Affinage

Showing COA3COX25 is a alias.

COA3

Cytochrome c oxidase assembly factor 3 homolog, mitochondrial · UniProt Q9Y2R0

Length
106 aa
Mass
11.7 kDa
Annotated
2026-06-09
28 papers in source corpus 11 papers cited in narrative 11 extracted findings
Cross-family judge vs UniProt: Affinage preferred faithfulness: 6/6 claims corpus-supported (100%)

Mechanistic narrative

Synthesis pass · prose summary of the discoveries below

COA3 is a small, intrinsically disordered intrinsic protein of the inner mitochondrial membrane that functions as an early assembly factor for cytochrome c oxidase (complex IV), coupling synthesis of the mitochondrially encoded COX1 subunit to its incorporation into the holoenzyme (PMID:20876281, PMID:23362268, PMID:27791355). It assembles with newly synthesized COX1 and the assembly factor COX14 into an early intermediate and co-translationally stabilizes COX1, with loss of COA3 reducing the stability and steady-state level of nascent COX1 (PMID:23362268, PMID:25604084). COA3 and COX14 are mutually interdependent for stability—neither protein is detectable in cells lacking the other—and together they gate COX1 maturation before recruitment of the COX4 and COX5a subunits (PMID:25604084, PMID:28082314). In yeast, COA3/Cox25 acts with Cox14 and Coa1 to recruit the translational activator Mss51 into a latent, translation-resting state, thereby providing negative feedback on COX1 synthesis; the same intermediate is further stabilized in humans by CMC1, which controls turnover rather than the rate of COX1 synthesis (PMID:20876281, PMID:21068384, PMID:28082314). The factor is essential for complex IV assembly across species, and in humans compound heterozygous COA3 mutations cause isolated complex IV deficiency (PMID:22610097, PMID:25604084). Deficiency provokes ROS-mediated release of mitochondrial RNA and sterile inflammation, paralleling the COX14 phenotype (PMID:39134548).

Mechanistic history

Synthesis pass · year-by-year structured walk · 10 steps
  1. 2010 High

    Established that COA3 is a core component of the earliest COX1-containing assembly intermediates and, with Cox14, governs a translational feedback loop that throttles COX1 synthesis via Mss51 sequestration.

    Evidence Genetic deletion, reciprocal Co-IP, sucrose gradient sedimentation and pulse-chase translation labeling in yeast

    PMID:20876281 PMID:21068384

    Open questions at the time
    • Whether the human ortholog reproduces the Mss51-based translational feedback was not addressed
    • Topology and biophysical basis of complex formation not resolved in these studies
  2. 2012 High

    Showed the requirement for COA3 in complex IV assembly is conserved in a metazoan, with specificity for complex IV among OXPHOS complexes.

    Evidence Two independent Drosophila knockout alleles with enzymatic assays, BN-PAGE and transgenic rescue

    PMID:22610097

    Open questions at the time
    • Did not define the molecular interaction partners in flies
    • Did not distinguish translational from post-translational COX1 effects
  3. 2013 High

    Demonstrated that the human protein co-translationally stabilizes nascent COX1 and bridges the mitochondrial translation machinery to COX structural subunits.

    Evidence siRNA knockdown, pulse-chase mitochondrial translation labeling, Co-IP and BN-PAGE in human cells

    PMID:23362268

    Open questions at the time
    • Did not resolve which translation-machinery components are directly contacted
    • Stoichiometry of the COX1-bound intermediate not defined
  4. 2015 High

    Linked COA3 loss-of-function directly to human disease and established mutual stability dependence with COX14.

    Evidence Whole exome sequencing, patient fibroblast biochemistry, pulse-chase labeling and retroviral complementation rescue

    PMID:25604084

    Open questions at the time
    • Structural basis of the COA3-COX14 interdependence unresolved
    • Genotype-phenotype relationships across additional patients not established
  5. 2017 High

    Refined the human intermediate by adding CMC1 and reframed COA3/COX14 function as regulating COX1 turnover rather than synthesis rate in human cells.

    Evidence TALEN knockout of CMC1 in HEK293T, Co-IP, BN-PAGE and pulse-chase labeling

    PMID:28082314

    Open questions at the time
    • Reconciliation of the human turnover model with the yeast translational-feedback model not fully resolved
    • Order of CMC1 vs COA3 recruitment to COX1 not defined
  6. 2017 Medium

    Placed COA3 in functional coupling with a mitoribosomal component (MrpL35) that coordinates COX1 synthesis with assembly.

    Evidence Genetic epistasis, respiratory growth assays and Co-IP in yeast

    PMID:28931599

    Open questions at the time
    • COA3 involvement inferred from genetic interaction, not direct biochemical reconstitution
    • Direct COA3-mitoribosome contact not demonstrated
  7. 2016 Medium

    Identified a COX1 synthesis pathway (Pet54) acting upstream of or in parallel to the COA3/COX14-Mss51 feedback loop, delimiting the regulatory scope of COA3.

    Evidence Genetic double-deletion analysis, pulse-chase labeling and RNA Co-IP in yeast

    PMID:26929411

    Open questions at the time
    • Mechanistic relationship between Pet54 and the COA3 complex not biochemically defined
    • Human relevance not tested
  8. 2016 Medium

    Characterized the human protein as intrinsically disordered and conformationally flexible, providing a biophysical rationale for its multivalent assembly-factor role.

    Evidence Fluorescence spectroscopy, circular dichroism, analytical ultracentrifugation, light scattering and computational modeling

    PMID:27791355

    Open questions at the time
    • No mutagenesis linking disorder to assembly function
    • Conformation within the native membrane complex not determined
  9. 2019 Low

    Reported a mitochondrial physical interaction between COA3 and EGFL9 associated with metabolic reprogramming.

    Evidence Co-IP, confocal co-localization, COX activity and metabolic flux assays

    PMID:31695034

    Open questions at the time
    • Single Co-IP without reciprocal validation or COA3 perturbation
    • Causal role of COA3 in the Warburg-like phenotype not tested
  10. 2024 Medium

    Demonstrated in vivo consequences of COA3 deficiency, linking complex IV failure to ROS-driven mitochondrial RNA release and sterile inflammation.

    Evidence COA3Y72C knock-in mouse with comparative phenotyping against a COX14 mutant, complex IV activity assays and cytosolic RNA sensing analysis

    PMID:39134548

    Open questions at the time
    • COA3 phenotype described as milder/secondary to COX14, leaving COA3-specific contribution incompletely separated
    • Tissue specificity of the inflammatory response not fully mapped

Open questions

Synthesis pass · forward-looking unresolved questions
  • It remains unresolved how the yeast Mss51 translational-feedback model and the human turnover-based model are mechanistically reconciled, and what structural arrangement COA3 adopts within the COX1-COA3-COX14-CMC1 intermediate.
  • No high-resolution structure of the early assembly intermediate
  • Direct human equivalent of Mss51-style regulation not established
  • Recruitment order and binding interfaces among COA3, COX14, CMC1 and COX1 unknown

Mechanism profile

Synthesis pass · controlled-vocabulary classification · explore literature graph →
Molecular activity
GO:0098772 molecular function regulator activity 2 GO:0140096 catalytic activity, acting on a protein 2
Pathway
R-HSA-1852241 Organelle biogenesis and maintenance 3 R-HSA-1643685 Disease 1
Partners
CMC1COA1COX1COX14EGFL9MRPL35MSS51SHY1
Complex memberships
MITRACearly complex IV (COX1-COA3-COX14-CMC1) assembly intermediate

Evidence

Reading pass · 11 per-paper findings extracted from the source corpus
Year Finding Method Journal Conf PMIDs
2010 Yeast Coa3 (Yjl062w-A) forms early assembly intermediates with newly synthesized Cox1 and Cox14, and is required for Mss51 association with these complexes. Coa3 and Cox14 promote formation of the 'latent' (translational resting) state of Mss51, thereby down-regulating COX1 translation. Loss of Coa3 traps Mss51 in the 'committed' (translation-effective) state and promotes Cox1 synthesis. Coa1 binding to sequestered Mss51 in complex with Cox14, Coa3, and Cox1 is essential for full inactivation. Genetic deletion, co-immunoprecipitation, sucrose gradient sedimentation, pulse-chase labeling of mitochondrial translation products The Journal of cell biology High 20876281
2010 Yeast Cox25 (the S. cerevisiae ortholog of COA3) is an inner mitochondrial membrane intrinsic protein with a hydrophilic C-terminus protruding into the matrix. It is an essential component of high-molecular-weight complexes containing newly synthesized Cox1, Ssc1, Mss51, and Cox14. A cox25 null mutation does not affect Cox1 synthesis (similar to cox14 null). Cox25 also interacts with Shy1 and Cox5 in a Mss51-free complex, suggesting it continues to associate with Cox14 and Cox1 after Ssc1-Mss51 release to facilitate formation of multisubunit COX assembly intermediates. Genetic deletion, co-immunoprecipitation, sucrose gradient fractionation, pulse-chase mitochondrial translation labeling, submitochondrial localization (carbonate extraction, protease protection) The Journal of biological chemistry High 21068384
2013 Human hCOA3 (CCDC56/MITRAC12) is a mitochondrial transmembrane protein that stabilizes newly synthesized COX1 co-translationally and promotes its assembly with COX partner subunits. hCOA3-silenced cells display decreased stability of newly synthesized COX1 and impaired holoenzyme assembly. hCOA3 physically interacts with both the mitochondrial translation machinery and COX structural subunits. siRNA knockdown, pulse-chase mitochondrial translation labeling, co-immunoprecipitation, BN-PAGE, immunoblotting The Journal of biological chemistry High 23362268
2012 Drosophila CCDC56 (ortholog of COA3) localizes to mitochondria and is essential for cytochrome c oxidase (COX/complex IV) assembly and activity. Knockout larvae show a significant decrease in fully assembled COX and its activity, while other OXPHOS complexes are unaffected or increased. The lethal developmental phenotype is partially rescued by reintroduction of a wild-type UAS-ccdc56 transgene. Genetic knockout (two alleles), enzymatic activity assays, BN-PAGE, transgenic rescue, subcellular fractionation/localization The Journal of biological chemistry High 22610097
2015 Human COA3 mutations (compound heterozygous c.199dupC, c.215A>G) cause isolated COX (complex IV) deficiency with decreased COX1 synthesis. Retroviral expression of wild-type COA3 fully rescued COX assembly and mitochondrial translation defects and increased COX1 steady-state levels, demonstrating COA3's role in stabilizing COX1. COA3 and COX14 are mutually interdependent: COX14 is undetectable in COA3-deficient fibroblasts and COA3 is undetectable in COX14-deficient fibroblasts. BN-PAGE, pulse-chase mitochondrial translation labeling, whole exome sequencing, retroviral complementation, immunoblotting of patient fibroblasts Journal of medical genetics High 25604084
2017 Human CMC1 forms an early CIV assembly intermediate with COX1, COA3, and COX14. CMC1 stabilizes a COX1-COA3-COX14 complex prior to incorporation of COX4 and COX5a subunits. CMC1 acts independently of COX10, COX11, SURF1 (metallation factors) and MITRAC7 (late stability factor). Importantly, whereas COX14 and COA3 had been proposed to affect COX1 mRNA translation, CMC1 (and by inference this complex) regulates turnover of newly synthesized COX1 without affecting the rate of COX1 synthesis. TALEN-mediated CMC1 knockout in HEK293T cells, co-immunoprecipitation, BN-PAGE, pulse-chase mitochondrial translation labeling, immunoblotting EMBO reports High 28082314
2017 Yeast MrpL35, a mitospecific ribosomal component, plays a key role in coordinating Cox1 synthesis with COX assembly in a manner that involves Cox14 and Coa3 proteins. mrpL35 mutants have a COX assembly defect without a global mitochondrial translation inhibition, placing Coa3 downstream of or interacting with the mitoribosome in COX1 synthesis-assembly coupling. Genetic epistasis, respiratory growth assays, mitochondrial protein synthesis analysis, co-immunoprecipitation Molecular biology of the cell Medium 28931599
2016 Pet54, a yeast COX3 translational activator, has a novel role in Cox1 synthesis that is independent of the Coa3/Cox14-mediated assembly feedback regulatory loop. Double deletion of coa3 (or cox14) in a pet54Δ background did not recover Cox1 synthesis (unlike what occurs in other assembly mutants), indicating that Pet54 acts upstream or in parallel to the Coa3-mediated Mss51 sequestration mechanism. Genetic double-deletion analysis, pulse-chase mitochondrial translation labeling, co-immunoprecipitation, RNA co-immunoprecipitation The Journal of biological chemistry Medium 26929411
2016 Human hCOA3 (MITRAC12/CCDC56) is an oligomeric, highly flexible protein in solution. It forms aggregates of different molecular masses in aqueous solution, has a partially solvent-shielded tryptophan and a relatively high but non-hydrogen-bonded secondary structure content. In the presence of detergents it shows a slightly higher content of nonrigid helical structure. The protein is predicted to be intrinsically disordered, and its conformational flexibility is proposed to be important for protein-protein interactions during COX assembly. Fluorescence spectroscopy, circular dichroism, hydrodynamic techniques (analytical ultracentrifugation, dynamic light scattering), computational modeling of primary structure Biochemistry Medium 27791355
2024 A COA3Y72C mouse model displays a mild inflammatory phenotype similar to but less severe than COX14 mutant mice, which show severe liver inflammation linked to mitochondrial RNA release into the cytosol (sensed by the RIG-I pathway) triggered by increased ROS production from complex IV deficiency. This places COA3 as cooperating with COX14 in early COX1 biogenesis, with deficiency causing ROS-mediated mitochondrial RNA release and sterile inflammation. Mouse knock-in model (COA3Y72C), comparative phenotyping with COX14M19I mouse, immunoblotting, complex IV activity assays, cytosolic RNA sensing pathway analysis Nature communications Medium 39134548
2019 Human COA3 physically interacts with EGFL9 within mitochondria. EGFL9 overexpression regulates COX activity and modulates cell metabolism toward a Warburg-like phenotype, and this effect is associated with the EGFL9-COA3 interaction. Co-immunoprecipitation, confocal co-localization, COX activity assay, metabolic flux analysis Nature communications Low 31695034

Source papers

Stage 0 corpus · 28 papers · ranked by NIH iCite citations
Year Title Journal Citations PMID
2010 Coa3 and Cox14 are essential for negative feedback regulation of COX1 translation in mitochondria. The Journal of cell biology 104 20876281
2010 Cox25 teams up with Mss51, Ssc1, and Cox14 to regulate mitochondrial cytochrome c oxidase subunit 1 expression and assembly in Saccharomyces cerevisiae. The Journal of biological chemistry 68 21068384
2017 A CMC1-knockout reveals translation-independent control of human mitochondrial complex IV biogenesis. EMBO reports 64 28082314
2015 Mutations in COA3 cause isolated complex IV deficiency associated with neuropathy, exercise intolerance, obesity, and short stature. Journal of medical genetics 51 25604084
2013 hCOA3 stabilizes cytochrome c oxidase 1 (COX1) and promotes cytochrome c oxidase assembly in human mitochondria. The Journal of biological chemistry 43 23362268
2019 EGFL9 promotes breast cancer metastasis by inducing cMET activation and metabolic reprogramming. Nature communications 40 31695034
2017 MrpL35, a mitospecific component of mitoribosomes, plays a key role in cytochrome c oxidase assembly. Molecular biology of the cell 32 28931599
2004 FLASH interacts with p160 coactivator subtypes and differentially suppresses transcriptional activity of steroid hormone receptors. The Journal of steroid biochemistry and molecular biology 26 15698540
2021 Bi-allelic loss of function variants in COX20 gene cause autosomal recessive sensory neuronopathy. Brain : a journal of neurology 25 33751098
2012 Coiled coil domain-containing protein 56 (CCDC56) is a novel mitochondrial protein essential for cytochrome c oxidase function. The Journal of biological chemistry 24 22610097
2024 Defective mitochondrial COX1 translation due to loss of COX14 function triggers ROS-induced inflammation in mouse liver. Nature communications 17 39134548
2016 A Novel Function of Pet54 in Regulation of Cox1 Synthesis in Saccharomyces cerevisiae Mitochondria. The Journal of biological chemistry 17 26929411
2022 COA3 overexpression promotes non-small cell lung cancer metastasis by reprogramming glucose metabolism. American journal of cancer research 12 36119836
2021 Comparative Proteomics of Rat Olfactory Bulb Reveal Insights into Susceptibility and Resiliency to Chronic-stress-induced Depression or Anxiety. Neuroscience 9 34425157
1987 Cloning of rat brain succinyl-CoA:3-oxoacid CoA-transferase cDNA. Regulation of the mRNA in different rat tissues and during brain development. The Biochemical journal 9 2893604
2023 Integrative genomics analysis highlights functionally relevant genes for equine behaviour. Animal genetics 7 36971191
2020 9-cis-UAB30, a novel rexinoid agonist, decreases tumorigenicity and cancer cell stemness of human neuroblastoma patient-derived xenografts. Translational oncology 7 33010553
2016 Application of citrate as a tricarboxylic acid (TCA) cycle intermediate, prevents diabetic-induced heart damages in mice. Iranian journal of basic medical sciences 5 27096063
2016 Human COA3 Is an Oligomeric Highly Flexible Protein in Solution. Biochemistry 4 27791355
2011 Low dose aspirin prevents duodenoesophageal reflux induced mucosal changes in wistar rat esophagus by MAP kinase mediated pathways. International journal of surgery (London, England) 4 22197650
2011 Harvest-inducibility of the promoter of alfalfa S-adenosyl-L-methionine: trans-caffeoyl-CoA3-O-methyltransferase gene. Molecular biology reports 3 21667113
2019 Coagulase gene polymorphisms of Staphylococcus aureus isolates from patients at Kosti Teaching Hospital, Sudan. Access microbiology 2 32974518
2023 N6-methyladenosine methylation regulatory pattern of pulmonary lymphoepithelioma-like carcinoma based on exosomal transcriptome analysis. Molecular carcinogenesis 1 37589421
2025 Genetic prediction of the relationship between mitochondrial proteins and diabetic polyneuropathy risk: a Mendelian randomization study. Endocrine research 0 40920026
2025 Transcriptome reveals differential expression of flavor and color in closely related strains of tomato (Solanum lycopersicum). PeerJ 0 41081095
2024 Molecular characterization of human HSPCs with different cell fates in vivo using single-cell transcriptome analysis and lentiviral barcoding technology. Clinical and translational medicine 0 39538416
2024 Unraveling the Complexity of Chikungunya Virus Infection Immunological and Genetic Insights in Acute and Chronic Patients. Genes 0 39596565
2017 Gene Regulation Network Based Analysis Associated with TGF-βeta Stimulation in Lung Adenocarcinoma Cells. Iranian journal of biotechnology 0 28959347

Missed literature

Know a paper Affinage missed for COA3? Flag it for the maintainers and the community.

No submissions yet.