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LXR-alpha Protein
LXR-alpha Protein
Pathway Diagram
```mermaid
flowchart TD
NR1H3["NR1H3<br/>(LXRalpha)"]
%% Lipid metabolism pathway
NR1H3 -->|"expressed_in"| CHOL["Cholesterol<br/>Homeostasis"]
NR1H3 -->|"expressed_in"| LIPID["Lipid<br/>Metabolism"]
NR1H3 -->|"interacts_with"| SREBF2["SREBF2<br/>(SREBP-2)"]
NR1H3 -->|"interacts_with"| PPARA["PPARalpha<br/>(Fatty Acid Oxidation)"]
%% Autophagy and cellular clearance
NR1H3 -->|"interacts_with"| AUTOPHAGY["Autophagy<br/>Pathway"]
NR1H3 -->|"interacts_with"| BECN1["BECLIN1<br/>(Autophagy Initiation)"]
NR1H3 -->|"interacts_with"| ULK1["ULK1<br/>(Autophagy Induction)"]
NR1H3 -->|"interacts_with"| LAMP2["LAMP2<br/>(Lysosomal Function)"]
%% mTOR signaling
NR1H3 -->|"interacts_with"| MTOR["mTOR<br/>(Growth Regulation)"]
NR1H3 -->|"interacts_with"| RPTOR["RAPTOR<br/>(mTORC1 Component)"]
%% Oxidative stress and cell death
NR1H3 -->|"interacts_with"| NFE2L2["NRF2<br/>(Antioxidant Response)"]
NR1H3 -->|"interacts_with"| TP53["p53<br/>(Tumor Suppressor)"]
NR1H3 -->|"interacts_with"| MAP3K5["ASK1<br/>(Stress Kinase)"]
%% Phagocytosis and inflammation
NR1H3 -->|"interacts_with"| PHAGO["Phagocytosis<br/>Pathway"]
NR1H3 -->|"interacts_with"| C1Q["C1Q<br/>(Complement System)"]
%% Disease outcomes
AUTOPHAGY -->|"dysfunction"| NEURODEGENERATION["Neurodegeneration<br/>Risk"]
CHOL -->|"dysregulation"| NEURODEGENERATION
NFE2L2 -->|"protection"| NEUROPROTECTION["Neuroprotection"]
style NR1H3 fill:#006494
style NEURO
LXR-alpha Protein
Pathway Diagram
<div class="infobox infobox-protein">
<table>
<tr><th colspan="2" style="background:#e8f4f8; text-align:center; font-size:1.1em;">LXR-alpha Protein</th></tr>
<tr><td><strong>Protein Name</strong></td><td>LXR-alpha (Liver X Receptor alpha)</td></tr>
<tr><td><strong>Gene Symbol</strong></td><td><a href="/genes/nr1h3">NR1H3</a></td></tr>
<tr><td><strong>UniProt ID</strong></td><td><a href="https://www.uniprot.org/uniprot/Q9GZN5">Q9GZN5</a></td></tr>
<tr><td><strong>PDB Structures</strong></td><td>3IPQ, 3IPS, 4NLL</td></tr>
<tr><td><strong>Molecular Weight</strong></td><td>50 kDa</td></tr>
<tr><td><strong>Subcellular Localization</strong></td><td>Nucleus</td></tr>
<tr><td><strong>Protein Family</strong></td><td>Nuclear Receptor Family</td></tr>
<tr>
<td class="label">Associated Diseases</td>
<td><a href="/wiki/als" style="color:#ef9a9a">Als</a>, <a href="/wiki/cancer" style="color:#ef9a9a">Cancer</a>, <a href="/wiki/carcinoma" style="color:#ef9a9a">Carcinoma</a>, <a href="/wiki/fatty-liver" style="color:#ef9a9a">Fatty Liver</a>, <a href="/wiki/hepatitis" style="color:#ef9a9a">Hepatitis</a></td>
</tr>
<tr>
<td class="label">KG Connections</td>
<td><a href="/atlas" style="color:#4fc3f7">170 edges</a></td>
</tr>
</table>
</div>
Overview
LXR-alpha (Liver X Receptor alpha), encoded by the NR1H3 gene, is a ligand-activated transcription factor that plays a central role in regulating genes involved in cholesterol metabolism, lipid transport, and inflammatory responses. As a member of the nuclear receptor superfamily, LXR-alpha functions as a sensor of oxysterols (oxygenated derivatives of cholesterol) and regulates gene expression programs that maintain lipid homeostasis[@zelcer2007].
LXR-alpha is expressed in many tissues, with highest expression in the liver, intestine, kidney, and adipose tissue. It is also expressed in the brain, including neurons and glial cells, where it regulates genes involved in neuroinflammation and neuronal survival. The receptor forms heterodimers with retinoic acid receptor X (RXRA) and binds to LXR response elements (LXREs) in the promoters of target genes.
In the context of neurodegenerative diseases, LXR-alpha has emerged as a potential therapeutic target for Alzheimer's disease (AD), Parkinson's disease (PD), and other disorders. The receptor's ability to regulate cholesterol efflux, reduce neuroinflammation, and promote amyloid-beta clearance makes it an attractive target for intervention[@Wang2021].
Structure
NR1H3 (LXR-alpha) has a characteristic nuclear receptor structure with distinct functional domains:
- N-terminal AF-1 domain: Contains a ligand-independent activation function that can modulate transcriptional activity
- DNA-binding domain (DBD): Contains two zinc fingers that recognize specific DNA sequences (LXREs)
- Hinge region: Flexible domain connecting the DBD to the LBD, important for cofactor interactions
- Ligand-binding domain (LBD): Contains a hydrophobic pocket that binds oxysterols and synthetic ligands
The LBD of LXR-alpha contains a large hydrophobic pocket that accommodates natural ligands including 22(R)-hydroxycholesterol, 24(S)-hydroxycholesterol, and 27-hydroxycholesterol. These oxysterols are generated during cholesterol metabolism and serve as endogenous LXR ligands. The receptor undergoes conformational changes upon ligand binding that promote coactivator recruitment and transcriptional activation.
LXR-alpha forms heterodimers with RXRA (Retinoid X Receptor alpha), and this heterodimer is the functional DNA-binding unit. The heterodimer binds to direct repeat 4 (DR-4) response elements in the promoters of target genes. The ligand-induced conformational change in the LBD reposition the AF-2 helix, allowing coactivator binding and transcriptional activation.
Normal Function
LXR-alpha is a master regulator of cholesterol homeostasis with multiple normal functions:
In the brain, LXR-alpha regulates genes important for neuronal function and survival. It controls cholesterol efflux from astrocytes and microglia, which is important for maintaining brain cholesterol balance. The receptor also regulates inflammatory responses in glial cells, with activation generally producing anti-inflammatory effects.
Key target genes include:
- ABCA1: ATP-binding cassette transporter A1, mediates cholesterol and phospholipid efflux
- ABCG1: ATP-binding cassette transporter G1, works with ABCA1 for cholesterol efflux
- APOE: Apolipoprotein E, the most significant lipid transport protein in the brain
- SREBP-1c: Sterol regulatory element-binding protein 1c, regulates fatty acid synthesis
Role in Disease
LXR-alpha is implicated in neurodegenerative diseases through its roles in cholesterol metabolism and inflammation:
Alzheimer's Disease
In Alzheimer's disease, LXR activation shows protective effects through multiple mechanisms:
- Upregulation of [ABCA1](/proteins/abca1-protein) and [APOE](/proteins/apoe-protein) to enhance [amyloid-beta](/proteins/amyloid-beta) clearance
- Promotion of cholesterol efflux from neurons and glial cells
- Reduction of neuroinflammation through repression of inflammatory mediators
- Potential modulation of tau pathology through cholesterol-dependent mechanisms
- Studies show LXR agonists reduce amyloid burden in AD mouse models
Parkinson's Disease
In Parkinson's disease, LXR-alpha provides neuroprotection through:
- Protection of dopaminergic neurons from oxidative stress
- Enhancement of mitochondrial function
- Anti-inflammatory effects in microglia
- Potential modulation of alpha-synuclein metabolism
- LXR-beta (NR1H2) is also important for dopamine neuron survival
Other Neurodegenerative Conditions
LXR signaling is relevant to:
- Amyotrophic lateral sclerosis (ALS): Altered cholesterol metabolism in motor neurons
- Multiple sclerosis: LXR affects demyelination and remyelination
- Huntington's disease: Cholesterol dysregulation and LXR involvement
- Brain aging: Declining LXR signaling with age may contribute to cognitive decline
The finding that LXR-beta is required for normal dopamine neuron function and survival highlights the importance of LXR signaling in PD[@vaya2012].
Therapeutic Targeting
LXR agonists have shown protective effects in neurodegenerative disease models, though challenges remain:
Preclinical Results
- LXR agonists (GW3965, T0901317) reduce amyloid pathology in AD mouse models
- Protective effects in PD models with dopaminergic neuron preservation
- Reduced neuroinflammation in multiple models
- Improved cognitive performance in aged animals
Challenges and Limitations
- First-generation LXR agonists caused side effects:
- Hypertriglyceridemia (elevated blood fats)
- Liver steatosis (fat accumulation in liver)
- Weight gain
- These side effects limit clinical applicability
Newer Approaches
- Brain-penetrant LXR agonists: Newer compounds with better brain penetration
- LXR-beta selective agonists: May avoid some side effects associated with LXR-alpha
- Selective LXR modulators (SLiMs): Compound that provide beneficial effects without side effects
- Gene therapy approaches: AAV-mediated LXR expression in the brain
- Combination therapies: LXR agonists combined with other therapeutic agents
Research continues to develop LXR modulators that provide neuroprotective benefits while avoiding the metabolic side effects of first-generation compounds[@kim2019].
Key Publications
See Also
- [NR1H3 Gene](/genes/nr1h3)
- [LXR Signaling in Neurodegeneration](/mechanisms/lxr-signaling-neurodegeneration)
- [Cholesterol Metabolism in AD](/mechanisms/cholesterol-metabolism-alzheimers)
- [PPAR Signaling in Neurodegeneration](/mechanisms/ppar-signaling-neurodegeneration)
References
▸Metadataorigin_type: v1_polymorphic_backfill
| slug | proteins-nr1h3-protein |
| kg_node_id | NR1H3PROTEIN |
| entity_type | protein |
| origin_type | v1_polymorphic_backfill |
| source_table | wiki_pages |
| wiki_page_id | wp-3caea5223dfe |
| __merged_from | {'merged_at': '2026-05-13', 'unprefixed_id': 'proteins-nr1h3-protein'} |
| _schema_version | 1 |
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