CASP12 Gene — Cysteine-Containing Aspartate-Specific Protease 12

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CASP12 Gene — Cysteine-Containing Aspartate-Specific Protease 12

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<div class="infobox infobox-gene">
<div class="infobox-header">CASP12 — Cysteine-Containing Aspartate-Specific Protease 12</div>

| Attribute | Value |
|-----------|-------|
| Gene Symbol | CASP12 |
| Full Name | Cysteine-Containing Aspartate-Specific Protease 12 |
| Chromosomal Location | 11q22.3 |
| NCBI Gene ID | 100506658 |
| Ensembl ID | ENSG00000244045 |
| UniProt ID | Q9Y252 |
| Gene Type | Protein coding |
| OMIM | 602394 |
| Protein Length | 341 amino acids |
| Expression | Primarily in brain, muscle, and peripheral tissues |
</div>

CASP12 Gene — Cysteine-Containing Aspartate-Specific Protease 12

Overview

CASP12 encodes caspase-12, a member of the cysteine-aspartic protease (caspase) family that plays a specialized role in endoplasmic reticulum (ER) stress-induced apoptosis. Unlike the executioner caspases (caspase-3, -6, -7) that execute the final stages of programmed cell death, caspase-12 functions as an initiator caspase specifically activated by ER stress signals rather than death receptor pathways [@nakagawa2000].

The CASP12 gene exhibits a remarkable population genetics characteristic: while functional caspase-12 is expressed in individuals of African descent, most other populations harbor a polymorphic variant that introduces a premature stop codon, resulting in a truncated, non-functional protein [@fischer2002]. This geographic distribution of CASP12 expression has significant implications for understanding variability in ER stress-related neuronal vulnerability across populations.

...

<div class="infobox infobox-gene">
<div class="infobox-header">CASP12 — Cysteine-Containing Aspartate-Specific Protease 12</div>

| Attribute | Value |
|-----------|-------|
| Gene Symbol | CASP12 |
| Full Name | Cysteine-Containing Aspartate-Specific Protease 12 |
| Chromosomal Location | 11q22.3 |
| NCBI Gene ID | 100506658 |
| Ensembl ID | ENSG00000244045 |
| UniProt ID | Q9Y252 |
| Gene Type | Protein coding |
| OMIM | 602394 |
| Protein Length | 341 amino acids |
| Expression | Primarily in brain, muscle, and peripheral tissues |
</div>

CASP12 Gene — Cysteine-Containing Aspartate-Specific Protease 12

Overview

CASP12 encodes caspase-12, a member of the cysteine-aspartic protease (caspase) family that plays a specialized role in endoplasmic reticulum (ER) stress-induced apoptosis. Unlike the executioner caspases (caspase-3, -6, -7) that execute the final stages of programmed cell death, caspase-12 functions as an initiator caspase specifically activated by ER stress signals rather than death receptor pathways [@nakagawa2000].

The CASP12 gene exhibits a remarkable population genetics characteristic: while functional caspase-12 is expressed in individuals of African descent, most other populations harbor a polymorphic variant that introduces a premature stop codon, resulting in a truncated, non-functional protein [@fischer2002]. This geographic distribution of CASP12 expression has significant implications for understanding variability in ER stress-related neuronal vulnerability across populations.

Gene Structure and Evolution

Genomic Organization

The CASP12 gene spans approximately 30 kb on chromosome 11q22.3. The gene structure includes:

Exon 1: Encodes the prodomain with the caspase recruitment domain (CARD)
Exons 2-6: Encode the catalytic domains (p20 and p10 subunits)

Evolutionary Context

Caspase-12 represents an evolutionary adaptation specific to primates. Rodents possess multiple caspase-12-like genes, while only a single functional CASP12 gene exists in humans. This suggests that caspase-12 function has been conserved despite the major structural changes between species.

Polymorphism and Population Genetics

The C125X polymorphism (rs497116) creates a premature stop codon in the CARD domain, resulting in a truncated protein that cannot be activated. Population studies reveal:

African populations: ~60-80% express functional caspase-12
European populations: ~5-10% express functional caspase-12
Asian populations: ~10-20% express functional caspase-12

This polymorphism has been the subject of extensive research regarding its implications for neurodegenerative disease susceptibility.

Protein Structure

Domain Architecture

Caspase-12 is a typical inactive zymogen consisting of:

Prodomain (1-95 aa): Contains the CARD domain required for recruitment to the ER membrane and interaction with adaptor proteins

Large Subunit (p20, 96-200 aa): Contains the catalytic cysteine residue and substrate-binding pocket

Small Subunit (p10, 201-341 aa): Completes the catalytic domain structure

Activation Mechanism

Unlike other caspases, caspase-12 activation is not mediated by cleavage but rather by:

Dissociation from the ER membrane under stress conditions
Formation of active caspase-12 tetramers
Autocatalytic processing

The CARD domain mediates homotypic interactions with proteins containing similar domains, including:

RIP-associated ICH-1 homologous protein with a CARD domain (RAIDD)
ER stress-specific adaptor proteins

Normal Physiological Function

ER Stress Response

Under normal physiological conditions, caspase-12 is maintained in an inactive state bound to the ER membrane. The protein is activated when cells experience ER stress, a condition characterized by:

Accumulation of unfolded or misfolded proteins
Disruption of calcium homeostasis
Glucose deprivation

The three major ER stress pathways (IRE1, PERK, ATF6) converge to regulate caspase-12 activation through both direct and indirect mechanisms.

Inflammatory Caspase Function

Caspase-12 also functions as an inflammatory caspase, distinct from its pro-apoptotic role:

Can be activated by necrotic cell release
Contributes to the inflammatory response following tissue injury
May interact with the NLRP3 inflammasome

Tissue-Specific Expression

Caspase-12 expression is highest in:

Brain: Neurons and glia, particularly vulnerable to ER stress
Muscle: Skeletal and cardiac muscle with high protein turnover
Pancreas: Cells with intensive secretory activity
Immune cells: Macrophages and dendritic cells

Role in Endoplasmic Reticulum Stress

ER Stress Pathways

The endoplasmic reticulum is the primary site for protein folding, lipid synthesis, and calcium storage. Disruption of ER homeostasis triggers the unfolded protein response (UPR), a complex signaling network that attempts to restore equilibrium.

Three ER transmembrane sensors coordinate the UPR:

IRE1 (Inositol-requiring enzyme 1): Activates XBP1 splicing and ASK1-JNK pathway

PERK (PKR-like ER kinase): Phosphorylates eIF2α to attenuate translation

ATF6 (Activating transcription factor 6): Cleaved to produce a transcription factor

Caspase-12 Activation by ER Stress

Caspase-12 is activated specifically by ER stress through multiple mechanisms:

Direct activation by IRE1: TheASK1-JNK pathway can activate caspase-12

Calcium-mediated activation: ER calcium release activates m-calpain, which can cleave and activate caspase-12

Proteolytic activation: Caspase-4 (the ER-resident caspase in rodents) can activate caspase-12

ER Stress-Induced Apoptosis

When ER stress cannot be resolved, the UPR switches from pro-survival to pro-apoptotic signaling:

CHOP transcription factor: Induced by all three UPR branches, promotes apoptosis through:

Downregulation of anti-apoptotic BCL-2
Upregulation of GADD34 (PP1 phosphatase cofactor)
ERO1α expression (oxidizes ER calcium channels)

Caspase cascade activation:

Caspase-12 activation initiates the apoptotic cascade
Caspase-9 is subsequently activated (mitochondrial-dependent pathway)
Caspase-3 executioner caspase completes the death program

Role in Alzheimer's Disease

ER Stress in AD Pathogenesis

Alzheimer's disease (AD) is characterized by:

Extracellular amyloid-beta (Aβ) plaque accumulation
Intracellular neurofibrillary tangles composed of hyperphosphorylated tau
Synaptic loss and neuronal death

ER stress is prominently implicated in AD pathogenesis through multiple mechanisms:

Aβ-induced ER stress: Soluble oligomers and fibrillar Aβ directly induce ER stress in neurons [@selznick2000]

Tau pathology: ER stress promotes tau phosphorylation and aggregation through GSK3β activation

Presenilin mutations: FAD-linked presenilin mutations impair ER calcium homeostasis, sensitizing neurons to ER stress

Caspase-12 in AD Brains

Immunohistochemical studies demonstrate:

Increased caspase-12 expression in AD brains compared to age-matched controls
Caspase-12 localizes to neurons in vulnerable regions (hippocampus, entorhinal cortex)
Active caspase-12 is present in proximity to amyloid plaques

Mechanisms of Neuronal Death

In populations expressing functional caspase-12, the enzyme contributes to AD-related neuronal loss through:

Direct cleavage of neuronal proteins: Substrates include:

Anti-apoptotic proteins (BCL-2, XIAP)
Structural proteins (actin, tubulin)
Signaling molecules (AKT, MAPK)

Amplification of the apoptotic cascade: Caspase-12 activates downstream caspases

Synaptic dysfunction: ER stress and caspase activation contribute to synaptic loss before cell death

Tau pathology acceleration: Caspase-12 can cleave tau, promoting its aggregation [@fernandes2016]

Therapeutic Implications for AD

The presence or absence of functional caspase-12 has implications for therapeutic strategies:

Caspase-12 inhibitors: Pharmacological inhibitors are being developed for populations expressing functional caspase-12

ER stress modulators: Compounds that reduce ER stress (e.g., TUDCA, sodium valproate) may attenuate caspase-12 activation

Population-specific approaches: Clinical trials may need stratification based on CASP12 genotype

Role in Parkinson's Disease

ER Stress in PD Pathogenesis

Parkinson's disease (PD) is characterized by:

Loss of dopaminergic neurons in the substantia nigra
Intraneuronal Lewy bodies (α-synuclein aggregates)
Mitochondrial dysfunction and oxidative stress

ER stress is increasingly recognized as a key contributor to PD pathology:

UPR activation detected in PD brains
ER stress markers elevated in substantia nigra
Genetic forms of PD (LRRK2, GBA) associated with ER stress

Caspase-12 Activation in PD Models

In PD models:

MPTP/MPP+ treatment induces caspase-12 activation in dopaminergic neurons [@holtz2005]
α-Synuclein overexpression triggers ER stress and caspase-12 cleavage
Mitochondrial toxins activate the ER stress pathway

Mechanisms

Caspase-12 contributes to dopaminergic neuron death through:

ER-mitochondrial cross-talk: Caspase-12 activation affects mitochondrial permeability

Calcium dysregulation: ER stress releases calcium that accumulates in mitochondria

Pro-inflammatory signaling: Caspase-12 can activate inflammatory pathways

Therapeutic Considerations

ER stress-targeted therapies for PD may be particularly relevant:

Caspase inhibitors: broad-spectrum and caspase-12 selective inhibitors
ER stress modulators: TUDCA, salubrinal
Autophagy enhancers: Reduce ER stress负荷

Role in Stroke and Cerebral Ischemia

Ischemic Injury and ER Stress

Cerebral ischemia triggers severe ER stress in neurons:

Energy failure disrupts protein folding
Calcium homeostasis disrupted
Oxidative stress damages ER function

Caspase-12 in Stroke

Caspase-12 plays a significant role in post-ischemic neuronal death:

Activated within hours of stroke onset
Contributes to delayed neuronal death (days after initial injury)
Mediates both caspase-dependent and independent pathways

Evidence from Models

In rodent stroke models:

Caspase-12 deficiency is neuroprotective
Caspase-12 inhibitors reduce infarct size
Antiapoptotic strategies targeting ER stress improve outcomes

Human Relevance

In human stroke:

Caspase-12 expression elevated in affected brain regions
Caspase-12 activation correlates with injury severity
The polymorphism may influence stroke outcomes

Role in Other Neurodegenerative Diseases

Amyotrophic Lateral Sclerosis (ALS)

ER stress is a prominent feature of ALS pathogenesis:

Mutant SOD1 proteins cause ER stress
C9orf72 repeats trigger ER stress
Caspase-12 activation observed in ALS models and human tissue [@hitomi2004]

Huntington's Disease

ER stress contributes to neuronal dysfunction in HD:

Mutant huntingtin protein causes ER stress
Caspase-12 may contribute to selective vulnerability
ER stress modulators show promise in models

Multiple Sclerosis

In demyelinating diseases:

ER stress in oligodendrocytes contributes to demyelination
Caspase-12 may be involved in oligodendrocyte death
Inflammation triggers ER stress in neural cells

Therapeutic Targeting

Caspase-12 Inhibitors

Several approaches are being developed:

Peptide inhibitors: Caspase-12 selective tetrapeptides

Small molecule inhibitors: Non-peptide compounds targeting the catalytic site

Natural compounds: Flavonoids and polyphenols with caspase-modulating activity

ER Stress Modulators

Broader strategies targeting ER stress include:

Chemical chaperones: TUDCA, sodium phenylbutyrate

Proteostasis enhancers: Autophagy inducers, proteasome modulators

Calcium stabilizers: Dantrolene (reduces ER calcium release)

Gene Therapy Approaches

Future directions include:

RNA interference to reduce caspase-12 expression
CRISPR-based gene editing
Viral delivery of protective factors

Challenges

Key challenges include:

Selectivity over other caspases (especially caspase-4 in rodents)
Blood-brain barrier penetration
Patient selection based on CASP12 genotype

Research Directions and Future Perspectives

Biomarker Development

Research is focused on:

Detecting caspase-12 activation in cerebrospinal fluid
Neuroimaging markers of ER stress
Genetic screening for CASP12 polymorphisms

Mechanistic Studies

Ongoing research aims to:

Identify novel caspase-12 substrates
Understand cell type-specific vulnerability
Map caspase-12 interactions in the neuronal interactome

Clinical Translation

The path to clinical application includes:

Development of selective inhibitors
Identification of patient subgroups
Combination with other disease-modifying approaches

Key Publications

Nakagawa T, Zhu H, Morishima N, et al. Caspase-12 mediates endoplasmic-reticulum-specific apoptosis and cytotoxicity by amyloid-beta. Nature. 2000;403(6765):98-103. PMID: 10638761(https://pubmed.ncbi.nlm.nih.gov/10638761/)

Selznick LA, Zhang J, Han X, et al. Caspase-12 is localized to the endoplasmic reticulum and mediates amyloid-beta induced neuronal apoptosis. J Neuropathol Exp Neurol. 2000;59(9):766-775. PMID: 11089579(https://pubmed.ncbi.nlm.nih.gov/11089579/)

Fischer H, Koenig U, Eckhart L, et al. Human caspase 12: a novel caspase related to the executioner caspases but located in the endoplasmic reticulum. Proc Natl Acad Sci U S A. 2002;99(9):5953-5958. PMID: 12417750(https://pubmed.ncbi.nlm.nih.gov/12417750/)

Moubarak RS, Zong WX, Dargusch C, et al. The death-associated protein kinase 2 is upstream of caspase-12 activation in endoplasmic reticulum stress induced apoptosis. Cell Death Differ. 2007;14(5):1049-1059. PMID: 16865286(https://pubmed.ncbi.nlm.nih.gov/16865286/)

Liu J, Wang Y, Song L, et al. Endoplasmic reticulum stress and caspase-12 in neurodegeneration: a double-edged sword. J Neuroinflammation. 2021;18(1):22. PMID: 33627112(https://pubmed.ncbi.nlm.nih.gov/33627112/)

Hitomi J, Katada T, Xie Y, et al. Endoplasmic reticulum stress and caspase activation in sporadic amyotrophic lateral sclerosis. J Neurochem. 2004;89(3):732-741. PMID: 15313203(https://pubmed.ncbi.nlm.nih.gov/15313203/)

Soane L, Siegel SM, Niculescu T, et al. The role of endoplasmic reticulum stress in neurodegenerative diseases. Antioxid Redox Signal. 2008;10(3):497-510. PMID: 18214852(https://pubmed.ncbi.nlm.nih.gov/18214852/)

Sokka AL, Putkonen N, Mudo G, et al. Endoplasmic reticulum stress inhibition ameliorates tau pathology and prevents memory deficit. J Neurosci. 2007;27(35):9094-9104. PMID: 17686974(https://pubmed.ncbi.nlm.nih.gov/17686974/)

Deegan S, Saveljeva S, Gorman AM, et al. ER stress-induced cell death: The role of mitochondria and the BCL-2 family. Methods Mol Biol. 2019;1917:67-86. PMID: 30555038(https://pubmed.ncbi.nlm.nih.gov/30555038/)

Samali A, Fitzgerald U, Deegan S, et al. Methods for measuring ER stress and apoptosis in cell models. Methods. 2010;50(1):11-17. PMID: 20176147(https://pubmed.ncbi.nlm.nih.gov/20176147/)

External Links

[NCBI Gene*: [CASP12](https://www.ncbi.nlm.nih.gov/gene/100506658)](/institutions/nih)
[Ensembl*: [ENSG00000244045](https://www.ensembl.org/Homo_sapiens/Gene/Summary?g=ENSG00000244045)](/genes/ar)
[UniProt*: [Q9Y252](https://www.uniprot.org/uniprot/Q9Y252)](/entities/htt)
[GeneCards*: [CASP12](https://www.genecards.org/cgi-bin/carddisp.pl?gene=CASP12)](/institutions/cas)
[OMIM*: [602394](https://www.omim.org/entry/602394)](/entities/htt)

Brain Atlas Resources

[Allen Human Brain Atlas*: [Gene expression search](https://human.brain-map.org/microarray/search/show?search_term=CASP12)](/datasets/allen-human-brain-atlas)
[Allen Mouse Brain Atlas*: [G](/projects/brain-atlas)ene search](https://mouse.brain-map.org/search/index.html?query=CASP12)
Allen Cell Type Atlas: [Transcriptomic cell type reference](https://portal.brain-map.org/atlases-and-data/rnaseq)
BrainSpan Developmental Transcriptome: [Developmental expression](https://www.brainspan.org/rnaseq/search/index.html?search_term=CASP12)

References

breckenridge2003, Regulation of apoptosis by endoplasmic reticulum calcium and stress (2003)
choi2014, The role of ER stress in alpha-synucleinopathies (2014)
deegan2019, ER stress-induced cell death: The role of mitochondria and the BCL-2 family (2019)
dupont2010, Modeling of the activation and inhibition of caspase-12 by ER stress (2010)
fernandes2016, Caspase-12 deficiency exacerbates tau pathology and accelerates neurodegeneration (2016)
fischer2002, Human caspase 12: a novel caspase related to the executioner caspases but located in the endoplasmic reticulum (2002)
hitomi2004, Endoplasmic reticulum stress and caspase activation in sporadic amyotrophic lateral sclerosis (2004)
holtz2005, Oxidative stress-triggered unfolded protein response in dopaminergic neurons (2005)
kim2008, Cell death and endoplasmic reticulum stress: disease relevance and therapeutic opportunities (2008)
liu2021, Endoplasmic reticulum stress and caspase-12 in neurodegeneration: a double-edged sword (2021)
moubarak2007, The death-associated protein kinase 2 is upstream of caspase-12 activation in endoplasmic reticulum stress induced apoptosis (2007)
nakagawa2000, Caspase-12 mediates endoplasmic-reticulum-specific apoptosis and cytotoxicity by amyloid-beta (2000)
oh2012, Beta-amyloid oligomer induces ER stress-mediated apoptosis in neuronal cells (2012)
rao2011, Coupling endoplasmic reticulum stress to the cell death program: role of the ER chaperone GRP78 (2011)
samali2010, Methods for measuring ER stress and apoptosis in cell models (2010)
selznick2000, Caspase-12 is localized to the endoplasmic reticulum and mediates amyloid-beta induced neuronal apoptosis (2000)
soane2008, The role of endoplasmic reticulum stress in neurodegenerative diseases (2008)
sokka2007, Endoplasmic reticulum stress inhibition ameliorates tau pathology and prevents memory deficit (2007)
szegezdi2006, Caspase-12 and ER-stress mediated apoptosis: the story so far (2006)
urra2013, When ER stress reaches a dead end (2013)
yuan2019, ER stress induces tau pathology and cognitive deficits in Alzheimer's disease (2019)

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Related Entities

CASP12

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entity_type	gene
origin_type	v1_polymorphic_backfill
source_table	wiki_pages
wiki_page_id	wp-fc0b90c823be
__merged_from	{'merged_at': '2026-05-13', 'unprefixed_id': 'genes-casp12'}
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📊 Evidence Profile Foundational

Evidence Balance

+0%

Certainty

75%

Debates

0

Incoming

15

Outgoing

17

0 supporting 0 contradicting 0 neutral

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📗 Cite This Artifact

CASP12 Gene — Cysteine-Containing Aspartate-Specific Protease 12

CASP12 Gene — Cysteine-Containing Aspartate-Specific Protease 12

Overview

CASP12 Gene — Cysteine-Containing Aspartate-Specific Protease 12

Overview

Gene Structure and Evolution

Genomic Organization

Evolutionary Context

Polymorphism and Population Genetics

Protein Structure

Domain Architecture

Activation Mechanism

Normal Physiological Function

ER Stress Response

Inflammatory Caspase Function

Tissue-Specific Expression

Role in Endoplasmic Reticulum Stress

ER Stress Pathways

Caspase-12 Activation by ER Stress

ER Stress-Induced Apoptosis

Role in Alzheimer's Disease

ER Stress in AD Pathogenesis

Caspase-12 in AD Brains

Mechanisms of Neuronal Death

Therapeutic Implications for AD

Role in Parkinson's Disease

ER Stress in PD Pathogenesis

Caspase-12 Activation in PD Models

Mechanisms

Therapeutic Considerations

Role in Stroke and Cerebral Ischemia

Ischemic Injury and ER Stress

Caspase-12 in Stroke

Evidence from Models

Human Relevance

Role in Other Neurodegenerative Diseases

Amyotrophic Lateral Sclerosis (ALS)

Huntington's Disease

Multiple Sclerosis

Therapeutic Targeting

Caspase-12 Inhibitors

ER Stress Modulators

Gene Therapy Approaches

Challenges

Research Directions and Future Perspectives

Biomarker Development

Mechanistic Studies

Clinical Translation

Key Publications

See Also

External Links

Brain Atlas Resources

References

💬 Discussion