学术探索
学术期刊
新闻热点
数据分析
智能评审

CONSTRUCTION OF A US3 LACZ INSERTION MUTANT OF HERPES-SIMPLEX VIRUS TYPE-2 AND CHARACTERIZATION OF ITS PHENOTYPE INVITRO AND INVIVO

被引:90
作者
NISHIYAMA, Y
YAMADA, Y
KURACHI, R
DAIKOKU, T
机构
[1] Laboratory of Virology, Research Institute for Disease Mechanism and Control, Nagoya University School of Medicine, Showa-ku, Nagoya, 466
来源
VIROLOGY | 1992年 / 190卷 / 01期
关键词
D O I
10.1016/0042-6822(92)91212-D
中图分类号
Q93 [微生物学];
学科分类号
071005 ; 100705 ;
摘要
We have constructed and characterized a mutant of herpes simplex virus type 2 (HSV-2) which was inserted a modified lacZ gene, placed under the control of HSV-1 β8 promotor, into the US3 protein kinase gene. The mutant, L1BR1, could not induce the virus-encoded protein kinase activity, but could replicate in Vero cells as efficiently as the parental virus. When the biological properties of L1BR1 were examined in mice by using four routes (footpad, intraperitoneal, corneal, and intracerebral) of infection, the mutant displayed the route-dependent reduction of virulence; after inoculation by footpad and intraperitoneal routes, the mutant was more than 10,000-fold less virulent than the parental virus, but it exhibited only about a 10-fold decrease in virulence following the corneal and intracerebral infection. In the intraperitoneal inoculation into adult mice, the replication of L1BR1 in the liver and spleen was severely restricted, but in newborn mice the mutant could grow as well as the parental virus in these organs. The adoptive transfer of peritoneal macrophages from adult mice resulted in a marked inhibition in the replication of L1BR1 in the liver and spleen of newborn mice, while the transfer exhibited little or no effect on the production of the wild-type virus in these organs. We also found that the mutant, unlike the parental virus, could not replicate in precultured peritoneal macrophages from adult mice. Taking these observations together, it seems likely that L1 BR1 lost the ability to overcome the mononuclear-phagocytic defense system and thereby lost its pathogenicity by intraperitoneal and footpad routes. Furthermore, the mutant was shown to be rescued by a 4.8-kb HindIII/XbaI fragment containing the entire US3 open reading frame. However, we could not rule out the possibility that some of the phenotypes of L1BR1 are due to mutations in the US3-neighboring genes, US2 and US4. © 1992.
引用
收藏
页码:256 / 268
页数:13
相关论文
共 50 条
[1]   HSV-1 DNA-SEQUENCE DETERMINING INTRAPERITONEAL PATHOGENICITY IN MICE IS REQUIRED FOR TRANSCRIPTION OF VIRAL IMMEDIATE-EARLY GENES IN MACROPHAGES [J].
BENHUR, T ;
ROSENWOLFF, A ;
LAMADE, W ;
DARAI, G ;
BECKER, Y .
VIROLOGY, 1988, 163 (02) :397-404
[2]   CHARACTERIZATION OF RNA TRANSCRIPTS FROM HERPES-SIMPLEX VIRUS-1 DNA FRAGMENT BAMHI-B [J].
BENHUR, T ;
MOYAL, M ;
ROSENWOLFF, A ;
DARAI, G ;
BECKER, Y .
VIROLOGY, 1989, 169 (01) :1-8
[3]   RIBONUCLEOTIDE REDUCTASE ENCODED BY HERPES-SIMPLEX VIRUS IS A DETERMINANT OF THE PATHOGENICITY OF THE VIRUS IN MICE AND A VALID ANTIVIRAL TARGET [J].
CAMERON, JM ;
MCDOUGALL, I ;
MARSDEN, HS ;
PRESTON, VG ;
RYAN, DM ;
SUBAKSHARPE, JH .
JOURNAL OF GENERAL VIROLOGY, 1988, 69 :2607-2612
[4]   MAPPING OF HERPES-SIMPLEX VIRUS-1 NEUROVIRULENCE TO GAMMA-134.5, A GENE NONESSENTIAL FOR GROWTH IN CULTURE [J].
CHOU, J ;
KERN, ER ;
WHITLEY, RJ ;
ROIZMAN, B .
SCIENCE, 1990, 250 (4985) :1262-1266
[5]   EVIDENCE THAT THE GENE FOR HERPES-SIMPLEX VIRUS TYPE-1 DNA-POLYMERASE ACCOUNTS FOR THE CAPACITY OF AN INTERTYPIC RECOMBINANT TO SPREAD FROM EYE TO CENTRAL NERVOUS-SYSTEM [J].
DAY, SP ;
LAUSCH, RN ;
OAKES, JE .
VIROLOGY, 1988, 163 (01) :166-173
[6]   COMPARATIVE NEUROVIRULENCE OF HERPES-SIMPLEX VIRUS TYPE-1 STRAINS AFTER PERIPHERAL OR INTRACEREBRAL INOCULATION OF BALB/C MICE [J].
DIX, RD ;
MCKENDALL, RR ;
BARINGER, JR .
INFECTION AND IMMUNITY, 1983, 40 (01) :103-112
[7]   LIPOFECTION - A HIGHLY EFFICIENT, LIPID-MEDIATED DNA-TRANSFECTION PROCEDURE [J].
FELGNER, PL ;
GADEK, TR ;
HOLM, M ;
ROMAN, R ;
CHAN, HW ;
WENZ, M ;
NORTHROP, JP ;
RINGOLD, GM ;
DANIELSEN, M .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1987, 84 (21) :7413-7417
[8]   IDENTIFICATION OF THE HERPES-SIMPLEX VIRUS PROTEIN-KINASE AS THE PRODUCT OF VIRAL GENE US3 [J].
FRAME, MC ;
PURVES, FC ;
MCGEOCH, DJ ;
MARSDEN, HS ;
LEADER, DP .
JOURNAL OF GENERAL VIROLOGY, 1987, 68 :2699-2704
[9]   BETA-GALACTOSIDASE AS A MARKER IN THE PERIPHERAL AND NEURAL TISSUES OF THE HERPES-SIMPLEX VIRUS-INFECTED MOUSE [J].
HO, DY ;
MOCARSKI, ES .
VIROLOGY, 1988, 167 (01) :279-283
[10]   ELECTROBLOTTING OF DOUBLE-STRANDED DNA FOR HYBRIDIZATION EXPERIMENTS - DNA TRANSFER IS COMPLETE WITHIN 10 MINUTES AFTER PULSED-FIELD GEL-ELECTROPHORESIS [J].
ISHIHARA, H ;
SHIKITA, M .
ANALYTICAL BIOCHEMISTRY, 1990, 184 (02) :207-212
12345