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跨物种肝微粒体和肝细胞中特比萘芬新型谷胱甘肽共轭物的鉴定。

Identification of novel glutathione conjugates of terbinafine in liver microsomes and hepatocytes across species.

作者信息

Patil Amol, Ladumor Mayurbhai Kathadbhai, Kamble Shyam H, Johnson Benjamin M, Subramanian Murali, Sinz Michael W, Singh Dilip Kumar, Putlur Sivaprasad, Bhutani Priyadeep, Ahire Deepak Suresh, Singh Saranjit

机构信息

Department of Pharmaceutical Analysis, National Institute of Pharmaceutical Education and Research (NIPER) , S.A.S. Nagar , India.

Biocon Bristol-Myers Squibb Research and Development Center, Syngene International Limited , Bangalore , India.

出版信息

Xenobiotica. 2019 Dec;49(12):1403-1413. doi: 10.1080/00498254.2019.1581959. Epub 2019 Mar 7.

DOI:10.1080/00498254.2019.1581959
PMID:30747549
Abstract
  1. Terbinafine (TBF), a common antifungal agent, has been associated with rare incidences of hepatotoxicity. It is hypothesized that bioactivation of TBF to reactive intermediates and subsequent binding to critical cellular proteins may contribute to this toxicity. In the present study, we have characterized the bioactivation pathways of TBF extensively in human, mouse, monkey, dog and rat liver microsomes and hepatocytes. 2. A total of twenty glutathione conjugates of TBF were identified in hepatocytes; thirteen of these conjugates were also detected in liver microsomes. To the best of our knowledge, only two of these conjugates have been reported previously. The conjugates were categorized into three groups based on their mechanism of formation: (a) alkene/alkyne oxidation followed by glutathione conjugation, with or without -demethylation, (b) arene oxidation followed by glutathione conjugation, with or without -demethylation, and (c) -dealkylation followed by glutathione conjugation of the allylic aldehyde, alcohol and acid intermediates. 3. Differences were observed across species in the contributions of these pathways toward overall metabolic turnover. We conclude that, in addition to the glutathione conjugates known to form by Michael addition to the allylic aldehyde, there are other pathways involving the formation of arene oxides and alkene/alkyne epoxides that may be relevant to the discussion of TBF-mediated idiosyncratic drug reactions.
摘要
  1. 特比萘芬(TBF)是一种常见的抗真菌药物,曾有过罕见的肝毒性报道。据推测,TBF生物活化形成反应性中间体并随后与关键细胞蛋白结合可能是导致这种毒性的原因。在本研究中,我们已在人、小鼠、猴、狗和大鼠的肝微粒体及肝细胞中广泛表征了TBF的生物活化途径。2. 在肝细胞中总共鉴定出了20种TBF的谷胱甘肽共轭物;其中13种共轭物在肝微粒体中也被检测到。据我们所知,此前仅报道过其中两种共轭物。这些共轭物根据其形成机制分为三组:(a)烯烃/炔烃氧化后进行谷胱甘肽共轭,有或没有去甲基化;(b)芳烃氧化后进行谷胱甘肽共轭,有或没有去甲基化;(c)烯丙基醛、醇和酸中间体进行去烷基化后再进行谷胱甘肽共轭。3. 观察到这些途径在不同物种中对整体代谢转换的贡献存在差异。我们得出结论,除了已知通过对烯丙基醛进行迈克尔加成形成的谷胱甘肽共轭物外,还有其他涉及芳烃氧化物和烯烃/炔烃环氧化物形成的途径,这些途径可能与TBF介导的特异质性药物反应的讨论相关。

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