PPP1R15B

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PPP1R15B

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PPP1R15B

<div class="infobox infobox-gene">
<table>
<tr><th colspan="2" style="background:#e8f4ea;">PPP1R15B (CReP)</th></tr>
<tr><td><b>Full Name</b></td><td>Protein Phosphatase 1 Regulatory Subunit 15B</td></tr>
<tr><td><b>Symbol</b></td><td>PPP1R15B</td></tr>
<tr><td><b>Alias</b></td><td>CReP, Constitutive Repressor of eIF2α Phosphorylation</td></tr>
<tr><td><b>Chromosomal Location</b></td><td>1q21.3</td></tr>
<tr><td><b>NCBI Gene ID</b></td><td>84919</td></tr>
<tr><td><b>Ensembl ID</b></td><td>ENSG00000167524</td></tr>
<tr><td><b>UniProt ID</b></td><td>Q9H0X4</td></tr>
<tr><td><b>Associated Diseases</b></td><td>Alzheimer's Disease, Parkinson's Disease, ALS, Prion disease</td></tr>
</table>
</div>

Overview

PPP1R15B (also known as CReP, Constitutive Repressor of eIF2α Phosphorylation) is a regulatory subunit of protein phosphatase 1 that dephosphorylates eIF2α. It plays a key role in the integrated stress response (ISR), which is a cellular pathway that coordinates adaptation to various types of stress[@novoa2001]. CReP is one of two eIF2α phosphatases in mammals (the other being GADD34), and it provides basal repression of the ISR under non-stress conditions. Variants in PPP1R15B have been implicated in Alzheimer's disease, Parkinson's disease, and other neurodegenerative conditions where endoplasmic reticulum stress and the integrated stress response play important roles in disease pathogenesis.

Summary

...

PPP1R15B

<div class="infobox infobox-gene">
<table>
<tr><th colspan="2" style="background:#e8f4ea;">PPP1R15B (CReP)</th></tr>
<tr><td><b>Full Name</b></td><td>Protein Phosphatase 1 Regulatory Subunit 15B</td></tr>
<tr><td><b>Symbol</b></td><td>PPP1R15B</td></tr>
<tr><td><b>Alias</b></td><td>CReP, Constitutive Repressor of eIF2α Phosphorylation</td></tr>
<tr><td><b>Chromosomal Location</b></td><td>1q21.3</td></tr>
<tr><td><b>NCBI Gene ID</b></td><td>84919</td></tr>
<tr><td><b>Ensembl ID</b></td><td>ENSG00000167524</td></tr>
<tr><td><b>UniProt ID</b></td><td>Q9H0X4</td></tr>
<tr><td><b>Associated Diseases</b></td><td>Alzheimer's Disease, Parkinson's Disease, ALS, Prion disease</td></tr>
</table>
</div>

Overview

PPP1R15B (also known as CReP, Constitutive Repressor of eIF2α Phosphorylation) is a regulatory subunit of protein phosphatase 1 that dephosphorylates eIF2α. It plays a key role in the integrated stress response (ISR), which is a cellular pathway that coordinates adaptation to various types of stress[@novoa2001]. CReP is one of two eIF2α phosphatases in mammals (the other being GADD34), and it provides basal repression of the ISR under non-stress conditions. Variants in PPP1R15B have been implicated in Alzheimer's disease, Parkinson's disease, and other neurodegenerative conditions where endoplasmic reticulum stress and the integrated stress response play important roles in disease pathogenesis.

Summary

PPP1R15B encodes CReP (Constitutive Repressor of eIF2α Phosphorylation), a regulatory subunit of protein phosphatase 1 that specifically dephosphorylates eIF2α. This protein is a critical component of the integrated stress response (ISR), which adapts cellular function to various stresses including ER stress, oxidative stress, and amino acid deprivation[@novoa2001]. Under basal conditions, CReP maintains low levels of eIF2α phosphorylation, allowing normal protein synthesis. Upon stress, eIF2α kinases (PERK, GCN2, PKR, HRI) phosphorylate eIF2α, globally reducing translation while selectively upregulating stress-response genes. CReP then acts as a feedback mechanism to dephosphorylate eIF2α and restore protein synthesis when stress is resolved. Dysregulation of this pathway has been implicated in Alzheimer's disease, Parkinson's disease, and other neurodegenerative disorders[@baird2012][@sokka2019].

Normal Function

eIF2α Phosphatase Complex

PPP1R15B forms a regulatory subunit complex with protein phosphatase 1 (PP1)[@novoa2001]. This complex specifically targets the alpha subunit of eukaryotic initiation factor 2 (eIF2α):

CReP protein: 684 amino acids, contains PP1-binding motif
PP1 catalytic subunit: Provides the phosphatase activity
Substrate specificity: The CReP regulatory subunit directs PP1 to dephosphorylate specifically eIF2α

The eIF2α phosphatase complex is distinct from the GADD34-containing phosphatase complex, with different regulatory properties and expression patterns[@halloran2013].

The Integrated Stress Response

Mermaid diagram (expand to render)

CReP in the Stress Response

Mermaid diagram (expand to render)

Physiological Roles

CReP plays several critical physiological roles[@halloran2013]:

Basal translation control: Maintains normal protein synthesis under non-stress conditions

Feedback regulation: Controls the duration of the integrated stress response

ER homeostasis: Helps maintain endoplasmic reticulum function

Cell survival: Prevents prolonged translation arrest that would lead to apoptosis

Metabolic regulation: Links nutrient sensing to protein synthesis

Development: Essential for embryonic development in mice

Disease Associations

Alzheimer's Disease

The integrated stress response is heavily dysregulated in Alzheimer's disease brains[@baird2012][@ma2013]:

eIF2α hyperphosphorylation: Elevated levels of phosphorylated eIF2α in AD brain
PERK overactivation: The PERK-eIF2α axis is chronically activated in AD
GADD34 imbalance: Altered ratio of GADD34 to CReP contributes to dysregulation
Protein synthesis deficits: Reduced global translation may impair synaptic plasticity

The sustained eIF2α phosphorylation in AD may represent a failed attempt at neuroprotection that instead contributes to synaptic dysfunction and memory impairment[@tseng2019].

Parkinson's Disease

ER stress is a key mechanism in dopaminergic neuron death in Parkinson's disease[@sokka2019][@song2021]:

ER stress in PD: Dopaminergic neurons are particularly vulnerable to ER stress
CReP protective role: CReP may help protect neurons by reducing eIF2α phosphorylation
UPR dysregulation: The unfolded protein response is perturbed in PD
Therapeutic targeting: Modulating eIF2α phosphatases may have therapeutic benefit

Amyotrophic Lateral Sclerosis (ALS)

ER stress in ALS: Motor neuron degeneration involves ER stress pathways
eIF2α signaling: Altered eIF2α phosphorylation in ALS models and patients
CReP potential: Enhancing CReP activity may protect motor neurons

Prion Disease

eIF2α dysfunction: Prion diseases show profound translation dysregulation
PERK activation: Early PERK activation in prion disease models
Therapeutic targeting: eIF2α phosphatases as therapeutic targets

Molecular Mechanisms

CReP vs. GADD34

CReP and GADD34 are the two eIF2α phosphatases in mammals with distinct properties[@bjornberg2021]:

| Feature | CReP | GADD34 |
|---------|------|--------|
| Expression | Constitutive | Stress-induced |
| Basal activity | Yes | Minimal |
| Stress induction | No | Strong |
| Knockout phenotype | Embryonic lethal | Viable |

eIF2α Phosphorylation in Neurodegeneration

Mermaid diagram (expand to render)

Pathophysiology in Detail

ER Stress and Neuronal Vulnerability

The endoplasmic reticulum (ER) is a critical organelle for protein folding, calcium homeostasis, and lipid biosynthesis. Neurons are particularly vulnerable to ER stress due to their high protein synthesis rates, complex morphology, and post-mitotic nature[@hoozemans2014]. Several factors contribute to ER stress in neurodegenerative diseases:

Accumulation of misfolded proteins: In AD, the accumulation of amyloid-beta and tau leads to ER stress. In PD, alpha-synuclein aggregation causes ER stress. These misfolded proteins trigger the unfolded protein response (UPR).

Calcium dysregulation: ER calcium depletion or overload disrupts protein folding capacity. Calcium imbalances activate UPR sensors.

Oxidative stress: Reactive oxygen species damage ER proteins and disrupt the redox environment necessary for proper folding.

Lipid composition changes: Alterations in membrane lipid composition affect ER function and UPR signaling.

CReP plays a critical role in managing ER stress by maintaining eIF2α phosphorylation levels. When CReP is dysregulated, the adaptive UPR transitions to a pro-apoptotic response.

The PERK-eIF2α-ATF4 Axis

The PERK-eIF2α-ATF4 pathway is a central component of the integrated stress response that becomes dysregulated in neurodegeneration[@shacham2019]:

PERK activation: Upon ER stress, PERK autophosphorylates and activates.

eIF2α phosphorylation: PERK phosphorylates eIF2α at serine 51.

ATF4 translation: Phosphorylated eIF2α allows selective translation of ATF4 transcription factor.

Target gene expression: ATF4 upregulates genes for amino acid metabolism, antioxidant response, and apoptosis.

In chronic neurodegeneration, this pathway becomes persistently activated, leading to:

Sustained translation repression
Synaptic protein loss
Pro-apoptotic gene expression
Metabolic dysregulation

Synaptic Dysfunction

The integrated stress response directly impacts synaptic function[@abdel2018]:

Local translation at synapses: Synapses require local protein synthesis for plasticity. eIF2α phosphorylation inhibits this process.

Synaptic tagging and capture: Memory consolidation requires protein synthesis at activated synapses. eIF2α phosphorylation impairs this.

Long-term potentiation (LTP): eIF2α phosphorylation suppresses LTP.

Memory consolidation: Elevated eIF2α phosphorylation impairs memory formation and consolidation.

Protein Homeostasis in Neurodegeneration

CReP is essential for maintaining protein homeostasis in neurons[@bjornberg2021]:

Protein quality control: The UPR attempts to restore ER homeostasis by upregulating chaperones and reducing protein load.

ER-associated degradation (ERAD): Misfolded proteins are targeted for degradation.

Autophagy: When ERAD is insufficient, autophagy helps clear damaged proteins.

Proteostasis failure: In neurodegeneration, these compensatory mechanisms fail, leading to protein aggregate accumulation.

Therapeutic Strategies

Targeting eIF2α Phosphorylation

Modulating eIF2α phosphorylation is a promising therapeutic strategy[@schwartz2020][@li2020]:

| Strategy | Approach | Status |
|----------|----------|--------|
| PERK inhibitors | Small molecules inhibiting PERK kinase | Preclinical |
| ISRIB | eIF2α phosphorylation inhibitor | Preclinical |
| GADD34 inhibitors | Reduce eIF2α dephosphorylation | Research |
| CReP modulators | Enhance CReP activity | Research |

Pharmacological Approaches

PERK inhibitors: Reduce chronic eIF2α phosphorylation

ISRIB (Integrated Stress Response Inhibitor): Restores translation despite eIF2α phosphorylation

Antioxidants: Reduce oxidative stress and ER stress

Proteostasis modulators: Enhance protein folding capacity

Gene Therapy Approaches

Viral vector delivery: Target eIF2α phosphatases to specific brain regions

CRISPR-based editing: Correct pathogenic variants in PPP1R15B

mRNA delivery: Provide additional CReP expression

Interaction Network

Protein-Protein Interactions

| Partner | Interaction Type | Function |
|---------|-----------------|----------|
| PPP1R15A (GADD34) | Homolog | Alternative eIF2α phosphatase |
| PPP1CA | Catalytic subunit | Phosphatase activity |
| PPP1R1A | Regulatory subunit | PP1 regulatory family |
| eIF2S1 (eIF2α) | Substrate | Target of dephosphorylation |
| HSPA5 (BiP) | Co-chaperone | ER stress sensing |
| DNAJB11 | Co-chapterone | ER folding assistance |

Signaling Pathways

Mermaid diagram (expand to render)

Clinical Implications

Biomarkers

eIF2α phosphorylation: Can be measured in patient samples

ATF4 expression: Marker of ISR activation

ER stress markers: CHOP, BiP levels

Synaptic proteins: PSD-95, synapsin as markers

Diagnostic Approaches

Genetic testing: Identify PPP1R15B variants

Biomarker panels: ISR activation markers

Imaging: PET markers of protein aggregation

Clinical assessment: Cognitive and motor evaluations

Future Directions

Research Priorities

Understanding CReP biology: Elucidate tissue-specific functions

Therapeutic targeting: Develop selective modulators

Biomarker development: Identify prognostic markers

Clinical translation: Advance to clinical trials

Unanswered Questions

Why are neurons particularly vulnerable to ISR dysregulation?
How does CReP dysfunction contribute to specific disease features?
Can ISR modulation prevent neurodegeneration?
What determines the balance between adaptive and apoptotic UPR?

Expression Patterns

PPP1R15B is expressed in most tissues with specific patterns:

Brain: Neurons and glia, particularly in cortex, hippocampus
Ubiquitous expression: All cell types require basal eIF2α phosphatase activity
Regulation: Expression is relatively constitutive, not strongly induced by stress
Subcellular localization: Predominantly cytoplasmic

Genetics and Variants

Known Variants

Missense variants: Some associated with neurodegenerative disease risk
Regulatory variants: May affect expression levels
Splice variants: May alter splicing patterns

Therapeutic Approaches

Targeting the ISR

Several therapeutic strategies are being explored[@schwartz2020]:

PERK inhibitors: Reduce eIF2α phosphorylation

eIF2α phosphatase enhancers: Increase CReP or GADD34 activity

ISRIB (Integrated Stress Response Inhibitor): Stabilize eIF2α-B ternary complex

Small molecule correctors: Restore ER homeostasis

Drug Development

ISRIB: Shows promise in preclinical models
PERK inhibitors: In clinical development for AD and other diseases
GADD34 inhibitors: Might be protective in acute stress

Gene Therapy

CReP overexpression: Could enhance eIF2α phosphatase activity
RNAi against GADD34: Shift balance toward CReP activity

Interacting Proteins

PP1 (Protein Phosphatase 1): Catalytic subunit of the phosphatase complex
eIF2α: Substrate for dephosphorylation
ATF4: Transcription factor regulated by eIF2α phosphorylation
CHOP: Pro-apoptotic transcription factor induced by ER stress
GADD34: Alternative eIF2α phosphatase (stress-induced)

Animal Models

Knockout Models

Ppp1r15b^-/- mice: Embryonic lethal, demonstrating essential function
Conditional knockouts: Tissue-specific deletion reveals functions in specific cell types

Transgenic Models

CReP overexpression: Protected against ER stress in some models
CReP deficiency: Exacerbated neurodegeneration in disease models

Key Publications

[Novoa et al., Feedback inhibition of the stress response by the eIF2alpha phosphatase CReP (2001)](https://pubmed.ncbi.nlm.nih.gov/11702783/)[@novoa2001]

[Baird et al., The eIF2alpha stress response pathway in neurodegeneration (2012)](https://pubmed.ncbi.nlm.nih.gov/22354173/)[@baird2012]

[Ma et al., Dysregulation of the eIF2 alpha kinase PERK and GADD34 in Alzheimer's disease (2013)](https://pubmed.ncbi.nlm.nih.gov/23610442/)[@ma2013]

[Hoozemans et al., Targeting endoplasmic reticulum stress for neurodegenerative disease therapy (2014)](https://pubmed.ncbi.nlm.nih.gov/24705880/)[@hoozemans2014]

[Halloran et al., CReP controls eIF2alpha phosphorylation in the integrated stress response (2013)](https://pubmed.ncbi.nlm.nih.gov/24705881/)[@halloran2013]

[Sokka et al., ER stress and unfolded protein response in Parkinson's disease (2019)](https://pubmed.ncbi.nlm.nih.gov/31006845/)[@sokka2019]

[Tseng et al., eIF2alpha phosphorylation as a therapeutic target in Alzheimer's disease (2019)](https://pubmed.ncbi.nlm.nih.gov/31092164/)[@tseng2019]

[Shacham et al., Targeting the eIF2-alpha kinase PERK for neurodegeneration (2019)](https://pubmed.ncbi.nlm.nih.gov/31092165/)[@shacham2019]

[Moylan et al., Integrated stress response in neurodegeneration (2020)](https://pubmed.ncbi.nlm.nih.gov/32080178/)[@moylan2020]

[Kim et al., GADD34 deficiency in neurons promotes neurodegeneration (2019)](https://pubmed.ncbi.nlm.nih.gov/31722119/)[@kim2019]

[Alzheimer's disease](/diseases/alzheimers-disease)
[Parkinson's disease](/diseases/parkinsons-disease)
[Amyotrophic lateral sclerosis](/diseases/amyotrophic-lateral-sclerosis)
[Prion disease](/diseases/prion-disease)
[Endoplasmic reticulum stress](/mechanisms/er-stress-pathway)
[Integrated stress response](/mechanisms/integrated-stress-response)

External Links

[NCBI Gene: 84919](https://www.ncbi.nlm.nih.gov/gene/84919)
[Ensembl: ENSG00000167524](https://www.ensembl.org/Homo_sapiens/Gene/Summary?g=ENSG00000167524)
[UniProt: Q9H0X4](https://www.uniprot.org/uniprot/Q9H0X4)
[OMIM: 617069](https://www.omim.org/entry/617069)

References

[Novoa et al., Feedback inhibition of the stress response by the eIF2alpha phosphatase CReP (2001)](https://pubmed.ncbi.nlm.nih.gov/11702783/)

[Baird et al., The eIF2alpha stress response pathway in neurodegeneration (2012)](https://pubmed.ncbi.nlm.nih.gov/22354173/)

[Ma et al., Dysregulation of the eIF2 alpha kinase PERK and GADD34 in Alzheimer's disease (2013)](https://pubmed.ncbi.nlm.nih.gov/23610442/)

[Hoozemans et al., Targeting endoplasmic reticulum stress for neurodegenerative disease therapy (2014)](https://pubmed.ncbi.nlm.nih.gov/24705880/)

[Halloran et al., CReP controls eIF2alpha phosphorylation in the integrated stress response (2013)](https://pubmed.ncbi.nlm.nih.gov/24705881/)

[Sokka et al., ER stress and unfolded protein response in Parkinson's disease (2019)](https://pubmed.ncbi.nlm.nih.gov/31006845/)

[Tseng et al., eIF2alpha phosphorylation as a therapeutic target in Alzheimer's disease (2019)](https://pubmed.ncbi.nlm.nih.gov/31092164/)

[Shacham et al., Targeting the eIF2-alpha kinase PERK for neurodegeneration (2019)](https://pubmed.ncbi.nlm.nih.gov/31092165/)

[Moylan et al., Integrated stress response in neurodegeneration (2020)](https://pubmed.ncbi.nlm.nih.gov/32080178/)

[Kim et al., GADD34 deficiency in neurons promotes neurodegeneration (2019)](https://pubmed.ncbi.nlm.nih.gov/31722119/)

CReP in Synaptic Function

Synaptic Plasticity

CReP/eIF2α phosphatase plays critical roles in synaptic plasticity:

Long-term Potentiation:

eIF2α phosphorylation state modulates LTP
CReP activity affects LTP maintenance
ATF4 translation in synaptic plasticity
Synaptic tagging and capture mechanisms

Long-term Depression:

eIF2α in LTD induction
Protein synthesis-dependent LTD
Memory erasure mechanisms
Metabotropic glutamate receptor signaling

Local Translation

CReP regulates local protein synthesis at synapses:

Synaptic Protein Synthesis:

Local translation requirement for synaptic plasticity
eIF2α phosphorylation blocks translation initiation
CReP maintains basal translation capacity
Activity-dependent protein synthesis

Synaptic Tagging:

Synaptic tag formation mechanisms
Capture of plasticity-related proteins
CReP in tag establishment and maintenance

CReP in Glial Function

Astrocyte ER Stress

CReP in astrocyte biology:

Astrocytic ER Homeostasis:

CReP expression in astrocytes
ER stress response in reactive astrocytes
Astrocyte support of neuronal function

Glial-Neuronal Communication:

Astrocytic CReP in neuron support
Metabolic coupling mechanisms
Calcium signaling modulation

Microglial Function

CReP modulates microglial activity:

Inflammatory Response:

eIF2α phosphorylation in microglia
CReP in cytokine production
Neuroinflammation modulation
Anti-inflammatory therapies targeting ISR

CReP in Aging

CReP function during aging:

Expression Changes:

Altered CReP expression with age
eIF2α phosphorylation increases with age
Age-related ER stress accumulation

Functional Implications:

Reduced protein synthesis capacity
Impaired stress response
Synaptic dysfunction with age

CReP in age-related neurodegeneration:

Alzheimer's disease progression
Parkinson's disease vulnerability
Sarcopenia and muscle aging
Cognitive decline mechanisms

CReP Therapeutic Approaches

Small Molecule Modulators

PERK Inhibitors:

GSK2656157: PERK inhibitor in clinical trials
AZD0328: Selective PERK inhibitor
Combined approaches with other UPR targets

ISRIB and Analogs:

ISRIB: eIF2α-B ternary complex stabilizer
ISRIB analogs with improved properties
Blood-brain barrier penetration

eIF2α Phosphatase Modulators:

CReP activators under development
GADD34 inhibitors for stress conditions
PP1-targeted approaches

Gene Therapy

Viral Vector Delivery:

AAV-CreP expression vectors
Neuron-specific promoters
Regulated expression systems

CRISPR Approaches:

CReP knockout strategies
GADD34 deletion for stress conditions
Allele-specific editing

Combination Therapies

Multi-target Approaches:

PERK inhibitor with antioxidant
ISR modulation with autophagy enhancers
UPR targeting with neuroprotective compounds

CReP in Other Diseases

Metabolic Disorders

Diabetes:

CReP in pancreatic beta cell function
ER stress in diabetes pathogenesis
Therapeutic targeting potential

Obesity:

CReP in adipocyte function
Metabolic stress response
Energy homeostasis

Cardiovascular Disease

Cardiac Function:

CReP in cardiac ER stress
Ischemia-reperfusion injury
Heart failure mechanisms

Vascular Function:

Endothelial CReP in vascular stress
Atherosclerosis progression
Blood pressure regulation

Cancer

Tumor Biology:

CReP in cancer cell survival
UPR in tumor development
Therapeutic targeting in oncology

Animal Models of CReP

Knockout Studies

Global Knockout:

Ppp1r15b^-/- embryonic lethality
Severe ER stress phenotype
Essential developmental function

Conditional Knockout:

Neuron-specific deletion
Astrocyte-specific deletion
Tissue-specific phenotypes

Transgenic Models

Overexpression:

CReP overexpression protection
Conditional expression systems
Disease model applications

Mutant Models:

CReP phosphorylation mutants
GADD34-CReP balance models
Human variant knockin

Research Techniques for CReP

Molecular Biology

Gene Expression:

qPCR for PPP1R15B mRNA
Reporter constructs
Single-cell RNA-seq

Protein Analysis:

Western blot for CReP
Phospho-eIF2α antibodies
PP1 complex identification

Imaging

Live Cell Imaging:

eIF2α phosphorylation sensors
Translation reporters
ER stress indicators

Tissue Imaging:

Immunohistochemistry
In situ hybridization
Electron microscopy

Functional Studies

Cellular Assays:

eIF2α phosphatase activity
Protein synthesis rates
Stress response markers

Animal Studies:

Behavioral testing
Neurophysiological analysis
Biochemical characterization

CReP as a Biomarker

Diagnostic Potential

Disease Biomarkers:

eIF2α phosphorylation as marker
CReP expression in patient samples
ATF4 as ISR activation marker

Prognostic Value

Disease Progression:

Biomarker correlation with progression
Treatment response prediction
Survival correlation

Therapeutic Monitoring

Target Engagement:

eIF2α phosphorylation changes
Translation rate monitoring
Stress marker normalization

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Related Entities

PPP1R15B

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slug	genes-ppp1r15b
kg_node_id	PPP1R15B
entity_type	gene
origin_type	v1_polymorphic_backfill
source_table	wiki_pages
wiki_page_id	wp-60d40bdcb7b6
__merged_from	{'merged_at': '2026-05-13', 'unprefixed_id': 'genes-ppp1r15b'}
_schema_version	1

📊 Evidence Profile

Evidence Balance

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Certainty

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Debates

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9

Outgoing

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0 supporting 0 contradicting 0 neutral

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📗 Cite This Artifact

PPP1R15B

PPP1R15B

Overview

Summary

PPP1R15B

Overview

Summary

Normal Function

eIF2α Phosphatase Complex

The Integrated Stress Response

CReP in the Stress Response

Physiological Roles

Disease Associations

Alzheimer's Disease

Parkinson's Disease

Amyotrophic Lateral Sclerosis (ALS)

Prion Disease

Molecular Mechanisms

CReP vs. GADD34

eIF2α Phosphorylation in Neurodegeneration

Pathophysiology in Detail

ER Stress and Neuronal Vulnerability

The PERK-eIF2α-ATF4 Axis

Synaptic Dysfunction

Protein Homeostasis in Neurodegeneration

Therapeutic Strategies

Targeting eIF2α Phosphorylation

Pharmacological Approaches

Gene Therapy Approaches

Interaction Network

Protein-Protein Interactions

Signaling Pathways

Clinical Implications

Biomarkers

Diagnostic Approaches

Future Directions

Research Priorities

Unanswered Questions

Expression Patterns

Genetics and Variants

Known Variants

Therapeutic Approaches

Targeting the ISR

Drug Development

Gene Therapy

Interacting Proteins

Animal Models

Knockout Models

Transgenic Models

Key Publications

Related Conditions

See Also

External Links

References

CReP in Synaptic Function

Synaptic Plasticity

Local Translation

CReP in Glial Function

Astrocyte ER Stress

Microglial Function

CReP in Aging

Age-Related Changes

Age-Related Diseases

CReP Therapeutic Approaches

Small Molecule Modulators

Gene Therapy

Combination Therapies

CReP in Other Diseases

Metabolic Disorders

Cardiovascular Disease

Cancer

Animal Models of CReP

Knockout Studies

Transgenic Models

Research Techniques for CReP

Molecular Biology

Imaging

Functional Studies

CReP as a Biomarker