学术探索
学术期刊
新闻热点
数据分析
智能评审

MYELOBLASTOSIS ASSOCIATED VIRUS (MAV) PROTEINASE SITE-MUTATED TO BE HIV-LIKE HAS A HIGHER ACTIVITY AND ALLOWS PRODUCTION OF INFECTIOUS BUT MORPHOLOGICALLY ALTERED VIRUS

被引:4
作者
SEDLACEK, J
FABRY, M
COWARD, JE
HOREJSI, M
STROP, P
LUFTIG, RB
机构
[1] LOUISIANA STATE UNIV, MED CTR, DEPT MICROBIOL IMMUNOL & PARASITOL, NEW ORLEANS, LA 70112 USA
[2] CZECHOSLOVAK ACAD SCI, INST ORGAN CHEM & BIOCHEM, DEPT BIOCHEM 2, CS-16610 PRAGUE 6, CZECHOSLOVAKIA
来源
VIROLOGY | 1993年 / 192卷 / 02期
关键词
D O I
10.1006/viro.1993.1085
中图分类号
Q93 [微生物学];
学科分类号
071005 ; 100705 ;
摘要
We have characterized the structure and infectivity of an avian retrovirus, myeloblastosis associated virus (MAV), containing a genetically altered proteinase (PR). A site-directed mutant of MAV-PR that shows an increased proteolytic activity in vitro (about 20 times higher k(cat)/K(m)) as a consequence of substituting five amino acids from the substrate-binding pocket with those corresponding to the HIV-1 PR was cloned into a full-sized MAV plasmid. In particular, the wild-type MAV-PR gene was replaced with the mutant one. Despite encoding for an enzyme with increased PR activity, mutant plasmid-transfected turkey fibroblasts displayed an unimpaired virus production in cell cultures. Further, the mutant progeny virus was infectious and its pattern of gag processing products appeared identical to that of wild-type virus. However, by electron microscopy we found that the predominant morphology of mutant viral particles was altered. Instead of a centrally collapsed avian retroviral core, a more diffuse core was visualized for wild-type mutant virions, similar to that observed in mammalian C-type retroviruses. © 1994 Academic Press, Inc.
引用
收藏
页码:667 / 672
页数:6
相关论文
共 38 条
[21]  
OHLENDORF DH, IN PRESS PROTEINS ST, V10
[22]  
OROSZLAN S, 1990, CURR TOP MICROBIOL, V157, P153
[23]  
PECENKA V, 1987, THESIS CZECHOSLOVAK
[24]   BIOLOGICALLY-ACTIVE PROVIRAL CLONE OF MYELOBLASTOSIS-ASSOCIATED VIRUS TYPE-1 - IMPLICATIONS FOR THE GENESIS OF AVIAN-MYELOBLASTOSIS VIRUS [J].
PERBAL, B ;
LIPSICK, JS ;
SVOBODA, J ;
SILVA, RF ;
BALUDA, MA .
JOURNAL OF VIROLOGY, 1985, 56 (01) :240-244
[25]   COMPLETE NUCLEOTIDE-SEQUENCE OF THE AIDS VIRUS, HTLV-III [J].
RATNER, L ;
HASELTINE, W ;
PATARCA, R ;
LIVAK, KJ ;
STARCICH, B ;
JOSEPHS, SF ;
DORAN, ER ;
RAFALSKI, JA ;
WHITEHORN, EA ;
BAUMEISTER, K ;
IVANOFF, L ;
PETTEWAY, SR ;
PEARSON, ML ;
LAUTENBERGER, JA ;
PAPAS, TS ;
GHRAYEB, J ;
CHANG, NT ;
GALLO, RC ;
WONGSTAAL, F .
NATURE, 1985, 313 (6000) :277-284
[26]   A SINGLE AMINO-ACID SUBSTITUTION WITHIN THE MATRIX PROTEIN OF A TYPE-D RETROVIRUS CONVERTS ITS MORPHOGENESIS TO THAT OF A TYPE-C RETROVIRUS [J].
RHEE, SS ;
HUNTER, E .
CELL, 1990, 63 (01) :77-86
[27]  
RICHARDS AD, 1990, J BIOL CHEM, V265, P7733
[28]   NON-CONDITIONAL REPLICATION MUTANTS OF TYPE-C AND TYPE-D RETROVIRUSES DEFECTIVE IN GAG GENE-CODED POLYPROTEIN POST-TRANSLATIONAL PROCESSING [J].
SACKS, TL ;
DEVARE, SG ;
BLENNERHASSETT, GT ;
STEPHENSON, JR .
VIROLOGY, 1978, 91 (02) :352-363
[29]  
Sambrook J., 1989, MOL CLONING LAB MANU
[30]   NUCLEOTIDE-SEQUENCE OF ROUS-SARCOMA VIRUS [J].
SCHWARTZ, DE ;
TIZARD, R ;
GILBERT, W .
CELL, 1983, 32 (03) :853-869
1234