学术探索
学术期刊
新闻热点
数据分析
智能评审

Synthesis and antitumor activity of CBI-bearing ester and carbamate prodrugs of CC-1065 analogue

被引:23
作者
Wang, Yuqiang [1 ]
Li, Lianfa
Tian, Zhiming
Jiang, Wei
Larrick, James W.
机构
[1] Jinan Univ, Coll Pharm, Inst New Drug Res, Guangzhou 510632, Peoples R China
[2] Panorama Res Inc, Mountain View, CA 94043 USA
来源
BIOORGANIC & MEDICINAL CHEMISTRY | 2006年 / 14卷 / 23期
关键词
anticancer agents; CC-1065; prodrugs; DHA; ENHANCED FUNCTIONAL ANALOGS; LEFT-HAND SUBUNIT; ANTI-TUMOR AGENT; DUOCARMYCIN DERIVATIVES; DOCOSAHEXAENOIC ACID; PRELIMINARY TOXICITY; FATTY-ACID; IN-VITRO; DNA; NSC-298223;
D O I
10.1016/j.bmc.2006.07.062
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
Prodrugs of a CBI-bearing CC-1065 analogue were synthesized. Antitumor activity of the compounds was evaluated against tumor cells in vitro and in mouse tumor models. Compounds 1 and 7, bearing methylpiperazine and DHA moieties, respectively, showed significant antitumor activity in both the L 1210 leukemia and Lewis lung carcinoma mouse tumor models. For the carbamate prodrugs 1-4 and 6, there is a good correlation between the drug's potency both in vitro and in animal tumor models; however, there is no correlation between the prodrug's antitumor activity and the type of bonds linking the free drug. There are no significant differences between the antitumor activities of those that can or cannot be protonated at physiological pH. Compounds 6 and 7, each bearing a DHA moiety, did not show significantly improved antitumor activity compared to other prodrugs bearing DHA moieties, suggesting that DHA may not be used universally to significantly improve a drug's antitumor efficacy. (c) 2006 Elsevier Ltd. All rights reserved.
引用
收藏
页码:7854 / 7861
页数:8
相关论文
共 42 条
[1]   Synthesis and antitumor activity of duocarmycin derivatives:: A-ring pyrrole compounds bearing (β-(5′,6′,7′-trimethoxy-2′-indolyl)acryloyl group [J].
Amishiro, N ;
Nagamura, S ;
Kobayashi, E ;
Okamoto, A ;
Gomi, K ;
Okabe, M ;
Saito, H .
BIOORGANIC & MEDICINAL CHEMISTRY, 2000, 8 (07) :1637-1643
[2]   New water-soluble duocarmycin derivatives:: Synthesis and antitumor activity of A-ring pyrrole compounds bearing β-heteroarylacryloyl groups [J].
Amishiro, N ;
Nagamura, S ;
Kobayashi, E ;
Gomi, K ;
Saito, H .
JOURNAL OF MEDICINAL CHEMISTRY, 1999, 42 (04) :669-676
[3]   DOCOSAHEXAENOIC ACID IS THE PREFERRED DIETARY N-3 FATTY-ACID FOR THE DEVELOPMENT OF THE BRAIN AND RETINA [J].
ANDERSON, GJ ;
CONNOR, WE ;
CORLISS, JD .
PEDIATRIC RESEARCH, 1990, 27 (01) :89-97
[4]   SYNTHESIS OF CBI-PDE-I-DIMER, THE BENZANNELATED ANALOG OF CC-1065 [J].
ARISTOFF, PA ;
JOHNSON, PD .
JOURNAL OF ORGANIC CHEMISTRY, 1992, 57 (23) :6234-6239
[5]  
Aristoff PA., 1993, ADV MED CHEM, V2, P67
[6]  
BHUYAN BK, 1982, CANCER RES, V42, P3532
[7]   SYNTHESIS OF N-(TERT-BUTYLOXYCARBONYL)-CBI, CBI, CBI-CDPI1, AND CBI-CDPI2 - ENHANCED FUNCTIONAL ANALOGS OF CC-1065 INCORPORATING THE 1,2,9,9A-TETRAHYDROCYCLOPROPA[C]BENZ[E]INDOL-4-ONE (CBI) LEFT-HAND SUBUNIT [J].
BOGER, DL ;
ISHIZAKI, T ;
KITOS, PA ;
SUNTORNWAT, O .
JOURNAL OF ORGANIC CHEMISTRY, 1990, 55 (23) :5823-5832
[8]   RESOLUTION OF A CBI PRECURSOR AND INCORPORATION INTO THE SYNTHESIS OF (+)-CBI, (+)-CBI-CDPI1, (+)-CBI-CDPI2 - ENHANCED FUNCTIONAL ANALOGS OF (+)-CC-1065 - A CRITICAL-APPRAISAL OF A PROPOSED RELATIONSHIP BETWEEN ELECTROPHILE REACTIVITY, DNA-BINDING PROPERTIES, AND CYTOTOXIC POTENCY [J].
BOGER, DL ;
ISHIZAKI, T .
TETRAHEDRON LETTERS, 1990, 31 (06) :793-796
[9]   CC-1065 AND THE DUOCARMYCINS - UNRAVELING THE KEYS TO A NEW CLASS OF NATURALLY DERIVED DNA ALKYLATING-AGENTS [J].
BOGER, DL ;
JOHNSON, DS .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1995, 92 (09) :3642-3649
[10]   TOTAL SYNTHESIS AND EVALUATION OF (+/-)-N-(TERT-BUTYLOXYCARBONYL)-CBI, (+/-)-CBI-CDPI1, AND (+/-)-CBI-CDPI2 - CC-1065 FUNCTIONAL AGENTS INCORPORATING THE EQUIVALENT 1,2,9,9A-TETRAHYDROCYCLOPROP[1,2-C]BENZ[1,2-E]INDOL-4-ONE (CBI) LEFT-HAND SUBUNIT [J].
BOGER, DL ;
ISHIZAKI, T ;
WYSOCKI, RJ ;
MUNK, SA ;
KITOS, PA ;
SUNTORNWAT, O .
JOURNAL OF THE AMERICAN CHEMICAL SOCIETY, 1989, 111 (16) :6461-6463
12345