FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2016983085> ?p ?o ?g. }

• W2016983085 endingPage "739" @default.
• W2016983085 startingPage "727" @default.
• W2016983085 abstract "The ER's capacity to process proteins is limited, and stress caused by accumulation of unfolded and misfolded proteins (ER stress) contributes to human disease. ER stress elicits the unfolded protein response (UPR), whose components attenuate protein synthesis, increase folding capacity, and enhance misfolded protein degradation. Here, we report that P58(IPK)/DNAJC3, a UPR-responsive gene previously implicated in translational control, encodes a cytosolic cochaperone that associates with the ER protein translocation channel Sec61. P58(IPK) recruits HSP70 chaperones to the cytosolic face of Sec61 and can be crosslinked to proteins entering the ER that are delayed at the translocon. Proteasome-mediated cytosolic degradation of translocating proteins delayed at Sec61 is cochaperone dependent. In P58(IPK-/-) mice, cells with a high secretory burden are markedly compromised in their ability to cope with ER stress. Thus, P58(IPK) is a key mediator of cotranslocational ER protein degradation, and this process likely contributes to ER homeostasis in stressed cells." @default.
• W2016983085 created "2016-06-24" @default.
• W2016983085 creator A5003539515 @default.
• W2016983085 creator A5010360422 @default.
• W2016983085 creator A5036980616 @default.
• W2016983085 creator A5037305891 @default.
• W2016983085 creator A5041797262 @default.
• W2016983085 creator A5042756187 @default.
• W2016983085 creator A5051950312 @default.
• W2016983085 creator A5054545550 @default.
• W2016983085 creator A5064945498 @default.
• W2016983085 creator A5068450634 @default.
• W2016983085 creator A5077934127 @default.
• W2016983085 creator A5080761072 @default.
• W2016983085 creator A5088448170 @default.
• W2016983085 date "2006-08-01" @default.
• W2016983085 modified "2023-10-12" @default.
• W2016983085 title "Cotranslocational Degradation Protects the Stressed Endoplasmic Reticulum from Protein Overload" @default.
• W2016983085 cites W1955276614 @default.
• W2016983085 cites W1964324370 @default.
• W2016983085 cites W1965843055 @default.
• W2016983085 cites W1967358425 @default.
• W2016983085 cites W1980355157 @default.
• W2016983085 cites W1981551685 @default.
• W2016983085 cites W1984685964 @default.
• W2016983085 cites W1997826161 @default.
• W2016983085 cites W2018557658 @default.
• W2016983085 cites W2023680254 @default.
• W2016983085 cites W2026357888 @default.
• W2016983085 cites W2033088972 @default.
• W2016983085 cites W2038171923 @default.
• W2016983085 cites W2038481055 @default.
• W2016983085 cites W2046933512 @default.
• W2016983085 cites W2069621752 @default.
• W2016983085 cites W2073323005 @default.
• W2016983085 cites W2080133175 @default.
• W2016983085 cites W2080508595 @default.
• W2016983085 cites W2096947423 @default.
• W2016983085 cites W2100291894 @default.
• W2016983085 cites W2106305244 @default.
• W2016983085 cites W2111538369 @default.
• W2016983085 cites W2115137627 @default.
• W2016983085 cites W2117631316 @default.
• W2016983085 cites W2118016880 @default.
• W2016983085 cites W2120103843 @default.
• W2016983085 cites W2120736516 @default.
• W2016983085 cites W2127906377 @default.
• W2016983085 cites W2138158290 @default.
• W2016983085 cites W2140577289 @default.
• W2016983085 cites W2140731089 @default.
• W2016983085 cites W2141300290 @default.
• W2016983085 cites W2151400756 @default.
• W2016983085 cites W2162824898 @default.
• W2016983085 cites W2164282000 @default.
• W2016983085 cites W4250374989 @default.
• W2016983085 cites W4256156441 @default.
• W2016983085 cites W4256495376 @default.
• W2016983085 doi "https://doi.org/10.1016/j.cell.2006.06.051" @default.
• W2016983085 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/16923392" @default.
• W2016983085 hasPublicationYear "2006" @default.
• W2016983085 type Work @default.
• W2016983085 sameAs 2016983085 @default.
• W2016983085 citedByCount "226" @default.
• W2016983085 countsByYear W20169830852012 @default.
• W2016983085 countsByYear W20169830852013 @default.
• W2016983085 countsByYear W20169830852014 @default.
• W2016983085 countsByYear W20169830852015 @default.
• W2016983085 countsByYear W20169830852016 @default.
• W2016983085 countsByYear W20169830852017 @default.
• W2016983085 countsByYear W20169830852018 @default.
• W2016983085 countsByYear W20169830852019 @default.
• W2016983085 countsByYear W20169830852020 @default.
• W2016983085 countsByYear W20169830852021 @default.
• W2016983085 countsByYear W20169830852022 @default.
• W2016983085 countsByYear W20169830852023 @default.
• W2016983085 crossrefType "journal-article" @default.
• W2016983085 hasAuthorship W2016983085A5003539515 @default.
• W2016983085 hasAuthorship W2016983085A5010360422 @default.
• W2016983085 hasAuthorship W2016983085A5036980616 @default.
• W2016983085 hasAuthorship W2016983085A5037305891 @default.
• W2016983085 hasAuthorship W2016983085A5041797262 @default.
• W2016983085 hasAuthorship W2016983085A5042756187 @default.
• W2016983085 hasAuthorship W2016983085A5051950312 @default.
• W2016983085 hasAuthorship W2016983085A5054545550 @default.
• W2016983085 hasAuthorship W2016983085A5064945498 @default.
• W2016983085 hasAuthorship W2016983085A5068450634 @default.
• W2016983085 hasAuthorship W2016983085A5077934127 @default.
• W2016983085 hasAuthorship W2016983085A5080761072 @default.
• W2016983085 hasAuthorship W2016983085A5088448170 @default.
• W2016983085 hasBestOaLocation W20169830851 @default.
• W2016983085 hasConcept C113584667 @default.
• W2016983085 hasConcept C139447449 @default.
• W2016983085 hasConcept C144647389 @default.
• W2016983085 hasConcept C156399914 @default.
• W2016983085 hasConcept C158617107 @default.
• W2016983085 hasConcept C158619295 @default.
• W2016983085 hasConcept C181199279 @default.
• W2016983085 hasConcept C199229279 @default.

• next