THE P-GENE OF THE PORCINE PARAMYXOVIRUS LPMV ENCODES 3 POSSIBLE POLYPEPTIDES-P, POLYPEPTIDE-V AND POLYPEPTIDE-C - THE P-PROTEIN MESSENGER-RNA IS EDITED

被引：33

作者：

BERG, M

HJERTNER, B

MORENOLOPEZ, J

LINNE, T

机构：

[1] Dept. of Veterinary Microbiology, Unit of Molecular Virology, University of Agricultural Sciences, S-751 23 Uppsala

来源：

JOURNAL OF GENERAL VIROLOGY | 1992年 / 73卷

关键词：

D O I：

10.1099/0022-1317-73-5-1195

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 nucleotide sequence of the P gene of the porcine paramyxovirus La-Piedad-Michoacan-Mexico virus (LPMV) was analysed. Three long open reading frames (ORFs) were found in the mRNA sense. Insertion of two G residues is necessary to obtain an ORF encoding the P protein, which gives a P protein of 404 amino acids with a calculated M(r) of 42475. This form of editing was demonstrated, two non-templated G residues being added in a portion of the mRNA transcripts. The LPMV V protein, which has a conserved cysteine-rich C-terminal region, is encoded by an exact copy of the P gene. The third ORF has the capacity to encode a protein of 126 amino acids, which may resemble the C proteins found in some paramyxoviruses. The ORF starts from an AUG codon downstream of the first AUG codon of the P/V ORF.

引用

页码：1195 / 1200

页数：6

共 29 条

[1] IDENTIFICATION OF THE PORCINE PARAMYXOVIRUS LPMV MATRIX PROTEIN GENE - COMPARATIVE SEQUENCE-ANALYSIS WITH OTHER PARAMYXOVIRUSES [J].

BERG, M ;

SUNDQVIST, A ;

MORENOLOPEZ, J ;

LINNE, T .

JOURNAL OF GENERAL VIROLOGY, 1991, 72 :1045-1050

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

CATTANEO, R ;

KAELIN, K ;

BACZKO, K ;

BILLETER, MA .

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

[3] DIFFERENT TYPES OF MESSENGER-RNA EDITING [J].

CATTANEO, R .

ANNUAL REVIEW OF GENETICS, 1991, 25 :71-88

[4] PHOSPHORYLATION WITHIN A SPECIFIC DOMAIN OF THE PHOSPHOPROTEIN OF VESICULAR STOMATITIS-VIRUS REGULATES TRANSCRIPTION INVITRO [J].

CHATTOPADHYAY, D ;

BANERJEE, AK .

CELL, 1987, 49 (03) :407-414

[5] CHARACTERIZATION OF THE SENDAI VIRUS V-PROTEIN WITH AN ANTIPEPTIDE ANTISERUM [J].

CURRAN, J ;

DEMELO, M ;

MOYER, S ;

KOLAKOFSKY, D .

VIROLOGY, 1991, 184 (01) :108-116

[6] SCANNING INDEPENDENT RIBOSOMAL INITIATION OF THE SENDAI VIRUS X-PROTEIN [J].

CURRAN, J ;

KOLAKOFSKY, D .

EMBO JOURNAL, 1988, 7 (09) :2869-2874

[7] A COMPREHENSIVE SET OF SEQUENCE-ANALYSIS PROGRAMS FOR THE VAX [J].

DEVEREUX, J ;

HAEBERLI, P ;

SMITHIES, O .

NUCLEIC ACIDS RESEARCH, 1984, 12 (01) :387-395

[8] STRAIN-VARIABLE EDITING DURING TRANSCRIPTION OF THE P-GENE OF MUMPS-VIRUS MAY LEAD TO THE GENERATION OF NONSTRUCTURAL PROTEINS NS1 (V) AND NS2 [J].

ELLIOTT, GD ;

YEO, RP ;

AFZAL, MA ;

SIMPSON, EJB ;

CURRAN, JA ;

RIMA, BK .

JOURNAL OF GENERAL VIROLOGY, 1990, 71 :1555-1560

[9] MOLECULAR-CLONING AND SEQUENCE-ANALYSIS OF THE HUMAN PARAINFLUENZA-3 VIRUS MESSENGER-RNA ENCODING THE P-PROTEIN AND C-PROTEIN [J].

GALINSKI, MS ;

MINK, MA ;

LAMBERT, DM ;

WECHSLER, SL ;

PONS, MW .

VIROLOGY, 1986, 155 (01) :46-60

[10] TRANSCRIPTIVE COMPLEX OF NEWCASTLE-DISEASE VIRUS .1. BOTH L-PROTEIN AND P-PROTEIN ARE REQUIRED TO CONSTITUTE AN ACTIVE COMPLEX [J].

HAMAGUCHI, M ;

YOSHIDA, T ;

NISHIKAWA, K ;

NARUSE, H ;

NAGAI, Y .

VIROLOGY, 1983, 128 (01) :105-117

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