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Título

Ribosome-associated Vesicles: A Dynamic Subcompartment of the Endoplasmic Reticulum in Secretory Cells

AutorCarter, Stephen D.; Hampton, Cheri M.; Langlois, Robert; Melero, Roberto CSIC ORCID; Zachary J. Farino; Calderon, Michael J.; Li, Wen; Wallace, Callen T.; ran, Ngoc Han; Grassucci, Robert A.; Siegmund, Stephanie E.; Pemberton, Joshua; Morgenstern, Travis J.; Eisenman, Leanna; Aguilar, Jenny I.; Greenberg, Nili L.; Levy, Elana S.; Yi, Edward; Mitchell, William G.; Rice, William J.; Pilli, Jyotsna; George, Emily W.; Aslanoglou, Despoina; Courel, Maïté; Freyberg, Robin J.; Javitch, Jonathan A.; Wills, Zachary P.; Area-Gomez, Estela CSIC ORCID; Shiva, Sruti; Bartolini, Francesca; Volchuk, Allen; Murray, Sandra A.; Aridor, Meir; Fish, Kenneth N.; Walter, Peter; Balla, Tamas; Fass, Deborah; Wolf, Sharon G.; Watkins, Simon C.; Carazo, José M.; Jensen, Grant J.; Frank, Joachim; Freyberg, Zachary
Fecha de publicaciónabr-2020
EditorAmerican Association for the Advancement of Science
CitaciónScience Advances 6(14): eaay9572 (2020)
ResumenThe endoplasmic reticulum (ER) is a highly dynamic network of membranes. Here, we combine live-cell microscopy with in situ cryo-electron tomography to directly visualize ER dynamics in several secretory cell types including pancreatic β-cells and neurons under near-native conditions. Using these imaging approaches, we identify a novel, mobile form of ER, ribosome-associated vesicles (RAVs), found primarily in the cell periphery, which is conserved across different cell types and species. We show that RAVs exist as distinct, highly dynamic structures separate from the intact ER reticular architecture that interact with mitochondria via direct intermembrane contacts. These findings describe a new ER subcompartment within cells.
Versión del editorhttps://doi.org/10.1126/sciadv.aay9572
URIhttp://hdl.handle.net/10261/212919
DOI10.1126/sciadv.aay9572
E-ISSN2375-2548
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