IRE1α抑制在逆转线粒体活性氧诱导的CD8 T细胞衰老及对多发性骨髓瘤发挥直接抗肿瘤作用中的双重作用

Dual roles of IRE1α inhibition in reversing mitochondrial ROS-induced CD8 T-cell senescence and exerting direct antitumor effects in multiple myeloma.

作者信息

Wan Yike, Wang Jingjing, Chen Mengping, Wang Junying, Nan Fajun, Huang Honghui, Liu Zhiqiang, Hou Jian

机构信息

Department of Hematology, Ren Ji Hospital, Shanghai Jiao Tong University School of Medicine, Shanghai, China.

Shandong Provincial Key Laboratory of Precision Oncology, Shandong Cancer Hospital and Institute, Shandong First Medical University and Shandong Academy of Medical Sciences, Jinan, China.

出版信息

J Immunother Cancer. 2025 May 26;13(5):e011044. doi: 10.1136/jitc-2024-011044.

DOI:10.1136/jitc-2024-011044

PMID:40425229

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC12107582/

Abstract

BACKGROUND

Multiple myeloma (MM) is characterized by the proliferation of malignant plasma cells within the bone marrow (BM) microenvironment, which significantly contributes to immune suppression of CD8 T cells. Our previous research identified that dysregulation of the IRE1α-XBP1s-SLC38A2 axis leads to decreased glutamine uptake and senescence of CD8 T cells in MM. However, the underlying mechanisms of T-cell senescence remain unclear.

METHODS

Single-cell RNA sequencing was used to analyze mitochondrial function in CD8 T cells in MM. The effects of XBP1s and SLC38A2 on mitochondrial reactive oxygen species (mtROS) were evaluated by flow cytometry under loss-of-function experiments. An IRE1α inhibitor (17#) was administered to explore its effects on T-cell senescence and MM cell growth. RNA sequencing was employed to disclose pathway alterations in T cells treated with 17#. The Vk*MYC mouse model was used to assess the impact of 17# on CD8 T cell senescence and anti-myeloma effects.

RESULTS

BM-derived CD8 T cells from patients with MM exhibited downregulated expressions of genes critical for glutamine transport (SLC38A2), mitochondrial respiratory chain, and ATP synthesis, while genes associated with ROS were upregulated. Suppression of XBP1s in CD8 T cells resulted in decreased mtROS levels, whereas inhibition of SLC38A2 increased mtROS levels. Compound 17# significantly reduced senescence marker KLRG1 expression and increased perforin expression in nutrient-deprived BM CD8 T cells from healthy donors and in BM CD8 T cells from patients with MM, while promoting T-cell proliferation. Importantly, 17# did not impair the viability of peripheral blood mononuclear cells from healthy donors or alter the immune phenotypes of healthy CD8 T cells. The NPR2-cGMP-PKG pathway was activated by IRE1α inhibition in restoring T-cell function. Furthermore, 17# exhibited direct inhibitory effects on MM cells. In Vk*MYC mouse model, 17# decreased mtROS levels in BM CD8 T cells, reduced the proportion of senescent (KLRG1CD57CD28) T cells, and resulted in a lower tumor burden.

CONCLUSION

Inhibiting IRE1α represents a promising strategy to reverse the senescence of CD8 T cells by mitigating mtROS production. This dual mechanism not only rejuvenates T cells but also directly targets myeloma cells, offering a novel therapeutic approach for MM treatment.

摘要

背景

多发性骨髓瘤（MM）的特征是骨髓（BM）微环境中恶性浆细胞的增殖，这显著导致CD8 T细胞的免疫抑制。我们之前的研究发现，IRE1α-XBP1s-SLC38A2轴的失调导致MM中CD8 T细胞的谷氨酰胺摄取减少和衰老。然而，T细胞衰老的潜在机制仍不清楚。

方法

使用单细胞RNA测序分析MM中CD8 T细胞的线粒体功能。在功能丧失实验中，通过流式细胞术评估XBP1s和SLC38A2对线粒体活性氧（mtROS）的影响。给予IRE1α抑制剂（17#）以探索其对T细胞衰老和MM细胞生长的影响。采用RNA测序揭示用17#处理的T细胞中的通路改变。使用Vk*MYC小鼠模型评估17#对CD8 T细胞衰老和抗骨髓瘤作用的影响。

结果

MM患者的BM来源的CD8 T细胞表现出谷氨酰胺转运（SLC38A2）、线粒体呼吸链和ATP合成关键基因的表达下调，而与ROS相关的基因上调。CD8 T细胞中XBP1s的抑制导致mtROS水平降低，而SLC38A2的抑制增加mtROS水平。化合物17#显著降低了来自健康供体的营养缺乏的BM CD8 T细胞和MM患者的BM CD8 T细胞中衰老标志物KLRG1的表达，并增加了穿孔素的表达，同时促进T细胞增殖。重要的是，17#不损害健康供体外周血单个核细胞的活力，也不改变健康CD8 T细胞的免疫表型。IRE1α抑制通过恢复T细胞功能激活NPR2-cGMP-PKG通路。此外，17#对MM细胞表现出直接抑制作用。在Vk*MYC小鼠模型中，17#降低了BM CD8 T细胞中的mtROS水平，降低了衰老（KLRG1CD57CD28）T细胞的比例，并导致较低的肿瘤负担。