HMGB1/STAT3/p65 轴驱动微胶质细胞活化,自噬在慢性应激诱导的重度抑郁症中发挥关键作用

IF 11.4 1区 综合性期刊 Q1 MULTIDISCIPLINARY SCIENCES
Ke Xu , Mingyang Wang , Haiyang Wang , Shuang Zhao , Dianji Tu , Xue Gong , Wenxia Li , Xiaolei Liu , Lianmei Zhong , Jianjun Chen , Peng Xie
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引用次数: 0

摘要

引言神经炎症和自噬与应激相关的重度抑郁障碍(MDD)有关,但其潜在的分子机制在很大程度上仍然未知。方法利用生物信息学分析重新分析了男性 MDD 患者死后背外侧前额叶皮层(dlPFC)的转录组数据。在 MDD 临床患者和慢性社会挫败应激(CSDS)诱导的抑郁模型小鼠中探讨了 HMGB1 的表达水平及其与抑郁症状的相关性。结果 MDD 患者的不同基因表达与 HMGB1/STAT3/p65 轴调控的小胶质细胞活化和自噬有关。MDD 患者血清 HMGB1 水平升高,并与症状严重程度呈正相关。CSDS 不仅能诱导小鼠出现类似抑郁症的状态,还能增强小胶质细胞的反应性、自噬以及 mPFC 中 HMGB1/STAT3/p65 轴的激活。HMGB1 的表达水平主要在 CSDS 易感小鼠的小胶质细胞中升高,这也与抑郁样行为相关。特异性敲除HMGB1可产生抗抑郁表型,并抑制CSDS诱导的相关小胶质细胞激活和自噬效应。外源给予rHMGB1或特异性过表达HMGB1可模拟CSDS诱导的效应,而STAT3抑制剂或p65敲除可阻断这些效应。在体外,抑制 HMGB1/STAT3/p65 轴可防止脂多糖诱导的小胶质细胞活化和自噬,而 rHMGB1 则可逆转这些变化。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

HMGB1/STAT3/p65 axis drives microglial activation and autophagy exert a crucial role in chronic Stress-Induced major depressive disorder

HMGB1/STAT3/p65 axis drives microglial activation and autophagy exert a crucial role in chronic Stress-Induced major depressive disorder

Introduction

Neuroinflammation and autophagy are implicated in stress-related major depressive disorder (MDD), but the underlying molecular mechanisms remain largely unknown.

Objectives

Here, we identified that MDD regulated by HMGB1/STAT3/p65 axis mediated microglial activation and autophagy for the first time. Further investigations were performed to uncover the effects of this axis on MDD in vivo and in vitro.

Methods

Bioinformatics analyses were used to re-analysis the transcriptome data from the dorsolateral prefrontal cortex (dlPFC) of post-mortem male MDD patients. The expression level of HMGB1 and its correlation with depression symptoms were explored in MDD clinical patients and chronic social defeat stress (CSDS)-induced depression model mice. Specific adeno-associated virus and recombinant (r)HMGB1 injection into the medial PFC (mPFC) of mice, and pharmacological inhibitors with rHMGB1 in two microglial cell lines exposed to lipopolysaccharide were used to analyze the effects of HMGB1/STAT3/p65 axis on MDD.

Results

The differential expression of genes from MDD patients implicated in microglial activation and autophagy regulated by HMGB1/STAT3/p65 axis. Serum HMGB1 level was elevated in MDD patients and positively correlated with symptom severity. CSDS not only induced depression-like states in mice, but also enhanced microglial reactivity, autophagy as well as activation of the HMGB1/STAT3/p65 axis in mPFC. The expression level of HMGB1 was mainly increased in the microglial cells of CSDS-susceptible mice, which also correlated with depressive-like behaviors. Specific HMGB1 knockdown produced a depression-resilient phenotype and suppressed the associated microglial activation and autophagy effects of CSDS-induced. The effects induced by CSDS were mimicked by exogenous administration of rHMGB1 or specific overexpression of HMGB1, while blocked by STAT3 inhibitor or p65 knockdown. In vitro, inhibition of HMGB1/STAT3/p65 axis prevented lipopolysaccharide-induced microglial activation and autophagy, while rHMGB1 reversed these changes.

Conclusion

Our study established the role of microglial HMGB1/STAT3/p65 axis in mPFC in mediating microglial activation and autophagy in MDD.

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来源期刊
Journal of Advanced Research
Journal of Advanced Research Multidisciplinary-Multidisciplinary
CiteScore
21.60
自引率
0.90%
发文量
280
审稿时长
12 weeks
期刊介绍: Journal of Advanced Research (J. Adv. Res.) is an applied/natural sciences, peer-reviewed journal that focuses on interdisciplinary research. The journal aims to contribute to applied research and knowledge worldwide through the publication of original and high-quality research articles in the fields of Medicine, Pharmaceutical Sciences, Dentistry, Physical Therapy, Veterinary Medicine, and Basic and Biological Sciences. The following abstracting and indexing services cover the Journal of Advanced Research: PubMed/Medline, Essential Science Indicators, Web of Science, Scopus, PubMed Central, PubMed, Science Citation Index Expanded, Directory of Open Access Journals (DOAJ), and INSPEC.
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