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Assessment of proteolytic degradation of the basement membrane: a fragment of type IV collagen as a biochemical marker for liver fibrosis

机译:评估基膜的蛋白水解降解:IV型胶原蛋白片段作为肝纤维化的生化标记

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摘要

BackgroundCollagen deposition and an altered matrix metalloproteinase (MMP) expression profile are hallmarks of fibrosis. Type IV collagen is the most abundant structural basement membrane component of tissue, which increases 14-fold during fibrogenesis in the liver. Proteolytic degradation of collagens by proteases produces small fragments, so-called neoepitopes, which are released systemically. Technologies investigating MMP-generated fragments of collagens may provide more useful information than traditional serological assays that crudely measure total protein. In the present study, we developed an ELISA for the quantification of a neoepitope generated by MMP degradation of type IV collagen and evaluated the association of this neoepitope with liver fibrosis in two animal models.
机译:背景胶原沉积和基质金属蛋白酶(MMP)表达谱的改变是纤维化的标志。 IV型胶原蛋白是组织中最丰富的结构基底膜成分,在肝纤维化过程中增加14倍。蛋白酶通过胶原蛋白对胶原蛋白的降解作用会产生小片段,即所谓的新表位,这些片段会全身释放。研究MMP生成的胶原蛋白片段的技术可能比粗略测量总蛋白的传统血清学检测方法提供更多有用的信息。在本研究中,我们开发了一种ELISA用于定量IV型胶原蛋白MMP降解产生的新表位,并在两种动物模型中评估了该新表位与肝纤维化的关系。

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