NUCLEOTIDE-SEQUENCE ANALYSIS OF A 38.5-KILOBASE-PAIR REGION OF THE GENOME OF HUMAN HERPESVIRUS-6 ENCODING HUMAN CYTOMEGALOVIRUS IMMEDIATE-EARLY GENE HOMOLOGS AND TRANSACTIVATING FUNCTIONS

被引：57

作者：

NICHOLAS, J ^{[1
]}

MARTIN, MED ^{[1
]}

机构：

[1] NATL INST MED RES, DIV VIROL, LONDON NW7 1AA, ENGLAND

来源：

JOURNAL OF VIROLOGY | 1994年 / 68卷 / 02期

关键词：

D O I：

10.1128/JVI.68.2.597-610.1994

中图分类号：

Q93 [微生物学];

学科分类号：

071005 ; 100705 ;

摘要：

Human herpesvirus 6 (HHV-6) is prevalent in the human population, with primary infection occurring early in life. Its predominant CD4(+) T-lymphocyte tropism, its ability to activate human immunodeficiency virus type 1 (HIV-1) gene expression in vitro, and its upregulation of CD4 expression has led to speculation that HHV-6 may act as a positive cofactor in the progression of HIV infection to AIDS in individuals infected with both viruses. Previous sequencing studies of restricted regions of the 161.5-kbp genome of HHV-6 have demonstrated unequivocally that it is a member of the betaherpesvirus subgroup and have indicated that the HHV-6 genome is generally collinear with the unique long (U-L) component of human cytomegalovirus (HCMV). In the work described in this report we have extended these sequencing studies by determining the primary structure of 38.5-kbp of the HHV-6 genome (genomic position 21.0 to 59.5 kbp). Within the sequenced region lie 31 open reading frames, 20 of which are homologous to positional counterparts in HCMV. Of particular significance is the identification of homologs of the HCMV UL36-38 and US22-type genes, which have been shown to encode transactivating proteins. We show that DNA sequences encoding these HHV-6 homologs were able to transactivate HIV-1 long terminal repeat-directed chloramphenicol acetyltransferase expression in cotransfection assays, thus demonstrating functional as well as structural conservation of these betaherpesvirus-specific gene products. Our data therefore confirm the close relationship between HHV-6 and HCMV and identify putative immediate-early regulatory genes of HHV-6 likely to play key roles in lytic replication and possibly also in the interactions between HHV-6 and HIV in dually infected cells.

引用

页码：597 / 610

页数：14

共 98 条

[1] THE STRUCTURE OF THE MAJOR IMMEDIATE EARLY GENE OF HUMAN CYTOMEGALO-VIRUS STRAIN AD169 [J].

AKRIGG, A ;

WILKINSON, GWG ;

ORAM, JD .

VIRUS RESEARCH, 1985, 2 (02) :107-121

[2] PRIMARY STRUCTURE OF THE HERPESVIRUS SAIMIRI GENOME [J].

ALBRECHT, JC ;

NICHOLAS, J ;

BILLER, D ;

CAMERON, KR ;

BIESINGER, B ;

NEWMAN, C ;

WITTMANN, S ;

CRAXTON, MA ;

COLEMAN, H ;

FLECKENSTEIN, B ;

HONESS, RW .

JOURNAL OF VIROLOGY, 1992, 66 (08) :5047-5058

[3] IDENTIFICATION AND SEPARATION OF THE 2 SUBUNITS OF THE HERPES-SIMPLEX VIRUS RIBONUCLEOTIDE REDUCTASE [J].

BACCHETTI, S ;

EVELEGH, MJ ;

MUIRHEAD, B .

JOURNAL OF VIROLOGY, 1986, 57 (03) :1177-1181

[4] DNA-SEQUENCE AND EXPRESSION OF THE B95-8 EPSTEIN-BARR VIRUS GENOME [J].

BAER, R ;

BANKIER, AT ;

BIGGIN, MD ;

DEININGER, PL ;

FARRELL, PJ ;

GIBSON, TJ ;

HATFULL, G ;

HUDSON, GS ;

SATCHWELL, SC ;

SEGUIN, C ;

TUFFNELL, PS ;

BARRELL, BG .

NATURE, 1984, 310 (5974) :207-211

[5]

BANKIER AT, 1987, METHOD ENZYMOL, V155, P51

[6] GENETIC-RELATIONSHIPS BETWEEN BOVINE HERPESVIRUS-4 AND THE GAMMAHERPESVIRUSES EPSTEIN-BARR-VIRUS AND HERPESVIRUS SAIMIRI [J].

BUBLOT, M ;

LOMONTE, P ;

LEQUARRE, AS ;

ALBRECHT, JC ;

NICHOLAS, J ;

FLECKENSTEIN, B ;

PASTORET, PP ;

THIRY, E .

VIROLOGY, 1992, 190 (02) :654-665

[7] SUPPRESSION OF HUMAN-IMMUNODEFICIENCY-VIRUS TYPE-1 REPLICATION BY HUMAN HERPESVIRUS-6 [J].

CARRIGAN, DR ;

KNOX, KK ;

TAPPER, MA .

JOURNAL OF INFECTIOUS DISEASES, 1990, 162 (04) :844-851

[8]

CHANG CK, 1991, J VIROL, V65, P7085, DOI 10.1128/JVI.65.12.7085-.1991

[9] IDENTIFICATION, CHARACTERIZATION, AND SEQUENCE-ANALYSIS OF A CDNA-ENCODING A PHOSPHOPROTEIN OF HUMAN HERPESVIRUS-6 [J].

CHANG, CK ;

BALACHANDRAN, N .

JOURNAL OF VIROLOGY, 1991, 65 (06) :2884-2894

[10] THE EPSTEIN-BARR-VIRUS ZTA TRANSACTIVATOR - A MEMBER OF THE BZIP FAMILY WITH UNIQUE DNA-BINDING SPECIFICITY AND A DIMERIZATION DOMAIN THAT LACKS THE CHARACTERISTIC HEPTAD LEUCINE ZIPPER MOTIF [J].

CHANG, YN ;

DONG, DLY ;

HAYWARD, GS ;

HAYWARD, SD .

JOURNAL OF VIROLOGY, 1990, 64 (07) :3358-3369

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