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马立克氏病疱疹病毒蛋白酶的连续自动加工与其他疱疹病毒不同。

Sequential autoprocessing of Marek's disease herpesvirus protease differs from that of other herpesviruses.

作者信息

Laurent S, Blondeau C, Belghazi M, Remy S, Esnault E, Rasschaert P, Rasschaert D

机构信息

Equipe Télomérase et Lymphome Viro-induit, UPR INRA 1282 IASP-213, INRA de Tours, 37380 Nouzilly, France.

出版信息

J Virol. 2007 Jun;81(11):6117-21. doi: 10.1128/JVI.02679-06. Epub 2007 Mar 21.

Abstract

Herpesviruses encode a unique serine protease essential for viral capsid maturation. This protease undergoes autoprocessing at two sites, R and M, at the consensus sequence (V, L, I)(P3)-X(P2)-A(P1)/S(P1') (where X is a polar amino acid). We observed complete autoprocessing at the R and M sites of Marek's disease virus (MDV) protease following production of the polyprotein in Escherichia coli. Site-directed mutagenesis confirmed the predicted sequence of the R and M sites, with the M site sequence being nonconsensual: M(P3)-N(P2)-A(P1)/S(P1'). Mutagenesis and expression kinetics studies suggested that the atypical MDV M site was cleaved exclusively by the processed short protease, a feature making MDV unique among herpesviruses.

摘要

疱疹病毒编码一种对病毒衣壳成熟至关重要的独特丝氨酸蛋白酶。这种蛋白酶在两个位点R和M处进行自我切割,切割位点的共有序列为(V, L, I)(P3)-X(P2)-A(P1)/S(P1')(其中X是极性氨基酸)。在大肠杆菌中产生多聚蛋白后,我们观察到马立克氏病病毒(MDV)蛋白酶的R和M位点发生了完全的自我切割。定点诱变证实了R和M位点的预测序列,其中M位点序列不符合共有序列:M(P3)-N(P2)-A(P1)/S(P1')。诱变和表达动力学研究表明,非典型的MDV M位点仅由加工后的短蛋白酶切割,这一特征使MDV在疱疹病毒中独一无二。

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