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潜伏转化生长因子-β:结构特征与激活机制

Latent transforming growth factor-beta: structural features and mechanisms of activation.

作者信息

Munger J S, Harpel J G, Gleizes P E, Mazzieri R, Nunes I, Rifkin D B

机构信息

Department of Cell Biology, New York University, New York, USA.

出版信息

Kidney Int. 1997 May;51(5):1376-82. doi: 10.1038/ki.1997.188.

Abstract

Transforming growth factor-beta are cytokines with a wide range of biological effects. They play a pathologic role in inflammatory and fibrosing diseases such as nephrosclerosis. TGF-beta s are secreted in a latent form due to noncovalent association with latency associated peptide (LAP), which is a homodimer formed from the propeptide region of TGF-beta. LAP is disulfide linked to another protein, latent TGF-beta binding protein (LTBP). LTBP has features in common with extracellular matrix proteins, and targets latent TGF-beta to the matrix. Activation of latent TGF-beta can be accomplished in vitro by denaturing treatments, plasmin digestion, ionizing radiation and interaction with thrombospondin. The mechanisms by which latent TGF-beta is activated physiologically are not well understood. Results to date suggest an important role for proteases, particularly plasmin, although other mechanisms probably exist. A general model of activation is proposed in which latent TGF-beta is released from the extracellular matrix by proteases, localized to cell surfaces, and activated by cell-associated plasmin.

摘要

转化生长因子-β是一类具有广泛生物学效应的细胞因子。它们在诸如肾硬化等炎症性和纤维化疾病中发挥病理作用。由于与潜伏相关肽(LAP)非共价结合,转化生长因子-β以潜伏形式分泌,LAP是由转化生长因子-β前肽区域形成的同二聚体。LAP通过二硫键与另一种蛋白质——潜伏转化生长因子-β结合蛋白(LTBP)相连。LTBP具有与细胞外基质蛋白相同的特征,并将潜伏转化生长因子-β靶向到基质中。潜伏转化生长因子-β的激活在体外可通过变性处理、纤溶酶消化、电离辐射以及与血小板反应蛋白相互作用来实现。潜伏转化生长因子-β在生理条件下被激活的机制尚不清楚。迄今为止的结果表明蛋白酶,尤其是纤溶酶起重要作用,不过可能还存在其他机制。本文提出了一个通用的激活模型,即潜伏转化生长因子-β通过蛋白酶从细胞外基质中释放出来,定位到细胞表面,并被细胞相关的纤溶酶激活。

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