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靶向自噬可克服 B 细胞恶性肿瘤中 CAR-T 免疫疗法的内在耐药性。

Targeting autophagy overcomes cancer-intrinsic resistance to CAR-T immunotherapy in B-cell malignancies.

机构信息

Institute of Hematology, Union Hospital, Tongji Medical College, Huazhong University of Science and Technology, Wuhan, Hubei, P. R. China.

Hubei Clinical Medical Center of Cell Therapy For Neoplastic Disease, Wuhan, Hubei, P. R. China.

出版信息

Cancer Commun (Lond). 2024 Mar;44(3):408-432. doi: 10.1002/cac2.12525. Epub 2024 Feb 26.

DOI:10.1002/cac2.12525

PMID:38407943

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10958674/

Abstract

BACKGROUND

Chimeric antigen receptor T (CAR-T) therapy has substantially revolutionized the clinical outcomes of patients with hematologic malignancies, but the cancer-intrinsic mechanisms underlying resistance to CAR-T cells remain yet to be fully understood. This study aims to explore the molecular determinants of cancer cell sensitivity to CAR-T cell-mediated killing and to provide a better understanding of the underlying mechanisms and potential modulation to improve clinical efficacy.

METHODS

The human whole-genome CRISPR/Cas9-based knockout screening was conducted to identify key genes that enable cancer cells to evade CD19 CAR-T-cell-mediated killing. The in vitro cytotoxicity assays and evaluation of tumor tissue and bone marrow specimens were further conducted to confirm the role of the key genes in cancer cell susceptibility to CAR-T cells. In addition, the specific mechanisms influencing CAR-T cell-mediated cancer clearance were elucidated in mouse and cellular models.

RESULTS

The CRISPR/Cas9-based knockout screening showed that the enrichment of autophagy-related genes (ATG3, BECN1, and RB1CC1) provided protection of cancer cells from CD19 CAR-T cell-mediated cytotoxicity. These findings were further validated by in vitro cytotoxicity assays in cells with genetic and pharmacological inhibition of autophagy. Notably, higher expression of the three autophagy-related proteins in tumor samples was correlated with poorer responsiveness and worse survival in patients with relapsed/refractory B-cell lymphoma after CD19 CAR-T therapy. Bulk RNA sequencing analysis of bone marrow samples from B-cell leukemia patients also suggested the clinical relevance of autophagy to the therapeutic response and relapse after CD19 CAR-T cell therapy. Pharmacological inhibition of autophagy and knockout of RB1CC1 could dramatically sensitize tumor cells to CD19 CAR-T cell-mediated killing in mouse models of both B-cell leukemia and lymphoma. Moreover, our study revealed that cancer-intrinsic autophagy mediates evasion of CAR-T cells via the TNF-α-TNFR1 axis-mediated apoptosis and STAT1/IRF1-induced chemokine signaling activation.

CONCLUSIONS

These findings confirm that autophagy signaling in B-cell malignancies is essential for the effective cytotoxic function of CAR-T cells and thereby pave the way for the development of autophagy-targeting strategies to improve the clinical efficacy of CAR-T cell immunotherapy.

摘要

背景

嵌合抗原受体 T（CAR-T）疗法极大地改变了血液系统恶性肿瘤患者的临床结局，但癌症内在的对 CAR-T 细胞耐药的机制仍有待充分理解。本研究旨在探索癌细胞对 CAR-T 细胞介导杀伤的敏感性的分子决定因素，并提供对潜在机制的更好理解和潜在的调节以提高临床疗效。

方法

采用人全基因组 CRISPR/Cas9 敲除筛选，鉴定使癌细胞逃避 CD19 CAR-T 细胞介导杀伤的关键基因。进一步进行体外细胞毒性测定，并评估肿瘤组织和骨髓标本，以确认关键基因在癌细胞对 CAR-T 细胞的敏感性中的作用。此外，在小鼠和细胞模型中阐明了影响 CAR-T 细胞介导的癌症清除的特定机制。

结果

基于 CRISPR/Cas9 的敲除筛选表明，自噬相关基因（ATG3、BECN1 和 RB1CC1）的富集为癌细胞提供了免受 CD19 CAR-T 细胞介导的细胞毒性的保护。这些发现通过体外细胞毒性测定在基因和自噬药理学抑制的细胞中得到了进一步验证。值得注意的是，在接受 CD19 CAR-T 治疗后复发/难治性 B 细胞淋巴瘤患者的肿瘤样本中，这三种自噬相关蛋白的高表达与对治疗的反应性较差和生存较差相关。来自 B 细胞白血病患者的骨髓样本的批量 RNA 测序分析也表明自噬与 CD19 CAR-T 细胞治疗后的治疗反应和复发相关。自噬的药理学抑制和 RB1CC1 的敲除可以显著增强肿瘤细胞对 CD19 CAR-T 细胞介导的杀伤作用，无论是在 B 细胞白血病还是淋巴瘤的小鼠模型中。此外，我们的研究表明，癌症内在的自噬通过 TNF-α-TNFR1 轴介导的细胞凋亡和 STAT1/IRF1 诱导的趋化因子信号激活来逃避 CAR-T 细胞。

结论

这些发现证实了 B 细胞恶性肿瘤中的自噬信号对于 CAR-T 细胞的有效细胞毒性功能是必不可少的，从而为开发针对自噬的策略以改善 CAR-T 细胞免疫治疗的临床疗效铺平了道路。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d90e/10958674/2e335677326d/CAC2-44-408-g004.jpg

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靶向自噬可克服 B 细胞恶性肿瘤中 CAR-T 免疫疗法的内在耐药性。

Targeting autophagy overcomes cancer-intrinsic resistance to CAR-T immunotherapy in B-cell malignancies.

机构信息

出版信息

BACKGROUND

METHODS

RESULTS

CONCLUSIONS

背景

方法

结果

结论

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