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β2整合素诱导的p38丝裂原活化蛋白激酶激活是肝细胞通过CD14/TLR4/MD2依赖性途径摄取脂多糖的关键介质。

Beta2-integrin-induced p38 MAPK activation is a key mediator in the CD14/TLR4/MD2-dependent uptake of lipopolysaccharide by hepatocytes.

作者信息

Scott Melanie J, Billiar Timothy R

机构信息

Department of Surgery, University of Pittsburgh School of Medicine, Pittsburgh, Pennsylvania 15213, USA.

出版信息

J Biol Chem. 2008 Oct 24;283(43):29433-46. doi: 10.1074/jbc.M803905200. Epub 2008 Aug 13.

Abstract

The liver is the main organ that clears circulating lipopolysaccharide (LPS), and hepatocytes are a major cell type involved in LPS uptake. Little is known about the mechanisms for LPS internalization in hepatocytes and what signaling pathways are involved. We show here that LPS uptake is initiated after formation of a multi-receptor complex within lipid rafts. We find that essential components for LPS uptake are CD14, TLR4, MD2, and the beta2-integrin CD11b/CD18. Activation of p38 MAPK is also essential for the initiation of LPS uptake, and interestingly, we show that this activation is not through TLR4 signaling by MyD88 but through activation of TIRAP via CD11b/CD18. However, TLR4/MD2 remain essential components at the cell surface as part of the LPS receptor complex. We therefore suggest novel roles for TLR4/MD2, CD11b/CD18, TIRAP, and p38 MAPK in LPS uptake by hepatocytes.

摘要

肝脏是清除循环中脂多糖(LPS)的主要器官,肝细胞是参与LPS摄取的主要细胞类型。目前对于肝细胞中LPS内化的机制以及涉及哪些信号通路知之甚少。我们在此表明,LPS摄取在脂筏内形成多受体复合物后启动。我们发现LPS摄取的必需成分是CD14、TLR4、MD2和β2整合素CD11b/CD18。p38丝裂原活化蛋白激酶(p38 MAPK)的激活对于LPS摄取的启动也至关重要,有趣的是,我们表明这种激活不是通过髓样分化因子88(MyD88)介导的TLR4信号通路,而是通过CD11b/CD18激活TIR结构域衔接蛋白(TIRAP)。然而,TLR4/MD2作为LPS受体复合物的一部分,仍然是细胞表面的必需成分。因此,我们提出TLR4/MD2、CD11b/CD18、TIRAP和p38 MAPK在肝细胞摄取LPS过程中具有新的作用。

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