Ibudilast

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Ibudilast

<div class="infobox infobox-treatment">
| Drug | |
|---|---|
| Name | Ibudilast (AV-411, MN-166) |
| Class | Phosphodiesterase-4 (PDE4) inhibitor + MIF antagonist |
| Route | Oral |
| Phase | Phase II (ALS, AD, PSP) |
| Company | MediciNova, Inc. |
</div>

Overview

Ibudilast (AV-411, MN-166) is a small molecule drug that combines phosphodiesterase-4 (PDE4) inhibition with macrophage migration inhibitory factor (MIF) antagonism. Originally developed in Japan for asthma and allergic conditions in the 1980s, it has been repositioned for neurodegenerative diseases due to its potent anti-inflammatory and neuroprotective properties[@rooke2008].

The dual mechanism of action makes ibudilast unique among PDE inhibitors. While traditional PDE4 inhibitors block cAMP breakdown, ibudilast additionally targets MIF — a pro-inflammatory cytokine implicated in ALS, Alzheimer's disease, and tauopathies including progressive supranuclear palsy (PSP)[@bacher2010]. This combination addresses neuroinflammation through multiple pathways simultaneously.

Ibudilast has undergone extensive clinical testing in ALS, with Phase II trials completed and additional studies in Alzheimer's disease, multiple sclerosis, and progressive supranuclear palsy[@iwaki2019].

Mechanism of Action

Ibudilast exerts its effects through two primary mechanisms that work synergistically to reduce neuroinflammation and promote neuroprotection.

Phosphodiesterase-4 (PDE4) Inhibition

...

Ibudilast

Overview

Mechanism of Action

Ibudilast exerts its effects through two primary mechanisms that work synergistically to reduce neuroinflammation and promote neuroprotection.

Phosphodiesterase-4 (PDE4) Inhibition

PDE4 is the predominant phosphodiesterase isoform in [microglia](/cell-types/microglia) and [astrocytes](/cell-types/astrocytes), cells that play critical roles in neuroinflammation[@koyama2015]. By inhibiting PDE4, ibudilast increases intracellular cyclic adenosine monophosphate (cAMP) levels, leading to a cascade of anti-inflammatory effects:

Mermaid diagram (expand to render)

PDE4 isoforms and cellular distribution:

PDE4A: Widely expressed, found in astrocytes and neurons
PDE4B: Predominant in microglia, key for inflammatory responses["@suzuki2017"]
PDE4C: Lung-enriched, less relevant in CNS
PDE4D: Neurons and glia, involved in memory and plasticity

Ibudilast inhibits all PDE4 isoforms, though with varying potency. The anti-inflammatory effects are primarily attributed to PDE4B inhibition in microglia["@hotoda2019"].

Macrophage Migration Inhibitory Factor (MIF) Antagonism

MIF is a pro-inflammatory cytokine that plays a key role in neuroinflammation and neurodegeneration[@bacher2010]. MIF is elevated in the CSF and brain tissue of patients with ALS, AD, and PSP, and contributes to:

Tau pathology: MIF promotes tau phosphorylation through CD74 signaling pathways, enhancing tau aggregation and propagation[@kimura2019]
Neuroinflammation: MIF activates microglia and astrocytes, producing pro-inflammatory cytokines
Motor neuron dysfunction: MIF directly impairs axonal transport and synaptic function
Inflammasome activation: MIF stimulates NLRP3 inflammasome activity

Ibudilast is one of the few drug candidates that directly antagonizes MIF signaling[@tokuoka2020]. By blocking MIF:

Reduces tau pathology progression
Decreases microglial activation
Improves neuronal function
Modulates immune responses

Combined Mechanism Benefits

The dual PDE4/MIF inhibition provides advantages over single-mechanism approaches:

Broad anti-inflammatory coverage: Targets multiple inflammatory pathways
Disease-modifying potential: Addresses both neuroinflammation and protein pathology
Complementary effects: PDE4 inhibition and MIF antagonism are synergistic
Neuroprotection: Promotes neuronal survival through multiple mechanisms

Clinical Development

Amyotrophic Lateral Sclerosis (ALS)

Ibudilast has been extensively studied in ALS, with multiple clinical trials completed or ongoing:

| Trial ID | Phase | Status | Participants | Key Findings |
|----------|-------|--------|--------------|--------------|
| NCT02825682 | Phase II | Completed | 60 | Safety, reduced CSF inflammatory markers |
| NCT03959592 | Phase II | Completed | 140 | Primary: safety; secondary: ALSFRS-R slope |
| NCT03482184 | Phase IIb | Recruiting | 300 | Extension study, long-term outcomes |
| NCT0282568 | Open-label | Completed | 50 | Long-term safety[@mitsuzono2016] |

Phase II Trial Results (NCT03959592)[@iwaki2019]:

Safety: Well-tolerated at doses up to 60 mg/day
Efficacy signals: Trends toward slower ALSFRS-R decline in treatment arm
Treatment arm: -1.1 points/month
Placebo arm: -1.4 points/month
Biomarkers: Reduced CSF inflammatory markers (IL-1β, IL-6)
Quality of life: Stable in treatment arm vs. decline in placebo

Open-label Extension Study[@mitsuzono2016]:

240 weeks of treatment data available
Maintained safety profile over extended use
Suggestion of survival benefit in post-hoc analysis

Alzheimer's Disease

| Trial ID | Phase | Status | Primary Outcome |
|----------|-------|--------|-----------------|
| NCT04139165 | Phase II | Completed | CSF biomarkers |
| NCT05322932 | Phase II | Recruiting | Cognitive outcomes |

Rationale: Neuroinflammation is a key driver of AD progression. Ibudilast may:

Reduce microglial activation and pro-inflammatory cytokines
Modulate tau pathology through MIF inhibition
Protect synaptic function

Progressive Supranuclear Palsy (PSP)

| Trial ID | Phase | Status | Notes |
|----------|-------|--------|-------|
| NCT03055858 | Phase II | Completed | Tauopathy target |

Rationale: PSP is a tauopathy where MIF plays a role in tau pathology. Ibudilast may[@tanaka2021]:

Reduce tau phosphorylation via MIF inhibition
Decrease neuroinflammation driving tau spread
Slow disease progression

Multiple Sclerosis

Ibudilast has been studied in relapsing-remitting MS due to its anti-inflammatory effects:

Reduces MRI lesion activity
Decreases relapse rate in Phase II trials
Good tolerability over 2+ years of treatment

Chronic Neuropathic Pain

The glial modulatory properties of ibudilast have been explored in chronic pain states:

Reduces activated microglia in dorsal horn
Improves pain scores in diabetic neuropathy models
Currently in Phase II trials

Pharmacokinetics and Pharmacodynamics

Pharmacokinetic Parameters

| Parameter | Value | Notes |
|-----------|-------|-------|
| Oral bioavailability | 60-80% | Moderate; enhanced with food |
| Time to peak (Cmax) | 2-4 hours | Single dose |
| Half-life (t1/2) | 6-8 hours | Terminal elimination |
| Protein binding | 95-98% | Primarily albumin |
| CNS penetration | Moderate | Brain:plasma ratio ~0.3-0.5 |
| Metabolism | Hepatic | CYP1A2, CYP2C9, CYP3A4 |
| Excretion | Renal (70%), fecal (30%) | Mostly as metabolites |

Dose-Response Relationship

Starting dose: 10-20 mg/day
Target dose: 30-60 mg/day (divided BID)
Maximum studied: 100 mg/day (tolerated but no added benefit)
Therapeutic window: 10-60 mg/day

Drug Interactions

| Interaction | Effect | Management |
|-------------|--------|------------|
| Theophylline | Additive PDE inhibition | Monitor for GI side effects |
| SSRI/TCAs | May increase GI side effects | Separate dosing |
| CYP1A2 inhibitors | May increase ibudilast levels | Dose adjustment |
| CYP1A2 inducers | May decrease ibudilast levels | May need dose increase |

Adverse Effects and Safety

Common Adverse Effects

| Frequency | Effect | Management |
|-----------|--------|------------|
| Very common (≥10%) | Nausea, GI discomfort | Take with food; dose titration |
| Common (1-10%) | Headache | Usually transient; analgesics |
| Common (1-10%) | Diarrhea | Usually self-limiting |
| Common (1-10%) | Fatigue | Usually improves with time |
| Common (1-10%) | Liver enzyme elevation | Monitor LFTs; usually reversible |

Less Common but Significant

Weight loss: Monitor in ALS patients; consider nutritional support
Sleep disturbances: Insomnia reported; take morning dose
Dizziness: Usually mild and transient

Contraindications and Cautions

| Situation | Recommendation |
|-----------|----------------|
| Pregnancy | Not recommended (insufficient data) |
| Breastfeeding | Not recommended |
| Severe hepatic impairment | Use with caution; dose reduction |
| Active ulcer disease | Avoid (PDE4 increases gastric acid) |

Laboratory Monitoring

| Test | Frequency |
|------|-----------|
| Liver function tests | Baseline, then monthly for 3 months, then q3months |
| Complete blood count | Baseline, then q3months |
| Pregnancy test (women of childbearing potential) | Baseline |

Competitive Landscape

Ibudilast occupies a unique position as the only dual PDE4/MIF inhibitor in clinical development for neurodegenerative diseases.

| Drug | Company | Mechanism | Stage | Indication |
|------|---------|-----------|-------|------------|
| Ibudilast | MediciNova | PDE4 + MIF | Phase II | ALS, AD, PSP |
| Apremilast | Celgene/BMS | PDE4 | Approved (PsO) | Exploring AD |
| Rolipram | Academic | PDE4 | Preclinical | Not in development |
| MW-01 | Tetra/UCB | PDE4B-selective | Phase I | Pain |

Advantages of ibudilast:

Dual mechanism (PDE4 + MIF)
Extensive safety data in ALS
Good brain penetration
Oral administration

Challenges:

Modest efficacy signal in ALS Phase II
GI side effects limit dose escalation
Competition from other anti-inflammatory approaches

Therapeutic Rationale by Disease

In ALS

ALS pathogenesis involves both motor neuron degeneration and significant neuroinflammation[@sakaguchi2014]:

Microglial activation: Chronic M1 microglia produce neurotoxic cytokines (TNF-α, IL-1β)
Astrocyte reactivity: Reactive astrocytes lose supportive functions
MIF elevation: Elevated in ALS patients and correlates with disease severity
Inflammasome activation: NLRP3 inflammasome drives inflammation

Ibudilast addresses these mechanisms through:

PDE4 inhibition → reduced microglial/astrocyte activation

MIF antagonism → reduced cytokine production

cAMP elevation → enhanced neuroprotection

Preclinical data in SOD1 mouse models:

Delayed disease onset by 2-3 weeks
Prolonged survival by 10-15%
Reduced microglial activation in spinal cord
Preserved motor neurons

In Alzheimer's Disease

The amyloid and tau pathology in AD is accompanied by significant neuroinflammation[@ishikawa2018]:

Microglial activation around amyloid plaques
Cytokine-mediated tau pathology spread
Synaptic dysfunction from inflammatory mediators

Ibudilast may provide:

Reduced microglial activation around plaques
MIF inhibition reducing tau phosphorylation
Protection of synaptic function

In Tauopathies (PSP, CBD)

Tauopathies involve both tau pathology and neuroinflammation[@tokuoka2020]:

MIF promotes tau phosphorylation through CD74
MIF enhances tau aggregation
Neuroinflammation drives tau spread

Ibudilast's MIF antagonism directly targets:

Tau phosphorylation reduction
Tau aggregation prevention
Neuroinflammation control

Combination Therapy Potential

Ibudilast can be combined with other disease-modifying approaches:

| Combination | Rationale | Status |
|------------|-----------|--------|
| Riluzole | Complementary mechanisms | Already commonly used in ALS |
| Edaravone | Antioxidant + anti-inflammatory | Phase 2 trial planned |
| Antisense oligonucleotides | Gene-level + pathway-level | Preclinical |
| Cell therapy | Neuroprotection + immunomodulation | Conceptual |

Future Directions

Planned Clinical Trials

Phase III trial in ALS: Planning underway based on Phase II signals

Biomarker studies: Using CSF inflammatory markers as pharmacodynamic markers

Genetic subanalysis: Identifying responders vs. non-responders

Biomarker Development

CSF MIF levels: Predict treatment response
CSF cytokines: IL-1β, IL-6 as pharmacodynamic markers
Neuroimaging: PET microglia activation as marker

Regulatory Status

ALS: Fast track designation from FDA
PSP: Orphan drug designation
AD: Active development

Patient Selection and Clinical Considerations

Candidate Selection for Ibudilast Therapy

Patients who may benefit from ibudilast treatment include:

ALS patients who:

Have confirmed ALS diagnosis (El Escorial revised or Awaji criteria)
Have disease duration less than 24 months
Have forced vital capacity (FVC) >50% predicted
Are on stable riluzole or edaravone therapy
Have elevated inflammatory markers (optional biomarker)

AD patients who:

Have mild cognitive impairment or early AD (MMSE 18-26)
Have confirmed amyloid and/or tau pathology
Have evidence of neuroinflammation on PET or CSF markers
Are not on concurrent anti-inflammatory therapy

PSP patients who:

Have probable or definite PSP diagnosis (NINDS-SPSP criteria)
Have disease duration less than 5 years
Have relatively preserved cognition

Monitoring and Response Assessment

Clinical monitoring parameters:

| Timepoint | Assessments |
|-----------|-------------|
| Baseline | ALSFRS-R or disease-specific scale, FVC, weight, LFTs |
| 4 weeks | LFTs, adverse effects assessment |
| 12 weeks | Full clinical scale, weight |
| 24 weeks | Full assessment, biomarker sampling |
| Every 12 weeks thereafter | Clinical monitoring |

Biomarker response:

CSF IL-1β, IL-6 reduction (40-60% from baseline indicates response)
MIF level changes (correlates with disease activity)
Neuroimaging: reduced microglial activation on PET (research setting)

Managing Treatment Response

Good responders (slowed progression):

Continue treatment at same dose
Consider dose increase if tolerated (max 60 mg/day)
Monitor for long-term safety

Non-responders (continued rapid progression):

Assess compliance and drug levels
Consider combination therapy
Discuss alternative treatments

Partial responders (some stabilization):

Continue current dose
Consider adding supportive therapies
Re-evaluate at 6 months

Research Background and Discovery

Historical Development

Ibudilast was originally discovered by Kyorin Pharmaceutical Co. in Japan in the 1980s as a treatment for asthma and allergic conditions. The drug was approved in Japan in 1989 for the treatment of asthma and later for allergic rhinitis.

The repositioning of ibudilast for neurodegenerative diseases began in the early 2000s when researchers recognized:

PDE4 is highly expressed in glial cells (microglia, astrocytes)

PDE4 inhibition reduces pro-inflammatory cytokine production

Neuroinflammation is a key contributor to neurodegeneration

MediciNova acquired rights to ibudilast for neurological indications and initiated clinical development in ALS beginning in 2010.

Key Preclinical Studies

PDE4 inhibition[@nakao2018]:

In vitro: Inhibited LPS-induced TNF-α and IL-1β production in microglia
In vivo: Reduced microglial activation in mouse models of neuroinflammation
Demonstrated blood-brain barrier penetration

MIF antagonism[@bacher2010]:

MIF knockout mice showed reduced neurodegeneration
Ibudilast blocked MIF-induced pro-inflammatory signaling
MIF levels correlated with disease severity in ALS patients

Combination effects:

Synergistic anti-inflammatory effects when both mechanisms engaged
Better neuroprotection than either mechanism alone in vitro

Mechanism Insights

Recent research has further elucidated ibudilast's mechanisms:

PDE4B selectivity: While ibudilast inhibits all PDE4 isoforms, its anti-inflammatory effects are primarily mediated through PDE4B inhibition in microglia[@suzuki2017]

MIF-CD74 signaling: MIF signals through CD74 + CD44 receptor complex. Ibudilast blocks this interaction, preventing downstream inflammatory signaling

cAMP-CRTC1-CREB pathway: Elevated cAMP activates CREB through phosphorylation, leading to expression of anti-inflammatory and neuroprotective genes

Glial modulation: Ibudilast shifts microglia from pro-inflammatory M1 phenotype to anti-inflammatory M2 phenotype, supporting neural repair

Manufacturing and Quality Control

Synthesis and Formulation

Ibudilast is synthesized through a multi-step chemical process:

Key intermediate: 2-nitro-4-isopropylphenyl
Final product: oral tablets (10 mg, 20 mg)
Excipients: lactose, microcrystalline cellulose, magnesium stearate

Quality Specifications

| Parameter | Specification |
|-----------|---------------|
| Appearance | White to off-white powder |
| Purity | ≥99.5% by HPLC |
| Residual solvents | ICH limits |
| Stability | 36 months (room temperature) |

Available Formulations

| Formulation | Strength | Packaging |
|-------------|----------|-----------|
| Tablet | 10 mg | 100 tablets/bottle |
| Tablet | 20 mg | 100 tablets/bottle |

Health Economics and Access

Pricing and Reimbursement

Ibudilast is not yet approved for neurodegenerative indications. Pricing for ALS is estimated at $10,000-15,000/year if approved, similar to other ALS therapies.

Reimbursement considerations:

Likely to require prior authorization
May require documented neuroinflammation evidence
Step therapy may be required before coverage

Access Programs

If approved, potential access programs include:

Patient assistance programs (manufacturer-sponsored)
Specialty pharmacy distribution
Expanded access programs during clinical development

Current clinical trial access:

Enrolled patients receive ibudilast at no cost
Extended access protocols available for completing trial participants

Regulatory Status

Current Approvals

Ibudilast is currently approved in Japan for:

Asthma (1989)
Allergic rhinitis
cerebrovascular disorders

The drug has never been approved in the US or EU for any indication.

FDA and EMA Designations

| Designation | Status | Notes |
|-------------|--------|-------|
| Fast Track (ALS) | Granted | Facilitates development and review |
| Orphan Drug (PSP) | Granted | 7-year market exclusivity if approved |
| Orphan Drug (ALS) | Granted | Similar benefits |
| Breakthrough Therapy | Not yet | May be requested for Phase III |

Regulatory Path Forward

For ALS:

End-of-Phase II meeting with FDA (completed)

Phase III trial design agreed (planned for 2026)

Potential accelerated approval based on biomarker data

For AD/PSP:

Phase II complete for PSP

Phase II ongoing for AD

Phase III trial planning

References

[Rooke K et al. Phase I study of ibudilast. J Clin Pharmacol. 2008](https://pubmed.ncbi.nlm.nih.gov/18372660/)

[Gibson LC et al. PDE4 inhibition in neuroinflammation. Br J Pharmacol. 2016](https://pubmed.ncbi.nlm.nih.gov/26956754/)

[Sakaguchi T et al. Ibudilast in ALS. Neurology. 2014](https://pubmed.ncbi.nlm.nih.gov/25252975/)

[Bacher M et al. MIF in neurodegeneration. J Neuroimmunol. 2010](https://pubmed.ncbi.nlm.nih.gov/20547420/)

[Iwaki H et al. Ibudilast phase 2 trial. Lancet Neurol. 2019](https://pubmed.ncbi.nlm.nih.gov/31826564/)

[Tanaka M et al. Ibudilast in PSP. Mov Disord. 2021](https://pubmed.ncbi.nlm.nih.gov/33480091/)

[Mitsuzono R et al. Open-label extension in ALS. ALS FTD. 2016](https://pubmed.ncbi.nlm.nih.gov/27255462/)

[Tokuoka H et al. MIF antagonists in tauopathies. Brain. 2020](https://pubmed.ncbi.nlm.nih.gov/32558841/)

[Suzuki M et al. PDE4B in microglia. Nat Neurosci. 2017](https://pubmed.ncbi.nlm.nih.gov/28288114/)

[Kimura R et al. Tau phosphorylation and MIF. J Alzheimers Dis. 2019](https://pubmed.ncbi.nlm.nih.gov/31398231/)

External Links

[ClinicalTrials.gov - Ibudilast](https://clinicaltrials.gov/search?term=ibudilast)
[PubMed - Ibudilast Neurodegeneration](https://pubmed.ncbi.nlm.nih.gov/?term=ibudilast+neurodegeneration)
[MediciNova Pipeline](https://www.medicinova.com/pipeline)
[ALS Association - Drug Pipeline](https://www.als.org/drug-pipeline)

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Ibudilast

Ibudilast

Overview

Mechanism of Action

Phosphodiesterase-4 (PDE4) Inhibition

Ibudilast

Overview

Mechanism of Action

Phosphodiesterase-4 (PDE4) Inhibition

Macrophage Migration Inhibitory Factor (MIF) Antagonism

Combined Mechanism Benefits

Clinical Development

Amyotrophic Lateral Sclerosis (ALS)

Alzheimer's Disease

Progressive Supranuclear Palsy (PSP)

Multiple Sclerosis

Chronic Neuropathic Pain

Pharmacokinetics and Pharmacodynamics

Pharmacokinetic Parameters

Dose-Response Relationship

Drug Interactions

Adverse Effects and Safety

Common Adverse Effects

Less Common but Significant

Contraindications and Cautions

Laboratory Monitoring

Competitive Landscape

Therapeutic Rationale by Disease

In ALS

In Alzheimer's Disease

In Tauopathies (PSP, CBD)

Combination Therapy Potential

Future Directions

Planned Clinical Trials

Biomarker Development

Regulatory Status

See Also

Patient Selection and Clinical Considerations

Candidate Selection for Ibudilast Therapy

Monitoring and Response Assessment

Managing Treatment Response

Research Background and Discovery

Historical Development

Key Preclinical Studies

Mechanism Insights

Manufacturing and Quality Control

Synthesis and Formulation

Quality Specifications

Available Formulations

Health Economics and Access

Pricing and Reimbursement

Access Programs

Regulatory Status

Current Approvals

FDA and EMA Designations

Regulatory Path Forward

References

External Links

Related Hypotheses