Myeloid Deletion of Cdc42 Protects Liver From Hepatic Ischemia-Reperfusion Injury via Inhibiting Macrophage-Mediated Inflammation in Mice

IF 7.1 1区医学 Q1 GASTROENTEROLOGY & HEPATOLOGY

Cellular and Molecular Gastroenterology and Hepatology Pub Date : 2024-01-01 DOI:10.1016/j.jcmgh.2024.01.023

Jing He , Meng-Yu Tang , Li-Xin Liu , Chen-Xian Kong , Wen Chen , Lu Wang , Shao-Bin Zhi , Hong-Wei Sun , Yu-Chun Huang , Guo-Yu Chen , Hong-Bo Xin , Ke-Yu Deng

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Abstract

Background & Aims

Hepatic ischemia-reperfusion injury (HIRI) often occurs in liver surgery, such as partial hepatectomy and liver transplantation, in which myeloid macrophage-mediated inflammation plays a critical role. Cell division cycle 42 (Cdc42) regulates cell migration, cytoskeleton rearrangement, and cell polarity. In this study, we explore the role of myeloid Cdc42 in HIRI.

Methods

Mouse HIRI models were established with 1-hour ischemia followed by 12-hour reperfusion in myeloid Cdc42 knockout (Cdc42^mye) and Cdc42^flox mice. Myeloid-derived macrophages were traced with Rosa^mTmG fluorescent reporter under LyzCre-mediated excision. The experiments for serum or hepatic enzymic activities, histologic and immunologic analysis, gene expressions, flow cytometry analysis, and cytokine antibody array were performed.

Results

Myeloid deletion of Cdc42 significantly alleviated hepatic damages with the reduction of hepatic necrosis and inflammation, and reserved hepatic functions following HIRI in mice. Myeloid Cdc42 deficiency suppressed the infiltration of myeloid macrophages, reduced the secretion of proinflammatory cytokines, restrained M1 polarization, and promoted M2 polarization of myeloid macrophages in livers. In addition, inactivation of Cdc42 promoted M2 polarization via suppressing the phosphorylation of STAT1 and promoting phosphorylation of STAT3 and STAT6 in myeloid macrophages. Furthermore, pretreatment with Cdc42 inhibitor, ML141, also protected mice from hepatic ischemia-reperfusion injury.

Conclusions

Inhibition or deletion of myeloid Cdc42 protects liver from HIRI via restraining the infiltration of myeloid macrophages, suppressing proinflammatory response, and promoting M2 polarization in macrophages.

Abstract Image

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通过抑制巨噬细胞介导的炎症，髓质删除 Cdc42 可保护小鼠肝脏免受肝缺血再灌注损伤。

背景与目的：肝脏缺血再灌注损伤（HIRI）常发生在肝部分切除术和肝移植等肝脏手术中，髓系巨噬细胞介导的炎症在其中起着关键作用。细胞分裂周期 42（Cdc42）调控细胞迁移、细胞骨架重排和细胞极性。在本研究中，我们旨在探讨髓系 Cdc42 在 HIRI 中的作用：方法：在髓系 Cdc42 基因敲除小鼠（Cdc42mye）和 Cdc42flox 小鼠中建立缺血 1 小时、再灌注 12 小时的小鼠 HIRI 模型。在 LyzCre 介导的切除下，使用 RosamTmG 荧光报告物追踪髓源性巨噬细胞。进行了血清或肝酶活性、组织学和免疫学分析、基因表达、流式细胞术分析和细胞因子抗体阵列实验：结果：髓样细胞缺失 Cdc42 能明显减轻肝损伤，减少肝坏死和炎症，并保留小鼠 HIRI 后的肝功能。髓系 Cdc42 的缺失抑制了髓系巨噬细胞的浸润，减少了促炎细胞因子的分泌，抑制了肝脏中髓系巨噬细胞的 M1 极化，促进了 M2 极化。此外，Cdc42 失活还能通过抑制 STAT1 的磷酸化、促进 STAT3 和 STAT6 的磷酸化来促进骨髓巨噬细胞的 M2 极化。此外，预处理 Cdc42 抑制剂 ML141 还能保护小鼠免受肝缺血再灌注损伤：结论：通过抑制髓系巨噬细胞的浸润、抑制促炎反应和促进巨噬细胞的 M2 极化，抑制或删除髓系 Cdc42 可保护肝脏免受肝缺血再灌注损伤。

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

Cellular and Molecular Gastroenterology and Hepatology Medicine-Gastroenterology

CiteScore

13.00

自引率

2.80%

发文量

246

审稿时长

42 days

期刊介绍： "Cell and Molecular Gastroenterology and Hepatology (CMGH)" is a journal dedicated to advancing the understanding of digestive biology through impactful research that spans the spectrum of normal gastrointestinal, hepatic, and pancreatic functions, as well as their pathologies. The journal's mission is to publish high-quality, hypothesis-driven studies that offer mechanistic novelty and are methodologically robust, covering a wide range of themes in gastroenterology, hepatology, and pancreatology. CMGH reports on the latest scientific advances in cell biology, immunology, physiology, microbiology, genetics, and neurobiology related to gastrointestinal, hepatobiliary, and pancreatic health and disease. The research published in CMGH is designed to address significant questions in the field, utilizing a variety of experimental approaches, including in vitro models, patient-derived tissues or cells, and animal models. This multifaceted approach enables the journal to contribute to both fundamental discoveries and their translation into clinical applications, ultimately aiming to improve patient care and treatment outcomes in digestive health.