Glucuronidation: driving factors and their impact on glucuronide disposition

葡萄糖醛酸化 化学 葡萄糖醛酸 新陈代谢 药物代谢 流出 葡萄糖醛酸转移酶 药代动力学 代谢途径 羟基化 药理学 运输机 排泄 生物化学 微粒体 生物 基因
作者
Tao Yi,Shufan Ge,Rashim Singh,Sumit Basu,Katherine Shatzer,Ming Zen,Jiong Liu,Yifan Tu,Chenning Zhang,Jinbao Wei,Jian Shi,Lijun Zhu,Zhongqiu Liu,Yuan Wang,Song Gao,Ming Hu
出处
期刊:Drug Metabolism Reviews [Taylor & Francis]
卷期号:49 (2): 105-138 被引量:101
标识
DOI:10.1080/03602532.2017.1293682
摘要

Glucuronidation is a well-recognized phase II metabolic pathway for a variety of chemicals including drugs and endogenous substances. Although it is usually the secondary metabolic pathway for a compound preceded by phase I hydroxylation, glucuronidation alone could serve as the dominant metabolic pathway for many compounds, including some with high aqueous solubility. Glucuronidation involves the metabolism of parent compound by UDP-glucuronosyltransferases (UGTs) into hydrophilic and negatively charged glucuronides that cannot exit the cell without the aid of efflux transporters. Therefore, elimination of parent compound via glucuronidation in a metabolic active cell is controlled by two driving forces: the formation of glucuronides by UGT enzymes and the (polarized) excretion of these glucuronides by efflux transporters located on the cell surfaces in various drug disposition organs. Contrary to the common assumption that the glucuronides reaching the systemic circulation were destined for urinary excretion, recent evidences suggest that hepatocytes are capable of highly efficient biliary clearance of the gut-generated glucuronides. Furthermore, the biliary- and enteric-eliminated glucuronides participate into recycling schemes involving intestinal microbes, which often prolong their local and systemic exposure, albeit at low systemic concentrations. Taken together, these recent research advances indicate that although UGT determines the rate and extent of glucuronide generation, the efflux and uptake transporters determine the distribution of these glucuronides into blood and then to various organs for elimination. Recycling schemes impact the apparent plasma half-life of parent compounds and their glucuronides that reach intestinal lumen, in addition to prolonging their gut and colon exposure.
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