Oxford BioDynamics, Plc (AIM: OBD, the Company), a precision
clinical diagnostics company bringing specific and sensitive tests
to the practice of medicine based on OBD’s EpiSwitch® 3D genomics
platform,[4] announces that it has formed a strategic consortium
which has been shortlisted for the UK Government’s Checkpoint
Inhibitor Response Research Platform (CIRRP) award call for
biomarker development around immunotherapies of cancer. If
successful, the consortium’s proposal would provide NHS patients
with access to OBD's EpiSwitch CiRT (Checkpoint inhibitor Response
Test) test.
- CIRRP is a £9M initiative aimed at putting the UK at the
forefront of cancer treatment, that was announced by The Medical
Research Council and the Office for Life Sciences, part of the
Department of Health and Social Care and the Department for
Science, Innovation and Technology earlier this year.
- CIRRP aims to enhance the benefits, and navigate the complexity
of cancer immunotherapy using PD-1/PD-L1 antagonists by addressing
the low and variable response rates to therapy as well as
predicting severe side effects.
- Oxford BioDynamics has formed a consortium with world leading
experts in molecular epigenetics at the University of Oxford, in
clinical metabolomics and lipidomics at the University of
Birmingham, and in cancer treatment with Imperial College
Healthcare NHS Trust and Norfolk and Norwich University NHS
Trust.
- The consortium submitted a proposal to advance immunotherapy in
NHS patients diagnosed with five of the most prevalent cancers
using Oxford BioDynamic’s EpiSwitch® CiRT and HiRT to predict both
response to ICIs and their potential side effects as well as
discover the underlying mechanisms behind different response
rates.
- The consortium’s proposal has been shortlisted for award
consideration.
- The EpiSwitch® Checkpoint Inhibitor Response Test (CiRT) is the
first in class, blood-based, accurate predictor of response to
ICIs. The test is commercially available through clinical
diagnostic labs in the US and UK.
- The EpiSwitch® Hyper Immune Response Test HiRT is a unique
prognostic blood test designed on the EpiSwitch platform with
support from the Partnership for Accelerating Cancer Therapies
(PACT, USA). The test accurately predicts individuals most likely
to exhibit hyperprogressive disease (HPD), a response to
immunotherapy which triggers life threatening, disease accelerating
side effects. An average of 12% of ICI-treated patients exhibit
HPD.
- If the consortium’s proposal is successful, NHS patients with
colorectal, prostate, breast, ovarian or lung cancer would be
prospectively evaluated with CiRT and HiRT, and together with their
clinical outcomes and individual genetic, epigenetic and metabolic
states used to offer mechanistic insights into their immune systems
and clinical outcomes.
The proposal to CIRRP is a public/private partnership which will
involve clinicians and academics from the Universities of Oxford
and Birmingham, Imperial Healthcare NHS Trust, Norfolk and Norwich
Universities NHS Trust, and OBD, to build on the successful
translation to clinical practice of a proven predictive tool for
response to immune checkpoint inhibitors (ICI) provided by OBD.
In the proposal to the UK government, a successful Cancer
Immunotherapy Response Research platform (CIRRP) outcome will
accurately predict a patient’s clinical response to current ICIs to
inform clinical treatment decisions, focus on optimization of NHS
resources, be applicable to and scalable across many cancers, be
flexible and adapt to new ICIs, identify new immunological targets
and treatment regimes, account for comorbidities and provide
insights into mechanisms of response.
If the proposal is accepted, the consortium will:
- Establish the CIRRP platform within an existing OBD
ISO15189/UKAS accredited clinical laboratory to offer UK-based
EpiSwitch CiRT and HiRT clinical screening on at least 350 patients
- in prostate, colorectal, breast, ovarian and lung cancers,
initially at the NHS trusts within the consortium, and then across
NHS networks across the UK, using an established transparent cost
per patient sample model.
- Create real-world impact data within NHS clinical practice for
prediction of ICI response and prognosis of Hyperprogressive
disease (HPD). The initial focus will be NHS patients considered
for or currently receiving anti-PD-1 or anti-PD-L1 ICI treatment
for prostate, colorectal, breast, ovarian and lung cancers.
Understanding the distinct Objective Response Rate to ICIs means
precise understanding of rates of response/non-response to
treatment, immune-related adverse events (irAEs) or HPD becomes
critical.
- Advance the understanding of genetic, metabolomic and
epigenetic mechanisms behind clinical outcomes, acquired resistance
and remission. The world-class expertise of the research team will
be guided through the multiomic complexity of genomes by focusing
on the functional genomic footprints of networks of 3D EpiSwitch
biomarkers strongly associated with clinical outcomes of ICI
treatments.
EpiSwitch® Checkpoint inhibitor Response Test
(CiRT)
Cancer does not exist in isolation. The most successful
approaches for treating cancer will need to consider the larger
systemic picture, comprising a combination of the tumour, its
interaction with its environment, the immune system, and a
patient’s genome and epigenome.[1,2] Most current predictive
biomarker tests focus on specific genetic markers such as (i)
tumour mutation burden (TMB), which measures the extent of DNA
mutations in a tumour acting as a proxy for how readily an engaged
immune system may recognize the tumour, or (ii) protein markers,
such as expression of PD-L1 protein in the tumour, a direct target
of ICI. These tests rely on retrieving a biopsy or resections from
a tumour, but these tumour-based methods show limited success at
predicting who will benefit from ICI treatment. A recent
retrospective analysis that systematically evaluated all clinical
trials leading to FDA approvals of ICIs from 2011 to 2019, found
that the most studied marker, tumour PD-L1 expression, was
predictive in only 24.4% of cases.[1,2] Unfortunately, the data
does not support either tool as a good predictor of response to ICI
treatment, as ICIs reset the immune system of the host to fight the
cancer and they do not directly target the tumour.
The EpiSwitch® CiRT is a first-of-its-kind blood test that
accurately predicts an individual cancer patient's therapeutic
response to immune checkpoint inhibitors (ICIs), providing unique
benefits for physicians in treatment planning and navigating
complex decisions.[3,4] ICIs offer a real hope of durable disease
control for some patients. Despite pre-screening with current
standard tests such as tumor PD-L1 expression, these ICIs offer a
long-term survival advantage to less than 1 in 4 patients, and many
may become seriously ill and require hospital admission.
An important consideration is the high cost of treatment with an
ICI. The anti-PD-1 and anti-PD-L1 therapies represent some of the
most expensive therapies employed today. In order to allow
equitable access by NHS patients to this technology, with the
promise of a disease-free future, better prediction of responders,
non-responders and informed clinical decision-making as to whether
ICI treatments should be continued or ended will have a significant
impact on costs and thus the number of patients who can be
treated.
EpiSwitch Hyper-progressive Immune Response Test
(HiRT)
Treatment with an ICI elicits a spectrum of side-effects and
immune related adverse events, including a subgroup of patients
with hyperprogressive disease (HPD). HPD patients demonstrate
significantly reduced progression free survival (PFS<2mo) and
overall survival (OS<5mo), with increased tumour growth rates
and underlying molecular trends of genomic amplifications (MDM2,
etc.) and lesion accumulation. A retrospective analysis of 24
studies and 3,109 patients revealed that the incidence of HPD
varies from 5.9% to 43.1% across different cancers, with an average
of 12%.[5]
With a special award from the Partnership for Accelerating
Cancer Treatment (PACT), Washington DC, OBD has developed the
prognostic HiRT, demonstrating over 85% accuracy for the first 60
participants in the independent validation cohort. When combined
with CiRT calls for response/non-response to ICI, it offers highly
specific prospective identification of patients who are likely to
1) respond to ICI therapy and 2) accurately identify patients
likely to exhibit an HPD response to ICI treatment, both extremely
useful for clinical patient management and potentially leading to
reduced costs, socioeconomic benefits and improved patient
outcome.
Dr Alexandre Akoulitchev, CSO at OBD, said: “The
EpiSwitch platform and its systemic biomarkers have already
delivered the most accurate test, as of today, for predicting
response to ICIs treatment – CiRT. The test has been adopted by a
growing number of institutions and practicing clinicians, and
patients in the USA and in private UK care have been benefiting
from its accuracy for many months now.
“The other benefit our consortium is offering is the power of
the EpiSwitch platform to capture the systemic aspects of cancer
biology. With the guidance from our academic and clinical
world-class experts, we can combine genetic, epigenetic and
metabolic specifics of every patient. We can gain insights into
predispositions to immune related adverse events (irAEs), side
effects to immune oncology treatment. Their burden is significant
and should not be overlooked. The CIRRP initiative is focused on
the challenge that could propel the UK as a world leader in cancer
treatment. We believe our consortium can help make it happen.”
Professor E. Jane Mellor, Department of Biochemistry,
University of Oxford, said: “It is a real privilege to be
involved in this potentially transformative initiative, to work
with visionary clinicians, entrepreneurs and basic scientists, and
to see how this disruptive technology, which combines epigenetics
and metabolomics, is being applied for the benefit of patients
within the NHS.”
References
[1] Hunter, E., et al. (2023). Development and validation of
blood‐based predictive biomarkers for response to PD‐1/PD-L1
checkpoint inhibitors: evidence of a universal systemic core of 3D
immunogenetic profiling across multiple oncological indications,
Cancers 15(10), 2696. https://www.mdpi.com/2072-6694/15/10/2696
[2] Zhao, B.; Zhao, H.; Zhao, J. (2020). Efficacy of PD-1/PD-L1
blockade monotherapy in clinical trials, Therapeutic Advances in
Medical Oncology, Vol. 12.
https://doi.org/10.1177/1758835920937612
[3] Oxford BioDynamics Plc. (2022). EpiSwitch CiRT.
https://www.mycirt.com
[4] Oxford BioDynamics Plc. (2023). Half-year report. HY results
link
[5] Park, H. J.; Kim, K. W.; Won, S. E.; Yoon, S.; Chae, Y. K.;
Tirumani, S. H.; Ramaiya, N. H. (2021). Definition, Incidence, and
Challenges for Assessment of Hyperprogressive Disease during Cancer
Treatment with Immune Checkpoint Inhibitors: A Systematic Review
and Meta-analysis, JAMA Network Open, Vol. 4, No. 3.
doi:10.1001/jamanetworkopen.2021.1136
For more information, please visit OBD’s website,
www.oxfordbiodynamics.com, or follow the Company on Twitter
(@OxBioDynamics) and LinkedIn.
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version on businesswire.com: https://www.businesswire.com/news/home/20240624074525/en/
Oxford BioDynamics Plc Jon Burrows, CEO Paul Stockdale, CFO +44
(0)1865 518910
Instinctif Partners (Media enquiries) Melanie Toyne-Sewell /
Katie Duffell Tel: +44 (0)20 7457 2020
OxfordBioDynamics@instinctif.com
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