SGD Paper 
Pagant S, et al. (2007) Inhibiting endoplasmic reticulum (ER)-associated degradation of misfolded Yor1p does not permit ER export despite the presence of a diacidic sorting signal. Mol Biol Cell 18(9):3398-413
Abstract: Monitoring Editor: Jeffrey Brodsky Capture of newly synthesized proteins into endoplasmic reticulum (ER)-derived COPII vesicles represents a critical juncture in the quality control of protein biogenesis within the secretory pathway. The yeast ABC transporter, Yor1p, is a pleiotropic drug pump that shows homology to the human cystic fibrosis transmembrane conductance regulator (CFTR). Deletion of a phenylalanine residue in Yor1p, equivalent to the major disease-causing mutation in CFTR, causes ER retention and degradation via ER-associated degradation (ERAD). We have examined the relationship between protein folding, ERAD and forward transport during Yor1p biogenesis. Uptake of Yor1p into COPII vesicles is mediated by an N-terminal di-acidic signal that likely interacts with the "B-site" cargo-recognition domain on the COPII subunit, Sec24p. Yor1p-DeltaF is subjected to complex ER quality control involving multiple cytoplasmic chaperones and degradative pathways. Stabilization of Yor1p-DeltaF by inhibiting its degradation does not permit access of Yor1p-DeltaF to COPII vesicles. We propose that the ER quality control checkpoint engages misfolded Yor1p even after it has been stabilized by inhibition of the degradative pathway.
| Status: Published | Type: Journal Article | PubMed ID: 17615300 |
Topics addressed in this paper
Number of different genes curated to this paper: 10
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| HLJ1 | HRD1 | HSC82 | HSP82 | SEC24 | SSM4 | UBC7 | UBX2 | YDJ1 | YOR1 | |
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