SemOpenAlex |

SemOpenAlex

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2242251224> ?p ?o ?g. }

Showing items 1 to 100 of ±138 with 100 items per page.

W2242251224 endingPage "19769" @default.
W2242251224 startingPage "19756" @default.
W2242251224 abstract "Combinatorial gene regulation through feed-forward loops (FFLs) can bestow specificity and temporal control to client gene expression; however, characteristics of binding sites that mediate these effects are not established. We previously showed that the glucocorticoid receptor (GR) and KLF15 form coherent FFLs that cooperatively induce targets such as the amino acid-metabolizing enzymes AASS and PRODH and incoherent FFLs exemplified by repression of MT2A by KLF15. Here, we demonstrate that GR and KLF15 physically interact and identify low affinity GR binding sites within glucocorticoid response elements (GREs) for PRODH and AASS that contribute to combinatorial regulation with KLF15. We used deep sequencing and electrophoretic mobility shift assays to derive in vitro GR binding affinities across sequence space. We applied these data to show that AASS GRE activity correlated (r2 = 0.73) with predicted GR binding affinities across a 50-fold affinity range in transfection assays; however, the slope of the linear relationship more than doubled when KLF15 was expressed. Whereas activity of the MT2A GRE was even more strongly (r2 = 0.89) correlated with GR binding site affinity, the slope of the linear relationship was sharply reduced by KLF15, consistent with incoherent FFL logic. Thus, GRE architecture and co-regulator expression together determine the functional parameters that relate GR binding site affinity to hormone-induced transcriptional responses. Utilization of specific affinity response functions and GR binding sites by FFLs may contribute to the diversity of gene expression patterns within GR-regulated transcriptomes. Combinatorial gene regulation through feed-forward loops (FFLs) can bestow specificity and temporal control to client gene expression; however, characteristics of binding sites that mediate these effects are not established. We previously showed that the glucocorticoid receptor (GR) and KLF15 form coherent FFLs that cooperatively induce targets such as the amino acid-metabolizing enzymes AASS and PRODH and incoherent FFLs exemplified by repression of MT2A by KLF15. Here, we demonstrate that GR and KLF15 physically interact and identify low affinity GR binding sites within glucocorticoid response elements (GREs) for PRODH and AASS that contribute to combinatorial regulation with KLF15. We used deep sequencing and electrophoretic mobility shift assays to derive in vitro GR binding affinities across sequence space. We applied these data to show that AASS GRE activity correlated (r2 = 0.73) with predicted GR binding affinities across a 50-fold affinity range in transfection assays; however, the slope of the linear relationship more than doubled when KLF15 was expressed. Whereas activity of the MT2A GRE was even more strongly (r2 = 0.89) correlated with GR binding site affinity, the slope of the linear relationship was sharply reduced by KLF15, consistent with incoherent FFL logic. Thus, GRE architecture and co-regulator expression together determine the functional parameters that relate GR binding site affinity to hormone-induced transcriptional responses. Utilization of specific affinity response functions and GR binding sites by FFLs may contribute to the diversity of gene expression patterns within GR-regulated transcriptomes." @default.
W2242251224 created "2016-06-24" @default.
W2242251224 creator A5003863511 @default.
W2242251224 creator A5005992047 @default.
W2242251224 creator A5026136298 @default.
W2242251224 creator A5027692415 @default.
W2242251224 creator A5040496643 @default.
W2242251224 creator A5058932447 @default.
W2242251224 creator A5071781397 @default.
W2242251224 creator A5082564778 @default.
W2242251224 creator A5091869329 @default.
W2242251224 date "2015-08-01" @default.
W2242251224 modified "2023-10-15" @default.
W2242251224 title "Response Element Composition Governs Correlations between Binding Site Affinity and Transcription in Glucocorticoid Receptor Feed-forward Loops" @default.
W2242251224 cites W1964520567 @default.
W2242251224 cites W1965509483 @default.
W2242251224 cites W1968154721 @default.
W2242251224 cites W1968345969 @default.
W2242251224 cites W1971617105 @default.
W2242251224 cites W1980666661 @default.
W2242251224 cites W1982615479 @default.
W2242251224 cites W1983191249 @default.
W2242251224 cites W1989780819 @default.
W2242251224 cites W1990157223 @default.
W2242251224 cites W1992726726 @default.
W2242251224 cites W1992927495 @default.
W2242251224 cites W1997792415 @default.
W2242251224 cites W1998000745 @default.
W2242251224 cites W2001540932 @default.
W2242251224 cites W2001554877 @default.
W2242251224 cites W2003020245 @default.
W2242251224 cites W2003967338 @default.
W2242251224 cites W2006819023 @default.
W2242251224 cites W2019117577 @default.
W2242251224 cites W2021606207 @default.
W2242251224 cites W2025919590 @default.
W2242251224 cites W2026370575 @default.
W2242251224 cites W2030600829 @default.
W2242251224 cites W2031050393 @default.
W2242251224 cites W2033567826 @default.
W2242251224 cites W2034836489 @default.
W2242251224 cites W2039085885 @default.
W2242251224 cites W2045273474 @default.
W2242251224 cites W2050275562 @default.
W2242251224 cites W2061425021 @default.
W2242251224 cites W2084885861 @default.
W2242251224 cites W2089554403 @default.
W2242251224 cites W2099017209 @default.
W2242251224 cites W2102473929 @default.
W2242251224 cites W2109110326 @default.
W2242251224 cites W2113112889 @default.
W2242251224 cites W2123436615 @default.
W2242251224 cites W2124080033 @default.
W2242251224 cites W2131610374 @default.
W2242251224 cites W2132134302 @default.
W2242251224 cites W2148361390 @default.
W2242251224 cites W2152043023 @default.
W2242251224 cites W2152407435 @default.
W2242251224 cites W2152879697 @default.
W2242251224 cites W2153913348 @default.
W2242251224 cites W2157009395 @default.
W2242251224 cites W2157952888 @default.
W2242251224 cites W2162424832 @default.
W2242251224 cites W2167807351 @default.
W2242251224 cites W2170551349 @default.
W2242251224 cites W2170830174 @default.
W2242251224 cites W2171419763 @default.
W2242251224 cites W3104066961 @default.
W2242251224 doi "https://doi.org/10.1074/jbc.m115.668558" @default.
W2242251224 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/4528137" @default.
W2242251224 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/26088140" @default.
W2242251224 hasPublicationYear "2015" @default.
W2242251224 type Work @default.
W2242251224 sameAs 2242251224 @default.
W2242251224 citedByCount "28" @default.
W2242251224 countsByYear W22422512242016 @default.
W2242251224 countsByYear W22422512242017 @default.
W2242251224 countsByYear W22422512242018 @default.
W2242251224 countsByYear W22422512242019 @default.
W2242251224 countsByYear W22422512242020 @default.
W2242251224 countsByYear W22422512242021 @default.
W2242251224 countsByYear W22422512242022 @default.
W2242251224 countsByYear W22422512242023 @default.
W2242251224 crossrefType "journal-article" @default.
W2242251224 hasAuthorship W2242251224A5003863511 @default.
W2242251224 hasAuthorship W2242251224A5005992047 @default.
W2242251224 hasAuthorship W2242251224A5026136298 @default.
W2242251224 hasAuthorship W2242251224A5027692415 @default.
W2242251224 hasAuthorship W2242251224A5040496643 @default.
W2242251224 hasAuthorship W2242251224A5058932447 @default.
W2242251224 hasAuthorship W2242251224A5071781397 @default.
W2242251224 hasAuthorship W2242251224A5082564778 @default.
W2242251224 hasAuthorship W2242251224A5091869329 @default.
W2242251224 hasBestOaLocation W22422512241 @default.
W2242251224 hasConcept C104317684 @default.
W2242251224 hasConcept C107824862 @default.
W2242251224 hasConcept C150194340 @default.
W2242251224 hasConcept C165864922 @default.