Palmitoylation Transduces the Regulation of Epidermal Growth Factor to Organic Anion Transporter 3
Zhou Yu, Jinghui Zhang, Jiaxu Feng, Guofeng You

TL;DR
This study shows that palmitoylation, a new mechanism, helps EGF regulate OAT3, a kidney transporter, and that EGFR inhibitors may affect drug clearance.
Contribution
The study reveals palmitoylation as a novel regulatory mechanism linking EGF/PKA signaling to OAT3 function.
Findings
EGF increases OAT3 expression and estrone sulfate transport by ~40%.
EGF/PKA signaling enhances OAT3 palmitoylation, which is blocked by H-89.
Osimertinib, an EGFR inhibitor, blocks EGF-stimulated OAT3 transport activity.
Abstract
Background: Organic anion transporter 3 (OAT3) in the kidney proximal tubule cells plays a critical role in renal clearance of numerous endogenous metabolites and exogenous drugs and toxins. In this study, we discovered that epidermal growth factor (EGF) regulates the expression and activity of OAT3 through palmitoylation, a novel mechanism that has never been described in the OAT field. Methods/Results: Our results showed that treatment of OAT3-expressing cells with EGF led to a ~40% increase in OAT3 expression and OAT3-mediated transport of estrone sulfate, a prototypical substrate for OAT3. EGF-stimulated OAT3 transport activity was abrogated by H-89, a protein kinase A (PKA) inhibitor, indicating that an EGF-PKA signaling pathway is involved in the regulation of OAT3. We also showed that treatment of OAT3-expressing cells with EGF resulted in an enhancement of OAT3 palmitoylation, a…
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Taxonomy
TopicsDrug Transport and Resistance Mechanisms · Pharmacogenetics and Drug Metabolism · Amino Acid Enzymes and Metabolism
