吡非尼酮
化学
醌甲酰胺
药理学
微粒体
谷胱甘肽
生物化学
肝细胞
特发性肺纤维化
醌
酶
内科学
体外
医学
肺
作者
Shenzhi Zhou,Wei Li,Wei Li,Min Tian,Na Zhang,Xiaojing Yang,Weiwei Li,Weiwei Li,Ying Peng,Jiang Zheng
标识
DOI:10.1021/acs.jmedchem.9b02073
摘要
-acetylcysteine (GSH/NAC) conjugates were detected in microsomal/primary hepatocyte incubations after exposure to pirfenidone. The GSH/NAC conjugates were also observed in bile and urine of rats given pirfenidone, respectively. The observation of the conjugates suggests the formation of a quinone methide intermediate derived from pirfenidone. The intermediate was possibly generated through two pathways. First, pirfenidone was directly metabolized to the quinone methide intermediate via dehydrogenation; second, pirfenidone was oxidized to 5-hydroxymethyl pirfenidone, followed by sulfation to a benzyl alcohol-sulfate derivative. The findings facilitate the understanding of the mechanisms of pirfenidone-induced idiosyncratic toxicity and assist medicinal chemists to minimize toxicities in the development of new pharmaceutical agents.
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