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Current Challenges in Providing Good Leukapheresis Products for Manufacturing of CAR-T Cells for Patients with Relapsed/Refractory NHL or ALL

机译:在为复发/难治性NHL或ALL患者提供良好的白细胞分离术产品以制造CAR-T细胞方面当前面临的挑战

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摘要

Background: T lymphocyte collection through leukapheresis is an essential step for chimeric antigen receptor T (CAR-T) cell therapy. Timing of apheresis is challenging in heavily pretreated patients who suffer from rapid progressive disease and receive T cell impairing medication. Methods: A total of 75 unstimulated leukaphereses were analyzed including 45 aphereses in patients and 30 in healthy donors. Thereof, 41 adult patients with Non-Hodgkin’s lymphoma (85%) or acute lymphoblastic leukemia (15%) underwent leukapheresis for CAR-T cell production. Results: Sufficient lymphocytes were harvested from all patients even from those with low peripheral lymphocyte counts of 0.18L. Only four patients required a second leukapheresis session. Leukapheresis products contained a median of 98 × 10 (9 - 341 × 10 ) total nucleated cells (TNC) with 38 × 10 (4 - 232 × 10 ) CD3+ T cells. Leukapheresis products from healthy donors as well as from patients in complete remission were characterized by high TNC and CD3+ T lymphocyte counts. CAR-T cell products could be manufactured for all but one patient. Conclusions: Sufficient yield of lymphocytes for CAR-T cell production is feasible also for patients with low peripheral blood counts. Up to 12–15 L blood volume should be processed in patients with absolute lymphocyte counts ≤ 1.0L.
机译:背景:通过白细胞分离术收集T淋巴细胞是嵌合抗原受体T(CAR-T)细胞治疗的重要步骤。在接受快速治疗且患有T细胞损害药物的经过大量预处理的患者中,血液采血的时机具有挑战性。方法:共分析了75种未刺激的白血球,包括患者中的45种和健康供体中的30种。其中,有41名成年非霍奇金淋巴瘤(85%)或急性淋巴细胞白血病(15%)患者接受了白细胞去除术以产生CAR-T细胞。结果:所有患者均收集了足够的淋巴细胞,即使外周血淋巴细胞计数低至0.18 / nL的患者也是如此。仅四名患者需要第二次白细胞清除术。白细胞分离术产品中位数为98×10(9-341×10)总有核细胞(TNC)和38×10(4-232×10)CD3 + T细胞。来自健康供体以及完全缓解患者的白细胞分离术产品的特征是TNC和CD3 + T淋巴细胞计数高。 CAR-T细胞产品可为一名患者以外的所有患者生产。结论:对于外周血计数低的患者,充足的淋巴细胞产量可用于CAR-T细胞的生产。绝对淋巴细胞计数≤1.0 / nL的患者应处理多达12-15 L的血容量。

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