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Kanehara K, et al.  (2010) Modularity of the Hrd1 ERAD complex underlies its diverse client range. J Cell Biol 188(5):707-16

Abstract: Secretory protein folding is monitored by endoplasmic reticulum (ER) quality control mechanisms. Misfolded proteins are retained and targeted to ER-associated degradation (ERAD) pathways. At their core are E3 ubiquitin ligases, which organize factors that recognize, ubiquitinate, and translocate substrates. Of these, we report that the Hrd1 complex manages three distinct substrate classes. A core complex is required for all classes and is sufficient for some membrane proteins. The accessory factors Usa1p and Der1p adapt the complex to process luminal substrates. Their integration is sufficient to process molecules bearing glycan-independent degradation signals. The presence of Yos9p extends the substrate range by mediating the recognition of glycan-based degradation signals. This modular organization enables the Hrd1 complex to recognize topologically diverse substrates. The Hrd1 system does not directly evaluate the folding state of polypeptides. Instead, it does so indirectly, by recognizing specific embedded signals displayed upon misfolding.

Status: Published Type: Journal Article | Research Support, Non-U.S. Gov't PubMed ID: 20212318

Topics addressed in this paper

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Topics Genes linked to topics (#1 - 10 )
CDC48 CUE1 DER1 HRD1 JEM1 KAR2 MNL1 PEP4 PRC1 SCJ1
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Topics Genes linked to topics (#11 - 12 )
USA1 YOS9
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