首页> 外文期刊>Journal of Medicinal Chemistry >Selective cytotoxicity of oxysterols through structural modulation on rings A and B. Synthesis, in vitro evaluation, and SAR
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Selective cytotoxicity of oxysterols through structural modulation on rings A and B. Synthesis, in vitro evaluation, and SAR

机译:通过对环A和环B的结构调节,对氧固醇的选择性细胞毒性。合成,体外评估和SAR

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摘要

Chemically diverse oxysterols were prepared and evaluated for cytotoxicity, aiming to push forward potency and selectivity. They were tested against seven cancer (HT-29, HepG2, A549, PC3, LAMA-84, MCF-7, and SH-SY5Y) and two noncancerous cell lines (ARPE-19 and BJ). The influence of the oxidation pattern on rings A and B was studied. Oxygen functionalities on ring B, such as oxo, oxime, acetamide, acetate, and alkoxy, were evaluated. Most oxysterols were cytotoxic in the low micromolar range, with emphasis to the tetrols 14 and 34, the 6β methoxy and acetoxy derivatives 21 and 45, and the oxime 28. In general, the oxysterols were more toxic to cancer cells and a set of compounds (9, 14, 21, 28, 45) with very high selectivity was identified. The cytotoxicity of 3β-acetates was lower than that of the parent alcohols, although incubation for a longer period rendered them equally cytotoxic, pointing them as potential prodrugs of oxysterols.
机译:制备化学上多样化的氧固醇并评估其细胞毒性,旨在提高药效和选择性。他们针对七种癌症(HT-29,HepG2,A549,PC3,LAMA-84,MCF-7和SH-SY5Y)和两种非癌细胞系(ARPE-19和BJ)进行了测试。研究了氧化方式对环A和B的影响。评价了环B上的氧官能度,例如氧代,肟,乙酰胺,乙酸酯和烷氧基。大多数氧固醇在低微摩尔范围内具有细胞毒性,重点是四醇14和34、6β甲氧基和乙酰氧基衍生物21和45以及肟28。通常,氧固醇对癌细胞和一组化合物的毒性更大。 (9,14,21,28,45)具有很高的选择性。 3β-乙酸盐的细胞毒性低于母体醇,尽管孵育时间较长使其具有相同的细胞毒性,指出它们是氧固醇的潜在前药。

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