In vivo selection of duck hepatitis B virus pre-S variants which escape from neutralization

被引：8

作者：

Sunyach, C ^{[1
]}

Chassot, S ^{[1
]}

Jamard, C ^{[1
]}

Kay, A ^{[1
]}

Trepo, C ^{[1
]}

Cova, L ^{[1
]}

机构：

[1] INSERM,U271,UNITE RECH VIRUS HEPATITES RETROVIRUS HUMAINS & P,F-69424 LYON 03,FRANCE

来源：

VIROLOGY | 1997年 / 234卷 / 02期

关键词：

D O I：

10.1006/viro.1997.8665

中图分类号：

Q93 [微生物学];

学科分类号：

071005 ; 100705 ;

摘要：

To better understand the role of specific residues within the duck hepatitis B virus (DHBV) pre-S protein in neutralization and infectivity, we have selected and identified pre-S variants which escape neutralization. A highly neutralizing monoclonal antibody (Mab 900) which recognizes an epitope (83)IPQPQWTP(90) localized previously on the DHBV pre-S protein, within a region suspected to mediate the virus interaction with hepatocytes, was used as immune pressure. After only two in vivo neutralization rounds with Mab 900, five different pre-S mutant genomes were identified, which harbored point mutations affecting only proline residues located at position 90 within this epitope ((83)IPQPQWTP(90)) and/or at a distance at position 5. We have shown that a single (P5L) or double proline (P5L + P90H) substitution affect neither virus replication capacity nor in vivo infectivity. However, the P5 mutation reduces mutant recognition by Mab 900 twofold, while the substitution of both prolines 5 and 90 almost completely abolishes mutant P5L + P90H reactivity with this Mab and leads to a decrease of neutralization. Therefore we describe here an experimental system which allows rapid in vivo selection and identification of DHBV pre-S variants and provide evidence that residues within and at a distance from the neutralization epitope are important in DHBV neutralization but do not affect its replication capacity and infectivity. (C) 1997 Academic Press.

引用

页码：291 / 299

页数：9

共 29 条

[1]

BROWN F, 1990, PICOMAVIRUSES, V2

[2] 2 REGIONS OF AN AVIAN HEPADNAVIRUS RNA PREGENOME ARE REQUIRED IN CIS FOR ENCAPSIDATION [J].

CALVERT, J ;

SUMMERS, J .

JOURNAL OF VIROLOGY, 1994, 68 (04) :2084-2090

[3] 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

[4] FINE MAPPING OF NEUTRALIZATION EPITOPES ON DUCK HEPATITIS-B VIRUS (DHBV) PRE-S-PROTEIN USING MONOCLONAL-ANTIBODIES AND OVERLAPPING PEPTIDES [J].

CHASSOT, S ;

LAMBERT, V ;

KAY, A ;

GODINOT, C ;

ROUX, B ;

TREPO, C ;

COVA, L .

VIROLOGY, 1993, 192 (01) :217-223

[5] EPITOPE MAPPING OF NEUTRALIZING MONOCLONAL-ANTIBODIES AGAINST DUCK HEPATITIS-B VIRUS [J].

CHEUNG, RC ;

ROBINSON, WS ;

MARION, PL ;

GREENBERG, HB .

JOURNAL OF VIROLOGY, 1989, 63 (06) :2445-2451

[6] EFFICIENT DUCK HEPATITIS-B VIRUS PRODUCTION BY AN AVIAN LIVER-TUMOR CELL-LINE [J].

CONDREAY, LD ;

ALDRICH, CE ;

COATES, L ;

MASON, WS ;

WU, TT .

JOURNAL OF VIROLOGY, 1990, 64 (07) :3249-3258

[7] EVIDENCE FOR THE PRESENCE OF DUCK HEPATITIS-B VIRUS IN WILD MIGRATING DUCKS [J].

COVA, L ;

LAMBERT, V ;

CHEVALLIER, A ;

HANTZ, O ;

FOUREL, I ;

JACQUET, C ;

PICHOUD, C ;

BOULAY, J ;

CHOMEL, B ;

VITVITSKI, L ;

TREPO, C .

JOURNAL OF GENERAL VIROLOGY, 1986, 67 :537-547

[8] DUCK HEPATITIS-B VIRUS-INFECTION, AFLATOXIN B-1 AND LIVER-CANCER IN DOMESTIC CHINESE DUCKS [J].

COVA, L ;

MEHROTRA, R ;

WILD, CP ;

CHUTIMATAEWIN, S ;

CAO, SF ;

DUFLOT, A ;

PRAVE, M ;

YU, SZ ;

MONTESANO, R ;

TREPO, C .

BRITISH JOURNAL OF CANCER, 1994, 69 (01) :104-109

[9] MECHANISMS OF NEUTRALIZATION OF ANIMAL VIRUSES [J].

DIMMOCK, NJ .

JOURNAL OF GENERAL VIROLOGY, 1984, 65 (JUN) :1015-1022

[10]

Dimmock NJ, 1993, NEUTRALIZATION ANIMA

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