S1PR2/RhoA/ROCK1通路通过诱导肠血管内皮屏障损伤和M1巨噬细胞极化促进炎症性肠病,BIOCHEMICAL PHARMACOLOGY

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S1PR2/RhoA/ROCK1通路通过诱导肠血管内皮屏障损伤和M1巨噬细胞极化促进炎症性肠病
BIOCHEMICAL PHARMACOLOGY ( IF 5.3 ) Pub Date : 2022-05-10 , DOI: 10.1016/j.bcp.2022.115077
Xuewen Wang ₁ , Shuhua Chen ₂ , Hong Xiang ₃ , Xiaoyan Wang ₄ , Jie Xiao ₅ , Shaoli Zhao ₆ , Zhihao Shu ₁ , Jie Ouyang ₁ , Ziwei Liang ₇ , Minzi Deng ₄ , Xuejie Chen ₄ , Jing Zhang ₁ , Huiqin Liu ₁ , Qisheng Quan ₁ , Peng Gao ₁ , Jianing Fan ₁ , Alex F Chen ₈ , Hongwei Lu ₉

Affiliation

Health Management Center, The Third Xiangya Hospital of Central South University, Changsha, China; Department of Cardiology, The Third Xiangya Hospital of Central South University, Changsha, China.
Department of Biochemistry, School of Life Sciences of Central South University, Changsha, China.
Center for Experimental Medicine, The Third Xiangya Hospital of Central South University, Changsha, China.
Department of Gastroenterology, The Third Xiangya Hospital of Central South University, Changsha, China.
Department of Emergency, The Third Xiangya Hospital of Central South University, Changsha, China.
Department of Endocrinology, The Third Xiangya Hospital of Central South University, Changsha, China.
Department of Clinical Laboratory, Yueyang People's Hospital, Yueyang, China.
Department of Surgery, University of Pittsburgh School of Medicine, Pittsburgh, PA, USA.
Health Management Center, The Third Xiangya Hospital of Central South University, Changsha, China; Department of Cardiology, The Third Xiangya Hospital of Central South University, Changsha, China; Center for Experimental Medicine, The Third Xiangya Hospital of Central South University, Changsha, China.

血管和免疫功能障碍被认为与炎症性肠病（IBD）的发病机制有关，但在此背后，黏膜血管内皮屏障功能障碍和巨噬细胞表型转变的确切机制尚不完全清楚。在这里，我们探讨了鞘氨醇 1-磷酸受体 2 (S1PR2) 及其下游 G 蛋白 RhoA/Rho 激酶 1 (ROCK1) 信号通路在 IBD 中肠内皮屏障损伤和 M1 巨噬细胞极化中的机制作用。我们发现 S1PR2 在 IBD 患者和 DSS 诱导的结肠炎小鼠的肠粘膜血管内皮细胞和巨噬细胞以及 LPS体外处理的血管内皮细胞和巨噬细胞中的表达显着增加。敲除或药理学抑制 S1PR2 可显着下调血管内皮细胞和巨噬细胞中 RhoA 和 ROCK1 的表达。此外，抑制 S1PR2 和 ROCK1在体内和体外逆转了受损的血管屏障功能和 M1 巨噬细胞极化，同时减少了血管内皮细胞中的 ER 应激和巨噬细胞中的糖酵解。此外，抑制 ER 应激或糖酵解可逆转 LPS 诱导的血管内皮细胞屏障功能损伤和 M1 巨噬细胞极化。总之，我们的研究结果表明，S1PR2/RhoA/ROCK1 信号通路可能通过调节血管内皮屏障功能和 M1 巨噬细胞极化参与 IBD 的发病机制。

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S1PR2/RhoA/ROCK1 pathway promotes inflammatory bowel disease by inducing intestinal vascular endothelial barrier damage and M1 macrophage polarization

Vascular and immune dysfunctions are thought to be related to the pathogenesis of inflammatory bowel disease (IBD), but behind this, the exact mechanism of mucosal vascular endothelial barrier dysfunction and macrophage phenotypic transition is not fully understood. Here, we explored the mechanistic role of sphingosine 1-phosphate receptor 2 (S1PR2) and its downstream G protein RhoA/Rho kinase 1 (ROCK1) signaling pathway in the intestinal endothelial barrier damage and M1 macrophage polarization in IBD. We found that the expression of S1PR2 in intestinal mucosal vascular endothelial cells and macrophages of IBD patients and DSS-induced colitis mice as well as vascular endothelial cells and macrophages treated with LPS in vitro was significantly increased. Knocking down or pharmacologically inhibiting S1PR2 significantly downregulated the expression of RhoA and ROCK1 in vascular endothelial cells and macrophages. Furthermore, inhibition of S1PR2 and ROCK1 reversed the impaired vascular barrier function and M1 macrophage polarization in vivo and in vitro, while reducing ER stress in vascular endothelial cells and glycolysis in macrophages. In addition, inhibition of ER stress or glycolysis reversed LPS-induced impairment of vascular endothelial cell barrier function and M1 macrophage polarization. Collectively, our results indicate that the S1PR2/RhoA/ROCK1 signaling pathway may participate in the pathogenesis of IBD by regulating vascular endothelial barrier function and M1 macrophage polarization.

更新日期：2022-05-10

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