FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2122922182> ?p ?o ?g. }

• W2122922182 abstract "Many years of oncogenic insult and hormonal flux have important long-term implications for breast cancer emergence and progression. Premature-induced senescence is proposed to be a protective response against cancer development. We hypothesize that the senescence response can be subverted in some breast carcinomas, which exhibit latent hormone-dependent proliferative capacity. The ARF-p53 pathway has long been known to play an important role in tumour surveillance halting cell cycle progression to transiently or permanently stop aberrant cells from proliferating. It is well documented that disruption of this pathway is involved in tumourigenesis, in part, through inactivation of cyclin D1. Cyclin D1 plays an important role in breast cancer progression as a regulator of CDK4/6. In addition cyclin D1 has been reported to stimulate estrogen receptor (ER) activity independent of CDK4/6. Our initial observations showed that reactivation of ARF-p53-p21 is indeed a potent rapid inhibitor of cell proliferation in MCF-7 breast cancer cells with a senescent phenotype, however controversially cyclin D1 expression was increased and predominantly located in the nucleus. High expression of nuclear cyclin D1 and p14ARF inversely correlated with cell proliferation. Our studies showed that p14ARF regulated cyclin D1 at the post-transcriptional level. Furthermore, we have evidence from microRNA array analysis that microRNAs known to bind to the cyclin D1 39UTR sequence were down regulated upon induction of p14ARF, contributing to cyclin D1 stability. We found that long-term exposure to p14ARF was not a failsafe barrier to tumour progression, senescent-like cells re-entering the cell cycle correlated with reduction of nuclear cyclin D1. Conversely, continuous p14ARF expression resulted in chaotic multinucleation and preceded neoplasia. These aberrant nuclei co-stained with cyclin D1 and Ki-67, a well-known marker of cell proliferation. These results suggest that induction of the p14ARF-p53 pathway does not entirely remove the threat of cancer resulting from hyperproliferative oncogenic signals and cyclin D1 plays a promiscuous role in prevention and progression. Arguably, in some breast cancers premature senescent cells may be precursor, or latent cancer cells. Citation Information: Cancer Res 2010;70(24 Suppl):Abstract nr P1-04-03." @default.
• W2122922182 created "2016-06-24" @default.
• W2122922182 creator A5031683008 @default.
• W2122922182 creator A5037120569 @default.
• W2122922182 creator A5059585715 @default.
• W2122922182 creator A5075874555 @default.
• W2122922182 creator A5075953252 @default.
• W2122922182 creator A5085811477 @default.
• W2122922182 date "2010-12-15" @default.
• W2122922182 modified "2023-09-27" @default.
• W2122922182 title "Abstract P1-04-03: A Role for Cyclin D1 in Neoplastic Transformation in MCF-7 Breast Cancer Cells Post p14ARF-p53 Induced Senescence" @default.
• W2122922182 doi "https://doi.org/10.1158/0008-5472.sabcs10-p1-04-03" @default.
• W2122922182 hasPublicationYear "2010" @default.
• W2122922182 type Work @default.
• W2122922182 sameAs 2122922182 @default.
• W2122922182 citedByCount "0" @default.
• W2122922182 crossrefType "proceedings-article" @default.
• W2122922182 hasAuthorship W2122922182A5031683008 @default.
• W2122922182 hasAuthorship W2122922182A5037120569 @default.
• W2122922182 hasAuthorship W2122922182A5059585715 @default.
• W2122922182 hasAuthorship W2122922182A5075874555 @default.
• W2122922182 hasAuthorship W2122922182A5075953252 @default.
• W2122922182 hasAuthorship W2122922182A5085811477 @default.
• W2122922182 hasConcept C11882975 @default.
• W2122922182 hasConcept C120089663 @default.
• W2122922182 hasConcept C121608353 @default.
• W2122922182 hasConcept C16438837 @default.
• W2122922182 hasConcept C199835354 @default.
• W2122922182 hasConcept C2776750431 @default.
• W2122922182 hasConcept C2778264664 @default.
• W2122922182 hasConcept C29537977 @default.
• W2122922182 hasConcept C502942594 @default.
• W2122922182 hasConcept C522857546 @default.
• W2122922182 hasConcept C530470458 @default.
• W2122922182 hasConcept C54355233 @default.
• W2122922182 hasConcept C555283112 @default.
• W2122922182 hasConcept C86803240 @default.
• W2122922182 hasConcept C94561458 @default.
• W2122922182 hasConcept C95444343 @default.
• W2122922182 hasConcept C9743823 @default.
• W2122922182 hasConceptScore W2122922182C11882975 @default.
• W2122922182 hasConceptScore W2122922182C120089663 @default.
• W2122922182 hasConceptScore W2122922182C121608353 @default.
• W2122922182 hasConceptScore W2122922182C16438837 @default.
• W2122922182 hasConceptScore W2122922182C199835354 @default.
• W2122922182 hasConceptScore W2122922182C2776750431 @default.
• W2122922182 hasConceptScore W2122922182C2778264664 @default.
• W2122922182 hasConceptScore W2122922182C29537977 @default.
• W2122922182 hasConceptScore W2122922182C502942594 @default.
• W2122922182 hasConceptScore W2122922182C522857546 @default.
• W2122922182 hasConceptScore W2122922182C530470458 @default.
• W2122922182 hasConceptScore W2122922182C54355233 @default.
• W2122922182 hasConceptScore W2122922182C555283112 @default.
• W2122922182 hasConceptScore W2122922182C86803240 @default.
• W2122922182 hasConceptScore W2122922182C94561458 @default.
• W2122922182 hasConceptScore W2122922182C95444343 @default.
• W2122922182 hasConceptScore W2122922182C9743823 @default.
• W2122922182 hasLocation W21229221821 @default.
• W2122922182 hasOpenAccess W2122922182 @default.
• W2122922182 hasPrimaryLocation W21229221821 @default.
• W2122922182 hasRelatedWork W1526550377 @default.
• W2122922182 hasRelatedWork W1899571856 @default.
• W2122922182 hasRelatedWork W1981609596 @default.
• W2122922182 hasRelatedWork W2013217382 @default.
• W2122922182 hasRelatedWork W2030606384 @default.
• W2122922182 hasRelatedWork W2032199394 @default.
• W2122922182 hasRelatedWork W2062349989 @default.
• W2122922182 hasRelatedWork W2092075416 @default.
• W2122922182 hasRelatedWork W2096261772 @default.
• W2122922182 hasRelatedWork W2131214970 @default.
• W2122922182 hasRelatedWork W2166888963 @default.
• W2122922182 hasRelatedWork W2254898664 @default.
• W2122922182 hasRelatedWork W2315926836 @default.
• W2122922182 hasRelatedWork W2709024209 @default.
• W2122922182 hasRelatedWork W2887164240 @default.
• W2122922182 hasRelatedWork W2892718458 @default.
• W2122922182 hasRelatedWork W2973263543 @default.
• W2122922182 hasRelatedWork W3082322777 @default.
• W2122922182 hasRelatedWork W3085552444 @default.
• W2122922182 hasRelatedWork W3092103280 @default.
• W2122922182 isParatext "false" @default.
• W2122922182 isRetracted "false" @default.
• W2122922182 magId "2122922182" @default.
• W2122922182 workType "article" @default.