FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W4281630168> ?p ?o ?g. }

• W4281630168 abstract "Background. Rearranged during transfection (RET) tyrosine kinase signaling has been previously implicated in endocrine resistant breast cancer, however the mechanism by which this signaling cascade promotes resistance is currently not well described. We recently reported that glial-cell derived neurotrophic factor (GDNF)-RET signaling appears to promote a positive feedback loop with the transcription factor early growth response 1 (EGR1). Here we investigate the mechanism behind this feedback loop and test the hypothesis that GDNF-RET signaling forms a regulatory loop with EGR1 to upregulate cyclin D1 (CCND1) transcription, leading to cell cycle progression and tamoxifen resistance. Methods. To gain a better understanding of the GDNF-RET-EGR1 resistance mechanism, we studied the GDNF-EGR1 positive feedback loop and the role of GDNF and EGR1 in endocrine resistance by modulating their transcription levels using CRISPR-dCAS9 in tamoxifen sensitive (TamS) and tamoxifen resistant (TamR) MCF-7 cells. Additionally, we performed kinetic studies using recombinant GDNF (rGDNF) treatment of TamS cells. Statistical significance for qPCR and chromatin immunoprecipitation (ChIP)-qPCR was determined using a student′s t-test. Results. GDNF-RET signaling formed a positive feedback loop with EGR1 and also downregulated estrogen receptor 1 (ESR1) transcription. Upregulation of GDNF and EGR1 promoted tamoxifen resistance in TamS cells and downregulation of GDNF promoted tamoxifen sensitivity in TamR cells. Additionally, we show that rGDNF treatment activated GDNF-RET signaling in TamS cells, leading to recruitment of p-ELK-1 to the EGR1 promoter, upregulation of EGR1 mRNA and protein, binding of EGR1 to the GDNF and CCND1 promoters, increased GDNF protein expression, and subsequent upregulation of CCND1 mRNA levels. Conclusion. Outcomes from these studies support the hypotheses that GDNF-RET signaling forms a positive feedback loop with the transcription factor EGR1, and that GDNF-RET-EGR1 signaling promotes endocrine resistance via signaling to cyclin D1. Inhibition of components of this signaling pathway could lead to therapeutic insights into the treatment of endocrine resistant breast cancer." @default.
• W4281630168 created "2022-06-13" @default.
• W4281630168 creator A5007598622 @default.
• W4281630168 creator A5024923108 @default.
• W4281630168 creator A5046857559 @default.
• W4281630168 creator A5083337209 @default.
• W4281630168 creator A5085666952 @default.
• W4281630168 creator A5086387749 @default.
• W4281630168 creator A5087768585 @default.
• W4281630168 date "2022-05-31" @default.
• W4281630168 modified "2023-10-14" @default.
• W4281630168 title "GDNF-RET signaling and EGR1 form a positive feedback loop that promotes tamoxifen resistance via cyclin D1" @default.
• W4281630168 doi "https://doi.org/10.1101/2022.05.31.492660" @default.
• W4281630168 hasPublicationYear "2022" @default.
• W4281630168 type Work @default.
• W4281630168 citedByCount "0" @default.
• W4281630168 crossrefType "posted-content" @default.
• W4281630168 hasAuthorship W4281630168A5007598622 @default.
• W4281630168 hasAuthorship W4281630168A5024923108 @default.
• W4281630168 hasAuthorship W4281630168A5046857559 @default.
• W4281630168 hasAuthorship W4281630168A5083337209 @default.
• W4281630168 hasAuthorship W4281630168A5085666952 @default.
• W4281630168 hasAuthorship W4281630168A5086387749 @default.
• W4281630168 hasAuthorship W4281630168A5087768585 @default.
• W4281630168 hasBestOaLocation W42816301681 @default.
• W4281630168 hasConcept C104317684 @default.
• W4281630168 hasConcept C121608353 @default.
• W4281630168 hasConcept C127561419 @default.
• W4281630168 hasConcept C1491633281 @default.
• W4281630168 hasConcept C160539049 @default.
• W4281630168 hasConcept C170493617 @default.
• W4281630168 hasConcept C185856081 @default.
• W4281630168 hasConcept C199835354 @default.
• W4281630168 hasConcept C2777176818 @default.
• W4281630168 hasConcept C2780600689 @default.
• W4281630168 hasConcept C29537977 @default.
• W4281630168 hasConcept C502942594 @default.
• W4281630168 hasConcept C530470458 @default.
• W4281630168 hasConcept C54355233 @default.
• W4281630168 hasConcept C55493867 @default.
• W4281630168 hasConcept C86339819 @default.
• W4281630168 hasConcept C86803240 @default.
• W4281630168 hasConcept C94296188 @default.
• W4281630168 hasConcept C95444343 @default.
• W4281630168 hasConceptScore W4281630168C104317684 @default.
• W4281630168 hasConceptScore W4281630168C121608353 @default.
• W4281630168 hasConceptScore W4281630168C127561419 @default.
• W4281630168 hasConceptScore W4281630168C1491633281 @default.
• W4281630168 hasConceptScore W4281630168C160539049 @default.
• W4281630168 hasConceptScore W4281630168C170493617 @default.
• W4281630168 hasConceptScore W4281630168C185856081 @default.
• W4281630168 hasConceptScore W4281630168C199835354 @default.
• W4281630168 hasConceptScore W4281630168C2777176818 @default.
• W4281630168 hasConceptScore W4281630168C2780600689 @default.
• W4281630168 hasConceptScore W4281630168C29537977 @default.
• W4281630168 hasConceptScore W4281630168C502942594 @default.
• W4281630168 hasConceptScore W4281630168C530470458 @default.
• W4281630168 hasConceptScore W4281630168C54355233 @default.
• W4281630168 hasConceptScore W4281630168C55493867 @default.
• W4281630168 hasConceptScore W4281630168C86339819 @default.
• W4281630168 hasConceptScore W4281630168C86803240 @default.
• W4281630168 hasConceptScore W4281630168C94296188 @default.
• W4281630168 hasConceptScore W4281630168C95444343 @default.
• W4281630168 hasLocation W42816301681 @default.
• W4281630168 hasOpenAccess W4281630168 @default.
• W4281630168 hasPrimaryLocation W42816301681 @default.
• W4281630168 hasRelatedWork W10480338 @default.
• W4281630168 hasRelatedWork W11835625 @default.
• W4281630168 hasRelatedWork W13627206 @default.
• W4281630168 hasRelatedWork W16191524 @default.
• W4281630168 hasRelatedWork W16955145 @default.
• W4281630168 hasRelatedWork W19669284 @default.
• W4281630168 hasRelatedWork W26244105 @default.
• W4281630168 hasRelatedWork W38828767 @default.
• W4281630168 hasRelatedWork W4874447 @default.
• W4281630168 hasRelatedWork W9238215 @default.
• W4281630168 isParatext "false" @default.
• W4281630168 isRetracted "false" @default.
• W4281630168 workType "article" @default.