HDAC10 Protein

HDAC10 Protein

Overview

HDAC10 (Histone Deacetylase 10) is a member of the histone deacetylase family of enzymes, classified as a Class IIb HDAC. The HDAC10 gene is located on chromosome 12q13.1 and encodes a 561-amino acid protein that plays a regulatory role in protein acetylation homeostasis. Unlike many other HDACs, HDAC10 is primarily expressed in the cytoplasm rather than the nucleus, which distinguishes it functionally and subcellularly from other deacetylase family members. This unique localization has significant implications for its role in cellular processes relevant to neurodegeneration. HDAC10 has gained particular attention in neurodegenerative disease research due to its involvement in autophagy regulation, mitochondrial function, and protein quality control—all processes critically compromised in Alzheimer's disease, Parkinson's disease, and Huntington's disease.

Function and Biology

HDAC10 catalyzes the removal of acetyl groups from lysine residues on histone and non-histone protein substrates, thereby regulating protein-protein interactions, enzymatic activity, and subcellular localization. The enzyme contains a zinc-dependent deacetylase domain characteristic of all HDACs, enabling its catalytic function. As a Class IIb HDAC, HDAC10 operates within a specific regulatory context distinct from Class I nuclear deacetylases and Class IIa HDACs that shuttle between nucleus and cytoplasm.

HDAC10 Protein

Overview

HDAC10 (Histone Deacetylase 10) is a member of the histone deacetylase family of enzymes, classified as a Class IIb HDAC. The HDAC10 gene is located on chromosome 12q13.1 and encodes a 561-amino acid protein that plays a regulatory role in protein acetylation homeostasis. Unlike many other HDACs, HDAC10 is primarily expressed in the cytoplasm rather than the nucleus, which distinguishes it functionally and subcellularly from other deacetylase family members. This unique localization has significant implications for its role in cellular processes relevant to neurodegeneration. HDAC10 has gained particular attention in neurodegenerative disease research due to its involvement in autophagy regulation, mitochondrial function, and protein quality control—all processes critically compromised in Alzheimer's disease, Parkinson's disease, and Huntington's disease.

Function and Biology

HDAC10 catalyzes the removal of acetyl groups from lysine residues on histone and non-histone protein substrates, thereby regulating protein-protein interactions, enzymatic activity, and subcellular localization. The enzyme contains a zinc-dependent deacetylase domain characteristic of all HDACs, enabling its catalytic function. As a Class IIb HDAC, HDAC10 operates within a specific regulatory context distinct from Class I nuclear deacetylases and Class IIa HDACs that shuttle between nucleus and cytoplasm.

A defining functional feature of HDAC10 is its predominant cytoplasmic localization, mediated by a C-terminal nuclear export signal. This localization positions HDAC10 to regulate non-histone substrate proteins involved in cellular metabolism, organellar dynamics, and protein degradation pathways. HDAC10 interacts with various protein complexes and modulates the acetylation status of proteins including autophagy-related factors and metabolic enzymes. The enzyme shows relatively selective substrate specificity compared to broader-spectrum HDACs, making it a more specialized regulator within the deacetylase family.

Role in Neurodegeneration

HDAC10 has emerged as an important regulator in multiple neurodegenerative disease contexts. In Huntington's disease models, HDAC10 dysfunction has been linked to impaired autophagy and accumulation of mutant huntingtin protein aggregates. The polyglutamine expansions characteristic of Huntington's disease compromise autophagy-lysosomal pathways, and evidence suggests HDAC10 participates in regulating autophagy flux through acetylation of autophagy-related proteins.

In Parkinson's disease research, HDAC10 has been implicated in mitochondrial quality control and α-synuclein processing. Impaired HDAC10 activity may contribute to mitochondrial dysfunction and failure to clear damaged organelles, exacerbating neuronal vulnerability. In Alzheimer's disease models, HDAC10 alterations correlate with dysregulation of tau protein acetylation and amyloid-β processing, though the precise mechanistic connections remain under investigation.

Notably, HDAC10 appears particularly relevant to autophagy-dependent neuronal homeostasis, a process essential for clearing protein aggregates and damaged mitochondria—hallmarks of all major neurodegenerative diseases.

Molecular Mechanisms

HDAC10 regulates neurodegeneration-relevant pathways primarily through acetylation-mediated protein modifications. The enzyme deacetylates critical autophagy proteins, including components of the ULK1 complex and LC3-associated factors, thereby modulating autophagy initiation and progression. HDAC10 also deacetylates mitochondrial outer membrane proteins, influencing mitochondrial dynamics and mitophagy—selective removal of damaged mitochondria.

The protein interacts with chaperone-mediated autophagy components and influences the balance between proteasomal and lysosomal protein degradation. In cellular stress conditions relevant to neurodegeneration, HDAC10 activity patterns shift, potentially representing either adaptive responses or maladaptive dysregulation depending on disease context and severity.

Clinical and Research Significance

HDAC10 represents a therapeutic target of growing interest in neurodegeneration research. Unlike broad-spectrum HDAC inhibitors that produce widespread deacetylation changes, HDAC10-selective modulators could theoretically provide more targeted intervention. Several research groups have developed HDAC10-selective inhibitors to test whether specific enhancement of autophagy and mitochondrial quality control provides neuroprotection in disease models.

HDAC10 expression levels and activity show altered patterns in postmortem neurodegenerative disease tissues, suggesting biomarker potential. Polymorphisms in the HDAC10 gene may influence disease susceptibility or progression rates, though genome-wide association studies have not yet identified HDAC10 as a major genetic risk locus.

Related Entities

• HDAC family proteins: HDAC1, HDAC3, HDAC6 (particularly relevant for autophagy and cytoplasmic function)
• Autophagy machinery: ULK1, LC3, ATG proteins, p