Long-term KRESLADITM follow-up data demonstrate
survival of 100% in the absence of allogeneic hematopoietic stem
cell transplantation (HSCT) from 18 to 45 months with a
well-tolerated safety profile in all nine patients with severe
LAD-I
Previously disclosed results from the global
RP-L102 Fanconi Anemia Phase 1/2 trial demonstrate genetic and
phenotypic correction combined with hematologic stabilization
extending to 42 months with polyclonal integration patterns
Sustained and clinically meaningful hemoglobin
improvement and well-tolerated safety profile in PKD patients up to
36 months after RP-L301 treatment
Rocket Pharmaceuticals, Inc. (NASDAQ: RCKT), a fully integrated,
late-stage biotechnology company advancing a sustainable pipeline
of genetic therapies for rare disorders with high unmet need, today
announced longer-term data updates from its lentiviral (LV) vector
hematology portfolio presented at the 27th Annual Meeting of the
American Society of Gene and Cell Therapy (ASGCT). Data updates
demonstrate the continued safety and efficacy of the Phase 1/2
pivotal studies of KRESLADI™ (marnetegragene autotemcel) for severe
Leukocyte Adhesion Deficiency-I (LAD-I) and RP-L102 for Fanconi
Anemia (FA), in addition to the Phase 1 study of RP-L301 for
Pyruvate Kinase Deficiency (PKD).
“The positive updates presented at this year’s annual meeting
demonstrate the sustained safety and efficacy across the totality
of our LV hematology portfolio,” said Jonathan Schwartz, M.D.,
Chief Medical & Gene Therapy Officer, Rocket Pharmaceuticals.
“Ahead of the upcoming PDUFA date, KRESLADITM continues to
demonstrate 100% HSCT-free survival and significant reductions in
infection-related hospitalizations following engraftment in
patients with severe LAD-I. In our pivotal studies of RP-L102 for
Fanconi Anemia, we continue to see maintained genetic and
phenotypic correction combined with hematologic stabilization.
Additionally, our Phase 1 study of RP-L301 for PKD shows sustained
clinically meaningful hemoglobin improvement in all patients. We
are very pleased with the safety profile demonstrated across our LV
hematology portfolio, with no drug-related serious adverse events
observed to date.”
Autologous Ex-Vivo Lentiviral Gene Therapy for Pediatric
Patients with Severe Leukocyte Adhesion Deficiency-I Provides
Sustained Efficacy with a Well-Tolerated Safety Profile
The oral presentation includes positive, updated data (cut-off
July 24, 2023) from the global Phase 1/2 pivotal studies
demonstrating sustained efficacy and safety of KRESLADITM from 18
to 45 months of follow-up for all nine patients with severe
LAD-I.
- Observed 100% survival in the absence of allogeneic HSCT at
least 18 months post-infusion in all nine patients; all patients
enrolled at less than 12 months of age have surpassed 24 months
without HSCT. All primary and secondary endpoints were met,
including sustained genetic and phenotypic correction.
- When compared with pre-treatment history, data showed
substantial decreases in the incidences of significant infections
requiring hospitalization or intravenous antimicrobials, combined
with evidence of resolution of LAD-I-related skin and periodontal
lesions and restoration of wound repair capabilities.
- KRESLADITM was well-tolerated in all patients with no
drug-related serious adverse events reported to date. Adverse
events related to other study procedures, including busulfan
conditioning, have been previously disclosed and are consistent
with the safety profiles of those agents and procedures. No cases
of graft failure or autologous graft-versus-host-disease (GvHD)
were reported.
- Based on the positive efficacy and safety data from the global
pivotal studies of KRESLADITM for severe LAD-I, the Biologics
License Application (BLA) was accepted for review by the U.S. Food
and Drug Administration (FDA) who has set the New Prescription Drug
User Fee Act (PDUFA) target date of June 30, 2024.
Lentiviral-Mediated Gene Therapy (RP-L102) for Fanconi Anemia
[Group A] is Associated with Polyclonal Integration Patterns in the
Absence of Conditioning
The oral presentation includes positive, updated data (cut-off
September 11, 2023) from the global Phase 1/2 pivotal studies of
RP-L102, Rocket’s ex vivo LV gene therapy candidate for FA.
- Consistent with results observed from the clinical program,
RP-L102 is a potentially curative therapy to prevent FA-related
bone marrow failure (BMF), which can be administered without a
suitable allogeneic donor or transplant-related toxicities.
- RP-L102 demonstrates sustained and progressively increasing
genetic correction in eight of 12 patients with greater than 12
months of follow-up. Observed genetic correction is associated with
phenotypic correction and hematologic stability.
- RP-L102 remains well-tolerated with no significant safety
signals.
- For the first time, data demonstrate that RP-L102 confers
polyclonal insertion patterns indicative of long-term hematopoietic
stem cell repopulation of the bone marrow and peripheral blood and
clonal diversity in the absence of conditioning.
- Based on the positive efficacy and safety data from the global
pivotal studies of RP-L102 for FA, the European Medicines Agency
(EMA) accepted the Marketing Authorization Application (MAA) for
review. Rocket expects to submit the BLA to the FDA in the first
half of 2024.
Gene Therapy for Adult and Pediatric Patients with Severe
Pyruvate Kinase Deficiency: Results from a Global Study of
RP-L301
The oral presentation includes positive, updated data (cut-off
February 5, 2024) from the Phase 1 study from two adult patients
with PKD treated with RP-L301 followed up to 36 months and two
pediatric patients followed up to 12 months.
- Sustained and clinically meaningful hemoglobin improvement
observed in all patients including hemoglobin normalization in
three of four patients. No patients have required red blood cell
transfusion following neutrophil engraftment. Improvements in
hemoglobin supported by improved markers of hemolysis and quality
of life have been observed.
- RP-L301 remains well-tolerated, with no drug-related serious
adverse events.
- Insertion site analyses in the peripheral blood and bone marrow
for both adult patients through 36 months post-RP-L301 demonstrated
highly polyclonal patterns with no clonal dominance or insertional
mutagenesis. Testing is ongoing for pediatric patients who were
more recently treated.
- Based on the positive safety and efficacy data from the global
Phase 1 study of RP-L301 for PKD, Rocket is working towards
initiation of the Phase 2 pivotal study.
About KRESLADITM (marnetegragene autotemcel)
KRESLADITM is an investigational gene therapy for severe
Leukocyte Adhesion Deficiency-I (LAD-I) that contains autologous
(patient-derived) hematopoietic stem cells that have been
genetically modified with a lentiviral (LV) vector to deliver a
functional copy of the ITGB2 gene, which encodes for the beta-2
integrin component CD18, a key protein that facilitates leukocyte
adhesion and enables their extravasation from blood vessels to
fight infection. Rocket holds FDA Regenerative Medicine Advanced
Therapy (RMAT), Rare Pediatric, and Fast Track designations in the
U.S., PRIME and Advanced Therapy Medicinal Product (ATMP)
designations in the EU, and Orphan Drug designations in both
regions for the program. KRESLADITM was in-licensed from the Centro
de Investigaciones Energéticas, Medioambientales y Tecnológicas
(CIEMAT), Centro de Investigación Biomédica en Red de Enfermedades
Raras and Instituto de Investigación Sanitaria Fundación Jiménez
Díaz. The LV vector was developed in a collaboration between
University College London and CIEMAT.
About Leukocyte Adhesion Deficiency-I
Severe Leukocyte Adhesion Deficiency-I (LAD-I) is a rare,
autosomal recessive pediatric disease caused by mutations in the
ITGB2 gene encoding for the beta-2 integrin component CD18. CD18 is
a key protein that facilitates leukocyte adhesion and extravasation
from blood vessels to combat infections. As a result, children with
severe LAD-I are often affected immediately after birth. During
infancy, they suffer from recurrent life-threatening bacterial and
fungal infections that respond poorly to antibiotics and require
frequent hospitalizations. Children who survive infancy experience
recurrent severe infections including pneumonia, gingival ulcers,
necrotic skin ulcers, and septicemia. Without a successful bone
marrow transplant, survival beyond childhood is rare. Currently the
only potential curative treatment is an allogeneic hematopoietic
stem cell transplant (HSCT), which may not be available in time for
these children and itself has substantial morbidity and mortality.
There is a high unmet medical need for patients with severe
LAD-I.
Rocket’s LAD-I research is made possible by a grant from the
California Institute for Regenerative Medicine (Grant Number
CLIN2-11480). The contents of this press release are solely the
responsibility of Rocket and do not necessarily represent the
official views of CIRM or any other agency of the State of
California.
About RP-L102
RP-L102 is an investigational gene therapy for Fanconi Anemia
(FA) that contains autologous (patient-derived) hematopoietic stem
cells that have been genetically modified with a lentiviral (LV)
vector to contain a functional copy of the FANCA gene. Rocket holds
FDA Regenerative Medicine Advanced Therapy (RMAT), Rare Pediatric
Disease, and Fast Track designations in the U.S., PRIME and
Advanced Therapy Medicinal Product (ATMP) designations in the EU,
and Orphan Drug designation in both regions for the program.
RP-L102 was in-licensed from the Centro de Investigaciones
Energéticas, Medioambientales y Tecnológicas (CIEMAT), Centro de
Investigación Biomédica en Red de Enfermedades Raras and Instituto
de Investigación Sanitaria Fundación Jiménez Díaz.
About Fanconi Anemia
Fanconi Anemia (FA) is a rare genetic disorder characterized by
bone marrow failure (BMF), cancer predisposition, and congenital
malformations. In the absence of allogeneic hematopoietic stem cell
transplant (HSCT), the primary cause of death among patients with
FA is BMF, which typically occurs during the first decade of life.
Allogeneic HSCT, when available, corrects the hematologic component
of FA, but requires myeloablative conditioning. Both chemotherapy
conditioning and graft-versus-host disease, a known complication of
allogeneic HSCT, are associated with an increased risk of solid
tumors, mainly squamous cell carcinomas of the head and neck
region. Approximately 60-70% of patients with FA have a Fanconi
Anemia complementation group A (FANCA) gene mutation, which encodes
for a protein essential for DNA repair. Mutations in the FANCA gene
lead to chromosomal breakage and increased sensitivity to oxidative
and environmental stress. Increased sensitivity to DNA-alkylating
agents such as mitomycin-C (MMC) or diepoxybutane (DEB) is a “gold
standard” test for FA diagnosis. Somatic mosaicism occurs when
there is a spontaneous correction of the mutated gene that can lead
to stabilization or correction of an FA patient’s blood counts in
the absence of any administered therapy. Somatic mosaicism, often
referred to as “natural gene therapy” provides a strong rationale
for the development of FA gene therapy because of the selective
growth advantage of gene-corrected hematopoietic stem cells over FA
cells. There is a high unmet medical need for patients with FA.
About RP-L301
RP-L301 is an investigational gene therapy that contains
autologous hematopoietic stem cells that have been genetically
modified with a lentiviral (LV) vector to contain a functional copy
of the PKLR gene, which is responsible for energy production in red
blood cells (RBCs). RBCs carry oxygen to the rest of the body.
Rocket holds FDA Regenerative Medicine Advanced Therapy (RMAT) and
Fast Track designations in the U.S., EMA PRIME designation in the
EU, and Orphan Drug designation in both regions for the program.
RP-L301 was in-licensed from the Centro de Investigaciones
Energéticas, Medioambientales y Tecnológicas (CIEMAT), Centro de
Investigación Biomédica en Red de Enfermedades Raras (CIBERER) and
Instituto de Investigación Sanitaria de la Fundación Jiménez Díaz
(IIS-FJD).
About Pyruvate Kinase Deficiency
Pyruvate Kinase Deficiency (PKD) is a rare, monogenic red blood
cell disorder resulting from a mutation in the PKLR gene encoding
for the pyruvate kinase enzyme, a key component of the red blood
cell glycolytic pathway. Mutations in the PKLR gene result in
increased red blood cell destruction and potentially
life-threatening anemia with a significant impact to quality of
life. PKD has an estimated prevalence of 4,000 to 8,000 patients in
the U.S. and Europe. Children are the most commonly and severely
affected subgroup of patients. Patients with PKD have a high unmet
medical need, as currently available treatments include splenectomy
and red blood cell transfusions, which are associated with immune
defects and chronic iron overload. Mitapivat, an oral enzyme
activator, is approved for use in adult patients, however its
efficacy is limited in more severely-afflicted patients, most
notably in those who are splenectomized, transfusion-dependent, or
whose disease results from deleterious mutations.
About Rocket Pharmaceuticals, Inc.
Rocket Pharmaceuticals, Inc. (NASDAQ: RCKT) is a fully
integrated, late-stage biotechnology company advancing a
sustainable pipeline of investigational genetic therapies designed
to correct the root cause of complex and rare disorders. Rocket’s
innovative multi-platform approach allows us to design the optimal
gene therapy for each indication, creating potentially
transformative options that enable people living with devastating
rare diseases to experience long and full lives.
Rocket’s lentiviral (LV) vector-based hematology portfolio
consists of late-stage programs for Fanconi Anemia (FA), a
difficult-to-treat genetic disease that leads to bone marrow
failure (BMF) and potentially cancer, Leukocyte Adhesion
Deficiency-I (LAD-I), a severe pediatric genetic disorder that
causes recurrent and life-threatening infections which are
frequently fatal, and Pyruvate Kinase Deficiency (PKD), a monogenic
red blood cell disorder resulting in increased red cell destruction
and mild to life-threatening anemia.
Rocket’s adeno-associated viral (AAV) vector-based
cardiovascular portfolio includes a late-stage program for Danon
Disease, a devastating heart failure condition resulting in
thickening of the heart, an early-stage program in clinical trials
for PKP2-arrhythmogenic cardiomyopathy (ACM), a life-threatening
heart failure disease causing ventricular arrhythmias and sudden
cardiac death, and a pre-clinical program targeting BAG3-associated
dilated cardiomyopathy (DCM), a heart failure condition that causes
enlarged ventricles.
For more information about Rocket, please visit
www.rocketpharma.com and follow us on LinkedIn, YouTube, and X.
Rocket Cautionary Statement Regarding Forward-Looking
Statements
This press release contains forward-looking statements
concerning Rocket’s future expectations, plans and prospects that
involve risks and uncertainties, as well as assumptions that, if
they do not materialize or prove incorrect, could cause our results
to differ materially from those expressed or implied by such
forward-looking statements. We make such forward-looking statements
pursuant to the safe harbor provisions of the Private Securities
Litigation Reform Act of 1995 and other federal securities laws.
All statements other than statements of historical facts contained
in this release are forward-looking statements. You should not
place reliance on these forward-looking statements, which often
include words such as “believe,” “expect,” “anticipate,” “intend,”
“plan,” “will give,” “estimate,” “seek,” “will,” “may,” “suggest”
or similar terms, variations of such terms or the negative of those
terms. These forward-looking statements include, but are not
limited to, statements concerning Rocket’s expectations regarding
the safety and effectiveness of product candidates that Rocket is
developing to treat Fanconi Anemia (FA), Leukocyte Adhesion
Deficiency-I (LAD-I), Pyruvate Kinase Deficiency (PKD), Danon
Disease (DD) and other diseases, the expected timing and data
readouts of Rocket’s ongoing and planned clinical trials, the
expected timing and outcome of Rocket’s regulatory interactions and
planned submissions, Rocket’s plans for the advancement of its DD
program, including its planned pivotal trial, and the safety,
effectiveness and timing of related pre-clinical studies and
clinical trials, Rocket’s ability to establish key collaborations
and vendor relationships for its product candidates, Rocket’s
ability to develop sales and marketing capabilities or enter into
agreements with third parties to sell and market its product
candidates, Rocket’s ability to expand its pipeline to target
additional indications that are compatible with its gene therapy
technologies and Rocket’s ability to transition to a commercial
stage pharmaceutical company. Although Rocket believes that the
expectations reflected in the forward-looking statements are
reasonable, Rocket cannot guarantee such outcomes. Actual results
may differ materially from those indicated by these forward-looking
statements as a result of various important factors, including,
without limitation, Rocket’s dependence on third parties for
development, manufacture, marketing, sales and distribution of
product candidates, the outcome of litigation, unexpected
expenditures, Rocket’s competitors’ activities, including decisions
as to the timing of competing product launches, pricing and
discounting, Rocket’s ability to develop, acquire and advance
product candidates into, enroll a sufficient number of patients
into, and successfully complete, clinical studies, the integration
of new executive team members and the effectiveness of the newly
configured corporate leadership team, Rocket’s ability to acquire
additional businesses, form strategic alliances or create joint
ventures and its ability to realize the benefit of such
acquisitions, alliances or joint ventures, Rocket’s ability to
obtain and enforce patents to protect its product candidates, and
its ability to successfully defend against unforeseen third-party
infringement claims, as well as those risks more fully discussed in
the section entitled “Risk Factors” in Rocket’s Annual Report on
Form 10-K for the year ended December 31, 2023, filed February 27,
2024 with the SEC and subsequent filings with the SEC including our
Quarterly Reports on Form 10-Q. Accordingly, you should not place
undue reliance on these forward-looking statements. All such
statements speak only as of the date made, and Rocket undertakes no
obligation to update or revise publicly any forward-looking
statements, whether as a result of new information, future events
or otherwise.
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version on businesswire.com: https://www.businesswire.com/news/home/20240510805823/en/
Media & Investors Meg Dodge
Media Kevin Giordano media@rocketpharma.com
Investors Brooks Rahmer investors@rocketpharma.com
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