Issued: 19 November 2024, London
UK
Linerixibat shows positive Phase III results in cholestatic
pruritus (relentless itch) in primary biliary cholangitis
(PBC)
· Primary endpoint met with a statistically significant
improvement in itch over 24 weeks compared
with placebo
· Linerixibat has the potential to be the first global therapy
indicated to treat itch in PBC
· Cholestatic pruritus is one of the most common symptoms of
PBC, an autoimmune disease that can lead to liver
failure
GSK plc (LSE/NYSE: GSK) today
announced positive headline results of GLISTEN, the ongoing global
phase III clinical trial evaluating linerixibat, an investigational
targeted inhibitor of the ileal bile acid transporter (IBAT), in
adults with cholestatic pruritus (relentless itch) associated with
primary biliary cholangitis (PBC), a rare autoimmune liver
disease.
GLISTEN met its primary endpoint,
with linerixibat resulting in an improvement in itch, as
demonstrated by a statistically significant reduction from baseline
in monthly itch score over 24 weeks versus placebo. The trial
recruited PBC patients with moderate to severe itch, who were
receiving stable doses of guideline-suggested therapies for
pruritus, or were treatment naïve, or had been previously treated.
The preliminary safety results are generally consistent with those
seen in prior studies of linerixibat. Further analysis of these data is ongoing.
Kaivan Khavandi, SVP & Global Head, Respiratory/Immunology
R&D, GSK, said:
"Linerixibat has the potential to be the first global therapy
specifically developed to treat itch in PBC. These positive data
suggest that it could have a place in supporting patients whose
quality of life is significantly affected in multiple ways by
persistent itching."
People who have been diagnosed with
PBC will reach 510,000 globally by 2030, and more than 240,000
people will experience relentless itch requiring treatment,
representing a significant unmet need. 1,2,3,4 Current
guideline suggested therapies available for cholestatic pruritus
are inadequate, with known limited impact on itch, and poor
tolerability. 5,6 PBC is a rare
disease of the bile ducts that primarily affects women and can
cause liver damage and possible liver failure if untreated. One of
the most common symptoms is constant, relentless itching or
skin-crawling sensations, as well as fatigue that is often made
worse by itching at night. The disease currently has no
cure.
Carol Roberts, President, The PBCers
Organization, said: "The itch
associated with PBC for many patients is unrelenting and often
severe but is a symptom that is frequently overlooked or dismissed.
It has a significant impact on quality of life and mental health
for people with PBC. The potential of a treatment option that
addresses a root cause of itch answers a previously unmet need for
people with PBC."
The full results of GLISTEN will be
presented at a future scientific congress. Linerixibat
is currently not approved anywhere in the world;
it has been granted Orphan Drug Designation in both the US and
EU.
About cholestatic pruritus in primary biliary
cholangitis
In primary biliary cholangitis (PBC),
a cholestatic liver disease, bile flow from the liver is disrupted.
The resulting excess bile acids in circulation are thought to play
a causal role in cholestatic pruritus, an internal itch that cannot
be relieved by scratching. Pruritus can occur at any stage of PBC
disease and is experienced by up to 90% of people living with
PBC.4 The first line treatment for PBC controls disease
in approximately 70% of patients, but does not reduce the severity
or impact of the pruritus.7 Cholestatic pruritus is a
serious condition that can be debilitating, with patients
experiencing sleep disturbance, fatigue, impaired quality of life
and even sometimes requiring liver transplantation in the absence
of liver failure.4
About linerixibat (GSK2330672)
Linerixibat is an ileal bile acid
transporter (IBAT) inhibitor, a targeted oral agent with potential
to treat cholestatic pruritus (itch) associated with the rare
autoimmune liver disease known as primary biliary cholangitis
(PBC). By inhibiting bile acid re-uptake, linerixibat aims to
address a root cause of cholestatic pruritus. The US Food and Drug
Administration and the European Medicines Agency have granted
orphan drug designation for linerixibat in the treatment of
cholestatic pruritus associated with PBC.
About the GLISTEN trial
GLISTEN is an ongoing double-blind,
randomised, placebo-controlled, phase III trial (NCT04950127; GSK
study 212620) conducted in PBC patients with cholestatic pruritus.
The primary analysis evaluated the efficacy (including impact on
sleep) and safety of linerixibat compared with placebo.
Participants with moderate to severe itch were enrolled. The trial
includes multiple arms where participants receive either
linerixibat or placebo and have the potential to cross over at one
point in the study. Primary and secondary outcome measures were
assessed using the Numerical Rating Scale (NRS) for worst itch and
itch-related sleep interference, and the PBC-40 questionnaire for
quality of life. Stable use of guideline suggested anti-itch
therapy was permitted. A small number of participants remain
ongoing in an exploratory portion of the trial.
About GSK
GSK is a global biopharma company
with a purpose to unite science, technology, and talent to get
ahead of disease together. Find out more at
gsk.com.
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Cautionary statement regarding forward-looking
statements
GSK cautions
investors that any forward-looking statements or projections made
by GSK, including those made in this announcement, are subject to
risks and uncertainties that may cause actual results to differ
materially from those projected. Such factors include, but are not
limited to, those described under Item 3.D "Risk factors" in GSK's
Annual Report on Form 20-F for 2023, and GSK's Q3 Results for
2024.
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References
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2 Sebode M et al. Z Gastroenterol. 2020 May;58(5):431-438
3 Tanaka A et al.
Hepatol
Res. 2019
Aug;49(8):881-889
4 Gungabissoon U, et al..
BMJ Open Gastroenterol
2024; 11(1)
5 Hegade VS,
et al. Clin Gastroenterol
Hepatol. 2019 Jun;17(7):1379-1387
6 Mayo MJ et
al. Dig Dis Sci. 2023
Mar;68(3):995-1005
7 Carbone M, et al.
Lancet
Gastroenterol Hepatol. 2018 Jul
13;3(9):626-634