在多发性骨髓瘤患者中,PD-1 和 TIM-3 T 细胞广泛表达共同 γ 链细胞因子受体,IL-2、IL-7、IL-15 的刺激可上调 T 细胞上的 PD-1 和 TIM-3。
PD-1 and TIM-3 T cells widely express common γ-chain cytokine receptors in multiple myeloma patients, and IL-2, IL-7, IL-15 stimulation up-regulates PD-1 and TIM-3 on T cells.
机构信息
Laboratory of Cellular Immunotherapy, Research Institute of Fundamental and Clinical Immunology, Novosibirsk, 630099, Russia.
V. Zelman Institute of Medicine and Psychology, Novosibirsk National Research State University, Novosibirsk, 630090, Russia.
出版信息
Oncol Res. 2024 Sep 18;32(10):1575-1587. doi: 10.32604/or.2024.047893. eCollection 2024.
BACKGROUND
Immune checkpoint ligand-receptor interactions appear to be associated with multiple myeloma (MM) progression. Simultaneously, previous studies showed the possibility of PD-1 and TIM-3 expression on T cells upon stimulation with common γ-chain family cytokines and during homeostatic proliferation. The aim of the present work was to study the impact of homeostatic proliferation on the expansion of certain T cell subsets up-regulating PD-1 and TIM-3 checkpoint molecules.
METHODS
The expression of CD25, CD122, CD127 common γ-chain cytokine receptors, phosphorylated signal transducer and activator of transcription-5 (pSTAT5) and eomesodermin (EOMES) was comparatively assessed with flow cytometry in PD-1- and TIM-3-negative and positive T cells before the conditioning and during the first post-transplant month in peripheral blood samples of MM patients.
RESULTS
Substantial proportions of PD-1- and TIM-3-positive T lymphocytes expressed common γ-chain cytokine receptors and pSTAT5. Frequencies of cytokine receptor expressing cells were significantly higher within TIM-3 T cells compared to PD-1TIM-3 subsets. Considerable proportions of both PD-1-/TIM-3-negative and positive CD8 T cells express EOMES, while only moderate frequencies of CD4 PD-1/TIM-3 T cells up-regulate this transcription factor. Besides, the surface presence of CD25 and intranuclear expression of EOMES in CD4 T cells were mutually exclusive regardless of PD-1 and TIM-3 expression. The stimulation with common γ-chain cytokines up-regulates PD-1 and TIM-3 during the proliferation of initially PD-1/TIM-3-negative T cells but fails to expand initially PD-1 and TIM-3 T cell subsets .
CONCLUSIONS
Both PD-1 and TIM-3 expressing T cells appear to be able to respond to homeostatic cytokine stimulation. Differences in common γ-chain cytokine receptor expression between PD-1 and TIM-3 T cells may reflect functional dissimilarity of these cell subsets. Checkpoint blockade appears to alleviate lymphopenia-induced proliferation of PD-1 T cells but may raise the possibility of immune-mediated adverse events.
背景
免疫检查点配体-受体相互作用似乎与多发性骨髓瘤(MM)的进展有关。同时,先前的研究表明,在受到共同γ链家族细胞因子刺激以及在稳态增殖期间,T 细胞上可能表达 PD-1 和 TIM-3。本研究旨在研究稳态增殖对某些上调 PD-1 和 TIM-3 检查点分子的 T 细胞亚群扩增的影响。
方法
使用流式细胞术比较评估了 MM 患者外周血样本中,在预处理前和移植后第一个月期间,PD-1-和 TIM-3-阴性和阳性 T 细胞中 CD25、CD122、CD127 共同 γ 链细胞因子受体、磷酸化信号转导和转录激活因子 5(pSTAT5)和 Eomesodermin(EOMES)的表达。
结果
大量 PD-1-和 TIM-3-阳性 T 淋巴细胞表达共同 γ 链细胞因子受体和 pSTAT5。与 PD-1/TIM-3 亚群相比,TIM-3 T 细胞中细胞因子受体表达细胞的频率显著更高。PD-1-/TIM-3-阴性和阳性 CD8 T 细胞均有相当比例表达 EOMES,而只有中度频率的 CD4 PD-1/TIM-3 T 细胞上调此转录因子。此外,CD4 T 细胞中 CD25 的表面存在和 EOMES 的核内表达是相互排斥的,无论 PD-1 和 TIM-3 的表达情况如何。共同 γ 链细胞因子的刺激可在最初 PD-1/TIM-3-阴性 T 细胞的增殖过程中上调 PD-1 和 TIM-3,但不能扩增最初的 PD-1 和 TIM-3 T 细胞亚群。
结论
表达 PD-1 和 TIM-3 的 T 细胞似乎都能够对稳态细胞因子刺激作出反应。PD-1 和 TIM-3 T 细胞之间共同 γ 链细胞因子受体表达的差异可能反映了这些细胞亚群的功能差异。检查点阻断似乎可以减轻淋巴细胞减少引起的 PD-1 T 细胞增殖,但可能增加免疫介导的不良事件的可能性。
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