FUNCTION OF THE ADENOVIRUS E1B ONCOGENE IN INFECTED AND TRANSFORMED-CELLS

被引：25

作者：

WHITE, E

机构：

[1] Center for Advanced Biotechnology and Medicine, Department of Biological Sciences, Rutgers University, Piscataway, NJ 08854

来源：

SEMINARS IN VIROLOGY | 1994年 / 5卷 / 05期

关键词：

APOPTOSIS; P53; E1A; E1B; BCL-2;

D O I：

10.1006/smvy.1994.1038

中图分类号：

Q93 [微生物学];

学科分类号：

071005 ; 100705 ;

摘要：

Adenovirus infection and E1A gene expression stimulates cellular proliferation as a mechanism to facilitate virus replication. Programmed cell death (apoptosis) is the cellular response to this deregulation of growth control by E1A during viral infection and neoplastic transformation. To combat the suicidal elimination of virus infected cells by apoptosis, adenovirus has evolved a mechanism to disengage the apoptotic program of the cell. This anti-apoptotic function is encoded within the adenovirus E1B 19 kDa and 55 kDa gene products. Both viral products encoded by E1B act at independent and overlapping points in the cell death process to ensure that the premature death of the host cell does not take place and that viral infection can progress to completion. The E1B 55K protein functions as an anti-apoptotic gene product by direct physical interference with the p53 tumor suppressor protein, whereas the E1B 19K protein acts to inhibit p53-dependent and probably p53-independent apoptosis by a mechanism that resembles that of the human bcl-2 protooncogene.

引用

页码：341 / 348

页数：8

共 66 条

[1] ADENOVIRUS PROTEINS FROM BOTH E1B READING FRAMES ARE REQUIRED FOR TRANSFORMATION OF RODENT CELLS BY VIRAL-INFECTION AND DNA TRANSFECTION [J].

BARKER, DD ;

BERK, AJ .

VIROLOGY, 1987, 156 (01) :107-121

[2]

BERK AJ, 1986, ANNU REV GENET, V20, P5

[3] APOPTOTIC CELL-DEATH INDUCED BY C-MYC IS INHIBITED BY BCL-2 [J].

BISSONNETTE, RP ;

ECHEVERRI, F ;

MAHBOUBI, A ;

GREEN, DR .

NATURE, 1992, 359 (6395) :552-554

[4] DEFINITION OF ADENOVIRUS TYPE-5 FUNCTIONS INVOLVED IN THE INDUCTION OF CHROMOSOMAL-ABERRATIONS IN HUMAN-CELLS [J].

CAPOROSSI, D ;

BACCHETTI, S .

JOURNAL OF GENERAL VIROLOGY, 1990, 71 :801-808

[5] BCL-2 BLOCKS P53-DEPENDENT APOPTOSIS [J].

CHIOU, SK ;

RAO, L ;

WHITE, E .

MOLECULAR AND CELLULAR BIOLOGY, 1994, 14 (04) :2556-2563

[6]

CHIOU SK, 1994, IN PRESS J VIROL

[7] THYMOCYTE APOPTOSIS INDUCED BY P53-DEPENDENT AND INDEPENDENT PATHWAYS [J].

CLARKE, AR ;

PURDIE, CA ;

HARRISON, DJ ;

MORRIS, RG ;

BIRD, CC ;

HOOPER, ML ;

WYLLIE, AH .

NATURE, 1993, 362 (6423) :849-852

[8] CLONING AND STRUCTURAL-ANALYSIS OF CDNAS FOR BCL-2 AND A HYBRID BCL-2/IMMUNOGLOBULIN TRANSCRIPT RESULTING FROM THE T(14-18) TRANSLOCATION [J].

CLEARY, ML ;

SMITH, SD ;

SKLAR, J .

CELL, 1986, 47 (01) :19-28

[9] WILD-TYPE P53 MEDIATES APOPTOSIS BY E1A, WHICH IS INHIBITED BY E1B [J].

DEBBAS, M ;

WHITE, E .

GENES & DEVELOPMENT, 1993, 7 (04) :546-554

[10] P53 FUNCTIONS AS A CELL-CYCLE CONTROL PROTEIN IN OSTEOSARCOMAS [J].

DILLER, L ;

KASSEL, J ;

NELSON, CE ;

GRYKA, MA ;

LITWAK, G ;

GEBHARDT, M ;

BRESSAC, B ;

OZTURK, M ;

BAKER, SJ ;

VOGELSTEIN, B ;

FRIEND, SH .

MOLECULAR AND CELLULAR BIOLOGY, 1990, 10 (11) :5772-5781

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