Phase I Trial of GD2.CART Cells Augmented With Constitutive Interleukin-7 Receptor for Treatment of High-Grade Pediatric CNS Tumors.

IF 42.1 1区医学 Q1 ONCOLOGY

Journal of Clinical Oncology Pub Date : 2024-08-10 Epub Date: 2024-05-21 DOI:10.1200/JCO.23.02019

Frank Y Lin, Austin Stuckert, Candise Tat, Mark White, Lucia Ruggieri, Huimin Zhang, Birju Mehta, Natalia Lapteva, Zhuyong Mei, Angela Major, Sachin Thakkar, Thomas Shum, Kathan Parikh, Meng-Fen Wu, Holly B Lindsay, Lauren Scherer, Meghan Shekar, Patricia Baxter, Tao Wang, Bambi Grilley, Karen Moeller, John Hicks, Angshumoy Roy, Jamie Anastas, Fatema Malbari, Guillermo Aldave, Murali Chintagumpala, Susan Blaney, D Williams Parsons, Malcolm K Brenner, Helen E Heslop, Cliona M Rooney, Bilal Omer

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引用次数: 0

Abstract

Purpose: T cells modified with chimeric antigen receptors (CARTs) have demonstrated efficacy for hematologic malignancies; however, benefit for patients with CNS tumors has been limited. To enhance T cell activity against GD2+ CNS malignancies, we modified GD2-directed CART cells (GD2.CARTs) with a constitutively active interleukin (IL)-7 receptor (C7R-GD2.CARTs).

Methods: Patients age 1-21 years with H3K27-altered diffuse midline glioma (DMG) or other recurrent GD2-expressing CNS tumors were eligible for this phase I trial (ClinicalTrials.gov identifier: NCT04099797). All subjects received standard-of-care adjuvant radiation therapy or chemotherapy before study enrollment. The first treatment cohort received GD2.CARTs alone (1 × 10⁷ cells/m²), and subsequent cohorts received C7R-GD2.CARTs at two dose levels (1 × 10⁷ cells/m²; 3 × 10⁷ cells/m²). Standard lymphodepletion with cyclophosphamide and fludarabine was included at all dose levels.

Results: Eleven patients (age 4-18 years) received therapy without dose-limiting toxicity. The GD2.CART cohort did not experience toxicity, but had disease progression after brief improvement of residual neurologic deficits (≤3 weeks). The C7R-GD2.CART cohort developed grade 1 tumor inflammation-associated neurotoxicity in seven of eight (88%) cases, controllable with anakinra. Cytokine release syndrome was observed in six of eight (75%, grade 1 in all but one patient) and associated with increased circulating IL-6 and IP-10 (P < .05). Patients receiving C7R-GD2.CARTs experienced temporary improvement from baseline neurologic deficits (range, 2 to >12 months), and seven of eight (88%) remained eligible for additional treatment cycles (range 2-4 cycles). Partial responses by iRANO criteria were observed in two of seven (29%) patients with DMG treated by C7R-GD2.CARTs.

Conclusion: Intravenous GD2.CARTs with and without C7R were well tolerated. Patients treated with C7R-GD2.CARTs exhibited transient improvement of neurologic deficits and increased circulating cytokines/chemokines. Treatment with C7R-GD2.CARTs represents a novel approach warranting further investigation for children with these incurable CNS cancers.

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用组成型白细胞介素-7受体扩增的 GD2.CART 细胞治疗高级别小儿中枢神经系统肿瘤的 I 期试验。

目的：用嵌合抗原受体（CARTs）修饰的 T 细胞对血液系统恶性肿瘤有疗效，但对中枢神经系统肿瘤患者的疗效有限。为了增强T细胞对抗GD2+中枢神经系统恶性肿瘤的活性，我们用组成型活性白细胞介素（IL）-7受体（C7R-GD2.CARTs）改造了GD2定向CART细胞（GD2.CARTs）：1-21岁患有H3K27改变的弥漫中线胶质瘤（DMG）或其他复发性GD2表达中枢神经系统肿瘤的患者有资格参加这项I期试验（ClinicalTrials.gov标识符：NCT04099797）。所有受试者在入组前都接受了标准辅助放疗或化疗。第一个治疗队列单独接受 GD2.CARTs 治疗（1 × 107 cells/m2），随后的治疗队列接受两种剂量水平的 C7R-GD2.CARTs 治疗（1 × 107 cells/m2; 3 × 107 cells/m2）。所有剂量水平均使用环磷酰胺和氟达拉滨进行标准淋巴清除：11名患者（4-18岁）接受了治疗，未出现剂量限制性毒性。GD2.CART队列未出现毒性，但在残余神经功能缺损短暂改善（≤3周）后出现疾病进展。C7R-GD2.CART队列的8个病例中有7个（88%）出现了1级肿瘤炎症相关神经毒性，使用阿纳金拉后可得到控制。8例患者中有6例（75%，除1例患者外均为1级）出现细胞因子释放综合征，并与循环中IL-6和IP-10的增加有关（P < .05）。接受 C7R-GD2.CARTs 治疗的患者的基线神经功能缺损得到暂时改善（2 至 12 个月），8 例患者中有 7 例（88%）仍符合接受其他治疗周期（2-4 个周期）的条件。在接受C7R-GD2.CARTs治疗的7例DMG患者中，有2例（29%）按照iRANO标准观察到部分反应：结论：静脉注射含或不含C7R的GD2.CARTs耐受性良好。接受C7R-GD2.CARTs治疗的患者神经功能缺损得到短暂改善，循环细胞因子/造血因子增加。使用C7R-GD2.CARTs治疗是一种新方法，值得对患有这些无法治愈的中枢神经系统癌症的儿童进行进一步研究。

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来源期刊

Journal of Clinical Oncology 医学-肿瘤学

CiteScore

41.20

自引率

2.20%

发文量

8215

审稿时长

2 months

期刊介绍： The Journal of Clinical Oncology serves its readers as the single most credible, authoritative resource for disseminating significant clinical oncology research. In print and in electronic format, JCO strives to publish the highest quality articles dedicated to clinical research. Original Reports remain the focus of JCO, but this scientific communication is enhanced by appropriately selected Editorials, Commentaries, Reviews, and other work that relate to the care of patients with cancer.