Thymocyte selection‐associated high mobility box protein regulates T lymphocytes exhaustion in patients with myelodysplastic syndromes by inhibiting PI3K/AKT/mTOR pathway

PI3K/AKT/mTOR通路 基因敲除 CD8型 Jurkat细胞 胸腺细胞 蛋白激酶B 癌症研究 生物 细胞毒性T细胞 穿孔素 小干扰RNA T细胞 细胞生物学 信号转导 免疫学 核糖核酸 免疫系统 细胞凋亡 生物化学 体外 基因
作者
Haiyue Niu,Mingjie Zhang,Mengyuan Liu,Liyan Yang,Liping Yang,Jie Ren,Yating Yu,Yumei Liu,Limin Xing,Zonghong Shao,Huaquan Wang
出处
期刊:Hematological Oncology [Wiley]
卷期号:42 (1) 被引量:2
标识
DOI:10.1002/hon.3224
摘要

Abstract Myelodysplastic syndromes (MDS) patients often experience CD8 + T lymphocytes exhaustion, which plays a crucial role in the development of MDS. However, the specific role of thymocyte selection‐associated high mobility box protein (TOX) in the CD8 + T lymphocytes exhaustion in MDS patients remains unclear. In this study, we investigated the role of TOX in CD8 + T lymphocytes exhaustion in patients with MDS. The expression of TOX, inhibitory receptors (IRs), and functional molecules in peripheral blood T lymphocytes of MDS patients and normal controls were detected using flow cytometry. Lentiviral transduction was used to create stable TOX‐knockdown CD8 + T lymphocytes, and small interfering RNA (si‐RNA) was used to knock down TOX in Jurkat cells. The expression of TOX was found to be significantly higher in CD8 + T lymphocytes of MDS patients compared to normal controls. This was associated with upregulated IRs and reduced expression of functional molecules such as Granzyme and Perforin. Myelodysplastic syndromes patients with higher TOX expression had poor clinical indicators and shorter survival. Knockdown of TOX using sh‐RNA partially reverses the exhausted phenotype and enhances the lethality of CD8 + T lymphocytes. Moreover, the knockdown of TOX using si‐RNA in Jurkat cells improved cell proliferation activity, down‐regulated IRs and activated PI3K/AKT/mTOR signaling pathway. TOX promotes the exhaustion of CD8 + T lymphocytes by inhibiting PI3K/AKT/mTOR pathway, and targeted inhibition of TOX could partially restore the effector functions and activity of CD8 + T lymphocytes.
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