Affinage

SUDS3

Sin3 histone deacetylase corepressor complex component SDS3 · UniProt Q9H7L9

Length
328 aa
Mass
38.1 kDa
Annotated
2026-06-10
12 papers in source corpus 11 papers cited in narrative 11 extracted findings
Cross-family judge vs UniProt: Affinage preferred faithfulness: 6/6 claims corpus-supported (100%)

Mechanistic narrative

Synthesis pass · prose summary of the discoveries below

SUDS3/SDS3 is a conserved, integral subunit of the Sin3/Rpd3(HDAC) corepressor complex that is essential for both the physical integrity of the complex and its histone deacetylase catalytic output (PMID:11024051, PMID:11909966). First defined genetically in yeast as a factor acting in the same transcriptional-silencing pathway as SIN3 and RPD3 (PMID:8978024, PMID:10655212), Sds3 was shown by chromatographic fractionation to be required to hold Sin3 and Rpd3 together; loss of Sds3 separates the subunits and abolishes HDAC activity (PMID:11024051). The mammalian ortholog associates with mSin3A/mSin3B in vivo, represses transcription in an HDAC-dependent manner, and is required to enable HDAC1 catalytic activity (PMID:11909966). Structurally, Sds3 engages Sin3A through a bipartite Sin3-interaction domain (SID) comprising a helix and an extended segment that samples two discrete conformations, and provides a homodimerization activity needed to assemble the 1–2 MDa Sin3L/Rpd3L complex (PMID:26522936). SDS3-associated HDAC activity is negatively regulated by a ubiquitin switch: SDS3 carries Lys-63-linked polyubiquitin chains that the deubiquitinase USP17 removes through a direct physical interaction (PMID:21239494). Through chromatin deacetylation at specific targets, SDS3 represses genes including ASK1 to control p38 MAPK signaling and microglial inflammatory responses (PMID:39008037), and is required in early mouse development for FGF4/ERK-dependent lineage specification (PMID:23123966).

Mechanistic history

Synthesis pass · year-by-year structured walk · 8 steps
  1. 1996 Medium

    Established that SDS3 acts in transcriptional silencing alongside SIN3 and RPD3, raising the question of whether it is a dedicated component of the same machinery.

    Evidence Suppressor genetic screen and epistasis with reporter assays in S. cerevisiae

    PMID:8978024

    Open questions at the time
    • Genetic only — no biochemical demonstration of complex membership
    • Did not show whether SDS3 is required for HDAC activity
  2. 2000 High

    Defined the core mechanistic role of Sds3 by showing it is physically required to hold the Rpd3·Sin3 complex together and to sustain its deacetylase activity.

    Evidence Chromatographic fractionation, Co-IP, and in vitro HDAC assays in sds3Δ yeast; complemented by reciprocal genetic/Co-IP analysis

    PMID:10655212 PMID:11024051

    Open questions at the time
    • Structural basis of how Sds3 bridges Sin3 and Rpd3 not resolved
    • Conducted in yeast — mammalian relevance not yet shown
  3. 2002 High

    Extended the function to mammals, establishing mSds3 as an integral Sin3A/B-HDAC subunit required for HDAC1 catalytic activity in vivo.

    Evidence Co-IP with mSin3, transcriptional repression assays, and HDAC activity assays in mammalian cells

    PMID:11909966

    Open questions at the time
    • Specific target genes in mammals not defined
    • Domain mediating Sin3 contact not mapped
  4. 2011 High

    Identified a post-translational control of SDS3-associated HDAC activity, showing K63-linked ubiquitination of SDS3 is reversed by USP17 to tune deacetylase output.

    Evidence Co-IP, GST pull-down, MALDI-TOF-MS, linkage-specific ubiquitination and HDAC activity assays

    PMID:21239494

    Open questions at the time
    • E3 ligase adding the K63 chains not identified
    • Site of ubiquitination on SDS3 not mapped
  5. 2012 Medium

    Resolved the molecular interface and oligomeric requirement, showing SDS3 binds Sin3A via a bipartite SID and homodimerizes to assemble the megadalton Sin3L/Rpd3L complex.

    Evidence Solution NMR spectroscopy with conformational-exchange analysis

    PMID:26522936

    Open questions at the time
    • Limited mutagenesis/functional validation of the dimerization interface
    • No full complex structure
  6. 2012 Low

    Connected SDS3 to specific physiological repression programs, including ligand-specific AhR/ARNT repression and a non-canonical hyaluronan-binding activity.

    Evidence Co-IP with ARNT plus knockdown in thymocytes; CPC hyaluronan binding and HABM-deletion assays

    PMID:22662218 PMID:22981438

    Open questions at the time
    • ARNT association rests on single Co-IP and knockdown without reciprocal validation
    • Functional consequence of hyaluronan binding unresolved
  7. 2012 Medium

    Placed SDS3 in a developmental program, showing it is required for FGF4/ERK signaling and primitive endoderm lineage specification in early mouse embryos.

    Evidence Suds3 knockdown in mouse blastocysts with lineage-marker immunofluorescence and FGF4 rescue

    PMID:23123966

    Open questions at the time
    • Direct transcriptional targets mediating FGF4 regulation not identified
    • Single-lab knockdown without genetic null
  8. 2024 Medium

    Identified direct SDS3 target genes, showing repression of ASK1 controls p38 MAPK activation and microglial inflammation.

    Evidence ChIP combined with transcriptomics/proteomics, SDS3 knockdown, and downstream pathway validation

    PMID:39008037

    Open questions at the time
    • Whether ASK1 regulation generalizes beyond microglia unknown
    • Recruitment of the complex to the ASK1 locus not defined

Open questions

Synthesis pass · forward-looking unresolved questions
  • How SDS3 recruitment, its ubiquitin switch, and its bipartite Sin3 interface are integrated to direct target-gene selection across tissues remains unresolved.
  • E3 ligase and ubiquitination sites unmapped
  • Genome-wide target catalog incomplete
  • No integrated structure of the assembled complex

Mechanism profile

Synthesis pass · controlled-vocabulary classification · explore literature graph →
Molecular activity
GO:0140096 catalytic activity, acting on a protein 3 GO:0140110 transcription regulator activity 3 GO:0060090 molecular adaptor activity 2
Localization
GO:0005634 nucleus 3
Pathway
R-HSA-4839726 Chromatin organization 2 R-HSA-74160 Gene expression (Transcription) 2 R-HSA-1266738 Developmental Biology 1
Partners
ARNTHDAC1SIN3ASIN3BUSP17
Complex memberships
Rpd3L (Sin3L) histone deacetylase complexSin3/HDAC corepressor complex

Evidence

Reading pass · 11 per-paper findings extracted from the source corpus
Year Finding Method Journal Conf PMIDs
1996 Genetic epistasis experiments in S. cerevisiae suggested SDS3 functions in a pathway related to, but potentially separable from, SIN3 and RPD3 in transcriptional silencing at HMR; sds3 mutations increase silencing at HML, HMR, and telomere-linked genes, similar to sin3 and rpd3 mutants, and SDS3 represses IME2 in haploid cells and is required for sporulation. Genetic screen for suppressors of defective silencing, epistasis analysis, reporter assays Genetics Medium 8978024
2000 Yeast Sds3p is an integral subunit of the high-molecular-weight Rpd3p·Sin3p histone deacetylase complex; in the absence of Sds3p, Sin3p and Rpd3p can be chromatographically separated, and the remaining Rpd3p complex has little or no HDAC activity, demonstrating that Sds3p is required for both complex integrity and catalytic activity. Biochemical fractionation (chromatography), co-immunoprecipitation, in vitro HDAC activity assay in sds3Δ yeast strain The Journal of biological chemistry High 11024051
2000 Genetic analysis in S. cerevisiae demonstrates that SDS3 functions in the same genetic pathway as SIN3 and RPD3, and co-immunoprecipitation confirms that Sds3 is physically present in the Sin3 complex. Genetic epistasis analysis, co-immunoprecipitation Genetics Medium 10655212
2002 Mammalian Sds3 (mSds3) was identified as an integral component of the mSin3A/mSin3B-HDAC corepressor complex: it physically associates with mSin3 proteins in vivo, represses transcription in a partially HDAC-dependent manner, and is required to enable HDAC1 catalytic activity in vivo. Co-immunoprecipitation (in vivo association with mSin3), transcriptional repression assays, HDAC activity assays Molecular and cellular biology High 11909966
2011 Human SDS3 undergoes endogenous Lys-63-linked (but not Lys-48-linked) polyubiquitination; the deubiquitinase USP17 physically interacts with SDS3 (shown by MALDI-TOF-MS, co-immunoprecipitation, and GST pull-down) and specifically removes Lys-63-linked ubiquitin chains from SDS3, which negatively regulates SDS3-associated HDAC activity. Co-immunoprecipitation, GST pull-down, MALDI-TOF-MS, ubiquitination linkage-specific assays, HDAC activity assay The Journal of biological chemistry High 21239494
2012 SDS3 contains hyaluronan binding motifs (HABMs) and directly binds hyaluronan (HA); deletion of HABMs in USP17 reduces its interaction with SDS3 but does not alter USP17's deubiquitinating activity toward SDS3 or USP17's functional regulation of SDS3-associated HDAC activity. CPC (cetylpyridinium chloride) binding assay, co-immunoprecipitation with HABM-deletion mutants, HDAC activity assay, soft agar/apoptosis/migration assays PloS one Medium 22662218
2012 Knockdown of Suds3 in mouse blastocysts disrupts FGF4/ERK signaling, impairs trophectoderm proliferation, and abolishes primitive endoderm formation, establishing that Suds3/Sin3/HDAC complexes are required for early lineage specification; exogenous FGF4 rescues these defects. Suds3 knockdown in mouse preimplantation embryos, immunofluorescence for lineage markers, FGF4 rescue experiment, HDAC1 knockdown comparison Developmental biology Medium 23123966
2012 SDS3 associates with ARNT (in a TCDD ligand-specific, but not B(a)P-specific, manner) as part of the Sin3/HDAC repressor complex, and reduction of SDS3 protein de-represses cKrox and S100A4 expression in CD4+CD8+ DPK thymocytes, placing SDS3 in AhR/ARNT ligand-specific transcriptional repression. Co-immunoprecipitation with anti-ARNT antibody, SDS3 protein knockdown, gene expression analysis Environmental toxicology and pharmacology Low 22981438
2015 Solution NMR revealed that the Sds3 Sin3 interaction domain (SID) samples two discrete conformations with lifetimes in the tens of milliseconds range, differing by a 5–7 Å translation of the main chain; Sds3 engages Sin3A via a bipartite motif within the SID comprising a helix and an extended segment, and Sds3 provides a homodimerization activity required for assembly of the 1–2 MDa Sin3L/Rpd3L complex. Solution NMR spectroscopy with functional validation of conformational exchange Journal of molecular biology Medium 26522936
2024 SDS3 modulates expression of ASK1, the upstream kinase of the p38 MAPK pathway, in microglia, thereby regulating p38 MAPK signaling activation and microglial inflammatory responses; SDS3 target genes were identified by chromatin immunoprecipitation combined with transcriptomics and proteomics. Chromatin immunoprecipitation (ChIP), SDS3 knockdown, transcriptomics, proteomics, downstream pathway validation Inflammation research Medium 39008037
2008 SUDS3 over-expression in BRMS1-non-expressing metastatic breast cancer cells did not suppress metastasis, motility, osteopontin secretion, or EGF receptor expression, demonstrating that SUDS3 and BRMS1 have functionally distinct roles within SIN3-HDAC complexes despite structural relatedness. SUDS3 over-expression in metastatic cell lines, motility assays, soft agar assay, EGF receptor expression analysis Cancer letters Medium 19070953

Source papers

Stage 0 corpus · 12 papers · ranked by NIH iCite citations
Year Title Journal Citations PMID
2002 Identification of mammalian Sds3 as an integral component of the Sin3/histone deacetylase corepressor complex. Molecular and cellular biology 100 11909966
2000 Sds3 (suppressor of defective silencing 3) is an integral component of the yeast Sin3[middle dot]Rpd3 histone deacetylase complex and is required for histone deacetylase activity. The Journal of biological chemistry 84 11024051
1996 Evidence that the transcriptional regulators SIN3 and RPD3, and a novel gene (SDS3) with similar functions, are involved in transcriptional silencing in S. cerevisiae. Genetics 66 8978024
2000 Roles for the Saccharomyces cerevisiae SDS3, CBK1 and HYM1 genes in transcriptional repression by SIN3. Genetics 40 10655212
2011 Lys-63-specific deubiquitination of SDS3 by USP17 regulates HDAC activity. The Journal of biological chemistry 35 21239494
2020 Long non-coding RNA SNHG22 facilitates the malignant phenotypes in triple-negative breast cancer via sponging miR-324-3p and upregulating SUDS3. Cancer cell international 28 32565736
2012 Hyaluronan binding motifs of USP17 and SDS3 exhibit anti-tumor activity. PloS one 20 22662218
2012 Depletion of Suds3 reveals an essential role in early lineage specification. Developmental biology 19 23123966
2008 Over-expression of the BRMS1 family member SUDS3 does not suppress metastasis of human cancer cells. Cancer letters 19 19070953
2024 SDS3 regulates microglial inflammation by modulating the expression of the upstream kinase ASK1 in the p38 MAPK signaling pathway. Inflammation research : official journal of the European Histamine Research Society ... [et al.] 5 39008037
2015 Solution NMR Studies of an Alternative Mode of Sin3 Engagement by the Sds3 Subunit in the Histone Deacetylase-Associated Sin3L/Rpd3L Corepressor Complex. Journal of molecular biology 4 26522936
2012 SDS3 interacts with ARNT in an AhR ligand-specific manner regulating expression of cKrox and S100A4 in CD4+CD8+ DPK thymocytes differentiation. Environmental toxicology and pharmacology 2 22981438

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