A PEPTIDE FROM THE GAP-BINDING DOMAIN OF THE RAS-P21 PROTEIN AS WELL AS AZATYROSINE BLOCK RAS-INDUCED MATURATION OF XENOPUS-OOCYTES

被引：15

作者：

CHUNG, DL

BRANDTRAUF, P

MURPHY, RB

NISHIMURA, S

YAMAIZUMI, Z

WEINSTEIN, IB

PINCUS, MR

机构：

[1] SUNY HLTH SCI CTR,DEPT PATHOL,750 E ADAMS ST,SYRACUSE,NY 13210

[2] NYU,DEPT CHEM,NEW YORK,NY 10003

[3] NYU,CTR NEURAL SCI,NEW YORK,NY 10003

[4] COLUMBIA UNIV COLL PHYS & SURG,DIV ENVIRONM SCI,NEW YORK,NY 10032

[5] NATL CANC CTR,RES INST,TOKYO 104,JAPAN

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

[7] COLUMBIA UNIV COLL PHYS & SURG,CTR COMPREHENS CANC,NEW YORK,NY 10032

来源：

BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS | 1991年 / 181卷 / 03期

关键词：

D O I：

10.1016/0006-291X(91)92091-W

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

The ras-oncogene-encoded p21 protein is known to produce malignant transmation of NIH 3T3 cells as well as maturation of Xenopus oocytes when microinjected into these cells. p21 protein is known to bind a GTPase activating protein (GAP) intracellularly; residues 32-45 have been implicated in interacting with GAP. We demonstrate here that a peptide corresponding to residues 35-47 of p21 as well as the antibiotic azatyrosine inhibit the ras-induced maturation of Xenopus oocytes in a dose-related manner upon microinjection. We have previously shown that this p21 peptide and azatyrosine could inhibit the effects of p21 protein on cell transformation and pinocytosis in NIH 3T3 cells. In the present study, in which we have extended these results to the oocyte system, we also demonstrate that both partially inhibit insulin-induced oocyte maturation, a process which is thought to involve activation of endogenous p21 protein; on the other hand, both agents fail to inhibit oocyte maturation induced by progesterone, which is known not to act through p21 protein activation. Control studies with other peptides and tyrosine analogues support the selective nature of these events. These results suggest that both the p21-related peptide and azatyrosine have potent anti-ras effects intracellularly. © 1991.

引用

页码：1378 / 1384

页数：7

共 16 条

[1] GUANOSINE TRIPHOSPHATASE ACTIVATING PROTEIN (GAP) INTERACTS WITH THE P21-RAS EFFECTOR BINDING DOMAIN
ADARI, H
LOWY, DR
WILLUMSEN, BM
DER, CJ
MCCORMICK, F
[J]. SCIENCE, 1988, 240 (4851) : 518 - 520
[2] RAS GENES
BARBACID, M
[J]. ANNUAL REVIEW OF BIOCHEMISTRY, 1987, 56 : 779 - 827
[3] INDUCTION OF MEMBRANE RUFFLING AND FLUID-PHASE PINOCYTOSIS IN QUIESCENT FIBROBLASTS BY RAS PROTEINS
BARSAGI, D
FERAMISCO, JR
[J]. SCIENCE, 1986, 233 (4768) : 1061 - 1068
[4] CHUNG DL, 1991, IN PRESS ANTICANCER
[5] EXPRESSION OF GENE-RRG IS ASSOCIATED WITH REVERSION OF NIH 3T3 TRANSFORMED BY LTR-C-H-RAS
CONTENTE, S
KENYON, K
RIMOLDI, D
FRIEDMAN, RM
[J]. SCIENCE, 1990, 249 (4970) : 796 - 798
[6] INSULIN INDUCTION OF XENOPUS-LAEVIS OOCYTE MATURATION IS INHIBITED BY MONOCLONAL-ANTIBODY AGAINST P21 RAS PROTEINS
DESHPANDE, AK
KUNG, HF
[J]. MOLECULAR AND CELLULAR BIOLOGY, 1987, 7 (03) : 1285 - 1288
[7] ACTIVATED N-RAS GENE INDUCES NEURONAL DIFFERENTIATION OF PC12 RAT PHEOCHROMOCYTOMA CELLS
GUERRERO, I
WONG, H
PELLICER, A
BURSTEIN, DE
[J]. JOURNAL OF CELLULAR PHYSIOLOGY, 1986, 129 (01) : 71 - 76
[8] STRUCTURAL RELAXATION BEHAVIOR AND MECHANICAL-PROPERTIES OF WARM-DRAWN FE75SI10B15 AND PD75NI8.5SI16.5 AMORPHOUS WIRES
INOUE, A
YANO, N
CHEN, HS
HAGIWARA, M
MASUMOTO, T
[J]. MATERIALS SCIENCE AND ENGINEERING, 1986, 77 (1-2): : 45 - 57
[9] IDENTIFICATION OF AN INTRACELLULAR PROTEIN THAT SPECIFICALLY INTERACTS WITH PHOTOAFFINITY-LABELED ONCOGENIC P21 PROTEIN
LEE, G
RONAI, ZA
PINCUS, MR
BRANDTRAUE, PW
MURPHY, RB
DELOHERY, TM
NISHIMURA, S
YAMAIZUMI, Z
WEINSTEIN, IB
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1989, 86 (22) : 8678 - 8682
[10] LEE G, 1990, Medical Science Research, V18, P771

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