Cx43-Delivered miR-181b Negatively Regulates Sirt1/FOXO3a Signalling Pathway-Mediated Apoptosis on Intestinal Injury in Sepsis.

IF 3 3区 医学 Q2 GASTROENTEROLOGY & HEPATOLOGY
Digestion Pub Date : 2023-01-01 Epub Date: 2023-05-25 DOI:10.1159/000529102
Zhaowei Zou, Jianyang Yu, Renli Huang, Jinlong Yu
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引用次数: 0

Abstract

Introduction: Gap junctions can transmit signals between cells, including miRNAs, leading to the amplification of adjacent cell damage. No previous study has addressed gap junctions and miRNAs in sepsis because the internal mechanism of sepsis-induced intestinal injury is complex. Therefore, we studied the relationship between connexin43 (Cx43) and miR-181b and provided a research direction for further study of sepsis.

Methods: A mouse caecal ligation and puncture method was used to construct a mouse sepsis model. Firstly, damage to intestinal tissues at different time points was analysed. The levels of Cx43, miR-181b, Sirt1, and FOXO3a in intestinal tissues and the transcription and translation of the apoptosis-related genes Bim and puma, which are downstream of FOXO3a were analysed. Secondly, the effect of Cx43 levels on miR-181b and Sirt1/FOXO3a signalling pathway activity was explored by using the Cx43 inhibitor heptanol. Finally, luciferase assays were used to determine miR-181b binding to the predicted target sequence.

Results: The results show that during sepsis, intestinal injury becomes increasingly worse with time, and the expression of Cx43 and miR-181b increase. In addition, we found that heptanol could significantly reduce intestinal injury. This finding indicates that inhibiting Cx43 regulates the transfer of miR-181b between adjacent cells, thereby reducing the activity of the Sirt1/FOXO3a signalling pathway and reducing the degree of intestinal injury during sepsis.

Conclusions: In sepsis, the enhancement of Cx43 gap junctions leads to an increase in miR-181b intercellular transfer, affects the downstream SIRT1/FOXO3a signalling pathway and causes cell and tissue damage.

Cx43递送的miR-181b对脓毒症肠损伤中Sirt1/FOXO3a信号通路介导的细胞凋亡负调控。
引言:间隙连接可以在细胞之间传递信号,包括miRNA,导致相邻细胞损伤的放大。以前没有研究涉及败血症中的间隙连接和miRNA,因为败血症诱导的肠道损伤的内部机制很复杂。因此,我们研究了连接蛋白43(Cx43)与miR-181b之间的关系,为进一步研究败血症提供了研究方向。方法:采用小鼠盲肠结扎穿刺法建立小鼠败血症模型。首先,分析了不同时间点对肠道组织的损伤。分析了肠道组织中Cx43、miR-181b、Sirt1和FOXO3a的水平,以及FOXO3a下游的凋亡相关基因Bim和puma的转录和翻译。其次,通过使用Cx43抑制剂庚醇来探索Cx43水平对miR-181b和Sirt1/FOXO3a信号通路活性的影响。最后,使用萤光素酶测定来确定miR-181b与预测的靶序列的结合。结果:研究结果表明,在败血症期间,肠道损伤随着时间的推移变得越来越严重,Cx43和miR-181b的表达增加。此外,我们发现庚醇可以显著减少肠道损伤。这一发现表明,抑制Cx43调节miR-181b在相邻细胞之间的转移,从而降低Sirt1/FOXO3a信号通路的活性,并降低败血症期间肠道损伤的程度。结论:在败血症中,Cx43间隙连接的增强导致miR-181b细胞间转移增加,影响下游SIRT1/FOXO3a信号通路,并导致细胞和组织损伤。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Digestion
Digestion 医学-胃肠肝病学
CiteScore
7.90
自引率
0.00%
发文量
39
审稿时长
6-12 weeks
期刊介绍: ''Digestion'' concentrates on clinical research reports: in addition to editorials and reviews, the journal features sections on Stomach/Esophagus, Bowel, Neuro-Gastroenterology, Liver/Bile, Pancreas, Metabolism/Nutrition and Gastrointestinal Oncology. Papers cover physiology in humans, metabolic studies and clinical work on the etiology, diagnosis, and therapy of human diseases. It is thus especially cut out for gastroenterologists employed in hospitals and outpatient units. Moreover, the journal''s coverage of studies on the metabolism and effects of therapeutic drugs carries considerable value for clinicians and investigators beyond the immediate field of gastroenterology.
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