Literature DB >> 22158970

Glucocorticoid-dependent phosphorylation of the transcriptional coregulator GRIP1.

Jana Dobrovolna1, Yurii Chinenov, Megan A Kennedy, Bill Liu, Inez Rogatsky.   

Abstract

Much of the regulatory diversity in eukaryotic transcription is provided by coregulators, which are recruited by DNA-binding factors to propagate signaling to basal machinery or chromatin. p160 family members, including the glucocorticoid receptor (GR)-interacting protein 1 (GRIP1), function as coactivators for GR, a ligand-dependent transcription factor of the nuclear receptor superfamily. Unlike other p160s, GRIP1 also potentiates GR-mediated repression of AP1 and NF-κB targets and, surprisingly, transcriptional activation by interferon regulatory factors. What enables GRIP1 activating or repressing properties or discrimination between physiologically antagonistic pathways is unknown. We found that endogenous GRIP1 in mammalian cells undergoes glucocorticoid-induced, GR interaction-dependent phosphorylation and identified one constitutive and six inducible phosphorylation sites and two putative GRIP1 kinases, casein kinase 2 and cyclin-dependent kinase 9. We raised phosphospecific antibodies to the four closely spaced sites in a previously uncharacterized part of GRIP1 which, combined with mutagenesis, revealed the conservation of GRIP1 phosphorylation across several cell types and species and its functional relevance to GR-activated transcription and to response element-specific recruitment of phospho-GRIP1 to native GR targets. We propose that cofactor engagement by GR is neither passive nor stochastic; rather, GR actively imparts modifications that dictate GRIP1 function in a subset of complexes, adding a layer of specificity to GR transcriptional control.

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Year:  2011        PMID: 22158970      PMCID: PMC3272970          DOI: 10.1128/MCB.06473-11

Source DB:  PubMed          Journal:  Mol Cell Biol        ISSN: 0270-7306            Impact factor:   4.272


  44 in total

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2.  CoCoA, a nuclear receptor coactivator which acts through an N-terminal activation domain of p160 coactivators.

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10.  Target-specific utilization of transcriptional regulatory surfaces by the glucocorticoid receptor.

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  14 in total

Review 1.  The Interactome of the Glucocorticoid Receptor and Its Influence on the Actions of Glucocorticoids in Combatting Inflammatory and Infectious Diseases.

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Review 2.  Minireview: nuclear receptor coregulators of the p160 family: insights into inflammation and metabolism.

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Review 3.  Transcriptional coregulators: emerging roles of SRC family of coactivators in disease pathology.

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4.  Role of transcriptional coregulator GRIP1 in the anti-inflammatory actions of glucocorticoids.

Authors:  Yurii Chinenov; Rebecca Gupte; Jana Dobrovolna; Jamie R Flammer; Bill Liu; Francesco E Michelassi; Inez Rogatsky
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Review 6.  The Role of Steroid Receptor Coactivators in Hormone Dependent Cancers and Their Potential as Therapeutic Targets.

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Review 7.  The circadian clock in cancer development and therapy.

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8.  cAMP response element-binding protein interacts with and stimulates the proteasomal degradation of the nuclear receptor coactivator GRIP1.

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Review 9.  Gene-Specific Actions of Transcriptional Coregulators Facilitate Physiological Plasticity: Evidence for a Physiological Coregulator Code.

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Review 10.  Glucocorticoid receptor control of transcription: precision and plasticity via allostery.

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Journal:  Nat Rev Mol Cell Biol       Date:  2017-01-05       Impact factor: 94.444

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