REVERSAL OF RADIATION-INDUCED CISPLATIN RESISTANCE IN MURINE FIBROSARCOMA CELLS BY SELECTIVE MODULATION OF THE CYCLIC GMP-DEPENDENT TRANSDUCTION PATHWAY

被引：10

作者：

EICHHOLTZWIRTH, H ^{[1
]}

机构：

[1] GSF MUNICH,INST STRAHLENBIOL,D-85758 NEUHERBERG,GERMANY

来源：

BRITISH JOURNAL OF CANCER | 1995年 / 72卷 / 02期

关键词：

CISPLATIN RESISTANCE; GMP-DEPENDENT PROTEIN KINASE; IRRADIATION;

D O I：

10.1038/bjc.1995.326

中图分类号：

R73 [肿瘤学];

学科分类号：

100214 ;

摘要：

Cisplatin resistance, induced in murine fibrosarcoma cells (SSK) in vitro or in vivo by low-dose irradiation, can be overcome by activation of the cyclic GMP(cGMP)-dependent transduction pathway. This is mediated either by stimulating cGMP formation with sodium nitroprusside or by replacing cGMP with a selective activator of the cGMP-dependent protein kinase, 8-bromo-cGMP. The cyclic AMP-dependent transduction pathway is not involved in cisplatin resistance. Instead, activation of cAMP sensitises both parental and resistant SSK cells equally to the action of cisplatin. There is a 1.8 to 2.5-fold increase in drug toxicity, depending on the activating agent. Enhancement of cisplatin sensitivity is induced by specific inhibition of cAMP hydrolysis, increase in cAMP formation or by increasing the activation potential to cAMP-dependent protein kinase by specific cAMP analogues. Cells that have lost cisplatin resistance respond to cGMP- or cAMP-elevating agents in the same way as the parental SSK cells. The radiation sensitivity is unchanged in all cell lines, even after activation of cAMP or cGMP. These results suggest that specific DNA repair pathways are altered by radiation but affected only in cisplatin damage repair, which is regulated by cGMP. Although there is ample cooperativity and interaction between the cAMP- and the cGMP-dependent transduction pathways, specific substrate binding by cGMP appears to play an important role in radiation-induced cisplatin resistance.

引用

页码：287 / 292

页数：6

共 37 条

[1] CYCLIC AMP-DEPENDENT PROTEIN-KINASE REGULATES SENSITIVITY OF CELLS TO MULTIPLE-DRUGS [J].

ABRAHAM, I ;

HUNTER, RJ ;

SAMPSON, KE ;

SMITH, S ;

GOTTESMAN, MM ;

MAYO, JK .

MOLECULAR AND CELLULAR BIOLOGY, 1987, 7 (09) :3098-3106

[2] SELECTIVE MODULATION OF PROTEIN-KINASE ISOZYMES BY THE SITE-SELECTIVE ANALOG 8-CHLOROADENOSINE 3',5'-CYCLIC-MONOPHOSPHATE PROVIDES A BIOLOGICAL MEANS FOR CONTROL OF HUMAN-COLON CANCER CELL-GROWTH [J].

ALLY, S ;

TORTORA, G ;

CLAIR, T ;

GRIECO, D ;

MERLO, G ;

KATSAROS, D ;

OGREID, D ;

DOSKELAND, SO ;

JAHNSEN, T ;

CHOCHUNG, YS .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1988, 85 (17) :6319-6322

[3]

BASU A, 1992, CANCER RES, V52, P3119

[4] PRIMARY SEQUENCE OF CYCLIC-NUCLEOTIDE PHOSPHODIESTERASE ISOZYMES AND THE DESIGN OF SELECTIVE INHIBITORS [J].

BEAVO, JA ;

REIFSNYDER, DH .

TRENDS IN PHARMACOLOGICAL SCIENCES, 1990, 11 (04) :150-155

[5] ANALYSIS OF THE FUNCTIONAL-ROLE OF CGMP-DEPENDENT PROTEIN-KINASE IN INTACT HUMAN PLATELETS USING A SPECIFIC ACTIVATOR 8-PARA-CHLOROPHENYLTHIO-CGMP [J].

BUTT, E ;

NOLTE, C ;

SCHULZ, S ;

BELTMAN, J ;

BEAVO, JA ;

JASTORFF, B ;

WALTER, U .

BIOCHEMICAL PHARMACOLOGY, 1992, 43 (12) :2591-2600

[6]

CHAMPAGNE MMV, 1991, CANCER RES, V51, P1600

[7] IDENTIFICATION OF INDUCIBLE DAMAGE-RECOGNITION PROTEINS THAT ARE OVEREXPRESSED IN HELA-CELLS RESISTANT TO CIS-DIAMMINEDICHLOROPLATINUM(II) [J].

CHAO, CCK ;

HUANG, SL ;

LEE, LY ;

LINCHAO, S .

BIOCHEMICAL JOURNAL, 1991, 277 :875-878

[8]

CHOCHUNG YS, 1990, CANCER RES, V50, P7093

[9] IN-VITRO MODULATION OF CISPLATIN ACCUMULATION IN HUMAN OVARIAN-CARCINOMA CELLS BY PHARMACOLOGICAL ALTERATION OF MICROTUBULES [J].

CHRISTEN, RD ;

JEKUNEN, AP ;

JONES, JA ;

THIEBAUT, F ;

SHALINSKY, DR ;

HOWELL, SB .

JOURNAL OF CLINICAL INVESTIGATION, 1993, 92 (01) :431-440

[10]

CONOLLY BJ, 1992, BIOCHEM PHARMACOL, V44, P2303

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