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Showing KAT7MYST2 is a alias.

KAT7

Histone acetyltransferase KAT7 · UniProt O95251

Length
611 aa
Mass
70.6 kDa
Annotated
2026-06-10
100 papers in source corpus 61 papers cited in narrative 61 extracted findings
Cross-family judge vs UniProt: Affinage preferred faithfulness: 8/8 claims corpus-supported (100%)

Mechanistic narrative

Synthesis pass · prose summary of the discoveries below

KAT7 (HBO1/MYST2) is a MYST-family lysine acetyltransferase that operates as the catalytic engine of multisubunit chromatin-modifying complexes and is the major cellular source of histone H3K14 acetylation in vivo (PMID:21149574, PMID:31767635). Its substrate specificity and chromatin targeting are dictated by mutually exclusive scaffold subunits: JADE1/2/3 directs acetylation toward histone H4 (K5/K12), while BRPF1/2/3 directs activity toward H3K14, with ING4/5 and the PHD/PZP modules of these partners reading the H3 tail to govern recruitment and substrate choice (PMID:18684714, PMID:19187766, PMID:21753189, PMID:26677226, PMID:38448574). Structural and kinetic studies show JADE1 presents the H3-H4 substrate to the MYST domain to boost catalytic efficiency, and a defined BRPF2-MYST interface potentiates H3K14 activity (PMID:28334966, PMID:29382722). Beyond acetylation, the same enzyme is a versatile acyltransferase that installs propionyl, butyryl, crotonyl, benzoyl, acetoacetyl, and lactyl marks in a scaffold-dependent manner, with H3K14 acylation and H3K9 lactylation at transcription start sites required for gene transcription (PMID:34259319, PMID:36388951, PMID:38670996, PMID:37382194). Functionally, KAT7-dependent H3K14ac is a prerequisite for de novo activation of repressed genes rather than maintenance of ongoing transcription, underlies neural and embryonic stem cell plasticity, hematopoietic stem cell quiescence and self-renewal, AIRE-dependent peripheral tolerance gene expression in thymic epithelium, and centromere integrity through antagonism of Suv39h1-mediated H3K9me3 to license CENP-A assembly (PMID:27270040, PMID:34724565, PMID:35061506, PMID:36641753, PMID:38421638). In its earliest-characterized role KAT7 acts as a coactivator of the licensing factor Cdt1, acetylating histone H4 at origins to drive chromatin decondensation and MCM2-7 loading, a function gated by p53, Geminin, and cell-cycle kinases (PMID:16428461, PMID:18832067, PMID:20129055). KAT7 stability and activity are tightly controlled by phosphorylation (Cdk1/Plk1, CDK2, PKD1, JNK, ATM/ATR), competing acyl modifications, deacetylation by SIRT1, and ubiquitin ligases (CRL4DDB2, Fbxw15, HUWE1) opposed by deubiquitinase USP25 and the stabilizing partner BRPF3 (PMID:18250300, PMID:21856198, PMID:26572825, PMID:30745998, PMID:33014433, PMID:36322781, PMID:32555450). KAT7 also acetylates non-histone substrates including calnexin K525cr (mTORC1 signaling), LDHA K118 (the Warburg effect), vimentin K104 (EMT), and RFX1, and is co-opted by oncogenic MLL-fusion and NUP98-fusion proteins to sustain leukemia stem cell transcriptional programs, making it a therapeutic target in AML (PMID:31827282, PMID:32764680, PMID:34431785, PMID:35266843, PMID:37424170, PMID:40536430, PMID:38593918).

Mechanistic history

Synthesis pass · year-by-year structured walk · 13 steps
  1. 1999 High

    Established KAT7 as a chromatin-associated acetyltransferase physically tied to the replication machinery, framing it as a candidate link between histone modification and origin function.

    Evidence Yeast two-hybrid, co-IP, and in vitro HAT assay identifying HBO1 as an ORC1-interacting protein with H3/H4 acetyltransferase activity

    PMID:10438470

    Open questions at the time
    • Did not show whether HAT activity is required at origins
    • Complex composition and scaffold subunits unknown
  2. 2001 High

    Defined a direct, domain-specific physical bridge between KAT7 and the MCM helicase, anchoring it mechanistically to pre-replication complex components.

    Evidence Yeast two-hybrid, in vitro binding, suppressor mutagenesis mapping MCM2 binding to the HBO1 C2HC zinc finger

    PMID:11278932

    Open questions at the time
    • Functional consequence of MCM2 binding for replication not yet tested
    • Did not implicate acetylation activity
  3. 2006 High

    Placed KAT7 functionally upstream of MCM loading, showing it is required for pre-RC assembly downstream of ORC/Cdc6.

    Evidence siRNA in human cells and immunodepletion of Xenopus egg extracts with recombinant Cdt1 rescue and chromatin fractionation

    PMID:16428461

    Open questions at the time
    • Did not establish whether enzymatic activity versus scaffolding drives MCM loading
    • Histone substrate at origins not defined
  4. 2008 High

    Identified KAT7 as a Cdt1 coactivator and revealed cell-cycle kinase control of its replication function, integrating it into G1/S licensing regulation.

    Evidence Co-IP, ChIP, rereplication assays for Cdt1 interaction; in vitro/in vivo kinase assays and phospho-mutants for Cdk1-primed Plk1 phosphorylation at Ser57

    PMID:18250300 PMID:18832067

    Open questions at the time
    • How phosphorylation alters complex composition not resolved
    • Direct origin acetyl substrate still inferred
  5. 2010 High

    Demonstrated that KAT7 catalytic activity, not just binding, is essential for replication licensing via H4 acetylation-driven chromatin decondensation, and is restrained by Geminin and p53.

    Evidence HAT-defective mutants, ChIP, MCM loading assays, Geminin co-IP, live-cell decondensation imaging, and p53-dependent HAT inhibition assays

    PMID:17954561 PMID:20129055 PMID:20980834

    Open questions at the time
    • Quantitative contribution of H4 acetylation versus other marks at origins unclear
    • Crosstalk between p53 and Geminin regulation not integrated
  6. 2011 High

    Resolved the scaffold logic dividing KAT7 activity into JADE-directed H4 acetylation and BRPF-directed H3K14 acetylation, and assigned KAT7 as the principal in vivo source of H3K14ac.

    Evidence JADE1 PHD reconstitution HAT assays, Brd1/BRPF2 KO mouse with genome-wide ChIP, and a conditional Hbo1 KO mouse profiling multiple histone marks

    PMID:18684714 PMID:19187766 PMID:19393168 PMID:21149574 PMID:21753189

    Open questions at the time
    • Structural basis of scaffold-imposed specificity not yet solved at this stage
    • Why H3K14ac loss arrests development mechanistically undefined
  7. 2015 High

    Distinguished a licensing-independent role for the HBO1-BRPF3 complex in origin firing and uncovered DNA-damage-triggered destruction of KAT7, linking it to genome surveillance.

    Evidence RNAi screen, ChIP-seq, and CDC45-versus-MCM assays for BRPF3; ATM/ATR phospho-site mapping (Ser50/53) with CRL4DDB2 reconstitution for damage-induced degradation

    PMID:26572825 PMID:26620551 PMID:26677226

    Open questions at the time
    • How a single enzyme partitions between licensing and firing roles unresolved
    • In vivo relevance of damage-induced degradation to repair outcomes incomplete
  8. 2017 High

    Provided structural definition of the BRPF2-MYST interface and JADE1-mediated substrate presentation, and positioned KAT7 in nucleotide excision repair chromatin remodeling.

    Evidence Crystal structure of MYST-BRPF2 with HAT assays and mutagenesis; kinetic reconstitution of JADE1-stimulated catalysis; UV-damage localization and XP-cell epistasis for NER

    PMID:28334966 PMID:28719581 PMID:29382722

    Open questions at the time
    • Full holocomplex structure not determined
    • Relative importance of NER role versus replication role in vivo unclear
  9. 2016 High

    Established KAT7's role in centromere maintenance by enabling CENP-A assembly through antagonism of Suv39h1 heterochromatin, broadening its function beyond replication and transcription.

    Evidence Co-IP with M18BP1, CRISPR KO with CENP-A/H3K9me3 immunofluorescence, and ectopic tethering at alphoid DNA

    PMID:27270040

    Open questions at the time
    • Whether centromeric function requires a specific scaffold complex not defined
    • Direct acetyl substrate at centromeres not pinpointed
  10. 2020 High

    Decoupled KAT7's histone substrates in human cells, showing it is essential for all H3K14ac but dispensable for replication, overturning the obligatory licensing role and refocusing on transcriptional output.

    Evidence CRISPR KO in multiple human cell lines with comprehensive histone-mark westerns and transcriptomics, plus complex-assembly studies of MEAF6 and HUWE1/BRPF3-controlled stability

    PMID:31767635 PMID:32555450 PMID:32918898

    Open questions at the time
    • Reconciliation with earlier Xenopus/human replication-licensing data not fully explained
    • Cell-type dependence of replication role unresolved
  11. 2022 High

    Defined KAT7 as a stem-cell and tolerance regulator that activates gene programs through genome-wide H3K14ac, and expanded its catalytic repertoire to non-acetyl acylations and non-histone substrates.

    Evidence Conditional KO with transplantation and ChIP-seq in HSCs; TEC-specific KO with ATAC-seq for AIRE-dependent genes; in vitro acylation and proteomics for crotonyl/benzoyl marks; CANX K525cr mTORC1 system

    PMID:34724565 PMID:35061506 PMID:35266843 PMID:36322781 PMID:36388951 PMID:38670996

    Open questions at the time
    • How a single enzyme selects among diverse acyl-CoA cosubstrates in vivo unclear
    • Physiological abundance of rarer acylations uncertain
  12. 2023 High

    Crystallized the principle that KAT7/H3K14ac licenses de novo gene activation rather than maintenance, and connected the complex to pluripotency and signaling pathways.

    Evidence Conditional KO with ChIP-seq and rescue in neural stem cells; HBO1-SMAD4 co-IP/ChIP-seq in hESCs with differentiation assays; lactyl/acetoacetyl transferase characterization

    PMID:36641753 PMID:37382194 PMID:38421638 PMID:38670996

    Open questions at the time
    • Mechanism distinguishing activatable from maintained genes not fully defined
    • Whether acylation marks (lactyl) drive distinct gene programs unclear
  13. 2025 High

    Consolidated KAT7 as a therapeutic target in fusion-driven leukemias, showing oncogenic MLL- and NUP98-fusions co-opt the KAT7 complex and its acetyl marks to sustain leukemia stem cell programs.

    Evidence CRISPR screens, ChIP-seq for histone marks and fusion proteins, co-IP via BRPF1, small-molecule HBO1 inhibitors, and xenograft/menin-inhibitor combination studies

    PMID:31827282 PMID:32764680 PMID:34431785 PMID:40536430

    Open questions at the time
    • Therapeutic window between leukemic dependence and normal HSC requirement not defined
    • Relative contribution of H3K14ac, H4K12ac, and H3K23ac to fusion recruitment varies between studies

Open questions

Synthesis pass · forward-looking unresolved questions
  • How KAT7 integrates its many regulatory inputs (competing acylations at K432, phosphorylation, deacetylation, scaffold choice) to select among histone and non-histone substrates in a given cellular context remains unresolved.
  • No unified model linking PTM state to substrate/scaffold selection
  • Quantitative hierarchy of competing acyl-CoA cosubstrates in vivo unknown
  • Structure of full holocomplex on nucleosome not determined

Mechanism profile

Synthesis pass · controlled-vocabulary classification · explore literature graph →
Molecular activity
GO:0016740 transferase activity 11 GO:0140096 catalytic activity, acting on a protein 5 GO:0140110 transcription regulator activity 4 GO:0042393 histone binding 3 GO:0016874 ligase activity 2
Localization
GO:0000228 nuclear chromosome 2 GO:0005634 nucleus 2 GO:0005829 cytosol 2 GO:0005730 nucleolus 1
Pathway
R-HSA-4839726 Chromatin organization 5 R-HSA-1643685 Disease 4 R-HSA-69306 DNA Replication 4 R-HSA-74160 Gene expression (Transcription) 4 R-HSA-1640170 Cell Cycle 3 R-HSA-73894 DNA Repair 2
Partners
BRPF2BRPF3CDT1ING4JADE1MCM2MEAF6ORC1
Complex memberships
HBO1-BRPF complexHBO1-JADE complexORC/pre-replication complex (associated)

Evidence

Reading pass · 61 per-paper findings extracted from the source corpus
Year Finding Method Journal Conf PMIDs
1999 HBO1 (KAT7) was identified as a novel protein that physically interacts with the human ORC1 subunit of the origin recognition complex. HBO1 exists as part of a multisubunit complex with histone H3 and H4 acetyltransferase activities, and a fraction associates with ORC1 in human cell extracts. Yeast two-hybrid screen, co-immunoprecipitation from human cell extracts, in vitro HAT assay The Journal of biological chemistry High 10438470
2001 HBO1 directly interacts with MCM2 via its C2HC zinc finger domain. An N-terminal domain of MCM2 is necessary for binding HBO1, and the C2HC zinc finger of HBO1 is essential for MCM2 binding. A suppressor screen in yeast confirmed the interaction is direct and mediated by the zinc finger. Yeast two-hybrid, in vitro binding assays, in vivo co-immunoprecipitation, reverse two-hybrid selection, suppressor mutagenesis The Journal of biological chemistry High 11278932
2000 HBO1 interacts with the androgen receptor (AR) in a ligand-enhanced manner and acts as a transcriptional repressor of AR-mediated transcription. A transcriptional repression domain was mapped to the N-terminal region of HBO1. HBO1 is localized to the nucleus. Yeast two-hybrid, in vitro and in vivo co-immunoprecipitation, immunofluorescence, transient transfection reporter assays, GAL4-DBD mapping The Journal of biological chemistry Medium 10930412
2006 Hbo1 is a positive regulatory factor for pre-replication complex (pre-RC) assembly. Depletion of Hbo1 in human cells caused failure of Mcm2-7 to associate with chromatin even though ORC and Cdc6 loading was normal. Immunodepletion of Xenopus Hbo1 from egg extracts abolished MCM loading and DNA replication, which could be rescued by addition of recombinant Cdt1. siRNA knockdown in human cells, immunodepletion of Xenopus egg extracts, chromatin fractionation, recombinant protein rescue Molecular and cellular biology High 16428461
2008 HBO1 is a coactivator of the replication licensing factor Cdt1. HBO1 associates with replication origins during G1 phase in a Cdt1-dependent manner, directly interacts with Cdt1, and enhances Cdt1-dependent rereplication. This association is independent of the Cdt1 repressor Geminin. Co-immunoprecipitation, chromatin immunoprecipitation (ChIP), rereplication assay, cell-cycle fractionation Genes & development High 18832067
2008 Plk1 phosphorylates Hbo1 on Ser-57 in vitro and in vivo during mitosis. Cdk1 first phosphorylates Hbo1 on Thr-85/88, creating a docking site for Plk1 recruitment. The Plk1 phosphorylation-defective mutant (S57A) causes G1/S arrest, inhibits MCM chromatin loading, and reduces DNA replication. Yeast two-hybrid, in vitro kinase assay, phospho-specific antibodies, cell-cycle analysis, chromatin fractionation, overexpression of phospho-mutants Proceedings of the National Academy of Sciences of the United States of America High 18250300
2008 Jade-1/1L is a crucial co-factor that positively regulates HBO1-mediated histone H4 acetylation. PHD fingers of Jade-1/1L are required for nucleosomal H4 acetylation but not for mutual binding. Co-expression of Jade-1/1L and HBO1 synergistically increases H4 acetylation in vivo and in vitro using reconstituted oligonucleosome substrates. Co-immunoprecipitation, in vitro HAT assay with oligonucleosome substrates, siRNA depletion, PHD finger deletion mutants, cell-based H4 acetylation assay The Journal of biological chemistry High 18684714
2009 HBO1 HAT complexes contain PHD finger domains in ING4/5 and JADE1/2/3 subunits that interact with the histone H3 N-terminal tail with distinct specificities toward its methylation status. Their combinatorial action regulates chromatin binding and substrate specificity of HBO1 complexes. HBO1 complexes are enriched throughout gene coding regions, supporting a role in transcription elongation. Biochemical analyses (pulldown, co-IP), genome-wide ChIP analysis, mutant analysis of PHD domains, cell growth assay Molecular cell High 19187766
2009 Recombinant Hbo1 acetylates nucleosomal histone H4 in vitro, with a preference for lysines 5 and 12. Hbo1 protein is approximately equimolar with active replication origins in normal human fibroblasts. In vitro HAT assay with nucleosomal substrates, semi-quantitative western blot Gene Medium 19393168
2007 p53 physically interacts with Hbo1 and negatively regulates its HAT activity in vitro and in cells. Physiological stresses that stabilize p53 (hyperosmotic shock and DNA replication fork arrest) inhibit Hbo1 HAT activity in a p53-dependent manner. Hyperosmotic stress during G1 specifically inhibits MCM2-7 chromatin loading. Co-immunoprecipitation, in vitro HAT assay, siRNA knockdown, chromatin fractionation under stress conditions Molecular and cellular biology High 17954561
2010 HBO1 HAT activity is essential for DNA replication licensing. A HAT-defective mutant of HBO1 bound at origins cannot load the MCM complex. H4 acetylation at origins is cell-cycle regulated (maximal at G1/S). Geminin inhibits HBO1 acetyltransferase activity in the context of a Cdt1-HBO1 complex and inhibits H4 acetylation and MCM loading in vivo. HAT-defective mutant analysis, ChIP, MCM loading assay, cell-cycle synchronization, Geminin overexpression and co-IP Molecular cell High 20129055
2010 Cdt1-induced large-scale chromatin decondensation required for MCM recruitment requires HBO1 HAT activity and histone H4 modifications. HDAC11 inhibits Cdt1-induced chromatin unfolding and MCM loading. This process is regulated positively by Cdt1 and HBO1 in G1 and repressed by Geminin-HDAC11 in S phase. Live-cell chromatin decondensation imaging, HAT-defective mutant, HDAC11 co-immunoprecipitation, MCM loading assay, cell-cycle analysis Cell cycle (Georgetown, Tex.) Medium 20980834
2010 HBO1 is the major source of histone H3K14 acetylation in vivo during embryonic development. Loss of HBO1 caused >90% reduction in H3K14ac with no significant reduction at other histone residues, developmental arrest at the 10-somite stage, and decreased expression of developmental genes. No defects in DNA replication or cell proliferation were observed in primary fibroblasts from mutant embryos. Conditional knockout mouse model, quantitative western blot for multiple histone marks, gene expression analysis, cell proliferation assays Molecular and cellular biology High 21149574
2011 The Hbo1-Brd1/BRPF2 complex is responsible for global acetylation of H3K14. BRD1 bridges HBO1 and its activator ING4. Depletion of Hbo1 similarly reduces H3K14 acetylation in erythroblasts, and the complex is required for fetal liver erythropoiesis and expression of key erythroid regulator genes including Gata1. Brd1-knockout mouse, biochemical co-immunoprecipitation, genome-wide ChIP mapping, western blot for H3K14ac, forced expression rescue Blood High 21753189
2011 JNK phosphorylates Cdt1 on threonine 29 in response to nongenotoxic stress, leading to rapid dissociation of HBO1 from replication origins and blocking DNA replication initiation. Simultaneously, JNK phosphorylates Jun (AP-1), increasing HBO1 recruitment to stress-response genes. This reciprocal regulation coordinates replication and transcription responses to stress. In vitro kinase assay, phospho-specific antibodies, ChIP, mutation of Thr29, DNA replication assay, cell-cycle analysis Molecular cell High 21856198
2011 ING4/5 PHD domain association with HBO1-JADE determines the growth inhibitory function of the complex, linked to tumor suppressor activity. HBO1/ING complexes are a major source of H3 and H4 acetylation in vivo. The p53/p21 pathway is a main transcriptional target regulated directly at the p21/CDKN1A initiation site. Molecular dissection of protein domains, co-immunoprecipitation, ChIP, PHD mutant analysis, cell growth assays Molecular and cellular biology Medium 22144582
2012 Plk1 phosphorylation of Hbo1 transcriptionally increases cFos expression and consequently elevates MDR1, conferring gemcitabine resistance in pancreatic cancer. Cells expressing Plk1-unphosphorylatable Hbo1 mutants are more sensitive to gemcitabine. Phospho-mutant overexpression, gene expression analysis, drug sensitivity assays, xenograft mouse model Molecular cancer therapeutics Medium 23188630
2013 Hbo1 is a cyclin E/CDK2 substrate; CDK2 phosphorylates Hbo1 at T88. The low-molecular weight cyclin E (LMW-E)/CDK2 complex phosphorylates Hbo1 at T88 without affecting its HAT activity. Wild-type Hbo1 coexpressed with LMW-E/CDK2 promotes cancer stem-like cell enrichment, whereas the T88A mutant reverses this phenotype. Protein microarray, in vitro kinase assay, phospho-mutant analysis, cancer stem cell (CD44hi/CD24lo) flow cytometry, mammosphere formation assay Cancer research Medium 23955388
2013 Fbxw15 directly interacts with HBO1 and mediates its ubiquitination at Lys338 and proteasomal degradation in the cytoplasm. Mek1 triggers HBO1 phosphorylation and degradation, and this process requires Fbxw15. Fbxw15-mediated HBO1 depletion reduces H3K14 acetylation and cellular proliferation. Co-immunoprecipitation, ubiquitination assay, mass spectrometry (Lys338 site), siRNA knockdown, cell proliferation assay The Journal of biological chemistry Medium 23319590
2013 Hbo1 promotes proteasome-dependent degradation of estrogen receptor α (ERα) through lysine 48-linked ubiquitination. The acetyltransferase activity of Hbo1 is linked to its ERα ubiquitination activity. Hbo1 depletion increases ERα expression. siRNA knockdown, ubiquitination assay, western blot, K48-linked ubiquitin chain analysis Cancer science Medium 24125069
2015 UV damage triggers ATM/ATR-dependent phosphorylation of HBO1 on Ser50 and Ser53, which causes preferential interaction with DDB2 and subsequent ubiquitylation by CRL4DDB2, leading to HBO1 degradation and suppression of cell proliferation. Ser50/53Ala mutants maintain H3K14ac and impair cell-cycle regulation in response to UV. Phospho-specific antibodies, co-immunoprecipitation, ubiquitination assay, CRL4DDB2 reconstitution, phospho-mutant analysis, UV survival assay Molecular and cellular biology High 26572825
2015 BRPF3 specifically forms a tetrameric complex with HBO1 (not with related acetyltransferases MOZ, MORF, TIP60, or MOF) and this complex specifically acetylates histone H3K14. Affinity purification, co-immunoprecipitation, western blot for histone marks, LacZ reporter mouse The Journal of biological chemistry Medium 26677226
2015 BRPF3 forms a complex with HBO1 that specifically acetylates histone H3K14. BRPF3 and HBO1 are enriched at ORC1-binding sites and replication origins near TSSs. BRPF3 is required for H3K14ac at selected origins and for efficient CDC45 recruitment (origin activation), but not for MCM2-7 loading, defining a distinct licensing-independent role in origin firing. RNAi screen for replication regulators, co-immunoprecipitation, genome-wide ChIP-seq, origin firing assay (CDC45 vs MCM loading by ChIP) The EMBO journal High 26620551
2016 KAT7 interacts with the CENP-A assembly factor M18BP1. KAT7 knockout in HeLa cells reduces centromeric CENP-A assembly and increases mitotic chromosome misalignment and micronuclei formation. Tethering KAT7 to an ectopic alphoid DNA site removes H3K9me3 and stimulates CENP-A or H3.3 assembly, antagonizing Suv39h1-mediated heterochromatin invasion. Co-immunoprecipitation, CRISPR knockout, immunofluorescence for CENP-A and H3K9me3, tethering assay at ectopic alphoid DNA locus Developmental cell High 27270040
2016 KAT7 interacts with the N-terminal domain (NTD) of progesterone receptor (PR) in a ligand-dependent manner via its MYST domain and induces SRC-1-dependent coactivation of PR-mediated transcription. HBO1 also interacts with SRC-1a. In HEK293 cells, HBO1 selectively enhances PRB but not PRA transcriptional activity. Yeast two-hybrid, GST pull-down, co-immunoprecipitation, transient transfection reporter assays, immunofluorescence, RT-PCR of endogenous target genes Molecular endocrinology (Baltimore, Md.) Medium 16645042
2017 The crystal structure of the HBO1 MYST domain in complex with the N-terminal region of BRPF2 reveals key residues for the HBO1-BRPF2 interaction. The N-terminal region of BRPF2 is sufficient to bind HBO1 and potentiate its HAT activity toward H3K14 (free H3, H4, and nucleosomal H3). Crystal structure determination, in vitro HAT assay, mutagenesis of key interface residues, cell biological validation Nucleic acids research High 28334966
2017 Phosphorylated HBO1 at CPD (cyclobutane pyrimidine dimer) sites mediates histone acetylation to facilitate XPC recruitment at UV-damaged DNA sites. HBO1 also facilitates accumulation of SNF2H-ACF1 chromatin remodeling complex at CPD sites. HBO1 depletion inhibits CPD repair and sensitizes cells to UV. siRNA knockdown, immunofluorescence at UV-damage sites, co-immunoprecipitation with DDB2, epistasis in XP patient-derived cells, UV survival assay Nature communications High 28719581
2017 Hbo1 has intrinsic ubiquitin E3 ligase activity toward ERα. Estradiol-17β inhibits this E3 ligase activity in vitro, while hyperactive ERα mutants from metastatic breast cancers are better substrates for Hbo1-mediated ubiquitination. In vitro ubiquitination assay, Hbo1 knockdown, western blot Proceedings of the Japan Academy. Series B, Physical and biological sciences Medium 28769019
2018 JADE1 physically links the catalytic HBO1 subunit with its histone H3-H4 substrate. JADE1 increases catalytic efficiency of HBO1 acetylation of H3-H4 substrate ~5-fold through an N-terminal 21-residue HBO1- and histone-binding domain. HBO1 also contains an N-terminal histone-binding domain (HBD) that makes additional H3-H4 contacts but does not significantly contribute to overall HAT activity. In vitro reconstitution with recombinant proteins, kinetic enzyme assays, JADE1 deletion mapping, in vivo validation by deletion mutants The Journal of biological chemistry High 29382722
2018 KAT7 mediates H3K14 and H4 acetylation in intragenic regions of EC-enriched genes including VEGFR-2, contributing to RNA polymerase II binding and VEGFR-2 transcription. KAT7 depletion reduces VEGFR-2 expression and disrupts angiogenic potential. KAT7 inhibition in zebrafish disrupts vessel formation, which is rescued by human KAT7. siRNA knockdown, ChIP with tiling array, microarray, KAT7 inhibition in zebrafish embryos, rescue with human KAT7 The Journal of biological chemistry Medium 29414790
2018 LPS elevates HBO1 protein stability by upregulating the deubiquitinase USP25, which associates with HBO1 and suppresses its ubiquitination. Stabilized HBO1 then modulates inflammatory gene transcription in THP-1 monocytes. Co-immunoprecipitation, ubiquitination assay, siRNA knockdown of USP25, western blot, LPS treatment Biochimica et biophysica acta. Gene regulatory mechanisms Medium 30745998
2019 The histone acetyltransferase domain of HBO1 is essential for H3K14 acetylation in AML LSCs. H3K14ac facilitates RNA polymerase II processivity to maintain high expression of HOXA9/HOXA10. A competitive acetyl-CoA analogue inhibitor (WM-3835) inhibits HBO1, recapitulating genetic loss-of-function in AML. CRISPR domain screen, quantitative mass spectrometry, H3K14ac ChIP-seq, RNA pol II ChIP-seq, shRNA screen in LSC model, small-molecule inhibitor characterization (competitive kinetics with acetyl-CoA) Nature High 31827282
2019 LYAR recruits KAT7 to rDNA loci via BRD2 and BRD4 interactions, resulting in enhanced local acetylation of histone H4 at rDNA, thereby promoting rRNA synthesis. BRD2 is required for KAT7 recruitment; LYAR also binds a BRD4-KAT7 complex that independently promotes H4 and H3 acetylation at rDNA. Co-immunoprecipitation, ChIP-qPCR, siRNA knockdown, rRNA synthesis measurement Nucleic acids research Medium 31504794
2019 UHRF1 interacts with methylated H3K14 and thereby suppresses H3K14 acetylation by KAT7, leading to transcriptional repression of the tumor suppressor TUSC3 in colon cancer cells. Co-immunoprecipitation, ChIP, siRNA knockdown, western blot for H3K14ac Oncogene Medium 31582837
2019 Myst2/Kat7 interacts with the tumour suppressor protein Niam (Nuclear Interactor of ARF and Mdm2) in mouse embryonic stem cells, as identified by affinity purification-mass spectrometry. Myst2 forms both H3 and H4 histone acetylation complexes in ESCs similar to those in somatic cells. Affinity purification coupled to mass spectrometry (AP-MS) in mouse ESCs Scientific reports Medium 28811661
2020 KAT7 knockout in HeLa and 293T human cells demonstrates that HBO1 is essential for all H3K14ac but is dispensable for H4 acetylation and DNA replication in human cells. Loss of HBO1 and H3K14ac secondarily causes near-complete loss of H4 acetylation after 4 weeks. HBO1 loss principally affects cell adhesion genes. CRISPR/Cas9 knockout, siRNA knockdown in multiple human cell lines, western blot for multiple histone marks, cell proliferation assay, transcriptomic analysis Molecular and cellular biology High 31767635
2020 KAT7 loss in AML cells driven by MLL-X fusions leads to rapid and complete loss of both H3K14ac and H4K12ac, reduced proliferation, apoptosis, and differentiation. Loss of these marks causes BRD4 and AF4 to dissociate from MLL-fusion target gene promoters (MEIS1, PBX3, SENP6), implicating acetylated histones as a platform for MLL-fusion adaptor recruitment. Genome-wide CRISPR screen, CRISPR KO, ChIP-seq for histone marks and co-factors, gene expression analysis, differentiation assays Leukemia High 32764680
2020 Protein kinase D1 (PKD1) directly interacts with and phosphorylates KAT7 at Thr97 and Thr331. PKD1-mediated phosphorylation enhances KAT7 stability by reducing ubiquitination-mediated degradation. Phospho-defective mutant KAT7-T97/331A attenuates H4 acetylation, MCM2/6 chromatin loading, DNA replication, and cell proliferation. Co-immunoprecipitation, in vitro kinase assay, phospho-mutant analysis, ubiquitination assay, chromatin fractionation, BrdU incorporation Cell death discovery Medium 33014433
2021 HBO1 is a versatile histone acyltransferase that catalyzes not only histone acetylation but also propionylation, butyrylation, and crotonylation in vivo and in vitro, and does so in a JADE or BRPF scaffold protein-dependent manner. The minimal HBO1/BRPF2 complex accommodates acetyl-CoA, propionyl-CoA, butyryl-CoA, and crotonyl-CoA. HBO1 is the key enzyme for H3K14 acylations at transcription start sites. In vitro acylation assays with different acyl-CoA substrates, in vivo acylation by mass spectrometry, genome-wide ChIP for acylation marks, CBP vs HBO1 comparison with KO cells Nucleic acids research High 34259319
2021 Leukemic MLL fusion proteins associate with the HBO1 HAT complex through their trithorax homology domain 2 (THD2) via ING4/5 and PHF16 subunits. MLL-ELL particularly depends on this association for leukemic transformation. HBO1 complex promotes loading of the AF4/ENL/P-TEFb (AEP) complex onto target promoters over EAF1 and p53. The NUP98-HBO1 fusion exerts oncogenic properties via interaction with MLL, not its intrinsic HAT activity. Co-immunoprecipitation in multiple human cell lines, ChIP, leukemic transformation assay in murine hematopoietic progenitors, domain deletion and HAT-dead mutant analysis eLife High 34431785
2022 HBO1 is required for H3K14ac throughout the genome in hematopoietic stem cells (HSCs). Loss of HBO1 causes abnormally high recruitment of quiescent HSCs into the cell cycle, leading to HSC pool exhaustion. HBO1 promotes expression of a transcription factor network (Mpl, Tek, Gfi1b, Egr1, Tal1, Gata2, Erg, Pbx1, Meis1, Hox9) essential for HSC quiescence and self-renewal. Conditional KO (Mx1-Cre and Rosa26-CreERT2), competitive transplantation, cell-cycle analysis, H3K14ac ChIP-seq, gene expression analysis Blood High 34724565
2022 HBO1 catalyzes lysine benzoylation (Kbz) in mammalian cells, acting as a 'writer' of this modification. At least 77 HBO1-targeted Kbz sites were identified in the benzoylome, including at chromatin-related proteins. In vitro benzoylation assay, mass spectrometry-based benzoylome analysis in KO cells, western blot iScience Medium 36388951
2022 SIRT1 deacetylates KAT7, activating it. SIRT1 loss leads to hyperacetylation of KAT7 and reduced H4K12ac. Overexpression of a non-acetylatable KAT7 mutant partly rescues SIRT1 loss-induced proliferation defects in T-ALL, establishing a NOTCH1-SIRT1-KAT7 regulatory axis. Global acetyl proteomics upon SIRT1 loss, KAT7 non-acetylatable mutant rescue, H4K12ac measurement, gene expression profiling Blood cancer discovery Medium 36322781
2022 KAT7 mediates the K525 crotonylation of CANX (calnexin). Loss of KAT7 renders MTORC1 insensitive to leucine deprivation. KAT7-mediated CANX K525 crotonylation is required for lysosomal translocation of CANX and subsequent inhibition of Ragulator activity toward RRAG GTPases during leucine deprivation. Cell-free MTORC1 activation system, co-immunoprecipitation, site-specific crotonylation mutagenesis (K525), KAT7 KO, lysosomal fractionation Autophagy Medium 35266843
2022 KAT7 is required for optimal expansion of medullary thymic epithelial cells (mTECs) and for expression of AIRE-dependent peripheral tissue genes (PTGs), associated with enhanced chromatin accessibility at PTG loci. TEC-specific Kat7 deletion leads to organ-specific autoimmunity resembling Aire-deficient mice. Conditional TEC-specific KO, ATAC-seq for chromatin accessibility, gene expression analysis, histological assessment of autoimmunity Science immunology High 35061506
2023 HBO1 functions as a lysine lactyltransferase: it catalyzes the addition of lysine lactylation (Kla) in vitro and intracellularly. E508 is a key site for lactyltransferase activity. HBO1 preferentially catalyzes histone H3K9la. Scaffold proteins JADE1 and BRPF2 promote enzymatic activity for histone Kla. H3K9la at TSSs is required for gene transcription. In vitro lactyltransferase assay, E508 mutagenesis, quantitative proteomics of Kla sites in KO cells, site-specific antibodies, CUT&Tag for H3K9la at TSSs Nature communications High 38670996
2023 KAT7 is required for neural stem cell plasticity and de novo gene activation. KAT7 and H3K14ac are present at inactive genes, intergenic regions, and in heterochromatin — not only at transcribed genes. KAT7 is not required for continued transcription of already-active genes but is indispensable for activation of repressed genes. Loss of KAT7 abolishes neural stem cell differentiation pathways; re-expression restores developmental potential. Conditional KO, H3K14ac ChIP-seq, gene expression profiling, neural stem cell differentiation assays, KAT7 re-expression rescue Cell reports High 36641753
2023 Identification of histone lysine acetoacetylation (Kacac) as a novel post-translational modification. HBO1, traditionally an acetyltransferase, also serves as an acetoacetyltransferase, adding acetoacetyl groups to histones. 33 Kacac sites on mammalian histones were identified. HPLC co-elution, MS/MS analysis with synthetic peptides, western blot, isotopic labeling, in vitro acetoacetyltransferase assay Advanced science (Weinheim, Baden-Wurttemberg, Germany) Medium 37382194
2023 HBO1 interacts with SMAD4 and co-binds open chromatin marked by H3K14ac and H3K4me3 in undifferentiated hESCs to maintain pluripotency. Upon BMP4-induced differentiation, HBO1/SMAD4 co-occupy mesoderm gene loci. HBO1-null hESCs fail to respond to TGF-β signaling to maintain pluripotency and cannot form mesendoderm. Co-immunoprecipitation, ChIP-seq for HBO1 and SMAD4, conditional KO hESCs, differentiation assays (gastruloids, teratomas) Nucleic acids research High 38421638
2023 NLRP11 bridges KAT7 to vimentin, enabling KAT7 to directly acetylate vimentin at Lys104. NLRP11 also induces cytoplasmic localization of KAT7 to facilitate vimentin K104Ac. This acetylation promotes EMT and malignant behavior in lung adenocarcinoma. Co-immunoprecipitation, in vitro acetylation assay (KAT7 + vimentin substrate), site-specific K104Q/R mutations, subcellular fractionation, in vivo xenograft Advanced science (Weinheim, Baden-Wurttemberg, Germany) Medium 37424170
2023 KAT7 acetylates H3K14 to enhance MRAS transcription, activating the MAPK/ERK pathway in colorectal cancer. Re-expression of KAT7, but not an acetyltransferase-deficient mutant, rescues MRAS expression and ERK phosphorylation after KAT7 knockdown. shRNA knockdown, CRISPR KO, acetyltransferase-dead mutant rescue, RNA-seq, ChIP-qPCR for H3K14ac at MRAS promoter, ERK phosphorylation western blot Theranostics Medium 39816686
2024 The PZP (PHD1-zinc-knuckle-PHD2) domain of JADE engages the nucleosome through binding to histone H3 and DNA, directing the HBO1 complex to chromatin targets. Recognition of unmethylated H3K4 by PZP directs enzymatic activity toward histone H4 acetylation, whereas H3K4 hypermethylation alters histone substrate selectivity. These structural findings were linked to leukemogenesis via the NUP98-JADE2 fusion. Structural analysis of PZP domain, genomic binding studies (ChIP-seq), complex assembly in vivo, nucleosome-binding assays, leukemic transformation assay Nature structural & molecular biology High 38448574
2024 KAT7 crotonylation at K432 (facilitated by hMOF) competes against its acetylation (regulated by HDAC2) at the same residue upon DNA damage. This competition reduces HBO1 histone acetyltransferase activity, leading to decreased H3K14ac at procentriole formation gene promoters and inhibition of procentriole formation. Site-specific K432 crotonylation/acetylation mutants, in vitro HAT assay, co-IP with hMOF/HDAC2, ChIP-qPCR for H3K14ac, procentriole formation assay Nature communications High 40064919
2025 KAT7 and KAT6A associate with NUP98 fusion oncoproteins on chromatin and within phase-separated condensates via the common subunit BRPF1. Genetic inactivation or pharmacologic inhibition of KAT7 decreases global H3K23ac, displaces NUP98::HOXA9 from chromatin at the Meis1 locus, and leads to myeloid differentiation. KAT6A/7 inhibition is efficacious in menin inhibitor-resistant NUP98-rearranged leukemia. CRISPR genetic inactivation, pharmacologic inhibition, ChIP-seq for H3K23ac and NUP98 fusion, co-IP, in vivo xenograft mouse models, synergy analysis with menin inhibitor Cancer discovery High 40536430
2025 Loss of KAT7 suppresses KAT7-mediated acetylation of the transcriptional repressor RFX1, stabilizing RFX1 (by blocking its proteasomal degradation) and thereby suppressing FGF1 transcription, leading to neuronal damage. NgBR regulates this axis by controlling KAT7 expression. RNA sequencing, co-immunoprecipitation (KAT7-RFX1 interaction), KAT7 KO, western blot for RFX1 stability, FGF1 transcription analysis, neuronal apoptosis assay Cellular and molecular life sciences : CMLS Medium 40192836
2024 KAT7 acetylates LDHA at lysine 118 in head and neck squamous carcinoma (HNSCC), enhancing LDHA activity and upregulating LDHA protein expression, thereby promoting the Warburg effect and tumor proliferation/metastasis. Co-immunoprecipitation, in vitro acetylation assay, site-specific K118 mutation, lactate production assay, KAT7 KO/OE with LDHA rescue, xenograft mouse model Cancer letters Medium 38593918
2020 MEAF6 modulates KAT7 complex assembly; in the absence of MEAF6, KAT7 increases its ability to interact with PHD-finger proteins (Brpfs/Jades). MEAF6 is essential for cell proliferation but not for HAT activity itself. Inducible Meaf6 KO in mouse ES cells, co-immunoprecipitation, histone acetylation western blot, cell proliferation assay Experimental cell research Medium 32918898
2020 BRPF3-mediated degradation pathway: the E3 ligase HUWE1 mediates ubiquitin-dependent degradation of Myst2/KAT7, and BRPF3 antagonizes HUWE1-mediated Myst2 degradation by direct protein-protein interaction, retaining Myst2 stability. This balance is required for normal differentiation and cell-cycle progression in embryonic stem cells. Co-immunoprecipitation, ubiquitination assay, BRPF3/HUWE1 overexpression/KD, Myst2 stability western blot, ESC differentiation assay Cell death and differentiation Medium 32555450
2006 HBO1 inhibits NF-κB activity by coactivator sequestration (squelching), not by binding p65/RelA or disrupting NF-κB DNA binding. The N-terminal serine-rich region of HBO1 (not its acetyltransferase domain) is required for this inhibitory activity. Reporter gene assay, EMSA, NF-κB component overexpression, N-terminal deletion mutants Biochemical and biophysical research communications Medium 16997280
2007 FAD24 interacts with HBO1 and recruits it to origins of DNA replication during late mitosis (when the pre-RC is assembled). When fad24 is knocked down, recruitment of HBO1 to origins is reduced, impairing mitotic clonal expansion during adipogenesis. Co-immunoprecipitation, ChIP at replication origins, siRNA knockdown, colocalization by immunofluorescence The Journal of biological chemistry Medium 18029353
2021 HBO1 promotes angiogenic tip cell sprouting through maintaining H3K14ac and appropriate gene expression in endothelial cells. Loss of HBO1 impairs developmental sprouting angiogenesis; single-cell RNA-seq reveals increased tip cell abundance and overcrowding in the sprouting front. Endothelial-specific conditional KO, retinal wholemount imaging, single-cell RNA-seq, H3K14ac ChIP-seq Development (Cambridge, England) High 34550360

Source papers

Stage 0 corpus · 100 papers · ranked by NIH iCite citations
Year Title Journal Citations PMID
1999 Histone acetyltransferase HBO1 interacts with the ORC1 subunit of the human initiator protein. The Journal of biological chemistry 263 10438470
2010 HBO1 histone acetylase activity is essential for DNA replication licensing and inhibited by Geminin. Molecular cell 202 20129055
2024 HBO1 catalyzes lysine lactylation and mediates histone H3K9la to regulate gene transcription. Nature communications 185 38670996
2011 The Hbo1-Brd1/Brpf2 complex is responsible for global acetylation of H3K14 and required for fetal liver erythropoiesis. Blood 173 21753189
2006 Regulation of replication licensing by acetyltransferase Hbo1. Molecular and cellular biology 162 16428461
2001 Replication factors MCM2 and ORC1 interact with the histone acetyltransferase HBO1. The Journal of biological chemistry 162 11278932
2009 HBO1 HAT complexes target chromatin throughout gene coding regions via multiple PHD finger interactions with histone H3 tail. Molecular cell 159 19187766
2019 HBO1 is required for the maintenance of leukaemia stem cells. Nature 148 31827282
2020 CircMRPS35 suppresses gastric cancer progression via recruiting KAT7 to govern histone modification. Molecular cancer 147 32164722
2010 HBO1 is required for H3K14 acetylation and normal transcriptional activity during embryonic development. Molecular and cellular biology 147 21149574
2008 HBO1 histone acetylase is a coactivator of the replication licensing factor Cdt1. Genes & development 147 18832067
2015 BRPF3-HBO1 regulates replication origin activation and histone H3K14 acetylation. The EMBO journal 115 26620551
2000 Androgen receptor interacts with a novel MYST protein, HBO1. The Journal of biological chemistry 109 10930412
2011 Conserved molecular interactions within the HBO1 acetyltransferase complexes regulate cell proliferation. Molecular and cellular biology 82 22144582
2016 KAT7/HBO1/MYST2 Regulates CENP-A Chromatin Assembly by Antagonizing Suv39h1-Mediated Centromere Inactivation. Developmental cell 79 27270040
2008 Role for Plk1 phosphorylation of Hbo1 in regulation of replication licensing. Proceedings of the National Academy of Sciences of the United States of America 79 18250300
2009 Histone acetyltransferase Hbo1: catalytic activity, cellular abundance, and links to primary cancers. Gene 76 19393168
2021 HBO1 is a versatile histone acyltransferase critical for promoter histone acylations. Nucleic acids research 71 34259319
2021 The histone acetyltransferase HBO1 functions as a novel oncogenic gene in osteosarcoma. Theranostics 70 33754016
2012 Plk1 phosphorylation of orc2 and hbo1 contributes to gemcitabine resistance in pancreatic cancer. Molecular cancer therapeutics 70 23188630
2008 Role of Jade-1 in the histone acetyltransferase (HAT) HBO1 complex. The Journal of biological chemistry 65 18684714
2022 The histone lysine acetyltransferase HBO1 (KAT7) regulates hematopoietic stem cell quiescence and self-renewal. Blood 59 34724565
2010 Chromatin unfolding by Cdt1 regulates MCM loading via opposing functions of HBO1 and HDAC11-geminin. Cell cycle (Georgetown, Tex.) 57 20980834
2006 Ligand-controlled interaction of histone acetyltransferase binding to ORC-1 (HBO1) with the N-terminal transactivating domain of progesterone receptor induces steroid receptor coactivator 1-dependent coactivation of transcription. Molecular endocrinology (Baltimore, Md.) 54 16645042
2007 Hbo1 Links p53-dependent stress signaling to DNA replication licensing. Molecular and cellular biology 52 17954561
2007 FAD24 acts in concert with histone acetyltransferase HBO1 to promote adipogenesis by controlling DNA replication. The Journal of biological chemistry 50 18029353
2012 Histone acetyl transferase (HAT) HBO1 and JADE1 in epithelial cell regeneration. The American journal of pathology 45 23159946
2021 Circular RNA Foxo3 Relieves Myocardial Ischemia/Reperfusion Injury by Suppressing Autophagy via Inhibiting HMGB1 by Repressing KAT7 in Myocardial Infarction. Journal of inflammation research 44 34880642
2018 Histone acetyltransferase 7 (KAT7)-dependent intragenic histone acetylation regulates endothelial cell gene regulation. The Journal of biological chemistry 44 29414790
2017 HBO1 promotes cell proliferation in bladder cancer via activation of Wnt/β-catenin signaling. Molecular carcinogenesis 44 28796367
2020 KAT7 is a genetic vulnerability of acute myeloid leukemias driven by MLL rearrangements. Leukemia 43 32764680
2019 Deciphering structure, function and mechanism of lysine acetyltransferase HBO1 in protein acetylation, transcription regulation, DNA replication and its oncogenic properties in cancer. Cellular and molecular life sciences : CMLS 43 31535175
2013 Hbo1 is a cyclin E/CDK2 substrate that enriches breast cancer stem-like cells. Cancer research 42 23955388
2016 Human T-cell leukemia virus type-1-encoded protein HBZ represses p53 function by inhibiting the acetyltransferase activity of p300/CBP and HBO1. Oncotarget 41 26625199
2011 JNK1 phosphorylation of Cdt1 inhibits recruitment of HBO1 histone acetylase and blocks replication licensing in response to stress. Molecular cell 41 21856198
2017 Phosphorylated HBO1 at UV irradiated sites is essential for nucleotide excision repair. Nature communications 38 28719581
2013 SCF(Fbxw15) mediates histone acetyltransferase binding to origin recognition complex (HBO1) ubiquitin-proteasomal degradation to regulate cell proliferation. The Journal of biological chemistry 38 23319590
2010 The dimeric structure and the bivalent recognition of H3K4me3 by the tumor suppressor ING4 suggests a mechanism for enhanced targeting of the HBO1 complex to chromatin. Journal of molecular biology 36 20053357
2019 HBO1 directs histone H4 specific acetylation, potentiating mechano-transduction pathways and membrane elasticity in ovarian cancer cells. Nanomedicine : nanotechnology, biology, and medicine 34 30759370
2015 The Chromatin Regulator BRPF3 Preferentially Activates the HBO1 Acetyltransferase but Is Dispensable for Mouse Development and Survival. The Journal of biological chemistry 34 26677226
2016 Essential role for the histone acetyltransferase KAT7 in T cell development, fitness, and survival. Journal of leukocyte biology 32 27733580
2015 UV Damage-Induced Phosphorylation of HBO1 Triggers CRL4DDB2-Mediated Degradation To Regulate Cell Proliferation. Molecular and cellular biology 32 26572825
2019 UHRF1-KAT7-mediated regulation of TUSC3 expression via histone methylation/acetylation is critical for the proliferation of colon cancer cells. Oncogene 31 31582837
2023 Stem cell plasticity, acetylation of H3K14, and de novo gene activation rely on KAT7. Cell reports 30 36641753
2013 Histone acetyltransferase Hbo1 destabilizes estrogen receptor α by ubiquitination and modulates proliferation of breast cancers. Cancer science 30 24125069
2023 Identification of Histone Lysine Acetoacetylation as a Dynamic Post-Translational Modification Regulated by HBO1. Advanced science (Weinheim, Baden-Wurttemberg, Germany) 29 37382194
2023 Histone acetylation by HBO1 (KAT7) activates Wnt/β-catenin signaling to promote leukemogenesis in B-cell acute lymphoblastic leukemia. Cell death & disease 29 37542030
2020 HBO1 (KAT7) Does Not Have an Essential Role in Cell Proliferation, DNA Replication, or Histone 4 Acetylation in Human Cells. Molecular and cellular biology 29 31767635
2020 NCAPG2 facilitates glioblastoma cells' malignancy and xenograft tumor growth via HBO1 activation by phosphorylation. Cell and tissue research 29 32897418
2019 LYAR potentiates rRNA synthesis by recruiting BRD2/4 and the MYST-type acetyltransferase KAT7 to rDNA. Nucleic acids research 29 31504794
2017 Structural and mechanistic insights into regulation of HBO1 histone acetyltransferase activity by BRPF2. Nucleic acids research 29 28334966
2018 The scaffolding protein JADE1 physically links the acetyltransferase subunit HBO1 with its histone H3-H4 substrate. The Journal of biological chemistry 28 29382722
2020 The Protective Effect of HBO1 on Cigarette Smoke Extract-Induced Apoptosis in Airway Epithelial Cells. International journal of chronic obstructive pulmonary disease 27 32021140
2015 The histone acetyltransferase Myst2 regulates Nanog expression, and is involved in maintaining pluripotency and self-renewal of embryonic stem cells. FEBS letters 27 25743411
2022 HBO1 catalyzes lysine benzoylation in mammalian cells. iScience 26 36388951
2023 A first-in-class HBO1 inhibitor WM-3835 inhibits castration-resistant prostate cancer cell growth in vitro and in vivo. Cell death & disease 25 36709328
2022 HBO1 induces histone acetylation and is important for non-small cell lung cancer cell growth. International journal of biological sciences 25 35637972
2021 HBO1 overexpression is important for hepatocellular carcinoma cell growth. Cell death & disease 25 34039960
2021 HBO1-MLL interaction promotes AF4/ENL/P-TEFb-mediated leukemogenesis. eLife 23 34431785
2018 LPS promotes HBO1 stability via USP25 to modulate inflammatory gene transcription in THP-1 cells. Biochimica et biophysica acta. Gene regulatory mechanisms 23 30745998
2014 Cell cycle-dependent chromatin shuttling of HBO1-JADE1 histone acetyl transferase (HAT) complex. Cell cycle (Georgetown, Tex.) 23 24739512
2006 Histone acetyltransferase HBO1 inhibits NF-kappaB activity by coactivator sequestration. Biochemical and biophysical research communications 23 16997280
2015 MYST2 acetyltransferase expression and Histone H4 Lysine acetylation are suppressed in AML. Experimental hematology 22 26072331
2023 Circ-myh8 Promotes Pulmonary Hypertension by Recruiting KAT7 to Govern Hypoxia-Inducible Factor-1α Expression. Journal of the American Heart Association 21 36942752
2022 KAT7-mediated CANX (calnexin) crotonylation regulates leucine-stimulated MTORC1 activity. Autophagy 20 35266843
2023 The NLRP11 Protein Bridges the Histone Lysine Acetyltransferase KAT7 to Acetylate Vimentin in the Early Stage of Lung Adenocarcinoma. Advanced science (Weinheim, Baden-Wurttemberg, Germany) 19 37424170
2019 A novel long non-coding RNA-KAT7 is low expressed in colorectal cancer and acts as a tumor suppressor. Cancer cell international 19 30858757
2019 NUP98-HBO1-fusion generates phenotypically and genetically relevant chronic myelomonocytic leukemia pathogenesis. Blood advances 19 30944097
2005 Cyclin-dependent kinase 11(p58) interacts with HBO1 and enhances its histone acetyltransferase activity. FEBS letters 19 15963510
2019 HBOA ameliorates CCl4-incuded liver fibrosis through inhibiting TGF-β1/Smads, NF-κB and ERK signaling pathways. Biomedicine & pharmacotherapy = Biomedecine & pharmacotherapie 18 31079002
2017 Intrinsic ubiquitin E3 ligase activity of histone acetyltransferase Hbo1 for estrogen receptor α. Proceedings of the Japan Academy. Series B, Physical and biological sciences 17 28769019
2025 KAT6A and KAT7 Histone Acetyltransferase Complexes Are Molecular Dependencies and Therapeutic Targets in NUP98-Rearranged Acute Myeloid Leukemia. Cancer discovery 16 40536430
2010 Estrogen receptor α (ERα) mediates 17β-estradiol (E2)-activated expression of HBO1. Journal of experimental & clinical cancer research : CR 15 21040551
2022 The acetyltransferase KAT7 is required for thymic epithelial cell expansion, expression of AIRE target genes, and thymic tolerance. Science immunology 14 35061506
2020 MicroRNA-639 is Down-Regulated in Hepatocellular Carcinoma Tumor Tissue and Inhibits Proliferation and Migration of Human Hepatocellular Carcinoma Cells Through the KAT7/Wnt/β-Catenin Pathway. Medical science monitor : international medical journal of experimental and clinical research 14 31955177
2017 Upregulated KAT7 in synovial fibroblasts promotes Th17 cell differentiation and infiltration in rheumatoid arthritis. Biochemical and biophysical research communications 14 28552525
2024 Spermidine metabolism regulates leukemia stem and progenitor cell function through KAT7 expression in patient-derived mouse models. Science translational medicine 13 39321266
2023 KAT7 promotes radioresistance through upregulating PI3K/AKT signaling in breast cancer. Journal of radiation research 13 36724120
2020 BRPF3-HUWE1-mediated regulation of MYST2 is required for differentiation and cell-cycle progression in embryonic stem cells. Cell death and differentiation 13 32555450
2020 Protein kinase D1 phosphorylation of KAT7 enhances its protein stability and promotes replication licensing and cell proliferation. Cell death discovery 13 33014433
2017 Myst2/Kat7 histone acetyltransferase interaction proteomics reveals tumour-suppressor Niam as a novel binding partner in embryonic stem cells. Scientific reports 13 28811661
2013 Expression and characterization of androgen receptor coregulators, SRC-2 and HBO1, during human testis ontogenesis and in androgen signaling deficient patients. Molecular and cellular endocrinology 13 23707616
2024 KAT7 enhances the proliferation and metastasis of head and neck squamous carcinoma by promoting the acetylation level of LDHA. Cancer letters 12 38593918
2023 The lncRNA ADAMTS9-AS1/miR-185-5p/KAT7 ceRNA network inhibits cardiomyocyte hypertrophy in hypertrophic obstructive cardiomyopathy. Biomedical research (Tokyo, Japan) 12 37258203
2025 Competitive antagonism of KAT7 crotonylation against acetylation affects procentriole formation and colorectal tumorigenesis. Nature communications 11 40064919
2024 Guiding the HBO1 complex function through the JADE subunit. Nature structural & molecular biology 11 38448574
2024 Multifunctional acyltransferase HBO1: a key regulatory factor for cellular functions. Cellular & molecular biology letters 11 39543485
2010 Histone acetylation by HBO1 tightens replication licensing. Molecular cell 11 20129050
2025 Targeting KAT7 inhibits the progression of colorectal cancer. Theranostics 10 39816686
2023 A Therapeutically Targetable NOTCH1-SIRT1-KAT7 Axis in T-cell Leukemia. Blood cancer discovery 10 36322781
2023 The circular RNA Rap1b promotes Hoxa5 transcription by recruiting Kat7 and leading to increased Fam3a expression, which inhibits neuronal apoptosis in acute ischemic stroke. Neural regeneration research 8 37056143
2021 The histone acetyltransferase HBO1 promotes efficient tip cell sprouting during angiogenesis. Development (Cambridge, England) 8 34550360
2020 LncRNA-KAT7 Negatively Regulates miR-10a Through an Epigenetic Pathway to Participate in Nonsmall Cell Lung Cancer. Cancer biotherapy & radiopharmaceuticals 8 32423237
2024 HBO1, a MYSTerious KAT and its links to cancer. Biochimica et biophysica acta. Gene regulatory mechanisms 7 38851533
2022 HBO1 as an Important Target for the Treatment of CCL4-Induced Liver Fibrosis and Aged-Related Liver Aging and Fibrosis. Oxidative medicine and cellular longevity 7 36524217
2016 Functional analysis of HBO1 in tumor development and inhibitor screening. International journal of molecular medicine 7 27247147
2025 Loss of NgBR causes neuronal damage through decreasing KAT7-mediated RFX1 acetylation and FGF1 expression. Cellular and molecular life sciences : CMLS 6 40192836
2024 HBO1 determines SMAD action in pluripotency and mesendoderm specification. Nucleic acids research 6 38421638
2022 KAT7 promoted gastric cancer progression through promoting YAP1 activation. Pathology, research and practice 6 35868058
2020 MEAF6 is essential for cell proliferation and plays a role in the assembly of KAT7 complexes. Experimental cell research 6 32918898

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