Refractory/Relapsed (R/R) acute myeloid leukemia (AML) is associated with a dis-mal prognosis.
In some subsets of AML such as AML driven by the t(8;21) translocation, leading to the RUNX1-RUNX1T1 (AML1-ETO) fusion transcript expression, CD19 B-cell antigen is aberrantly expressed on malignant blasts in around 80 % of cases. Interestingly, the expression of the CD19 antigen is also detected in the CD34+ CD38-population leukemic stem cells.
t(8;21) AML subtype has a rather good prognosis with an intensive chemotherapy regimen, but relapses occur in around 40 % of the patients and new therapeutic options are needed for these patients.
Plesa et al, reported a successful treatment of a refractory t(8;21) AML with bispecific monoclonal antibodies that targets CD19. More recently, Danylesko et al, have reported long-term remission following CD19 CAR-T cells in a heavily pre-treated patient with t(8;21) AML(1). The same group has just submitted an abstract of 6 treated patients to the European Haematology Association (EHA) 2023 meet-ing: Six patients (adults-5, child-1) with t(8; 21) AML (confirmed by cytogenetic and FISH) and aberrant CD19 expression were included. One patient had a complex karyotype. Molecular analysis for CKIT, NPM1, IDH1, IDH2, and CBPa were nega-tive in all pts. One pt harbors the FLT3 ITD and TKD mutations. Median number of previous chemotherapy (CT) lines was 4 (3-8). Four patients were with chemo re-sistant relapse post allo-HCT (MSD-1, 10/10 MUD -3) 5-18 months before CAR T-cell infusion. All patients developed CRS (grade 1-3) and were treated with i.v tocili-zumab and dexamethasone. 2/6 patients suffered from ICANS and were treated with steroids. In 4/6 patients, day 28 BM aspiration disclosed normal hematopoie-sis with no excess blasts and lack of t(8;21) by FISH confirming clinical and cyto-genetic remission, while 2/6 pts with progressive AML had no response (Danylesko etal. Abstract EHA 2023, submitted).
Interestingly, other subsets of AML display an aberrant expression of CD19. These observations indicate that CD19 can be a target of choice for CAR-T cells in patients with R/R AML expressing this antigen.
In this study, we plan to offer anti-CD19 CAR-T cell therapy to patients with re-lapsed/refractory AML expressing CD19 for whom no curative alternatives are available.
To this end, CAR-T cells will be manufactured using closed semi-automated bioreactor CliniMACS Prodigy (Miltenyi Biotec) in academic setting.

Start Date10 Jul 2025

Sponsor / Collaborator

University Hospital of Lille

[+1]

100 Clinical Results associated with CD19 CAR-T Cell(University Hospital of Lille)

100 Translational Medicine associated with CD19 CAR-T Cell(University Hospital of Lille)

100 Patents (Medical) associated with CD19 CAR-T Cell(University Hospital of Lille)

Literatures (Medical) associated with CD19 CAR-T Cell(University Hospital of Lille)

01 Aug 2025·Med

CD19 CAR-T cell therapy in a pediatric patient with MDA5+ dermatomyositis and rapidly progressive interstitial lung disease

Article

Author: Pertíñez, Lidia ; Ruiz de Valbuena, Marta ; de la Cruz-Benito, Ana ; Remesal, Agustín ; Galán-Gómez, Víctor ; Martínez-Romera, Isabel ; Dorao, Paloma ; París-Muñoz, Andrés ; Alcobendas-Rueda, Rosa M ; Cámara, Carmen ; González-Martínez, Berta ; Gómez-Zamora, Ana ; Ríos-Blanco, Juan J ; Minguillón, Jordi ; Udaondo, Clara ; Sánchez-Zapardiel, Elena ; Pérez-Martínez, Antonio ; Sanz-Rupérez, Alejandro ; Serrano-Olmedo, María G ; Del Pino-Molina, Lucía ; Fernández-García, Miguel A ; Climent, Francisco ; de Manuel-Gómez, Cristina ; Español-Rego, Marta ; Andrade, José D ; Menéndez, Juan J ; Verdú-Sánchez, Cristina ; Ruiz-Zurita, Gonzalo

BACKGROUND:

Anti-melanoma differentiation-associated protein 5 dermatomyositis (MDA5⁺DM) is a potentially fatal subtype of dermatomyositis. The most severe cases are characterized by rapidly progressive interstitial lung disease (RPILD), the leading cause of death in these patients. There is currently no curative treatment for these patients, and indeed, MDA5⁺DM-RPILD is considered one of the most challenging pathologies in medicine. Nevertheless, the recent introduction of CD19 chimeric antigen receptor (CAR)-T cell therapies appears to offer a serious opportunity to develop solutions for complex autoimmune diseases refractory to multiple immunosuppressant treatments, mainly rheumatic diseases such as rheumatoid arthritis, dermatomyositis, and systemic lupus erythematosus.

METHODS:

In this report, we describe the first use of a second-generation CD19 CAR-T cell therapy (ARI-0001) in a pediatric patient with severe MDA5⁺DM-RPILD.

FINDINGS:

Conventional treatments stabilized MDA5⁺DM-RPILD before CAR-T cell inoculation (-34 days). The presence of CD19⁺ B lymphocytes that might serve as target cells in deeper tissues was suspected due to CAR-T cell expansion in a context of B cell aplasia. No fever or cytokine release syndrome/cell-associated neurotoxicity syndrome was evident. In global terms, B cell reconstitution and cutaneous, motor, respiratory, and neurological improvements were observed gradually in the patient in an immunosuppressant-free context (-7 to +325 days).

CONCLUSIONS:

A pediatric patient with aggressive MDA5⁺DM-RPILD achieved progressive long-term improvement and immunosuppressant-free remission over 11 months after compassionate use of a CD19 CAR-T cell therapy (ARI-0001).

FUNDING:

This work was supported by the Programa Investigo (PI_SEPE_APM) and grants from the ISC-III (PI22/01226) from the Comunidad de Madrid (S2022/BMD-7225) and from the CRIS Cancer Foundation.

01 Jun 2025·Journal for ImmunoTherapy of Cancer

Bystander CAR⁻CD8⁺ T cells in a CAR-T cell product can expand and enhance the antitumor effects of a bispecific antibody

Article

Author: Doi, Yasukazu ; Miyazaki, Yukihiro ; Kato, Junichi ; Takenaka, Katsuto ; Maruta, Masaki ; Konishi, Tatsuya ; Yamanouchi, Jun ; Nabe, Shogo ; Matsumoto, Meika ; Takasuka, Yasunori ; Ochi, Toshiki ; Masuda, Yuya ; Honda, Takatsugu ; Kawasaki, Natsumi

Although bispecific antibody (BsAb) treatment is a valuable therapeutic option for post chimeric antigen receptor (CAR)-T cell therapy against relapsed/refractory large B-cell lymphoma, it remains to be clarified why it is still effective after intensive T-cell redirection therapy. Recently, the therapeutic potential of bystander CD8+ T cells in the field of cancer immunotherapy have been discussed. In this study, we have shown a clinical impact where bystander CAR-negative CD8+ T cells from a CAR-T cell product have a potential to augment immune responses of BsAb therapy through a case with relapsed diffuse large B-cell lymphoma after CD19 CAR-T cell therapy. T cells in a CAR-T-cell product dominantly showed central and effector memory T cells, and such T-cell phenotypes in peripheral blood significantly increased after CAR-T cell therapy. Furthermore, chronological T-cell receptor-β repertoire analyses for both CD8+ T cells and CD4+ T cells suggested that product-derived bystander CAR−CD8+ T cells successfully existed in a relapsed lymph node and expanded in the body after BsAb therapy. Further analyses are necessary, but our findings might help to explain the mechanisms and benefits of this sequential approach and strengthen the sequence of CAR-T cell therapy prior to BsAb therapy.

01 Jan 2025·[Rinsho ketsueki] The Japanese journal of clinical hematology

[Identification of genes regulating human CAR-T cell proliferation by genome-wide CRISPR screening].

Article

Author: Adachi, Yoshitaka

In vivo expansion and long-term maintenance of CAR-T cells are considered to be the hallmark of treatment success after CD19 CAR-T cell therapy. Genome-wide CRISPR screening has emerged as a powerful tool for large-scale gene screens. Genome-wide CRISPR screening revealed that CUL5 gene knockout (KO) improved the proliferation of CD19 CAR-T cells. CUL5KO improved not only the proliferation but also the effector function of CAR-T cells. The JAK-STAT pathway was upregulated in CUL5KO CAR-T cells, and CUL5 was associated with the degradation of JAK3 upon activation through IL-2 signaling. CUL5KO CD19 CAR-T cells efficiently suppressed in vivo tumor progression as compared to control CD19 CAR-T cells.

100 Deals associated with CD19 CAR-T Cell(University Hospital of Lille)

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Indication	Highest Phase	Country/Location	Organization	Date
Refractory acute myeloid leukemia	Phase 1	France	University Hospital of Lille	10 Jul 2025
Relapsing acute myeloid leukemia	Phase 1	France	University Hospital of Lille	10 Jul 2025
Treatment related acute myeloid leukaemia	Phase 1	France	University Hospital of Lille	10 Jul 2025

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