The endoplasmic reticulum (ER) is the start site of the secretory pathway, where newly synthesized secreted and membrane proteins are packaged into COPII vesicles through direct interaction with the COPII coat or aided by specific cargo receptors. Little is known about how post-translational modification events regulate packaging of cargo into COPII vesicles. Erv14/Cornichon belongs to a conserved family of cargo receptors required for the selection and ER export of transmembrane proteins. In this work, we show the importance of a phosphorylation consensus site (Serine-134) at the C-terminus of Erv14. Mimicking phosphorylation of S134 (S134D) prevents the incorporation of Erv14 into COPII vesicles, delays cell growth, exacerbates growth of sec mutants, modifies ER structure, and affects localization of several plasma membrane transporters. In contrast, the dephosphorylated mimic (S134A) had less deleterious effects, but still modifies ER structure and slows cell growth. Our results suggest that a possible cycle of phosphorylation and dephosphorylation is important for the correct functioning of Erv14p.
The C-terminus of the cargo receptor Erv14p affects COPII vesicle formation and cargo delivery
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- Funder(s): Consejo Nacional de Ciencia y Tecnologia
- Award Id(s): 2041
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Daniel Lagunas-Gomez, Carolina Yañez-Dominguez, Guadalupe Zavala-Padilla, Charles Barlowe, Omar Pantoja; The C-terminus of the cargo receptor Erv14p affects COPII vesicle formation and cargo delivery. J Cell Sci 2023; jcs.260527. doi: https://doi.org/10.1242/jcs.260527
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