Affinage

ARHGAP4

Rho GTPase-activating protein 4 · UniProt P98171

Length
946 aa
Mass
105.0 kDa
Annotated
2026-06-09
18 papers in source corpus 11 papers cited in narrative 13 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

ARHGAP4 is a multi-domain Rho GTPase-activating protein that integrates cytoskeletal regulation with the control of cell and axon motility (PMID:12414125, PMID:17804252). Recombinant ARHGAP4 stimulates the intrinsic GTPase activity of Rac1, Cdc42, and RhoA, establishing it as a functional GAP for multiple Rho-family members (PMID:12414125). Its modular architecture partitions these activities: the FCH domain directs localization to the leading edges of migrating cells and to axon growth cones, while the GAP domain and C-terminus are required for its inhibition of cell migration and axon outgrowth (PMID:17804252). Through its RhoGAP and SH3 domains, ARHGAP4 assembles a complex with the septins SEPT2 and SEPT9 that reorganizes focal adhesions and modulates integrin-β1–dependent migration and invasion (PMID:34524873), and it suppresses epithelial-to-mesenchymal transition and focal-adhesion–driven force generation, with Septin9 acting as a negative regulator that promotes EMT via FAK/Src signaling (PMID:32378260). Beyond its canonical GAP role, ARHGAP4 functions as a scaffolding and regulatory protein in cancer: it promotes ubiquitination of HDAC2 to suppress β-catenin activation and tumor cell invasion (PMID:30958531), binds p53 to repress DRAM1-dependent apoptosis in acute myeloid leukemia (PMID:37443303), and drives colorectal cancer stemness through a MYH9/β-catenin/c-Jun feedback loop (PMID:40817404). Its expression is suppressed by miR-939-5p (PMID:32021284).

Mechanistic history

Synthesis pass · year-by-year structured walk · 8 steps
  1. 2002 High

    Established ARHGAP4 as a biochemically active GAP and placed it at the Golgi and motility structures, defining its candidate cellular context.

    Evidence In vitro GTPase assays with recombinant protein on Rac1/Cdc42/RhoA plus subcellular fractionation and immunofluorescence of endogenous protein

    PMID:12414125

    Open questions at the time
    • In vitro substrate preference among Rac1/Cdc42/RhoA not quantified
    • Functional consequence of Golgi/microtubule localization unresolved
  2. 2007 Medium

    Mapped functional roles to specific domains, showing the FCH domain governs localization while the GAP domain and C-terminus drive motility inhibition.

    Evidence Domain-deletion structure/function analysis with live-cell migration and hippocampal axon outgrowth assays

    PMID:17804252

    Open questions at the time
    • Which Rho GTPase mediates the migration/axon phenotype in cells not established
    • Endogenous loss-of-function not tested (overexpression-based)
  3. 2019 Medium

    Revealed a non-canonical scaffolding mechanism whereby ARHGAP4 promotes HDAC2 ubiquitination to restrain β-catenin and tumor invasion, and placed it upstream of the mTOR/HIF-1α Warburg axis.

    Evidence Co-IP, ubiquitination assay, siRNA knockdown, pharmacological rescue (CAY10683, XAV939, rapamycin, YC-1), invasion/migration and metabolic assays in pancreatic cancer cells

    PMID:30958531 PMID:31303760

    Open questions at the time
    • Whether ARHGAP4 has direct E3 ligase activity or recruits one is not defined
    • Link between GAP activity and HDAC2/β-catenin axis unresolved
  4. 2020 Medium

    Identified upstream regulation by miR-939-5p and a septin-mediated route to EMT control, with Septin9 acting as a negative regulator via FAK/Src.

    Evidence Luciferase reporter target validation and rescue; RhoGAP siRNA screen, proteomics, traction force microscopy and 3D morphogenesis in mammary epithelial cells

    PMID:32021284 PMID:32378260

    Open questions at the time
    • Mechanism by which Septin9 inhibits ARHGAP4 not defined at molecular level
    • Direct ARHGAP4–Septin9 binding interface not mapped here
  5. 2021 High

    Defined a direct ARHGAP4–SEPT2–SEPT9 complex and showed it bidirectionally controls integrin-β1–dependent focal adhesions and invasion.

    Evidence Reciprocal Co-IP with RhoGAP/SH3 domain mapping, siRNA knockdown, overexpression of multiple complex members, focal adhesion and migration/invasion assays

    PMID:34524873

    Open questions at the time
    • Stoichiometry and structural architecture of the complex unknown
    • Whether GAP catalytic activity is required for focal adhesion remodeling not tested
  6. 2023 Medium

    Established a p53-binding, apoptosis-suppressing role in leukemia by placing ARHGAP4 upstream of p53/DRAM1.

    Evidence Co-IP (ARHGAP4-p53), siRNA knockdown, DRAM1 epistatic rescue, in vivo AML model and apoptosis/colony assays

    PMID:37443303

    Open questions at the time
    • Binding interface and effect of ARHGAP4 on p53 transcriptional activity not detailed
    • Relationship between GAP function and p53 regulation unknown
  7. 2024 Low

    Extended ARHGAP4's pro-tumor/EMT activity to colon cancer (TGF-β/Smad) and to apoptosis/inflammation in ovarian granulosa cells (PI3K-Akt).

    Evidence siRNA knockdown with Western blotting for pathway and EMT markers; CCK-8, annexin-V/PI, ELISA in granulosa cells and clinical tissue

    PMID:38355537 PMID:38805788

    Open questions at the time
    • No direct binding or rescue experiments to establish causality
    • Context-dependent opposite roles (pro- vs anti-tumor) not reconciled
  8. 2025 Medium

    Identified a MYH9/β-catenin/c-Jun positive feedback loop through which ARHGAP4 drives cancer stemness.

    Evidence Co-IP (ARHGAP4-MYH9), ChIP (c-Jun binding), FRAP, in vitro/in vivo stemness assays

    PMID:40817404

    Open questions at the time
    • How the GAP/scaffolding domains engage MYH9 not mapped
    • Reconciliation with ARHGAP4's β-catenin-suppressing role in pancreatic cancer unresolved

Open questions

Synthesis pass · forward-looking unresolved questions
  • It remains unresolved how ARHGAP4's canonical Rho-GAP catalytic activity mechanistically connects to its diverse scaffolding functions (HDAC2 ubiquitination, p53, MYH9), and why it acts as a migration suppressor in some contexts but a tumor/stemness driver in others.
  • No structural model linking GAP and scaffolding activities
  • Context-determinants of opposing phenotypes undefined
  • In vivo physiological (non-cancer) function not established

Mechanism profile

Synthesis pass · controlled-vocabulary classification · explore literature graph →
Molecular activity
GO:0098772 molecular function regulator activity 2 GO:0060089 molecular transducer activity 1 GO:0060090 molecular adaptor activity 1
Localization
GO:0005794 Golgi apparatus 1 GO:0005856 cytoskeleton 1 GO:0005886 plasma membrane 1
Pathway
R-HSA-1643685 Disease 3 R-HSA-162582 Signal Transduction 2
Partners
HDAC2MYH9SEPT2SEPT9TP53
Complex memberships
ARHGAP4–SEPT2–SEPT9 complex

Evidence

Reading pass · 13 per-paper findings extracted from the source corpus
Year Finding Method Journal Conf PMIDs
2002 Recombinant ARHGAP4 stimulates the GTPase activity of Rac1, Cdc42, and RhoA in vitro, establishing it as a functional GAP for multiple Rho family members. In vitro GTPase activity assay with recombinant protein Brain research. Molecular brain research High 12414125
2002 Endogenous ARHGAP4 localizes to the Golgi complex and can redistribute to microtubules during mitosis; it is also detected at the tips of differentiating neurites in PC12 cells. Subcellular fractionation and immunofluorescence/localization studies Brain research. Molecular brain research Medium 12414125
2007 The FCH domain of ARHGAP4 is required for localizing the protein to the leading edges of migrating NIH/3T3 cells and to axon growth cones, while the GAP domain and C-terminus are necessary for ARHGAP4-mediated inhibition of cell migration and axon outgrowth. Structure/function analysis with domain deletion constructs; live-cell migration assay and hippocampal axon outgrowth assay Molecular and cellular neurosciences Medium 17804252
2007 Overexpression of ARHGAP4 inhibits NIH/3T3 cell migration and hippocampal axon outgrowth, establishing a functional role as an inhibitor of cell and axon motility. Overexpression in NIH/3T3 cells (migration assay) and hippocampal neurons (axon outgrowth assay) Molecular and cellular neurosciences Medium 17804252
2019 ARHGAP4 interacts with and promotes ubiquitination of HDAC2, which in turn inhibits β-catenin activation, suppressing MMP2/MMP9 expression and pancreatic cancer cell invasion and migration. Co-immunoprecipitation, ubiquitination assay, siRNA knockdown, pharmacological inhibitors (CAY10683, XAV939), invasion/migration assays Carcinogenesis Medium 30958531
2019 ARHGAP4 overexpression inhibits cell viability, glucose uptake, lactate release, PKM2 expression, and mTOR/HIF-1α pathway activation in pancreatic cancer cells; mTOR inhibitor (rapamycin) or HIF-1α inhibitor (YC-1) rescues the morphological changes induced by ARHGAP4 downregulation, placing ARHGAP4 upstream of the mTOR/HIF-1α axis in the Warburg effect. Lentiviral overexpression and siRNA knockdown; pharmacological inhibition of mTOR and HIF-1α; glucose uptake and lactate release assays; Western blotting OncoTargets and therapy Medium 31303760
2020 miR-939-5p directly targets and suppresses ARHGAP4 expression (validated by luciferase reporter assay), thereby promoting pancreatic cancer cell viability, invasion, and migration; ARHGAP4 overexpression reverses these effects. Luciferase reporter assay, RT-PCR, Western blot, Transwell invasion/migration assay, rescue experiment OncoTargets and therapy Medium 32021284
2020 ARHGAP4 suppresses epithelial-to-mesenchymal transition (EMT) in human mammary epithelial cells, regulating epithelial/mesenchymal marker expression, cell proliferation, migration, 3D morphogenesis, and focal adhesion/stress fiber-driven force generation; Septin9 was identified by proteomics as a negative regulator of ARHGAP4 that promotes EMT via FAK/Src signaling. Comprehensive RhoGAP siRNA screen, proteomic analysis, cell morphology/migration assays, traction force microscopy, 3D morphogenesis assay FASEB journal Medium 32378260
2021 ARHGAP4 forms a complex with SEPT2 and SEPT9 via its RhoGAP domain and SH3 domain; silencing ARHGAP4 or overexpressing SEPT2/SEPT9 independently induces reorganization of focal adhesions with upregulation of Integrin Beta 1, enhancing cell migration and invasion in a microenvironment-dependent manner. Co-immunoprecipitation, domain mapping, siRNA knockdown, overexpression, focal adhesion analysis, migration/invasion assays Molecular biology of the cell High 34524873
2023 ARHGAP4 binds p53 to inhibit DRAM1 expression in AML cells; ARHGAP4 knockdown activates DRAM1 signaling and induces apoptosis, while DRAM1 knockdown rescues the defects caused by ARHGAP4 deletion, placing ARHGAP4 upstream of p53/DRAM1 in AML leukemogenesis. Co-immunoprecipitation (ARHGAP4-p53 interaction), siRNA knockdown, in vivo AML progression model, apoptosis assay, colony formation assay Oncogene Medium 37443303
2024 ARHGAP4 knockdown inhibits migration and invasion of colon cancer cells and decreases expression of TGF-β1, p-Smad2, and p-Smad3, while increasing E-cadherin and decreasing N-cadherin/Vimentin, placing ARHGAP4 upstream of the TGF-β/Smad pathway and EMT in colon cancer. siRNA knockdown, Western blotting for TGF-β/Smad pathway proteins and EMT markers, Transwell migration/invasion assay Biochemical and biophysical research communications Low 38805788
2024 ARHGAP4 promotes apoptosis and inflammation in ovarian granulosa cells via the PI3K-Akt signaling pathway. CCK-8 assay, annexin-V/PI staining, ELISA, Western blot for PI3K-Akt pathway components, cell line and clinical tissue samples Journal of ovarian research Low 38355537
2025 ARHGAP4 drives colorectal cancer stemness through a positive feedback loop with MYH9/β-catenin/c-Jun, as demonstrated by co-immunoprecipitation (ARHGAP4-MYH9 interaction), chromatin immunoprecipitation (c-Jun binding), and FRAP. Co-immunoprecipitation, chromatin immunoprecipitation, FRAP, in vitro and in vivo stemness assays, bioinformatics NPJ precision oncology Medium 40817404

Source papers

Stage 0 corpus · 18 papers · ranked by NIH iCite citations
Year Title Journal Citations PMID
2007 ARHGAP4 is a novel RhoGAP that mediates inhibition of cell motility and axon outgrowth. Molecular and cellular neurosciences 55 17804252
2019 ARHGAP4 mediates the Warburg effect in pancreatic cancer through the mTOR and HIF-1α signaling pathways. OncoTargets and therapy 37 31303760
2002 Cloning of rat ARHGAP4/C1, a RhoGAP family member expressed in the nervous system that colocalizes with the Golgi complex and microtubules. Brain research. Molecular brain research 35 12414125
2002 Two novel types of contiguous gene deletion of the AVPR2 and ARHGAP4 genes in unrelated Japanese kindreds with nephrogenic diabetes insipidus. Human mutation 34 11754100
2019 ARHGAP4 regulates the cell migration and invasion of pancreatic cancer by the HDAC2/β-catenin signaling pathway. Carcinogenesis 33 30958531
2020 miR-939-5p Contributes to the Migration and Invasion of Pancreatic Cancer by Targeting ARHGAP4. OncoTargets and therapy 24 32021284
2020 Comprehensive analysis on the whole Rho-GAP family reveals that ARHGAP4 suppresses EMT in epithelial cells under negative regulation by Septin9. FASEB journal : official publication of the Federation of American Societies for Experimental Biology 24 32378260
2021 ARHGAP4-SEPT2-SEPT9 complex enables both up- and down-modulation of integrin-mediated focal adhesions, cell migration, and invasion. Molecular biology of the cell 19 34524873
2012 A novel contiguous gene deletion of AVPR2 and ARHGAP4 genes in male dizygotic twins with nephrogenic diabetes insipidus and intellectual disability. American journal of medical genetics. Part A 19 22965914
2008 Immunological profile in a family with nephrogenic diabetes insipidus with a novel 11 kb deletion in AVPR2 and ARHGAP4 genes. BMC medical genetics 16 18489790
2015 ARHGAP4 mutated in a Chinese intellectually challenged family. Gene 8 26707211
2023 ARHGAP4 promotes leukemogenesis in acute myeloid leukemia by inhibiting DRAM1 signaling. Oncogene 7 37443303
2022 Candidate Oncogenes, ARHGAP4, NOS3, and OR51B5, for the Development of Scirrhous-type Gastric Cancer. Anticancer research 6 36288877
2018 Contiguous 22.1-kb deletion embracing AVPR2 and ARHGAP4 genes at novel breakpoints leads to nephrogenic diabetes insipidus in a Chinese pedigree. BMC nephrology 6 29394883
2024 ARHGAP4 promotes colon cancer metastasis through the TGF-β signaling pathway and may be associated with T cell exhaustion. Biochemical and biophysical research communications 4 38805788
2024 Cai's prescription inhibits granulosa cell apoptosis through ARHGAP4 on poor ovarian responders. Journal of ovarian research 1 38355537
2024 ARHGAP4 Inhibits Proliferation and Growth of SW620 Colon Cancer Cells by Cell Cycle and Differentiation Pathways. Scientifica 1 38938545
2025 ARHGAP4/MYH9/β-catenin/c-Jun positive feedback loop promotes colorectal cancer stemness. NPJ precision oncology 0 40817404

Missed literature

Know a paper Affinage missed for ARHGAP4? Flag it for the maintainers and the community.

No submissions yet.