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dc.creatorCaligiuri, I
dc.creatorToffoli, G
dc.creatorGiordano, A
dc.creatorRizzolio, F
dc.date.accessioned2021-01-31T20:40:16Z
dc.date.available2021-01-31T20:40:16Z
dc.date.issued2013-01-01
dc.identifier.issn1949-2553
dc.identifier.issn1949-2553
dc.identifier.doihttp://dx.doi.org/10.34944/dspace/5403
dc.identifier.other23900261 (pubmed)
dc.identifier.urihttp://hdl.handle.net/20.500.12613/5421
dc.description.abstractA cross talk between the Estrogen Receptor (ESR1) and the Retinoblastoma (pRb) pathway has been demonstrated to influence the therapeutic response of breast cancer patients but the full mechanism remains poorly understood. Here we show that the N-terminal domain of pRb interacts with the CD domain of ESR1 to allow for the assembly of intermediate complex chaperone proteins HSP90 and p23. We demonstrated that a loss of pRb in human/mouse breast cells decreases the expression of the ESR1 protein through the proteasome pathway. Our work reveals a novel regulatory mechanism of ESR1 basal turnover and activity and an unanticipated relationship with the pRb tumor suppressor.
dc.format.extent875-883
dc.language.isoen
dc.relation.haspartOncotarget
dc.relation.isreferencedbyImpact Journals, LLC
dc.rightsCC BY
dc.rights.urihttp://creativecommons.org/licenses/by/3.0/
dc.subjectpRb
dc.subjectEstrogen receptor alpha
dc.subjectproteasome
dc.subjectchaperone proteins
dc.subjectbreast cancer
dc.titlepRb controls estrogen receptor alpha protein stability and activity
dc.typeArticle
dc.type.genreJournal Article
dc.relation.doi10.18632/oncotarget.1036
dc.ada.noteFor Americans with Disabilities Act (ADA) accommodation, including help with reading this content, please contact scholarshare@temple.edu
dc.creator.orcidGiordano, Antonio|0000-0002-5959-016X
dc.date.updated2021-01-31T20:40:12Z
refterms.dateFOA2021-01-31T20:40:16Z


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