[No authors listed]
Proteins that fail to correctly fold or assemble into oligomeric complexes in the endoplasmic reticulum (ER) are degraded by a ubiquitin- and proteasome-dependent process known as ER-associated degradation (ERAD). Although many individual components of the ERAD system have been identified, how these proteins are organized into a functional network that coordinates recognition, ubiquitylation and dislocation of substrates across the ER membrane is not well understood. We have investigated the functional organization of the mammalian ERAD system using a systems-level strategy that integrates proteomics, functional genomics and the transcriptional response to ER stress. This analysis supports an adaptive organization for the mammalian ERAD machinery and reveals a number of metazoan-specific genes not previously linked to ERAD.
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SAE1, PSMD14, EMC8, TUBA1B, PGRMC2, TOMM40, CIB2, ARL6IP5, ERLIN1, OS9, GCN1, SLC27A3, RAB35, ERLIN2, RPL35, OSBPL8, CLPTM1, COX4I1, BRI3BP, CSE1L, SLC25A10, DUSP3, TMEM201, EMD, ENO1, TUBB, EPHX1, FDFT1, EMC1, FLNA, UBXN4, GANAB, FAF2, PSME4, ARL6IP1, ESYT1, KLHDC2, MTCH1, GALK1, AMFR, ERLEC1, EMC10, ANK2, UBQLN2, HMGCR, HMOX1, HNRNPA2B1, HNRNPU, DNAJB1, UBAC2, STT3A, ARF3, ARF5, KRT6A, KRT8, KRT18, MARCKS, MCM2, COX2, MYH9, MYH10, HNRNPM, OAT, ATP5B, DERL2, EMC9, EMC4, FAM8A1, UBE2J1, LARS, ATP5F1, TUBA8, PFKL, PFKP, POR, CPVL, TMED9, PPIB, AUP1, LIN7C, SYNJ2BP, LRRC59, IPO9, NGLY1, VIMP, EMC3, CAND1, PRKDC, TUBB7P, PSMA1, PSMA2, PSMA3, EMC7, PSMA4, PSMA5, PSMA6, PSMA7, PSMB1, PSMB2, PSMB3, PSMB4, PSMB5, PSMB6, PSMB7, TOMM22, PSMC2, PSMD1, PSMD3, PSMD7, RTN4, ESYT2, TXNDC16, DIP2B, ACTA1, PEX19, ABCD3, SELK, RAD23B, RPL10, RPN1, RPN2, SEL1L, TBC1D15, CAPRIN2, SURF4, ACTG1, HSP90B1, ACTG2, UBC, UBE2G2, UQCRC2, USH2A, VCP, VDAC1, VDAC2, VDAC3, TUBA1A, RAB7A, DERL1, TMEM43, TBC1D17, UBXN8, FOXRED2, KMT2D, CLPTM1L, HM13, CANX, EMC6, TMUB1, LONP2, FAM186B, TAGLN2, SYVN1, DPY30, NIPSNAP1, CASK, SERPINH1, PEX11B, GGH, YIF1B, TMEM259, VAPB, VAPA, MMGT1, UBE4A, RAB9A, NPEPPS, SEC22B, EMC2, EDEM1, CKAP5, TOMM20, PSMD6
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