20% of all subjects that completed the 24-week
treatment period achieved SALT ≤ 20
29% of completed subjects with moderate to
severe disease (baseline SALT 35 to <95) achieved SALT ≤ 20
EQ101 was well tolerated in subjects with
alopecia areata with no serious adverse events reported
Data supports advancing EQ101 development in
alopecia areata to include dose and delivery optimization
Data provides further support for opportunistic
expansion in other dermatological conditions where IL-2, IL-9 and
IL-15 inhibition is important such as vitiligo and atopic
dermatitis
Equillium Inc. (Nasdaq: EQ), a clinical-stage biotechnology
company leveraging a deep understanding of immunobiology to develop
novel therapeutics to treat severe autoimmune and inflammatory
disorders, today announced positive topline data from its Phase 2,
single dose, proof-of-concept (PoC) study of EQ101 in adult
patients with moderate, severe or very-severe alopecia areata (AA),
an autoimmune disease driven by an immune cell attack of the hair
follicles that causes hair loss. The primary objectives of the
study were to evaluate the safety and tolerability profile of
EQ101, as well as signs of efficacy using Severity of Alopecia Tool
(SALT) scores, where a score of 100 represents total scalp hair
loss and a score of 0 represents no scalp hair loss.
Results from the study demonstrated a favorable safety and
tolerability profile with no serious adverse events (SAEs), and
improvements in SALT scores above the published historically low
placebo response rates. Of all subjects that completed 24 weeks of
treatment (baseline SALT of 35 to 100, n=25), 20% achieved a SALT
score of less than or equal to 20 by week 24. Of those subjects
with moderate to severe AA at baseline that completed 24 weeks of
treatment (SALT score 35 to < 95, n=17), 29% achieved a SALT
score of less than or equal to 20 by week 24, and a mean SALT
improvement from baseline of 18%.
“The results from this Phase 2 proof-of-concept study of EQ101
in alopecia areata patients are very compelling,” said principal
investigator, Rodney Sinclair, MD, Sinclair Dermatology, Melbourne,
Victoria, Australia. “Placebo rates in this indication across
studies have been consistently low – generally less than 10 percent
of patients achieve a SALT score of 20 or less. To have 20 percent
of patients completing the study reach a SALT score of less than or
equal to 20 across all subjects, and 29 percent of moderate and
severe patients, is a very encouraging sign of drug activity. With
Janus kinase inhibitors currently the only approved therapies to
treat alopecia areata, a significant unmet need remains for novel
drug mechanisms that are effective and well tolerated; and the
targeted multi-cytokine activity of EQ101 represents a welcome
approach.”
EQ101 is a novel multi-cytokine inhibitor with a targeted
mechanism of action against cytokines IL-2, IL-9 and IL-15, which
are key drivers of the pathogenic T cells implicated in AA. To be
eligible for the Phase 2 study for the treatment of AA, subjects
were required to have at least 35 percent scalp hair loss due to
AA, as measured by SALT, and a current hair loss episode of at
least six months, but not more than seven years. The study enrolled
36 subjects at multiple clinical trial sites, with a mean baseline
SALT score of 76. Twenty-five subjects completed the study; eleven
subjects discontinued the study early, of which only five were
attributed to adverse events. Throughout 24 weeks of treatment and
4 weeks of follow up, EQ101 was well tolerated with no SAEs and no
notable changes in safety laboratory (coagulation, hematology,
chemistry, liver function, urinalysis, cholesterol),
electrocardiogram, vital signs, or physical exam findings were
reported. The majority (98.9%) of adverse events were Grade 1 or 2,
with the most common being upper respiratory tract infection,
headache and fatigue. The two (1.1%) Grade 3 events in two subjects
considered related to study treatment were a case of transient
lymphocytopenia and fatigue.
Table 1 outlines response data on the 25 subjects that completed
24 weeks of treatment:
Table 1
Completed Subjects (24 weeks of
treatment)
SALT Baseline by
Subgroups
n (%)
Mean SALT @ Baseline
SALT ≤ 20 @ W24
n (%)
Mean SALT Improvement from
Baseline @ W24
35 to <95
(moderate to severe)
17 (68%)
66.1
5 (29.4%)
18.4%
35 to <50 (moderate)
3 (12%)
39.9
2 (66.7%)
23.8%
50 to <95 (severe)
14 (56%)
71.8
3 (21.4%)
17.2%
95 to 100 (very severe,
AU/AT*)
8 (32%)
99.8
0 (0.0%)
3.1%
Completed Subjects 35 - 100
25
76.9
5 (20%)
13.5%
* Alopecia areata universalis (AU) or
totalis (AT)
To better understand the depth of response in baseline SALT
improvement, Equillium conducted an analysis of 21 subjects
characterized as responders (excluding subjects that had a 20% or
more increase in SALT score, n=4) as shown in Table 2:
Table 2
Completed Subjects evaluated as
Responders**
SALT Baseline by Subgroups
Mean SALT Improvement from Baseline @
W24
n
(%)
35 to <95 (moderate to
severe)
13
40.5%
35 to <50 (moderate)
2
78.8%
50 to <95 (severe)
11
33.5%
95 to 100 (very severe, AU/AT)
8
3.1%
Responders Only: 35 - 100
21
26.3%
** Responders (n=21): excludes subjects
that had a 20% or more increase in SALT score (n=4)
In addition to these compelling signs of clinical activity,
preliminary data indicate reductions of cell surface CD132 on both
CD8 and NK cells in peripheral blood consistent with EQ101 target
engagement and pharmacodynamic response.
“We are very pleased with these positive clinical results,
indicating EQ101 to be well-tolerated and clinically efficacious in
alopecia areata patients with significant hair loss,” said Dr.
Maple Fung, chief medical officer at Equillium. “We look forward to
transitioning to a subcutaneous delivery in placebo-controlled,
dose and regimen optimization studies where we expect to continue
to investigate EQ101 across alopecia areata disease severity
subgroups, including the important population of moderate patients
with a SALT score between 35 and less than 50. Though hair loss is
lower in patients with moderate disease, the impact on their
quality of life is very much in line with more severe patients, yet
current systemic Janus kinase inhibitor therapies are only approved
for patients with severe disease.”
A presentation outlining the data is available on the “Events
& Presentations” page under the Investor Relations tab on the
Company’s website at
https://www.equilliumbio.com/investors/events-and-presentations/default.aspx.
About EQ101 Phase 2 Study in Alopecia Areata
This was a multicenter, open-label, proof-of-concept Phase 2
study in 36 adult subjects between 18 and 60 years of age, with at
least 35% scalp hair loss due to alopecia areata (AA) with a
current hair loss episode of at least 6 months but not more than 7
years. Subjects were dosed intravenously once weekly for 24 weeks
with EQ101 at a dose level of 2 mg/kg, and subsequently followed
for an additional four weeks. The primary objective of the study
was to evaluate the safety profile and tolerability of EQ101 in
subjects with moderate to very severe AA over a 24-week treatment
period; secondary objectives included the evaluation of drug
efficacy, pharmacokinetic/pharmacodynamic (PK/PD) properties, and
assessment of changes in patient biomarkers.
About Alopecia Areata
Alopecia areata (AA) is a common, inflammatory, non-scarring
condition resulting in hair loss that occurs when the immune system
attacks hair follicles on any hair-bearing area of the body, most
frequently on the head and face. The lifetime incidence of AA is
estimated at about two percent globally, affecting men and women of
all racial and ethnic groups. It has a higher prevalence in
children and adolescents with 40% of cases occurring prior to age
20, and 80% before age 40. AA is associated with other
immune-mediated or autoimmune disorders such as thyroiditis,
vitiligo, and atopic diseases. Approximately 50% of patients have
chronic relapsing, remitting disease persisting more than 12 months
and approximately 10% to 35% ultimately experience complete loss of
scalp hair (alopecia totalis, or AT) or complete loss of scalp and
body hair (alopecia universalis, or AU). AA has a significant
psychosocial burden that can have a significant negative impact on
health-related quality of life and has been associated with
depression and anxiety.
There are currently limited treatment options and few countries
have approved drugs for the treatment of AA. IL-2, IL-9, and IL-15
are cytokines of the common gamma chain receptor known to be
upregulated in animal models and human biopsies of AA and may
provide a selective and potent approach to disease treatment.
About Multi-Cytokine Platform and Multi-Cytokine Inhibitors
EQ101 & EQ302
Our proprietary multi-cytokine platform generates rationally
designed composite peptides that selectively block key cytokines at
the shared receptor level targeting pathogenic cytokine
redundancies and synergies while preserving non-pathogenic
signaling. This approach is expected to avoid the broad
immuno-suppression and off-target safety liabilities that may be
associated with other therapeutic classes, such as Janus kinase
inhibitors. Many immune-mediated diseases are driven by the same
combination of dysregulated cytokines, and we believe identifying
the key cytokines for these diseases will allow us to target and
develop customized treatment strategies for multiple autoimmune and
inflammatory diseases.
Current platform assets include EQ101, a clinical stage,
first-in-class, selective, tri-specific inhibitor of IL-2, IL-9,
and IL-15 for intravenous and subcutaneous delivery, and EQ302, a
preclinical stage, first-in-class, selective, bi-specific inhibitor
of IL-15 and IL-21 for oral delivery.
About Equillium
Equillium is a clinical-stage biotechnology company leveraging a
deep understanding of immunobiology to develop novel therapeutics
to treat severe autoimmune and inflammatory disorders with high
unmet medical need. The company’s pipeline consists of the
following novel first-in-class immunomodulatory assets and product
platform targeting immuno-inflammatory pathways. EQ101: a selective
tri-specific cytokine inhibitor targeting IL-2, IL-9, and IL-15;
recently announced positive results from a Phase 2 proof-of-concept
clinical study of patients with alopecia areata in Australia and
New Zealand by Equillium’s Australian subsidiary as the trial
sponsor. EQ302: an orally delivered, selective bi-specific cytokine
inhibitor targeting IL-15 and IL-21; currently in pre-clinical
development. The multi-cytokine platform: generates rationally
designed composite peptides that selectively block key cytokines at
the shared receptor level targeting pathogenic cytokine
redundancies and synergies while preserving non-pathogenic
signaling. Itolizumab: a monoclonal antibody that targets the
CD6-ALCAM signaling pathway which plays a central role in the
modulation of effector T cells; currently under evaluation in a
Phase 3 clinical study of patients with acute graft-versus-host
disease (aGVHD) and recently completed a Phase 1b clinical study of
patients with lupus/lupus nephritis. Equillium acquired rights to
itolizumab through an exclusive partnership with Biocon Limited and
has entered a strategic partnership with Ono Pharmaceutical Co.,
Ltd., for the development and commercialization of itolizumab under
an option and asset purchase agreement.
For more information, visit www.equilliumbio.com.
Forward Looking Statements
Statements contained in this press release regarding matters
that are not historical facts are “forward-looking Statements”
within the meaning of the Private Securities Litigation Reform Act
of 1995. Forward-looking statements may be identified by the use of
words such as “anticipate”, “believe”, “could”, “continue”,
“expect”, “estimate”, “may”, “plan”, “outlook”, “future” and
“project” and other similar expressions that predict or indicate
future events or trends or that are not statements of historical
matters. These statements include, but are not limited to,
statements regarding Equillium’s plans for further developing
EQ101, EQ302 and itolizumab and the expected timeline for
initiation of and results from clinical studies, and the potential
benefits of Equillium’s product candidates. Because such statements
are subject to risks and uncertainties, many of which are outside
of Equillium’s control, actual results may differ materially from
those expressed or implied by such forward-looking statements.
Risks that contribute to the uncertain nature of the
forward-looking statements include: Equillium’s ability to execute
its plans and strategies; risks related to performing clinical and
pre-clinical studies; whether the results from clinical and
pre-clinical studies will validate and support the safety and
efficacy of Equillium’s product candidates; changes in the
competitive landscape; the risk that the FDA will expand the use of
approved JAK inhibitors for the treatment of moderate AA;
uncertainties related to Equillium’s capital requirements; and
having to use cash in ways or on timing other than expected and the
impact of market volatility on cash reserves. These and other risks
and uncertainties are described more fully under the caption "Risk
Factors" and elsewhere in Equillium's filings and reports, which
may be accessed for free by visiting the Securities and Exchange
Commission’s website and on Equillium’s website under the heading
“Investors.” Investors should take such risks into account and
should not rely on forward-looking statements when making
investment decisions. All forward-looking statements contained in
this press release speak only as of the date on which they were
made. Equillium undertakes no obligation to update such statements
to reflect events that occur or circumstances that exist after the
date on which they were made, except as required by law.
View source
version on businesswire.com: https://www.businesswire.com/news/home/20240604360716/en/
Investor Contact Michael Moore Vice President, Investor
Relations & Corporate Communications 619-302-4431
ir@equilliumbio.com
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