Identification of hepatitis A virus non-structural protein 2B and its release by the major virus protease 3C

被引：20

作者：

Gosert, R ^{[1
]}

Cassinotti, P ^{[1
]}

Siegl, G ^{[1
]}

Weitz, M ^{[1
]}

机构：

[1] INST CLIN MICROBIOL & IMMUNOL,CH-9001 ST GALLEN,SWITZERLAND

来源：

JOURNAL OF GENERAL VIROLOGY | 1996年 / 77卷

关键词：

D O I：

10.1099/0022-1317-77-2-247

中图分类号：

Q81 [生物工程学（生物技术）]; Q93 [微生物学];

学科分类号：

071005 ; 0836 ; 090102 ; 100705 ;

摘要：

The RNA genome of hepatitis A virus (HAV) encodes a giant polyprotein that is putatively cleaved proteolytically into four structural and seven non-structural proteins. So far, most of the proposed non-structural proteins and their respective cleavage sites have not been identified. A vaccinia virus recombinant (vRGORF) containing the complete HAV ORF under the control of the bacteriophage T7 promoter was used to express HAV in recombinant animal cells (BT7-H) that constitutively expressed T7 DNA-dependent RNA polymerase. A HAV-specific 27.5 kDa expression product was identified as peptide 2B. The 27.5 kDa 2B antigen was also found in HAV-infected MRC-5 cells. The N-terminal amino acid residues of the new peptide 2B are Ala-Lys-Ile-Ser-Leu-Phe and polyprotein cleavage between 2A and 2B occurred at amino acids 836-837 (Gln-Ala). Furthermore, heterologous expression in the same system of regions P1-P2 and of the protease 3C (3C(pro)) gene, showed that P1-P2 polyprotein is not cleaved autocatalytically but by 3C(pro). Hence, 3C(pro) is effective in cleaving the polyprotein 2A-2B junction.

引用

页码：247 / 255

页数：9

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