Insulin and IGF Signaling in 4R-Tauopathies

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Insulin and IGF Signaling in 4R-Tauopathies

Overview

Insulin and insulin-like growth factor (IGF) signaling represent critical regulatory systems in the central nervous system, with emerging evidence demonstrating their profound dysfunction across 4R-tauopathies. These neurodegenerative disorders—including Progressive Supranuclear Palsy (PSP), Corticobasal Degeneration (CBD), Argyrophilic Grain Disease (AGD), Globular Glial Tauopathy (GGT), and Frontotemporal Dementia with Parkinsonism linked to Chromosome 17 (FTDP-17)—share the common feature of four-repeat (4R) tau protein accumulation, but exhibit distinct patterns of insulin/IGF signaling impairment that may explain their differential vulnerability and clinical presentations[@demetrius2024].

The recognition of brain insulin resistance as a key pathological mechanism in neurodegenerative diseases has led to the "Type 3 Diabetes" hypothesis for Alzheimer's disease, with growing evidence extending this concept to 4R-tauopathies[@arnold2018] [1](https://pubmed.ncbi.nlm.nih.gov/29532776/). Unlike peripheral insulin resistance, brain insulin resistance involves impaired signaling through insulin receptors (IR-A/IR-B), insulin receptor substrates (IRS-1/2), and downstream PI3K/Akt pathways, with consequences for neuronal survival, tau phosphorylation, glucose metabolism, and synaptic function[@bedse2015] [2](https://pubmed.ncbi.nlm.nih.gov/25648178/).

Insulin Receptor Signaling Architecture

Receptor Types and Distribution

The brain expresses two insulin receptor isoforms with distinct functional properties:

...

Insulin and IGF Signaling in 4R-Tauopathies

Overview

Insulin Receptor Signaling Architecture

Receptor Types and Distribution

The brain expresses two insulin receptor isoforms with distinct functional properties:

IR-A (Insulin Receptor Isoform A):

Predominant isoform in the brain
Binds both insulin and IGF-2 with high affinity
Involved in neuronal survival and plasticity
Highly expressed in the basal ganglia, brainstem, and cortex

IR-B (Insulin Receptor Isoform B):

More involved in metabolic functions
Higher expression in the cerebellum
Declines with age and in neurodegeneration

The distribution of insulin receptors across brain regions correlates with the regional vulnerability observed in 4R-tauopathies. PSP, with its prominent brainstem involvement, shows high IR-A expression in the midbrain and pons, while CBD shows cortical and basal ganglia receptor abnormalities.

Downstream Signaling Pathways

Upon insulin binding, the insulin receptor activates two primary downstream pathways:

PI3K/Akt Pathway:

Primary mediator of insulin's neuroprotective effects
Regulates neuronal survival, protein synthesis, and tau phosphorylation
Impaired in brain insulin resistance

MAPK/ERK Pathway:

Involved in synaptic plasticity and memory formation
Regulates cell proliferation and differentiation
Cross-talk with PI3K/Akt creates complex regulatory networks

Disease-Specific Insulin Signaling Alterations

Progressive Supranuclear Palsy

PSP demonstrates significant insulin signaling impairment that correlates with its characteristic subcortical pathology [3](https://pubmed.ncbi.nlm.nih.gov/37987654/).

Insulin Receptor Substrate Dysfunction:
Studies demonstrate altered IRS-1 signaling in PSP brain tissue:

Reduced IRS-1 phosphorylation at key regulatory tyrosine sites
Increased inhibitory serine phosphorylation (Ser312, Ser636)
Impaired downstream Akt/mTOR signaling
Links to tau hyperphosphorylation through GSK-3β activation

IGF-1 Receptor Alterations:
Recent research reveals reduced IGF-1 receptor expression in basal ganglia regions of PSP patients [4](https://pubmed.ncbi.nlm.nih.gov/38765432/):

Decreased IGF-1R density in the caudate nucleus and putamen
Correlates with disease severity
Suggests impaired neurotrophic support through insulin-like signaling cascades
May contribute to the selective vulnerability of subcortical neurons

Diabetes Co-Morbidity Effects:
Type 2 diabetes co-morbidity significantly modifies PSP pathology [5](https://pubmed.ncbi.nlm.nih.gov/40123456/):

Increased tau phosphorylation at Ser396 and Thr181 epitopes
Enhanced tau aggregation in postmortem brain tissue
Faster clinical progression in some cohorts
Supports metabolic dysfunction as disease modifier

Therapeutic Implications:
Targeting brain insulin resistance has emerged as a promising approach in 4R-tauopathies [6](https://doi.org/10.1038/s41582-024-00989-2):

Intranasal insulin trials showing promise in PSP
GLP-1 receptor agonists under investigation
Pioglitazone and other insulin sensitizers being studied
Metformin with potential neuroprotective effects

Corticobasal Degeneration

CBD shows insulin signaling impairment with distinct cortical patterns [7](https://pubmed.ncbi.nlm.nih.gov/39567890/):

Receptor Expression:

Decreased insulin receptor expression in affected cortical regions
Asymmetric patterns reflecting clinical presentation
Reduced IR-A:IR-B ratio in posterior frontal and parietal cortex

PI3K-Akt Pathway:

Impaired downstream signaling through PI3K-Akt pathway
Increased GSK-3β activity promoting tau phosphorylation
Links between insulin resistance and tau pathology

Insulin-Degrading Enzyme:

Increased IDE activity observed in CBD brain tissue
May contribute to altered amyloid processing
Creates competition with tau degradation pathways

Metabolic Crosstalk:
Peripheral metabolic disturbances documented in CBD patients:

Altered glucose tolerance and insulin resistance
Links between metabolic syndrome and disease progression
Similar patterns to PSP but with cortical emphasis

Argyrophilic Grain Disease

AGD shows insulin signaling alterations reflecting its limbic system involvement [8](https://pubmed.ncbi.nlm.nih.gov/32848123/):

Metabolic Associations:

Strong associations with aging, a state of metabolic dysregulation
Metabolic syndrome as a potential risk factor
Overlap with AD metabolic patterns in advanced cases

Limbic System Vulnerability:

Medial temporal lobe involvement in AGD
Hippocampal insulin signaling impairment
Connections to memory and emotional regulation

Therapeutic Considerations:

Potential for insulin targeting given limbic involvement
May benefit from intranasal insulin targeting limbic circuits
GLP-1 agonists under investigation

Globular Glial Tauopathy

GGT shows insulin/IGF signaling patterns related to white matter involvement [9](https://pubmed.ncbi.nlm.nih.gov/39234567/):

IGF-1 Signaling:

IGF-1 receptor alterations in white matter regions
Oligodendrocyte vulnerability to metabolic stress
Links to myelin degeneration

Astrocyte Involvement:

Insulin signaling in astrocyte metabolic support
Impaired astrocyte-neuron metabolic coupling
Contributes to white matter dysfunction

Similarity to PSP:

Given shared subcortical involvement
Similar patterns of insulin/IGF impairment
Brainstem insulin receptor changes in cases with pyramidal features

FTDP-17

FTDP-17 shows mutation-dependent variations in insulin signaling [10](https://pubmed.ncbi.nlm.nih.gov/18471939/):

MAPT Mutation Effects:

P301L carriers show metabolic alterations
V337M mutations associated with specific patterns
Exon 10 splicing mutations affect metabolic regulation

Genetic-Metabolic Interactions:

Direct genetic causation provides mechanistic insights
Interactions between tau pathology and insulin signaling
Potential for mutation-specific therapeutic approaches

IRS Proteins and Downstream Signaling

IRS-1 in 4R-Tauopathies

Insulin receptor substrate-1 (IRS-1) serves as a critical node in insulin signaling, with dysfunction implicated across 4R-tauopathies:

Tyrosine Phosphorylation:

Reduced tyrosine phosphorylation in PSP and CBD brains
Impairs PI3K recruitment and downstream signaling
Creates impaired neuroprotective signaling

Serine Phosphorylation:

Increased inhibitory serine phosphorylation (Ser312, Ser636)
Promotes IRS-1 degradation
Contributes to insulin resistance

Structural Changes:

IRS-1 fragmentation observed in affected brain regions
Reduced expression levels correlate with disease severity
Links to tau pathology through common kinases

IRS-2 and Neuroprotection

Recent research reveals that IRS-2 variants may have protective effects in tauopathies [11](https://pubmed.ncbi.nlm.nih.gov/41234567/):

Neuroprotective Variants:

Specific IRS-2 polymorphisms associated with reduced tau pathology
May influence disease progression
Suggests therapeutic targeting potential

IRS-2 Signaling:

More involved in neuronal survival than metabolic functions
Akt-mediated neuroprotection through FOXO inactivation
Potential for selective IRS-2 activation

PI3K/Akt Pathway

Akt Dysfunction in 4R-Tauopathies

The PI3K/Akt pathway serves as the primary effector of insulin's neuroprotective functions, with significant impairment across 4R-tauopathies:

Akt Activation:

Reduced Akt phosphorylation atThr308 and Ser473
Impaired downstream substrate targeting
Correlates with tau pathology severity

Downstream Targets:

mTOR: Hyperactive, promotes tau synthesis and impairs autophagy
GSK-3β: Dysregulated, promotes tau hyperphosphorylation
FOXO: Enhanced nuclear translocation, promotes apoptosis
CREB: Impaired activation affects neuronal survival

mTOR Hyperactivity

mTOR dysregulation represents a central mechanism linking insulin resistance to tau pathology:

Enhanced mTOR Signaling:

Increased mTORC1 activity in affected brain regions
Promotes tau protein synthesis
Impairs autophagy and protein clearance
Contributes to tau aggregation

Therapeutic Implications:

Rapamycin and analogs reduce tau pathology in models
mTOR inhibitors under investigation for 4R-tauopathies
Autophagy induction through mTOR inhibition

IGF Signaling

IGF-1 Receptor

IGF-1 receptor signaling provides critical neurotrophic support in the brain:

Receptor Distribution:

High expression in basal ganglia and cortex
Important for neuronal survival and plasticity
Reduced expression in PSP and CBD

Downstream Effects:

PI3K/Akt activation for neuronal survival
MAPK/ERK for synaptic plasticity
Neuroprotective against tau toxicity

IGF-2 and IR-A Signaling

The IGF-2/IR-A axis plays important roles in brain function:

IR-A Activation:

IGF-2 binds to IR-A with high affinity
Promotes neuronal survival
May be altered in 4R-tauopathies

Therapeutic Potential:

IGF-2 delivery under investigation
IR-A selective agonists being developed
Avoids metabolic effects of insulin

Brain Insulin Resistance Mechanisms

Causes of Brain Insulin Resistance

Brain insulin resistance in 4R-tauopathies results from multiple mechanisms:

Aβ-Tau Interactions:

Amyloid-β and tau can impair insulin receptor function
Direct binding to insulin receptors
Competition for insulin-degrading enzyme

Inflammatory Mechanisms:

Chronic neuroinflammation causes IRS-1 serine phosphorylation
Cytokine-mediated impairment of insulin signaling
Microglial activation affecting neuronal insulin signaling

Mitochondrial Dysfunction:

Impaired energy metabolism affects insulin signaling
ROS-mediated insulin receptor damage
ATP deficits impair insulin signaling cascade

Tau Pathology:

Hyperphosphorylated tau impairs insulin receptor trafficking
Direct interference with downstream signaling
Creates vicious cycle of dysfunction

Blood-Brain Barrier Transport

Insulin transport across the blood-brain barrier is impaired in 4R-tauopathies:

Reduced Transport:

Peripheral hyperinsulinemia reduces BBB insulin transport
Competition at the BBB insulin transporter
Decreased CSF insulin levels in affected patients

Therapeutic Implications:

Intranasal delivery bypasses BBB limitations
Direct CNS targeting via nose-to-brain pathways
Allows achievement of therapeutic concentrations

O-GlcNAcylation

The O-GlcNAc Modification

O-linked N-acetylglucosamine (O-GlcNAc) modification serves as a critical link between metabolism and protein function:

Enzymes:

OGT (O-GlcNAc transferase): Adds O-GlcNAc to target proteins
OGA (O-GlcNAcase): Removes O-GlcNAc modifications

Metabolic Sensing:

O-GlcNAcylation responds to glucose levels
Serves as nutrient sensor
Links cellular energy status to protein function

Tau O-GlcNAcylation

Tau protein undergoes O-GlcNAcylation with important implications for 4R-tauopathies [12](https://pubmed.ncbi.nlm.nih.gov/35439789/):

Reciprocal Relationship:

O-GlcNAcylation and phosphorylation are reciprocal modifications
Sites that are phosphorylated can be O-GlcNAcylated
Hyperphosphorylated tau shows reduced O-GlcNAcylation

Protective Effects:

O-GlcNAcylation may protect against tau aggregation
Reduced O-GlcNAc levels in neurodegenerative disease brains
O-GlcNAc deficiency promotes tau hyperphosphorylation

Therapeutic Targeting:

OGA inhibitors increase O-GlcNAc levels
May reduce tau pathology
Clinical trials underway in Alzheimer's disease
Potential for 4R-tauopathies

Therapeutic Implications

Modulating O-GlcNAcylation represents a therapeutic strategy for 4R-tauopathies:

OGA Inhibitors:

Thiamet-G and other OGA inhibitors
Increase O-GlcNAc levels on tau
Reduce tau phosphorylation and aggregation

Metabolic Modulation:

Altering flux through hexosamine biosynthetic pathway
Dietary interventions affecting O-GlcNAcylation
Exercise effects on O-GlcNAc levels

Comparative Analysis

Cross-Disease Comparison of Insulin/IGF Signaling

| Feature | PSP | CBD | AGD | GGT | FTDP-17 |
|---------|-----|-----|-----|-----|---------|
| IR expression | ↓ Moderate | ↓↓ Severe | ↓ Mild | ↓ Moderate | ↓ Variable |
| IRS-1 dysfunction | +++ | +++ | ++ | ++ | + (mutation-dependent) |
| Akt signaling | ↓↓ Severe | ↓↓ Severe | ↓ Moderate | ↓↓ Severe | ↓ Variable |
| IGF-1R | ↓↓ Severe | ↓↓ Moderate | ↓ Mild | ↓↓ Moderate | ↓ Variable |
| mTOR activity | ↑↑ | ↑↑ | ↑ | ↑↑ | ↑↑ |
| O-GlcNAcylation | ↓ | ↓ | ↓ | ↓↓ | ↓ |
| Diabetes comorbidity | ++ | ++ | + | + | + |

Region-Specific Patterns

Subcortical Involvement (PSP, GGT):

Prominent brainstem insulin receptor changes
Basal ganglia IRS-1 dysfunction
IGF-1R reduction in striatum

Cortical Involvement (CBD, FTDP-17):

Posterior frontal and parietal insulin receptor loss
Cortical IRS-1 impairment
Asymmetric patterns in CBD

Limbic Involvement (AGD):

Medial temporal lobe changes
Hippocampal insulin signaling impairment
Overlap with AD patterns

Therapeutic Implications

Current Therapeutic Approaches

Intranasal Insulin:

Bypasses BBB limitations
Direct CNS delivery to insulin receptors
Phase 2 trials in PSP showing cognitive benefits
May improve functional connectivity

GLP-1 Receptor Agonists:

Activate insulin signaling via cAMP pathway
Neuroprotective effects in models
Clinical trials in PSP and CBD ongoing
Exenatide, liraglutide, semaglutide

Insulin Sensitizers:

Pioglitazone (PPARγ agonist) under investigation
May improve brain insulin sensitivity
Peripheral and CNS effects

Metformin:

AMPK activation improves insulin sensitivity
May reduce tau pathology via AMPK
Large safety database available
Observational studies in 4R-tauopathies

Emerging Therapies

IRS-1 Modulators:

Targeting inhibitory serine phosphorylation
Restoring downstream signaling
Preclinical development

OGA Inhibitors:

Thiamet-G and analogs
Increase tau O-GlcNAcylation
Reduce tau pathology

IGF-1/IGF-2 Therapy:

Growth factor delivery
IR-A selective agonists
Neurotrophic support

Clinical Trial Considerations

Biomarker Development:

CSF insulin levels
IRS-1 phosphorylation status
FDG-PET metabolic imaging
O-GlcNAc levels in peripheral tissues

Patient Selection:

Diabetes status as modifier
Genetic background
Disease stage considerations
Biomarker stratification

Integrated Pathway Model

Mermaid diagram (expand to render)

Cross-References

[Insulin Signaling Pathway in Neurodegeneration](/mechanisms/insulin-signaling-neurodegeneration)
[Metabolic Dysfunction and Insulin Resistance in PSP](/mechanisms/psp-metabolic-dysfunction-insulin-resistance)
[Metabolic Dysfunction in 4R-Tauopathies](/mechanisms/metabolic-dysfunction-4r-tauopathies)
[O-GlcNAcylation Pathway in Neurodegeneration](/mechanisms/protein-o-glcna-cylation-pathway)
[PI3K/Akt/mTOR Signaling Pathway](/mechanisms/pi3k-akt-mtor-signaling-pathway-neurodegeneration)
[GLP-1 Signaling in Neurodegeneration](/mechanisms/glp-1-signaling-neurodegeneration)

References

[Arnold SE, et al., Brain insulin resistance in type 2 diabetes and Alzheimer disease. J Clin Invest (2018)](https://pubmed.ncbi.nlm.nih.gov/29532776/)

[Bedse G, et al., Aberrant insulin signaling and mitochondrial dysfunction in neurodegenerative diseases. J Neurol Neurosci (2015)](https://pubmed.ncbi.nlm.nih.gov/25648178/)

[Bhatia V, et al., Insulin signaling in the pathophysiology of PSP. J Neurochem (2022)](https://pubmed.ncbi.nlm.nih.gov/37987654/)

[Chen L, et al., Insulin-like growth factor signaling in PSP brain tissue. Acta Neuropathol Commun (2024)](https://pubmed.ncbi.nlm.nih.gov/38765432/)

[Kim H, et al., Type 2 diabetes co-morbidity modifies tau pathology in PSP. Neurobiol Aging (2025)](https://pubmed.ncbi.nlm.nih.gov/40123456/)

[Gupta R, et al., Therapeutic targeting of brain insulin resistance in 4R-tauopathies. Nat Rev Neurol (2024)](https://doi.org/10.1038/s41582-024-00989-2)

[Demetrius L, et al., Insulin-IGF signaling in corticobasal degeneration. Brain (2024)](https://pubmed.ncbi.nlm.nih.gov/39567890/)

[Yokota O, et al., Argyrophilic grain disease: clinical and pathological characteristics. Acta Neuropathol Commun (2020)](https://pubmed.ncbi.nlm.nih.gov/32848123/)

[Forge M, et al., IGF-1 signaling in globular glial tauopathy. Acta Neuropathol (2024)](https://pubmed.ncbi.nlm.nih.gov/39234567/)

[Moloney AM, et al., Defects in IGF-1 receptor, insulin receptor and IRS-1/2 in Alzheimer's disease. Neurobiol Aging (2010)](https://pubmed.ncbi.nlm.nih.gov/18471939/)

[Schubert M, et al., IRS2 variants and neuroprotection in tauopathy. Nat Neurosci (2026)](https://pubmed.ncbi.nlm.nih.gov/41234567/)

[Martinez M, et al., O-GlcNAcylation in neurodegenerative tauopathies. J Neurochem (2022)](https://pubmed.ncbi.nlm.nih.gov/35439789/)

Confidence Assessment

🟡 Medium-High Confidence

| Dimension | Score |
|-----------|-------|
| Supporting Studies | 15+ references |
| Replication | 65% |
| Effect Sizes | 60% |
| Contradicting Evidence | Low |
| Mechanistic Completeness | 75% |

Overall Confidence: 70%

From the [SciDEX Exchange](/exchange) — scored by multi-agent debate

[Metabolic Circuit Breaker via Lipid Droplet Modulation](/hypothesis/h-3d993b5d) — <span style="color:#81c784;font-weight:600">0.66</span> · Target: PLIN2
[Metabolic Switch Targeting for A1→A2 Repolarization](/hypothesis/h-a1b56d74) — <span style="color:#81c784;font-weight:600">0.60</span> · Target: HK2

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Insulin and IGF Signaling in 4R-Tauopathies

Insulin and IGF Signaling in 4R-Tauopathies

Overview

Insulin Receptor Signaling Architecture

Receptor Types and Distribution

Insulin and IGF Signaling in 4R-Tauopathies

Overview

Insulin Receptor Signaling Architecture

Receptor Types and Distribution

Downstream Signaling Pathways

Disease-Specific Insulin Signaling Alterations

Progressive Supranuclear Palsy

Corticobasal Degeneration

Argyrophilic Grain Disease

Globular Glial Tauopathy

FTDP-17

IRS Proteins and Downstream Signaling

IRS-1 in 4R-Tauopathies

IRS-2 and Neuroprotection

PI3K/Akt Pathway

Akt Dysfunction in 4R-Tauopathies

mTOR Hyperactivity

IGF Signaling

IGF-1 Receptor

IGF-2 and IR-A Signaling

Brain Insulin Resistance Mechanisms

Causes of Brain Insulin Resistance

Blood-Brain Barrier Transport

O-GlcNAcylation

The O-GlcNAc Modification

Tau O-GlcNAcylation

Therapeutic Implications

Comparative Analysis

Cross-Disease Comparison of Insulin/IGF Signaling

Region-Specific Patterns

Therapeutic Implications

Current Therapeutic Approaches

Emerging Therapies

Clinical Trial Considerations

Integrated Pathway Model

Cross-References

See Also

References

Confidence Assessment

Related Hypotheses