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新型紫杉醇类似物的合成与生物评价及高效抗肿瘤剂的发现。

Synthesis and biological evaluation of new paclitaxel analogs and discovery of potent antitumor agents.

机构信息

Department of Chemistry, The Scripps Research Institute, 10550 North Torrey Pines Road, La Jolla, California 92037, USA.

出版信息

Org Biomol Chem. 2013 Jul 7;11(25):4154-63. doi: 10.1039/c3ob40654g.

Abstract

Reaction of 10-deacetylbaccatin III (III) and its 7-TES derivative (IV) with DAST under various conditions resulted in the formation of an array of new fluorinated and non-fluorinated 13-keto taxoid compounds (2a–4a) through a vinylogous pinacol–pinacolone rearrangement. Further fluorination of some of these products (2a, 3a) with NFSi or Selectfluor gave additional derivatives. Sodium borohydride reduction of the 13-keto group of these products (2a, 2b, 3a, 3b, 4a, 8, 9, 11–14) led to a series of 9α-hydroxy taxoid derivatives, which were esterified using the docetaxel side chain employing the corresponding protected β-lactam, followed by deprotection to furnish a library of docetaxel analogs and related compounds. A selected number of synthesized compounds (7, 10, 19a, 19b, 21a, 21b, 23, 27, 29, 34–36) were submitted to the National Cancer Institute (NCI) 60 cell line screening program and tested for cytotoxic properties. Taxoids 19a, 19b, 21a, 21b, 23, 27, 29, 34 and 35 were found to exhibit significant anticancer activity against various cancerous cell lines with 23, 27, and 29 being the most potent compounds, demonstrating GI50 values of ≤5 nM in several assays.

摘要

在各种条件下,10-去乙酰基巴卡丁 III(III)及其 7-TES 衍生物(IV)与 DAST 的反应通过乙烯基频哪醇-频哪酮重排生成了一系列新的氟化和非氟化的 13-酮紫杉烷化合物(2a-4a)。进一步用 NFSi 或 Selectfluor 对这些产物中的一些(2a、3a)进行氟化得到了额外的衍生物。这些产物(2a、2b、3a、3b、4a、8、9、11-14)的 13-酮基用硼氢化钠还原得到了一系列 9α-羟基紫杉烷衍生物,然后使用相应的保护β-内酰胺对其进行酯化,再进行脱保护,得到了一组多西他赛类似物和相关化合物。选择了一些合成的化合物(7、10、19a、19b、21a、21b、23、27、29、34-36)提交给国家癌症研究所(NCI)60 细胞系筛选计划,并测试其细胞毒性。化合物 19a、19b、21a、21b、23、27、29、34 和 35 被发现对各种癌细胞系具有显著的抗癌活性,其中 23、27 和 29 是最有效的化合物,在几项测定中 GI50 值均≤5 nM。

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