Galapagos presents at EBMT-EHA annual meeting 2024
Showcases meaningful advances in
decentralized CAR T-cell manufacturing and presents translational
and clinical data from ongoing Phase 1/2 CD19 CAR-T
studies
Mechelen, Belgium; 15 February 2024,
22:01 CET; Galapagos NV (Euronext & NASDAQ: GLPG) to present
new preliminary translational data and previously disclosed data at
the European Society for Blood and Marrow Transplantation
(EBMT)-European Hematology Association (EHA)
6th European CAR T-cell meeting
taking place from 15–17 February 2024 in Valencia,
Spain.
The preliminary translational data from its
EUPLAGIA-1 Phase 1/2 study demonstrate that Galapagos’
differentiated point-of-care manufacturing platform offers the
potential for a single infusion of fresh early-phenotype CD19 CAR-T
cells with robust expansion and persistence in patients with
relapsed/refractory chronic lymphocytic leukemia (rrCLL) and
patients with Richter transformation (RT). Further, previously
disclosed safety, efficacy and feasibility data from EUPLAGIA-1 and
ATALANTA-1 support the potential of Galapagos’ innovative approach
to CAR-T manufacturing and of the transformational impact on
patients with severe hematologic cancers.
“At Galapagos, we are committed to accelerating
transformative innovation to address the unmet needs of patients
with advanced cancers, and the data we are presenting today
demonstrates our positive momentum toward this goal,” said Dr
Jeevan Shetty, M.D., Head of Clinical Development Oncology at
Galapagos. “We are pleased for the opportunity to present
encouraging data that supports the potential of our innovative,
decentralized approach to CAR-T manufacturing and the
transformational impact CAR-T treatment could have on patients with
serious hematologic cancers.”
Summary of preliminary translational
data from EUPLAGIA-1 with GLPG5201 (cut-off date: 6 September
2023):Patient recruitment of the Phase 1 dose-finding part
of EUPLAGIA-1 has been completed and 15 patients were enrolled (6
at dose level 1 (DL1); and 9 at dose level 2 (DL2)), all of whom
were diagnosed with rrCLL and 9 with additional RT. All 15 Phase 1
batches were manufactured at the point-of-care and infused as a
single fresh, fit product within a median vein-to-vein time of
seven days, with 80% of patients receiving the product in seven
days.
GLPG5201 final product showed an increase in
early phenotypes of CD4+ and CD8+ CAR-T cells (naïve, stem cell
memory (TN/SCM) and central memory) compared to apheresis starting
material. A robust in vivo expansion of GLPG5201 occurred with a
median time-to-peak expansion of 14 days, regardless of dose level,
and a higher exposure for patients infused with DL2 compared to
DL1. GLPG5201 expansion and exposure were similar in patients with
rrCLL and in patients with RT. Persisting CAR-T cells were detected
up to 15 months post-infusion. Moreover, the abundance of both CD4+
and CD8+ TN/SCM CAR-T cells in the final product correlated with
CAR-T-cell exposure in patients.
Key data highlights accepted by
EBMT-EHA:
|
Abstract Title |
Authors/Presenter |
Presentation date/time |
|
Galapagos abstracts |
|
Seven-Day Vein-to-Vein Point-of-Care–Manufactured GLPG5201
Anti-CD19 CAR-T Cells Display Early Phenotype in
Relapsed/Refractory Chronic Lymphocytic Leukemia (rrCLL) Including
Richter's Transformation (RT) |
Sandra Blum, Claire Vennin, Esmée P. Hoefsmit, Kirsten Van Hoorde,
Sergi Betriu,Leticia Alserawan, Julio Delgado, Nadia Verbruggen,
Anna D.D. van Muyden, Henriëtte Rozema, Ruiz Astigarraga, Margot J.
Pont |
Poster Number: AS-CART-2024-00104Date: 15 February 2024; 8:15 pm
–8:45 pmSession: PT2 (Poster Tour 2) |
|
Galapagos encore abstracts |
|
Seven-Day Vein-to-Vein Point-of-Care Manufactured CD19 CAR-T Cells
(GLPG5101) in Relapsed/Refractory Non-Hodgkin Lymphoma (rrNHL):
Results from the Phase 1 ATALANTA-1 Trial |
Marie José Kersten, Kirsten Saevels, Sophie Servais, Yves Beguin,
Joost S.P. Vermaat, Eva Santermans, Stavros Milatos, Maike Spoon,
Marte C. Liefaard, Claire Vennin, Margot J. Pont, Anna D.D. van
Muyden, Maria T. Kuipers, Sébastien Anguille |
Poster Number: AS-CART-2024-00090Date: 15 February 2024; 7:45 pm
–8:15 pmSession: PT1 (Poster Tour 1) |
|
Seven-Day Vein-to-Vein Point-of-Care–Manufactured CD19 CAR T-Cell
Therapy (GLPG5201) in Relapsed/Refractory Chronic Lymphocytic
Leukemia (rrCLL) Including Richter’s Transformation: Results from
the Phase 1 EUPLAGIA-1 Trial |
Natalia Tovar, Nuria Martinez-Cibrian, Julio Delgado, Sergi Betriu,
Leticia Alserawan, Ana Triguero, Nadia Verbruggen, Maike Spoon,
Marte C. Liefaard, Anna D.D. van Muyden, Valentin
Ortiz-Maldonado |
Oral Presentation Number: AS-CART-2024-00099Date: 16 February 2024;
6:38 pm –6:44 pm (session runs 6:20 pm –7:15 pm)Session: BA2 (Best
Abstracts 2); Auditorium 1 |
|
Phase 1/2, Multicenter, Open-Label Study to Evaluate Feasibility,
Safety and Efficacy of Point-of-Care–Manufactured Anti-BCMA CAR
T-Cell Therapy (GLPG5301) in Relapsed/Refractory Multiple Myeloma
(rrMM) |
Niels W.C.J. van de Donk, Sébastien Anguille, Jo Caers, Marte C.
Liefaard, Christian Jacques, Anna D.D. van Muyden |
Poster Number: AS-CART-2024-00103Date: 17 February 2024; 08:30
am–1:45 pmSession: PE17p (Poster Exhibition) |
About Galapagos’ decentralized CAR-T
manufacturing platform Galapagos’ decentralized,
innovative point-of-care CAR T-cell manufacturing platform offers
the potential for the administration of fresh, fit cells with a
vein-to-vein time of seven days, greater physician control and a
significantly improved patient experience. The platform consists of
an end-to-end xCellit™ workflow management and monitoring software
system, a decentralized, functionally closed, automated
manufacturing platform for cell therapies (using Lonza’s Cocoon®)
and a proprietary quality control testing and release
strategy.
About the EUPLAGIA-1 study (EudraCT
2021-003815-25)EUPLAGIA-1 is an ongoing Phase 1/2
open-label, multi-center study evaluating the safety, efficacy and
feasibility of point-of-care manufactured GLPG5201, a CD19 CAR-T
product candidate, in patients with relapsed/refractory lymphocytic
leukemia (rrCLL) and small cell lymphocytic lymphoma (rrSLL), with
or without Richter transformation (RT). GLPG5201 is a second
generation anti-CD19/4-1BB CAR-T product candidate, administered as
a single fixed intravenous dose. Patients with CD19+ rrCLL or rrSLL
with ≥2 lines of prior therapy are eligible to participate, and
patients with RT are eligible regardless of prior therapy. The
primary objective of the Phase 1 part of the study was to evaluate
safety and determine the recommended dose for the Phase 2 part of
the study. The dose levels that were evaluated in the Phase 1 part
of the study are 35x106 (DL1), and 100x106 (DL2) CAR+ viable T
cells. The primary objective of the Phase 2 part of the study is to
assess the Objective Response Rate (ORR) and the secondary
objectives include the analysis of the Complete Response (CR),
duration of response, progression free survival, overall survival,
safety, pharmacokinetic profile, and feasibility of point-of-care
manufacturing.
About chronic lymphocytic
leukemia Chronic lymphocytic leukemia (CLL) is one of the
chronic lymphoproliferative disorders (lymphoid neoplasms). It is
characterized by a progressive accumulation of functionally
incompetent lymphocytes, which are usually monoclonal in origin.
CLL affects B-cells in the blood and bone marrow.1 RT is an
uncommon clinicopathological condition observed in patients with
CLL. It is characterized by the sudden transformation of the CLL
into a significantly more aggressive form of large cell lymphoma
and occurs in approximately 2-10% of all CLL patients. CLL usually
follows an indolent course and is an incurable disease. Patients
who develop relapsed and refractory disease and become resistant to
new agents have a dismal prognosis and a high unmet medical need
for new therapeutic options such as CAR-T cells. With estimated
incidence of 4.7 new cases per 100,000 individuals, CLL is the most
prevalent lymphoid malignancy and is the most common adult leukemia
in the US and in Europe.2 The annual incidence of patients with RT
has been estimated at 1,900 new patients in the US and 2,000 in the
EU5.3
About the ATALANTA-1 study (EudraCT
2021-003272-13)ATALANTA-1 is an ongoing Phase 1/2,
open-label, multicenter study to evaluate the safety, efficacy and
feasibility of point-of-care manufactured GLPG5101, a CD19 CAR-T
product candidate, in patients with relapsed/refractory
non-Hodgkin’s lymphoma (rrNHL). GLPG5101 is a second generation
anti-CD19/4-1BB CAR-T product candidate, administered as a single
fixed intravenous dose. The primary objective of the Phase 1 part
of the study was to evaluate safety and to determine the
recommended dose for the Phase 2 part of the study. Secondary
objectives include assessment of efficacy and feasibility of near
the point-of-care manufacturing of GLPG5101. The dose levels that
were evaluated in Phase 1 are 50x106 (DL1) and 110x106 (DL2) and
250x106 (DL3) CAR+ viable T cells. The primary objective of the
Phase 2 part of the study is to evaluate the Objective Response
Rate (ORR) while the secondary objectives include Complete Response
(CR), duration of response, progression free survival, overall
survival, safety, pharmacokinetic profile, and the feasibility of
point-of-care manufacturing. Each enrolled patient will be followed
for 24 months.
About non-Hodgkin’s
lymphomaNon-Hodgkin’s lymphoma is a cancer originating
from lymphocytes, a type of white blood cell which is part of the
body’s immune system. Non-Hodgkin’s lymphoma can occur at any age
although it is more common in adults over 50 years old. Initial
symptoms usually are enlarged lymph nodes, fever, and weight loss.
There are many different types of non-Hodgkin’s lymphoma. These
types can be divided into aggressive (fast-growing) and indolent
(slow-growing) types, and they can be formed from either B
lymphocytes (B cells) or in lesser extent from T lymphocytes (T
cells) or Natural Killer cells (NK cells). B-cell lymphoma makes up
about 85% of non-Hodgkin’s lymphomas diagnosed in the US. Prognosis
and treatment of non-Hodgkin’s lymphoma depend on the stage and
type of disease.
About the PAPILIO-1 Phase 1/2 study (EU
CT 2022-500782-27-00)PAPILIO-1 is a Phase 1/2, open-label,
multicenter study to evaluate the safety, efficacy and feasibility
of point-of-care manufactured GLPG5301, a BCMA CAR-T product
candidate, in patients with relapsed/refractory multiple myeloma
(rrMM) after ≥2 prior lines of therapy. The primary objective of
the Phase 1 part of the PAPILIO-1 study is to evaluate safety and
determine the recommended dose for the Phase 2 part of the study.
The primary objective of the Phase 2 part of the study is to
evaluate the efficacy of GLPG5301, as measured by the Objective
Response Rate (ORR). Secondary objectives for both Phase 1 and
Phase 2 include further assessment of the safety of GLPG5301,
additional efficacy endpoints, including assessment of Minimal
Residual Disease (MRD), as well as the feasibility of point-of-care
manufacture of GLPG5301 in rrMM patients. Each enrolled patient
will be followed for 24 months. During Phase 1, up to 3 dose levels
will be evaluated and at least 12 patients will be enrolled to
establish the recommended Phase 2 dose. Approximately 30 additional
patients will be enrolled in the Phase 2 part of the study to
further evaluate the safety and efficacy of GLPG5301.
About relapsed/refractory multiple
myeloma (rrMM)Multiple myeloma (MM) is typically
characterized by the neoplastic proliferation of plasma cells
producing a monoclonal immunoglobulin. The plasma cells proliferate
in the bone marrow and may result in extensive skeletal destruction
with osteopenia, and osteolytic lesions with or without pathologic
fractures. The diagnosis of MM is made when one (or more) of the
following clinical presentations are present: bone pain with lytic
lesions discovered on routine skeletal films or other imaging
modalities, an increased total serum protein concentration with the
presence of a monoclonal protein in the urine or serum, and anemia,
hypercalcemia or renal failure. The patient may be either
symptomatic or their disease may be discovered incidentally.
Despite improvements in treatment, patients with MM ultimately
relapse or become refractory to available regimens.
Triple-refractory patients (refractory to CD38 monoclonal
antibodies (mAbs), proteasome inhibitor (PI) and immunomodulatory
drug (IMiD)), or penta-refractory patients (refractory to CD38
mAbs, 2 Pls and 2 IMiDs) have a poor prognosis and are in urgent
need of novel treatment options.
About GalapagosWe are a global
biotechnology company with operations in Europe and the US
dedicated to developing transformational medicines for more years
of life and quality of life. Focusing on high unmet medical needs,
we synergize compelling science, technology, and collaborative
approaches to create a deep pipeline of best-in-class small
molecules, CAR-T therapies, and biologics in oncology and
immunology. With capabilities from lab to patient, including a
decentralized, point-of-care CAR-T manufacturing network, we are
committed to challenging the status quo and delivering results for
our patients, employees and shareholders. For additional
information, please visit www.glpg.com or follow us
on LinkedIn or X (formerly Twitter).
Contact
|
Media inquiries:Marieke Vermeersch +32 479
490 603media@glpg.com |
Investor inquiries:Sofie Van Gijsel +1 781
296 1143ir@glpg.comSandra Cauwenberghs+32 495 58 46
63 ir@glpg.com |
Forward-looking statementsThis
press release includes forward-looking statements within the
meaning of the Private Securities Litigation Reform Act of 1995, as
amended. These statements are often, but are not always, made
through the use of words or phrases such as “anticipate,” “expect,”
“plan,” “estimate,” “will,” “continue,” “aim,” “intend,” “future,”
“potential,” “could,” ”indicate,” “forward,” as well as similar
expressions. Forward-looking statements contained in this release
include, but are not limited to, statements regarding preliminary,
interim and topline data from the EUPLAGIA-1, ATALANTA-1 and
PAPILIO-1 studies and other analyses related to CD19 CAR-T,
statements related to Galapagos’ plans, expectations and strategy
with respect to the EUPLAGIA-1, ATALANTA-1 and PAPILIO-1 studies,
and statements regarding the expected timing, design and readouts
of the EUPLAGIA-1, ATALANTA-1 and PAPILIO-1 studies, including the
expected recruitment for trials. Forward-looking statements involve
known and unknown risks, uncertainties and other factors which
might cause our actual results to be materially different from
those expressed or implied by such forward-looking statements.
These risks, uncertainties and other factors include, without
limitation, the risk that preliminary or interim clinical results
may not be replicated in ongoing or subsequent clinical trials; the
risk that ongoing and future clinical studies with GLPG5201 and
GLPG5101 may not be completed in the currently envisaged timelines
or at all, the inherent uncertainties associated with competitive
developments, clinical trial and product development activities and
regulatory approval requirements (including that data from the
ongoing and planned clinical research programs may not support
registration or further development of GLPG5201 and GLPG5101 due to
safety, efficacy or other reasons), Galapagos' reliance on
collaborations with third parties (including its collaboration
partner Lonza) and that Galapagos’ estimations regarding its
GLPG5201 and GLPG5101 development programs and regarding the
commercial potential of GLPG5201 and GLPG5101, may be incorrect, as
well as those risks and uncertainties identified in Galapagos’
Annual Report on Form 20-F for the year ended 31 December 2022
filed with the U.S. Securities and Exchange Commission (SEC) and
its subsequent filings with the SEC. All statements other than
statements of historical fact are statements that could be deemed
forward-looking statements. The forward-looking statements
contained herein are based on management’s current expectations and
beliefs and speak only as of the date hereof, and Galapagos makes
no commitment to update or publicly release any revisions to
forward-looking statements in order to reflect new information or
subsequent events, circumstances or changes in expectations.
1 Wierda WG. Chronic lymphocytic leukemia/ Small
lymphocytic lymphoma fact sheet. In: Foundation LR,
editor: https://www.lymphoma.org/wp-content/uploads/2018/04/LRF_FACTSHEET_CLL_SLL.pdf.2018.2
Siegel RL, Miller KD, Fuchs HE, Jemal A. Cancer Statistics, 2021.
CA: A Cancer Journal for Clinicians. 2021;71(1):7-33.
https://www.ncbi.nlm.nih.gov/books/NBK4931733 IMARC report, 2023;
2-15% of incidence per Lightning Health literature review; Sigmund
AM et al. 2022; Thompson PhA et al. 2022.
- Galapagos presents at EBMT-EHA annual meeting 2024
Grafico Azioni Galapagos (TG:GXE)
Storico
Da Ott 2024 a Nov 2024
Grafico Azioni Galapagos (TG:GXE)
Storico
Da Nov 2023 a Nov 2024
