哺乳动物 MsrA 对含亚砜基化合物的选择性还原提示了提高药物疗效的策略。
Selective reduction of methylsulfinyl-containing compounds by mammalian MsrA suggests a strategy for improved drug efficacy.
出版信息
ACS Chem Biol. 2011 Oct 21;6(10):1029-35. doi: 10.1021/cb2001395. Epub 2011 Aug 22.
Abstract
Identification of pathways of drug metabolism provides critical information regarding efficacy and safety of these compounds. Particularly challenging cases involve stereospecific processes. We found that broad classes of compounds containing methylsulfinyl groups are reduced to methylsulfides specifically by methionine sulfoxide reductase A, which acts on the S-stereomers of methionine sulfoxides, whereas the R-stereomers of these compounds could not be efficiently reduced by any methionine sulfoxide reductase in mammals. The findings of efficient reduction of S-methylsulfinyls and deficiency in the reduction of R-methylsulfinyls by methionine sulfoxide reductases suggest strategies for improved efficacy and decreased toxicity of drugs and natural compounds containing methylsulfinyls through targeted use of their enantiomers.
摘要
鉴定药物代谢途径为这些化合物的疗效和安全性提供了关键信息。特别具有挑战性的情况涉及立体特异性过程。我们发现,含有亚甲基砜基的广泛化合物类别被甲硫氨酸亚砜还原酶 A 特异性还原为甲硫醚,而这些化合物的 R-对映异构体不能被哺乳动物中的任何甲硫氨酸亚砜还原酶有效还原。甲硫氨酸亚砜还原酶对 S-亚甲基砜的有效还原和对 R-亚甲基砜还原的缺乏的发现,为含有亚甲基砜的药物和天然化合物通过有针对性地使用其对映异构体来提高疗效和降低毒性提供了策略。
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