Firm evidence for the detoxification of senecionine-induced hepatotoxicity via N-glucuronidation in UGT1A4–humanized transgenic mice

葡萄糖醛酸化 毒性 药理学 戒毒(替代医学) 葡萄糖醛酸转移酶 吡咯里嗪 吡咯里嗪生物碱 药物代谢 化学 生物化学 生物 微粒体 医学 药品 立体化学 病理 有机化学 替代医学
作者
Yan Chen,Weiqian Wang,Xia-Li Jia,Changhong Wang,Li Yang,Zhengtao Wang,Aizhen Xiong
出处
期刊:Food and Chemical Toxicology [Elsevier]
卷期号:165: 113185-113185 被引量:6
标识
DOI:10.1016/j.fct.2022.113185
摘要

Uridine diphosphate glucuronosyltransferase (UGT)1A4 is responsible for N-glucuronidation of tertiary amines but is a pseudogene in commonly used rodent models in toxicity and safety assessment. As a continuation of our investigation into the toxicity and safety assessment of pyrrolizidine alkaloid (PA)-containing herbs, we generated a UGT1A4-humanized (hUGT1A4) transgenic mouse model to systematically study the toxicity, metabolism network, and toxicokinetic characteristics of senecionine (a representative toxic PA) and compared with that in the wide-type controls in parallel. As results, senecionine-induced toxicity was significantly decreased as approved by mortality, pathology, and biochemistry assays in hUGT1A4 mice and cultured primary hepatocytes. More importantly N-glucuronidation adduct was exclusively identified in all the hUGT1A4 mice, liver microsomes, and cultured primary hepatocytes, yet absent in the wide-type controls. The variation in toxicokinetic characters was also observed between hUGT1A4 mice and the wide-type controls with a notably inhibition of the toxification metabolites, i.e., pyrrole-protein adducts, in hUGT1A4 mice. Conclusively, UGT1A4 plays an important role in detoxification of senecionine and the hUGT1A4 mouse model is promising for the pre-clinical evaluation of the efficacy and toxicity of tertiary amine agents in drug development and safety assessment.
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