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脂肪酶和低密度脂蛋白受体相关蛋白在富含甘油三酯脂蛋白分解代谢中的作用。

The role of lipases and LRP in the catabolism of triglyceride-rich lipoproteins.

作者信息

Beisiegel U, Krapp A, Weber W, Olivecrona G, Gliemann J

机构信息

Medical Clinic, University Hospital Hamburg, Germany.

出版信息

Z Gastroenterol. 1996 Jun;34 Suppl 3:108-9.

PMID:8767481
Abstract

A strong candidate for the long searched CR receptor might be the a2MR/LRP. We oversee a whole series of in vitro experiments from different laboratories today which show that LRP expresses all features for being such a receptor protein. LRP is localized on the liver cell surface, as well as on most other animal cells. It recognizes apo E enriched lipoproteins, as beta-VLDL and CR. There is evidence that CR contains LPL and it has been demonstrated that LPL binds with high affinity to LRP. This has been shown in cell binding experiments with subsequent cross-linking and in direct binding assays on purified receptor protein. HL which is expressed in liver cells and localized at the liver cell surface is also able to bind to LRP. LRP is moreover found in endosomes and can mediate the uptake of beta-VLDL and CR. Further studies are necessary to evaluate its role in vivo as well as its regulation. The interplay between the different ligands of this large multifunctional receptor protein needs to be clarified. It should be emphasized here that by describing LPL as a new mediator of CR untake in the liver and providing evidence for an interaction between LPL and LRP the role of LRP in the remnant catabolism has become even more likely.

摘要

长期以来一直在寻找的CR受体的一个有力候选者可能是α2MR/LRP。我们今天监督了来自不同实验室的一系列体外实验,这些实验表明LRP具备作为这种受体蛋白的所有特征。LRP定位于肝细胞表面以及大多数其他动物细胞表面。它能识别富含载脂蛋白E的脂蛋白,如β-VLDL和CR。有证据表明CR含有LPL,并且已经证明LPL与LRP具有高亲和力结合。这已在后续交联的细胞结合实验以及对纯化受体蛋白的直接结合测定中得到证实。在肝细胞中表达并定位于肝细胞表面的HL也能够与LRP结合。此外,LRP存在于内体中,并能介导β-VLDL和CR的摄取。需要进一步研究以评估其在体内的作用及其调节。这种大型多功能受体蛋白的不同配体之间的相互作用需要阐明。这里应该强调的是,通过将LPL描述为肝脏中CR摄取的新介质,并提供LPL与LRP之间相互作用的证据,LRP在残余物分解代谢中的作用变得更加可能。

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