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Showing TBC1D31WDR67 is a alias.

TBC1D31

TBC1 domain family member 31 · UniProt Q96DN5

Length
1066 aa
Mass
124.2 kDa
Annotated
2026-06-10
8 papers in source corpus 5 papers cited in narrative 6 extracted findings
Cross-family judge vs UniProt: Affinage preferred faithfulness: 4/4 claims corpus-supported (100%)

Mechanistic narrative

Synthesis pass · prose summary of the discoveries below

TBC1D31 (also called WDR67) is a centrosomal/centriolar scaffold that couples signaling and structural control of the centriole to primary ciliogenesis (PMID:33934390, PMID:40707486). At the centrosome it assembles a complex with the E3 ubiquitin ligase praja2, protein kinase A (PKA), and OFD1; upon GPCR-cAMP stimulation PKA phosphorylates OFD1 at Ser735, driving its praja2-dependent ubiquitin-proteasome degradation, a step required for cilium biogenesis, with loss of TBC1D31 impairing ciliogenesis in cultured cells and in vivo in Medaka (PMID:33934390). Structurally, it localizes to the centriolar A-C linker in a complex with CCDC77 and MIIP that bridges adjacent microtubule triplets at the proximal region to maintain triplet cohesion and regulate centriole duplication (PMID:40707486). Independently, TBC1D31 acts as a Rab22A GTPase-activating protein that suppresses Rab22A-mediated endolysosomal trafficking and degradation of EGFR, sustaining EGFR signaling and promoting hepatocellular carcinoma growth, where its expression is transcriptionally activated by ZSCAN16 (PMID:39206796, PMID:39511655).

Mechanistic history

Synthesis pass · year-by-year structured walk · 6 steps
  1. 2021 High

    Established TBC1D31 as a centrosomal scaffold that links GPCR-cAMP/PKA signaling to controlled OFD1 turnover, answering how a signaling input gates ciliogenesis.

    Evidence Reciprocal Co-IP, centrosome localization, OFD1 S735A phospho-mutant analysis, and in vivo knockdown in Medaka

    PMID:33934390

    Open questions at the time
    • Does not define how TBC1D31 itself is recruited to the centrosome
    • Stoichiometry and assembly order of the praja2/PKA/OFD1 complex unresolved
  2. 2021 High

    Demonstrated that TBC1D31 is functionally required for primary ciliogenesis, moving it from a complex component to an essential biogenesis factor.

    Evidence Loss-of-function depletion in cell lines and Medaka with cilium morphology and developmental readouts

    PMID:33934390

    Open questions at the time
    • Whether ciliogenesis defects derive solely from OFD1 dysregulation or other pathways
    • No human disease/genetic link established in the corpus
  3. 2024 Medium

    Identified a distinct cytoplasmic role for TBC1D31 as a Rab22A GAP controlling EGFR trafficking, explaining a pro-tumorigenic function separate from its centriolar role.

    Evidence In vitro GAP activity assay, knockdown/overexpression in HCC cells and xenografts, endolysosomal and EGFR degradation assays

    PMID:39206796

    Open questions at the time
    • Single-lab findings without independent replication
    • Relationship between Rab-GAP function and centriolar localization unclear
  4. 2024 Medium

    Placed TBC1D31 downstream of a defined transcriptional activator in cancer, showing ZSCAN16 drives its expression to sustain HCC malignancy.

    Evidence ChIP-qPCR, dual-luciferase reporter, lentiviral knockdown/overexpression with functional rescue and xenograft models

    PMID:39511655

    Open questions at the time
    • Whether ZSCAN16-driven expression operates through the Rab22A/EGFR axis specifically not resolved
    • Single-lab evidence
  5. 2024 Low

    Associated elevated TBC1D31 with a glycolytic metabolic phenotype in TNBC, broadening its cancer relevance beyond HCC.

    Evidence Transcriptomics/metabolomics correlation and siRNA knockdown with metabolic readouts in TNBC cell lines

    PMID:39231952

    Open questions at the time
    • No mechanistic pathway connecting TBC1D31 to glycolysis established
    • Correlative, single-lab evidence
  6. 2025 High

    Resolved the structural role of TBC1D31/WDR67 at the centriolar A-C linker, showing it physically bridges microtubule triplets and supports centriole architecture and duplication.

    Evidence Ultrastructure expansion microscopy, siRNA/KO depletion, co-localization, and co-depletion epistasis with inner scaffold components

    PMID:40707486

    Open questions at the time
    • Molecular basis of triplet bridging by the CCDC77/WDR67/MIIP complex not defined
    • How the A-C linker role integrates with the praja2/PKA/OFD1 signaling function unknown

Open questions

Synthesis pass · forward-looking unresolved questions
  • It remains unknown how TBC1D31's centriolar structural/ciliogenic functions and its cytoplasmic Rab22A-GAP/EGFR-trafficking role are coordinated within a single protein.
  • No structure-function mapping separating GAP, scaffold, and A-C linker activities
  • No data on whether the two functions are spatially or temporally exclusive

Mechanism profile

Synthesis pass · controlled-vocabulary classification · explore literature graph →
Molecular activity
GO:0005198 structural molecule activity 1 GO:0060090 molecular adaptor activity 1 GO:0098772 molecular function regulator activity 1
Localization
GO:0005815 microtubule organizing center 2 GO:0005929 cilium 1
Pathway
R-HSA-162582 Signal Transduction 2 R-HSA-1852241 Organelle biogenesis and maintenance 1 R-HSA-5653656 Vesicle-mediated transport 1
Partners
CCDC77MIIPOFD1PJA2PRKACARAB22A
Complex memberships
CCDC77/WDR67/MIIP A-C linker complexpraja2/PKA/OFD1 centrosomal complex

Evidence

Reading pass · 6 per-paper findings extracted from the source corpus
Year Finding Method Journal Conf PMIDs
2021 TBC1D31 assembles a novel complex at centrosomes comprising the E3 ubiquitin ligase praja2, protein kinase A (PKA), and OFD1. Upon GPCR-cAMP stimulation, PKA phosphorylates OFD1 at Ser735, promoting OFD1 proteolysis via the praja2-ubiquitin-proteasome system, a pathway essential for primary ciliogenesis. Co-immunoprecipitation, centrosome localization assays, phospho-mutant analysis (non-phosphorylatable OFD1 S735A), in vivo knockdown in Medaka fish The EMBO journal High 33934390
2021 TBC1D31 is essential for primary ciliogenesis; loss of TBC1D31 function impairs cilium biogenesis both in cultured cells and in vivo in Medaka fish, resulting in developmental defects. Loss-of-function (knockdown/depletion) in cell lines and in vivo Medaka fish model with cilium morphology and developmental phenotype readouts The EMBO journal High 33934390
2025 WDR67 (alias TBC1D31) localizes to the A-C linker of centrioles, where it forms a complex with CCDC77 and MIIP connecting adjacent microtubule triplets at the proximal region. Depletion of A-C linker components disrupts microtubule triplet cohesion, causing breakage at the proximal end; co-depletion with inner scaffold components demonstrates their joint role in centriole architecture. The A-C linker also regulates centriole duplication through torus regulation. Ultrastructure expansion microscopy (U-ExM), protein depletion (siRNA/KO), co-localization and complex characterization, epistasis by co-depletion with inner scaffold Nature communications High 40707486
2024 TBC1D31 acts as a Rab GTPase-activating protein (Rab-GAP) that catalyzes GTP hydrolysis for Rab22A, thereby reducing Rab22A-mediated endolysosomal trafficking and degradation of EGFR, leading to sustained EGFR signaling and promoting HCC growth and metastasis. In vitro GAP activity assay, overexpression and knockdown in HCC cell lines and xenograft models, endolysosomal trafficking assays, EGFR degradation assays Advanced science Medium 39206796
2024 ZSCAN16 transcriptionally activates TBC1D31 expression in hepatocellular carcinoma cells, as demonstrated by ChIP-qPCR and dual-luciferase reporter assays. TBC1D31 overexpression rescues the inhibitory effects of ZSCAN16 knockdown on HCC cell proliferation, migration, invasion, and in vivo tumor growth. ChIP-qPCR, dual-luciferase assay, lentiviral knockdown/overexpression, functional rescue experiments, xenograft tumor model Cell division Medium 39511655
2024 Elevated TBC1D31 expression is causally associated with a glycolytic metabolic phenotype in triple-negative breast cancer (TNBC) cell lines, as demonstrated by transcriptomics/metabolomics correlation and functional knockdown experiments. Transcriptomics/metabolomics correlation, siRNA knockdown with metabolic phenotype readout in TNBC cell lines Cell death & disease Low 39231952

Source papers

Stage 0 corpus · 8 papers · ranked by NIH iCite citations
Year Title Journal Citations PMID
2021 The TBC1D31/praja2 complex controls primary ciliogenesis through PKA-directed OFD1 ubiquitylation. The EMBO journal 33 33934390
2025 The A-C linker controls centriole structural integrity and duplication. Nature communications 10 40707486
2017 Purification of glucomannan from salep: Part 2. Structural characterization. Carbohydrate polymers 9 28504162
2024 A susceptibility gene signature for ERBB2-driven mammary tumour development and metastasis in collaborative cross mice. EBioMedicine 8 39067134
2024 Genomic Amplification of TBC1D31 Promotes Hepatocellular Carcinoma Through Reducing the Rab22A-Mediated Endolysosomal Trafficking and Degradation of EGFR. Advanced science (Weinheim, Baden-Wurttemberg, Germany) 8 39206796
2024 TBC1 domain-containing proteins are frequently involved in triple-negative breast cancers in connection with the induction of a glycolytic phenotype. Cell death & disease 4 39231952
2023 A novel homozygous missense variant in TBC1D31 in a consanguineous family with congenital anomalies of the kidney and urinary tract (CAKUT). Clinical genetics 4 37468454
2024 ZSCAN16 expedites hepatocellular carcinoma progression via activating TBC1D31. Cell division 2 39511655

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