| CLU — Clusterin (Apolipoprotein J) | |
|---|---|
| Symbol | CLU |
| Full Name | Clusterin (Apolipoprotein J, ApoJ) |
| Chromosome | 8p21.1 |
| NCBI Gene | 1115 |
| Ensembl | ENSG00000120885 |
| OMIM | 185551 |
| UniProt | P10909 |
| Diseases | [Alzheimer's Disease](/diseases/alzheimers-disease), [Huntington's Disease](/diseases/huntingtons-disease), ALS |
| Expression | Hippocampus, Cortex, Basal ganglia, Cerebellum |
| Key Variants | |
| rs11136000 (protective, OR ~0.86) rs2279590 (eQTL) rs42039 (coding) |
|
| Associated Diseases | ALZHEIMER, ALZHEIMER'S, ALZHEIMER'S DISEASE, Aging, Als |
| KG Connections | 341 edges |
CLU — Clusterin (Apolipoprotein J)
Introduction
CLU (also known as Clusterin or Apolipoprotein J, ApoJ) is a gene located on chromosome 8p21.1 that encodes a highly conserved multifunctional glycoprotein. CLU was first identified as a significant genetic risk factor for late-onset Alzheimer’s disease (AD) in the landmark genome-wide association study (GWAS) published in 2009, alongside PICALM and CR1 1Genome-wide association study identifies variants at CLU and CR1 associatedOpen reference. The protective variant rs11136000 has an odds ratio of approximately 0.86, meaning carriers have approximately 14% reduced risk of developing AD.
Clusterin is one of the most abundant proteins in the brain and is involved in numerous physiological processes including lipid transport, complement regulation, apoptosis inhibition, and protein homeostasis. Its role in AD pathogenesis is particularly significant due to its ability to bind amyloid-beta (Aβ) and facilitate its clearance from the brain.
Gene Structure and Expression
Genomic Organization
The CLU gene spans approximately 16 kb on chromosome 8p21.1 (coordinates: chr8:27,456,000-27,472,000, GRCh38). It consists of 9 exons encoding a precursor protein that undergoes extensive post-translational modification. The gene uses alternative transcription start sites and alternative splicing to produce multiple isoforms with distinct cellular localizations.
Brain Expression
Clusterin is widely expressed throughout the brain:
-
Hippocampus — highest expression in CA1-CA3 pyramidal neurons and dentate gyrus granule cells
-
Cerebral cortex — strong expression in layers II-IV, particularly in pyramidal neurons
-
Basal ganglia — moderate expression in striatum
-
Cerebellum — expression in Purkinje cells
-
Brainstem and thalamus — lower but detectable expression
Cellular Distribution
In the brain, clusterin is produced by multiple cell types:
-
Neurons — principal producers in the healthy brain, both as secreted and nuclear isoforms
-
Astrocytes — significantly upregulated in reactive astrocytes in AD and other pathological conditions
-
Oligodendrocytes — associated with myelin sheaths
-
Microglia — increased expression in activated microglia
Expression data is available from the Allen Human Brain Atlas.
Allen Brain Atlas Data
Gene Expression
Clusterin (CLU) shows widespread expression in the brain:
-
Neurons - High expression in pyramidal neurons throughout cortex and hippocampus
-
Astrocytes - Strong expression in reactive astrocytes in AD
-
Oligodendrocytes - Moderate expression
-
Microglia - Upregulated in activated microglia
Single-Cell Expression
Single-cell RNA-seq data from the Allen Brain Atlas shows:
-
Excitatory neurons - High expression
-
Inhibitory neurons - Moderate expression
-
Astrocytes - Variable, higher in reactive states
-
Microglia - Increased in disease states
Brain Region Expression Levels
| Region | Expression Level | Data Source |
|---|---|---|
| Cortex | Very High | Human MTG |
| Hippocampus | Very High | Mouse Brain |
| Cerebellum | High | Mouse Brain |
| Striatum | Medium | Mouse Brain |
External Resources
Protein Structure and Function
Domain Architecture
Clusterin is a 449-amino acid glycoprotein with distinct structural domains:
-
Signal Peptide (1-22) — Enables secretion via the classical secretory pathway
-
N-terminal Domain (23-227) — Contains complement-binding regions (CBRs) that interact with complement proteins. This domain is responsible for the complement regulatory function of clusterin.
-
C-terminal Domain (228-427) — The chaperone activity domain that binds misfolded proteins including Aβ. Contains a methionine-rich region that contributes to antioxidant properties.
-
Heavily Glycosylated Regions — Five N-linked glycosylation sites are essential for secretion, stability, and function.
Post-translational Modifications
Clusterin undergoes several important post-translational modifications:
-
Glycosylation — Essential for secretion and function; affects protein stability and receptor interactions
-
Proteolytic Cleavage — The secreted form is cleaved at position 205 to generate alpha (23-205) and beta (206-449) subunits that are linked by disulfide bonds
-
Phosphorylation — Affects receptor interactions and cellular signaling
Alternative Splicing and Isoforms
Multiple isoforms of clusterin exist:
-
Secreted Clusterin (sCLU) — The predominant form, secreted into extracellular fluids including cerebrospinal fluid (CSF) and plasma
-
Nuclear Clusterin (nCLU) — Alternative splicing produces an intracellular isoform (lacking the signal peptide) that localizes to the nucleus and has pro-apoptotic functions
Normal Physiological Functions
Lipid Transport
As an apolipoprotein, clusterin participates in:
-
Cholesterol transport — Mediates reverse cholesterol transport from peripheral tissues to the liver
-
Lipid droplet formation — Associates with lipid storage organelles
-
Membrane repair — Facilitates plasma membrane damage repair
-
Myelin maintenance — Supports oligodendrocyte function and myelin integrity
Complement Regulation
Clusterin is a potent regulator of the complement system:
-
Complement inhibition — Binds to C5b-7 and C5b-8 complexes, preventing formation of the membrane attack complex
-
Inflammatory modulation — Reduces complement-mediated inflammatory damage in the brain
Apoptosis Regulation
Clusterin inhibits both caspase-dependent and caspase-independent cell death pathways:
-
Intrinsic pathway — Blocks Bax translocation to mitochondria, preventing cytochrome c release
-
Extrinsic pathway — Inhibits caspase-8 activation
-
ER stress — Modulates the unfolded protein response
-
Necroptosis — Reduces MLKL phosphorylation
Molecular Chaperone Activity
The defining function of clusterin is its ability to act as a molecular chaperone:
-
Binds to misfolded proteins to prevent aggregation
-
Prevents toxic oligomer formation
-
Facilitates clearance of aberrant proteins through receptor-mediated endocytosis
Ferroptosis Protection
Emerging research has identified clusterin as a key protector against ferroptosis, an iron-dependent form of programmed cell death 2Clusterin protects against ferroptosis in Alzheimer's diseaseOpen reference:
-
Lipid Peroxidation Inhibition — Clusterin scavenges lipid reactive oxygen species (ROS)
-
Iron Metabolism — Modulates cellular iron homeostasis through ferritin regulation
-
GPX4 Interaction — May support glutathione peroxidase 4 (GPX4) function
-
Neuroprotection — Prevents iron-induced neuronal death in AD models
Mitochondrial Function
Clusterin supports mitochondrial health:
-
Mitochondrial Membrane Stability — Preserves mitochondrial membrane potential
-
ATP Production — Supports optimal mitochondrial function
-
Apoptosis Prevention — Blocks mitochondrial apoptosis pathways
-
Mitophagy Regulation — Modulates removal of damaged mitochondria
-
Autophagy Regulation — Clusterin regulates autophagy and lysosomal function in AD, supporting clearance of protein aggregates 3Clusterin regulates autophagy and lysosomal function in Alzheimer's diseaseOpen reference
APOE-Dependent Effects
Clusterin interacts with APOE in an isoform-dependent manner:
-
ApoE4 carriers show reduced clusterin-mediated Aβ clearance compared to ApoE3
-
Combined APOE4 and specific CLU variants have synergistic effects on AD risk
-
Clusterin may compensate for reduced ApoE4 function in Aβ clearance 4ApoE isoform-dependent effects of clusterin on amyloid-beta aggregationOpen reference
Disease Associations
Alzheimer’s Disease — GWAS Evidence
CLU was identified as an AD risk locus in the landmark 2009 GWAS meta-analysis, representing one of the first novel loci beyond APOE to reach genome-wide significance 1Genome-wide association study identifies variants at CLU and CR1 associatedOpen reference5Genome-wide analysis of genetic loci associated with Alzheimer diseaseOpen reference. The association has been robustly replicated across multiple independent cohorts.
Key Genetic Variants
-
rs11136000 — The lead protective variant, located in an intronic region. The protective T allele is associated with reduced AD risk (OR ~0.86). This variant affects CLU expression levels through an expression quantitative trait locus (eQTL) effect.
-
rs2279590 — An eQTL variant that affects CLU expression in brain tissue
-
rs42039 — A coding variant that may influence protein function
These variants are associated with altered CLU expression, with protective alleles associated with higher clusterin levels. This suggests that increased clusterin expression is protective against AD, consistent with its role in Aβ clearance.
Population Genetics
-
European ancestry — rs11136000-T allele frequency ~57% (protective)
-
Asian ancestry — Similar patterns but somewhat weaker LD
-
African ancestry — Different allele frequencies
Amyloid-beta Clearance
Clusterin plays a critical role in clearing amyloid-beta from the brain through multiple mechanisms 6Clusterin in Alzheimer''s disease: Mechanisms and therapeutic potentialOpen reference7Clusterin promotes amyloid clearance and the blood-brain barrierOpen reference:
-
Chaperone Activity — Clusterin’s beta chain binds Aβ peptides with high affinity, preventing their aggregation into toxic oligomers and plaques. This interaction is one of the most important therapeutic mechanisms being explored.
-
Receptor-mediated Uptake — Clusterin-Aβ complexes are cleared through LRP-1 and LRP-2 (megalin) receptor-mediated endocytosis at the blood-brain barrier (BBB), facilitating transport out of the CNS.
-
Proteolytic Degradation — Clusterin facilitates Aβ degradation by matrix metalloproteinases (MMPs) and other proteases.
-
Perivascular Drainage — Clusterin-Aβ complexes exit the brain via perivascular lymphatic drainage pathways, a major route for Aβ clearance.
Tau Pathology
Clusterin interacts with tau at multiple levels:
-
Tau Binding — Clusterin directly binds to phosphorylated tau, influencing its aggregation propensity
-
Tau Secretion — Neuronal release of tau is facilitated by clusterin, potentially enabling propagation of pathology
-
Oligomer Neutralization — Clusterin neutralizes toxic tau oligomers before fibril formation
-
Clearance Enhancement — Promotes extracellular tau clearance through proteolytic degradation
Synaptic Protection
Clusterin protects synaptic function in several ways:
-
Synaptic Membrane Stability — Stabilizes lipid rafts at synaptic membranes
-
Oxidative Stress Protection — Scavenges reactive oxygen species through its methionine-rich domain
-
Calcium Homeostasis — Modulates calcium signaling in neurons
-
Synaptic Plasticity — Supports long-term potentiation and memory consolidation
Neuroinflammation Regulation
Clusterin modulates neuroinflammatory responses 8"Clusterin mediates A\u03B2-induced neuroinflammation through NF-\u03BA\Open reference:
-
Complement Regulation — Inhibits complement activation, reducing inflammatory damage
-
Cytokine Modulation — Regulates production of pro-inflammatory cytokines
-
Microglial Activation — Influences microglial phenotype and phagocytic activity
-
Peripheral Immune Cell Trafficking — Modulates immune cell entry into the CNS
-
NF-κB Pathway Modulation — Clusterin-Aβ complexes activate anti-inflammatory signaling through NF-κB pathway inhibition
Other Neurodegenerative Diseases
Huntington’s Disease
-
Mutant huntingtin promotes clusterin aggregation
-
Clusterin may help clear mutant huntingtin aggregates
-
Altered expression in HD brains
ALS and Frontotemporal Dementia
-
Clusterin inclusions found in motor neurons of ALS patients
-
Elevated clusterin in cerebrospinal fluid of ALS patients
-
Genetic variants may modify disease progression
Prion Disease
-
Clusterin is upregulated in serum and CSF in Creutzfeldt-Jakob disease
-
May serve as a biomarker for prion diseases
Biomarker Potential
Clusterin has significant potential as a biomarker for Alzheimer’s disease 9Clusterin as a biomarker and therapeutic target in neurodegenerative diseaseOpen reference:
Cerebrospinal Fluid (CSF) Clusterin
-
Elevated in AD patients compared to controls
-
Correlates with disease severity and progression
-
Levels correlate with other AD biomarkers including Aβ42, total tau, and phosphorylated tau
-
Genetic variation in CLU associates with CSF biomarker levels in preclinical AD 2Clusterin protects against ferroptosis in Alzheimer's diseaseOpen reference0
Plasma Clusterin
-
Associated with brain atrophy rates in AD
-
May predict conversion from mild cognitive impairment (MCI) to AD
-
Combined with other biomarkers improves diagnostic accuracy
-
Circulating clusterin shows promise for early AD detection 2Clusterin protects against ferroptosis in Alzheimer's diseaseOpen reference1
Clinical Applications
-
AD Biomarker Panel — Combined with Aβ42, tau, and p-tau improves diagnostic accuracy
-
Disease Progression Marker — Tracks cognitive decline over time
-
Treatment Response — Monitors therapeutic efficacy
-
At-risk Identification — Identifies preclinical AD in combination with other markers
Therapeutic Implications
Clusterin-based Therapies
Recombinant clusterin (rCLU) is being developed as a therapeutic agent:
-
Aβ Clearance — rCLU enhances amyloid clearance in preclinical models
-
Neuroprotection — Protects neurons from multiple insults
-
Blood-Brain Barrier Delivery — Crosses BBB, enabling CNS delivery
Gene Therapy Approaches
-
CLU Overexpression — AAV-mediated CLU delivery to enhance neuroprotection
-
CRISPR Editing — Correct CLU variants associated with increased AD risk
-
Small Molecule Inducers — Pharmacological agents that increase clusterin expression
Small Molecule Mimetics
-
Peptide Mimetics — Small molecules mimicking clusterin’s chaperone function
-
Chaperone Enhancers — Compounds that enhance clusterin’s Aβ-binding affinity
Brain Network Connectivity
Recent neuroimaging studies have revealed that CLU genetic variants influence brain network connectivity in AD 2Clusterin protects against ferroptosis in Alzheimer's diseaseOpen reference2:
Default Mode Network (DMN) Effects
-
Reduced Connectivity — CLU risk variants associated with decreased DMN connectivity
-
Amyloid Relationship — Effects amplified in amyloid-positive individuals
-
Clinical Correlation — Network changes correlate with cognitive performance
Tau-Clusterin Interaction
-
PET Imaging Studies — CSF clusterin correlates with amyloid PET SUVr in preclinical AD 2Clusterin protects against ferroptosis in Alzheimer's diseaseOpen reference3
-
Network Dysfunction — Combined tau and clusterin pathology leads to greater network disruption
Astrocyte-Microglia Crosstalk
Clusterin plays a critical role in mediating astrocyte-microglia communication 2Clusterin protects against ferroptosis in Alzheimer's diseaseOpen reference4:
Astrocyte-Derived Clusterin
-
Microglial Activation Modulation — Astrocyte clusterin regulates microglial phenotype
-
Neuroinflammatory Balance — Controls the pro-inflammatory vs. anti-inflammatory microglial states
-
Phagocytic Enhancement — Promotes microglia-mediated clearance of Aβ
Therapeutic Implications
-
Targeting Astrocyte Clusterin — Enhancing astrocyte clusterin production may reduce neuroinflammation
-
Combination Therapy — Clusterin enhancers with anti-amyloid antibodies may improve efficacy
Relationship to Other AD Risk Genes
CLU interacts with several other AD risk genes:
-
APOE — Both are apolipoproteins involved in lipid transport and Aβ clearance; they may have synergistic effects
-
PICALM — Both were identified in the same GWAS and are involved in endocytic pathways
-
BIN1 — Another GWAS gene involved in endocytosis; may converge on similar pathways
-
CR1 — Another complement-related gene identified in the same GWAS
Brain Atlas Resources
Brain Region Expression Levels
| Region | Expression Level | Data Source |
|---|---|---|
| Hippocampus | High | Human MTG |
| Cortex | High | Human MTG |
| Corpus callosum | High | Mouse Brain |
| Cerebellum | Medium | Mouse Brain |
| Substantia nigra | Medium | Mouse Brain |
See Also
External Links
References
- Genome-wide association study identifies variants at CLU and CR1 associated
- Clusterin protects against ferroptosis in Alzheimer's disease
- Clusterin regulates autophagy and lysosomal function in Alzheimer's disease
- ApoE isoform-dependent effects of clusterin on amyloid-beta aggregation
- Genome-wide analysis of genetic loci associated with Alzheimer disease
- Clusterin in Alzheimer''s disease: Mechanisms and therapeutic potential
- Clusterin promotes amyloid clearance and the blood-brain barrier
- "Clusterin mediates A\u03B2-induced neuroinflammation through NF-\u03BA\
- Clusterin as a biomarker and therapeutic target in neurodegenerative disease
- Genetic variation in CLU associates with cerebrospinal fluid biomarkers
- Circulating clusterin as a potential biomarker for early Alzheimer's disease
- Clusterin genetic variants and brain network connectivity in Alzheimer's
- Cerebrospinal fluid clusterin correlates with amyloid PET SUVr in preclinical
- Astrocyte-derived clusterin modulates microglia-mediated neuroinflammation
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