Structural insights into the interaction and activation of histone deacetylase 3 by nuclear receptor corepressors

Codina, Anna; Love, J.; Li, Yun; Lazar, Mitchell A.; Neuhaus, David; Schwabe, John W. R.

doi:10.1073/pnas.0500299102

Cited by 85 publications

(100 citation statements)

References 43 publications

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“…Interestingly, the second SANT motif is part of a histone-interacting domain and functions synergistically with the DAD to promote histone deacetylation (Yu et al, 2003). The DAD of N-CoR/SMRT binds both the aminoand carboxy-termini of HDAC3 (Guenther et al, 2001) and forms a unique four-helical structure (Codina et al, 2005). The requirement for an intricately folded HDAC3 surface for interaction with the corepressors might allow for better regulation of its activity and prevent ectopic functions.…”

Section: Regulation Of Hdac3 Activitymentioning

confidence: 99%

HDAC3: taking the SMRT-N-CoRrect road to repression

2007

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Known histone deacetylases (HDACs) are divided into different classes, and HDAC3 belongs to Class I. Through forming multiprotein complexes with the corepressors SMRT and N-CoR, HDAC3 regulates the transcription of a plethora of genes. A growing list of nonhistone substrates extends the role of HDAC3 beyond transcriptional repression. Here, we review data on the composition, regulation and mechanism of action of the SMRT/ N-CoR-HDAC3 complexes and provide several examples of nontranscriptional functions, to illustrate the wide variety of physiological processes affected by this deacetylase. Furthermore, we discuss the implication of HDAC3 in cancer, focusing on leukemia. We conclude with some thoughts about the potential therapeutic efficacies of HDAC3 activity modulation.

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Section: Regulation Of Hdac3 Activitymentioning

confidence: 99%

HDAC3: taking the SMRT-N-CoRrect road to repression

2007

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“…12 Interestingly, a DAD mutation K449A which was inoffensive to HDAC3:DAD complex formation also abolished deacetylase activity. 16 As K449 is close to the IP4 binding site, the K449A mutation may inactivate the deacetylase via mediation of IP4-HDAC3 interactions, which would suggest that IP4 plays an additional role in the activation of HDAC3, aside from stabilizing the HDAC3:DAD complex. Here, we examine the structural ensemble of HDAC3, specifically: (i) how does this ensemble of HDAC3 structures change between the active HDAC3:DAD:IP4 complex and the inactive apo HDAC3 state?…”

Section: Introductionmentioning

confidence: 99%

Structural insight into the separate roles of inositol tetraphosphate and deacetylase‐activating domain in activation of histone deacetylase 3

et al. 2012

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Histone deacetylases (HDACs) repress transcription by deacetylating acetyllysines on specific histone tails. HDAC3 is implicated in neurodegenerative diseases, certain leukemias, and even in disrupting HIV-1 latency. A recent crystal structure of HDAC3 in complex with the deacetylase-activating domain (DAD) of its corepressor complex revealed an inositol tetraphosphate (IP4) molecule at the protein-protein interface. IP4 was shown to play an important, yet mechanistically ambiguous, role in the activity of HDAC3. The goal of this article is to explore the conformational ensemble of HDAC3 in its inactive apo state and in the presence of each or both of DAD and IP4. Using triplicate, 100 ns molecular dynamic simulations, we study the apo, ternary, and intermediate DAD-bound or IP4-bound HDAC3 states. We find that a population-shift effect is induced by the presence of each corepressor, and is most notable in the presence of both. Our results offer new insights into the change in dynamics necessary for the activation of HDAC3 and highlight the roles of IP4 and DAD in this process.

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“…NCoR (nuclear corepressor 1) and the homologous protein SMRT (silencing mediator or retinoic and thyroid hormone receptors or NCoR2) were identified by their interaction with unliganded thyroid hormone receptors (TRs) and retinoic acid receptors (2, 3), although later studies demonstrated that they also could bind to other transcription factors (4). NCoR and SMRT belong to large complexes that contain histone deacetylases (HDACs), thereby inducing chromatin compaction and gene silencing (4)(5)(6)(7). Although these corepressors interact with multiple HDACs, HDAC3 plays a key role in mediating their actions (8,9) and is essential for repression by TRs (10,11).…”

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confidence: 99%

Autoregulatory loop of nuclear corepressor 1 expression controls invasion, tumor growth, and metastasis

Martínez-Iglesias

Alonso-Merino

Gómez-Rey

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

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Nuclear corepressor 1 (NCoR) associates with nuclear receptors and other transcription factors leading to transcriptional repression. We show here that NCoR depletion enhances cancer cell invasion and increases tumor growth and metastatic potential in nude mice. These changes are related to repressed transcription of genes associated with increased metastasis and poor prognosis in patients. Strikingly, transient NCoR silencing leads to heterochromatinization and stable silencing of the NCoR gene, suggesting that NCoR loss can be propagated, contributing to tumor progression even in the absence of NCoR gene mutations. Down-regulation of the thyroid hormone receptor β1 (TRβ) appears to be associated with cancer onset and progression. We found that expression of TRβ increases NCoR levels and that this induction is essential in mediating inhibition of tumor growth and metastasis by this receptor. Moreover, NCoR is down-regulated in human hepatocarcinomas and in the more aggressive breast cancer tumors, and its expression correlates positively with that of TRβ. These data provide a molecular basis for the anticancer actions of this corepressor and identify NCoR as a potential molecular target for development of novel cancer therapies.nuclear corepressor 1 | thyroid hormone receptor | tumor growth | metastasis | transcription

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Structural insights into the interaction and activation of histone deacetylase 3 by nuclear receptor corepressors

Cited by 85 publications

References 43 publications

HDAC3: taking the SMRT-N-CoRrect road to repression

HDAC3: taking the SMRT-N-CoRrect road to repression

Structural insight into the separate roles of inositol tetraphosphate and deacetylase‐activating domain in activation of histone deacetylase 3

Autoregulatory loop of nuclear corepressor 1 expression controls invasion, tumor growth, and metastasis

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