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miR-223通过FOXO1介导的自噬调节在脓毒症诱导的免疫抑制中的作用

FOXO1-mediated autophagy regulation by miR-223 in sepsis-induced immunosuppression.

作者信息

Xiang Guoan, Li Qi, Lian Di, Su Chengcheng, Li Xin, Deng Shoulong, Xie Lixin

机构信息

College of Pulmonary and Critical Care Medicine, Chinese PLA General Hospital, Beijing, China.

Chinese PLA Medical School, Beijing, China.

出版信息

Front Pharmacol. 2024 Oct 8;15:1469286. doi: 10.3389/fphar.2024.1469286. eCollection 2024.

DOI:10.3389/fphar.2024.1469286
PMID:39439897
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11493625/
Abstract

INTRODUCTION

Immunosuppression is the main cause of the high mortality rate in patients with sepsis. The decrease in the number and dysfunction of CD4 T lymphocytes is crucial to the immunosuppressed state of sepsis, in turn affecting the development and prognosis of sepsis. Autophagy has been shown to play an important role in the immune imbalance exhibited during sepsis.

METHODS

In this study, we modulate the expression of miR-223 in CD4 T lymphocytes, via the transfection of a mimic or an inhibitor of miR-223 to establish cell models of miR-223 overexpression and knockdown, respectively. Levels of autophagy were monitored using a double-labeled lentivirus (mRFP-GFP-LC3) and electron microscopy, and western blot analysis was used to estimate the levels of autophagy-related proteins and FOXO1 in the two cell models after co-treatment with lipopolysaccharide (LPS) and siRNA against FOXO1.

RESULTS

We found that when the expression of miR-223 increased, FOXO1 expression decreased and autophagy decreased; whereas, when FOXO1 expression was inhibited, autophagy decreased significantly in different cell models after LPS induction.

CONCLUSION

Thus, this study proved that miR-223 participate in the regulation of LPS-induced autophagy via the regulation of FOXO1 expression in CD4 T lymphocytes which shed a new light for the diagnosis and treatment of sepsis.

摘要

引言

免疫抑制是脓毒症患者高死亡率的主要原因。CD4 T淋巴细胞数量减少和功能障碍对脓毒症的免疫抑制状态至关重要,进而影响脓毒症的发展和预后。自噬已被证明在脓毒症期间表现出的免疫失衡中起重要作用。

方法

在本研究中,我们通过转染miR-223模拟物或抑制剂来调节CD4 T淋巴细胞中miR-223的表达,分别建立miR-223过表达和敲低的细胞模型。使用双标记慢病毒(mRFP-GFP-LC3)和电子显微镜监测自噬水平,并通过蛋白质印迹分析评估在与脂多糖(LPS)和针对FOXO1的小干扰RNA(siRNA)共同处理后两种细胞模型中自噬相关蛋白和FOXO1的水平。

结果

我们发现,当miR-223表达增加时,FOXO1表达降低且自噬减少;而当FOXO1表达被抑制时,LPS诱导后不同细胞模型中的自噬显著减少。

结论

因此,本研究证明miR-223通过调节CD4 T淋巴细胞中FOXO1的表达参与LPS诱导的自噬调节,这为脓毒症的诊断和治疗提供了新的思路。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0a59/11493625/101109b029db/fphar-15-1469286-g009.jpg
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