DEFINING FUNCTIONAL DRUG-INTERACTION DOMAINS ON TOPOISOMERASE-II BY EXPLOITING MECHANISTIC DIFFERENCES BETWEEN DRUG CLASSES

被引：26

作者：

OSHEROFF, N

CORBETT, AH

ELSEA, SH

WESTERGAARD, M

机构：

[1] Department of Biochemistry, Vanderbilt University School of Medicine, Nashville, 37232-0146, TN

来源：

CANCER CHEMOTHERAPY AND PHARMACOLOGY | 1994年 / 34卷

关键词：

DRUG-INTERACTION DOMAINS; TOPOISOMERASE II; DNA STRAND-BREAK; DNA STRAND-PASSAGE;

D O I：

10.1007/BF00684859

中图分类号：

R73 [肿瘤学];

学科分类号：

100214 ;

摘要：

Topoisomerase II is the primary cellular target for a variety of antineoplastic drugs that are active against human cancers. These drugs exert their cytotoxic effects by stabilizing covalent topoisomerase II-cleaved DNA complexes that are fleeting intermediates in the catalytic cycle of the enzyme. Despite this common feature of drug action, a number of mechanistic differences between drug classes have been described. These mechanistic differences (in eluding effects on DNA cleavage/religation, DNA strand passage, and adenosine triphosphate hydrolysis) were used as the basis for a series of competition experiments to determine whether different compounds share a common site of action on topoisomerase II or interact at distinct sites. Results of the present study strongly suggest that at least four structurally disparate antineoplastic drugs, etoposide, amsacrine, genistein, and the quinolone CP-115,953, share an overlapping interaction domain on the enzyme.

引用

页码：S19 / S25

页数：7

共 8 条

[1] EXPLOITING MECHANISTIC DIFFERENCES BETWEEN DRUG CLASSES TO DEFINE FUNCTIONAL-DRUG INTERACTION DOMAINS ON TOPOISOMERASE-II - EVIDENCE THAT SEVERAL DIVERSE DNA CLEAVAGE-ENHANCING AGENTS SHARE A COMMON SITE OF ACTION ON THE ENZYME
CORBETT, AH
HONG, D
OSHEROFF, N
JOURNAL OF BIOLOGICAL CHEMISTRY, 1993, 268 (19) : 14394 - 14398
[2] EFFECTS OF TOPOISOMERASE-II-TARGETED DRUGS ON ENZYME-MEDIATED DNA CLEAVAGE AND ATP HYDROLYSIS - EVIDENCE FOR DISTINCT DRUG-INTERACTION DOMAINS ON TOPOISOMERASE-II
ROBINSON, MJ
CORBETT, AH
OSHEROFF, N
BIOCHEMISTRY, 1993, 32 (14) : 3638 - 3643
[3] Topoisomerase II-drug interaction domains: Identification of substituents on etoposide that interact with the enzyme
Wilstermann, Amy M.
Bender, Ryan P.
Godfrey, Murrell
Choi, Sungjo
Anklin, Clemens
Berkowitz, David B.
Osheroff, Neil
Graves, David E.
BIOCHEMISTRY, 2007, 46 (28) : 8217 - 8225
[4] STRUCTURE AND BIOLOGICAL-ACTIVITY OF N-SUBSTITUTED ANTHRACYCLINES - CORRELATION WITH DRUG-DNA TOPOISOMERASE-II INTERACTION
POTMESIL, M
ISRAEL, M
SESHADRI, R
SWEATMAN, TW
KIRSCHENBAUM, S
SILBER, R
PROCEEDINGS OF THE AMERICAN ASSOCIATION FOR CANCER RESEARCH, 1987, 28 : 262 - 262
[5] DELETION AND DUPLICATION SEQUENCES INDUCED IN CHO CELLS BY TENIPOSIDE (VM-26), A TOPOISOMERASE-II TARGETING DRUG, CAN BE EXPLAINED BY THE PROCESSING OF DNA NICKS PRODUCED BY THE DRUG-TOPOISOMERASE INTERACTION
RIPLEY, LS
MUTATION RESEARCH, 1994, 312 (02): : 67 - 78
[6] TOPOISOMERASE-II ACTIVITY INVOLVED IN CLEAVING DNA INTO TOPOLOGICAL DOMAINS IS ALTERED IN A MULTIPLE DRUG-RESISTANT CHINESE-HAMSTER OVARY CELL-LINE
SULLIVAN, DM
ESKILDSEN, LA
GROOM, KR
WEBB, CD
LATHAM, MD
MARTIN, AW
WELLHAUSEN, SR
KROEGER, PE
ROWE, TC
MOLECULAR PHARMACOLOGY, 1993, 43 (02) : 207 - 216
[7] DRUG FEATURES THAT CONTRIBUTE TO THE ACTIVITY OF QUINOLONES AGAINST MAMMALIAN TOPOISOMERASE-II AND CULTURED-CELLS - CORRELATION BETWEEN ENHANCEMENT OF ENZYME-MEDIATED DNA CLEAVAGE IN-VITRO AND CYTOTOXIC POTENTIAL
ELSEA, SH
MCGUIRK, PR
GOOTZ, TD
MOYNIHAN, M
OSHEROFF, N
ANTIMICROBIAL AGENTS AND CHEMOTHERAPY, 1993, 37 (10) : 2179 - 2186
[8] Inhibition of cell cycle progression by a synthetic peptide corresponding to residues 65-79 of an HLA class II sequence: Functional similarities but mechanistic differences with the immunosuppressive drug rapamycin
Boytim, ML
Lyu, SC
Jung, R
Krensky, AM
Clayberger, C
JOURNAL OF IMMUNOLOGY, 1998, 160 (05): : 2215 - 2222

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