SAR442257 抗 CD38 三特异性 T 细胞衔接子在达雷妥尤单抗和 BCMA 靶向治疗后复发的多发性骨髓瘤中的体外疗效。
Ex Vivo Efficacy of SAR442257 Anti-CD38 Trispecific T-cell Engager in Multiple Myeloma Relapsed After Daratumumab and BCMA-targeted Therapies.
机构信息
Division of Hematology, Department of Medicine, University of Colorado Anschutz Medical Campus, Aurora, Colorado.
Sanofi R&D, North America, Cambridge, Massachusetts.
出版信息
Cancer Res Commun. 2024 Mar 12;4(3):757-764. doi: 10.1158/2767-9764.CRC-23-0434.
UNLABELLED
T cell-engaging antibodies (TCEs) are showing promising efficacy in relapsed/refractory multiple myeloma, even in patients that relapsed after B-cell maturation antigen (BCMA)-targeted therapy. Patients with multiple myeloma may have compromised T-cell health unaccounted for by preclinical models. Here, we use Myeloma Drug Sensitivity Testing (My-DST) for ex vivo measurement of anti-multiple myeloma cytotoxicity for the trispecific CD38/CD28xCD3 TCE SAR442257 through activation of the patients' own endogenous T cells to inform clinical development of the compound in multiple myeloma. My-DST incubates primary mononuclear cells in humanized media for 48 hours followed by flow cytometry for multiple myeloma cell viability with or without drug treatment. SAR442257 was tested on 34 samples from patients with multiple myeloma across disease settings. Potential biomarkers, T-cell dependence, and degranulation were assessed. SAR442257 was effective at low dose in My-DST cultures. High ex vivo response rates were observed in primary aspirates taken from patients with multiple myeloma at diagnosis, with modestly reduced response in multiple myeloma recently treated with anti-CD38 mAbs. SAR442257 was highly effective in patients relapsing after BCMA therapy. The CD38/CD28xCD3 trispecific format was substantially more effective than a conventional bispecific CD38/CD3 antibody format and CD38 mAbs. Anti-multiple myeloma cell cytotoxicity was dependent on the presence of endogenous T cells. Surface CD38 expression was the strongest biomarker of TCE response. My-DST is capable of measuring T cell-dependent killing using the multiple myeloma patient's own bone marrow-derived T cells. SAR442257 shows promise for multiple myeloma and may be best suited for patients declared resistant to both CD38 mAbs and BCMA-targeted therapy.
SIGNIFICANCE
This study introduces the use of My-DST to measure and characterize sensitivity to anti-CD38 T-cell engager SAR442257 in primary samples using matched endogenous T cells. Preclinical testing in samples from patients with diverse treatment history supports further testing in post-chimeric antigen receptor T-cell multiple myeloma.
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T 细胞结合抗体(TCEs)在复发性/难治性多发性骨髓瘤中显示出有希望的疗效,即使在针对 B 细胞成熟抗原(BCMA)的治疗后复发的患者中也是如此。多发性骨髓瘤患者的 T 细胞健康可能因临床前模型而无法解释。在这里,我们使用多发性骨髓瘤药物敏感性测试(My-DST)通过激活患者自身内源性 T 细胞来测量抗多发性骨髓瘤细胞毒性,以告知三特异性 CD38/CD28xCD3 TCE SAR442257 在多发性骨髓瘤中的临床开发。My-DST 将原代单核细胞在人源化培养基中孵育 48 小时,然后用流式细胞术检测有无药物治疗的多发性骨髓瘤细胞活力。SAR442257 在 34 名多发性骨髓瘤患者的样本中进行了测试,这些患者来自不同疾病环境。评估了潜在的生物标志物、T 细胞依赖性和脱颗粒作用。SAR442257 在 My-DST 培养物中在低剂量时有效。在多发性骨髓瘤患者的初次抽吸物中观察到高的体外反应率,在最近用抗 CD38 mAb 治疗的多发性骨髓瘤患者中反应适度降低。SAR442257 在 BCMA 治疗后复发的患者中非常有效。CD38/CD28xCD3 三特异性格式比传统的双特异性 CD38/CD3 抗体格式和 CD38 mAb 更有效。抗多发性骨髓瘤细胞细胞毒性依赖于内源性 T 细胞的存在。表面 CD38 表达是 TCE 反应的最强生物标志物。My-DST 能够使用多发性骨髓瘤患者自身的骨髓源性 T 细胞测量和表征对 T 细胞结合的抗 CD38 药物 SAR442257 的敏感性。SAR442257 对多发性骨髓瘤有希望,可能最适合既对 CD38 mAb 又对 BCMA 靶向治疗耐药的患者。
意义
本研究引入了使用 My-DST 在使用匹配的内源性 T 细胞的原发性样本中测量和表征对三特异性抗 CD38 T 细胞结合剂 SAR442257 的敏感性。对来自具有不同治疗史的患者样本的临床前测试支持在嵌合抗原受体 T 细胞多发性骨髓瘤后进一步测试。
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