NOVEL MECHANISM FOR REVERSE TRANSCRIPTION IN HEPATITIS-B VIRUSES

被引：255

作者：

WANG, GH ^{[1
]}

SEEGER, C ^{[1
]}

机构：

[1] FOX CHASE CANC CTR,INST CANC RES,7701 BURHOLME AVE,PHILADELPHIA,PA 19111

来源：

JOURNAL OF VIROLOGY | 1993年 / 67卷 / 11期

关键词：

D O I：

10.1128/JVI.67.11.6507-6512.1993

中图分类号：

Q93 [微生物学];

学科分类号：

071005 ; 100705 ;

摘要：

Reverse transcription of all retroviruses and most retroid elements requires tRNA as a primer for DNA synthesis. However, in hepatitis B viruses the viral polymerase itself acts as a primer for reverse transcription (G.-H. Wang and C. Seeger, Cell 71:663-670, 1992). We have now demonstrated that in order to prime DNA synthesis, the polymerase binds to an RNA hairpin, which then serves as a template for the formation of a short DNA primer that is covalently linked to protein. Following its synthesis, the nascent DNA strand apparently dissociates from its template and reanneals with complementary sequences at the 3' end of the RNA genome, where DNA synthesis continues. Since this RNA hairpin also functions as a packaging signal for viral RNA, hepadnaviruses have adopted a replication strategy that relies on the same signal for two biochemically distinct events, RNA packaging and reverse transcription. This mechanism is without precedent among all known retroid elements and among other viruses and bacteriophages that use protein as a primer for RNA or DNA synthesis. It could provide an effective target for antiviral therapy, which is required for the treatment of more than 300 million carriers of hepatitis B virus.

引用

页码：6507 / 6512

页数：6

共 28 条

[11] INITIATION AND TERMINATION OF DUCK HEPATITIS-B VIRUS-DNA SYNTHESIS DURING VIRUS MATURATION [J].

LIEN, JM ;

PETCU, DJ ;

ALDRICH, CE ;

MASON, WS .

JOURNAL OF VIROLOGY, 1987, 61 (12) :3832-3840

[12]

LIES J, 1993, REVERSE TRANSCRIPTAS, P33

[13] NUCLEOTIDE-SEQUENCE OF A CLONED DUCK HEPATITIS-B VIRUS GENOME - COMPARISON WITH WOODCHUCK AND HUMAN HEPATITIS-B VIRUS SEQUENCES [J].

MANDART, E ;

KAY, A ;

GALIBERT, F .

JOURNAL OF VIROLOGY, 1984, 49 (03) :782-792

[14] PROTEIN COVALENTLY BOUND TO MINUS-STRAND DNA INTERMEDIATES OF DUCK HEPATITIS-B VIRUS [J].

MOLNARKIMBER, KL ;

SUMMERS, J ;

TAYLOR, JM ;

MASON, WS .

JOURNAL OF VIROLOGY, 1983, 45 (01) :165-172

[15] AN RNA STEM-LOOP STRUCTURE DIRECTS HEPATITIS-B VIRUS GENOMIC RNA ENCAPSIDATION [J].

POLLACK, JR ;

GANEM, D .

JOURNAL OF VIROLOGY, 1993, 67 (06) :3254-3263

[16] DUCK HEPATITIS-B VIRUS (DHBV) PARTICLES PRODUCED BY TRANSIENT EXPRESSION OF DHBV DNA IN A HUMAN HEPATOMA-CELL LINE ARE INFECTIOUS INVITRO [J].

PUGH, JC ;

YAGINUMA, K ;

KOIKE, K ;

SUMMERS, J .

JOURNAL OF VIROLOGY, 1988, 62 (09) :3513-3516

[17]

Sambrook J., 1989, MOL CLONING LAB MANU

[18] BIOCHEMICAL AND GENETIC-EVIDENCE FOR THE HEPATITIS-B VIRUS-REPLICATION STRATEGY [J].

SEEGER, C ;

GANEM, D ;

VARMUS, HE .

SCIENCE, 1986, 232 (4749) :477-484

[19] IDENTIFICATION OF A SIGNAL NECESSARY FOR INITIATION OF REVERSE TRANSCRIPTION OF THE HEPADNAVIRUS GENOME [J].

SEEGER, C ;

MARAGOS, J .

JOURNAL OF VIROLOGY, 1991, 65 (10) :5190-5195

[20] IDENTIFICATION AND CHARACTERIZATION OF THE WOODCHUCK HEPATITIS-VIRUS ORIGIN OF DNA-REPLICATION [J].

SEEGER, C ;

MARAGOS, J .

JOURNAL OF VIROLOGY, 1990, 64 (01) :16-23

← 1 2 3 →