AI Article Synopsis
- * The study reveals that blocking the sorting mechanism that delivers EGFR to the plasma membrane can be an effective approach for treating EGFR-dependent tumors, with palmitoylation playing a crucial role in this process.
- * A new cell-permeable peptide, N-myristoylated GKVL-TAT, has been developed to disrupt EGFR's plasma membrane localization, demonstrating significant inhibition of tumor progression, thereby indicating its therapeutic potential.
Article Abstract
Aberrant activation of EGFR due to overexpression or mutation is associated with poor prognosis in many types of tumors. Here we show that blocking the sorting system that directs EGFR to plasma membrane is a potent strategy to treat EGFR-dependent tumors. We find that EGFR palmitoylation by DHHC13 is critical for its plasma membrane localization and identify ARF6 as a key factor in this process. N-myristoylated ARF6 recognizes palmitoylated EGFR via lipid-lipid interaction, recruits the exocyst complex to promote EGFR budding from Golgi, and facilitates EGFR transporting to plasma membrane in a GTP-bound form. To evaluate the therapeutic potential of this sorting system, we design a cell-permeable peptide, N-myristoylated GKVL-TAT, and find it effectively disrupts plasma membrane localization of EGFR and significantly inhibits progression of EGFR-dependent tumors. Our findings shed lights on the underlying mechanism of how palmitoylation directs protein sorting and provide an potential strategy to manage EGFR-dependent tumors.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9556547 | PMC |
| http://dx.doi.org/10.1038/s41467-022-33788-7 | DOI Listing |
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