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钙网蛋白在体外作为糖基化和非糖基化蛋白质的分子伴侣发挥作用。

Calreticulin functions in vitro as a molecular chaperone for both glycosylated and non-glycosylated proteins.

作者信息

Saito Y, Ihara Y, Leach M R, Cohen-Doyle M F, Williams D B

机构信息

Department of Biochemistry, Medical Sciences Building, University of Toronto, Toronto, Ontario, Canada M5S 1A8.

出版信息

EMBO J. 1999 Dec 1;18(23):6718-29. doi: 10.1093/emboj/18.23.6718.

Abstract

Calreticulin (CRT) is thought to be a molecular chaperone that interacts with glycoproteins exclusively through a lectin site specific for monoglucosylated oligosaccharides. However, this chaperone function has never been directly demonstrated nor is it clear how lectin-oligosaccharide interactions facilitate glycoprotein folding. Using purified components, we show that CRT suppresses the aggregation not only of a glycoprotein bearing monoglucosylated oligosaccharides but also that of non-glycosylated proteins. Furthermore, CRT forms stable complexes with unfolded, non-glycosylated substrates but does not associate with native proteins. ATP and Zn(2+) enhance CRT's ability to suppress aggregation of non- glycoproteins, whereas engagement of its lectin site with purified oligosaccharide attenuates this function. CRT also confers protection against thermal inactivation and maintains substrates in a folding-competent state. We conclude that in addition to being a lectin CRT possesses a polypeptide binding capacity capable of discriminating between protein conformational states and that it functions in vitro as a classical molecular chaperone.

摘要

钙网蛋白(CRT)被认为是一种分子伴侣,它仅通过对单糖基化寡糖具有特异性的凝集素位点与糖蛋白相互作用。然而,这种伴侣功能从未得到直接证明,凝集素-寡糖相互作用如何促进糖蛋白折叠也不清楚。我们使用纯化的组分表明,CRT不仅能抑制带有单糖基化寡糖的糖蛋白的聚集,还能抑制非糖基化蛋白的聚集。此外,CRT与未折叠的非糖基化底物形成稳定的复合物,但不与天然蛋白结合。ATP和Zn(2+)增强了CRT抑制非糖蛋白聚集的能力,而其凝集素位点与纯化寡糖的结合则减弱了该功能。CRT还能提供抗热失活保护,并使底物保持在折叠能力状态。我们得出结论,除了作为一种凝集素外,CRT还具有能够区分蛋白质构象状态的多肽结合能力,并且它在体外作为一种经典的分子伴侣发挥作用。

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