一种MHVR/mph嵌合体以及N端结构域缺乏N-连接糖基化的MHVR突变体的小鼠肝炎病毒受体活性。
Mouse hepatitis virus receptor activities of an MHVR/mph chimera and MHVR mutants lacking N-linked glycosylation of the N-terminal domain.
作者信息
Dveksler G S, Basile A A, Cardellichio C B, Holmes K V
机构信息
Department of Pathology, Uniformed Services University of the Health Sciences, Bethesda, Maryland 20814-4799.
出版信息
J Virol. 1995 Jan;69(1):543-6. doi: 10.1128/JVI.69.1.543-546.1995.
Abstract
Mouse hepatitis virus binds to the N-terminal domain of its receptor, MHVR, a murine biliary glycoprotein with four immunoglobulin-like domains (G.S. Dveksler, M. N. Pensiero, C. W. Dieffenbach, C. B. Cardellichio, A.A. Basile, P.E. Elia, and K. V. Holmes, Proc. Natl. Acad. Sci. USA 90:1716-1720, 1993). A recombinant protein with only the anchored N-terminal domain was not a functional receptor, but a recombinant protein with the N-terminal domain of MHVR linked to the second and third immunoglobulin-like domains and anchor from the mouse poliovirus receptor homolog, mph, was a functional receptor for mouse hepatitis virus. The native four-domain MHVR has 16 potential N-linked glycosylation sites, including three on the N-terminal domain. Recombinant proteins lacking each one of these three sites or all three of them were functional receptors. Thus, glycosylation of the N-terminal domain is not required, but a glycoprotein longer than the N-terminal domain is required for virus receptor activity.
摘要
小鼠肝炎病毒与其受体MHVR的N端结构域结合,MHVR是一种具有四个免疫球蛋白样结构域的鼠胆汁糖蛋白(G.S. 德夫克斯勒、M.N. 彭西埃罗、C.W. 迪芬巴赫、C.B. 卡德利乔、A.A. 巴西莱、P.E. 埃利亚和K.V. 霍姆斯,《美国国家科学院院刊》90:1716 - 1720, 1993)。仅具有锚定N端结构域的重组蛋白不是功能性受体,但将MHVR的N端结构域与小鼠脊髓灰质炎病毒受体同源物mph的第二个和第三个免疫球蛋白样结构域及锚定序列相连的重组蛋白是小鼠肝炎病毒的功能性受体。天然的四结构域MHVR有16个潜在的N - 糖基化位点,其中三个在N端结构域上。缺少这三个位点中的任何一个或全部三个位点的重组蛋白都是功能性受体。因此,N端结构域的糖基化不是必需的,但病毒受体活性需要一种比N端结构域更长的糖蛋白。
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