Bax-independent inhibition of apoptosis by Bcl-x(L)

被引：429

作者：

Cheng, EHY

Levine, B

Boise, LH

Thompson, CB

Hardwick, JM

机构：

[1] COLUMBIA UNIV COLL PHYS & SURG,DEPT MED,NEW YORK,NY 10032

[2] UNIV CHICAGO,HOWARD HUGHES MED INST,CHICAGO,IL 60637

[3] UNIV CHICAGO,DEPT MED,CHICAGO,IL 60637

[4] UNIV CHICAGO,DEPT MOLEC GENET,CHICAGO,IL 60637

[5] UNIV CHICAGO,DEPT CELL BIOL,CHICAGO,IL 60637

来源：

NATURE | 1996年 / 379卷 / 6565期

关键词：

D O I：

10.1038/379554a0

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 Bcl-2-related protein, Bcl-x(L), has been shown to block apoptosis induced by a variety of stimuli(1-5) and to be a stronger protector against apoptosis than Bcl-2 under certain circumstances(2,5). Using site-specific mutagenesis, we show here that the amino-acid residues critical for protection of cells by Bcl-x(L) against Sindbis virus-induced apoptosis are clustered within the Bcl-2-homology regions 1 and 2 (BH1 and BH2 regions). The residues necessary for Bcl-x(L) function are not identical to those required for Bcl-2 function(6), Although it has been suggested that heterodimerization between Bcl-x(L) and Bax is essential for the anti death activity of Bcl-x(L) (refs 7, 8), our results suggest that the interaction with Bax is not required for Bcl-x(L) to exert its death-repressing activity, Specific mutations that disrupt the ability of Bcl-x(L) to interact with Bax or Bak still preserve 70-80% of the anti-death activity of wild-type Bcl-x(L).

引用

页码：554 / 556

页数：3

共 29 条

[21] DISAPPEARANCE OF THE LYMPHOID SYSTEM IN BCL-2 HOMOZYGOUS MUTANT CHIMERIC MICE
NAKAYAMA, K
NAKAYAMA, K
NEGISHI, I
KUIDA, K
SHINKAI, Y
LOUIE, MC
FIELDS, LE
LUCAS, PJ
STEWART, V
ALT, FW
LOH, DY
[J]. SCIENCE, 1993, 261 (5128) : 1584 - 1588
[22] BCL-2 HETERODIMERIZES IN-VIVO WITH A CONSERVED HOMOLOG, BAX, THAT ACCELERATES PROGRAMMED CELL-DEATH
OLTVAI, ZN
MILLIMAN, CL
KORSMEYER, SJ
[J]. CELL, 1993, 74 (04) : 609 - 619
[23] MULTIPLE BCL-2 FAMILY MEMBERS DEMONSTRATE SELECTIVE DIMERIZATIONS WITH BAX
SEDLAK, TW
OLTVAI, ZN
YANG, E
WANG, K
BOISE, LH
THOMPSON, CB
KORSMEYER, SJ
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1995, 92 (17) : 7834 - 7838
[24] PREVENTION OF HYPOXIA-INDUCED CELL-DEATH BY BCL-2 AND BCL-XL
SHIMIZU, S
EGUCHI, Y
KOSAKA, H
KAMIIKE, W
MATSUDA, H
TSUJIMOTO, Y
[J]. NATURE, 1995, 374 (6525) : 811 - 813
[25] TANAKA S, 1993, J BIOL CHEM, V268, P10920
[26] NEUROVIRULENT STRAINS OF ALPHAVIRUS INDUCE APOPTOSIS IN BCL-2-EXPRESSING CELLS - ROLE OF A SINGLE AMINO-ACID CHANGE IN THE E2 GLYCOPROTEIN
UBOL, S
TUCKER, PC
GRIFFIN, DE
HARDWICK, JM
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1994, 91 (11) : 5202 - 5206
[27] BCL-2-DEFICIENT MICE DEMONSTRATE FULMINANT LYMPHOID APOPTOSIS, POLYCYSTIC KIDNEYS, AND HYPOPIGMENTED HAIR
VEIS, DJ
SORENSON, CM
SHUTTER, JR
KORSMEYER, SJ
[J]. CELL, 1993, 75 (02) : 229 - 240
[28] BAD, A HETERODIMERIC PARTNER FOR BCL-X(L) AND BCL-2, DISPLACES BAX AND PROMOTES CELL-DEATH
YANG, E
ZHA, JP
JOCKEL, J
BOISE, LH
THOMPSON, CB
KORSMEYER, SJ
[J]. CELL, 1995, 80 (02) : 285 - 291
[29] BH1 AND BH2 DOMAINS OF BCL-2 ARE REQUIRED FOR INHIBITION OF APOPTOSIS AND HETERODIMERIZATION WITH BAX
YIN, XM
OLTVAI, ZN
KORSMEYER, SJ
[J]. NATURE, 1994, 369 (6478) : 321 - 323

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