CHARACTERIZATION OF V-PROTEIN IN MEASLES VIRUS-INFECTED CELLS

被引：38

作者：

WARDROP, EA ^{[1
]}

BRIEDIS, DJ ^{[1
]}

机构：

[1] MCGILL UNIV,DEPT MICROBIOL & IMMUNOL,3775 UNIV ST,MONTREAL H3A 2B4,QUEBEC,CANADA

来源：

JOURNAL OF VIROLOGY | 1991年 / 65卷 / 07期

关键词：

D O I：

10.1128/JVI.65.7.3421-3428.1991

中图分类号：

Q93 [微生物学];

学科分类号：

071005 ; 100705 ;

摘要：

An edited mRNA transcribed from the phosphoprotein (P) gene of measles virus (MV) has been predicted to encode a cysteine-rich protein designated V. This mRNA contains a single additional nontemplated G residue which permits access to an additional protein-coding reading frame. Such an edited P gene-specific mRNA has been detected in MV-infected cells, but no corresponding protein has yet been identified in vivo. We report the use of antisera directed against synthetic peptides corresponding to five different regions of the predicted MV V protein amino acid sequence to analyse MV-specific proteins synthesized in vivo and in vitro. The MV V protein (40 kDa) was detected in MV-infected cells in a diffuse cytoplasmic distribution, a predominant subcellular localization distinct from that of virus nucleocapsids. The protein was found to be phosphorylated and to be maximally synthesized at 16 h postinfection, when MV-specific structural protein synthesis was also maximal. Antiserum directed against a peptide (PV2) corresponding to amino acids 65 to 87 of the V protein amino acid recognized the P protein but not the V protein, indicating that the P and V proteins may be folded differently at or near this region so that the PV2 sequence is in an exposed position at the surface of the P protein but not at the surface of the V protein.

引用

页码：3421 / 3428

页数：8

共 29 条

[1] THE PREDICTED PRIMARY STRUCTURE OF THE MEASLES-VIRUS HEMAGGLUTININ [J].

ALKHATIB, G ;

BRIEDIS, DJ .

VIROLOGY, 1986, 150 (02) :479-490

[2] EXPRESSION OF BICISTRONIC MEASLES VIRUS-P/C MESSENGER-RNA BY USING HYBRID ADENOVIRUSES - LEVELS OF C PROTEIN SYNTHESIZED INVIVO ARE UNAFFECTED BY THE PRESENCE OR ABSENCE OF THE UPSTREAM-P INITIATOR CODON [J].

ALKHATIB, G ;

MASSIE, B ;

BRIEDIS, DJ .

JOURNAL OF VIROLOGY, 1988, 62 (11) :4059-4069

[3] PURIFICATION AND MOLECULAR-WEIGHT DETERMINATION OF MEASLES-VIRUS GENOMIC RNA [J].

BACZKO, K ;

BILLETER, M ;

TERMEULEN, V .

JOURNAL OF GENERAL VIROLOGY, 1983, 64 (JUN) :1409-1413

[4] MEASLES VIRUS-P GENE CODES FOR 2 PROTEINS [J].

BELLINI, WJ ;

ENGLUND, G ;

ROZENBLATT, S ;

ARNHEITER, H ;

RICHARDSON, CD .

JOURNAL OF VIROLOGY, 1985, 53 (03) :908-919

[5] CLONING OF DNA CORRESPONDING TO 4 DIFFERENT MEASLES-VIRUS GENOMIC REGIONS [J].

BILLETER, MA ;

BACZKO, K ;

SCHMID, A ;

TERMEULEN, V .

VIROLOGY, 1984, 132 (01) :147-159

[6] MEASLES-VIRUS EDITING PROVIDES AN ADDITIONAL CYSTEINE-RICH PROTEIN [J].

CATTANEO, R ;

KAELIN, K ;

BACZKO, K ;

BILLETER, MA .

CELL, 1989, 56 (05) :759-764

[7] DEVELOPMENT OF ATTENUATED MEASLES-VIRUS VACCINES - A SUMMARY OF RECENT INVESTIGATION [J].

ENDERS, JF ;

KATZ, SL ;

HOLLOWAY, A .

AMERICAN JOURNAL OF DISEASES OF CHILDREN, 1962, 103 (03) :335-&

[8] MEASLES VIRUS - HISTORICAL REVIEW, ISOLATION, AND BEHAVIOUR IN VARIOUS SYSTEMS [J].

ENDERS, JF .

AMERICAN JOURNAL OF DISEASES OF CHILDREN, 1962, 103 (03) :282-&

[9] DIFFERENTIAL POST-TRANSLATIONAL MODIFICATION OF HUMAN TYPE-I KERATINS SYNTHESIZED IN A RABBIT RETICULOCYTE CELL-FREE SYSTEM [J].

GIBBS, PEM ;

ZOUZIAS, DC ;

FREEDBERG, IM .

BIOCHIMICA ET BIOPHYSICA ACTA, 1985, 824 (03) :247-255

[10] MEASLES-VIRUS POLYPEPTIDES IN INFECTED-CELLS STUDIED BY IMMUNE PRECIPITATION AND ONE-DIMENSIONAL PEPTIDE-MAPPING [J].

GRAVES, MC .

JOURNAL OF VIROLOGY, 1981, 38 (01) :224-230

← 1 2 3 →