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Cytoprotective pyridinol antioxidants as potential therapeutic agents for neurodegenerative and mitochondrial diseases

机译:具有细胞保护性的吡啶醇抗氧化剂可作为神经退行性疾病和线粒体疾病的潜在治疗剂

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As part of our ongoing efforts to identify compounds having potential utility in treating neurodegenerative and mitochondrial disorders, a series of pyridinol analogues have been prepared. The synthetic route employed for the preparation of the new analogues is different, and considerably more efficient, than that used in previously reported studies. The new route yields a pair of pyridinol regioisomers that can be readily separated and evaluated. Their ability to quench lipid peroxidation and reactive oxygen species (ROS), and to preserve mitochondrial membrane potential (Delta psi(m)) and support ATP synthesis is reported. The optimal side chain length was found to be 16 carbon atoms. The metabolic stability of those compounds having optimal biological activities was evaluated in vitro using bovine liver microsomes. The omission of any side chain hydroxyl group and introduction of an azetidine moiety at position 6 of the pyridinol redox core (8 and 9) increased their microsomal stability as compared to the exocyclic dimethylamino group. The favorable metabolic stability conferred by the azetidine moiety in compounds 8 and 9 makes these compounds excellent candidates for further evaluation. (C) 2014 Published by Elsevier Ltd.
机译:作为我们正在进行的鉴定具有治疗神经退行性疾病和线粒体疾病潜能的化合物的努力的一部分,已制备了一系列吡啶醇类似物。与以前报道的研究相比,用于制备新类似物的合成途径是不同的,并且效率更高。新路线产生了一对吡啶醇区域异构体,可以容易地对其进行分离和评估。据报道,它们具有抑制脂质过氧化和活性氧(ROS)以及保持线粒体膜电位(Delta psi(m))和支持ATP合成的能力。发现最佳侧链长度为16个碳原子。使用牛肝微粒体在体外评估了那些具有最佳生物学活性的化合物的代谢稳定性。与环二甲基氨基基团相比,省略任何侧链羟基基团和在吡啶醇氧化还原核心(8和9)的6位引入氮杂环丁烷部分,增加了它们的微粒体稳定性。化合物8和9中氮杂环丁烷部分所赋予的有利的代谢稳定性使这些化合物成为进一步评估的极佳候选者。 (C)2014由Elsevier Ltd.出版

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