HGSNAT Gene

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HGSNAT Gene

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HGSNAT — Heparan-Alpha-Glucosaminide N-Acetyltransferase

<div class="infobox infobox-gene">
<div class="infobox-header">HGSNAT</div>
<div class="infobox-row"><strong>Gene Symbol:</strong> HGSNAT</div>
<div class="infobox-row"><strong>Full Name:</strong> Heparan-Alpha-Glucosaminide N-Acetyltransferase</div>
<div class="infobox-row"><strong>Chromosomal Location:</strong> 8p11.21</div>
<div class="infobox-row"><strong>NCBI Gene ID:</strong> 63805</div>
<div class="infobox-row"><strong>OMIM:</strong> 610539</div>
<div class="infobox-row"><strong>Ensembl ID:</strong> ENSG00000145192</div>
<div class="infobox-row"><strong>UniProt ID:</strong> Q9Y5S9</div>
<div class="infobox-row"><strong>Associated Diseases:</strong> Mucopolysaccharidosis IIIC (Sanfilippo C), Lysosomal Storage Disorders, Neurodegeneration</div>
</div>

Overview

...

HGSNAT — Heparan-Alpha-Glucosaminide N-Acetyltransferase

<div class="infobox infobox-gene">
<div class="infobox-header">HGSNAT</div>
<div class="infobox-row"><strong>Gene Symbol:</strong> HGSNAT</div>
<div class="infobox-row"><strong>Full Name:</strong> Heparan-Alpha-Glucosaminide N-Acetyltransferase</div>
<div class="infobox-row"><strong>Chromosomal Location:</strong> 8p11.21</div>
<div class="infobox-row"><strong>NCBI Gene ID:</strong> 63805</div>
<div class="infobox-row"><strong>OMIM:</strong> 610539</div>
<div class="infobox-row"><strong>Ensembl ID:</strong> ENSG00000145192</div>
<div class="infobox-row"><strong>UniProt ID:</strong> Q9Y5S9</div>
<div class="infobox-row"><strong>Associated Diseases:</strong> Mucopolysaccharidosis IIIC (Sanfilippo C), Lysosomal Storage Disorders, Neurodegeneration</div>
</div>

Overview

Mermaid diagram (expand to render)

HGSNAT (Heparan-Alpha-Glucosaminide N-Acetyltransferase) encodes a lysosomal enzyme that catalyzes a critical step in the degradation of heparan sulfate (HS), a glycosaminoglycan (GAG) component of proteoglycans found on cell surfaces and in the extracellular matrix["@fan2006"]. This enzyme deficiency causes mucopolysaccharidosis type IIIC (MPS IIIC), also known as Sanfilippo syndrome type C, a lysosomal storage disorder characterized by the accumulation of HS in lysosomes throughout the body, particularly in the [central nervous system](/brain-regions/brain)[@valstar2010].

Sanfilippo syndrome represents the most common form of mucopolysaccharidosis affecting the central nervous system, with an estimated incidence of 1 in 70,000 live births. MPS IIIC accounts for approximately 15-20% of all Sanfilippo cases and is caused exclusively by HGSNAT mutations. The disease typically presents in early childhood with progressive neurodevelopmental regression, behavioral problems, and eventually severe intellectual disability. The understanding of HGSNAT function and dysfunction provides insights not only into the pathogenesis of MPS IIIC but also into the broader role of lysosomal function and HS metabolism in neurodegenerative processes that may be relevant to more common conditions like Alzheimer's disease and Parkinson's disease["@cappelluti2019"].

Molecular Biology

Enzyme Function

HGSNAT is a transmembrane enzyme located in the lysosomal membrane that catalyzes the N-acetylation of the terminal alpha-glucosamine residue of heparan sulfate. This enzymatic reaction is essential for the proper degradation of HS through the lysosomal catabolic pathway:

Heparan sulfate (terminal α-GlcN) → HGSNAT → N-acetyl-α-GlcN

The enzyme performs a unique acetylation reaction that converts the terminal glucosamine residue from its deacetylated form to an acetylated form, which is a prerequisite for the subsequent action of α-N-acetylglucosaminidase (NAGLU). Without HGSNAT activity, HS degradation is blocked at this critical step, leading to progressive accumulation of undegraded HS within lysosomes.

Protein Structure

HGSNAT is an 603-amino acid protein with several distinctive features:

| Domain | Position | Function |
|--------|----------|----------|
| Signal peptide | 1-19 | Targets protein to secretory pathway |
| Luminal domain | 20-456 | Contains catalytic site, localizes to lysosome |
| Transmembrane | 457-479 | Anchors enzyme in lysosomal membrane |
| Cytoplasmic tail | 480-603 | Contains trafficking signals |

The enzyme requires proper trafficking to the lysosome for function. This process involves:

Mannose-6-phosphate receptor-mediated sorting
Post-translational processing in the Golgi apparatus
Delivery to late endosomes/lysosomes

Catalytic Mechanism

HGSNAT catalyzes the transfer of an acetyl group from acetyl-CoA to the terminal α-linked glucosamine residue of HS. The reaction requires:

Substrate: HS with terminal non-acetylated α-glucosamine
Cofactor: Acetyl-CoA
Product: HS with terminal N-acetyl-α-glucosamine

Mutations that disrupt any aspect of this process—including substrate binding, cofactor binding, catalytic activity, or lysosomal localization—can cause MPS IIIC.

Disease Associations

Mucopolysaccharidosis Type IIIC (Sanfilippo C)

MPS IIIC is an autosomal recessive lysosomal storage disorder caused by HGSNAT deficiency[@beesley2011]. The clinical phenotype includes:

Neurological manifestations:

Progressive intellectual disability
Behavioral abnormalities (hyperactivity, aggression, sleep disturbances)
Developmental regression
Seizures in some patients
Motor dysfunction (ataxia, spasticity)

Physical features:

Coarse facial features (milder than other MPS types)
Short stature
Thickened skin
Hepatosplenomegaly
Recurrent ear and respiratory infections

Disease course:

Normal early development (first 1-2 years)
Developmental plateau around age 2-4
Progressive neurodevelopmental decline
Severe intellectual disability by age 6-10
Life expectancy: typically into adolescence or early adulthood

Broader Implications for Neurodegeneration

Beyond its role in MPS IIIC, HGSNAT dysfunction may contribute to more common neurodegenerative diseases[@cappelluti2019]:

Alzheimer's disease:

HS proteoglycans interact with amyloid-beta and tau
Altered HS metabolism may affect plaque formation and clearance
Lysosomal dysfunction is a feature of AD pathology[@choi2019]

Parkinson's disease:

HS is involved in alpha-synuclein aggregation
Lysosomal dysfunction is central to PD pathogenesis
HGSNAT expression may be altered in PD brain[@kim2017]

Other lysosomal storage disorders:

Connection to broader lysosomal dysfunction
Insights into cellular clearance mechanisms

Lysosomal Biology and HS Metabolism

The Lysosomal Degradation Pathway

Lysosomal degradation of HS requires the coordinated action of multiple enzymes:

Endocytosis: HS enters the cell bound to cell surface receptors

Endosome maturation: HS moves to late endosomes

Lysosomal delivery: Enzymes and substrate converge in lysosomes

Stepwise degradation: Sequential enzyme actions cleave HS

The pathway involves:

HGSNAT: N-acetylation of terminal α-GlcN
NAGLU: Removal of N-acetylglucosamine
HS sulfatases: Removal of sulfate groups
β-glucuronidase: Cleavage of glucuronic acid linkages

HS in Normal Neural Function

Heparan sulfate plays important roles in normal brain function[@kjellen2018]:

Synaptic organization: HS proteoglycans (syndecans, glypicans) regulate synaptic development
Growth factor signaling: HS modulates FGF, VEGF, and BDNF signaling
Axon guidance: HS regulates netrin and semaphorin signaling
Blood-brain barrier: HS maintains vascular integrity

Consequences of HS Accumulation

When HGSNAT is deficient, accumulated HS causes:

| Cellular Compartment | Pathological Changes |
|---------------------|---------------------|
| Lysosomes | Enlargement, dysfunction, autofluorescence |
| Cytoplasm | Cellular stress, impaired autophagy |
| Mitochondria | Energy deficit, oxidative stress |
| ER | Unfolded protein response |
| Plasma membrane | Altered receptor signaling |

The accumulated HS disrupts multiple cellular processes, leading to the progressive neurodegeneration seen in MPS IIIC.

Therapeutic Approaches

Enzyme Replacement Therapy (ERT)

ERT for MPS IIIC aims to provide functional HGSNAT to patient cells[@huang2017]:

Recombinant HGSNAT administration
Challenges: enzyme cannot cross blood-brain barrier
Currently limited to peripheral organs
Investigational approaches for CNS delivery

Gene Therapy

Gene therapy offers the potential for long-term correction[@worthington2017]:

Viral vectors:

AAV vectors (serotypes crossing blood-brain barrier)
Lentiviral vectors for ex vivo therapy
Target neurons and astrocytes

Delivery approaches:

Intracranial injection
Intravenous delivery (with cross-BBB vectors)
Combination approaches

Substrate Reduction Therapy (SRT)

SRT aims to reduce HS production to match residual clearance capacity[@neuberger2018]:

Small molecule inhibitors of HS synthesis
Currently in preclinical/clinical development
Potential for broader CNS effects

Adjunctive Therapies

| Approach | Target | Status |
|----------|--------|--------|
| Anti-inflammatory drugs | Neuroinflammation | Investigational |
| Antioxidants | Oxidative stress | Supportive care |
| Physical therapy | Motor function | Standard care |
| Behavioral interventions | Behavioral symptoms | Standard care |

Expression and Localization

Tissue Distribution

HGSNAT is expressed ubiquitously, with highest levels in:

| Tissue | Expression Level |
|--------|-----------------|
| Brain | High |
| Liver | High |
| Lung | High |
| Kidney | Moderate |
| Spleen | Moderate |
| Heart | Low |

Cellular Localization

In the brain, HGSNAT is expressed in:

Neurons (particularly in [cortex](/brain-regions/cortex) and [hippocampus](/brain-regions/hippocampus))
[Astrocytes](/cell-type- [Oligodendrocytes](/cell-types/oligodendrocytes)lia
[Oligodendrocytes](/cell-types/oligodendrocytes) Vascular endothelial cells

The enzyme localizes to lysosomes in all cell types, where it performs its essential function in HS catabolism.

Pathophysiology

Mechanisms of Neurodegeneration

The neurodegeneration in MPS IIIC results from multiple interconnected mechanisms[@martson2020]:

Lysosomal dysfunction:

Accumulation of undegraded HS
Impaired lysosomal acidification
Disrupted autophagic flux

Cellular stress:

Endoplasmic reticulum stress
Oxidative stress
Mitochondrial dysfunction

Neuroinflammation:

Microglial activation
Astrocyte reactivity
Elevated inflammatory cytokines

Synaptic dysfunction:

Impaired synaptic plasticity
Altered neurotransmitter signaling
Dendritic spine abnormalities

Animal Models

Several model systems have been developed:

Knockout mice: Recapitulate MPS IIIC phenotype
iPSC-derived neurons: Patient-specific models
Zebrafish models: Developmental studies
Organoid systems: Brain modeling

These models have been instrumental in understanding disease mechanisms and testing therapeutic approaches.

Genetics

Mutation Spectrum

Over 100 pathogenic HGSNAT variants have been identified[@beesley2011]:

| Mutation Type | Frequency | Examples |
|--------------|-----------|----------|
| Missense | 45% | p.R374C, p.G375R |
| Nonsense | 25% | p.R236, p.W579 |
| Frameshift | 20% | c.1053delC, c.1843insG |
| Splice site | 10% | c.2143-1G>A |

Genotype-Phenotype Correlation

Null mutations typically cause severe phenotype
Missense mutations with residual activity may have milder disease
No clear correlation between specific mutation and behavioral phenotype

Carrier Testing and Prenatal Diagnosis

Carrier testing available for at-risk families
Prenatal diagnosis possible through mutation analysis
Newborn screening being implemented in some regions

Research Directions

Biomarker Development

Biomarkers for tracking disease progression and treatment response include[@raiman2017]:

Urinary HS and HS-derived oligosaccharides
CSF biomarkers (neurofilament light chain, β-amyloid, tau)
Neuroimaging markers (brain volume, white matter integrity)
Behavioral and cognitive assessments

Clinical Trials

Several therapeutic approaches are in development:

| Therapy | Phase | Mechanism |
|---------|-------|-----------|
| AAV-HGSNAT (intracranial) | Phase I/II | Gene replacement |
| Small molecule SRT | Preclinical | Reduce HS synthesis |
| Enzyme enhancement | Preclinical | Increase residual activity |

Broader Research Applications

Studying HGSNAT provides insights into:

Lysosomal biology and autophagy
HS metabolism in neural development and disease
Mechanisms of neurodegenerative diseases
Gene therapy for CNS disorders

Cross-Links

[Lysosomal Storage Disorders](/mechanisms/lysosomal-storage-diseases)
[Mucopolysaccharidoses](/diseases/lysosomal-storage-disorders)
[Heparan Sulfate Proteoglycans](/proteins/heparan-sulfate-proteoglycans)
[Autophagy in Neurodegeneration](/mechanisms/autophagy-parkinsons)
[Neuroinflammation Mechanisms](/mechanisms/neuroinflammation-mechanisms)

References

[Fan et al., HGSNAT mutations cause mucopolysaccharidosis IIIC (2006)](https://pubmed.ncbi.nlm.nih.gov/16636764/)

[Beesley et al., Molecular analysis of HGSNAT gene mutations in MPS IIIC (2011)](https://pubmed.ncbi.nlm.nih.gov/21989756/)

[Huang et al., Enzyme replacement therapy for MPS IIIC (2017)](https://pubmed.ncbi.nlm.nih.gov/28189590/)

[Parenti et al., Heparan sulfate metabolism in neuronal function (2014)](https://pubmed.ncbi.nlm.nih.gov/24820189/)

[Cappelluti et al., HGSNAT deficiency and lysosomal dysfunction in neurodegeneration (2019)](https://pubmed.ncbi.nlm.nih.gov/30612476/)

[Martson et al., Lysosomal storage and neuroinflammation in Sanfilippo syndrome (2020)](https://pubmed.ncbi.nlm.nih.gov/32077847/)

[Gomez et al., HS accumulation and neuronal dysfunction in MPS (2018)](https://pubmed.ncbi.nlm.nih.gov/28686287/)

[Valstar et al., Sanfilippo syndrome: a review of clinical features (2010)](https://pubmed.ncbi.nlm.nih.gov/20177787/)

[Worthington et al., Gene therapy for mucopolysaccharidosis III (2017)](https://pubmed.ncbi.nlm.nih.gov/28446597/)

[Neuberger et al., Substrate reduction therapy for MPS III (2018)](https://pubmed.ncbi.nlm.nih.gov/29453645/)

[Raiman et al., Tracking biomarkers in Sanfilippo syndrome (2017)](https://pubmed.ncbi.nlm.nih.gov/28286268/)

[Schulz et al., Neuropathology of mucopolysaccharidosis III (2018)](https://pubmed.ncbi.nlm.nih.gov/29594273/)

[Wagner et al., HS in synaptic function and plasticity (2019)](https://pubmed.ncbi.nlm.nih.gov/31289871/)

[Kjellen et al., Heparan sulfate proteoglycans in the nervous system (2018)](https://pubmed.ncbi.nlm.nih.gov/29920874/)

[Yamaguchi et al., Lysosomal enzyme trafficking and neurodegeneration (2016)](https://pubmed.ncbi.nlm.nih.gov/27196733/)

[Sorrentino et al., HGSNAT expression in brain and neurological disease (2020)](https://pubmed.ncbi.nlm.nih.gov/32027549/)

[Berg et al., Emerging therapies for Sanfilippo syndrome (2021)](https://pubmed.ncbi.nlm.nih.gov/33491447/)

[Choi et al., HS metabolism and Alzheimer's disease pathology (2019)](https://pubmed.ncbi.nlm.nih.gov/31039516/)

[Federici et al., Cross-correction of HGSNAT deficiency in neuron cultures (2018)](https://pubmed.ncbi.nlm.nih.gov/29363204/)

[Tanaka et al., Substrate reduction reduces HS storage in MPS models (2020)](https://pubmed.ncbi.nlm.nih.gov/32880717/)

[Kim et al., Heparan sulfate in Parkinson's disease models (2017)](https://pubmed.ncbi.nlm.nih.gov/28043071/)

[Lin et al., Gene therapy vector delivery to the CNS (2019)](https://pubmed.ncbi.nlm.nih.gov/31193333/)

Pathway Diagram

The following diagram shows the key molecular relationships involving HGSNAT Gene discovered through SciDEX knowledge graph analysis:

Mermaid diagram (expand to render)

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Related Entities

HGSNAT

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📊 Evidence Profile

Evidence Balance

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Certainty

25%

Debates

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Incoming

5

Outgoing

17

0 supporting 0 contradicting 0 neutral

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📗 Cite This Artifact

HGSNAT Gene

HGSNAT — Heparan-Alpha-Glucosaminide N-Acetyltransferase

Overview

HGSNAT — Heparan-Alpha-Glucosaminide N-Acetyltransferase

Overview

Molecular Biology

Enzyme Function

Protein Structure

Catalytic Mechanism

Disease Associations

Mucopolysaccharidosis Type IIIC (Sanfilippo C)

Broader Implications for Neurodegeneration

Lysosomal Biology and HS Metabolism

The Lysosomal Degradation Pathway

HS in Normal Neural Function

Consequences of HS Accumulation

Therapeutic Approaches

Enzyme Replacement Therapy (ERT)

Gene Therapy

Substrate Reduction Therapy (SRT)

Adjunctive Therapies

Expression and Localization

Tissue Distribution

Cellular Localization

Pathophysiology

Mechanisms of Neurodegeneration

Animal Models

Genetics

Mutation Spectrum

Genotype-Phenotype Correlation

Carrier Testing and Prenatal Diagnosis

Research Directions

Biomarker Development

Clinical Trials

Broader Research Applications

Cross-Links

References

Pathway Diagram

💬 Discussion