Feasibility and Safety of Personalized, Multi-Target, Adoptive Cell Therapy (IMA101): First-in-Human Clinical Trial in Patients with Advanced Metastatic Cancer

医学 氟达拉滨 白细胞清除术 细胞因子释放综合征 内科学 T细胞 CD8型 不利影响 免疫疗法 耐受性 肿瘤科 细胞疗法 癌症 免疫学 胃肠病学 环磷酰胺 嵌合抗原受体 抗原 免疫系统 化疗 细胞 干细胞 生物 川地34 遗传学
作者
Apostolia Maria Tsimberidou,Kerstin Guenther,Borje S. Andersson,Regina Mendrzyk,Amir Alpert,Claudia Wagner,Anna Nowak,Katrin Aslan,Arun Satelli,Fabian Richter,Sabrina Kuttruff-Coqui,Oliver Schoor,Jens Fritsche,Zoe Coughlin,Ali S. Mohamed,Kerry Sieger,Becky Norris,Rita Ort,Jennifer Beck,Henry Hiep. Vo,Franziska Hoffgaard,Manuel Ruh,Linus Backert,Ignacio I. Wistuba,David Fuhrmann,Nuhad K. Ibrahim,Jeffrey S. Morris,Bryan K. Kee,Daniel M. Halperin,Graciela M. Nogueras-Gonzalez,Partow Kebriaei,Elizabeth J. Shpall,David Vining,Patrick Hwu,Harpreet Singh-Jasuja,Carsten Reinhardt,Cedrik M. Britten,Norbert Hilf,Toni Weinschenk,Dominik Maurer,Steffen Walter
出处
期刊:Cancer immunology research [American Association for Cancer Research]
卷期号:: OF1-OF21
标识
DOI:10.1158/2326-6066.cir-22-0444
摘要

Abstract IMA101 is an actively personalized, multi-targeted adoptive cell therapy (ACT), whereby autologous T cells are directed against multiple novel defined peptide-HLA (pHLA) cancer targets. HLA-A*02:01-positive patients with relapsed/refractory solid tumors expressing ≥1 of 8 predefined targets underwent leukapheresis. Endogenous T cells specific for up to 4 targets were primed and expanded in vitro. Patients received lymphodepletion (fludarabine, cyclophosphamide), followed by T-cell infusion and low-dose IL2 (Cohort 1). Patients in Cohort 2 received atezolizumab for up to 1 year (NCT02876510). Overall, 214 patients were screened, 15 received lymphodepletion (13 women, 2 men; median age, 44 years), and 14 were treated with T-cell products. IMA101 treatment was feasible and well tolerated. The most common adverse events were cytokine release syndrome (Grade 1, n = 6; Grade 2, n = 4) and expected cytopenias. No patient died during the first 100 days after T-cell therapy. No neurotoxicity was observed. No objective responses were noted. Prolonged disease stabilization was noted in three patients lasting for 13.7, 12.9, and 7.3 months. High frequencies of target-specific T cells (up to 78.7% of CD8+ cells) were detected in the blood of treated patients, persisted for >1 year, and were detectable in posttreatment tumor tissue. Individual T-cell receptors (TCR) contained in T-cell products exhibited broad variation in TCR avidity, with the majority being low avidity. High-avidity TCRs were identified in some patients’ products. This study demonstrates the feasibility and tolerability of an actively personalized ACT directed to multiple defined pHLA cancer targets. Results warrant further evaluation of multi-target ACT approaches using potent high-avidity TCRs. See related Spotlight by Uslu and June, p. 865
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