Detailed Structural-Functional Analysis of the Krüppel-like Factor 16 (KLF16) Transcription Factor Reveals Novel Mechanisms for Silencing Sp/KLF Sites Involved in Metabolism and Endocrinology

Krüppel-like factor (KLF) proteins have elicited significant attention due to their emerging key role in metabolic and endocrine diseases. Here, we extend this knowledge through the biochemical characterization of KLF16, unveiling novel mechanisms regulating expression of genes involved in reproduct...

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Autores principales: Daftary, Gaurang S., Lomberk, Gwen A., Buttar, Navtej S., Allen, Thomas W., Grzenda, Adrienne, Zhang, Jinsan, Zheng, Ye, Mathison, Angela J., Gada, Ravi P., Calvo, Ezequiel, Iovanna, Juan L., Billadeau, Daniel D., Prendergast, Franklyn G., Urrutia, Raul
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Biochemistry and Molecular Biology 2012
Materias:
Gene Regulation
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3293586/
https://www.ncbi.nlm.nih.gov/pubmed/22203677
http://dx.doi.org/10.1074/jbc.M111.266007
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author Daftary, Gaurang S.
Lomberk, Gwen A.
Buttar, Navtej S.
Allen, Thomas W.
Grzenda, Adrienne
Zhang, Jinsan
Zheng, Ye
Mathison, Angela J.
Gada, Ravi P.
Calvo, Ezequiel
Iovanna, Juan L.
Billadeau, Daniel D.
Prendergast, Franklyn G.
Urrutia, Raul
author_facet Daftary, Gaurang S.
Lomberk, Gwen A.
Buttar, Navtej S.
Allen, Thomas W.
Grzenda, Adrienne
Zhang, Jinsan
Zheng, Ye
Mathison, Angela J.
Gada, Ravi P.
Calvo, Ezequiel
Iovanna, Juan L.
Billadeau, Daniel D.
Prendergast, Franklyn G.
Urrutia, Raul
author_sort Daftary, Gaurang S.
collection PubMed
description Krüppel-like factor (KLF) proteins have elicited significant attention due to their emerging key role in metabolic and endocrine diseases. Here, we extend this knowledge through the biochemical characterization of KLF16, unveiling novel mechanisms regulating expression of genes involved in reproductive endocrinology. We found that KLF16 selectively binds three distinct KLF-binding sites (GC, CA, and BTE boxes). KLF16 also regulated the expression of several genes essential for metabolic and endocrine processes in sex steroid-sensitive uterine cells. Mechanistically, we determined that KLF16 possesses an activation domain that couples to histone acetyltransferase-mediated pathways, as well as a repression domain that interacts with the histone deacetylase chromatin-remodeling system via all three Sin3 isoforms, suggesting a higher level of plasticity in chromatin cofactor selection. Molecular modeling combined with molecular dynamic simulations of the Sin3a-KLF16 complex revealed important insights into how this interaction occurs at an atomic resolution level, predicting that phosphorylation of Tyr-10 may modulate KLF16 function. Phosphorylation of KLF16 was confirmed by in vivo (32)P incorporation and controlled by a Y10F site-directed mutant. Inhibition of Src-type tyrosine kinase signaling as well as the nonphosphorylatable Y10F mutation disrupted KLF16-mediated gene silencing, demonstrating that its function is regulatable rather than constitutive. Subcellular localization studies revealed that signal-induced nuclear translocation and euchromatic compartmentalization constitute an additional mechanism for regulating KLF16 function. Thus, this study lends insights on key biochemical mechanisms for regulating KLF sites involved in reproductive biology. These data also contribute to the new functional information that is applicable to understanding KLF16 and other highly related KLF proteins.
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spelling pubmed-32935862012-03-07 Detailed Structural-Functional Analysis of the Krüppel-like Factor 16 (KLF16) Transcription Factor Reveals Novel Mechanisms for Silencing Sp/KLF Sites Involved in Metabolism and Endocrinology Daftary, Gaurang S. Lomberk, Gwen A. Buttar, Navtej S. Allen, Thomas W. Grzenda, Adrienne Zhang, Jinsan Zheng, Ye Mathison, Angela J. Gada, Ravi P. Calvo, Ezequiel Iovanna, Juan L. Billadeau, Daniel D. Prendergast, Franklyn G. Urrutia, Raul J Biol Chem Gene Regulation Krüppel-like factor (KLF) proteins have elicited significant attention due to their emerging key role in metabolic and endocrine diseases. Here, we extend this knowledge through the biochemical characterization of KLF16, unveiling novel mechanisms regulating expression of genes involved in reproductive endocrinology. We found that KLF16 selectively binds three distinct KLF-binding sites (GC, CA, and BTE boxes). KLF16 also regulated the expression of several genes essential for metabolic and endocrine processes in sex steroid-sensitive uterine cells. Mechanistically, we determined that KLF16 possesses an activation domain that couples to histone acetyltransferase-mediated pathways, as well as a repression domain that interacts with the histone deacetylase chromatin-remodeling system via all three Sin3 isoforms, suggesting a higher level of plasticity in chromatin cofactor selection. Molecular modeling combined with molecular dynamic simulations of the Sin3a-KLF16 complex revealed important insights into how this interaction occurs at an atomic resolution level, predicting that phosphorylation of Tyr-10 may modulate KLF16 function. Phosphorylation of KLF16 was confirmed by in vivo (32)P incorporation and controlled by a Y10F site-directed mutant. Inhibition of Src-type tyrosine kinase signaling as well as the nonphosphorylatable Y10F mutation disrupted KLF16-mediated gene silencing, demonstrating that its function is regulatable rather than constitutive. Subcellular localization studies revealed that signal-induced nuclear translocation and euchromatic compartmentalization constitute an additional mechanism for regulating KLF16 function. Thus, this study lends insights on key biochemical mechanisms for regulating KLF sites involved in reproductive biology. These data also contribute to the new functional information that is applicable to understanding KLF16 and other highly related KLF proteins. American Society for Biochemistry and Molecular Biology 2012-03-02 2011-12-27 /pmc/articles/PMC3293586/ /pubmed/22203677 http://dx.doi.org/10.1074/jbc.M111.266007 Text en © 2012 by The American Society for Biochemistry and Molecular Biology, Inc. Author's Choice—Final version full access. Creative Commons Attribution Non-Commercial License (http://creativecommons.org/licenses/by-nc/3.0/) applies to Author Choice Articles
spellingShingle Gene Regulation
Daftary, Gaurang S.
Lomberk, Gwen A.
Buttar, Navtej S.
Allen, Thomas W.
Grzenda, Adrienne
Zhang, Jinsan
Zheng, Ye
Mathison, Angela J.
Gada, Ravi P.
Calvo, Ezequiel
Iovanna, Juan L.
Billadeau, Daniel D.
Prendergast, Franklyn G.
Urrutia, Raul
Detailed Structural-Functional Analysis of the Krüppel-like Factor 16 (KLF16) Transcription Factor Reveals Novel Mechanisms for Silencing Sp/KLF Sites Involved in Metabolism and Endocrinology
title Detailed Structural-Functional Analysis of the Krüppel-like Factor 16 (KLF16) Transcription Factor Reveals Novel Mechanisms for Silencing Sp/KLF Sites Involved in Metabolism and Endocrinology
title_full Detailed Structural-Functional Analysis of the Krüppel-like Factor 16 (KLF16) Transcription Factor Reveals Novel Mechanisms for Silencing Sp/KLF Sites Involved in Metabolism and Endocrinology
title_fullStr Detailed Structural-Functional Analysis of the Krüppel-like Factor 16 (KLF16) Transcription Factor Reveals Novel Mechanisms for Silencing Sp/KLF Sites Involved in Metabolism and Endocrinology
title_full_unstemmed Detailed Structural-Functional Analysis of the Krüppel-like Factor 16 (KLF16) Transcription Factor Reveals Novel Mechanisms for Silencing Sp/KLF Sites Involved in Metabolism and Endocrinology
title_short Detailed Structural-Functional Analysis of the Krüppel-like Factor 16 (KLF16) Transcription Factor Reveals Novel Mechanisms for Silencing Sp/KLF Sites Involved in Metabolism and Endocrinology
title_sort detailed structural-functional analysis of the krüppel-like factor 16 (klf16) transcription factor reveals novel mechanisms for silencing sp/klf sites involved in metabolism and endocrinology
topic Gene Regulation
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3293586/
https://www.ncbi.nlm.nih.gov/pubmed/22203677
http://dx.doi.org/10.1074/jbc.M111.266007
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