siRNA沉默锌指蛋白A20基因促进人类风湿关节炎成纤维细胞样滑膜细胞焦亡

doi:10.16352/j.issn.1001-6325.2024.10.1407

基础医学与临床 ›› 2024, Vol. 44 ›› Issue (10): 1407-1413.doi: 10.16352/j.issn.1001-6325.2024.10.1407

siRNA沉默锌指蛋白A20基因促进人类风湿关节炎成纤维细胞样滑膜细胞焦亡

赵紫琴^*, 董淑慧, 尹海波, 刘爱东, 杨勇, 熊光宜

天津大学天津医院病理科,天津 300211

收稿日期:2024-02-23 修回日期:2024-06-04 出版日期:2024-10-05 发布日期:2024-09-27
通讯作者: ^* starelr_99@126.com
基金资助:
天津市企业博士后择优资助项目(TJQYBSH2018021)

Zinc finger protein A20-targeting siRNA promotes pyroptosis of human rheumatoid arthritis fibroblast-like synoviocytes

ZHAO Ziqin^*, DONG Shuhui, YIN Haibo, LIU Aidong, YANG Yong, XIONG Guangyi

Department of Pathology, Tianjin Hospital of Tianjin University, Tianjin 300211, China

Received:2024-02-23 Revised:2024-06-04 Online:2024-10-05 Published:2024-09-27
Contact: ^* starelr_99@126.com

摘要/Abstract

摘要： 目的探讨小干扰RNA(siRNA)沉默锌指蛋白A20基因对人类风湿关节炎(RA)成纤维细胞样滑膜细胞(HFLS-RA)焦亡的调节作用。方法培养人HFLS-RA细胞系(MH7A细胞),通过RNA干扰技术靶向敲降人类A20基因,合成siRNA-A20,用脂质体法将siRNA-A20(沉默组)和siRNA-NC(阴性对照组)转染MH7A细胞。RT-qPCR 检测细胞中NLRP3和Caspase-1 mRNA 的表达;Western blot 法检测细胞中NLRP3和Caspase-1蛋白表达;ELISA法检测细胞培养液中IL-1β和IL-18的水平;透射电子显微镜(TEM)检测细胞焦亡。结果 siRNA-A20组MH7A细胞中NLRP3和Caspase-1 mRNA和蛋白表达水平与对照组相比均显著增高(P＜0.01);siRNA-A20组细胞培养上清液中IL-1β、IL-18浓度与对照组相比均显著增高(P＜0.01)。与对照组相比,siRNA-A20组部分细胞肿胀和破裂,细胞膜的完整性也丧失,细胞内出现大面积水肿区,细胞核局部核膜凹陷模糊,异染色质固缩增加,分布不均匀并在核膜周围聚集。结论通过siRNA沉默A20表达后可促进HFLS-RA中NLRP3/Caspase-1介导细胞焦亡,为探讨RA临床治疗新方案提供了实验依据。

关键词: 类风湿关节炎, NLRP3炎性小体, 锌指蛋白A20, 细胞焦亡, 成纤维细胞样滑膜细胞

Abstract: Objective To investigate the regulatory effect of small interfering RNA (siRNA) silencing zinc finger protein A20 on pyroptosis of rheumatoid arthritis(RA) fibroblast-like synoviocytes (HFLS-RA). Methods Human FLS-RA cell line MH7A cells were cultivated, A20 siRNA silencing group was synthesized for knocking down the human A20 gene, and then specific A20 gene siRNA and siRNA-NC(negative control)were transfected into MH7A cells using liposome method. RT-qPCR was applied to detect the expression of NLRP3 and Caspase-1 mRNA in cells.The protein expression of NLRP3 and Caspase-1 was detected by Western blot, and IL-1β and IL-18 in cell culture medium were detected by ELISA method. Transmission electron microscopy (TEM) was used to detect pyroptosis. Results After A20 knockdown, the mRNA and expression of NLRP3 and Caspase-1 in MH7A cells in the siRNA-A20 group were significantly increased as compared with the siRNA-NC group(P＜0.01). The concentration of IL-1β and IL-18 in the cell culture supernatant of the siRNA-A20 group was significantly increased compared with the siRNA-NC group (P＜0.01). Compared with the siRNA-NC group, some cells in the siRNA-A20 group showed swollen and ruptured. The integrity of the cell membrane was also lost, and a large area of edema was present in the cell. In addition, a blurred depression of the local nuclear membrane was noted, while an increase in heterochromatin pyknosis was accompanied by their uneven distribution as well as their aggregation around the nuclear membrane. Conclusions Silencing of A20 gene with siRNA might promote NLRP3/Caspase-1 mediated pyroptosis in HFLS-RA, which lays an experimental foundation for new clinical treatment methods of RA.

Key words: rheumatoid arthritis, NLRP3 inflammasome, zinc finger protein A20, pyroptosis, fibroblast-like synoviocytes

中图分类号:

R684.3

赵紫琴, 董淑慧, 尹海波, 刘爱东, 杨勇, 熊光宜. siRNA沉默锌指蛋白A20基因促进人类风湿关节炎成纤维细胞样滑膜细胞焦亡[J]. 基础医学与临床, 2024, 44(10): 1407-1413.

参考文献

[1]Huang YJ, Han L, Li J, et al. Acquired coagulation dysfunction resulting from vitamin K-dependent coagulation factor deficiency associated with rheumatoid arthritis: a case report[J]. World J Clin Cases, 2022, 10: 236-241.
[2]Cui SB, Wang TX, Liu ZW, et al. Zinc finger protein A20 regulates the development and progression of osteoarthritis by affecting the activity of NF-kappaB p65[J]. Immunopharm Immunot, 2021, 43: 713-723.
[3]Vande Walle L, Van Opdenbosch N, Jacques P, et al. Negative regulation of the NLRP3 inflammasome by A20 protects against arthritis.[J] Nature, 2014, 512:69-73.
[4]Huang J, Fu X, Chen X, et al. Promising therapeutic targets for treatment of rheumatoid arthritis[J]. Front Immunol, 2021,12:686155. doi: 10.3389/fimmu.2021.686155.
[5]He L, Luan H, He J, et al. Shikonin attenuates rheumatoid arthritis by targeting SOCS1/JAK/STAT signaling pathway of fibroblast like synoviocytes[J]. Chin Med, 2021,16:96. doi: 10.1186/s13020-021-00510-6.
[6]Martens A, van Loo G. A20 at the crossroads of cell death, inflammation, and autoimmunity[J]. Cold Spring Harb Perspect Biol, 2020, 12:a036418. doi: 10.1101/cshperspect.a036418.
[7]Priem D, van Loo G, Bertrand MJM. A20 and cell death-driven inflammation[J].Trends Immunol, 2020, 41:421-435.
[8]Arne Martens, Dario Priem, Esther Hoste, et al. Two distinct ubiquitin-binding motifs in A20 mediate its anti-inflammatory and cell-protective activities[J]. Nat Immunol, 2020, 21:381-387.
[9]Elsby LM, Orozco G, Denton J, et al. Functional evaluation of TNFAIP3 (A20) in rheumatoid arthritis[J]. Clin Exp Rheumatol, 2010, 28: 708-714.
[10]Jia C, Chen H, Zhang J, et al. Role of pyroptosis in cardiovascular diseases[J]. Int Immunopharmacol, 2019, 67:311-318.
[11]Leu SY, Tsang YL, Ho LC, et al. NLRP3 inflammasome activation, metabolic danger signals, and protein binding partners[J]. J Endocrinol, 2023, 257: e220184. doi: 10.1530/JOE-22-0184.
[12]Wu T, Zhang X-P, Zhang Q, et al. Gasdermine mediated pyroptosisa novel mechanism regulating migration, invasion and release of inflammatory cytokines in rheumatoid arthritis fibroblast-like synoviocytes[J]. Front Cell Dev Biol, 2022, 9: 810635. doi: 10.3389/fcell.2021.810635.
[13]赵紫琴,徐瑾,王瑞琳,等. 类风湿性关节炎滑膜组织中NLRP3炎性小体及下游因子IL-1β/IL-18的表达及意义[J]. 临床与实验病理学杂志,2019, 35:534-538.
[14]卢珊, 张冰清, 叶菜英, 等. GSDMD-N和p-MLKL蛋白在类风湿关节炎滑膜组织中上调[J]. 基础医学与临床, 2022, 42: 560-564.
[15]Duong BH, Onizawa M, Oses-Prieto JA, et al. A20 restricts ubiquitination of pro-interleukin-1β protein complexes and suppresses NLRP3 inflammasome activity[J]. Immunity, 2015, 42:55-67.

siRNA沉默锌指蛋白A20基因促进人类风湿关节炎成纤维细胞样滑膜细胞焦亡

Zinc finger protein A20-targeting siRNA promotes pyroptosis of human rheumatoid arthritis fibroblast-like synoviocytes

PDF

可视化

摘要/Abstract

引用本文

使用本文

参考文献

相关文章 13

编辑推荐

Metrics

本文评价

[1]	高源, 郑刚, 齐靖, 张凤. NLRP3炎性小体在心脏病发病中的作用研究进展[J]. 基础医学与临床, 2023, 43(7): 1162-1166.
[2]	录亚鹏, 谢建琴. NLRP3炎性小体在缺血再灌注损伤治疗中作用的研究进展[J]. 基础医学与临床, 2023, 43(4): 706-710.
[3]	代志新, 王玉敏. NLRP3炎性小体在高尿酸血症肾病中作用的研究进展[J]. 基础医学与临床, 2023, 43(2): 322-326.
[4]	陈才伟, 吴月平, 王转锁, 罗强, 邢博真. 大豆苷元减轻高糖诱导的肾小管上皮细胞焦亡[J]. 基础医学与临床, 2023, 43(12): 1801-1807.
[5]	卢珊, 张冰清, 叶菜英, 朱蕾. GSDMD-N和p-MLKL蛋白在类风湿关节炎滑膜组织中上调[J]. 基础医学与临床, 2022, 42(4): 560-564.
[6]	刘新兵, 张美红. 钩吻碱通过下调circ_001680抑制类风湿关节炎滑膜成纤维细胞增殖和侵袭[J]. 基础医学与临床, 2022, 42(3): 429-435.
[7]	刘帆, 苏思, 王涛, 袁勃, 马超. 敲除背根神经节Fcgr1减弱类风湿关节炎模型大鼠NF-κB/NLRP3通路活化[J]. 基础医学与临床, 2021, 41(7): 963-969.
[8]	郭艳芹, 殷博凯, 张娟, 何治. NLRP3炎性小体在脑缺血再灌注中的作用[J]. 基础医学与临床, 2021, 41(1): 120-124.
[9]	周永婷, 叶菜英, 朱蕾. NLRP3炎性小体激活调控机制及抑制剂研究新进展[J]. 基础医学与临床, 2020, 40(8): 1113-1118.
[10]	朱坤, 戴日蕾, 朱文婷, 李贞燕, 曹春梅. 细胞焦亡与心血管疾病研究进展[J]. 基础医学与临床, 2020, 40(12): 1711-1715.
[11]	郭雄飞, 王挺, 汤立新. miR-29a对类风湿关节炎成纤维样滑膜细胞增殖和凋亡的影响[J]. 基础医学与临床, 2020, 40(1): 9-15.
[12]	黄晨恺甘达凯张望罗方云陈江汪安江李弼民朱萱. 熊果酸对肝纤维化大鼠NOX2/ROS/NLRP3炎性小体活化的影响[J]. 基础医学与临床, 2018, 38(4): 485-491.
[13]	吴燕升高建东. 细胞焦亡在肾脏炎性反应中的作用研究进展[J]. 基础医学与临床, 2017, 37(10): 1470-1473.