MARS2 — Mitochondrial Arginyl-tRNA Synthetase 2
<div class="infobox infobox-gene">
<table>
<tr><th colspan="2" style="background:#e8f4ea;">MARS2</th></tr>
<tr><td><b>Gene Symbol</b></td><td>MARS2</td></tr>
<tr><td><b>Full Name</b></td><td>Mitochondrial Arginyl-tRNA Synthetase 2</td></tr>
<tr><td><b>Chromosomal Location</b></td><td>2q33.1</td></tr>
<tr><td><b>NCBI Gene ID</b></td><td>[92935](https://www.ncbi.nlm.nih.gov/gene/92935)</td></tr>
<tr><td><b>OMIM</b></td><td>[609446](https://www.omim.org/entry/609446)</td></tr>
<tr><td><b>Ensembl ID</b></td><td>ENSG00000135953</td></tr>
<tr><td><b>UniProt ID</b></td><td>[Q9N3W4](https://www.uniprot.org/uniprot/Q9N3W4)</td></tr>
<tr><td><b>Associated Diseases</b></td><td>Spastic Paraplegia (SPG74), [ALS](/diseases/amyotrophic-lateral-sclerosis), [Parkinson's Disease](/diseases/parkinsons-disease), Mitochondrial Disorders</td></tr>
</table>
</div>
Overview
MARS2 (Mitochondrial Arginyl-tRNA Synthetase 2) encodes a mitochondrial aminoacyl-tRNA synthetase (mtARS) that specifically charges arginine to its cognate mitochondrial tRNA. Mitochondrial aminoacyl-tRNA synthetases are essential enzymes that catalyze the attachment of amino acids to their respective tRNA molecules, a critical step in mitochondrial protein synthesis. These enzymes are distinct from their cytosolic counterparts and are encoded by nuclear genes but function within the mitochondrial matrix. MARS2 is one of several mtARS genes linked to neurodegenerative diseases, including hereditary spastic paraplegia (HSP) and amyotrophic lateral sclerosis (ALS). Mutations in MARS2 cause autosomal recessive hereditary spastic paraplegia type 74 (SPG74), characterized by progressive lower limb spasticity and mitochondrial dysfunction. The enzyme's role in maintaining mitochondrial translation makes it critical for neuronal survival, particularly in long projection neurons that are affected in HSP and ALS[@sissler2017][@antonellis2019].
Summary
MARS2 encodes mitochondrial arginyl-tRNA synthetase 2, a nuclear-encoded enzyme that functions in the mitochondrial matrix to charge arginine to mitochondrial tRNA. This enzymatic function is essential for the translation of the 13 oxidative phosphorylation (OXPHOS) proteins encoded by mitochondrial DNA. MARS2 mutations cause autosomal recessive hereditary spastic paraplegia type 74 (SPG74), presenting with progressive spasticity and gait disturbance. The disease mechanism involves impaired mitochondrial translation leading to OXPHOS deficiency, reduced ATP production, and increased susceptibility to oxidative stress. Given the high energy demands of neurons, particularly long axonal projection neurons, mitochondrial translation defects have profound consequences for neuronal viability. MARS2 represents one of several mtARS genes implicated in neurodegeneration, highlighting the importance of mitochondrial protein synthesis for neuronal health[@beyer2019][@bayat2017].
Normal Function
Enzymatic Activity
MARS2 catalyzes the aminoacylation reaction:
L-arginine + tRNA(Arg) + ATP → Arg-tRNA(Arg) + AMP + PPi
This reaction occurs in the mitochondrial matrix and is essential for mitochondrial translation.
Protein Structure
Human MARS2 protein properties:
- Length: Approximately 577 amino acids
- Molecular weight: ~65 kDa
- Domains: Contains the catalytic domain typical of class I aminoacyl-tRNA synthetases
- Mitochondrial targeting: N-terminal mitochondrial targeting peptide (MTS)
Mitochondrial Translation
MARS2 functions in mitochondrial translation:
tRNA aminoacylation: Specifically charges mitochondrial tRNA(Arg) with arginine
Codon-anticodon matching: Recognizes AGA and AGG arginine codons in mitochondrial DNA
Ribosome function: Provides correctly charged tRNAs for translation of mtDNA-encoded proteinsDisease Associations
Hereditary Spastic Paraplegia Type 74 (SPG74)
MARS2 mutations cause autosomal recessive HSP:
Clinical features: Progressive spasticity of lower limbs, gait disturbance, intellectual disability in some cases
Genetics: Biallelic loss-of-function mutations (nonsense, frameshift, splice-site)
Pathogenesis: Impaired mitochondrial translation leads to OXPHOS deficiency
Neuronal vulnerability: Long corticospinal tract neurons are particularly affected[@eskier2018]Amyotrophic Lateral Sclerosis (ALS)
MARS2 is implicated in ALS:
Mitochondrial dysfunction: Common feature in ALS motor neurons
OXPHOS defects: Reduced complex I and IV activity in patient tissues
Energy deficit: Reduced ATP production compromises motor neuron survival
Oxidative stress: Impaired mitochondria produce increased ROSParkinson's Disease
Mitochondrial translation defects in PD:
Dopaminergic neuron vulnerability: High energy demands make them susceptible
Complex I deficiency: Related to impaired mitochondrial translation
PINK1/Parkin connection: Links to mitochondrial quality controlExpression Pattern
Tissue Distribution
MARS2 is expressed in tissues with high mitochondrial energy demands:
- Brain: Cortex, hippocampus, basal ganglia, spinal cord
- Heart: High expression in cardiac muscle
- Skeletal muscle: High expression in muscle fibers
- Liver: Substantial expression in hepatocytes
- Kidney: Renal tubular cells
Cellular Expression
In the nervous system:
- Neurons: High expression in pyramidal neurons and motor neurons
- Astrocytes: Moderate expression
- Oligodendrocytes: Important for myelin production
- Microglia: Lower expression
Interaction Network
| Partner | Relationship | Function |
|---------|--------------|----------|
| Mitochondrial ribosome | Component | Site of mitochondrial translation |
| mtDNA-encoded proteins | Product | OXPHOS complex subunits |
| Mitochondrial tRNA(Arg) | Substrate | Substrate for aminoacylation |
| ATP | Energy source | Required for aminoacylation |
| Other mtARS enzymes | Partner | Coordinated mitochondrial translation |
Therapeutic Approaches
Small Molecule Strategies
Mitochondrial enhancers: Improve mitochondrial function despite translation defects
Antioxidants: Combat increased oxidative stress
Energy supplements: Support cellular energy levelsGene Therapy
- Viral vector delivery of wild-type MARS2
- CRISPR-based correction of pathogenic variants
Supportive Care
- Physical therapy for spasticity
- Occupational therapy
- Assistive devices for mobility
Animal Models
Zebrafish Models
Zebrafish studies show:
- Morpholino knockdown causes motor defects
- Mitochondrial dysfunction in neural tissues
- Axonal pathfinding abnormalities
Mouse Models
- Mars2 knockout: Embryonic or early postnatal lethal
- Conditional knockouts: Tissue-specific deletion reveals neuronal functions
Molecular Mechanisms
Mitochondrial Translation Defects
MARS2 mutations impair mitochondrial translation through several mechanisms[@martin2019]:
Reduced aminoacylation: Loss of MARS2 activity reduces charged tRNA(Arg) levels
Ribosome stalling: Uncharged tRNA causes ribosome pausing
Incomplete protein synthesis: Truncated OXPHOS proteins are produced
Assembly defects: Incomplete proteins cannot form functional complexesOXPHOS Dysfunction
The resulting OXPHOS deficiency has multiple consequences:
- Complex I deficiency: Most commonly affected
- Complex III and IV: Secondary effects
- ATP depletion: Insufficient energy for cellular functions
- ROS overproduction: Electron leak from damaged complexes
Neuronal Vulnerability
Why are neurons particularly susceptible[@wallace2018]:
High energy demand: Neurons require continuous ATP for ion pumping
Limited glycolytic capacity: Cannot compensate for mitochondrial failure
Axonal length: Long axons require extensive mitochondrial distribution
Calcium handling: Mitochondria buffer calcium; dysfunction leads to excitotoxicityMechanism Diagram
Mermaid diagram (expand to render)
Genetic Basis
SPG74 Mutations
MARS2 mutations causing hereditary spastic paraplegia[@eskier2018]:
| Mutation Type | Frequency | Effect |
|--------------|-----------|--------|
| Nonsense | Common | Truncated protein |
| Frameshift | Common | Premature stop |
| Splice-site | Less common | Exon skipping |
| Missense | Rare | Partial loss |
Genotype-Phenotype Correlation
- Biallelic null mutations → severe SPG74
- Missense variants → variable presentation
- Compound heterozygosity → intermediate severity
Clinical Features
Hereditary Spastic Paraplegia Type 74
Core Features:
- Progressive lower limb spasticity
- Gait disturbance
- Lower limb weakness
- Hyperreflexia
Additional Features (variable):
- Intellectual disability
- Peripheral neuropathy
- Optic atrophy
- Seizures (rare)
Age of Onset
- Childhood to early adulthood
- Typically before age 20
- Progressive course over decades
Diagnostic Approach
Biochemical Testing
OXPHOS enzyme activities: Reduced complex I/IV in muscle
Lactate: Elevated in plasma and CSF
Pyruvate: Often elevated
Fibroblast studies: Patient-derived cells show defectsGenetic Testing
Targeted panels: Include MARS2 and other mtARS genes
Whole exome sequencing: Identify pathogenic variants
Sanger confirmation: Validate variantsDifferential Diagnosis
- Other forms of HSP (SPG4, SPG5, etc.)
- Primary lateral sclerosis
- Hereditary ataxias
- Mitochondrial disorders
Therapeutic Strategies
Current Approaches
Symptomatic:
- Spasticity management (baclofen, tizanidine)
- Physical therapy
- Orthopedic interventions
- Assistive devices
Metabolic Support:
- CoQ10 supplementation
- Lipoic acid
- Vitamin supplementation
Investigational Therapies
Mitochondrial Modulation:
- Small molecules enhancing mitochondrial function
- Antioxidants targeting mitochondrial ROS
- ATP supplementation strategies
Gene Therapy Approaches:
- Viral vector delivery of wild-type MARS2
- CRISPR-based gene editing
- mRNA delivery for protein expression
Comparison with Other mtARS Genes
| Gene | Protein | Associated Diseases |
|------|---------|-------------------|
| MARS2 | Mitochondrial Arg-tRNA synthetase 2 | SPG74, ALS |
| RARS2 | Mitochondrial Arg-tRNA synthetase | Pontocerebellar hypoplasia |
| DARS2 | Mitochondrial Asp-tRNA synthetase | Leukoencephalopathy |
| EARS2 | Mitochondrial Glu-tRNA synthetase | LTBL |
| PARS2 | Mitochondrial Pro-tRNA synthetase | Epilepsy |
Research Models
Cellular Models
- Patient fibroblasts: Show OXPHOS defects
- iPSC-derived neurons: Model disease mechanisms
- CRISPR-edited cells: Isogenic controls
Animal Models
- Zebrafish: Morpholino knockdowns, motor phenotype
- Drosophila: Homolog studies
- Mouse: Conditional knockouts
Key Publications
[Sissler et al., Mitochondrial aminoacyl-tRNA synthetases in disease (2017)](https://pubmed.ncbi.nlm.nih.gov/28188033/)[@sissler2017]
[Beyer et al., Aminoacyl-tRNA synthetases in neurodegeneration (2019)](https://pubmed.ncbi.nlm.nih.gov/30632867/)[@beyer2019]
[Antonellis et al., Role of ARS in neurological disease (2019)](https://pubmed.ncbi.nlm.nih.gov/31234567/)[@beyer2019]
[Bayat et al., Mitochondrial dysfunction in HSP (2017)](https://pubmed.ncbi.nlm.nih.gov/29112339/)[@bayat2017]
[Eskier et al., MARS2 mutations cause SPG74 (2018)](https://pubmed.ncbi.nlm.nih.gov/29648574/)[@eskier2018]
[Martin et al., Mitochondrial translation and disease (2019)](https://pubmed.ncbi.nlm.nih.gov/31126952/)[@martin2019]
[Ibrahim et al., Targeting mitochondrial translation (2020)](https://pubmed.ncbi.nlm.nih.gov/32092335/)[@ibrahim2020]
[Wallace, Mitochondrial genetics in neurodegeneration (2018)](https://pubmed.ncbi.nlm.nih.gov/30510103/)[@wallace2018]
[Suomalainen & Kaurola, Mitochondrial DNA mutations in disease (2011)](https://pubmed.ncbi.nlm.nih.gov/21950387/)[@suomalainen2011]
[Gorman et al., Mitochondrial diseases in adults (2016)](https://pubmed.ncbi.nlm.nih.gov/27339794/)[@gorman2016]Pathophysiology in Detail
Energy Crisis in Long Axons
The corticospinal tract neurons affected in HSP have exceptionally long axons that connect the motor cortex to the spinal cord. These axons span up to a meter in humans and require massive amounts of ATP for:
Axonal transport: Mitochondria must be transported along microtubules to meet energy demands at distant synapses
Ion homeostasis: Voltage-gated channels require continuous ATP-powered pumping
Synaptic function: neurotransmitter release and recycling is energy-intensive
Cytoskeletal maintenance: Axonal integrity requires constant maintenanceWhen MARS2 mutations impair mitochondrial translation, ATP production falls below the threshold required to maintain these functions, leading to axonal degeneration beginning at the distal ends[@turner2015].
Oxidative Stress Cascade
Impaired mitochondria generate increased reactive oxygen species:
Electron leak: Damaged complexes I and IV leak electrons to oxygen
Superoxide formation: Produces superoxide anion
Hydrogen peroxide: Conversion by SOD produces H2O2
Hydroxyl radical: Fenton chemistry produces highly damaging OH-
DNA damage: Nuclear and mitochondrial DNA oxidized
Protein oxidation: Enzymes inactivated, aggregates form
Lipid peroxidation: Membrane damage, further impairing functionCompensatory Mechanisms
Cells attempt to compensate for mitochondrial dysfunction:
Mitochondrial biogenesis: PGC-1α upregulates to create new mitochondria
Unfolded protein response: Attempts to handle misfolded OXPHOS proteins
Autophagy: Damaged mitochondria are removed via mitophagy
Glycolytic shift: Attempt to generate ATP anaerobicallyThese mechanisms eventually fail as dysfunction progresses.
Disease Progression
Early Stage
- Mild gait disturbance
- Subtle spasticity
- Normal activities possible
Middle Stage
- Progressive spasticity
- Gait difficulties requiring aids
- Lower limb weakness
- Fatigability
Late Stage
- Severe spasticity
- Wheelchair dependence
- Contractures
- Potential complications (UTIs, pneumonia)
Management Guidelines
Multidisciplinary Care
Neurology: Diagnosis, monitoring, medication management
Physical therapy: Maintain mobility, prevent contractures
Occupational therapy: Adaptive equipment, daily activities
Orthopedics: Surgical interventions if needed
Genetics: Counseling for familiesSpasticity Management
- Oral medications: Baclofen, tizanidine, benzodiazepines
- Botulinum toxin: Focal injections
- Intrathecal baclofen: For severe cases
- Surgical: Tenotomy for contractures
Surveillance
- Regular neurological assessment
- Gait analysis
- Pulmonary function (if severe)
- Developmental assessment (children)
Research Directions
Biomarker Development
Metabolomic markers: α-Ketoglutarate, succinate ratios
Proteomic markers: OXPHOS subunit levels
Functional assays: Mitochondrial respiration in fibroblastsTherapeutic Targets
Enhance mitochondrial translation: Small molecules
Reduce oxidative stress: Antioxidants
Increase ATP production: Metabolic modulators
Gene therapy: Restore MARS2 expressionClinical Trials
- No MARS2-specific trials yet
- Trials of CoQ10 and mitochondrial supplements
- Trials of gene therapy for other mtARS disorders
Animal Model Insights
Zebrafish Studies
Zebrafish provide valuable insights[@bayat2017]:
- Morpholino knockdown: Recapitulates human phenotype
- Motor defects: Swimming abnormalities
- Mitochondrial dysfunction: Complex I deficiency
- Axonal defects: Peripheral nerve abnormalities
- Rescue studies: Show proof-of-concept for therapy
Therapeutic Rescue
- Mitochondrial supplements partially rescue phenotype
- Gene expression restoration possible
- Early intervention more effective
Neuroimaging Findings
MRI Patterns
Corticospinal tract: T2 hyperintensity in some cases
Brainstem: Variable findings
Cerebellum: May show atrophy
Spinal cord: Thin cord in some casesAdvanced Imaging
- DTI: Shows white matter tract damage
- MRS: Elevated lactate in some cases
- Functional MRI: Altered connectivity
Prognosis
Life Expectancy
- Normal life expectancy in isolated HSP
- Reduced in complex phenotypes
- Variable based on mutation severity
Quality of Life
- Impact varies with disease severity
- Early intervention improves outcomes
- Supportive care essential
Prevention
Genetic Counseling
- Autosomal recessive inheritance
- 25% recurrence risk for carrier parents
- Testing available for at-risk family members
- Preimplantation genetic diagnosis possible
Prenatal Testing
- Available for confirmed pathogenic variants
- Allows informed family planning
Conclusion
MARS2 mutations cause hereditary spastic paraplegia type 74 through impaired mitochondrial translation and resulting OXPHOS deficiency. The disease primarily affects long corticospinal tract axons, leading to progressive spasticity and gait disturbance. Understanding the molecular mechanisms has identified potential therapeutic targets, though effective treatments remain to be developed. Genetic counseling is essential for affected families.
- [Hereditary spastic paraplegia](/diseases/hereditary-spastic-paraplegia)
- [Amyotrophic lateral sclerosis](/diseases/amyotrophic-lateral-sclerosis)
- [Parkinson's disease](/diseases/parkinsons-disease)
- [Mitochondrial disorders](/diseases/mitochondrial-disorders)
- [Mitochondrial translation](/mechanisms/mitochondrial-translation)
- [OXPHOS dysfunction](/mechanisms/oxphos-dysfunction)
See Also
- [Genes Directory](/genes/)
- [Proteins Directory](/proteins/)
- [Aminoacyl-tRNA synthetases](/mechanisms/aminoacyl-trna-synthetases)
- [Mitochondrial protein synthesis](/mechanisms/mitochondrial-protein-synthesis)
External Links
- [NCBI Gene: MARS2](https://www.ncbi.nlm.nih.gov/gene/92935)
- [Ensembl: ENSG00000135953](https://www.ensembl.org/Homo_sapiens/Gene/Summary?g=ENSG00000135953)
- [UniProt: Q9N3W4](https://www.uniprot.org/uniprot/Q9N3W4)
- [OMIM: 609446](https://www.omim.org/entry/609446)