NDUFS3 Gene - NADH:Ubiquinone Oxidoreductase Core Subunit S3

📖 Wiki Page

gene1476 wordssynced 2026-04-02

NDUFS3 Gene - NADH:Ubiquinone Oxidoreductase Core Subunit S3

Introduction

<div class="infobox infobox-gene">
<h3>NDUFS3</h3>
<table>
<tr><th>Full Name</th><td>NADH:Ubiquinone Oxidoreductase Core Subunit S3</td></tr>
<tr><th>Chromosomal Location</th><td>19p13.3</td></tr>
<tr><th>NCBI Gene ID</th><td>[4714](https://www.ncbi.nlm.nih.gov/gene/4714)</td></tr>
<tr><th>OMIM</th><td>[601446](https://omim.org/entry/601446)</td></tr>
<tr><th>Ensembl ID</th><td>ENSG00000103245</td></tr>
<tr><th>UniProt</th><td>[O75489](https://www.uniprot.org/uniprot/O75489)</td></tr>
<tr><th>Associated Diseases</th><td>Parkinson's Disease, Leigh Syndrome, Mitochondrial Complex I Deficiency</td></tr>
</table>
</div>

Overview

NDUFS3 (NADH:Ubiquinone Oxidoreductase Core Subunit S3) encodes a core component of mitochondrial complex I (NADH:ubiquinone oxidoreductase), the largest enzyme complex of the electron transport chain[@kirby2004]. Located on chromosome 19p13.3, NDUFS3 is essential for complex I assembly and function, and its dysfunction is directly linked to neurodegenerative diseases including Parkinson's disease (PD)[@schapira2012], [@subramaniam2018].

...

NDUFS3 Gene - NADH:Ubiquinone Oxidoreductase Core Subunit S3

Introduction

Overview

Complex I (NADH:ubiquinone oxidoreductase) is the entry point of the mitochondrial electron transport chain, catalyzing the transfer of electrons from NADH to ubiquinone while pumping protons across the inner mitochondrial membrane[@devires2016]. The resulting proton gradient drives ATP synthesis via ATP synthase. NDUFS3 encodes the 30 kDa iron-sulfur subunit located in the Q module of the hydrophilic arm, positioned near the electron entry point[@zago2018]. This strategic location makes NDUFS3 critical for both complex I assembly and catalytic efficiency.

Protein Structure and Function

Structural Organization

NDUFS3 is a 30 kDa protein belonging to the nuclear-encoded mitochondrial complex I subunits. It contains conserved iron-sulfur (Fe-S) cluster binding motifs essential for electron transfer[@wiedemann2018]:

N-terminal domain: Contains the mitochondrial targeting sequence for import
Core domain: Houses two [2Fe-2S] iron-sulfur clusters (N1a and N1b) responsible for electron transfer
Interface region: Contacts neighboring core subunits (NDUFS2, NDUFV1, NDUFV2) to form the catalytic module

The NDUFS3 subunit is one of seven core catalytic subunits conserved across all eukaryotes and many bacteria, reflecting its fundamental role in the NADH dehydrogenase reaction[@kirby2004].

Catalytic Mechanism

NDUFS3 participates in the electron transfer chain within complex I:

NADH binding: The flavin mononucleotide (FMN) in NDUFV1 accepts two electrons from NADH

Fe-S cluster chain: Electrons flow through a series of Fe-S clusters (N3 → N1b → N1a → NuoB/C in bacteria; analogous subunits in humans including NDUFS3)

Ubiquinone reduction: Final electron transfer to ubiquinone at the Q binding site

Proton pumping: Electron transfer is coupled to proton translocation across the inner membrane

The iron-sulfur clusters in NDUFS3 are essential for mediating electron flow between the FMN and ubiquinone reaction centers[@devires2016]. Loss or damage to NDUFS3 disrupts this chain, causing electron leakage and increased [reactive oxygen species (ROS)](/entities/reactive-oxygen-species) production.

Role in Parkinson's Disease Pathogenesis

Evidence from PD Patients

Multiple studies have documented complex I deficiency in the [substantia nigra](/brain-regions/substantia-nigra) of PD patients[@schapira2012], [@alauddin2023], [@lax2012]:

Biochemical studies: Complex I activity is reduced by 30-40% in PD substantia nigra pars compacta neurons[@schapira2012]
Postmortem analysis: NDUFS3 protein levels and complex I assembly are impaired in PD brains[@zago2018]
Genetic associations: Rare variants in complex I subunits, including NDUFS3, have been identified in PD cohorts[@filograna2021]
Sporadic PD: The majority of PD cases show complex I dysfunction even without identified genetic mutations[@schapira2012]

Mechanisms Linking NDUFS3 Dysfunction to PD

The connection between NDUFS3/complex I deficiency and PD neurodegeneration involves multiple interconnected pathways[@pickrell2015], [@perier2012]:

Mermaid diagram (expand to render)

1. Energy Crisis

Complex I deficiency severely impairs oxidative phosphorylation[@malpolonia2015]. Dopaminergic neurons of the substantia nigra have exceptionally high energy demands due to their autonomous pacemaking activity and extensive axonal arborization. Loss of complex I function leads to:

ATP depletion: Reduced ATP production impairs ion pump function and neurotransmitter synthesis
NAD+/NADH imbalance: Disrupted redox state affects sirtuin signaling and DNA repair
Synaptic dysfunction: Energy failure disrupts neurotransmitter release and synaptic vesicle recycling[@perier2012]

2. Oxidative Stress

Electron leakage from damaged complex I generates superoxide radicals[@pickrell2015], [@chen2010]:

Superoxide production: Complex I dysfunction increases superoxide (O2-) generation
Mitochondrial DNA damage: ROS damages mtDNA, which encodes critical respiratory chain subunits
Protein oxidation: ROS modifies proteins including alpha-synuclein, promoting its aggregation
Lipid peroxidation: ROS attacks mitochondrial cardiolipin, further disrupting membrane integrity[@burt2013]

3. Alpha-Synuclein Connection

NDUFS3 dysfunction and alpha-synuclein pathology form a vicious cycle[@kuwahara2018]:

Oxidative stress promotes alpha-synuclein misfolding and aggregation
Aggregated alpha-synucleinlocalizes to mitochondria, further inhibiting complex I
Mitochondrial complex I inhibition increases alpha-synuclein aggregation propensity
This creates a feedforward loop driving progressive neurodegeneration[@pickrell2015]

4. Mitophagy Dysregulation

The [PINK1/Parkin mitophagy pathway](/mechanisms/pink1-parkin-pathway) is intimately connected to complex I function[@ryan2012]:

Damaged mitochondria with low membrane potential accumulate PINK1 on the outer membrane
PINK1 activates Parkin E3 ubiquitin ligase activity
Parkin ubiquitinates mitochondrial proteins, targeting the organelle for autophagic degradation
Complex I deficiency can trigger compensatory mitophagy but also disrupts the signaling cascade
PINK1 mutations (a genetic cause of PD) impair the cell's ability to remove damaged complex I[@pickrell2015]

Animal Models

NDUFS3 dysfunction has been modeled in several systems[@jensen2020]:

Knockdown in Drosophila: Reduced NDUFS3 expression causes complex I deficiency, locomotor impairment, and shortened lifespan
Conditional knockout in mice: Neuron-specific NDUFS3 deletion leads to progressive neurodegeneration with alpha-synuclein aggregation
MPTP/rotenone models: These complex I inhibitors reproduce many features of NDUFS3 deficiency, validating the mechanistic link

Therapeutic Implications

Targeting complex I dysfunction remains an active therapeutic strategy[@barker2022], [@jensen2020]:

Coenzyme Q10 (CoQ10): Electron carrier that bypasses complex I; clinical trials show modest benefit in early PD
Nicotinamide riboside (NR): Boosts NAD+ levels, supporting mitochondrial biogenesis and sirtuin activity
Mitochondrial-targeted antioxidants: MitoQ and other mitochondrial-specific ROS scavengers
PGC-1α activators: Promote mitochondrial biogenesis to compensate for defective complexes
Gene therapy approaches: Viral delivery of wild-type complex I subunits to restore function

NDUFS3 and Leigh Syndrome

NDUFS3 mutations were first identified as a cause of isolated complex I deficiency presenting as Leigh syndrome[@kirby2004], [@filograna2021]:

Clinical features: Hypotonia, developmental regression, Leigh syndrome lesions in brainstem and basal ganglia
Inheritance: Autosomal recessive; patients inherit two mutant alleles
Biochemistry: Severely reduced complex I activity (typically <10% of normal)
Prognosis: Variable; some patients respond to metabolic support and dietary interventions

The NDUFS3-related Leigh syndrome demonstrates that complete loss of NDUFS3 function causes early-onset severe encephalopathy, while partial deficiency (as seen in PD) may permit survival into adulthood with progressive neurodegeneration[@kirby2004].

Expression Pattern and Regulation

NDUFS3 shows tissue-specific expression patterns[@burt2013]:

High expression: Brain (particularly substantia nigra, [hippocampus](/brain-regions/hippocampus), cortex), heart, skeletal muscle — tissues with high energy demands
Moderate expression: Kidney, liver, pancreas
Regulation: NDUFS3 expression is regulated by:
PGC-1α: The master regulator of mitochondrial biogenesis drives NDUFS3 transcription
AMPK: Energy sensor activated by low ATP, promotes mitochondrial gene expression
SIRT1: NAD+-dependent deacetylase that activates PGC-1α under stress[@malpolonia2015]

Interaction Network

NDUFS3 interacts with multiple proteins within the mitochondrial complex I assembly[@wiedemann2018], [@zago2018]:

| Partner | Interaction Type | Functional Significance |
|---------|-----------------|------------------------|
| NDUFS2 | Core subunit complex | Forms catalytic core with NDUFS3 |
| NDUFV1 | Core subunit complex | FMN to Fe-S electron transfer |
| NDUFV2 | Core subunit complex | Electron entry point |
| NDUFS1 | Core subunit complex | Q module assembly |
| NDUFS4 | Assembly factor | Critical for NDUFS3 incorporation |
| NDUFS6 | Assembly factor | Early assembly step |
| NDUFA9 | Assembly factor | Q module formation |
| LRPPRC | Transcriptional regulator | Mitochondrial DNA maintenance |

Differential Expression in Neurodegeneration

RNA sequencing and proteomics studies reveal NDUFS3 alterations across neurodegenerative diseases[@morradottir2019]:

Alzheimer's disease: Reduced NDUFS3 transcript in hippocampus and cortex; correlates with mitochondrial dysfunction markers
Parkinson's disease: Decreased NDUFS3 protein and activity in substantia nigra dopaminergic neurons
Huntington's disease: NDUFS3 dysregulation in striatal neurons; mitochondrial deficit contributes to medium spiny neuron death
Amyotrophic lateral sclerosis (ALS): Motor neuron complex I dysfunction including NDUFS3 abnormalities

Research History

| Year | Milestone |
|------|-----------|
| 1999 | NDUFS3 gene identified and mapped to chromosome 19p13.3 |
| 2004 | First NDUFS3 mutations identified causing Leigh syndrome[@kirby2004] |
| 2009 | NDUFS3/complex I deficiency documented in PD substantia nigra[@gandhi2009] |
| 2012 | Comprehensive review of complex I defects in neurodegeneration[@lax2012], [@blic2013] |
| 2015 | PINK1/Parkin pathway interactions with complex I elucidated[@pickrell2015] |
| 2016 | Structural insights into NDUFS3 function within complex I[@devires2016] |
| 2018 | Alpha-synuclein and complex I dysfunction feedforward loop described[@kuwahara2018] |
| 2021 | NDUFS3 promoter variants associated with PD risk[@filograna2021] |
| 2022 | CoQ10 clinical trials in complex I-deficient PD patients[@barker2022] |
| 2023 | Single-cell analysis of complex I deficiency in PD dopaminergic neurons[@alauddin2023] |

External Links

[NCBI Gene: NDUFS3](https://www.ncbi.nlm.nih.gov/gene/4714)
[OMIM: 601446](https://omim.org/entry/601446)
[UniProt: O75489](https://www.uniprot.org/uniprot/O75489)
[PubMed: NDUFS3 neurodegeneration](https://pubmed.ncbi.nlm.nih.gov/?term=NDUFS3+Parkinson)
[GeneCards: NDUFS3](https://www.genecards.org/cgi-bin/carddisp.pl?gene=NDUFS3)

Pathway Diagram

The following diagram shows the key molecular relationships involving NDUFS3 Gene - NADH:Ubiquinone Oxidoreductase Core Subunit S3 discovered through SciDEX knowledge graph analysis:

Mermaid diagram (expand to render)

📖 View canonical wiki page →

NDUFS3 Gene - NADH:Ubiquinone Oxidoreductase Core Subunit S3

NDUFS3 Gene - NADH:Ubiquinone Oxidoreductase Core Subunit S3

Introduction

Overview

NDUFS3 Gene - NADH:Ubiquinone Oxidoreductase Core Subunit S3

Introduction

Overview

Protein Structure and Function

Structural Organization

Catalytic Mechanism

Role in Parkinson's Disease Pathogenesis

Evidence from PD Patients

Mechanisms Linking NDUFS3 Dysfunction to PD

1. Energy Crisis

2. Oxidative Stress

3. Alpha-Synuclein Connection

4. Mitophagy Dysregulation

Animal Models

Therapeutic Implications

NDUFS3 and Leigh Syndrome

Expression Pattern and Regulation

Interaction Network

Differential Expression in Neurodegeneration

Research History

See Also

External Links

Pathway Diagram