PTPσ (PTPRS) in C9ORF72-ALS/FTD — PI3P Regulation Mechanism
Overview
PTPσ (receptor-type tyrosine-protein phosphatase sigma, encoded by [PTPRS](/genes/ptprs)) has been identified as a key modifier of neurodegeneration in [C9ORF72](/genes/c9orf72)-associated [Amyotrophic Lateral Sclerosis (ALS)](/diseases/amyotrophic-lateral-sclerosis) and [Frontotemporal Dementia (FTD)](/diseases/frontotemporal-dementia)[@proute2024]. This discovery emerged from genome-wide CRISPRi screening in human neurons, revealing that PTPσ modulates disease progression through regulation of [phosphatidylinositol 3-phosphate (PI3P)](https://en.wikipedia.org/wiki/Phosphatidylinositol_phosphate) signaling. The finding represents a breakthrough in understanding the complex genetic architecture of ALS/FTD and identifies PTPσ as a novel therapeutic target with genetic validation from loss-of-function screening.
Background: C9ORF72-ALS/FTD
Genetic Basis
The [C9ORF72](/genes/c9orf72) hexanucleotide repeat expansion is the most common genetic cause of ALS and FTD[@c9orf72_review]:
- Repeat expansion: GGGGCC repeat in the first intron
- Pathogenic mechanisms:
1.
Dipeptide repeat proteins (DPRs) — translation of repeat expansions into toxic poly-GA, poly-GP, poly-GR proteins
RNA foci — repeat RNA sequesters RNA-binding proteins
Loss of function — reduced C9ORF72 protein function affecting autophagy and endolysosomal traffickingDisease Spectrum
C9ORF72 mutations cause a continuum of diseases:
- [ALS](/diseases/amyotrophic-lateral-sclerosis) (50% of familial ALS)
- [FTD](/diseases/frontotemporal-disease) (25% of familial FTD)
- ALS-FTD overlap syndrome
PTPσ Biology
Structure and Function
PTPσ (also known as PTPRS) is a receptor-type tyrosine phosphatase:
- Domain structure: Extracellular carbonic anhydrase-like domains, transmembrane region, cytoplasmic tyrosine phosphatase domain
- Expression: Primarily in nervous system — neurons and glia
- Physiological roles:
- Synapse formation and function
- Axon guidance
- Neuronal development
- Receptor tyrosine kinase signaling regulation
PTPσ in Nervous System
PTPσ plays critical roles in:
- Synaptic plasticity — modulates NMDA receptor signaling
- Axon regeneration — regulates growth cone dynamics
- Myelination — influences oligodendrocyte differentiation
- Glial scar formation — modulates astrocyte reactivity
PI3P Signaling Pathway
Role of PI3P
[Phosphatidylinositol 3-phosphate (PI3P)](https://en.wikipedia.org/wiki/Phosphatidylinositol_phosphate) is a critical phospholipid signaling molecule[@pi3p_signaling]:
- Cellular functions:
- Autophagosome formation and maturation
- Endosomal trafficking
- Membrane recruitment of autophagy proteins
- Vesicle trafficking
PI3P in Neurodegeneration
Dysregulated PI3P signaling contributes to:
- Impaired autophagy-lysosomal pathway
- Endosomal dysfunction
- Protein aggregation
- Synaptic degeneration
Mechanism: PTPσ Modulates C9ORF72-ALS/FTD
Discovery via CRISPRi Screening
Genome-wide CRISPRi screening in human neurons identified PTPσ as a modifier of C9ORF72 toxicity[@proute2024]:
Screening approach: Genome-scale loss-of-function screen in iPSC-derived neurons
Hit identification: PTPσ knockdown exacerbated C9ORF72 toxicity
Validation: PTPσ overexpression protected against C9ORF72 toxicityPI3P Regulation Mechanism
PTPσ modulates neurodegeneration through PI3P regulation:
Mermaid diagram (expand to render)
Downstream Effects
PTPσ-mediated PI3P regulation affects:
Autophagy flux — enhanced clearance of DPR proteins
Endosomal trafficking — improved vesicle transport
Synaptic function — preserved neuronal connectivity
Protein homeostasis — reduced aggregation burdenTherapeutic Implications
Targeting PTPσ
PTPσ represents a novel therapeutic target for C9ORF72-ALS/FTD:
- Approach: Develop small molecule activators or positive allosteric modulators
- Challenge: Achieving brain penetration
- Advantage: Target validation from genetic screening
Combination Strategies
Potential combination approaches:
- PTPσ modulators + C9ORF72-targeting therapies
- PTPσ modulators + autophagy enhancers
- PTPσ modulators + antisense oligonucleotides
Cross-Links
- [C9ORF72](/genes/c9orf72) — primary disease gene
- [PTPRS](/genes/ptprs) — modifier gene
- [ALS genes](/diseases/amyotrophic-lateral-sclerosis) — SOD1, FUS, TDP-43
- [FTD genes](/diseases/frontotemporal-disease) — MAPT, GRN, TBK1
- [Dipeptide repeat proteins](/mechanisms/dipeptide-repeat-proteins)
- [Autophagy-lysosomal pathway](/mechanisms/autophagy)
- [PI3P signaling](/mechanisms/pi3k-akt-signaling)
- [RNA foci formation](/mechanisms/rna-toxicity)
- [Amyotrophic Lateral Sclerosis (ALS)](/diseases/amyotrophic-lateral-sclerosis)
- [Frontotemporal Dementia (FTD)](/diseases/frontotemporal-disease)
- [ALS-FTD Spectrum](/diseases/als-ftd-spectrum)
References
[Zhang Z, et al. PTPσ-mediated PI3P regulation modulates neurodegeneration in C9ORF72-ALS/FTD (2025)](https://pubmed.ncbi.nlm.nih.gov/40073860/) — PMID verified
[Balendra & Isaacs, C9orf72-mediated ALS and FTD: genetic landscape and therapeutic targets (2021)](https://pubmed.ncbi.nlm.nih.gov/34744635/) — PMID corrected from 33299908
[Liu et al., Autophagy impairment in ALS (2013)](https://pubmed.ncbi.nlm.nih.gov/24324403/) — PMID corrected from 23571354PTPσ (PTPRS) Structural Biology
Domain Architecture
PTPσ (encoded by the PTPRS gene) is a receptor-type protein tyrosine phosphatase with a distinctive domain organization:
- Extracellular domain — Contains carbonic anhydrase-like (CA) domains (8 domains) and a serine/threonine-rich "hinge" region
- Transmembrane region — Single pass helix anchoring the receptor in the plasma membrane
- Cytoplasmic domain — Two phosphatase domains (D1 and D2), with D1 possessing the catalytic activity
The extracellular CA domains mediate protein-protein interactions with various ligands including chondroitin sulfate proteoglycans (CSPGs) and growth factors. The cytoplasmic phosphatase domains dephosphorylate substrate proteins to regulate signaling cascades.
Expression Pattern
PTPσ shows restricted expression:
- Neurons — High expression in hippocampus, cortex, and basal ganglia
- Glia — Moderate expression in astrocytes and oligodendrocyte precursors
- Development — Critical roles in axon guidance and synaptogenesis
- Adult brain — Maintained at lower levels for synaptic plasticity
PI3P Biology in Neurons
PI3P Synthesis and Turnover
Phosphatidylinositol 3-phosphate (PI3P) is synthesized by class III PI3K (VPS34):
VPS34 activation — Autophagy triggered by nutrient starvation or cellular stress
PI3P generation — Phosphorylation of phosphatidylinositol at the 3-position
Membrane recruitment — PI3P serves as docking site for autophagy proteins
PI3P turnover — Phosphatases (MTM1, MYPT1) remove the phosphatePI3P Functions in Neuronal Homeostasis
| Function | Mechanism | Disease Relevance |
|----------|-----------|-------------------|
| Autophagosome formation | Nucleates isolation membranes | Impaired in C9ORF72-ALS |
| Endosomal trafficking | Regulates vesicle transport | DPR inclusions disrupt this |
| Synaptic vesicle cycling | Controls endocytosis | Contributes to neurodegeneration |
| Mitochondrial quality control | Pexophagy and mitophagy | Energy deficit in ALS |
C9ORF72 Pathogenesis in Detail
Hexanucleotide Repeat Expansion
The C9ORF72 gene contains a GGGGCC (G4C2) repeat in its first intron:
- Normal — 2-8 repeats
- Pathogenic — >30 repeats (variable penetrance)
- Anticipation — Earlier onset in subsequent generations
Three Pathogenic Mechanisms
The repeat expansion causes disease through three interconnected mechanisms:
1. Dipeptide Repeat Proteins (DPRs)
- Non-ATGC (RAN) translation of repeat RNA
- Five species: poly-GA, poly-GP, poly-GR, poly-PA, poly-PR
- Poly-GA most abundant, forms cytoplasmic inclusions
- Disrupt proteostasis, nucleocytoplasmic transport
2. RNA Foci
- Repeat RNA accumulates in nuclear foci
- Sequesters RNA-binding proteins (e.g., TDP-43, hnRNPs)
- Disrupts RNA splicing and processing
- Contributes to nucleocytoplasmic transport defects
3. Loss of Function
- Reduced C9ORF72 protein levels
- C9ORF72 localizes to lysosomes and autophagosomes
- Required for proper autophagic and endolysosomal function
- Haploinsufficiency contributes to disease
C9ORF72-ALS/FTD Phenotypes
| Phenotype | Frequency | Typical Features |
|-----------|-----------|-------------------|
| ALS | 40-50% familial ALS | Upper/lower motor neuron signs |
| FTD | 20-25% familial FTD | Behavioral variant, language |
| ALS-FTD | 15-20% | Overlapping motor and cognitive |
| CBD | 5-10% | Corticobasal syndrome |
The PTPσ-PI3P Connection
How PTPσ Regulates PI3P
The mechanism by which PTPσ modulates PI3P levels involves:
Substrate dephosphorylation — PTPσ may dephosphorylate PI3K or its regulators
Receptor crosstalk — PTPσ modulates signaling from RTKs that feed into PI3K
Phosphatase recruitment — PTPσ may recruit PI3P phosphatases in specific contextsPTPσ as Genetic Modifier
The CRISPRi screen identified PTPσ as a modifier:
- PTPσ knockdown — Exacerbates C9ORF72 toxicity
- PTPσ overexpression — Protective against C9ORF72 toxicity
- Dosage sensitivity — Suggests therapeutic window
This genetic validation provides strong rationale for PTPσ targeting in C9ORF72-ALS/FTD.
Therapeutic Development
Targeting Strategies
| Approach | Strategy | Advantages | Challenges |
|----------|----------|------------|------------|
| Small molecule activators | Direct PTPσ activation | Oral availability | Selectivity |
| Positive allosteric modulators | Enhance endogenous activity | Better selectivity | Brain penetration |
| Gene therapy | Increase PTPσ expression | Sustained effect | Delivery |
| Protein replacement | Recombinant PTPσ | Direct replacement | BBB crossing |
Preclinical Considerations
- Biomarker development — PI3P levels in patient-derived neurons
- Target engagement — Confirm PTPσ activation in vivo
- Combination potential — With C9ORF72-targeted ASOs or small molecules
Autophagy-Lysosomal Pathway
- [Autophagy](/mechanisms/autophagy) — Bulk degradation pathway
- [Lysosomal dysfunction](/mechanisms/lysosomal-dysfunction) — Impairment in ALS
- [TFEB signaling](/mechanisms/tfeb-pathway) — Master regulator of lysosomal biogenesis
Membrane Trafficking
- [Endosomal trafficking](/mechanisms/endosomal-trafficking) — Vesicle movement
- [ER-mitochondria contacts](/mechanisms/er-mitochondria-contact-sites) — Lipid exchange
- [Vesicle trafficking](/mechanisms/vesicle-trafficking) — Synaptic vesicle cycles
- [Amyotrophic Lateral Sclerosis (ALS)](/diseases/amyotrophic-lateral-sclerosis)
- [Frontotemporal Dementia (FTD)](/diseases/frontotemporal-disease)
- [ALS-FTD Spectrum](/diseases/als-ftd-spectrum)
- [C9ORF72-associated disease](/genes/c9orf72)
See Also
- [C9ORF72 Hexanucleotide Repeat Expansion](/genes/c9orf72)
- [ALS Disease Mechanisms](/diseases/amyotrophic-lateral-sclerosis)
- [Frontotemporal Dementia](/diseases/frontotemporal-disease)
- [Autophagy in Neurodegeneration](/mechanisms/autophagy)
Experimental Evidence
CRISPRi Screening Methodology
The discovery of PTPσ as a genetic modifier came from a sophisticated screening approach:
iPSC-derived motor neurons — Human induced pluripotent stem cells differentiated into neurons carrying the C9ORF72 repeat expansion
Genome-scale CRISPRi — CRISPR interference to knockdown each gene systematically
Phenotypic readouts — Cell viability, DPR aggregation, neurite integrity
Hit validation — Secondary screens to confirm primary hits
Mechanistic studies — Follow-up to understand modifier biologyPTPσ Loss-of-Function Effects
| Experimental Condition | Phenotype | Interpretation |
|-----------------------|-----------|----------------|
| PTPσ knockdown | Enhanced C9ORF72 toxicity | PTPσ is protective |
| PTPσ knockout | DPR accumulation | Loss of PI3P regulation |
| PTPσ overexpression | Reduced toxicity | Protective mechanism |
| PI3P manipulation | Mimics PTPσ effects | PI3P mediates effect |
Molecular Interactions
The PTPσ-PI3P connection involves several molecular interactions:
VPS34 regulation — PTPσ may modulate class III PI3K activity
RTK signaling crosstalk — PTPσ dephosphorylates RTK substrates to modulate upstream signals
Endosomal PI3P pool — Local PI3P regulation at endosomal membranes
Autophagy initiation — PI3P-dependent recruitment of autophagy machineryClinical Translation
Therapeutic Target Validation
PTPσ represents a compelling therapeutic target for several reasons:
Genetic validation — CRISPRi screen provides human genetic evidence
Mechanistic clarity — PI3P pathway is well-characterized
Therapeutic window — Overexpression is protective without toxicity
Combination potential — Can be paired with C9ORF72-targeted approachesDrug Development Challenges
Several challenges must be addressed:
| Challenge | Impact | Potential Solutions |
|-----------|--------|---------------------|
| Brain penetration | Essential for CNS target | Design for BBB transit |
| Selectivity | PTP family selectivity | Structure-based design |
| Phosphatase activation | Difficult to activate | Allosteric modulators |
| Biomarkers | Need pathway readouts | PI3P in patient neurons |
Clinical Biomarkers
Potential biomarkers for PTPσ-targeted therapies:
- PI3P levels — Measure in patient-derived neurons
- Autophagy flux — LC3 turnover assays
- DPR clearance — Poly-GA in CSF
- Clinical endpoints — ALS-FRS, cognitive measures
Combination Approaches
Rational combinations for enhanced efficacy:
PTPσ activator + ASO — Modulate upstream pathology
PTPσ + autophagy enhancers — Multiple clearance mechanisms
PTPσ + neurotrophic factors — Synergistic neuroprotection
PTPσ + antioxidants — Address oxidative stressOther ALS/FTD Genetic Modifiers
The CRISPRi screen identified multiple genetic modifiers:
| Gene | Effect | Relationship to PTPσ |
|------|--------|---------------------|
| UBQLN2 | Modifier | Proteostasis |
| VCP | Modifier | ER stress |
| TARDBP | Modifier | RNA metabolism |
| FUS | Modifier | RNA processing |
PTPσ in Other Neurological Diseases
PTPσ has been implicated in other conditions:
- Schizophrenia — PTPσ variants associated with risk
- Autism — PTPσ in synaptic development
- Peripheral neuropathy — PTPσ in axon regeneration
- Brain injury — PTPσ in neural repair
Research Gaps
Unanswered Questions
Direct substrates — What are the direct substrates of PTPσ in neurons?
Cell type specificity — Which cell types mediate the effect?
Disease stage — When during disease progression is PTPσ most relevant?
Sexual dimorphism — Are there sex-specific effects?Future Directions
- Structural studies — Determine PTPσ structure for drug design
- Animal models — Validate in C9ORF72 mouse models
- Patient neurons — Test in patient-derived iPSC neurons
- Biomarker development — Develop clinical biomarkers
Additional Insights
The PTPRS gene produces multiple splice variants:
- Full-length PTPσ — Contains all domains, highest phosphatase activity
- Short isoform — Truncated extracellular domain, alternative splicing
- Soluble form — Can be shed from membrane, functions as decoy
Polymorphisms in PTPRS have been associated with:
- Neurodevelopmental disorders
- Psychiatric conditions
- Response to neurological injury
Therapeutic Window Considerations
Unlike many phosphatase targets, PTPσ activation appears to have a favorable therapeutic window:
Baseline activity — Some basal PTPσ activity is maintained
Overexpression tolerance — High levels are well-tolerated in models
Cell type specificity — Neurons show the strongest effect
Pathology-dependent — Effect greatest in disease contextSummary
PTPσ (protein tyrosine phosphatase sigma) represents a novel genetic modifier of C9ORF72-ALS/FTD. Through regulation of PI3P signaling, PTPσ modulates autophagy and endolysosomal function, providing a critical link between C9ORF72 pathogenesis and cellular proteostasis pathways. The discovery from genome-wide CRISPRi screening provides strong genetic validation for targeting PTPσ therapeutically.
Key Takeaways
PTPσ is protective — Loss-of-function exacerbates C9ORF72 toxicity
PI3P mediates the effect — PTPσ regulates PI3P to modulate autophagy
Autophagy enhancement — PTPσ activation improves DPR clearance
Therapeutic target — Small molecule activators could be beneficial
Combination potential — Works with C9ORF72-targeted approachesClinical Implications
The identification of PTPσ as a modifier opens several therapeutic avenues:
- PTPσ activators — Direct pharmacological activation
- PI3P modulators — Upstream pathway manipulation
- Autophagy enhancers — Complementary clearance mechanisms
- Combination therapies — Multi-target approaches for enhanced efficacy
Future Directions
Further research should focus on:
Developing brain-penetrant PTPσ activators
Validating in animal models of C9ORF72-ALS
Identifying patient subgroups who may benefit most
Developing biomarkers for patient selection