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首页> 外文期刊>Journal of Lipid Research >High-throughput screening for fatty acid uptake inhibitors in humanized yeast identifies atypical antipsychotic drugs that cause dyslipidemias
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High-throughput screening for fatty acid uptake inhibitors in humanized yeast identifies atypical antipsychotic drugs that cause dyslipidemias

机译:高通量筛选人源化酵母中的脂肪酸摄取抑制剂可鉴定出导致血脂异常的非典型抗精神病药

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Fatty acids are implicated in the development of dyslipidemias, leading to type 2 diabetes and cardiovascular disease. We used a standardized small compound library to screen humanized yeast to identify compounds that inhibit fatty acid transport protein (FATP)-mediated fatty acid uptake into cells. This screening procedure used live yeast cells expressing human FATP2 to identify small compounds that reduced the import of a fluorescent fatty acid analog, 4,4-difluoro-5-methyl-4-bora-3a, 4a-diaza-s-indacene-3-dodecanoic acid (C-1-BODIPY-C-12). The library used consisted of 2,080 compounds with known biological activities. Of these, similar to 1.8% reduced cell-associated C-1-BODIPY-C-12 fluorescence and were selected as potential inhibitors of human FATP2-mediated fatty acid uptake. Based on secondary screens, 28 compounds were selected as potential fatty acid uptake inhibitors. Some compounds fell into four groups with similar structural features. The largest group was structurally related to a family of tricyclic, phenothiazine-derived drugs used to treat schizophrenia and related psychiatric disorders, which are also known to cause metabolic side effects, including hypertriglyceridemia. Potential hit compounds were studied for specificity of interaction with human FATP and efficacy in human Caco-2 cells.
机译:脂肪酸与血脂异常有关,导致2型糖尿病和心血管疾病。我们使用标准化的小型化合物库筛选人源化酵母,以鉴定抑制脂肪酸转运蛋白(FATP)介导的脂肪酸摄入细胞的化合物。该筛选程序使用表达人FATP2的活酵母细胞来鉴定可减少荧光脂肪酸类似物4,4-二氟-5-甲基-4-硼3a,4a-二氮杂-s-茚并三烯3进口的小化合物。 -十二烷酸(C-1-BODIPY-C-12)。使用的文库由具有已知生物学活性的2,080种化合物组成。其中,与细胞相关的C-1-BODIPY-C-12荧光减少了1.8%,并被选作人类FATP2介导的脂肪酸摄取的潜在抑制剂。基于二次筛选,选择了28种化合物作为潜在的脂肪酸摄取抑制剂。一些化合物分为具有相似结构特征的四类。最大的一组在结构上与用于治疗精神分裂症和相关精神疾病的三环吩噻嗪衍生药物家族有关,后者也已知会引起代谢性副作用,包括高甘油三酯血症。研究了与人FATP相互作用的特异性以及在人Caco-2细胞中的功效的潜在命中化合物。

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