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Showing CYRIACYRI-A is a alias.

CYRIA

CYFIP-related Rac1 interactor A · UniProt Q9H0Q0

Length
323 aa
Mass
37.3 kDa
Annotated
2026-06-09
16 papers in source corpus 3 papers cited in narrative 5 extracted findings
Cross-family judge vs UniProt: Affinage preferred faithfulness: 5/5 claims corpus-supported (100%)

Mechanistic narrative

Synthesis pass · prose summary of the discoveries below

CYRI-A is a RAC1-interacting protein that negatively regulates actin dynamics to control macropinocytosis and integrin trafficking (PMID:34165494, PMID:33217330). It is transiently recruited to nascent macropinosomes in a PI3K- and RAC1-dependent manner, arriving after RAC1 and actin signaling but before RAB5A, consistent with a role as a local inhibitor of actin polymerization at these sites (PMID:34165494). Mechanistically, CYRI-family proteins bind active GTP-bound RAC1 through an N-terminal RAC1-binding subdomain and compete with the Scar/WAVE complex for this interaction, establishing a negative feedback loop on RAC1-driven actin assembly (PMID:33217330). CYRI-A and its paralog CYRI-B can additionally form autoinhibited homo- and heterodimers, adding a further regulatory layer to RAC1 signaling (PMID:33217330). Functionally, loss of CYRI proteins reduces internalization of high-molecular-weight dextran, confirming their requirement for macropinocytosis (PMID:35530513), while co-depletion of CYRI-A and CYRI-B elevates surface α5β1 integrin via reduced internalization and enhances cell migration, invasion, and anchorage-independent growth (PMID:34165494).

Mechanistic history

Synthesis pass · year-by-year structured walk · 5 steps
  1. 2020 High

    Establishing how CYRI proteins act on RAC1 was needed to explain their effect on actin; the structure showed CYRI-B binds active RAC1 and competes with Scar/WAVE, defining a negative-feedback mechanism on actin dynamics.

    Evidence Crystal structure of CYRI-B:RAC1Q61L complex with competitive binding assays

    PMID:33217330

    Open questions at the time
    • CYRI-A itself was characterized largely as a family member by dimerization behavior, not by an independent CYRI-A:RAC1 structure
    • the cellular consequence of dimerization on RAC1 binding was not functionally dissected
    • stoichiometry and dynamics of CYRI vs Scar/WAVE competition in cells not resolved
  2. 2020 High

    Beyond a single inhibitory mode, it was unknown how CYRI activity is itself regulated; demonstrating that CYRI-A and CYRI-B form autoinhibited homo- and heterodimers added an additional regulatory layer to RAC1 signaling.

    Evidence Biochemical analysis of CYRI-A/B dimerization alongside crystallographic domain architecture analysis

    PMID:33217330

    Open questions at the time
    • trigger and kinetics of dimer assembly/disassembly in cells unknown
    • relative abundance and biological role of homodimers vs heterodimers not defined
  3. 2021 High

    Where and when CYRI-A acts in the cell was unknown; live imaging placed it transiently at nascent macropinosomes downstream of PI3K/RAC1/actin and before RAB5A, localizing its inhibitory function to an early macropinosome stage.

    Evidence Live-cell imaging, subcellular localization, PI3K/RAC1 pharmacological inhibition, and depletion in cultured cells

    PMID:34165494

    Open questions at the time
    • molecular signal driving the transient recruitment and departure not identified
    • whether RAB5A timing is a direct consequence of CYRI-A action untested
  4. 2021 Medium

    The downstream physiological output of CYRI loss was unclear; co-depletion of CYRI-A and CYRI-B raised surface α5β1 integrin via reduced internalization and increased migration, invasion, and 3D growth, linking CYRI to integrin trafficking and invasive behavior.

    Evidence siRNA knockdown, surface integrin flow cytometry, Transwell migration/invasion and 3D growth assays

    PMID:34165494

    Open questions at the time
    • CYRI-A-specific contribution not separated from CYRI-B in the co-depletion phenotype
    • direct mechanistic link between actin/macropinosome regulation and integrin internalization not established
  5. 2022 Medium

    A dedicated functional readout was needed to confirm the macropinocytosis role; CYRI-depleted cells internalized less high-molecular-weight dextran, directly confirming a requirement for CYRI proteins in macropinocytosis.

    Evidence Image-based dextran uptake assay with fluorescence quantification in CYRI-depleted cells

    PMID:35530513

    Open questions at the time
    • single-method assay from one lab
    • does not separate CYRI-A from CYRI-B contributions to dextran uptake

Open questions

Synthesis pass · forward-looking unresolved questions
  • It remains unknown how CYRI-A and CYRI-B activities are individually apportioned across macropinocytosis, integrin trafficking, and migration, and how dimerization-based autoinhibition is dynamically controlled in living cells.
  • no CYRI-A-specific loss-of-function dissection separating it from CYRI-B
  • no characterization of the upstream signal that toggles dimer autoinhibition

Mechanism profile

Synthesis pass · controlled-vocabulary classification · explore literature graph →
Molecular activity
GO:0098772 molecular function regulator activity 2 GO:0008092 cytoskeletal protein binding 1
Localization
GO:0031410 cytoplasmic vesicle 1
Pathway
R-HSA-5653656 Vesicle-mediated transport 2 R-HSA-162582 Signal Transduction 1
Partners

Evidence

Reading pass · 5 per-paper findings extracted from the source corpus
Year Finding Method Journal Conf PMIDs
2021 CYRI-A is transiently recruited to nascent macropinosomes in a PI3K- and RAC1-dependent manner; its recruitment follows RAC1 and actin signaling but precedes RAB5A recruitment, consistent with CYRI-A acting as a local inhibitor of actin polymerization at macropinosomes. Live-cell imaging, subcellular fractionation/localization, pharmacological inhibition of PI3K and RAC1, depletion experiments The Journal of cell biology High 34165494
2021 Depletion of both CYRI-A and CYRI-B results in enhanced surface expression of α5β1 integrin via reduced integrin internalization, and co-depletion enhances cell migration, invasion, and anchorage-independent growth in 3D. siRNA knockdown, flow cytometry for surface integrin levels, Transwell migration and invasion assays, 3D growth assays The Journal of cell biology Medium 34165494
2020 CYRI-A and CYRI-B can form autoinhibited hetero- or homodimers, adding an additional regulatory layer to RAC1 signaling. The CYRI protein family members share a domain architecture with an N-terminal RAC1-binding subdomain and a C-terminal Ratchet subdomain. Crystal structure of CYRI-B:RAC1Q61L complex; biochemical analysis of CYRI-A/B dimerization Structure (London, England : 1993) High 33217330
2020 CYRI proteins (including CYRI-A) compete with the Scar/WAVE complex for binding to active (GTP-bound) RAC1, providing a feedback mechanism that negatively regulates actin dynamics. Crystal structure of CYRI-B:RAC1Q61L complex; competitive binding assays Structure (London, England : 1993) High 33217330
2022 Cells lacking CYRI proteins (CYRI-A and CYRI-B) internalize less high-molecular-weight dextran compared to wild-type cells, confirming a role for CYRI proteins in macropinocytosis. Image-based dextran uptake assay in CYRI-depleted cultured cells, fluorescence microscopy quantification Bio-protocol Medium 35530513

Source papers

Stage 0 corpus · 16 papers · ranked by NIH iCite citations
Year Title Journal Citations PMID
2010 Gene amplification as double minutes or homogeneously staining regions in solid tumors: origin and structure. Genome research 194 20631050
2016 A multi-ethnic genome-wide association study identifies novel loci for non-syndromic cleft lip with or without cleft palate on 2p24.2, 17q23 and 19q13. Human molecular genetics 188 27033726
2005 Effect of cryopreservation on sea bass sperm proteins. Biology of reproduction 43 15659707
2018 Identification of novel lncRNAs regulated by the TAL1 complex in T-cell acute lymphoblastic leukemia. Leukemia 38 29654272
2021 CYRI-A limits invasive migration through macropinosome formation and integrin uptake regulation. The Journal of cell biology 27 34165494
2021 Phenome risk classification enables phenotypic imputation and gene discovery in developmental stuttering. American journal of human genetics 26 34861174
2020 The Rac2 GTPase contributes to cathepsin H-mediated protection against cytokine-induced apoptosis in insulin-secreting cells. Molecular and cellular endocrinology 16 32814070
2022 Image-based Quantification of Macropinocytosis Using Dextran Uptake into Cultured Cells. Bio-protocol 12 35530513
2020 Structural Basis of CYRI-B Direct Competition with Scar/WAVE Complex for Rac1. Structure (London, England : 1993) 12 33217330
2022 Genome-wide association study of multiethnic nonsyndromic orofacial cleft families identifies novel loci specific to family and phenotypic subtypes. Genetic epidemiology 11 35191549
2018 Genetic variants of MGMT, RHPN2, and FAM49A contributed to susceptibility of nonsyndromic orofacial clefts in a Chinese population. Journal of oral pathology & medicine : official publication of the International Association of Oral Pathologists and the American Academy of Oral Pathology 10 29949196
2016 Microscopy and Microanalysis of Blood in a Snake Head Fish, Channa gachua Exposed to Environmental Pollution. Microscopy and microanalysis : the official journal of Microscopy Society of America, Microbeam Analysis Society, Microscopical Society of Canada 8 26914995
2025 A non-syndromic orofacial cleft risk locus links tRNA splicing defects to neural crest cell pathologies. American journal of human genetics 2 40250422
2024 Association of selected gene variants with nonsyndromic orofacial clefts in Kuwait. Gene 2 39442823
2023 Alectinib relieves ischemic strokes caused by left atrial metastasis in a NSCLC patient with a novel SLC34A2-ALK (exon 1: exon 15) fusion. Lung cancer (Amsterdam, Netherlands) 2 37542770
2026 Transcription-based identification of uncharacterized genes in the human immune response. European journal of human genetics : EJHG 0 42120540

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