IARS1

Isoleucine--tRNA ligase, cytoplasmic · UniProt P41252

Length: 1262 aa
Mass: 144.5 kDa
Annotated: 2026-06-10

11 papers in source corpus 6 papers cited in narrative 7 extracted findings

Cross-family judge vs UniProt: tie faithfulness: 3/3 claims corpus-supported (100%)

Mechanistic narrative

Synthesis pass · prose summary of the discoveries below

IARS1 encodes the cytoplasmic isoleucyl-tRNA synthetase, an enzyme whose aminoacylation activity charges tRNA with isoleucine; the catalytic essentiality of this function is established by the V79L variant reducing aminoacylation activity in vitro (PMID:23700453) and by wild-type human IARS1 rescuing growth of ILS-null yeast where the p.Asp249Gly disease variant fails to complement (PMID:40365325). Biallelic loss-of-function mutations cause a multisystem developmental disorder: zebrafish modeling of compound heterozygous variants recapitulates defects in embryonic, neuro-, liver, and muscle development (PMID:35668413). Beyond its canonical synthetase role, loss of IARS1 function drives mitochondrial dysfunction — knockdown in HepG2 cells lowers mitochondrial membrane potential and raises ROS (PMID:37108118), and a hypomorphic V79L knock-in mouse develops hepatic triglyceride accumulation and elevated serum ornithine carbamoyltransferase with reduced mitochondrial NME4 (PMID:37108118).

Mechanistic history

Synthesis pass · year-by-year structured walk · 6 steps

2013 Medium
Establishing whether a disease-associated residue is catalytically important required direct enzymatic testing; the V79L assay showed this residue is needed for the synthetase's aminoacylation activity.

Evidence In vitro aminoacylation assay comparing mutant and wild-type IARS1 protein

PMID:23700453
Open questions at the time
- Single residue tested; does not map the full catalytic or substrate-binding architecture
- In vitro activity not linked to organismal phenotype in this study
2022 Medium
Whether human disease variants are loss-of-function and which tissues they affect was unresolved; zebrafish modeling of compound heterozygous variants showed loss of function recapitulating multi-organ developmental defects.

Evidence Zebrafish embryo loss-of-function modeling of p.L234P and p.R519C with developmental, neuro, liver, and myogenic readouts

PMID:35668413
Open questions at the time
- Does not resolve the molecular mechanism linking synthetase loss to each organ phenotype
- Phenotypes in fish embryos may not map directly to human pathophysiology
2023 Medium
How cytoplasmic synthetase loss produces hepatopathy was unknown; cellular and in vivo work connected IARS1 loss to mitochondrial dysfunction.

Evidence siRNA knockdown in HepG2 cells (membrane potential, ROS) and V79L knock-in mouse (hepatic triglyceride, serum OCT, NME4 proteomics)

PMID:37108118
Open questions at the time
- Causal chain from reduced aminoacylation to mitochondrial membrane potential loss not defined
- Role of decreased NME4 in the phenotype not functionally tested
- Whether mitochondrial defect is secondary to global translational stress unresolved
2025 Medium
Whether the human Asp249Gly variant is truly loss-of-function needed an orthogonal functional test; yeast complementation confirmed it fails to support growth where wild-type rescues.

Evidence Complementation of ILS-null yeast by wild-type versus mutant human IARS1

PMID:40365325
Open questions at the time
- Binary growth readout does not quantify residual catalytic activity
- Yeast context lacks human multisynthetase complex partners
2025 Low
How non-catalytic domain mutations cause disease was unclear; a UNE-L domain variant was shown to destabilize the protein and dysregulate the integrated stress response without altering bulk translation.

Evidence Cell-based expression of mutant vs wild-type with western blot, protein synthesis and proliferation assays, and ISR analysis (preprint)

PMID:bio_10.1101_2025.08.21.671621
Open questions at the time
- Preprint, single lab, not independently confirmed
- Direct link between multisynthetase complex disruption and ISR activation not reconstituted
- Glucose-dependent exacerbation mechanism undefined
2026 Low
Whether IARS1 deficiency drives an immune/clearance phenotype was open; patient PBMC analysis correlated biallelic mutations with monocyte/macrophage dysfunction.

Evidence scRNA-seq of patient PBMCs, BALF staining, western blot, and electron microscopy

PMID:42237414
Open questions at the time
- Observational and correlative; no functional rescue or mechanistic reconstitution
- Intrinsic vs systemic origin of the monocyte defect not established
- Link to synthetase catalytic loss not demonstrated

Open questions

Synthesis pass · forward-looking unresolved questions

The mechanistic bridge between reduced isoleucine aminoacylation, multisynthetase complex integrity, integrated stress response activation, and the tissue-specific phenotypes (liver, mitochondria, monocytes, neurodevelopment) remains undefined.
No structural model of IARS1 catalytic or UNE-L domains in the corpus
Whether mitochondrial and immune phenotypes are downstream of the same translational defect unknown
Quantitative genotype-to-residual-activity-to-severity relationship not mapped

Mechanism profile

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

Molecular activity

GO:0140098 catalytic activity, acting on RNA 2 GO:0003723 RNA binding 1 GO:0016874 ligase activity 1

Localization

GO:0005829 cytosol 1

Pathway

R-HSA-392499 Metabolism of proteins 2

Complex memberships

aminoacyl-tRNA multisynthetase complex

Evidence

Reading pass · 7 per-paper findings extracted from the source corpus

Year	Finding	Method	Journal	Conf	PMIDs
2013	The IARS1 p.Val79Leu (V79L) missense mutation decreases aminoacylation (isoleucyl-tRNA synthetase) activity, establishing that this residue is functionally critical for catalytic function.	In vitro aminoacylation activity assay of mutant vs. wild-type IARS1 protein	PloS one	Medium	23700453
2023	IARS1 knockdown (siRNA) in HepG2 cells decreases mitochondrial membrane potential and increases reactive oxygen species, linking loss of cytoplasmic isoleucyl-tRNA synthetase function to mitochondrial dysfunction and hepatopathy.	siRNA knockdown in HepG2 cells with measurement of mitochondrial membrane potential and ROS	International journal of molecular sciences	Medium	37108118
2023	IARS1V79L mutant mice show elevated hepatic triglyceride and serum ornithine carbamoyltransferase levels compared to wild-type, indicating the V79L mutation causes mitochondrial hepatopathy in vivo; proteomic analysis revealed decreased levels of mitochondrial nucleoside diphosphate kinase NME4.	Hypomorphic knock-in mouse model (V79L), biochemical assays (hepatic triglyceride, serum OCT), proteomics	International journal of molecular sciences	Medium	37108118
2025	The human IARS1 p.Asp249Gly disease variant causes loss of function as demonstrated by failure to complement yeast ILS (isoleucyl-tRNA synthetase) deletion, while wild-type human IARS1 supports robust yeast growth in the absence of yeast ILS.	Yeast complementation assay (functional rescue of ILS-null yeast by wild-type vs. mutant human IARS1)	JIMD reports	Medium	40365325
2025	A disease-causing mutation in the UNE-L domain of IARS1 (which mediates interactions within the multisynthetase complex) leads to severely reduced protein levels compared to wild-type, without affecting bulk protein synthesis or cell proliferation, but alters integrated stress response signaling — an effect exacerbated in low-glucose conditions.	Cell-based expression of mutant vs. wild-type IARS1 with western blot (protein levels), protein synthesis assay, cell proliferation assay, integrated stress response pathway analysis	bioRxivpreprint	Low	bio_10.1101_2025.08.21.671621
2022	Compound heterozygous IARS1 mutations (p.L234P and p.R519C) cause loss of gene function as modeled in zebrafish embryos, recapitulating defects in embryo development, neurodevelopment, liver development, and myogenesis.	Zebrafish embryo loss-of-function modeling of IARS1 variants with phenotypic readouts (development, neurodevelopment, liver, myogenesis)	BMC pediatrics	Medium	35668413
2026	Biallelic IARS1 mutations are associated with monocyte/macrophage dysfunction: single-cell RNA sequencing of PBMCs from affected patients showed depletion of CD14+CD16+ intermediate monocytes and transcriptional downregulation of phagosome/lysosome pathways in CD14+ classical monocytes, suggesting an intrinsic defect contributing to surfactant clearance dysfunction in childhood interstitial lung disease/pulmonary alveolar proteinosis.	scRNA-seq of PBMCs, PAS and Oil-Red O staining of BALF, western blotting, transmission electron microscopy	Human genomics	Low	42237414

Source papers

Stage 0 corpus · 11 papers · ranked by NIH iCite citations

Year	Title	Journal	Citations	PMID
2018	Circular RNA IARS (circ-IARS) secreted by pancreatic cancer cells and located within exosomes regulates endothelial monolayer permeability to promote tumor metastasis.	Journal of experimental & clinical cancer research : CR	308	30064461
2013	Mapping and exome sequencing identifies a mutation in the IARS gene as the cause of hereditary perinatal weak calf syndrome.	PloS one	31	23700453
2016	IARS mutation causes prenatal death in Japanese Black cattle.	Animal science journal = Nihon chikusan Gakkaiho	11	27229878
2022	Compound heterozygous variations in IARS1 cause recurrent liver failure and growth retardation in a Chinese patient: a case report.	BMC pediatrics	9	35668413
2023	Novel IARS1 variants cause syndromic developmental disorder with epilepsy in a Chinese patient and the literature review.	Molecular genetics & genomic medicine	7	38014478
2023	Molecular and Pathological Analyses of IARS1-Deficient Mice: An IARS Disorder Model.	International journal of molecular sciences	6	37108118
2023	circ-IARS depletion inhibits the progression of non-small-cell lung cancer by circ-IARS/miR-1252-5p/HDGF ceRNA pathway.	Open medicine (Warsaw, Poland)	3	36694627
2024	Circular RNA IARS modulates the progression and ferroptosis of osteosarcoma via sponging miR-188-5p from RAB14.	Neoplasma	2	38958715
2025	Atypical Presentation of IARS1-Related Disorder: Expanding the Phenotype and Genotype.	JIMD reports	1	40365325
2020	Carrier rate of the c.235G>C mutation in the bovine isoleucyl-tRNA synthetase (IARS) gene of Japanese Black cows at Kagoshima prefecture, Japan, and analysis of the metabolic profiling and reproductive performance of heterozygous cows.	The Journal of veterinary medical science	1	33298632
2026	Linking childhood interstitial lung disease to IARS-related disorder: clinical and preliminary functional studies in four new cases.	Human genomics	0	42237414

UniProt P41252 ↗

Location Cytoplasm; Cytoplasm, cytosol

Catalyzes the specific attachment of an amino acid to its cognate tRNA in a 2 step reaction: the amino acid (AA) is first activated by ATP to form AA-AMP and then transferred to the acceptor end of the tRNA

DepMap portal ↗

Common Essential

Dependent 1208/1208 lines

OpenCell profile ↗

IP-MS CAPRIN1 CAPZB CTCF DRG1 G3BP2 NCAPH

Human Protein Atlas profile ↗

Subcell. Nucleoplasm Cytosol

RNA spec. Low tissue specificity

AlphaFold structure ↗

pLDDT 89

Domains 3.40.50.620 3.90.740.10 1.10.730.10 3.30.1330,3.30.2320 3.30.720,3.30.720 3.10.20.90

OMIM disease links

MIM:617093 GROWTH RETARDATION, IMPAIRED INTELLECTUAL DEVELOPMENT, HYPOTONIA, AND HEPATOPATHY

MIM:600709 ISOLEUCYL-tRNA SYNTHETASE 1

Sources data + JSON

JSON record ↗ UniProt ↗ PubMed ↗

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