NMR AND MOLECULAR MODELING INVESTIGATION OF THE MECHANISM OF ACTIVATION OF THE ANTITUMOR DRUG TEMOZOLOMIDE AND ITS INTERACTION WITH DNA

被引：354

作者：

DENNY, BJ

WHEELHOUSE, RT

STEVENS, MFG

TSANG, LLH

SLACK, JA

机构：

[1] UNIV NOTTINGHAM,DEPT PHARMACEUT SCI,CANC RES LABS,CANC RES CAMPAIGN,EXPTL CANC CHEMOTHERAPY GRP,NOTTINGHAM NG7 2RD,ENGLAND

[2] UNIV ASTON,INST PHARMACEUT SCI,BIRMINGHAM B4 7ET,W MIDLANDS,ENGLAND

来源：

BIOCHEMISTRY | 1994年 / 33卷 / 31期

关键词：

D O I：

10.1021/bi00197a003

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 hypothesis that the antitumor prodrug temozolomide is ring-opened to MTIC which then further breaks down to a reactive diazonium ion at guanine-rich sequences in DNA has been probed by NMR spectroscopy and computational techniques. Temozolomide is stable at acid pH but decomposes to MTIC at pH > 7; in contrast, MTIC is stable at alkaline pH values but rapidly fragments in a methylating mode at pH < 7. The proximate methylating agent is the reactive methyldiazonium species. Runs of guanine residues represent an accessible nucleophilic microenvironment in DNA which would facilitate the site-specific conversion of the prodrug temozolomide to MTIC possibly via an activated water molecule in the major groove. Molecular modeling of the structure of temozolomide indicates that the prodrug can make a favorable noncovalent encounter with DNA. The known structure-activity relationships as well as the biological and clinical properties of temozolomide can be interpreted in terms of this model.

引用

页码：9045 / 9051

页数：7

共 33 条

[1] CHARGE CALCULATIONS IN MOLECULAR MECHANICS .6. THE CALCULATION OF PARTIAL ATOMIC CHARGES IN NUCLEIC-ACID BASES AND THE ELECTROSTATIC CONTRIBUTION TO DNA-BASE PAIRING
ABRAHAM, RJ
SMITH, PE
[J]. NUCLEIC ACIDS RESEARCH, 1988, 16 (06) : 2639 - 2657
[2] ARNOTT S, 1983, NUCLEIC ACIDS RES, V11, P4145
[3] DEPLETION OF O6-ALKYLGUANINE-DNA ALKYLTRANSFERASE CORRELATES WITH POTENTIATION OF TEMOZOLOMIDE AND CCNU TOXICITY IN HUMAN TUMOR-CELLS
BAER, JC
FREEMAN, AA
NEWLANDS, ES
WATSON, AJ
RAFFERTY, JA
MARGISON, GP
[J]. BRITISH JOURNAL OF CANCER, 1993, 67 (06) : 1299 - 1302
[4] Black T. H., 1983, ALDRICHIM ACTA, V16, P3
[5] THE MECHANISM OF DECOMPOSITION OF N-METHYL-N-NITROSOUREA IN AQUEOUS-SOLUTION ACCORDING TO C-13 AND N-15 NMR-STUDIES - QUANTITATIVE FRAGMENTATION TO CYANATE
BLEASDALE, C
GOLDING, BT
MCGINNIS, J
MULLER, S
WATSON, WP
[J]. JOURNAL OF THE CHEMICAL SOCIETY-CHEMICAL COMMUNICATIONS, 1991, (24) : 1726 - 1728
[6] CITRON M, 1991, CANCER RES, V51, P4131
[7] CLARK AS, 1990, ANTI-CANCER DRUG DES, V5, P63
[8] GIBSON NW, 1984, CANCER RES, V44, P1772
[9] GIBSON NW, 1988, CARCINOGENESIS, V9, P669
[10] ANTITUMOR IMIDAZOTETRAZINES .20. PREPARATION OF THE 8-ACID DERIVATIVE OF MITOZOLOMIDE AND ITS UTILITY IN THE PREPARATION OF ACTIVE ANTITUMOR AGENTS
HORSPOOL, KR
STEVENS, MFG
NEWTON, CG
LUNT, E
WALSH, RJA
PEDGRIFT, BL
BAIG, GU
LAVELLE, F
FIZAMES, C
[J]. JOURNAL OF MEDICINAL CHEMISTRY, 1990, 33 (05) : 1393 - 1399

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