Efficient preclinical treatment of cortical T cell acute lymphoblastic leukemia with T lymphocytes secreting anti-CD1a T cell engagers

Jiménez-Reinoso, Anaïs; Tirado, Néstor; Martínez-Moreno, Alba; Dı́az, Vı́ctor M.; García-Peydró, Marina; Hangiu, Oana; Díez-Alonso, Laura; Albitre, Ángela; Penela, Petronila; Toribio, Marı́a L.; Menéndez, Pablo; Álvarez‐Vallina, Luís; Sánchez-Martínez, Diego

doi:10.1136/jitc-2022-005333

Cited by 8 publications

(9 citation statements)

References 44 publications

(56 reference statements)

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“…CD1a, a cell surface antigen, is specifically expressed in coT-ALL and retained in relapsed coT-ALL, but barely expressed in normal cells/tissues. CD1a-specific CAR-T therapy has been validated preclinically for relapsed/refractory coT-ALL [ 59 ]. A recent phase II clinical trial of anti-CD1a CAR-T in treating R/R T-ALL was initiated (NCT05745181).…”

Section: Resultsmentioning

confidence: 99%

“…Meanwhile, it is challenging to achieve sufficient effector T cells from relapsed/refractory patients owing to the aggressiveness and hyper leukocytic of the disease. A study suggests that engineered T cells secreting CD1a XCD3 T-cell-engaging antibodies (CD1a-STAb) may be applied for coT-ALL patients with limited numbers of effector T cells [ 59 ]. This study showed that CD1a-T-cell engagers induce specific T-cell activation through binding to CD1a and CD3 on the cell surface.…”

Section: Resultsmentioning

confidence: 99%

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An Update on Clinical Trials and Potential Therapeutic Strategies in T-Cell Acute Lymphoblastic Leukemia

Patel

Gao

Wang

2023

IJMS

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Current therapies for T-cell acute leukemia are based on risk stratification and have greatly improved the survival rate for patients, but mortality rates remain high owing to relapsed disease, therapy resistance, or treatment-related toxicities/infection. Patients with relapsed disease continue to have poor outcomes. In the past few years, newer agents have been investigated to optimize upfront therapies for higher-risk patients in the hopes of decreasing relapse rates. This review summarizes the progress of chemo/targeted therapies using Nelarabine/Bortezomib/CDK4/6 inhibitors for T-ALL in clinical trials and novel strategies to target NOTCH-induced T-ALL. We also outline immunotherapy clinical trials using monoclonal/bispecific T-cell engaging antibodies, anti-PD1/anti-PDL1 checkpoint inhibitors, and CAR-T for T-ALL therapy. Overall, pre-clinical studies and clinical trials showed that applying monoclonal antibodies or CAR-T for relapsed/refractory T-ALL therapy is promising. The combination of target therapy and immunotherapy may be a novel strategy for T-ALL treatment.

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

An Update on Clinical Trials and Potential Therapeutic Strategies in T-Cell Acute Lymphoblastic Leukemia

Patel

Gao

Wang

2023

IJMS

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“…First evidence of efficacy has recently been shown in phase I clinical trials of novel CAR T-cell products targeting CD30 in Hodgkin lymphoma 23 and CD7 in T-ALL, 24-26 with additional products for T-ALL under investigation. 27-29 Objective responses now also support the general promise of CAR T-cell targeting in pediatric solid cancers. 30-33 CAR T-cell therapy has been reported to be beneficial in diffuse intrinsic pontine gliomas, a cancer with a very poor prognosis, 32 and complete and even durable remissions have been obtained in neuroblastoma.…”

mentioning

confidence: 92%

Chimeric Antigen Receptor (CAR) T-Cell Products for Pediatric Cancers: Why Alternative Development Paths Are Needed

Rossig,

Pearson,

Vassal

et al. 2024

JCO

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“…Sustained in vivo TCE secretion results in effective serum concentrations of the TCE (28). Furthermore, expansion and persistence of adoptively transferred STAb-T cells (29,30), as well as polyclonal recruitment of both genemodified STAb-T cells and unmodified bystander T cells to the tumor microenvironment (TME), can lead to substantially increased antitumor responses (29)(30)(31). The therapeutic potential of STAb-T cells has been demonstrated in B cell (29)(30)(31)(32) and T cell hematological malignancies (30).…”

Section: Introductionmentioning

confidence: 99%

“…Furthermore, expansion and persistence of adoptively transferred STAb-T cells (29,30), as well as polyclonal recruitment of both genemodified STAb-T cells and unmodified bystander T cells to the tumor microenvironment (TME), can lead to substantially increased antitumor responses (29)(30)(31). The therapeutic potential of STAb-T cells has been demonstrated in B cell (29)(30)(31)(32) and T cell hematological malignancies (30). Here, we report the generation of STAb-T cells secreting an anti-BCMA TCE and demonstrate their superior efficacy over BCMA-specific CAR-T cells under T cell-limiting conditions simulating those found in patients with multitreated MM.…”

Section: Introductionmentioning

confidence: 99%

Engineered T cells secreting anti-BCMA T cell engagers control multiple myeloma and promote immune memory in vivo

Díez-Alonso,

Falgas,

Arroyo-Ródenas

et al. 2024

Sci. Transl. Med.

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Multiple myeloma is the second most common hematological malignancy in adults and remains an incurable disease. B cell maturation antigen (BCMA)–directed immunotherapy, including T cells bearing chimeric antigen receptors (CARs) and systemically injected bispecific T cell engagers (TCEs), has shown remarkable clinical activity, and several products have received market approval. However, despite promising results, most patients eventually become refractory and relapse, highlighting the need for alternative strategies. Engineered T cells secreting TCE antibodies (STAb) represent a promising strategy that combines the advantages of adoptive cell therapies and bispecific antibodies. Here, we undertook a comprehensive preclinical study comparing the therapeutic potential of T cells either expressing second-generation anti-BCMA CARs (CAR-T) or secreting BCMAxCD3 TCEs (STAb-T) in a T cell–limiting experimental setting mimicking the conditions found in patients with relapsed/refractory multiple myeloma. STAb-T cells recruited T cell activity at extremely low effector-to-target ratios and were resistant to inhibition mediated by soluble BCMA released from the cell surface, resulting in enhanced cytotoxic responses and prevention of immune escape of multiple myeloma cells in vitro. These advantages led to robust expansion and persistence of STAb-T cells in vivo, generating long-lived memory BCMA-specific responses that could control multiple myeloma progression in xenograft models, outperforming traditional CAR-T cells. These promising preclinical results encourage clinical testing of the BCMA-STAb-T cell approach in relapsed/refractory multiple myeloma.

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Efficient preclinical treatment of cortical T cell acute lymphoblastic leukemia with T lymphocytes secreting anti-CD1a T cell engagers

Cited by 8 publications

References 44 publications

An Update on Clinical Trials and Potential Therapeutic Strategies in T-Cell Acute Lymphoblastic Leukemia

An Update on Clinical Trials and Potential Therapeutic Strategies in T-Cell Acute Lymphoblastic Leukemia

Chimeric Antigen Receptor (CAR) T-Cell Products for Pediatric Cancers: Why Alternative Development Paths Are Needed

Engineered T cells secreting anti-BCMA T cell engagers control multiple myeloma and promote immune memory in vivo

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