Design, synthesis and cytotoxicity studies of dithiocarbamate ester derivatives of emetine in prostate cancer cell lines

被引:19
|
作者
Akinboye, Emmanuel S. [1 ,5 ]
Bamji, Zebalda D. [2 ,3 ]
Kwabi-Addo, Bernard [2 ,3 ]
Ejeh, David
Copeland, Robert L. [4 ]
Denmeade, Samuel R. [5 ]
Bakare, Oladapo [1 ]
机构
[1] Howard Univ, Dept Chem, Washington, DC 20059 USA
[2] Howard Univ, Dept Biochem, Washington, DC 20059 USA
[3] Howard Univ, Ctr Canc, Washington, DC 20059 USA
[4] Howard Univ, Coll Med, Dept Pharmacol, Washington, DC 20059 USA
[5] Johns Hopkins Sch Med, Sidney Kimmel Comprehens Canc Ctr Johns Hopkins, Baltimore, MD 21231 USA
基金
美国国家科学基金会;
关键词
Emetine; Dithiocarbamate ester; Anti-cancer activities; Prostate cancer; Emetine derivatives; PHASE-I; NSC-33669;
D O I
10.1016/j.bmc.2015.06.072
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
A small library of emetine dithiocarbamate ester derivatives were synthesized in 25-86% yield via derivatization of the N2'-position of emetine. Anticancer evaluation of these compounds in androgen receptor positive LNCaP and androgen receptor negative PC3 and DU145 prostate cancer cell lines revealed time dependent and dose-dependent cytotoxicity. With the exception of compound 4c, all the dithiocarbamate ester analogs in this study showed appreciable potency in all the prostate cancer cell lines (regardless of whether it is androgen receptor positive or negative) with a cytotoxicity IC50 value ranging from 1.312 +/- 0.032 mu M to 5.201 +/- 0.125 mu M by day 7 of treatment. Compared to the sodium dithiocarbamate salt 1, all the dithiocarbamate ester analogs (2 and 4a-4g) displayed lower cytotoxicity than compound 1 (PC3, IC50 = 0.087 +/- 0.005 mu M; DU145, IC50 = 0.079 +/- 0.003 mu M and LNCaP, IC50 = 0.079 +/- 0.003 mu M) on day 7 of treatment. Consequently, it appears that S-alkylation of compound 1 leads to a more stable dithiocarbamate ester derivative that resulted in lower anticancer activity in the prostate cancer cell lines. (C) 2015 Elsevier Ltd. All rights reserved.
引用
收藏
页码:5839 / 5845
页数:7
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