developed using our deep understanding in cell therapy
industrial scale production standards, and the quality methods designed to support implementation in Phase III development and marketing.
Achieving this significant technological challenge is expected to provide us with large-scale, highly consistent production with operational
independency from third party suppliers for standard serum, an expensive and quantity limited product. There can be no guarantee that
we will successfully implement the use of our serum-free formulation to support the manufacturing of cell therapy products or any other
future product candidates, if any, that we seek to produce using such formulation, or that such implementation of the serum-free formulation
will decrease our dependency on third party suppliers for raw materials.
We rely and will continue to rely on third
parties to conduct our clinical trials. If these third parties do not successfully carry out their contractual duties or meet expected
deadlines, we may not be able to obtain regulatory approval of or commercialize our product candidates.
We depend and will depend
upon independent investigators and collaborators, such as universities, medical institutions, CROs, vendors and strategic partners to
conduct our pre-clinical and clinical trials under agreements with us. We negotiate budgets and contracts with CROs, vendors and study
sites which may result in delays to our development timelines and increased costs. We rely heavily on these third parties over the course
of our clinical trials, and we control only certain aspects of their activities. Nevertheless, we are responsible for ensuring that each
of our studies is conducted in accordance with applicable protocol, legal, regulatory and scientific standards, and our reliance on third
parties does not relieve us of our regulatory responsibilities. We and these third parties are required to comply with current good clinical
practices, or cGCPs, which are regulations and guidelines enforced by the FDA and comparable foreign regulatory authorities for product
candidates in clinical development.
Regulatory authorities enforce
these cGCPs through periodic inspections of trial sponsors, principal investigators and trial sites. If we or any of these third parties
fail to comply with applicable cGCP regulations, the clinical data generated in our clinical trials may be deemed unreliable and the FDA
or comparable foreign regulatory authorities may require us to perform additional clinical trials before approving our marketing applications.
We cannot assure that, upon inspection, such regulatory authorities will determine that any of our clinical trials comply with the cGCP
regulations. In addition, any Phase III clinical trials which we may conduct must be conducted with biologic product produced under cGMP
and may require a large number of test patients. Biologic products for commercial purposes must also be produced under cGMP. Our failure
or any failure by these third parties to comply with these regulations or to recruit a sufficient number of patients may require us to
repeat clinical trials, which would delay the regulatory approval process. Moreover, our business may be implicated if any of these third
parties violates federal or state fraud and abuse or false claims laws and regulations or healthcare privacy and security laws and regulations.
Any third parties conducting
our clinical trials are not and will not be our employees and, except for remedies available to us under our agreements with such third
parties, which in some instances may be limited, we cannot control whether or not they devote sufficient time and resources to our ongoing
pre-clinical, clinical and nonclinical programs. These third parties may also have relationships with other commercial entities, including
our competitors, for whom they may also be conducting clinical trials or other drug development activities, which could affect
their performance on our behalf. If these third parties do not successfully carry out their contractual duties or obligations or meet
expected deadlines, if they declare bankruptcy or if they need to be replaced for whatever reason or if the quality or accuracy of the
clinical data they obtain is compromised due to the failure to adhere to our clinical protocols or regulatory requirements or for other
reasons, our clinical trials may be extended, delayed or terminated and we may not be able to complete development of, obtain regulatory
approval of or successfully commercialize our product candidates. As a result, our financial results and the commercial prospects for
our product candidates would be harmed, our costs could increase and our ability to generate revenue could be delayed. Switching or adding
third parties to conduct our clinical trials involves substantial cost and requires extensive management time and focus. In addition,
there is a natural transition period when a new third party commences work. As a result, delays occur, which can materially impact our
ability to meet our desired clinical development timelines.
A cybersecurity
incident, other technology disruptions or failure to comply with laws and regulations relating to privacy and the protection of data
relating to individuals could negatively impact our business and our reputation.
We rely on and utilize services
provided by third parties in connection with our clinical trials, which services involve the collection, use, storage and analysis of
personal health information. While we receive assurances from these vendors that their services are compliant with the Health Insurance
Portability and Accountability Act, or HIPAA, and other applicable privacy laws, there can be no assurance that such third parties will
comply with applicable laws or regulations. Non-compliance by such vendors may result in liability for us which would have a material
adverse effect on our business, financial conditions and results of operations.
During November 2021, we experienced
a cybersecurity incident in which one or more third parties were able to impersonate one of our vendors by using a falsified email domain
account and asked to make a payment to a false bank account. As a result of this incident, the third parties managed to extract a sum
of approximately $616,000 from us. Following the incident, we hired the services of a cybersecurity investigation firm to fully access
the incident and notified the appropriate government authorities, including the banks involved in the transaction. During February 2022,
with the assistance of local and global law enforcement agencies, we were able to recover an amount of approximately $412,000 from the
false bank account. Together with the reimbursement received from our insurance company, we were able to recover the full amount lost.
The cybersecurity incident
has not had any material effect on our ability to meet our financial obligations, including our ability to carry out our operations and
business activities, and our investigation has confirmed that, other than the funds referenced above, none of our information or data
was stolen or damaged. Nonetheless, despite the implementation of security measures, including the steps we have taken following the November
2021 cybersecurity incident, our internal computer systems and those of our current and future CROs and other contractors and consultants
may not prevent future incidents of a similar nature or other cyber-attacks. We are constantly exploring new and advanced security protection
measures to prevent future cybersecurity incidents.
Future security breaches or
any material system failure events could result in a material disruption of our development programs and our business operations. For
example, the loss of clinical trial data from completed or future clinical trials could result in delays in our regulatory approval efforts
and significantly increase our costs to recover or reproduce the data. To the extent that any disruption or security breach were to result
in a loss of, or damage to, our data or applications, or inappropriate disclosure of confidential or proprietary information, we could
incur liability and the further development and commercialization of our product candidates could be delayed.
In
addition, we are subject to laws, rules and regulations in the Israeli, United States, the European Union and other jurisdictions relating
to the collection, use and security of personal information and data. Such data privacy laws, regulations and other obligations may require
us to change our business practices and may negatively impact our ability to expand our business and pursue business opportunities. We
may incur significant expenses to comply with the laws, regulations and other obligations that apply to us. Additionally, the privacy-
and data protection-related laws, rules and regulations applicable to us are subject to significant change. Several jurisdictions have
passed new laws and regulations in this area, and other jurisdictions are considering imposing additional restrictions. Privacy- and data
protection-related laws and regulations also may be interpreted and enforced inconsistently over time and from jurisdiction to jurisdiction.
Any actual or perceived inability to comply with applicable privacy or data protection laws, regulations, or other obligations could result
in significant cost and liability, litigation or governmental investigations, damage our reputation, and adversely affect our business.
Unsuccessful compliance with certain European
privacy regulations could have an adverse effect on our business and reputation.
The collection and use of
personal health data in the European Union is governed by the provisions of the General Data Protection Regulation, or GDPR. This directive
imposes several requirements relating to the consent of the individuals to whom the personal data relates, the information provided to
the individuals, notification of data processing obligations to the competent national data protection authorities and the security and
confidentiality of the personal data. The GPDR also extends the geographical scope of European Union data protection law to non-European
Union entities under certain conditions, tightens existing European Union data protection principles and creates new obligations for companies
and new rights for individuals. Failure to comply with the requirements of the GDPR and the related national data protection laws of the
European Union Member States may result in fines and other administrative penalties. There may be circumstances under which a failure
to comply with GDPR, or the exercise of individual rights under the GDPR, would limit our ability to utilize clinical trial data collected
on certain subjects. The GDPR regulations impose additional responsibility and liability in relation to personal data that we process,
and we intend to put in place additional mechanisms ensuring compliance with these and/or new data protection rules.
Changes to these European
privacy regulations and unsuccessful compliance may be onerous and adversely affect our business, financial condition, prospects, results
of operations and reputation.
We may be exposed to liabilities under the
Foreign Corrupt Practices Act, and any determination that we violated the Foreign Corrupt Practices Act could have a material adverse
effect on our business.
We are subject to the Foreign
Corrupt Practice Act, or FCPA, and other laws that prohibit U.S. companies or their agents and employees from providing anything of value
to a foreign official or political party for the purposes of influencing any act or decision of these individuals in their official capacity
to help obtain or retain business, direct business to any person or corporate entity or obtain any unfair advantage. We have operations
and agreements with third parties. Our international activities create the risk of unauthorized and illegal payments or offers of payments
by our employees or consultants, even though they may not always be subject to our control. We discourage these practices by our employees
and consultants. However, our existing safeguards and any future improvements may prove to be less than effective, and our employees or
consultants, may engage in conduct for which we might be held responsible for Any failure by us to adopt appropriate compliance procedures
and ensure that our employees and consultants comply with the FCPA and applicable laws and regulations in foreign jurisdictions could
result in substantial penalties or restrictions on our ability to conduct business in certain foreign jurisdictions.
Violations of the FCPA may
result in severe criminal or civil sanctions, and we may be subject to other liabilities, which could negatively affect our business,
operating results, and financial condition. In addition, the U.S. government may seek to hold our Company liable for successor liability
FCPA violations committed by companies in which we invest or that we acquire.