SemOpenAlex |

SemOpenAlex

Matches in SemOpenAlex for { <https://semopenalex.org/work/W4387406909> ?p ?o ?g. }

Showing items 1 to 75 of 75 with 100 items per page.

W4387406909 endingPage "101871" @default.
W4387406909 startingPage "101871" @default.
W4387406909 abstract "Subclonal heterogeneity and evolution are characteristics of breast cancer (BC), playing a key role in tumour development, progression, and resistance to current therapies. Single-cell (s.c) sequencing studies suggest that subclonal heterogeneity drives therapy response in BC. Here, we sought to identify whether pre-existing transcriptomically defined cell subpopulations underpin CDK4/6 inhibitors (CDK4/6i) resistance in ER+ BC, and to identify the differential resistance mechanisms between different CDK4/6i. ER+ BC cell lines were infected with a lentiviral barcode library and were long-term exposed to DMSO, abemaciclib or palbociclib until resistance was achieved. Barcodes were detected at DNA and s.c RNA level coupled with s.c transcriptomic and whole exome sequencing, as well as protein analysis of the G1/S cell cycle checkpoint. S.c lineage tracing identified stochastic CDK4/6i resistance in MCF7 cells, while resistance in T47D cells was conserved. In all cell models, abemaciclib exerted a stronger selective pressure than palbociclib. Detection of barcodes from dead cells highlighted differential selective pressures of the drugs. S.c transcriptomic sequencing identified shared and differential mechanisms of resistance between cell lines and specific CDK4/6i, suggestive of different subclonal, non-genetic mechanisms driving resistance. Some of these subclones were pre-defined, whereas others were demarked by acquisition of pathway up-regulation. For instance, RB1 copy number loss was identified in palbociclib-resistant T47D cells, indicating RB1 as a genetic driver of resistance. Interestingly, only a subclonal cluster was identified with loss of RB1 expression in palbociclib-resistant MCF7 cells. Abemaciclib-resistant MCF7 cells lost RB1 protein levels, suggesting differential non-genetic mechanisms of resistance to CDK4/6i in MCF7 cells. We identified that resistance to CDK4/6i can be stochastic or conserved as well as pre-existing or acquired according to the cell model, suggesting transcriptomic and epigenomic mechanisms of resistance, with drug-tolerant or drug-induced persistent properties." @default.
W4387406909 created "2023-10-07" @default.
W4387406909 creator A5038111669 @default.
W4387406909 creator A5042973046 @default.
W4387406909 creator A5052903538 @default.
W4387406909 creator A5055633694 @default.
W4387406909 creator A5057324933 @default.
W4387406909 creator A5074169715 @default.
W4387406909 creator A5093018050 @default.
W4387406909 date "2023-10-01" @default.
W4387406909 modified "2023-10-08" @default.
W4387406909 title "61P Deconvoluting the intra-tumour heterogeneity and subclonal evolution of CDK4/6 inhibitor resistance in ER+ breast cancer" @default.
W4387406909 doi "https://doi.org/10.1016/j.esmoop.2023.101871" @default.
W4387406909 hasPublicationYear "2023" @default.
W4387406909 type Work @default.
W4387406909 citedByCount "0" @default.
W4387406909 crossrefType "journal-article" @default.
W4387406909 hasAuthorship W4387406909A5038111669 @default.
W4387406909 hasAuthorship W4387406909A5042973046 @default.
W4387406909 hasAuthorship W4387406909A5052903538 @default.
W4387406909 hasAuthorship W4387406909A5055633694 @default.
W4387406909 hasAuthorship W4387406909A5057324933 @default.
W4387406909 hasAuthorship W4387406909A5074169715 @default.
W4387406909 hasAuthorship W4387406909A5093018050 @default.
W4387406909 hasBestOaLocation W43874069091 @default.
W4387406909 hasConcept C104317684 @default.
W4387406909 hasConcept C120089663 @default.
W4387406909 hasConcept C121608353 @default.
W4387406909 hasConcept C132917006 @default.
W4387406909 hasConcept C141231307 @default.
W4387406909 hasConcept C150194340 @default.
W4387406909 hasConcept C162317418 @default.
W4387406909 hasConcept C199649820 @default.
W4387406909 hasConcept C2775930923 @default.
W4387406909 hasConcept C2779744173 @default.
W4387406909 hasConcept C29537977 @default.
W4387406909 hasConcept C502942594 @default.
W4387406909 hasConcept C530470458 @default.
W4387406909 hasConcept C54355233 @default.
W4387406909 hasConcept C86803240 @default.
W4387406909 hasConceptScore W4387406909C104317684 @default.
W4387406909 hasConceptScore W4387406909C120089663 @default.
W4387406909 hasConceptScore W4387406909C121608353 @default.
W4387406909 hasConceptScore W4387406909C132917006 @default.
W4387406909 hasConceptScore W4387406909C141231307 @default.
W4387406909 hasConceptScore W4387406909C150194340 @default.
W4387406909 hasConceptScore W4387406909C162317418 @default.
W4387406909 hasConceptScore W4387406909C199649820 @default.
W4387406909 hasConceptScore W4387406909C2775930923 @default.
W4387406909 hasConceptScore W4387406909C2779744173 @default.
W4387406909 hasConceptScore W4387406909C29537977 @default.
W4387406909 hasConceptScore W4387406909C502942594 @default.
W4387406909 hasConceptScore W4387406909C530470458 @default.
W4387406909 hasConceptScore W4387406909C54355233 @default.
W4387406909 hasConceptScore W4387406909C86803240 @default.
W4387406909 hasIssue "1" @default.
W4387406909 hasLocation W43874069091 @default.
W4387406909 hasOpenAccess W4387406909 @default.
W4387406909 hasPrimaryLocation W43874069091 @default.
W4387406909 hasRelatedWork W2520173420 @default.
W4387406909 hasRelatedWork W2791202581 @default.
W4387406909 hasRelatedWork W2885920666 @default.
W4387406909 hasRelatedWork W2918928681 @default.
W4387406909 hasRelatedWork W2945182925 @default.
W4387406909 hasRelatedWork W2953375339 @default.
W4387406909 hasRelatedWork W2992891112 @default.
W4387406909 hasRelatedWork W3087024909 @default.
W4387406909 hasRelatedWork W3167626185 @default.
W4387406909 hasRelatedWork W4237244757 @default.
W4387406909 hasVolume "8" @default.
W4387406909 isParatext "false" @default.
W4387406909 isRetracted "false" @default.
W4387406909 workType "article" @default.