基于血小板输注体外细胞模型探究ASIC3驱动Ca2+-CaN-NFAT信号轴诱发Treg/Th17免疫失衡的作用*

doi:10.3969/j.issn.1671-2587.2025.06.006

临床输血与检验 ›› 2025, Vol. 27 ›› Issue (6): 782-788.DOI: 10.3969/j.issn.1671-2587.2025.06.006

基于血小板输注体外细胞模型探究ASIC3驱动Ca²⁺-CaN-NFAT信号轴诱发Treg/Th17免疫失衡的作用^*

梁静, 范娜, 郑淑贤, 刘雯

新疆医科大学第六附属医院,新疆乌鲁木齐 830002

收稿日期:2025-06-12 出版日期:2025-12-20 发布日期:2025-12-24
通讯作者: 刘雯,主要从事临床输血学的免疫机制研究,E-mail：1277879139@qq.com。
作者简介:梁静,主要从事临床输血学的免疫机制研究,E-mail：1793645027@qq.com。
基金资助:
^*本课题受新疆维吾尔自治区自然科学基金面上项目（No.2022D01C585）、新疆维吾尔自治区自然科学基金青年基金项目（No.2022D01C822）资助

Role of ASIC3-driven Ca²⁺-CaN-NFAT Signaling Axis in Inducing Treg/Th17 Immune Imbalance Platelet Transfusion in Vitro Cell Model

LIANG Jing, FAN Na, ZHENG Shuxian, LIU Wen

The Sixth Affiliated Hospital of Xinjiang Medical University, Urumqi 830002

Received:2025-06-12 Online:2025-12-20 Published:2025-12-24

摘要/Abstract

摘要： 目的探讨酸敏感离子通道3（ASIC3）通过调控Ca²⁺-钙调磷酸酶（CaN）-活化T细胞核因子（NFAT）信号轴对调节性T细胞（Treg）/辅助性T细胞17（Th17）免疫平衡的作用机制。方法将供者血小板与受者外周血单个核细胞（PBMCs）按250∶1比例进行体外共培养模拟体内血小板输注状态,通过构建ASIC3过表达慢病毒,与体外细胞模型共培养,将其分为三组：（1）空白对照组;（2）阴性对照慢病毒组;（3）ASIC3过表达慢病毒组。采用流式细胞术检测Treg（Foxp3⁺）和Th17（IL-17A⁺）细胞比例及细胞内Ca²⁺水平;Western blot检测ASIC3、磷脂酶CB（PLCB）、CaN、NFATC1及其磷酸化蛋白（p-NFATC1）的表达。结果与空白对照组相比,ASIC3过表达慢病毒组Th17细胞比例显著升高（P<0.01）,Treg比例显著降低（P<0.05）;细胞内Ca²⁺浓度升高1.8倍（P<0.001）。蛋白检测显示,ASIC3过表达组PLCB、CaN及p-NFATC1表达均显著上调（均P<0.05）。结论 ASIC3过表达通过激活Ca²⁺-CaN-NFAT信号轴,上调PLCB/CaN/p-NFATC1表达,促进NFAT持续性活化,进而驱动IL-17转录,最终导致Treg/Th17免疫失衡。

关键词: 酸敏离子通道, 细胞实验, Treg/Th17平衡, 钙离子, 外周血单个核细胞

Abstract: Objective To investigate the regulatory mechanism underlying the effect of acid-sensing ion channel 3 (ASIC3) on the balance between regulatory T (Treg) cells and T helper type 17 (Th17) cells via the Ca²⁺-calcineurin (CaN)-nuclear factor of activated T cells (NFAT) signaling axis. Methods Donor platelets and recipient peripheral blood mononuclear cells (PBMCs) were co-cultured in vitro at a ratio of 250∶1 to simulate the state of platelet transfusion in vitro. By constructing ASIC3 overexpression lentivirus and co-culturing with in vitro cell model, they were divided into three groups: (1) blank control group; (2) negative control lentivirus group; (3) ASIC3 overexpression lentivirus group. The proportion of Treg (Foxp3⁺) and Th17 (IL-17A⁺) cells and intracellular Ca²⁺ level were detected by flow cytometry. The expression of ASIC3, phospholipase CB (PLCB), CaN, NFATC1 and its phosphorylated protein (p-NFATC1) were detected by Western blot. Results Compared with the blank control group, the proportion of Th17 cells in the ASIC3 overexpression lentivirus group was significantly increased (P<0.01), and the proportion of Treg cells was significantly decreased (P<0.05). Intracellular Ca²⁺ concentration increased 1.8 times (P<0.001). Protein detection showed that the expression of PLCB, CaNand p-NFATC1 in ASIC3 overexpression group were significantly up-regulated (all P<0.05). Conclusion ASIC3 overexpression up-regulates the expression of PLCB/CaN/p-NFATC1 by activating the Ca²⁺-CaN-NFAT signaling axis, promotes the continuous activation of NFAT, and then drives IL-17 transcription, eventually leading to Treg/Th17 immune imbalance.

Key words: ASIC3, Cell experiment, Treg/Th17 balance, Calcium ion, PBMCs

中图分类号:

R392.11

梁静, 范娜, 郑淑贤, 刘雯. 基于血小板输注体外细胞模型探究ASIC3驱动Ca²⁺-CaN-NFAT信号轴诱发Treg/Th17免疫失衡的作用^*[J]. 临床输血与检验, 2025, 27(6): 782-788.

LIANG Jing, FAN Na, ZHENG Shuxian, LIU Wen. Role of ASIC3-driven Ca²⁺-CaN-NFAT Signaling Axis in Inducing Treg/Th17 Immune Imbalance Platelet Transfusion in Vitro Cell Model[J]. JOURNAL OF CLINICAL TRANSFUSION AND LABORATORY MEDICINE, 2025, 27(6): 782-788.

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基于血小板输注体外细胞模型探究ASIC3驱动Ca²⁺-CaN-NFAT信号轴诱发Treg/Th17免疫失衡的作用^*

Role of ASIC3-driven Ca²⁺-CaN-NFAT Signaling Axis in Inducing Treg/Th17 Immune Imbalance Platelet Transfusion in Vitro Cell Model

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