The hepatitis B virus X gene induces p53-mediated programmed cell death

被引：185

作者：

Chirillo, P

Pagano, S

Natoli, G

Puri, PL

Burgio, VL

Balsano, C

Levrero, M

机构：

[1] UNIV ROMA LA SAPIENZA,GENE EXPRESS LAB,FDN ANDREA CESALPINO,IST CLIN MED 1,POLICLIN UMBERTO I,I-00161 ROME,ITALY

[2] UNIV AQUILA,DIPARTIMENTO MED INTERNA,I-67100 LAQUILA,ITALY

[3] UNIV CAGLIARI,IST MED INTERNA,I-60281 CAGLIARI,ITALY

来源：

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA | 1997年 / 94卷 / 15期

关键词：

D O I：

10.1073/pnas.94.15.8162

中图分类号：

O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];

学科分类号：

07 ; 0710 ; 09 ;

摘要：

The human hepatitis B virus (HBV) protein pX is a multifunctional regulatory protein that is known to affect both transcription and cell growth. Here we describe induction of apoptosis in NIH 3T3 polyclonal cell lines upon stimulation of pX expression from a dexamethasone inducible mouse mammary tumor virus (MMTV)-X expression vector, The effect of long-term pX expression on the cell survival of mouse fibroblasts was confirmed in colony generation assays, This effect is not shared either by the other HBV products and it is c-myc mediated, as shown by the use of a dominant negative deletion mutant of c-myc. pX also sensitize cells to programmed cell death after exposure to DNA damaging agents, Taking advantage of stable transfectants carrying the p53val135 temperature-sensitive allele, we directly demonstrate that induction of apoptosis by pX requires p53, In p53 null mouse embryo fibroblasts pX activates transcription and confers an evident growth advantage without loss of cell viability, Although pX protein was not detectable in the experimental conditions we used, our results Indicate that its expression affects both cell growth and cell death control.

引用

页码：8162 / 8167

页数：6

共 51 条

[21] MALIGNANT TRANSFORMATION OF IMMORTALIZED TRANSGENIC HEPATOCYTES AFTER TRANSFECTION WITH HEPATITIS-B VIRUS-DNA [J].

HOHNE, M ;

SCHAEFER, S ;

SEIFER, M ;

FEITELSON, MA ;

PAUL, D ;

GERLICH, WH .

EMBO JOURNAL, 1990, 9 (04) :1137-1145

[22] 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

[23] EXPRESSION OF TRANSCRIPTION FACTOR E2F1 INDUCES QUIESCENT CELLS TO ENTER S-PHASE [J].

JOHNSON, DG ;

SCHWARZ, JK ;

CRESS, WD ;

NEVINS, JR .

NATURE, 1993, 365 (6444) :349-352

[24] HEPATITIS-B VIRUS TRANSACTIVATOR HBX USES A TUMOR PROMOTER SIGNALING PATHWAY [J].

KEKULE, AS ;

LAUER, U ;

WEISS, L ;

LUBER, B ;

HOFSCHNEIDER, PH .

NATURE, 1993, 361 (6414) :742-745

[25] THE PRES2/S REGION OF INTEGRATED HEPATITIS-B VIRUS-DNA ENCODES A TRANSCRIPTIONAL TRANSACTIVATOR [J].

KEKULE, AS ;

LAUER, U ;

MEYER, M ;

CASELMANN, WH ;

HOFSCHNEIDER, PH ;

KOSHY, R .

NATURE, 1990, 343 (6257) :457-461

[26] HBX GENE OF HEPATITIS-B VIRUS INDUCES LIVER-CANCER IN TRANSGENIC MICE [J].

KIM, CM ;

KOIKE, K ;

SAITO, I ;

MIYAMURA, T ;

JAY, G .

NATURE, 1991, 351 (6324) :317-320

[27] p53: Puzzle and paradigm [J].

Ko, LJ ;

Prives, C .

GENES & DEVELOPMENT, 1996, 10 (09) :1054-1072

[28] INDUCTION OF CELL-CYCLE PROGRESSION BY HEPATITIS-B VIRUS HBX GENE-EXPRESSION IN QUIESCENT MOUSE FIBROBLASTS [J].

KOIKE, K ;

MORIYA, K ;

YOTSUYANAGI, H ;

LINO, S ;

KUROKAWA, K .

JOURNAL OF CLINICAL INVESTIGATION, 1994, 94 (01) :44-49

[29] HEPATITIS-B VIRUS X-PROTEIN INTERACTS WITH A PROBABLE CELLULAR DNA-REPAIR PROTEIN [J].

LEE, TH ;

ELLEDGE, SJ ;

BUTEL, JS .

JOURNAL OF VIROLOGY, 1995, 69 (02) :1107-1114

[30] P53-DEPENDENT APOPTOSIS MODULATES THE CYTOTOXICITY OF ANTICANCER AGENTS [J].

LOWE, SW ;

RULEY, HE ;

JACKS, T ;

HOUSMAN, DE .

CELL, 1993, 74 (06) :957-967

← 1 2 3 4 5 6 →