Three dimensional structure of human cytomegalovirus protease

被引：144

作者：

Shieh, HS

Kurumbail, RG

Stevens, AM

Stegeman, RA

Sturman, EJ

Pak, JY

Wittwer, AJ

Palmier, MO

Wiegand, RC

Holwerda, BC

Stallings, WC

机构：

[1] MONSANTO SEARLE,SEARLE DISCOVERY RES,DEPT INFECT DIS,ST LOUIS,MO 63198

[2] MONSANTO SEARLE,SEARLE DISCOVERY RES,DEPT BIOL SCI,ST LOUIS,MO 63198

来源：

NATURE | 1996年 / 383卷 / 6597期

关键词：

D O I：

10.1038/383279a0

中图分类号：

O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];

学科分类号：

07 ; 0710 ; 09 ;

摘要：

HERPESVIRUSES encode a serine protease(1,2) that specifically cleaves assembly protein(3). This protease is critical for replication(4), and represents a new target for antiviral drug design(5). Here we report the three-dimensional structure of the protease from human cytomegalovirus (hCMV) at 2.27 Angstrom resolution. The structure reveals a unique fold and new catalytic strategy for cleavage. The monomer fold of the enzyme, a seven-stranded beta-barrel encircled by a chain of helices that form the carboxy terminus of the molecule, is unrelated to those observed in classic serine proteases such as chymotrypsin and subtilisin. The serine nucleophile at position 132 is activated by two juxtaposed histidine residues at positions 63 and 157. Dimerization, which seems to be necessary for activity(6,7), is observed in the crystals. Correlations of the structure with the sequences of herpesvirus proteases(1,5,8) suggest that dimerization may confer specificity and recognition in substrate binding.

引用

页码：279 / 282

页数：4

共 30 条

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