The Chromatin-Associated Phf12 Protein Maintains Nucleolar Integrity and Prevents Premature Cellular Senescence

Graveline, Richard; Marcinkiewicz, Katarzyna; Choi, Seyun; Paquet, Marilène; Wurst, Wolfgang; Floss, Thomas; Gourichon, David

doi:10.1128/mcb.00522-16

Cited by 13 publications

(10 citation statements)

References 53 publications

(65 reference statements)

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“…Consistent with previous reports, we identified several members of the canonical Sin3-HDAC complex, which include the following: Sin3A, HDAC1, HDAC2, RBBP7, SAP130, ARID4B, ING1, ING2, SUDS3, SAP30, SAP30L, BRMS1L, and BRMS1 ( Bansal et al, 2016 ) ( Figure 1A ). Additionally, several members of a recently characterized smaller Sin3B complex were identified as well ( Graveline et al, 2017 ; Jelinic et al, 2011 ). These proteins include the following: PHF12, KDM5A, EMSY, and MORF4L1.…”

Section: Resultsmentioning

confidence: 99%

The HDAC-Associated Sin3B Protein Represses DREAM Complex Targets and Cooperates with APC/C to Promote Quiescence

et al. 2018

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SUMMARY The mammalian DREAM complex is responsible for the transcriptional repression of hundreds of cell-cycle-related genes in quiescence. How the DREAM complex recruits chromatin-modifying entities to aid in its repression remains unknown. Using unbiased proteomics analysis, we have uncovered a robust association between the chromatin-associated Sin3B protein and the DREAM complex. We have determined that genetic inactivation of Sin3B results in the de-repression of DREAM target genes during quiescence but is insufficient to allow quiescent cells to resume proliferation. However, inactivation of APC/CCDH1 was sufficient for Sin3B−/− cells, but not parental cells, to re-enter the cell cycle. These studies identify Sin3B as a transcriptional corepressor associated with the DREAM complex in quiescence and reveals a functional cooperation between E2F target repression and APC/CCDH1 in the negative regulation of cell-cycle progression.

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Section: Resultsmentioning

confidence: 99%

The HDAC-Associated Sin3B Protein Represses DREAM Complex Targets and Cooperates with APC/C to Promote Quiescence

et al. 2018

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“…RXFP2 encodes a receptor for glycoprotein hormones that contains a unique low-density lipoprotein type A (LDLa) module ( 57 ); though this gene is not expressed in the adult human retina ( 54 ), its homolog in zebrafish is transcribed in the developing brain and retina ( 58 ). PHF12 encodes a member of the PHD zinc finger family of proteins involved in regulation of ribosomal biogenesis and senescence ( 59 ) and could contribute to AMD pathology through activation of senescence. Although present in only two families, the findings of rare variants in SPEF2 and BCAR1 are also noteworthy as both of these candidates were highlighted as most likely candidate at the AMD-GWAS loci based on a gene priority score ( 16 ).…”

Section: Discussionmentioning

confidence: 99%

Family-based exome sequencing identifies rare coding variants in age-related macular degeneration

Ratnapriya

Acar

Geerlings

et al. 2020

Human Molecular Genetics

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Genome-wide association studies (GWAS) have identified 52 independent variants at 34 genetic loci that are associated with age-related macular degeneration (AMD), the most common cause of incurable vision loss in the elderly worldwide. However, causal genes at the majority of these loci remain unknown. In this study, we performed whole exome sequencing of 264 individuals from 63 multiplex families with AMD and analyzed the data for rare protein-altering variants in candidate target genes at AMD-associated loci. Rare coding variants were identified in the CFH, PUS7, RXFP2, PHF12 and TACC2 genes in three or more families. In addition, we detected rare coding variants in the C9, SPEF2 and BCAR1 genes, which were previously suggested as likely causative genes at respective AMD susceptibility loci. Identification of rare variants in the CFH and C9 genes in our study validated previous reports of rare variants in complement pathway genes in AMD. We then extended our exome-wide analysis and identified rare protein-altering variants in 13 genes outside the AMD-GWAS loci in three or more families. Two of these genes, SCN10A and KIR2DL4, are of interest because variants in these genes also showed association with AMD in case-control cohorts, albeit not at the level of genome-wide significance. Our study presents the first large-scale, exome-wide analysis of rare variants in AMD. Further independent replications and molecular investigation of candidate target genes, reported here, would assist in gaining novel insights into mechanisms underlying AMD pathogenesis.

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“…SUDS3/BRMS1/BRMS1L, SAP30/SAP30L, and ING1/ING2 have homology to Rpd3L-specific components Sds3, Sap30, and Pho23, respectively ( 12 , 13 , 14 ). Components specifically found within Rpd3S, Rco1, and Eaf3, share homology with human PHF12 and MORF4L1, respectively ( 15 , 16 ). Although SIN3A can clearly interact with Rpd3L component homologs, data supports the existence of SIN3B complexes that contain Rpd3S component homologs ( 17 , 18 ).…”

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confidence: 99%

Differential Complex Formation via Paralogs in the Human Sin3 Protein Interaction Network

Adams

Banks

Thornton

et al. 2020

Molecular & Cellular Proteomics

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Despite the continued analysis of HDAC inhibitors in clinical trials, the heterogeneous nature of the protein complexes they target limits our understanding of the beneficial and off-target effects associated with their application. Among the many HDAC protein complexes found within the cell, Sin3 complexes are conserved from yeast to humans and likely play important roles as regulators of transcriptional activity. The presence of two Sin3 paralogs in humans, SIN3A and SIN3B, may result in a heterogeneous population of Sin3 complexes and contributes to our poor understanding of the functional attributes of these complexes. Here, we profile the interaction networks of SIN3A and SIN3B to gain insight into complex composition and organization. In accordance with existing data, we show that Sin3 paralog identity influences complex composition. Additionally, chemical crosslinking mass spectrometry identifies domains that mediate interactions between Sin3 proteins and binding partners. The characterization of rare SIN3B proteoforms provides additional evidence for the existence of conserved and divergent elements within human Sin3 proteins. Together, these findings shed light on both the shared and divergent properties of human Sin3 proteins and highlight the heterogeneous nature of the complexes they organize.

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The Chromatin-Associated Phf12 Protein Maintains Nucleolar Integrity and Prevents Premature Cellular Senescence

Cited by 13 publications

References 53 publications

The HDAC-Associated Sin3B Protein Represses DREAM Complex Targets and Cooperates with APC/C to Promote Quiescence

The HDAC-Associated Sin3B Protein Represses DREAM Complex Targets and Cooperates with APC/C to Promote Quiescence

Family-based exome sequencing identifies rare coding variants in age-related macular degeneration

Differential Complex Formation via Paralogs in the Human Sin3 Protein Interaction Network

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