Misfolded proteins retained in the endoplasmic reticulum (ER) are degraded by the ER-associated degradation pathway. The mechanisms used to sort them from correctly folded proteins remain unclear. Analysis of substrates with defined folded and misfolded domains has revealed a system of sequential checkpoints that recognize topologically distinct domains of polypeptides. The first checkpoint examines the cytoplasmic domains of membrane proteins. If a lesion is detected, it is retained statically in the ER and rapidly degraded without regard to the state of its other domains. Proteins passing this test face a second checkpoint that monitors domains localized in the ER lumen. Proteins detected by this pathway are sorted from folded proteins and degraded by a quality control mechanism that requires ER-to-Golgi transport. Although the first checkpoint is obligatorily directed at membrane proteins, the second monitors both soluble and membrane proteins. Our data support a model whereby “properly folded” proteins are defined biologically as survivors that endure a series of distinct checkpoints.
Misfolded proteins are sorted by a sequential checkpoint mechanism of ER quality control
Abbreviations used in this paper: CFTR, cystic fibrosis transmembrane conductance regulator; CPY*, mutant carboxypeptidase Y; CT*, membrane-bound CPY* lacking a cytosolic domain; CTG*, CT* with GFP as its cytosolic domain; Endo H, endoglycosidase H; ERAD, ER-associated degradation; ERAD-C, ERAD-Cytosolic; ERAD-L, ERAD-Luminal; GT, glucosyltransferase; KHN, yeast Kar2p signal sequence fused to the simian virus 5 HA-Neuraminidase ectodomain; KWS, KHN luminal domain/Wsc1p transmembrane domain/Ste6-166p mutant cytosolic domain; KWW, KHN luminal domain/Wsc1p transmembrane domain/Wsc1p cytosolic domain.
Shilpa Vashist, Davis T.W. Ng; Misfolded proteins are sorted by a sequential checkpoint mechanism of ER quality control . J Cell Biol 12 April 2004; 165 (1): 41–52. doi: https://doi.org/10.1083/jcb.200309132
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