SUPPRESSION OF MYC, BUT NOT E1A, TRANSFORMATION ACTIVITY BY MAX-ASSOCIATED PROTEINS, MAD AND MXI1

被引：130

作者：

LAHOZ, EG ^{[1
]}

XU, L ^{[1
]}

SCHREIBERAGUS, N ^{[1
]}

DEPINHO, RA ^{[1
]}

机构：

[1] YESHIVA UNIV ALBERT EINSTEIN COLL MED, DEPT MED, BRONX, NY 10461 USA

来源：

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA | 1994年 / 91卷 / 12期

关键词：

D O I：

10.1073/pnas.91.12.5503

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：

Mad and Mxi1, two members of the Myc-related basic-region helix-loop-helix/leucine-zipper family of proteins, associate directly with Max to form sequence-specific DNA binding heterodimers that are transactivation-incompetent. Mad-Max complexes have been shown to exert a strong repressive effect on Myc-induced transactivation, perhaps through the competitive occupation of common promoter binding sites also recognized by active Myc-Max heterodimers. To place these recent biochemical observations in a biological context, mad and mxi1 expression vectors were tested for their ability to influence Myc transformation activity in the rat embryo fibroblast cooperation assay. Addition of an equimolar amount of mad or mxi1 expression vector to mouse c-myc/ras cotransfections resulted in a dramatic reduction in both the number of foci generated and the severity of the malignant phenotype. Myc-specific suppression by Mad and Mxi1 was demonstrated by their ability to affect c- and N-myc-, but not ela-, induced transformation. In contrast, mad and mxi1 expression constructs bearing deletions in the basic region exerted only mild repressive effects on Myc transformation activity, suggesting that occupation of common DNA binding sites by transactivation-incompetent Mad-Max or Mxi1-Max complexes appears to play a more dominant role in this suppression than titration of limited intracellular pools of Max away from active Myc-Max complexes. Thus, these biological data support a current model for regulation of Myc function in which relative intracellular levels of Mad and Mxi1 in comparison to those of Myc may determine the degree of activation of Myc-responsive growth pathways.

引用

页码：5503 / 5507

页数：5

共 47 条

[31]

MORGENBESSER SD, 1994, SEMIN CANCER BIOL, V5, P21

[32] MYC FAMILY ONCOPROTEINS FUNCTION THROUGH A COMMON PATHWAY TO TRANSFORM NORMAL-CELLS IN CULTURE - CROSS-INTERFERENCE BY MAX AND TRANS-ACTING DOMINANT MUTANTS [J].

MUKHERJEE, B ;

MORGENBESSER, SD ;

DEPINHO, RA .

GENES & DEVELOPMENT, 1992, 6 (08) :1480-1492

[33] METHYLATION-SENSITIVE SEQUENCE-SPECIFIC DNA-BINDING BY THE C-MYC BASIC REGION [J].

PRENDERGAST, GC ;

ZIFF, EB .

SCIENCE, 1991, 251 (4990) :186-189

[34] ASSOCIATION OF MYN, THE MURINE HOMOLOG OF MAX, WITH C-MYC STIMULATES METHYLATION-SENSITIVE DNA-BINDING AND RAS COTRANSFORMATION [J].

PRENDERGAST, GC ;

LAWE, D ;

ZIFF, EB .

CELL, 1991, 65 (03) :395-407

[35] BIPHASIC EFFECT OF MAX ON MYC COTRANSFORMATION ACTIVITY AND DEPENDENCE ON AMINO-TERMINAL AND CARBOXY-TERMINAL MAX FUNCTIONS [J].

PRENDERGAST, GC ;

HOPEWELL, R ;

GORHAM, BJ ;

ZIFF, EB .

GENES & DEVELOPMENT, 1992, 6 (12A) :2429-2439

[36] COMPLEMENTATION OF TRANSFORMING DOMAINS IN E1A/MYC CHIMERAS [J].

RALSTON, R .

NATURE, 1991, 353 (6347) :866-868

[37] DEVELOPMENTAL CONTROL OF A PROMOTER-SPECIFIC FACTOR THAT IS ALSO REGULATED BY THE E1A GENE-PRODUCT [J].

REICHEL, R ;

KOVESDI, I ;

NEVINS, JR .

CELL, 1987, 48 (03) :501-506

[38] INCREASED EXPRESSION OF EUKARYOTIC TRANSLATION INITIATION-FACTORS EIF-4E AND EIF-2-ALPHA IN RESPONSE TO GROWTH INDUCTION BY C-MYC [J].

ROSENWALD, IB ;

RHOADS, DB ;

CALLANAN, LD ;

ISSELBACHER, KJ ;

SCHMIDT, EV .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1993, 90 (13) :6175-6178

[39] DIRECT ROLE FOR MYC IN TRANSCRIPTION INITIATION MEDIATED BY INTERACTIONS WITH TFII-I [J].

ROY, AL ;

CARRUTHERS, C ;

GUTJAHR, T ;

ROEDER, RG .

NATURE, 1993, 365 (6444) :359-361

[40] COMPARATIVE-ANALYSIS OF THE EXPRESSION AND ONCOGENIC ACTIVITIES OF XENOPUS C-MYC, N-MYC, AND L-MYC HOMOLOGS [J].

SCHREIBERAGUS, N ;

TORRES, R ;

HORNER, J ;

LAU, A ;

JAMRICH, M ;

DEPINHO, RA .

MOLECULAR AND CELLULAR BIOLOGY, 1993, 13 (04) :2456-2468

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