Showing DNAAF5 — HEATR2 is a alias.

DNAAF5

Dynein axonemal assembly factor 5 · UniProt Q86Y56

Length: 855 aa
Mass: 93.5 kDa
Annotated: 2026-06-09

8 papers in source corpus 4 papers cited in narrative 4 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

DNAAF5 is a cytoplasmic dynein axonemal assembly factor required for the function of motile cilia (PMID:37104040, PMID:36712068). It promotes the assembly of dynein motor complexes prior to their incorporation into the axoneme, such that its loss reduces both axonemal regulatory and structural proteins and produces severe cilia motor assembly defects; complete loss-of-function is embryonic lethal in mice (PMID:37104040, PMID:36712068). The requirement for DNAAF5 is allele- and tissue-specific: the same missense variant yields divergent cilia function across different multiciliated tissues, indicating tissue-specific molecular requirements for dynein arm assembly (PMID:37104040, PMID:36712068). This role is conserved in vertebrate development, where dnaaf5 is expressed in motile ciliated tissues of zebrafish embryos and its loss produces ciliopathic phenotypes (PMID:42029186). In a non-ciliary context, DNAAF5 acts as a scaffold that directly binds PFKL and recruits the deubiquitinase USP39, forming a ternary complex that stabilizes PFKL by promoting its deubiquitination and thereby enhancing glycolysis in hepatocellular carcinoma cells (PMID:36276075).

Mechanistic history

Synthesis pass · year-by-year structured walk · 4 steps

2022 Medium
Identified a non-ciliary, scaffolding function for DNAAF5, establishing that it can bridge a substrate to a deubiquitinase to control protein stability and metabolic output.

Evidence Co-IP, mass spectrometry, knockout/overexpression cell lines, xenografts, and USP39 knockdown rescue in hepatocellular carcinoma cells

PMID:36276075
Open questions at the time
- Single lab, non-ciliary context may represent a gain-of-function or context-restricted role
- Structural basis of the DNAAF5–PFKL–USP39 ternary complex not resolved
- Relationship between this glycolytic scaffold role and the cilia assembly function unknown
2023 High
Established DNAAF5 as a dynein motor assembly factor essential for motile cilia, defining its in vivo requirement and the proteomic consequences of its loss.

Evidence CRISPR-Cas9 engineered missense and frameshift-null Dnaaf5 alleles in mice, with cilia ultrastructure, proteomics of isolated airway cilia, and transcriptional readouts

PMID:36712068 PMID:37104040
Open questions at the time
- Precise biochemical step in dynein arm preassembly catalyzed or scaffolded by DNAAF5 not defined
- Direct dynein-chain or co-chaperone partners not identified
2023 Medium
Revealed that DNAAF5 dependence is allele- and tissue-specific, explaining how a single variant can produce divergent cilia phenotypes across multiciliated tissues.

Evidence Comparative ultrastructure and proteomic profiling of cilia from multiple multiciliated tissues in Dnaaf5 missense homozygous and compound heterozygous mice

PMID:36712068 PMID:37104040
Open questions at the time
- Molecular basis of tissue-specific dynein arm assembly requirements not identified
- Single-lab allelic series
2025 Medium
Demonstrated evolutionary conservation of the motile cilia role, showing DNAAF5 acts in motile ciliated tissues during vertebrate development.

Evidence In situ hybridization expression mapping and CRISPR crispant phenotyping in zebrafish embryos

PMID:42029186
Open questions at the time
- Single method per finding; crispant rescue not described
- Molecular partners in zebrafish not defined

Open questions

Synthesis pass · forward-looking unresolved questions

How DNAAF5 reconciles its cytoplasmic dynein preassembly role with the non-ciliary glycolytic scaffold function, and the precise biochemical step it performs in dynein arm assembly, remain unresolved.
No structural model of DNAAF5 or its complexes
Direct dynein assembly substrates/co-factors unidentified
Whether scaffolding for deubiquitination is a general DNAAF5 mechanism is unknown

Mechanism profile

Synthesis pass · controlled-vocabulary classification · explore literature graph →

Molecular activity

GO:0060090 molecular adaptor activity 1

Localization

GO:0005929 cilium 2 GO:0005829 cytosol 1

Pathway

R-HSA-1266738 Developmental Biology 1 R-HSA-1852241 Organelle biogenesis and maintenance 1

Partners

PFKL USP39

Evidence

Reading pass · 4 per-paper findings extracted from the source corpus

Year	Finding	Method	Journal	Conf	PMIDs
2023	DNAAF5 functions as a dynein motor assembly factor required for motile cilia function; loss-of-function (null allele homozygosity) is embryonic lethal in mice, and compound heterozygous missense/null animals show severe cilia motor assembly defects with reduced axonemal regulatory and structural proteins detectable by proteomics of isolated airway cilia.	CRISPR-Cas9 genome editing in mice to generate missense and frameshift-null Dnaaf5 alleles; ultrastructure analysis of cilia; proteomic analysis of isolated airway cilia; transcriptional analysis of mouse and human mutant cells	JCI insight	High	36712068 37104040
2023	DNAAF5 allele dosage shows allele-specific and tissue-specific effects on cilia motor assembly: the same missense variant allele produces divergent cilia function across different multiciliated tissues, indicating tissue-specific molecular requirements for dynein arm assembly that depend on DNAAF5.	Comparative ultrastructure analysis and proteomic profiling of cilia from multiple multiciliated tissues in Dnaaf5 missense homozygous and compound heterozygous mice	JCI insight	Medium	36712068 37104040
2022	DNAAF5 acts as a scaffold protein that directly binds PFKL (phosphofructokinase, liver type) and recruits the deubiquitinase USP39, forming a ternary complex that stabilizes PFKL protein by promoting its deubiquitination, thereby enhancing glycolysis in hepatocellular carcinoma cells.	Co-immunoprecipitation, mass spectrometry, transcriptome sequencing, stable cell line overexpression/knockout, in vivo xenograft; USP39 knockdown rescue experiment	Frontiers in oncology	Medium	36276075
2025	dnaaf5 mRNA is expressed in motile ciliated tissues of zebrafish embryos (Kupffer's vesicle, pronephros, floor plate, brain, olfactory placode), and dnaaf5 crispants develop ciliopathic defects, indicating a conserved role in motile cilia biogenesis and function during vertebrate development.	In situ hybridization for spatio-temporal mRNA expression; CRISPR crispant phenotype analysis in zebrafish embryos	The International journal of developmental biology	Medium	42029186

Source papers

Stage 0 corpus · 8 papers · ranked by NIH iCite citations

Year	Title	Journal	Citations	PMID
2023	The effect of Dnaaf5 gene dosage on primary ciliary dyskinesia phenotypes.	JCI insight	17	37104040
2022	DNAAF5 promotes hepatocellular carcinoma malignant progression by recruiting USP39 to improve PFKL protein stability.	Frontiers in oncology	17	36276075
2023	Genome-Wide Meta-Analysis of Cerebrospinal Fluid Biomarkers in Alzheimer's Disease and Parkinson's Disease Cohorts.	Movement disorders : official journal of the Movement Disorder Society	9	37539664
2024	Identification of candidate genes affecting the tibia quality in Nonghua duck.	Poultry science	3	38350390
2023	Genome-wide meta-analysis of CSF biomarkers in Alzheimer's disease and Parkinson's disease cohorts.	medRxiv : the preprint server for health sciences	1	37398091
2025	Comprehensive Proteomics and Machine Learning Analysis to Distinguish Follicular Adenoma and Follicular Thyroid Carcinoma from Indeterminate Thyroid Nodules.	Endocrinology and metabolism (Seoul, Korea)	0	40205804
2025	Dynein axonemal assembly factors (dnaaf) 5 and 9 are expressed in ciliated organs of zebrafish embryos.	The International journal of developmental biology	0	42029186
2023	The effect of Dnaaf5 gene dosage on primary ciliary dyskinesia phenotypes.	bioRxiv : the preprint server for biology	0	36712068

UniProt Q86Y56 ↗

Location Cytoplasm; Dynein axonemal particle

Cytoplasmic protein involved in the delivery of the dynein machinery to the motile cilium. It is required for the assembly of the axonemal dynein inner and outer arms, two structures attached to the peripheral outer doublet A microtubule of the axoneme, that play a crucial role in cilium motility

DepMap portal ↗

Not essential

Human Protein Atlas profile ↗

Subcell. Cytosol Nucleoli Microtubules

RNA spec. Low tissue specificity

AlphaFold structure ↗

pLDDT 92

Domains 1.25.10,1.25.40 1.25.40,1.20.930 1.25.40 1.25.40

OMIM disease links

MIM:614874 CILIARY DYSKINESIA, PRIMARY, 18

MIM:614864 DYNEIN, AXONEMAL, ASSEMBLY FACTOR 5

MIM:244400 CILIARY DYSKINESIA, PRIMARY, 1

Sources data + JSON

JSON record ↗ UniProt ↗ PubMed ↗

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