11 November 2024
Syncona
Limited
Autolus receives US FDA
approval for AUCATZYL® (obe-cel)
Syncona Ltd, ("Syncona") a leading
life science investor focused on creating,
building and scaling global leaders in life science,
today notes that its portfolio company Autolus
Therapeutics ("Autolus"), an early-commercial stage
biopharmaceutical company developing next-generation programmed T
cell therapies, has announced that the U.S. Food and Drug
Administration (FDA) has granted marketing approval for
AUCATZYL® (obe-cel) for the treatment of adult patients
with relapsed or refractory B-cell precursor acute lymphoblastic
leukaemia (r/r B-ALL).
Key highlights are as
follows:
· The
approval of AUCATZYL was based on results from the FELIX clinical
trial of obe-cel in r/r B-ALL
· The
FELIX trial confirmed a strong safety profile compared to current
CD19 CAR T-cell therapies, with AUCATZYL the first CAR T-cell
therapy to be approved by the FDA with no requirement for a Risk
Evaluation and Mitigation Strategy programme, which is implemented
for drugs with serious safety concerns
· ALL is
an aggressive type of blood cancer where there are approximately
8,400 new cases diagnosed every year in the US and EU, with around
3,000 of these patients in the relapsed refractory
setting[1]
· Survival rates are very poor in adult r/r ALL, with a median
overall survival of eight months[2]
· In the
65 patients in the FELIX trial where efficacy could be evaluated,
63% achieved overall complete remission, representing the
elimination of all signs of cancer in response to
treatment
· Complete remission within three months was achieved in 42% of
patients, with a median duration of remission of 14.1
months
· AUCATZYL will be manufactured at Autolus' commercial
manufacturing site in Stevenage, UK, which will supply the therapy
globally
Chris Hollowood, CEO of Syncona Investment Management Limited,
said: "We are delighted for Autolus
to receive FDA approval for its novel CAR T-cell therapy for the
treatment of adult ALL. Adult ALL is a devastating disease and
AUCATZYL will bring a much-needed new treatment option to patients
suffering from the condition. This is a proud moment for Syncona.
We co-founded Autolus in 2014 and it is the first company we have
supported from the academic bench through to regulatory approval.
We would like to congratulate the Autolus team, as well as those
that have worked alongside the company, to help it reach this
important milestone."
Autolus management will host a
conference call and webcast on 11 November at 8:30
EST / 13:30 GMT, to discuss the AUCATZYL approval. To
listen to the webcast, please go to: https://www.autolus.com/investor-relations/events/
The announcement can be accessed on
Autolus' investor website at https://www.autolus.com/investor-relations/news/
and the full text of the announcement from Autolus
is contained below.
[ENDS]
Enquiries
Syncona Ltd
Natalie Garland-Collins / Fergus
Witt
Tel: +44 (0) 20 3981 7912
FTI Consulting
Ben Atwell / Tim Stamper
Tel: +44 (0) 20 3727 1000
About Syncona
Syncona's purpose is to invest to
extend and enhance human life. We do this by creating, building and
scaling companies to deliver transformational treatments to
patients in areas of high unmet need.
We aim to build and maintain a
diversified portfolio of 20-25 globally leading life science
businesses, across development stage, modality and therapeutic
area, for the benefit of all our stakeholders. We focus on
developing treatments that deliver patient impact by working in
close partnership with world-class academic founders and
experienced management teams. Our balance sheet underpins our
strategy, enabling us to take a long-term view as we look to
improve the lives of patients with no or poor treatment options,
build sustainable life science companies and deliver strong
risk-adjusted returns to shareholders.
Syncona Limited seeks to achieve returns over the long term.
Investors should seek to ensure they understand the risks and
opportunities of an investment in Syncona Limited, including the
information in our published documentation, before
investing.
Autolus Therapeutics
Announces FDA Approval of AUCATZYL® (obecabtagene autoleucel -
obe-cel) for adults with relapsed/refractory B-cell acute
lymphoblastic leukemia (r/r B-ALL)
- AUCATZYL is the first CAR T
therapy approved by the FDA with no requirement for a REMS program
(Risk Evaluation Mitigation Strategy)
- Approval based on FELIX
clinical trial of obe-cel in adult patients with r/r
B-ALL
- Conference call to be held
on November 11 at 08:30 am EDT/13:30 pm BST:
conference call participants should pre-register using the link at
the bottom of this press release
LONDON, November 8, 2024
-- Autolus Therapeutics plc (Nasdaq: AUTL), an
early-commercial stage biopharmaceutical company developing
next-generation programmed T cell therapies, today announces the
U.S. Food and Drug Administration (FDA) has granted marketing
approval for AUCATZYL® (obecabtagene autoleucel) for the treatment
of adult patients with relapsed or refractory B-cell precursor
acute lymphoblastic leukemia (r/r B-ALL).
"Adult ALL is an extremely
aggressive cancer, and there is a high unmet medical need that
exists in the treatment of patients with this disease once they
relapse, where historically they suffer from poor outcomes,"
said Elias Jabbour, MD, U.S. lead
investigator of the FELIX study and professor of Leukemia, ALL
Section Chief, at The University of Texas MD Anderson Cancer
Center, Houston, Texas. "This milestone approval,
based on the demonstrated clinical benefit of AUCATZYL, brings new
hope for adult patients with relapsed/refractory B-ALL."
AUCATZYL was approved by the FDA
based on results from the FELIX clinical trial of obe-cel in adult
patients with r/r B-ALL. In the morphological disease cohort, 94
patients received at least one infusion of AUCATZYL of which 65
patients had > 5% blasts in the bone
marrow after screening and prior to the start of lymphodepletion
therapy and received a conforming product, qualifying them as
efficacy evaluable. In the efficacy evaluable patients (n=65), 63%
achieved overall complete remission (OCR[3]) which includes 51% of patients with CR at any time and 12% patients with CRi
at any time. The major efficacy outcome was complete remission within 3 months, which was achieved in 42%
patients, and the median duration of remission (DOR) was 14.1
months. AUCATZYL showed low levels of Cytokine Release Syndrome
(CRS), with 3% Grade 3 events, and no Grade 4 or 5 events. Grade ≥
3 Immune Effector Cell-Associated Neurotoxicity Syndrome (ICANS)
was reported in 7% of patients. No REMS was required by the FDA for
AUCATZYL.
The safety of AUCATZYL includes a
boxed warning for CRS, neurologic toxicities, and secondary
hematological malignancies. ICANS, including fatal or
life-threatening reactions, occurred in patients receiving
AUCATZYL. T-cell malignancies have occurred following treatment of
hematologic malignancies with BCMA- and CD19-directed genetically
modified autologous T-cell immunotherapies. In the FELIX trial, the
most common non-laboratory adverse reactions (incidence ≥ 20%)
included CRS, infections-pathogen unspecified, musculoskeletal
pain, viral infections, fever, nausea, bacterial infectious
disorders, diarrhea, febrile neutropenia, ICANS, hypotension, pain,
fatigue, headache, encephalopathy, and hemorrhage.
"Based on the experience in the
FELIX trial AUCATZYL is highly active and can be well managed,
offering an attractive risk benefit profile for B-ALL patients."
said Dr. Claire Roddie, MD, PhD,
FRCPath, Lead investigator of the FELIX study and
Associate Professor of Haematology at the University College London
(UCL) Cancer Institute. "In the FELIX trial AUCATZYL has
shown long term persistence and deep responses which we believe are
critical for long term remissions in B-ALL."
"We are so pleased to now be able to
offer AUCATZYL, our
first commercial product, to adult r/r B-ALL patients in the U.S.
This approval would not have been possible without the support of
all the patients, their families and caregivers, their treating
physicians and the nurses and investigators at the treatment
centers - thank you" said Dr.
Christian Itin, Chief Executive Officer of Autolus. "This
milestone is the culmination of many years of hard work, the
foundational work by our partners at UCL and the unwavering
commitment of our internal team, our external partners and
shareholders. This is a proud day for Autolus."
AUCATZYL will be manufactured at
Autolus' dedicated commercial manufacturing site, the Nucleus, in
Stevenage, UK. The site was granted a
Manufacturer's Importation Authorization (MIA) and a GMP
certificate from the U.K. Medicines and Healthcare products
Regulatory Agency (MHRA) in March 2024, and was inspected as part
of the FDA approval process. No major or critical observations were
identified by either the MHRA or FDA during the site inspections.
The Nucleus will supply AUCATZYL globally,
with Cardinal Health serving as Autolus' commercial distribution
partner in the U.S. Autolus will now engage with existing treatment
centers to complete the onboarding process and initiate the first
scheduling of patients to make AUCATZYL commercially available in
the U.S.
ALL is an aggressive type of blood
cancer that can also involve the lymph nodes, spleen, liver,
central nervous system and other organs. Approximately 8,400 new
cases of adult ALL are diagnosed every year in the US and EU, with
around 3,000 patients in the relapsed refractory
setting.1 Survival rates remain very poor in adult
patients with r/r ALL, with median overall survival of eight
months.2 In frontline treatment for adult r/r B-ALL, up
to 50% of patients will ultimately relapse, and the
standard-of-care treatment can trigger severe toxicities and may be
burdensome for some patients.3,4
Marketing authorisation applications
(MAAs) for obe-cel in adult r/r ALL are being reviewed by the
regulators in both the EU and the UK, with a submission to the
European Medicines Agency (EMA) accepted in March 2024, and a
submission accepted by the UK MHRA in August 2024.
Conference Call
Management will host a conference
call and webcast on November 11 at 8:30 am EDT/1:30 pm BST to
discuss the AUCATZYL approval. Conference call participants should
pre-register using this
link to receive the dial-in
numbers and a personal PIN, which are required to access the
conference call.
A simultaneous audio webcast and
replay will be accessible on the
events section of Autolus'
website.
About Autolus Therapeutics plc
Autolus is a biopharmaceutical
company developing next-generation, programmed T cell therapies for
the treatment of cancer and autoimmune disease. Using a broad suite
of proprietary and modular T cell programming technologies, Autolus
is engineering precisely targeted, controlled and highly active T
cell therapies that are designed to better recognize target cells,
break down their defense mechanisms and eliminate these cells.
Autolus has an FDA approved product, AUCATZYL, and a pipeline of product
candidates in development for the treatment of hematological
malignancies, solid tumors and autoimmune diseases. For more
information, please visit www.autolus.com
About AUCATZYL® (obecabtagene autoleucel, obe-cel,
AUTO1)
AUCATZYL is
a B-lymphocyte antigen CD19 (CD19) chimeric antigen receptor (CAR)
T cell therapy designed to overcome the limitations in clinical
activity and safety compared to current CD19 CAR T cell
therapies. AUCATZYL
is designed with a fast target binding off-rate to
minimize excessive activation of the programmed T cells.
AUCATZYL was approved by
the FDA for the treatment of adult patients with relapsed or
refractory B-cell precursor acute lymphoblastic leukemia on
November 16, 2024. In the EU a regulatory submission to the EMA was
accepted in April 2024, while in the UK, an MAA was submitted to
MHRA in July 2024.
INDICATION
AUCATZYL® is a
CD19-directed genetically modified autologous T cell immunotherapy
indicated for the treatment of adult patients with relapsed or
refractory B-cell precursor acute lymphoblastic leukemia
(ALL).
IMPORTANT SAFETY INFORMATION
|
WARNING: CYTOKINE RELEASE SYNDROME, NEUROLOGIC
TOXICITIES, and SECONDARY HEMATOLOGICAL
MALIGNANCIES
· Cytokine Release Syndrome
(CRS) occurred in patients receiving AUCATZYL. Do not administer
AUCATZYL to patients with active infection or inflammatory
disorders. Prior to administering AUCATZYL, ensure that healthcare
providers have immediate access to medications and resuscitative
equipment to manage CRS.
· Immune Effector
Cell-Associated Neurotoxicity Syndrome (ICANS), including fatal and
life-threatening reactions, occurred in patients receiving
AUCATZYL, including concurrently with CRS or after CRS resolution.
Monitor for neurologic signs and symptoms after treatment with
AUCATZYL. Prior to administering AUCATZYL, ensure that healthcare
providers have immediate access to medications and resuscitative
equipment to manage neurologic toxicities. Provide supportive care
and/or corticosteroids, as needed.
· T cell malignancies have
occurred following treatment of hematologic malignancies with BCMA-
and CD19-directed genetically modified autologous T cell
immunotherapies.
|
WARNINGS AND PRECAUTIONS
Cytokine Release Syndrome (CRS)
Cytokine Release Syndrome (CRS)
occurred following treatment with AUCATZYL. CRS was reported in 75%
(75/100) of patients including Grade 3 CRS in 3% of patients. The
median time to onset of CRS was 8 days following the first infusion
(range: 1 to 23 days) with a median duration of 5 days (range: 1 to
21 days). The most common manifestations of CRS included fever
(100%), hypotension
(35%), and hypoxia (19%).
Prior to administering AUCATZYL,
ensure that healthcare providers have immediate access to
medications and resuscitative equipment to manage CRS.
During and following treatment with AUCATZYL,
closely monitor patients for signs and symptoms of CRS daily for at
least 14 days at the healthcare facility following the first
infusion. Continue to monitor patients for CRS for at least 4 weeks
following each infusion with AUCATZYL. Counsel patients to seek
immediate medical attention should signs or symptoms of CRS occur
at any time. At the first sign of CRS, immediately evaluate the
patient for hospitalization and institute treatment with supportive
care based on severity and consider further management per current
practice guidelines.
Neurologic Toxicities
Neurologic toxicities including
Immune Effector Cell-associated Neurotoxicity Syndrome (ICANS),
which were fatal or life-threatening, occurred following treatment
with AUCATZYL. Neurologic toxicities were reported in 64% (64/100)
of patients, including Grade ≥ 3 in 12% of patients. The median
time to onset of neurologic toxicities was 10 days (range: 1 to 246
days) with a median duration of 13 days (range: 1 to 904 days).
Among patients with neurologic toxicities, the most common symptoms
(> 5%) included ICANS (38%), headache (34%), encephalopathy
(33%), dizziness (22%), tremor (13%), anxiety (9%), insomnia (9%),
and delirium (8%).
Immune Effector Cell-associated Neurotoxicity Syndrome
(ICANS)
ICANS events occurred in 24%
(24/100) of patients, including Grade ≥ 3 in 7% (7/100) of
patients. Of the 24 patients who experienced ICANS, 33% (8/24)
experienced an onset after the first infusion, but prior to the second infusion of
AUCATZYL.
The median time to onset for ICANS
events after the first infusion was 8 days (range: 1 to 10 days)
and 6.5 days (range: 2 to 22 days) after the second infusion, with
a median duration of 8.5 days (range: 1 to 53 days).
Eighty-eight percent (21/24) of
patients received treatment for ICANS. All treated patients
received high-dose corticosteroids and 42% (10/24) of patients
received anti-epileptics prophylactically. Prior to administering
AUCATZYL, ensure that healthcare providers have immediate access to
medications and resuscitative equipment to manage ICANS.
Counsel patients to seek medical
attention should signs or symptoms of neurologic toxicity/ ICANS
occur. At the first sign of Neurologic Toxicity /ICANS, immediately
evaluate patients for hospitalization and institute treatment with
supportive care based on severity and consider further management
per current practice guidelines.
Effect on Ability to Drive and Use Machines
Due to the potential for neurologic
events, including altered mental status or seizures, patients
receiving AUCATZYL are at risk for altered or decreased
consciousness or coordination in the eight weeks following AUCATZYL
infusion or until resolution of the neurological event by the
treating physician. Advise patients to refrain from driving and
engaging in hazardous occupations or activities, such as operating
heavy or potentially dangerous machinery, during this initial
period.
Prolonged Cytopenias
Patients may exhibit cytopenias
including anemia, neutropenia, and thrombocytopenia for several
weeks after treatment with lymphodepleting chemotherapy and
AUCATZYL. In patients who were responders
to AUCATZYL, Grade
≥ 3 cytopenias that persisted beyond Day 30 following
AUCATZYL infusion were
observed in 71% (29/41) of patients and included neutropenia (66%,
27/41) and thrombocytopenia (54%, 22/41). Grade 3 or higher
cytopenias that persisted beyond Day 60 following
AUCATZYL infusion was
observed in 27% (11/41) of patients and included neutropenia (17%,
7/41) and thrombocytopenia (15%, 6/41). Monitor blood counts after
AUCATZYL infusion.
Infections
Severe, including life-threatening
and fatal infections occurred in patients after AUCATZYL infusion.
Non‑COVID-19
infections of all grades occurred in 67% (67/100) of patients.
Grade 3 or higher non-COVID-19 infections occurred in 41% (41/100)
of patients. AUCATZYL should not be
administered to patients with clinically significant active
systemic infections. Monitor patients for signs and symptoms of
infection before and after AUCATZYL infusion and treat
appropriately. Administer
prophylactic antimicrobials according to local
guidelines.
Grade 3 or higher febrile
neutropenia was observed in 26%
(26/100) of patients after AUCATZYL
infusion and may be concurrent with CRS. In the event of febrile
neutropenia, evaluate for infection and manage with broad-spectrum
antibiotics, fluids, and other supportive care as medically
indicated.
Viral reactivation, potentially
severe or life-threatening, can occur in patients treated with
drugs directed against B cells. There is no experience with
manufacturing AUCATZYL for patients with a positive test for human
immunodeficiency virus (HIV) or with active hepatitis B virus (HBV)
or active hepatitis C virus (HCV). Perform screening for HBV, HCV
and HIV in accordance with clinical guidelines before collection of
cells for manufacturing.
Hypogammaglobulinemia
Hypogammaglobulinemia and B-cell
aplasia can occur in patients after AUCATZYL infusion.
Hypogammaglobulinemia was reported in 10%
(10/100) of patients treated with AUCATZYL
including Grade 3 events in 2 patients
(2%).
Immunoglobulin levels should be
monitored after treatment with AUCATZYL and managed per
institutional guidelines including infection precautions,
antibiotic or antiviral prophylaxis, and immunoglobulin
replacement.
The safety of immunization with live
viral vaccines during or following treatment with AUCATZYL has not
been studied. Vaccination with live viral vaccines is not
recommended for at least 6 weeks prior to the start of
lymphodepleting chemotherapy treatment, during AUCATZYL treatment,
and until immune recovery following treatment with
AUCATZYL.
Hemophagocytic Lymphohistiocytosis/Macrophage Activation
Syndrome (HLH/MAS)
HLH/MAS including
fatal and life-threatening reactions
occurred after treatment with AUCATZYL.
HLH/MAS was reported in 2% (2/100) of patients and included Grade 3
and Grade 4 events with a time of onset at Day 22 and Day 41,
respectively. One patient experienced a concurrent ICANS events
after AUCATZYL infusion and died due to
sepsis with ongoing HLH/MAS that had not
resolved. Administer treatment for HLH/MAS
according to institutional standards.
Hypersensitivity Reactions
Serious hypersensitivity reactions,
including anaphylaxis, may occur due to dimethyl sulfoxide (DMSO),
an excipient used in AUCATZYL. Observe patients for
hypersensitivity reactions during and after AUCATZYL
infusion.
Secondary Malignancies
Patients treated with AUCATZYL may
develop secondary malignancies. T cell malignancies have occurred
following treatment of hematologic malignancies with BCMA- and
CD19-directed genetically modified autologous T cell
immunotherapies. Mature T cell malignancies, including CAR-positive
tumors, may present as soon as weeks following infusion, and may
include fatal outcomes. Monitor lifelong for secondary
malignancies. In the event that a secondary malignancy occurs,
contact Autolus at 1-855-288-5227 for reporting and to obtain
instructions on the collection of patient samples for
testing.
Adverse Reactions
The safety of AUCATZYL was evaluated
in the FELIX study in which 100 patients with relapsed or
refractory B-cell acute lymphoblastic leukemia (B-ALL) received
AUCATZYL at a median dose of 410 × 106 CD19 CAR-positive
viable T cells (range: 10 to 480 × 106 CD19 CAR-positive
viable T cells with 90% of patients receiving the recommended dose
of 410 × 106 +/- 25%).
The most common serious adverse
reactions of any Grade (incidence ≥ 2%) included
infections-pathogen unspecified, febrile neutropenia, ICANS, CRS,
fever, bacterial infectious disorders, encephalopathy, fungal
infections, hemorrhage, respiratory failure, hypotension, ascites,
HLH/MAS, thrombosis and hypoxia.
Nine patients (9%) experienced fatal adverse
reactions which included infections (sepsis, pneumonia,
peritonitis), ascites, pulmonary embolism, acute respiratory
distress syndrome, HLH/MAS and ICANS. Of the 9 patients, five
patients who died from infections had pre-existing and ongoing
neutropenia prior to receiving bridging therapy, lymphodepletion
chemotherapy treatment and/or AUCATZYL.
Please see full Prescribing
Information, including BOXED
WARNING and Medication Guide.
Forward-Looking Statements
This press release contains
forward-looking statements within the meaning of the "safe harbor"
provisions of the Private Securities Litigation Reform Act of 1995.
Forward-looking statements are statements that are not historical
facts, and in some cases can be identified by terms such as "may,"
"will," "could," "expects," "plans," "anticipates," and "believes."
These statements include, but are not limited to: statements
regarding the market and therapeutic potential of for
AUCATZYL for adult r/r B-ALL; Autolus' development and commercialization of its product
candidates; the expected clinical benefits of AUCATZYL; Autolus' manufacturing,
sales and marketing plans for AUCATZYL, including expectations
regarding the timing of commercial launch in the United States and
the ability to reach patients in a timely manner; the amount and
timing of milestone payments under Autolus' collaboration and
license agreements; and future development plans of
AUCATZYL, including the
timing or likelihood of expansion into additional markets or
geographies and related regulatory approvals. Any forward-looking
statements are based on management's current views and assumptions
and involve risks and uncertainties that could cause actual
results, performance, or events to differ materially from those
expressed or implied in such statements. Actual results and the
timing of events could differ materially from those anticipated in
such forward-looking statements as a result of various risks and
uncertainties, which include, without limitation: Autolus' ability
to maintain regulatory approval of AUCATZYL; its ability to execute its
commercialization strategy for AUCATZYL; its ability to develop,
manufacture and commercialize its other product candidates and the
timing or likelihood of expansion of AUCATZYL into additional markets or
geographies; Autolus' ability to establish and expand a commercial
infrastructure and to successfully launch, market and sell
AUCATZYL; actions of
regulatory agencies, which may affect the initiation, timing and
progress of clinical trials or future regulatory approval; the
labelling for AUCATZYL/obe-cel in any future indication or
patient population, if approved; the potential for payors to delay,
limit or deny coverage for AUCATZYL; Autolus' ability to obtain,
maintain and enforce intellectual property protection for
AUCATZYL or any product
candidates it is developing; the results of clinical trials are not
always being predictive of future results; the cost, timing and
results of clinical trials; that many product candidates do not
become approved drugs on a timely or cost effective basis or at
all; the ability to enroll patients in clinical trials; and
possible safety and efficacy concerns. For a discussion of other
risks and uncertainties, and other important factors, any of which
could cause Autolus' actual results to differ from those contained
in the forward-looking statements, see the section titled "Risk
Factors" in Autolus' Annual Report on Form 10-K filed with the
Securities and Exchange Commission, or the SEC, on March 21, 2024
as well as discussions of potential risks, uncertainties, and other
important factors in Autolus' subsequent filings with the
Securities and Exchange Commission. All information in this press
release is as of the date of the release, and Autolus undertakes no
obligation to publicly update any forward-looking statement,
whether as a result of new information, future events, or
otherwise, except as required by law. You should, therefore, not
rely on these forward-looking statements as representing Autolus'
views as of any date subsequent to the date of this press
release.
Contact:
Olivia Manser
+44 (0) 7780 471 568
o.manser@autolus.com
Julia Wilson
+44 (0) 7818 430877
j.wilson@autolus.com
Susan A. Noonan
S.A. Noonan
Communications
+1-917-513-5303
susan@sanoonan.com
References
1. SEER and EUCAN estimates for US
and EU respectively
2.
https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7894150/
3. Aureli A, Marziani B, Venditti A,
Sconocchia T, Sconocchia G. Acute lymphoblastic leukemia
immunotherapy treatment: now, next, and beyond. Cancers (Basel).
2023;15:3346.
4. Dhakal P, Kaur J, Gundabolu K,
Bhatt VR. Immunotherapeutic options for management of relapsed or
refractory B-cell acute lymphoblastic leukemia: how to select newly
approved agents? Leuk Lymphoma. 2020;61:7-17.
11/24 US-AUC-0082