Evidence supporting a signal transduction pathway leading to the radiation-resistant phenotype in human tumor cells

被引：66

作者：

Pirollo, KF ^{[1
]}

Hao, ZM ^{[1
]}

Rait, A ^{[1
]}

Ho, CW ^{[1
]}

Chang, EH ^{[1
]}

机构：

[1] STANFORD UNIV, MED CTR, DEPT SURG, DIV OTOLARYNGOL HEAD & NECK SURG, STANFORD, CA 94305 USA

来源：

BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS | 1997年 / 230卷 / 01期

关键词：

D O I：

10.1006/bbrc.1996.5922

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：

A signal transduction pathway, involving oncogenes and their normal counterparts the proto-oncogenes, analogous to that for cell growth and differentiation has been proposed to lead to the phenotype of cellular radioresistance (RR). In this report we provide evidence demonstrating the existence of such a pathway by using antisense oligonucleotides (ASO) to reverse the RR phenotype. Utilizing ASO directed against the raf-1 gene, a central component of this proposed pathway, we were able to reverse the RR phenotype of human tumor cell Lines having elevated HER-2 expression or a mutant form of Ha-ras, two genes upstream of raf-1 in signal transduction. Additionally, anti-ras ASO were able to radiosensitize HER-2 overexpressing cells. These results, which verify the presence of a signaling pathway leading to cellular RR, also have possible clinical implications for the use of ASO as a means to sensitize radioresistant tumors to radiation therapy. (C) 1997 Academic Press

引用

页码：196 / 201

页数：6

共 34 条

[1]

BROWN D, 1989, ONCOGENE RES, V4, P243

[2] EPIDERMAL GROWTH-FACTOR REGULATES P21(RAS) THROUGH THE FORMATION OF A COMPLEX OF RECEPTOR, GRB2 ADAPTER PROTEIN, AND SOS NUCLEOTIDE EXCHANGE FACTOR [J].

BUDAY, L ;

DOWNWARD, J .

CELL, 1993, 73 (03) :611-620

[3]

CAMPBELL JS, 1995, RECENT PROG HORM RES, V50, P131

[4] HEREGULIN ACTIVATION OF EXTRACELLULAR ACIDIFICATION IN MAMMARY-CARCINOMA CELLS IS ASSOCIATED WITH EXPRESSION OF HER2 AND HER3 [J].

CHAN, SDH ;

ANTONIUCCI, DM ;

FOK, KS ;

ALAJOKI, ML ;

HARKINS, RN ;

THOMPSON, SA ;

WADA, HG .

JOURNAL OF BIOLOGICAL CHEMISTRY, 1995, 270 (38) :22608-22613

[5]

CHANG EH, 1989, ANTI-CANCER DRUG DES, V4, P221

[6] ONCOGENES IN RADIORESISTANT, NONCANCEROUS SKIN FIBROBLASTS FROM A CANCER-PRONE FAMILY [J].

CHANG, EH ;

PIROLLO, KF ;

ZHI, QZ ;

CHEUNG, HY ;

LAWLER, EL ;

GARNER, R ;

WHITE, E ;

BERNSTEIN, WB ;

FRAUMENI, JW ;

BLATTNER, WA .

SCIENCE, 1987, 237 (4818) :1036-1039

[7] ANTISENSE INHIBITION OF RAS P21 EXPRESSION THAT IS SENSITIVE TO A POINT MUTATION [J].

CHANG, EH ;

MILLER, PS ;

CUSHMAN, C ;

DEVADAS, K ;

PIROLLO, KF ;

TSO, POP ;

YU, ZP .

BIOCHEMISTRY, 1991, 30 (34) :8283-8286

[8] THE INS AND OUTS OF RAF KINASES [J].

DAUM, G ;

EISENMANNTAPPE, I ;

FRIES, HW ;

TROPPMAIR, J ;

RAPP, UR .

TRENDS IN BIOCHEMICAL SCIENCES, 1994, 19 (11) :474-480

[9] THE MAMMALIAN ULTRAVIOLET RESPONSE IS TRIGGERED BY ACTIVATION OF SRC TYROSINE KINASES [J].

DEVARY, Y ;

GOTTLIEB, RA ;

SMEAL, T ;

KARIN, M .

CELL, 1992, 71 (07) :1081-1091

[10] A SINGLE AMINO-ACID CHANGE IN RAF-1 INHIBITS RAS BINDING AND ALTERS RAF-1 FUNCTION [J].

FABIAN, JR ;

VOJTEK, AB ;

COOPER, JA ;

MORRISON, DK .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1994, 91 (13) :5982-5986

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