MOLECULAR DESIGN AND CHEMICAL SYNTHESIS OF POTENT ENEDIYNES .2. DYNEMICIN MODEL SYSTEMS EQUIPPED WITH C-3 TRIGGERING DEVICES AND EVIDENCE FOR QUINONE METHIDE FORMATION IN THE MECHANISM OF ACTION OF DYNEMICIN-A

被引：95

作者：

NICOLAOU, KC ^{[1
]}

DAI, WM ^{[1
]}

机构：

[1] UNIV CALIF SAN DIEGO, DEPT CHEM, LA JOLLA, CA 92093 USA

来源：

JOURNAL OF THE AMERICAN CHEMICAL SOCIETY | 1992年 / 114卷 / 23期

关键词：

D O I：

10.1021/ja00049a023

中图分类号：

O6 [化学];

学科分类号：

0703 ;

摘要：

Continuing the theme of the preceding article, this paper describes the synthesis and chemical properties of designed enediynes related to dynemicin A. These model systems are equipped with triggering devices at C-3 of the aromatic nucleus. The design of these compounds (1 and 2) was based on the hypothesis that a C-3 phenolic group generated in situ would be capable of promoting epoxide opening and subsequent Bergman cycloaromatization according to the dynemicin A cascade. Compound 1 carrying a tert-butyl ester group at C-3 was synthesized from quinoline derivative 28 via the sequence 28 --> 36 --> 45 --> 46 --> 47 --> 48 --> 44 --> 49 --> 50 --> 1. Compound 2 carrying the photoremovable (2-nitrobenzyl)oxy group at C-3 was constructed from quinoline 29 by a similar sequence. Exposure of 1 and 49 to aqueous LiOH in EtOH led to Bergman cycloaromatization products 58 and 57, respectively. Compounds 2 and 62 bearing the 2-nitrobenzyl group at C-3 were photolytically converted to free phenolic systems 63 and 64, respectively. Reaction of 63 and 64 with the nucleophiles EtOH, EtSH, or nPrNH2 under anaerobic conditions in basic buffer solutions led to aromatized products 66-70. Exposure of 63 and 75, on the other hand, with EtOH under aerobic conditions in basic buffer solutions furnished the novel quinone methide epoxide systems 71 and 76-77, respectively. The chemistry of compounds 63 and 64 combined with their DNA-cleaving capabilities provides support for the quinone methide mechanism of action of dynemicin A.

引用

页码：8908 / 8921

页数：14

共 25 条

[1] REACTIVE 1,4-DEHYDROAROMATICS [J].

BERGMAN, RG .

ACCOUNTS OF CHEMICAL RESEARCH, 1973, 6 (01) :25-31

[2]

Fujita E., 1989, ADV HETEROCYCL CHEM, V45, P1

[3]

GANDIANO G, 1990, J AM CHEM SOC, V112, P9423

[4] PARA BENZYNE - GENERATION AS AN INTERMEDIATE IN A THERMAL ISOMERIZATION REACTION AND TRAPPING EVIDENCE FOR 1,4-BENZENEDIYL STRUCTURE [J].

JONES, RR ;

BERGMAN, RG .

JOURNAL OF THE AMERICAN CHEMICAL SOCIETY, 1972, 94 (02) :660-&

[5] CLEAVAGE OF T-BUTYLDIMETHYLSILYL ETHERS WITH BORON-TRIFLUORIDE ETHERATE [J].

KELLY, DR ;

ROBERTS, SM ;

NEWTON, RF .

SYNTHETIC COMMUNICATIONS, 1979, 9 (04) :295-299

[6] THE DYNEMICIN DNA INTERCALATION COMPLEX - A MODEL BASED ON DNA AFFINITY CLEAVAGE AND MOLECULAR-DYNAMICS SIMULATION [J].

LANGLEY, DR ;

DOYLE, TW ;

BEVERIDGE, DL .

JOURNAL OF THE AMERICAN CHEMICAL SOCIETY, 1991, 113 (12) :4395-4403

[7] CALICHEAMICINS - DISCOVERY, STRUCTURE, CHEMISTRY, AND INTERACTION WITH DNA [J].

LEE, MD ;

ELLESTAD, GA ;

BORDERS, DB .

ACCOUNTS OF CHEMICAL RESEARCH, 1991, 24 (08) :235-243

[8] KINETIC EVIDENCE FOR THE FORMATION OF DISCRETE 1,4-DEHYDROBENZENE INTERMEDIATES - TRAPPING BY INTERMOLECULAR AND INTRAMOLECULAR HYDROGEN-ATOM TRANSFER AND OBSERVATION OF HIGH-TEMPERATURE CIDNP [J].

LOCKHART, TP ;

COMITA, PB ;

BERGMAN, RG .

JOURNAL OF THE AMERICAN CHEMICAL SOCIETY, 1981, 103 (14) :4082-4090

[9] EVIDENCE FOR THE REACTIVE SPIN STATE OF 1,4-DEHYDROBENZENES [J].

LOCKHART, TP ;

BERGMAN, RG .

JOURNAL OF THE AMERICAN CHEMICAL SOCIETY, 1981, 103 (14) :4091-4096

[10] SYNTHETIC AND MECHANISTIC STUDIES ON ESPERAMICIN-A1 AND CALICHEAMICIN-GAMMA-1 - MOLECULAR STRAIN RATHER THAN PI-BOND PROXIMITY DETERMINES THE CYCLOAROMATIZATION RATES OF BICYCLO[7.3.1] ENEDIYNES [J].

MAGNUS, P ;

FORTT, S ;

PITTERNA, T ;

SNYDER, JP .

JOURNAL OF THE AMERICAN CHEMICAL SOCIETY, 1990, 112 (12) :4986-4987

← 1 2 3 →