SPECIFIC DELETIONS IN THE HEPATITIS-B VIRUS CORE OPEN READING FRAME IN PATIENTS WITH CHRONIC ACTIVE HEPATITIS-B

被引：30

作者：

ACKRILL, AM ^{[1
]}

NAOUMOV, NV ^{[1
]}

EDDLESTON, ALWF ^{[1
]}

WILLIAMS, R ^{[1
]}

机构：

[1] KINGS COLL,SCH MED & DENT,INST LIVER STUDIES,LONDON SE5 9PJ,ENGLAND

来源：

JOURNAL OF MEDICAL VIROLOGY | 1993年 / 41卷 / 02期

关键词：

VIRAL MUTANTS; HBV DNA SEQUENCING; POLYMERASE CHAIN REACTION; CHRONIC HBV INFECTION;

D O I：

10.1002/jmv.1890410213

中图分类号：

Q93 [微生物学];

学科分类号：

071005 ; 100705 ;

摘要：

The polymerase chain reaction (PCR) and DNA sequencing were used to examine genomic variation in the pre-core/core open reading frame of the hepatitis B virus (HBV) in chronically infected patients. Gel electrophoresis of amplification products showed the presence of shortened forms of the core gene in addition to the full length product. These shortened forms were seen only in patients with chronic active hepatitis (CAH) seropositive for HBeAg and not in patients with chronic persistent hepatitis (CPH) or HBeAg minus CAH. Cloning and DNA sequencing revealed the presence of a number of overlapping deletions within the core gene, the majority being in-frame, which were clustered within aa 81-114 of the core gene product. These deletions were found in patients with CAH from different racial and geographical backgrounds, whereas PCR analysis of the surface and X open reading frames showed no shortened forms suggesting deletions to be specific to the core gene ih these patients. Because the product of the core gene-the HBV core antigen-is believed to be the major target for T-cell-mediated liver damage, it seems likely that the products of core genes carrying deletions will alter immune recognition and may be of importance in the progression of inflammatory liver damage. (C) 1993 Wiley-Liss, Inc.

引用

页码：165 / 169

页数：5

共 20 条

[1] COMPARISON OF PRECORE CORE HEPATITIS-B VIRUS REGION IN LIVER-TISSUE AND SERUM FROM PATIENTS WITH CHRONIC HEPATITIS-B INFECTION [J].

ACKRILL, AM ;

NAOUMOV, NV ;

EDDLESTON, ALWF ;

WILLIAMS, R .

JOURNAL OF HEPATOLOGY, 1992, 16 (1-2) :224-227

[2] HLA CLASS-I-RESTRICTED HUMAN CYTOTOXIC T-CELLS RECOGNIZE ENDOGENOUSLY SYNTHESIZED HEPATITIS-B VIRUS NUCLEOCAPSID ANTIGEN [J].

BERTOLETTI, A ;

FERRARI, C ;

FIACCADORI, F ;

PENNA, A ;

MARGOLSKEE, R ;

SCHLICHT, HJ ;

FOWLER, P ;

GUILHOT, S ;

CHISARI, FV .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1991, 88 (23) :10445-10449

[3]

BRUNETTO MR, 1989, ITAL J GASTROENTEROL, V21, P151

[4] VACCINE-INDUCED ESCAPE MUTANT OF HEPATITIS-B VIRUS [J].

CARMAN, WF ;

ZANETTI, AR ;

KARAYIANNIS, P ;

WATERS, J ;

MANZILLO, G ;

TANZI, E ;

ZUCKERMAN, AJ ;

THOMAS, HC .

LANCET, 1990, 336 (8711) :325-329

[5]

CARMAN WF, 1989, LANCET, V2, P588

[6] VARIATIONS IN CODONS 84-101 IN THE CORE NUCLEOTIDE-SEQUENCE CORRELATE WITH HEPATOCELLULAR INJURY IN CHRONIC HEPATITIS-B VIRUS-INFECTION [J].

EHATA, T ;

OMATA, M ;

YOKOSUKA, O ;

HOSODA, K ;

OHTO, M .

JOURNAL OF CLINICAL INVESTIGATION, 1992, 89 (01) :332-338

[7] IDENTIFICATION OF IMMUNODOMINANT T-CELL EPITOPES OF THE HEPATITIS-B VIRUS NUCLEOCAPSID ANTIGEN [J].

FERRARI, C ;

BERTOLETTI, A ;

PENNA, A ;

CAVALLI, A ;

VALLI, A ;

MISSALE, G ;

PILLI, M ;

FOWLER, P ;

GIUBERTI, T ;

CHISARI, FV ;

FIACCADORI, F .

JOURNAL OF CLINICAL INVESTIGATION, 1991, 88 (01) :214-222

[8]

FERRARI C, 1987, J IMMUNOL, V139, P539

[9] NUCLEOTIDE-SEQUENCE OF THE HEPATITIS-B VIRUS GENOME (SUBTYPE AYW) CLONED IN ESCHERICHIA-COLI [J].

GALIBERT, F ;

MANDART, E ;

FITOUSSI, F ;

TIOLLAIS, P ;

CHARNAY, P .

NATURE, 1979, 281 (5733) :646-650

[10] EXPRESSION MECHANISM OF THE HEPATITIS-B VIRUS (HBV) C-GENE AND BIOSYNTHESIS OF HBE ANTIGEN [J].

JEANJEAN, O ;

LEVRERO, M ;

WILL, H ;

PERRICAUDET, M ;

ROSSIGNOL, JM .

VIROLOGY, 1989, 170 (01) :99-106

← 1 2 →