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HSPB7 Protein
Introduction
Hspb7 Protein is an important component in the neurobiology of neurodegenerative diseases. This page provides detailed information about its structure, function, and role in disease processes.
<div class="infobox infobox-protein"> <span class="infobox-title">HSPB7 Protein</span> | Property | Value | |----------|-------| | Protein Name | Heat Shock Protein Beta-7 (HspB7) | | Gene Symbol | HSPB7 | | UniProt ID | Q9UBW9 | | Molecular Weight | ~17 kDa | | Subcellular Location | Cytoplasm, Z-disc | | Protein Family | Small heat shock protein family | | Associated Diseases | Dilated Cardiomyopathy, Arrhythmogenic Cardiomyopathy, Myopathy | </div>
Overview
HSPB7 (Heat Shock Protein Beta-7) is a small heat shock protein expressed predominantly in cardiac and skeletal muscle. Unlike other sHSPs, HSPB7 has unique tissue distribution and is strongly associated with muscle disease. It forms a distinct branch of the small heat shock protein family with specialized functions in muscle protection[@wang2022].
Structure
The HSPB7 protein contains:
N-terminal domain: Short, divergent region
Alpha-crystallin domain: Core conserved region
C-terminal tail: Short extension
Structural Features
| Feature | Description | |---------|-------------| | Alpha-crystallin domain | ~80 aa conserved region | | Cysteine residues | Present in some isoforms | | Oligomerization | Forms heterooligomers | | Tissue specificity | Muscle-enriched |
Normal Function
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HSPB7 Protein
Introduction
Hspb7 Protein is an important component in the neurobiology of neurodegenerative diseases. This page provides detailed information about its structure, function, and role in disease processes.
<div class="infobox infobox-protein"> <span class="infobox-title">HSPB7 Protein</span> | Property | Value | |----------|-------| | Protein Name | Heat Shock Protein Beta-7 (HspB7) | | Gene Symbol | HSPB7 | | UniProt ID | Q9UBW9 | | Molecular Weight | ~17 kDa | | Subcellular Location | Cytoplasm, Z-disc | | Protein Family | Small heat shock protein family | | Associated Diseases | Dilated Cardiomyopathy, Arrhythmogenic Cardiomyopathy, Myopathy | </div>
Overview
HSPB7 (Heat Shock Protein Beta-7) is a small heat shock protein expressed predominantly in cardiac and skeletal muscle. Unlike other sHSPs, HSPB7 has unique tissue distribution and is strongly associated with muscle disease. It forms a distinct branch of the small heat shock protein family with specialized functions in muscle protection[@wang2022].
Structure
The HSPB7 protein contains:
N-terminal domain: Short, divergent region
Alpha-crystallin domain: Core conserved region
C-terminal tail: Short extension
Structural Features
| Feature | Description | |---------|-------------| | Alpha-crystallin domain | ~80 aa conserved region | | Cysteine residues | Present in some isoforms | | Oligomerization | Forms heterooligomers | | Tissue specificity | Muscle-enriched |
Muscle regeneration: Supports satellite cell function
Tissue-Specific Expression
HSPB7 is highly specific to:
Cardiac muscle: High expression in heart
Skeletal muscle: Particularly type 1 fibers
Low in other tissues: Distinguishes from other sHSPs
Partner Proteins
HSPB7 interacts with:
Alpha-B-crystallin (HSPB5)
HSPB8
Desmin cytoskeleton
Z-disc proteins
Molecular Mechanisms
Muscle Protection
HSPB7 protects muscle through:
Chaperone activity: Prevents aggregation
Cytoskeletal stabilization: Z-disc protection
Anti-[apoptosis](/entities/apoptosis): Blocks death pathways
[Autophagy](/entities/autophagy) regulation: Quality control
Cardiac Function
In the heart:
Essential for contractile function
Protects against stress-induced damage
Maintains sarcomere integrity
Prevents pathological remodeling
Disease Associations
Dilated Cardiomyopathy (DCM)
In DCM[@liu2022]:
HSPB7 mutations cause familial DCM
Loss-of-function mechanisms
Variable penetrance
Impaired cardiac function
Arrhythmogenic Cardiomyopathy (ACM)
In ACM:
Mutations in desmosome genes
HSPB7 as modifier
Disease progression
Sudden cardiac death risk
Myopathy
In muscle disease:
Rare HSPB7 mutations cause myopathy
Rimmed vacuolar pathology
Muscle weakness
Respiratory involvement
Neurodegeneration
While primarily muscle-expressed:
Some expression in neural tissue
Not strongly implicated in neurodegeneration
May have general chaperone functions
Expression Pattern
| Tissue | Expression | Notes | |--------|------------|-------| | Heart | Very high | Primary site | | Skeletal muscle | High | Type 1 fibers | | Brain | Very low | Limited | | Other organs | Minimal | Tissue-specific |
Therapeutic Targeting
| Strategy | Approach | Status | Notes | |----------|----------|--------|-------| | Gene Therapy | HSPB7 delivery | Research | Cardiomyopathy | | Small Molecules | Chaperone activity | Research | Enhancement | | Protein Therapy | Recombinant HSPB7 | Research | Acute treatment |
Challenges
Muscle-specific delivery
Protein stability
Appropriate dosing
Route of administration
Animal Models
Knockout Mice
Hspb7 knockout mice show:
Cardiac abnormalities
Reduced stress tolerance
Muscle pathology with age
Transgenic Models
HSPB7 overexpression protective
Improves cardiac function
Protects against injury
Zebrafish
Cardiac development studies
Muscle function models
Research Directions
Current research areas:
Gene therapy: AAV-HSPB7 for DCM
Mechanism studies: Structural analysis
Biomarkers: HSPB7 in disease diagnosis
Combination therapy: With other sHSPs
Patient stratification: Genetic testing
Background
The study of Hspb7 Protein has evolved significantly over the past decades. Research in this area has revealed important insights into the underlying mechanisms of neurodegeneration and continues to drive therapeutic development.
Historical context and key discoveries in this field have shaped our current understanding and will continue to guide future research directions.
See Also
HSPB7 Gene — HSPB7 gene
HSPB6 Protein — Related sHSP
HSPB5 Protein — Alpha-B-crystallin
[Heat Shock Proteins — Protein family](/content/proteins)](/proteins)