The PI3K-Akt signaling pathway represents one of the most critical cell survival pathways in the nervous system, and its dysfunction plays a central role in Parkinson's disease pathogenesis. This pathway regulates neuronal survival, mitochondrial function, autophagy, and protein homeostasis—all processes compromised in PD. Understanding PI3K-Akt signaling provides insights into disease mechanisms and therapeutic targets.
Phosphoinositide 3-kinases (PI3Ks) are lipid kinases that phosphorylate phosphatidylinositol (4,5)-bisphosphate (PIP2) to generate phosphatidylinositol (3,4,5)-trisphosphate (PIP3). Class IA PI3Ks consist of a p85 regulatory subunit and a p110 catalytic subunit. In neurons, PI3K activation occurs through:
- Receptor tyrosine kinase activation: Growth factors bind to RTKs (TrkA, TrkB, IGF-1R)
- IRS-1/2 recruitment: Insulin receptor substrate proteins dock at phosphotyrosine motifs
- PI3K membrane recruitment: p85 SH2 domains bind phosphorylated IRS
- PIP3 generation: p110 catalytic subunit phosphorylates PIP2 to PIP3
Akt (PKB) is a serine/threonine kinase with three isoforms (Akt1, Akt2, Akt3) expressed in the brain. Akt activation requires:
- PH domain binding: Akt PH domain binds PIP3 at the plasma membrane
- PDK1 phosphorylation: Phosphoinositide-dependent kinase-1 phosphorylates Akt at Thr308
- mTORC2 phosphorylation: mTOR complex 2 phosphorylates Akt at Ser473
- Full activation: Fully activated Akt translocates to various cellular compartments
Akt directly activates mTORC1 through multiple mechanisms:
- TSC2 phosphorylation: Akt phosphorylates tuberin (TSC2), relieving mTORC1 inhibition
- Rheb activation: Active Rheb-GTP directly activates mTORC1
- Translation regulation: mTORC1 promotes protein synthesis via S6K and 4E-BP1
In PD, mTORC1 dysregulation affects:
- Autophagy inhibition: mTORC1 suppresses autophagy, leading to protein aggregate accumulation
- Synaptic plasticity: Altered translation affects synaptic function
- Cell growth: Aberrant mTORC1 signaling disrupts neuronal homeostasis
Akt phosphorylates GSK-3β at Ser9, inhibiting its kinase activity. GSK-3β is a key tau kinase and its dysregulation contributes to:
- Tau hyperphosphorylation: Active GSK-3β phosphorylates tau at multiple sites
- α-Synuclein aggregation: GSK-3β may promote α-synuclein phosphorylation at Ser129
- Mitochondrial dysfunction: GSK-3β affects mitochondrial quality control
¶ Bad and Apoptosis Regulation
Akt phosphorylates the pro-apoptotic protein Bad at Ser136, sequestering it in the cytoplasm and preventing apoptosis. This provides a critical survival signal for dopaminergic neurons, which are particularly vulnerable to apoptotic insults.
Post-mortem studies of PD substantia nigra demonstrate:
- Decreased Akt phosphorylation at both Thr308 and Ser473
- Reduced PI3K activity
- Increased PTEN activity (negative regulator)
- Correlation between Akt reduction and disease severity
Several PD-linked genes affect PI3K-Akt signaling:
| Gene |
Effect on PI3K-Akt |
Mechanism |
| SNCA |
Inhibits |
α-Synuclein oligomers interfere with Akt signaling |
| LRRK2 |
Complex |
Mutant LRRK2 may affect Akt pathway |
| PARKIN |
Protects |
Parkin regulates Akt activity |
| PINK1 |
Protects |
PINK1 affects Akt-mediated survival |
| DJ-1 |
Protects |
DJ-1 positively regulates PI3K-Akt |
| GBA |
Impairs |
Glucocerebrosidase deficiency affects Akt |
PI3K-Akt signaling critically regulates mitochondrial quality control:
- PGC-1α activation: Akt promotes mitochondrial biogenesis via PGC-1α
- Mitophagy: Akt regulates autophagy of damaged mitochondria
- Mitochondrial dynamics: Akt affects fission/fusion balance
- Energy metabolism: Akt influences glycolysis and oxidative phosphorylation
Neurotrophic factors that activate PI3K-Akt:
- GDNF: Glial cell line-derived neurotrophic factor activates Ret receptor → PI3K-Akt
- BDNF: Brain-derived neurotrophic factor via TrkB
- IGF-1: Insulin-like growth factor-1
- ** Akt activators**: Direct Akt activators in development
- mTOR inhibitors: Rapamycin and analogs to restore autophagy
- GSK-3β inhibitors: To reduce tau pathology
- AAV-GDNF: Clinical trials for PD
- AAV-BDNF: Neuroprotective approaches
- PI3K isoform-specific modulators: Targeting neuronal PI3K-C2α
flowchart TD
A["Growth Factors<br/>GDNF, BDNF, IGF-1"] --> B["RTK / Trk Receptors"]
B --> C["IRS-1/2"]
C --> D["PI3K p85/p110"]
D --> E["PIP3 Production"]
E --> F["Akt Recruitment"]
F --> G["PDK1"]
F --> H["mTORC2"]
G --> I["Akt Thr308 Phos"]
H --> J["Akt Ser473 Phos"]
I --> K["Fully Active Akt"]
J --> K
K --> L["mTORC1 Activation"]
K --> M["GSK-3β Inhibition"]
K --> N["Bad Phosphorylation"]
K --> O["PGC-1α Activation"]
L --> P["Protein Synthesis"]
L --> Q["Autophagy Inhibition"]
M --> R["Tau Phosphorylation ↓"]
M --> S["α-Syn Phosphorylation ↓"]
N --> T["Apoptosis Block"]
O --> U["Mitochondrial Biogenesis"]
V["PD Pathology"] --> W["α-Syn Aggregation"]
V --> X["Mitochondrial Dysfunction"]
V --> Y["Autophagy Impairment"]
W --> Z["PI3K-Akt Inhibition"]
X --> Z
Y --> Z
Z -.-> |Reduced| D
style K fill:#c8e6c9
style T fill:#ffcdd2
style Z fill:#ffcdd2
Multiple studies have documented PI3K-Akt pathway dysregulation in PD brain tissue:
- Substantia nigra pars compacta: Reduced Akt phosphorylation at both Thr308 and Ser473 sites compared to age-matched controls [saluja2010]
- Frontal cortex: Altered PI3K subunit expression, particularly reduced p85α
- Temporal correlation: Degree of Akt inhibition correlates with disease duration and severity
Peripheral blood studies have identified:
- Lymphocyte Akt activity: Reduced in PD patients compared to healthy controls
- Serum IGF-1: Decreased levels correlate with motor symptom severity
- CSF biomarkers: Phospho-Akt/total Akt ratio reduced in PD CSF
PET studies using Akt pathway markers suggest:
- Reduced Akt signaling in the substantia nigra correlates with dopaminergic neuron loss
- Akt pathway activity predicts response to dopaminergic therapy
GDNF activates the PI3K-Akt pathway through Ret receptor tyrosine kinase, providing potent neuroprotection for dopaminergic neurons:
| Aspect |
Details |
| Receptor |
RET/GFRα1 complex |
| Downstream |
PI3K-Akt, MAPK/ERK pathways |
| Clinical trials |
Multiple Phase I-II trials |
| Delivery methods |
AAV-GDNF, protein infusion |
BDNF activates TrkB receptors, stimulating PI3K-Akt signaling:
- Neuroprotective effects: Prevents dopaminergic neuron death in vitro and in vivo
- Synaptic plasticity: Enhances synaptic function through Akt-mediated mechanisms
- Clinical challenge: Poor brain penetration limits therapeutic utility
Direct Akt activators under development include:
| Compound |
Mechanism |
Development Stage |
| GSK2147895 |
Allosteric Akt activator |
Preclinical |
| SC66 |
Akt inhibitor with paradoxical activation |
Research |
| PRT41607 |
Akt pathway modulator |
Preclinical |
Several FDA-approved drugs indirectly activate PI3K-Akt:
- Metformin: Activates LKB1-AMPK, upstreams of Akt pathway
- Exenatide: GLP-1R agonist activates PI3K-Akt through insulin signaling
- Lithium: Inhibits GSK-3β, downstream of Akt
| Approach |
Target |
Status |
| AAV-GDNF |
Neuronal survival |
Phase II |
| AAV-BDNF |
Neuroprotection |
Phase I |
| AAV-PI3K |
Pathway activation |
Preclinical |
| AAV-Akt |
Cell survival |
Preclinical |
Given the complexity of PD pathogenesis, PI3K-Akt targeted therapies may be combined with:
| Combination |
Rationale |
Status |
| PI3K-Akt + mTOR inhibitor |
Complete pathway modulation |
Preclinical |
| PI3K-Akt + MAO-B inhibitor |
Symptomatic + disease-modifying |
Phase I |
| PI3K-Akt + GLP-1 agonist |
Multi-target metabolic protection |
Phase II |
| PI3K-Akt + antioxidant |
Oxidative stress + survival |
Preclinical |
Patients most likely to benefit from PI3K-Akt targeting:
- LRRK2 G2019S carriers: Pathway dysregulation documented
- GBA mutation carriers: PI3K-Akt impairment from glucocerebrosidase loss
- PINK1/PARKIN mutations: Akt-mediated survival pathways compensatory
- Early stage (Hoehn-Yahr 1-2): Maximum benefit from neuroprotective therapy
- Mid stage (Hoehn-Yahr 2.5-3): May slow progression
- Late stage: Limited benefit due to neuron loss
| Biomarker |
Predictive Value |
| Low lymphocyte Akt activity |
Good responder |
| Reduced serum IGF-1 |
Consider growth factor therapy |
| High CSF α-synuclein |
May benefit from autophagy modulation |
¶ Adverse Effects and Safety
- Intracranial delivery: Risk of infection, hemorrhage
- Immunogenicity: Antibody formation against delivered proteins
- Off-target effects: Non-specific neurotrophic effects
- Metabolic effects: Hyperglycemia with some Akt activators
- Cardiovascular: Potential effects on cardiac function
- Cancer risk: Long-term Akt activation concerns
- PI3K isoform-specific inhibitors/activators: Targeting neuronal PI3K-C2α
- Akt isoform-selective modulators: Akt1 vs Akt2 specificity
- PTEN inhibitors: Restoring PIP3 production
- Neuroprotective trials: Require long duration, biomarker enrichment
- Combination designs: Multi-arm trials with multiple mechanisms
- Personalized medicine: Genetic stratification for optimal response
- [proteins/akt] - Akt/PKB
- [proteins/gsk3b] - GSK-3β
- [proteins/mtor] - mTOR
- [proteins/gdnf] - GDNF
- [proteins/bdnf] - BDNF
- [genes/parkin] - PARKIN
- [genes/pink1] - PINK1
- [genes/lrrk2] - LRRK2
- [genes/gba] - GBA
- [mechanisms/mitochondrial-dysfunction] - Mitochondrial Dysfunction
- [mechanisms/autophagy-lysosome-pathway] - Autophagy
- [mechanisms/insulin-signaling-neurodegeneration] - Insulin Signaling
- [diseases/parkinsons-disease] - Parkinson's Disease
The PI3K-Akt pathway provides critical survival signals for dopaminergic neurons, and its dysfunction contributes to multiple aspects of PD pathogenesis. Therapeutic strategies targeting this pathway, including growth factor delivery, small molecule activators, and gene therapy approaches, represent promising avenues for disease modification in PD. Clinical translation remains challenging due to delivery issues and pathway complexity, but biomarker-driven patient selection and combination approaches offer promise for future development.