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抗肿瘤药物。272. 新型 neo-tanshinlactone 类似物的结构-活性关系及体内选择性抗乳腺癌活性。

Antitumor agents. 272. Structure-activity relationships and in vivo selective anti-breast cancer activity of novel neo-tanshinlactone analogues.

机构信息

Natural Products Research Laboratories, UNC Eshelman School of Pharmacy, University of North Carolina at Chapel Hill, North Carolina 27599, USA.

出版信息

J Med Chem. 2010 Mar 11;53(5):2299-308. doi: 10.1021/jm1000858.

Abstract

Neo-tanshinlactone (1) and its previously reported analogues, such as 2, are potent and selective in vitro antibreast cancer agents. The synthetic pathway to 2 was optimized from seven to five steps, with a better overall yield. Structure-activity relationships studies on these compounds revealed some key molecular determinants for this family of antibreast agents. Several derivatives (19-21 and 24) exerted potent and selective antibreast cancer activity with IC(50) values of 0.3, 0.2, 0.1, and 0.1 microg/mL, respectively, against the ZR-75-1 cell lines. Compound 24 was 2- to 3-fold more potent than 1 against SK-BR-3 and ZR-75-1. Importantly, 21 exhibited high selectivity; it was 23 times more active against ZR-75-1 than MCF-7. Compound 20 had an approximately 12-fold ratio of SK-BR-3/MCF-7 selectivity. In addition, analogue 2 showed potent activity against a ZR-75-1 xenograft model, but not PC-3 and MDA-MB-231 xenografts, as well as high selectivity against breast cancer cell line compared with normal breast tissue-derived cell lines. Further development of lead compounds 19-21 and 24 as clinical trial candidates is warranted.

摘要

新丹参酮(1)及其先前报道的类似物,如 2,是体外抗乳腺癌的有效且选择性的药物。2 的合成途径从 7 步优化到 5 步,总收率更好。对这些化合物的构效关系研究揭示了此类抗乳腺癌药物的一些关键分子决定因素。几种衍生物(19-21 和 24)对 ZR-75-1 细胞系的 IC50 值分别为 0.3、0.2、0.1 和 0.1μg/mL,表现出有效的选择性抗乳腺癌活性。化合物 24 对 SK-BR-3 和 ZR-75-1 的活性比 1 强 2 到 3 倍。重要的是,21 表现出高选择性;它对 ZR-75-1 的活性是 MCF-7 的 23 倍。化合物 20 对 SK-BR-3/MCF-7 的选择性约为 12 倍。此外,类似物 2 对 ZR-75-1 异种移植模型表现出有效活性,但对 PC-3 和 MDA-MB-231 异种移植模型无效,并且与正常乳腺组织来源的细胞系相比对乳腺癌细胞系具有高选择性。有必要进一步开发先导化合物 19-21 和 24 作为临床试验候选药物。

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