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- W4376109416 abstract "Abstract The epidermal growth factor receptor (EGFR) is a central regulator of cell physiology that is stimulated by multiple distinct ligands. Although ligands bind to EGFR while the receptor is exposed on the plasma membrane, EGFR incorporation into endosomes following receptor internalization is an important aspect of EGFR signaling, with EGFR internalization behavior dependent upon the type of ligand bound. We develop quantitative modeling, both kinetic and with spatial details, for EGFR recruitment to and internalization from clathrin domains and competition with ligand unbinding from EGFR. We find that a combination of spatial and kinetic proofreading leads to enhanced EGFR internalization ratios in comparison to unbinding differences between ligand types. Various stages of the EGFR internalization process, including recruitment to and internalization from clathrin domains, modulate the internalization differences between receptors bound to different ligands. Our results indicate that following ligand binding, EGFR may encounter multiple clathrin domains before successful recruitment and internalization. The quantitative modeling we have developed describes competition between EGFR internalization and ligand unbinding and the resulting proofreading." @default.
- W4376109416 created "2023-05-12" @default.
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- W4376109416 date "2023-05-10" @default.
- W4376109416 modified "2023-10-16" @default.
- W4376109416 title "Quantitative modeling of EGF receptor ligand discrimination via internalization proofreading" @default.
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- W4376109416 doi "https://doi.org/10.1101/2023.05.09.539827" @default.
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