Systematic Analysis of SIN3 Histone Modifying Complex Components During Development

Barnes, Valerie L.; Laity, Kelly A; Pilecki, Maksymilian; Pile, Lori A.

doi:10.1038/s41598-018-35093-0

Cited by 11 publications

(9 citation statements)

References 51 publications

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“…Interestingly simultaneous inactivation of SIN3S and SIN3L complex subunits in both athp-1;suds-3 and athp-1;hda-3 double mutant animals resulted in fully penetrant sterility (Figure 2C), suggesting redundant functions in the maintenance of germline function. Alternatively, or in addition, athp-1 , hda-3 and suds-3 may play redundant, sin-3 independent functions required for fertility (Barnes et al, 2018).…”

Section: Resultsmentioning

confidence: 99%

SIN3 acts in distinct complexes to regulate the germline transcriptional program inC. elegans

Caron

Robert

Gely

et al. 2023

Preprint

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The SIN3 transcriptional coregulator influences gene expression through multiple interactions that include histone deacetylases (HDACs). Haploinsufficiency and mutations in SIN3 are the underlying cause of Witteveen-Kolk syndrome and related intellectual disability (ID)/autism syndromes, emphasizing its key role in development. However, little is known about the diversity of its interactions and functions in developmental processes. Here we show that loss of SIN-3, the single SIN3 homologue in Caenorhabditis elegans, results in maternal effect sterility associated with deregulation of the germline transcriptome, including desilencing of X-linked genes. We identify at least two distinct SIN3 complexes containing specific HDACs, and show that they differentially contribute to fertility. Single cell smFISH reveals that in sin-3 mutants, the X chromosome becomes re-expressed prematurely and in a stochastic manner in individual germ cells. Furthermore, we identify histone residues whose acetylation increases in the absence of SIN3. Together, this work provides a powerful framework for the in vivo study of SIN3 and associated proteins.

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Section: Resultsmentioning

confidence: 99%

SIN3 acts in distinct complexes to regulate the germline transcriptional program inC. elegans

Caron

Robert

Gely

et al. 2023

Preprint

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“…Histone demethylase KDM5B, which is part of the PF1 complex, inhibits genes involved in inflammatory response, cell proliferation and cell adhesion in MDA-MB-231 cell line [ 40 , 41 ]. We previously reported that disrupting the interaction of KDM5B with SIN3A results in decrease in H3K4me3 signal and enhances binding of KDM5B to the promoter of ITGA6 gene [11] .…”

Section: Discussionmentioning

confidence: 99%

Invasive phenotype in triple negative breast cancer is inhibited by blocking SIN3A–PF1 interaction through KLF9 mediated repression of ITGA6 and ITGB1

Kadamb¹,

Leibovitch²,

Farías³

et al. 2022

Translational Oncology

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Highlights We show that the PAH2 domain of SIN3A is a target when it is inhibited from binding to PF1 results in inhibition of invasive phenotype in TNBC. Epigenetic repression of integrins expression and downstream pathways results from enhanced binding of KLF9 /SIN3A repressor complex to their promoters. Genome wide transcriptomic analysis showed downregulation of multiple invasion related genes. Tumor growth and lung metastasis were markedly decreased in vivo. Our studies highlight that PF1 might serve as a gatekeeper for trafficking SID protein binding to PAH2 of SIN3A and has functional role in presentation of different regulatory complexes. Blocking the function of PAH2 offers a promising targeted therapy approach for inhibiting the invasive phenotype in TNBC.

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“…Depletion of SIN3A causes loss of proliferative potential 21–23 and depletion of SIN3B inhibits the ability of proliferating cells to exit the cell cycle 21,24–26 . Because of the ability of SIN3 complexes to regulate cell differentiation 4–6 and proliferation in cancer cells, they are drug targets 27–30 . Consequently, several inhibitors have been developed and used in clinical trials 31,32 , however success on this has been limited by the lack of specificity of these compounds towards the distinct HDAC1/2 complexes 33 .…”

Section: Introductionmentioning

confidence: 99%

“…Class I HDACs (HDAC1/2/3/8) represent the principle nuclear deacetylases that regulate transcription. HDAC1 and HDAC2 (HDAC1/2) are essential for cellular differentiation, development [4][5][6][7] and function as part of multi-subunit complexes 8 . HDAC1/2 are Zn 2+ -dependent enzymes which catalyse the nucleophilic attack of a Zn 2+bound water molecule to a Zn 2+ -polarized N-ε-acetyl-lysine side-chain carbonyl.…”

Section: Introductionmentioning

confidence: 99%

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Mechanism of assembly, activation and lysine selection by the SIN3B histone deacetylase complex

Muhammad

Koliopoulos

Roumeliotis

et al. 2023

Preprint

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Histone deacetylase complexes remove histone lysine acetylation, a key post-translational modification that activates transcription at each gene. Although these complexes are drug targets and crucial regulators of organismal physiology, their structure and mechanisms of action are largely unclear. Here, we present the first structure of a complete human SIN3B histone deacetylase holo-complex with and without a substrate mimic. Remarkably, SIN3B encircles the deacetylase and contacts its allosteric basic patch thereby stimulating catalysis. A SIN3B loop inserts into the catalytic tunnel, rearranges to accommodate the acetyl-lysine moiety and stabilises the substrate for specific deacetylation, which is guided by a substrate receptor subunit. Our findings provide a model of specificity for a main transcriptional regulator conserved from yeast to human and a resource of protein-protein interactions for future drug designs.

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Systematic Analysis of SIN3 Histone Modifying Complex Components During Development

Cited by 11 publications

References 51 publications

SIN3 acts in distinct complexes to regulate the germline transcriptional program inC. elegans

SIN3 acts in distinct complexes to regulate the germline transcriptional program inC. elegans

Invasive phenotype in triple negative breast cancer is inhibited by blocking SIN3A–PF1 interaction through KLF9 mediated repression of ITGA6 and ITGB1

Mechanism of assembly, activation and lysine selection by the SIN3B histone deacetylase complex

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