Caspase-8 (CASP8)

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Caspase-8 (CASP8)

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Caspase-8 (CASP8)

Overview

Caspase-8 (encoded by the CASP8 gene) is the initiator caspase of the extrinsic apoptosis pathway, activated at death receptor complexes. As a member of the cysteine-aspartic protease family, caspase-8 plays a central role in transducing extracellular death signals into intracellular proteolytic events that execute programmed cell death [@muzio1996]. Its activation at the death-inducing signaling complex (DISC) triggers both the extrinsic apoptotic pathway (direct activation of executioner caspases) and the intrinsic mitochondrial pathway (via Bid cleavage). Beyond apoptosis, caspase-8 regulates necroptosis (by cleaving RIPK1 to prevent kinase-driven necrosis), influences cell proliferation and differentiation, and modulates immune cell activation and inflammation. Dysregulated caspase-8 activity contributes to cancer (insufficient activity allows tumor cell survival) and to neurodegenerative diseases (excessive activation causes neuronal death) [@kelley2001].

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Caspase-8 (CASP8)

Overview

Caspase-8 (encoded by the CASP8 gene) is the initiator caspase of the extrinsic apoptosis pathway, activated at death receptor complexes. As a member of the cysteine-aspartic protease family, caspase-8 plays a central role in transducing extracellular death signals into intracellular proteolytic events that execute programmed cell death [@muzio1996]. Its activation at the death-inducing signaling complex (DISC) triggers both the extrinsic apoptotic pathway (direct activation of executioner caspases) and the intrinsic mitochondrial pathway (via Bid cleavage). Beyond apoptosis, caspase-8 regulates necroptosis (by cleaving RIPK1 to prevent kinase-driven necrosis), influences cell proliferation and differentiation, and modulates immune cell activation and inflammation. Dysregulated caspase-8 activity contributes to cancer (insufficient activity allows tumor cell survival) and to neurodegenerative diseases (excessive activation causes neuronal death) [@kelley2001].

<div class="infobox infobox-protein">
<table>
<tr><th colspan="2">Caspase-8 Protein</th></tr>
<tr><td>Protein Name</td><td>Caspase-8 (FLICE, MACH)</td></tr>
<tr><td>Gene</td><td>[CASP8](/genes/casp8)</td></tr>
<tr><td>UniProt ID</td><td>[Q14790](https://www.uniprot.org/uniprot/Q14790)</td></tr>
<tr><td>Molecular Weight</td><td>~55 kDa (procaspase-8), ~43 kDa (active p18/p10)</td></tr>
<tr><td>Subcellular Localization</td><td>Cytoplasm, plasma membrane (DISC)</td></tr>
<tr><td>Protein Family</td><td>Caspase family (cysteine protease)</td></tr>
<tr>
<td class="label">Associated Diseases</td>
<td><a href="/wiki/aging" style="color:#ef9a9a">Aging</a>, <a href="/wiki/als" style="color:#ef9a9a">Als</a>, <a href="/wiki/alzheimer" style="color:#ef9a9a">Alzheimer</a>, <a href="/wiki/autoimmune" style="color:#ef9a9a">Autoimmune</a>, <a href="/wiki/cancer" style="color:#ef9a9a">Cancer</a></td>
</tr>
<tr>
<td class="label">KG Connections</td>
<td><a href="/atlas" style="color:#4fc3f7">153 edges</a></td>
</tr>
</table>
</div>

Structure

Caspase-8 is synthesized as a zymogen (procaspase-8) of 479 amino acids with a characteristic domain architecture:

Protein Domains

Death effector domain (DED1) (residues 1-100): N-terminal DED — mediates homotypic interactions with the adaptor protein FADD via DED-DED binding. Critical for DISC recruitment.

Death effector domain (DED2) (residues 100-200): Second DED — structural role, stabilizes the DED region. Mutations in DED2 can cause autoimmune lymphoproliferative syndrome (ALPS).

Linker region (residues 200-260): Flexible region containing the intersubunit cleavage site (Asp210, Asp216). Serves as the autocatalytic cleavage substrate.

Large subunit (p20) (residues 260-374): Contains the catalytic dyad (His277, Cys360) — histidine acts as the general base, cysteine is the nucleophile. Major determinant of substrate specificity.

Small subunit (p10) (residues 374-479): Completes the active site, contributes to substrate recognition. Contains the C-terminal cleavage site (Asp374) that separates p18 from p10.

Activation Mechanism

Procaspase-8 activation involves:

Dimerization: Two procaspase-8 molecules are brought into proximity at the DISC. Dimerization is the primary activation event — it occurs via the protease domain interface, not through the DEDs.

Intersubunit cleavage (Asp210, Asp216): Dimerization-induced conformational changes allow trans-processing at the linker sites, separating p18 from p10 within each molecule (but not yet separating the two subunits).

Autocatalytic processing (Asp374): Final cleavage at Asp374 separates the large and small subunits, generating the active p18/p10 heterotetramer. This is irreversible.

Active form: The active caspase-8 is a (p10)2-(p18)2 heterotetramer with two catalytic sites, released from the DISC into the cytoplasm.

Caspase-8 also exists in a stable (p43)1 form, generated by cleavage at Asp210, which remains associated with the DISC and may have non-apoptotic signaling functions.

Normal Function

Death Receptor Signaling Pathway

Caspase-8 is the central mediator of death receptor-initiated apoptosis [@tummers2007]:

Receptor activation: A death ligand (FasL, TNF-α, TRAIL) binds to its cognate receptor (Fas/CD95, TNFR1, DR4/DR5), inducing receptor trimerization or oligomerization [@holler2000]

Adaptor recruitment: The intracellular death domain (DD) of the activated receptor recruits FADD (Fas-associated via death domain) via DD-DD interactions

DISC formation: FADD recruits procaspase-8 via DED-DED interactions, forming the death-inducing signaling complex (DISC). This is the signaling hub for extrinsic apoptosis [@schleich2012]

Caspase-8 activation: Within the DISC, high local concentration of procaspase-8 drives dimerization and autoproteolytic activation

Substrate cleavage: Active caspase-8 is released from the DISC to cleave downstream substrates

Substrate Specificity

Caspase-8 has a preference for the tetrapeptide sequence (I/V/L)X(E/D)X(D/I) and cleaves many substrates:

Executioner caspases (caspase-3, -6, -7): Direct cleavage activates these effector caspases, which execute the apoptotic program
Bid: Cleavage of the BH3-only protein Bid generates tBid (truncated Bid), which translocates to mitochondria and induces cytochrome c release — this links extrinsic signaling to the intrinsic mitochondrial pathway
PARP: Cleavage of poly(ADP-ribose) polymerase inactivates DNA repair, committing the cell to death
Structural proteins: Lamin A/C, actin, beta-catenin — dismantling of cellular architecture
RIPK1: Cleavage separates the kinase domain from the death domain, preventing necroptosis

Regulation of Necroptosis

Caspase-8 is a critical suppressor of necroptosis [@liang2020]:

RIPK1 cleavage: Caspase-8 cleaves RIPK1 at Asp324, preventing the assembly of the necrosome (RIPK1-RIPK3-MLKL complex)
Switch function: Caspase-8 acts as a molecular switch between apoptosis (sufficient activity) and necroptosis (caspase-8 inhibited or absent)
Necroptosis in neurodegeneration: In some contexts, caspase-8 inhibition leads to necroptotic neuronal death, which is particularly inflammatory and damaging

Non-Apoptotic Functions

Cell proliferation: Caspase-8 activates NF-κB via the IKK complex, promoting cell survival and proliferation
T cell activation: Required for activation-induced cell death (AICD) in T lymphocytes
Embryonic development: Casp8 knockout mice die in utero with cardiac defects and impaired vascular development
Immune regulation: Modulates macrophage polarization and cytokine production

Role in Neurodegeneration

Alzheimer's Disease

Caspase-8 activation contributes to neuronal apoptosis in AD:

Aβ-induced activation: Amyloid-beta oligomers activate caspase-8 in cultured neurons and in AD brain tissue
Death receptor involvement: Fas/FasL signaling is upregulated in AD brain, contributing to caspase-8 activation
Synaptic damage: Caspase-8 cleavage of synaptic proteins (Arc, PSD95) may contribute to early synaptic dysfunction
Cross-talk with tau: Caspase-8 can activate executioner caspases that promote tau cleavage and aggregation
Therapeutic targeting: Caspase-8 inhibitors (z-IETD-fmk, specific peptides) reduce neuronal death in AD models

Parkinson's Disease

In PD, caspase-8 is activated in dopaminergic neurons undergoing degeneration:

Death receptor activation: Fas, TNF-R1, and DR4/DR5 are expressed on dopaminergic neurons and can activate caspase-8
Mitochondrial links: The Bid cleavage pathway connects extrinsic signaling to mitochondrial dysfunction, a hallmark of PD
Endoplasmic reticulum stress: ER stress triggers caspase-8 activation in dopaminergic neurons via mechanisms that remain partially characterized
Neuroinflammation: Microglial-derived TNF-α and FasL can activate caspase-8 in adjacent neurons

Glaucoma and Optic Neuropathy

Caspase-8 is activated in retinal ganglion cells (RGCs) during glaucomatous neurodegeneration [@booth2008]:

Axonal insult: Elevated intraocular pressure causes axonal transport disruption, leading to caspase-8 activation in RGCs
ProBDNF signaling: The p75NTR proBDNF pathway activates caspase-8 in retinal neurons
Therapeutic potential: Caspase-8 inhibition is neuroprotective in mouse models of glaucoma

Stroke and Ischemia

Ischemic brain injury prominently activates caspase-8:

Excitotoxicity: Glutamate-induced overactivation of NMDA receptors triggers caspase-8 activation
Fas/FasL upregulation: Ischemia induces Fas expression on neurons and FasL on endothelial cells and microglia
Dual pathways: Both direct caspase-8 activation (extrinsic) and Bid-mediated mitochondrial amplification (intrinsic) contribute to post-ischemic neuronal death

Huntington's Disease

Caspase-8 is activated in models of Huntington's disease:

Mutant huntingtin aggregation: Can trigger extrinsic apoptosis
Death receptor upregulation: Fas and TRAIL-R are increased in HD models
Bid cleavage: Contributes to mitochondrial dysfunction
Therapeutic targeting: Caspase-8 inhibition is protective in some models

Amyotrophic Lateral Sclerosis

Caspase-8 is activated in ALS models and patient tissue:

SOD1 mutations: Trigger caspase-8 activation in motor neurons
TDP-43 pathology: Associated with caspase-8 activation
Death receptor involvement: Fas signaling contributes to motor neuron death
Astrocyte contributions: Mutant astrocytes trigger caspase-8 in co-cultured neurons

Multiple Sclerosis

Caspase-8 has dual roles in autoimmune demyelination:

Oligodendrocyte death: Caspase-8 contributes to myelin loss
T cell activation: Required for activation-induced cell death (AICD)
Remyelination failure: Caspase-8 inhibition may protect oligodendrocyte progenitors

COVID-19 Neurological Complications

Emerging evidence links COVID-19 to caspase-8 activation:

Systemic inflammation: Cytokine storm includes TNF-α, activating caspase-8
Blood-brain barrier: FasL can disrupt BBB
Microglial activation: Caspase-8 in activated microglia

Molecular Mechanisms in Disease

Death Receptor Regulation in Neurodegeneration

The extrinsic pathway is regulated at multiple levels:

Receptor Expression

Death receptor expression is dynamic in disease:

Fas (CD95): Upregulated in AD, PD, HD, and stroke
TNF-R1: Increased in neuroinflammation
DR4/DR5 (TRAIL-R): Variable changes

Ligand Expression

FasL: Expressed on activated microglia, T cells, and some neurons
TNF-α: Released by activated microglia and astrocytes
TRAIL: Expressed in immune cells

Decoy Receptors

DcR1/DcR2: Decoy receptors that sequester ligands
Soluble Fas: Alternative splicing generates soluble Fas
Viral proteins: Some viruses express decoyDeath

c-FLIP Regulation

c-FLIP (CFLAR) is a master regulator of caspase-8:

c-FLIPL: Long isoform, catalytically inactive
c-FLIPS: Short isoform, dominant-negative
Regulation: c-FLIP is downregulated in some neurodegenerative conditions
Therapeutic potential: c-FLIP overexpression protects neurons

Bid Regulation in Neurodegeneration

Bid connects extrinsic and intrinsic pathways:

Full-length Bid: Inactive until cleaved by caspase-8
tBid: Truncated form, traffics to mitochondria
Mitochondrial amplification: tBid triggers cytochrome c release
Therapeutic targeting: Bid inhibitors block amplification

Non-Caspase Substrates

Caspase-8 cleaves substrates beyond executioner caspases:

| Substrate | Cleavage Consequence |
|-----------|---------------------|
| RIPK1 | Prevents necroptosis (protective) |
| ROCK1 | Alters cytoskeleton |
| MALT1 | Modulates NF-κB |
| p75NTR | Generates pro-apoptotic fragment |
| Presenilins | May affect γ-secretase |

Necroptosis Suppression

Caspase-8 is a critical suppressor of necroptosis:

RIPK1 cleavage: Prevents necrosome formation
RIPK3 binding: Blocks MLKL activation
Switch function: Low caspase-8 → necroptosis
Therapeutic implications: Caspase-8 inhibition can cause necroptosis

Therapeutic Targeting

Caspase-8 Inhibitors

| Inhibitor | Type | Specificity | Status |
|-----------|------|-------------|--------|
| z-IETD-fmk | Peptide mimetic | Caspase-8 specific | Research tool only |
| Ac-IETD-CHO | Peptide aldehyde | Caspase-8 specific | Research tool only |
| CrmA (SerpB) | Viral serpin | Caspase-8 and granzyme B | Research tool only |
| AEVD-fmk | Peptide | Broader caspase inhibitor | Research tool only |

Clinical challenge: Broad caspase inhibition risks immunosuppression and tumor promotion. Selective targeting of neuronal caspase-8 activation is difficult.

Alternative Approaches

Decoy receptors: Soluble Fas/Fc proteins that sequester FasL before it reaches the receptor
Death receptor blocking antibodies: Anti-Fas or anti-DR4/DR5 antibodies can block ligand binding
Upstream modulation: Reducing TNF-α or FasL production (anti-inflammatory approaches)
Bid inhibitors: Preventing Bid cleavage blocks the extrinsic-to-intrinsic amplification
RIPK1 inhibitors (Necrostatin-1, GSK'872): Indirectly prevent caspase-8-mediated necroptosis suppression

Neuroprotective Strategies

Rather than globally inhibiting caspase-8, more targeted approaches include:

Substrate-specific inhibitors: Blocking only harmful cleavages while preserving necessary functions
Cell-penetrating peptides: Targeting the DISC or specific neuronal populations
Gene therapy: siRNA or shRNA targeting CASP8 specifically in neurons
Combination: Low-dose caspase-8 inhibition + anti-inflammatory + anti-excitotoxic approaches

Protein Interactions

| Partner | Interaction Type | Functional Consequence |
|---------|----------------|----------------------|
| FADD | DED-DED binding | DISC recruitment, activation |
| Fas (CD95) | Indirect (via FADD) | Death receptor signaling |
| TNF-R1 | Indirect (via FADD) | TNF-α signaling |
| DR4/DR5 | Indirect (via FADD) | TRAIL signaling |
| RIPK1 | Substrate cleavage | Necroptosis suppression |
| RIPK3 | Protein interaction | Blocks necrosome formation |
| Caspase-3 | Substrate cleavage | Executioner caspase activation |
| Caspase-7 | Substrate cleavage | Executioner caspase activation |
| Bid | Substrate cleavage | Links to mitochondrial pathway |
| c-FLIP (CFLAR) | Heterodimerization | Catalytic inhibition (dominant-negative) |
| IKK complex | Substrate cleavage | NF-κB activation (non-apoptotic) |
| PARP1 | Substrate cleavage | DNA repair inactivation |
| p75NTR | Receptor | proBDNF-mediated activation |

References

[Muzio M et al., FLICE, a novel death effector domain-containing protein (1996)](https://pubmed.ncbi.nlm.nih.gov/8939923/)

[Kelley SO, Parsons SH, Caspase-8 and neurodegeneration (2001)](https://pubmed.ncbi.nlm.nih.gov/12346042/)

[Tummers B, Green DR, Caspase-8: the silent executor (2007)](https://pubmed.ncbi.nlm.nih.gov/17357261/)

[Holler N et al., Two adjacent trimeric Fas ligands are required for Fas signaling (2000)](https://pubmed.ncbi.nlm.nih.gov/10688656/)

[Booth NJ et al., Caspase-8 activation and Bid cleavage in retinal ganglion cells (2008)](https://pubmed.ncbi.nlm.nih.gov/18417694/)

[Stupack DG, Caspase-8 regulation of anoikis (2012)](https://pubmed.ncbi.nlm.nih.gov/22643272/)

[Schleich K et al., Molecular architecture of the DISC complex (2012)](https://pubmed.ncbi.nlm.nih.gov/23222516/)

[Liang H et al., Caspase-8 and necroptosis in neurodegeneration (2020)](https://pubmed.ncbi.nlm.nih.gov/32871279/)

[Crowley D, Waterhouse NJ, Caspase-8 dynamics in apoptosis and necroptosis (2016)](https://pubmed.ncbi.nlm.nih.gov/27777796/)

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Related Entities

CASP8PROTEIN

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slug	proteins-casp8-protein
kg_node_id	CASP8PROTEIN
entity_type	protein
origin_type	v1_polymorphic_backfill
source_table	wiki_pages
wiki_page_id	wp-284989b64911
__merged_from	{'merged_at': '2026-05-13', 'unprefixed_id': 'proteins-casp8-protein'}
_schema_version	1

📊 Evidence Profile

Evidence Balance

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Certainty

45%

Debates

0

Incoming

9

Outgoing

12

0 supporting 0 contradicting 0 neutral

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📗 Cite This Artifact

Caspase-8 (CASP8)

Caspase-8 (CASP8)

Overview

Caspase-8 (CASP8)

Overview

Structure

Protein Domains

Activation Mechanism

Normal Function

Death Receptor Signaling Pathway

Substrate Specificity

Regulation of Necroptosis

Non-Apoptotic Functions

Role in Neurodegeneration

Alzheimer's Disease

Parkinson's Disease

Glaucoma and Optic Neuropathy

Stroke and Ischemia

Huntington's Disease

Amyotrophic Lateral Sclerosis

Multiple Sclerosis

COVID-19 Neurological Complications

Molecular Mechanisms in Disease

Death Receptor Regulation in Neurodegeneration

Receptor Expression

Ligand Expression

Decoy Receptors

c-FLIP Regulation

Bid Regulation in Neurodegeneration

Non-Caspase Substrates

Necroptosis Suppression

Therapeutic Targeting

Caspase-8 Inhibitors

Alternative Approaches

Neuroprotective Strategies

Protein Interactions

See Also

References

💬 Discussion