A Parent–Metabolite Middle-Out PBPK Model for Genistein and Its Glucuronide Metabolite in Rats: Integrating Liver and Enteric Metabolism with Hepatobiliary and Enteroluminal Transport to Assess Glucuronide Recycling
Bhargavi Srija Ramisetty, Rashim Singh, Ming Hu, Michael Zhuo Wang

TL;DR
This study creates a detailed model to understand how genistein and its glucuronide metabolite are processed in rats, focusing on how glucuronide recycling affects drug levels in the gut and bloodstream.
Contribution
A novel middle-out PBPK model integrating liver and gut metabolism with transporters to assess glucuronide recycling in rats.
Findings
The model successfully estimates systemic and local exposure of genistein and its glucuronide metabolite in rats.
Glucuronide recycling significantly impacts drug concentrations in the colon and plasma.
The model highlights the role of transporters and metabolism in drug–drug interactions affecting local drug exposure.
Abstract
Background: Glucuronide recycling in the gut and liver profoundly affects the systemic and/or local exposure of drugs and their glucuronide metabolites, impacting both clinical efficacy and toxicity. This recycling also alters drug exposure in the colon, making it critical to establish local concentration for drugs targeting colon (e.g., drugs for colon cancer and inflammatory bowel disease). Methods: In this study, a parent–metabolite middle-out physiologically based pharmacokinetic (PBPK) model was built for genistein and its glucuronide metabolite to estimate the systemic and local exposure of the glucuronide and its corresponding aglycone in rats by incorporating UDP-glucuronosyltransferase (UGT)-mediated metabolism and transporter-dependent glucuronide disposition in the liver and intestine, as well as gut microbial-mediated deglucuronidation that enables the recycling of the…
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Taxonomy
TopicsDrug Transport and Resistance Mechanisms · Liver Disease Diagnosis and Treatment · Phytoestrogen effects and research
