FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2046751322> ?p ?o ?g. }

• W2046751322 endingPage "390a" @default.
• W2046751322 startingPage "390a" @default.
• W2046751322 abstract "Light microscopically detectable, non-membrane bound cellular “bodies” are large protein assemblies with liquid-like properties, but the biophysical basis of their formation is unclear. Weak, multivalent protein interactions can result in higher-order complexes and can enable the formation of cellular bodies. The inherent size heterogeneity of higher-order complexes renders them difficult to characterize biophysically. As a result, their size distributions remain largely unquantified, limiting molecular insight into their biological functions. We report a novel mechanism governing cellular body formation of the Speckle-type POZ protein (SPOP), which was recently identified as tumor suppressor, is a ubiquitin ligase substrate adaptor that localizes to nuclear puncta. We demonstrate that its cellular localization is dependent upon the ability of SPOP to form higher-order homo-oligomers through indefinite self-association, mediated by two distinct oligomerization domains. Furthermore, in vitro ubiquitination of substrates is enhanced through higher-order self-association of SPOP, suggesting that SPOP puncta are hotspots of substrate ubiquitination. One of SPOP's domains dimerizes with nanomolar affinity yielding stable SPOP dimers as “building blocks” for indefinite self-association, while the other domain dimerizes with micromolar affinity, rendering SPOP oligomers highly dynamic. Together, this results in isodesmic self-association, in which each addition of a dimer occurs with the same affinity, independent of the oligomer size. From this model, we describe the size distribution of SPOP oligomers, providing for the first time a quantitative analysis of protein assemblies participating in the formation of cellular bodies. Mutations within both oligomerization domains have been observed in a variety of cancers, supporting our conclusion that SPOP self-association is important for its biological function. We propose that dynamic, higher-order protein self-association is a general mechanism underlying the formation of cellular bodies, which may serve as switches to fine-tune signaling cascades." @default.
• W2046751322 created "2016-06-24" @default.
• W2046751322 creator A5016735960 @default.
• W2046751322 creator A5017768072 @default.
• W2046751322 creator A5024895227 @default.
• W2046751322 creator A5027447638 @default.
• W2046751322 creator A5042319862 @default.
• W2046751322 creator A5054568408 @default.
• W2046751322 creator A5058009413 @default.
• W2046751322 creator A5085540282 @default.
• W2046751322 date "2015-01-01" @default.
• W2046751322 modified "2023-09-28" @default.
• W2046751322 title "The Role of Higher-Order SPOP Oligomers for Localization to Cellular “Bodies” and Ubiquitination Activity" @default.
• W2046751322 doi "https://doi.org/10.1016/j.bpj.2014.11.2135" @default.
• W2046751322 hasPublicationYear "2015" @default.
• W2046751322 type Work @default.
• W2046751322 sameAs 2046751322 @default.
• W2046751322 citedByCount "0" @default.
• W2046751322 crossrefType "journal-article" @default.
• W2046751322 hasAuthorship W2046751322A5016735960 @default.
• W2046751322 hasAuthorship W2046751322A5017768072 @default.
• W2046751322 hasAuthorship W2046751322A5024895227 @default.
• W2046751322 hasAuthorship W2046751322A5027447638 @default.
• W2046751322 hasAuthorship W2046751322A5042319862 @default.
• W2046751322 hasAuthorship W2046751322A5054568408 @default.
• W2046751322 hasAuthorship W2046751322A5058009413 @default.
• W2046751322 hasAuthorship W2046751322A5085540282 @default.
• W2046751322 hasBestOaLocation W20467513221 @default.
• W2046751322 hasConcept C104317684 @default.
• W2046751322 hasConcept C12554922 @default.
• W2046751322 hasConcept C134459356 @default.
• W2046751322 hasConcept C178790620 @default.
• W2046751322 hasConcept C185592680 @default.
• W2046751322 hasConcept C25602115 @default.
• W2046751322 hasConcept C2779546866 @default.
• W2046751322 hasConcept C2780642029 @default.
• W2046751322 hasConcept C55493867 @default.
• W2046751322 hasConcept C86803240 @default.
• W2046751322 hasConcept C95444343 @default.
• W2046751322 hasConceptScore W2046751322C104317684 @default.
• W2046751322 hasConceptScore W2046751322C12554922 @default.
• W2046751322 hasConceptScore W2046751322C134459356 @default.
• W2046751322 hasConceptScore W2046751322C178790620 @default.
• W2046751322 hasConceptScore W2046751322C185592680 @default.
• W2046751322 hasConceptScore W2046751322C25602115 @default.
• W2046751322 hasConceptScore W2046751322C2779546866 @default.
• W2046751322 hasConceptScore W2046751322C2780642029 @default.
• W2046751322 hasConceptScore W2046751322C55493867 @default.
• W2046751322 hasConceptScore W2046751322C86803240 @default.
• W2046751322 hasConceptScore W2046751322C95444343 @default.
• W2046751322 hasIssue "2" @default.
• W2046751322 hasLocation W20467513221 @default.
• W2046751322 hasOpenAccess W2046751322 @default.
• W2046751322 hasPrimaryLocation W20467513221 @default.
• W2046751322 hasRelatedWork W1978281344 @default.
• W2046751322 hasRelatedWork W1997999470 @default.
• W2046751322 hasRelatedWork W1998363973 @default.
• W2046751322 hasRelatedWork W2023262742 @default.
• W2046751322 hasRelatedWork W2038058791 @default.
• W2046751322 hasRelatedWork W2039275754 @default.
• W2046751322 hasRelatedWork W2046891927 @default.
• W2046751322 hasRelatedWork W2060043254 @default.
• W2046751322 hasRelatedWork W2062044289 @default.
• W2046751322 hasRelatedWork W2085405404 @default.
• W2046751322 hasRelatedWork W2088376141 @default.
• W2046751322 hasRelatedWork W2094460693 @default.
• W2046751322 hasRelatedWork W2306920531 @default.
• W2046751322 hasRelatedWork W2478720019 @default.
• W2046751322 hasRelatedWork W2756277728 @default.
• W2046751322 hasRelatedWork W2760842882 @default.
• W2046751322 hasRelatedWork W2950057192 @default.
• W2046751322 hasRelatedWork W3092687939 @default.
• W2046751322 hasRelatedWork W3111769181 @default.
• W2046751322 hasRelatedWork W2613566146 @default.
• W2046751322 hasVolume "108" @default.
• W2046751322 isParatext "false" @default.
• W2046751322 isRetracted "false" @default.
• W2046751322 magId "2046751322" @default.
• W2046751322 workType "article" @default.