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由多嗜性弗氏貂细胞集落形成病毒的糖蛋白70和嗜亲性弗氏鼠白血病病毒的糖蛋白71中的结构元件,通过二硫键模式和有限蛋白酶解来定义。

Structural elements in glycoprotein 70 from polytropic Friend mink cell focus-inducing virus and glycoprotein 71 from ecotropic Friend murine leukemia virus, as defined by disulfide-bonding pattern and limited proteolysis.

作者信息

Linder M, Wenzel V, Linder D, Stirm S

机构信息

Biochemisches Institut am Klinikum, Justus-Liebig-Universität, Giessen, Germany.

出版信息

J Virol. 1994 Aug;68(8):5133-41. doi: 10.1128/JVI.68.8.5133-5141.1994.

DOI:10.1128/JVI.68.8.5133-5141.1994
PMID:8035513
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC236457/
Abstract

The disulfide-bonding pattern of glycoprotein 70 (gp70), the surface glycoprotein (SU) encoded by the envelope gene of polytropic Friend milk cell focus-inducing virus, was elucidated and compared with that of glycoprotein 71 (gp71), the corresponding glycoprotein of the ecotropic Friend murine leukemia virus, which had previously been determined (M. Linder, D. Linder, J. Hahnen, H.-H. Schott, and Stirm, Eur. J. Biochem. 203:65-73, 1992). In the carboxy-terminal constant domain, in which these glycoproteins have about 97% sequence homology, the location of the four disulfide bonds was found to be analogous. In the amino-terminal differential domain, with about 37% sequence homology, 8 of the 12 cysteine residues of the ecotropic SU are conserved in the polytropic SU. In this domain, a similar clustering of disulfide bonds was detected, which led to the identification of three distinct disulfide-bonded regions in both glycoproteins. However, because of deletions and sequence deviations, the glycoproteins must have significantly different three-dimensional structures in these regions. Since the receptor-binding functions of both glycoproteins have been attributed to their amino-terminal domains and since each binds to a different receptor, these disulfide-bonded structures are likely candidates for receptor-binding functions. Limited proteolysis of both glycoproteins with various endoproteinases led to the identification of preferential proteolytic sites between disulfide-bonded regions, at the beginning of the hypervariable proline-rich region, and between differential and constant domains, further confirming the structural organization of the folded glycoproteins.

摘要

多嗜性弗氏乳细胞病灶诱导病毒包膜基因编码的表面糖蛋白(SU)即糖蛋白70(gp70)的二硫键连接模式已得到阐明,并与亲嗜性弗氏小鼠白血病病毒相应的糖蛋白糖蛋白71(gp71)的二硫键连接模式进行了比较,后者的二硫键连接模式先前已确定(M. 林德、D. 林德、J. 哈嫩、H.-H. 肖特和施蒂姆,《欧洲生物化学杂志》203:65 - 73,1992年)。在这些糖蛋白具有约97%序列同源性的羧基末端恒定结构域中,发现四个二硫键的位置是类似的。在序列同源性约为37%的氨基末端差异结构域中,亲嗜性SU的12个半胱氨酸残基中有8个在多嗜性SU中保守。在该结构域中,检测到二硫键有类似的聚集情况,这使得在两种糖蛋白中都鉴定出三个不同的二硫键连接区域。然而,由于缺失和序列偏差,这些糖蛋白在这些区域必定具有显著不同的三维结构。由于两种糖蛋白的受体结合功能都归因于它们的氨基末端结构域,并且由于每种糖蛋白都与不同的受体结合,这些二硫键连接结构很可能是受体结合功能的候选结构。用各种内肽酶对两种糖蛋白进行有限的蛋白酶解,导致在二硫键连接区域之间、富含脯氨酸的高变区起始处以及差异结构域和恒定结构域之间鉴定出优先的蛋白水解位点,进一步证实了折叠糖蛋白的结构组织。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f17b/236457/e1959b666bad/jvirol00017-0444-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f17b/236457/e1959b666bad/jvirol00017-0444-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f17b/236457/e1959b666bad/jvirol00017-0444-a.jpg

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