BIIB122

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BIIB122

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Overview

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Overview

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BIIB122, formerly known as DNL151, is a highly selective, brain-penetrant small molecule inhibitor of leucine-rich repeat kinase 2 (LRRK2) developed through a collaboration between Biogen and Denali Therapeutics. Originally discovered and advanced through Phase 1 clinical trials by Denali, BIIB122 was subsequently licensed to Biogen in 2023 as part of a broader neuroscience partnership. The compound represents one of the most advanced LRRK2 inhibitor programs in clinical development for Parkinson's disease["@dnl151"][@biogen].

LRRK2 is one of the most common genetic risk factors for Parkinson's disease, with gain-of-function mutations causing increased kinase activity that leads to impaired lysosomal function, altered autophagy, neuroinflammation, and ultimately dopaminergic neuron death. BIIB122 aims to restore normal LRRK2 activity through reversible kinase inhibition, potentially slowing or halting disease progression rather than merely treating symptoms["@lrrk2biology"].

<div class="infobox infobox-entity">
<table>
<tr><th colspan="2" style="background:#e8f4f8; text-align:center; font-size:1.1em;">BIIB122 (DNL151)</th></tr>
<tr><td><strong>Drug Name</strong></td><td>BIIB122 (DNL151)</td></tr>
<tr><td><strong>Target</strong></td><td>LRRK2 (Leucine-Rich Repeat Kinase 2)</td></tr>
<tr><td><strong>Company</strong></td><td>Biogen / Denali Therapeutics</td></tr>
<tr><td><strong>Indication</strong></td><td>Parkinson's Disease</td></tr>
<tr><td><strong>Mechanism</strong></td><td>Reversible, selective LRRK2 kinase inhibition</td></tr>
<tr><td><strong>Route</strong></td><td>Oral (tablet)</td></tr>
<tr><td><strong>Development Phase</strong></td><td>Phase 2</td></tr>
</table>
</div>

LRRK2 Biology and Parkinson's Disease

LRRK2 Structure and Function

LRRK2 is a large multidomain protein (2527 amino acids, ~286 kDa) with complex architecture that includes multiple functional domains[@lrrk2structure]:

Armadillo repeats (N-terminal): Protein-protein interactions

Ankyrin repeats: Membrane association and localization

LRR (Leucine-Rich Repeat) domain: Protein binding

Kinase domain: Catalytic activity (autophosphorylation, substrate phosphorylation)

WD40 domain (C-terminal): Protein interactions and regulatory functions

The kinase domain is the therapeutic target for small molecule inhibitors like BIIB122. It catalyzes the phosphorylation of multiple substrates, including:

Rab GTPases (Rab10, Rab8A, Rab12, Rab29)
Auto-regulatory sites (Ser1292 autophosphorylation)
Rotatin, AEP, and other neuronal substrates

LRRK2 Mutations in Parkinson's Disease

Over 100 LRRK2 pathogenic variants have been identified, with the G2019S mutation being the most common:

| Mutation | Effect | Prevalence |
|----------|--------|------------|
| G2019S | Increased kinase activity (~2-fold) | ~5% familial PD, ~1% sporadic PD |
| R1441C/G/H | Decreased GTPase activity | ~3-5% familial PD |
| N1437H | Increased kinase activity | Rare |
| Y1699C | Altered protein function | Rare |

The G2019S mutation, located in the kinase domain activation loop, is particularly amenable to pharmacological inhibition, as it results in a kinase that is hyperactive but structurally similar to wild-type[@g2019s].

Pathogenic Mechanisms

LRRK2 gain-of-function mutations cause neurodegeneration through multiple mechanisms:

1. Lysosomal Dysfunction

LRRK2 regulates lysosomal biogenesis and function through phosphorylation of Rab proteins. Mutant LRRK2 leads to[@lysosomal]:

Impaired autophagosome-lysosome fusion
Decreased clearance of alpha-synuclein aggregates
Accumulation of lipofuscin
Lysosomal membrane destabilization

2. Neuroinflammation

LRRK2 is highly expressed in microglia, where its activity modulates inflammatory responses[@neuroinflammation]:

Enhanced pro-inflammatory cytokine production
Increased microglial phagocytosis
Elevated expression of disease-associated microglial markers
Neurotoxic microglial phenotypes

3. Mitochondrial Dysfunction

LRRK2 affects mitochondrial quality control:

Impaired mitophagy through Rab32 and Rab39B interactions
Reduced mitochondrial dynamics
Increased oxidative stress

4. Synaptic Dysfunction

LRRK2 regulates synaptic vesicle trafficking:

Altered dopamine release
Impaired synaptic vesicle recycling
Reduced synaptic plasticity

Mechanism of Action

BIIB122 Pharmacology

BIIB122 is a highly selective LRRK2 kinase inhibitor with the following characteristics[@dnl151][@pkpd]:

Target Selectivity: >100-fold selectivity for LRRK2 over 400+ kinases tested

Reversible Binding: ATP-competitive inhibitor that does not form irreversible adducts

Brain Penetration: Demonstrated CSF exposure at therapeutic doses

Pharmacodynamics: Dose-dependent inhibition of LRRK2 autophosphorylation (Ser1292) in peripheral blood mononuclear cells

Mechanism of Therapeutic Benefit

By inhibiting LRRK2 kinase activity, BIIB122[@preclinical]:

Restores Lysosomal Function: Normalizes autophagy-lysosome pathway activity

Reduces Neuroinflammation: Modulates microglial activation state

Protects Dopaminergic Neurons: Prevents mitochondrial dysfunction and apoptosis

Enhances Protein Clearance: Improves clearance of alpha-synuclein and other aggregates

Biomarker Strategy

BIIB122 development employs pharmacodynamic biomarkers to confirm target engagement[@biomarkers]:

LRRK2 pSer1292: Autophosphorylation marker in blood cells
Rab10 pThr73: Direct LRRK2 substrate phosphorylation
NfL (Neurofilament Light Chain): Neuronal injury marker
Alpha-synuclein in CSF: Disease progression marker

Clinical Development

LUMA Phase 1 Study

The LUMA Phase 1 trial evaluated single and multiple ascending doses of BIIB122 in healthy volunteers[@luma]:

| Parameter | Results |
|-----------|---------|
| Single doses tested | 10-400 mg |
| Multiple doses tested | 25-200 mg daily for 14 days |
| Maximum tolerated dose | Not reached (good safety margin) |
| Target engagement | Dose-dependent LRRK2 pSer1292 inhibition |
| Pharmacokinetics | Linear PK, Tmax 2-4 hours, half-life 8-12 hours |
| Adverse events | Mild-moderate, mainly GI (nausea, diarrhea) |

Key findings:

>80% LRRK2 inhibition achieved at doses ≥100 mg
No serious adverse events
Low dropout rate (<5%)
Supports once-daily or twice-daily dosing

LIGHTHOUSE Phase 2 Trial

The LIGHTHOUSE trial (NCT05477376) is evaluating BIIB122 in patients with Parkinson's disease carrying LRRK2 pathogenic mutations[@lighthouse]:

Study Design:

Randomized, double-blind, placebo-controlled
12-month treatment period
Primary endpoint: Change in MDS-UPDRS Part III (motor) score
Key secondary endpoints: Non-motor symptoms, biomarkers

Patient Population:

Age 40-80 years
Confirmed LRRK2 pathogenic mutation (G2019S, R1441C/G/H, etc.)
Hoehn & Yahr stage 1-3
On stable dopaminergic therapy

Status: Currently recruiting (as of early 2026)

SUNRISE Phase 2 Trial

The SUNRISE trial (NCT05879852) is evaluating BIIB122 in patients with sporadic (non-genetic) Parkinson's disease[@sunrise]:

Study Design:

Similar design to LIGHTHOUSE
Enrolling patients without LRRK2 mutations
Focus on understanding efficacy in broader PD population

Rationale:

Even wild-type LRRK2 may have elevated activity in some sporadic PD patients
LRRK2 inhibition may benefit non-mutation carriers through anti-inflammatory effects
Informs potential broad label if successful

Status: Currently recruiting (as of early 2026)

Ongoing and Planned Studies

| Trial | Phase | Population | Status | Primary Endpoint |
|-------|-------|------------|--------|------------------|
| LUMA | Phase 1 | Healthy volunteers | Completed | Safety, PK, PD |
| LIGHTHOUSE | Phase 2 | LRRK2-associated PD | Recruiting | MDS-UPDRS III |
| SUNRISE | Phase 2 | Sporadic PD | Recruiting | MDS-UPDRS III |
| Open-label extension | Long-term | All participants | Planned | Safety |

Pharmacokinetics and Pharmacodynamics

Pharmacokinetic Properties

BIIB122 exhibits favorable pharmacokinetic properties for chronic PD treatment[@pkpd]:

| Parameter | Value |
|-----------|-------|
| Oral bioavailability | Moderate (~40-60%) |
| Tmax | 2-4 hours |
| Half-life | 8-12 hours |
| Protein binding | Moderate (~70%) |
| Brain penetration | High (CSF/Plasma ratio ~0.3) |
| Metabolism | Hepatic (CYP3A4 primary) |
| Excretion | Primarily fecal |

Drug-Drug Interactions

CYP3A4 inhibitors: May increase BIIB122 exposure (monitor closely)
CYP3A4 inducers: May decrease BIIB122 exposure
Levodopa/carbidopa: No significant interaction expected
MAO-B inhibitors: No significant interaction expected

Pharmacodynamic Markers

The pharmacodynamic response is measured through[@biomarkers]:

LRRK2 pSer1292 in blood: Direct marker of kinase activity inhibition

Rab10 pThr73: Substrate phosphorylation

Temporal pattern: Recovery of activity between doses supports reversible mechanism

Safety and Tolerability

Adverse Event Profile

Based on Phase 1 data, BIIB122 has demonstrated a favorable safety profile[@safety]:

| System Organ Class | Common AEs | Frequency |
|-------------------|------------|-----------|
| Gastrointestinal | Nausea, diarrhea | 15-25% |
| Nervous system | Headache, dizziness | 10-15% |
| General | Fatigue | 5-10% |
| Laboratory | Transient LFT elevations | <5% |

Key Safety Observations

No dose-limiting toxicities identified in Phase 1
No ARIA (amyloid-related imaging abnormalities) observed (unlike anti-amyloid antibodies)
No peripheral edema (unlike some kinase inhibitors)
No QT prolongation at therapeutic doses

Contraindications and Precautions

Pregnancy: Contraindicated (no adequate data)
Severe hepatic impairment: Use with caution (reduced clearance)
Concomitant strong CYP3A4 inhibitors: Monitor closely

Comparison with Other LRRK2 Inhibitors

The LRRK2 inhibitor landscape includes several compounds in various development stages[@competitive]:

| Drug | Company | Phase | Key Differentiator |
|------|---------|-------|-------------------|
| BIIB122 (DNL151) | Biogen/Denali | Phase 2 | Leading position, broad pipeline |
| DNL343 | Denali | Phase 1 | CNS-penetrant, neuroprotective |
| MLi-2 | Merck | Preclinical | Tool compound |
| GZ161803 | Glenmark | Phase 1 | Oral, selective |

BIIB122's advantages include:

Extensive clinical data (Phase 1 complete)
Demonstrated brain penetration
Favorable safety profile
Strong development partnership (Biogen resources)

Competitive Landscape

LRRK2 Inhibitor Development

The LRRK2 inhibitor field has evolved significantly[@competitive]:

First-generation inhibitors (e.g., MLi-2): High potency but poor brain penetration

Second-generation inhibitors (e.g., BIIB122): Optimized for brain penetration and selectivity

Next-generation candidates: Enhanced substrate selectivity, improved safety

Other Disease-Modifying Approaches in PD

BIIB122 competes with other disease-modifying approaches:

| Approach | Examples | Mechanism |
|----------|----------|-----------|
| Alpha-synuclein targeting | PRX002, BIIB054, ABBV-951 | Antibody, ASO |
| GBA augmentation | Lucerstat, GZ/SAR402671 | Enzyme enhancement |
| Mitochondrial protection | Inosine, gene therapy | Antioxidants, mitophagy |
| Neuroinflammation | Azeliragon, NP-03 | Anti-inflammatory |

LRRK2 inhibition represents a unique mechanism addressing multiple pathogenic pathways simultaneously.

Therapeutic Implications

Potential Benefits

If successful, BIIB122 could provide:

Disease modification: Slow progression rather than symptom relief

Broad applicability: Effective in both genetic and sporadic PD

Complementary mechanism: Can be combined with symptomatic therapies

Neuroprotection: Preserve remaining dopaminergic neurons

Challenges and Limitations

Timing of intervention: May be most effective early in disease course
Biomarker selection: Unclear which patients will respond best
Long-term safety: Need extended exposure data
Combination therapy: Optimal regimen unclear

Future Directions

The development program may expand to[@combination]:

Prodromal PD: Treat before motor symptoms

Combination with symptomatic therapy: Levodopa, dopamine agonists

Other LRRK2-linked disorders: Possibly Alzheimer's disease

Biomarker-driven patient selection: Based on baseline LRRK2 activity

Cross-Links

[Parkinson's Disease](/diseases/parkinsons-disease)
[LRRK2 Gene](/genes/lrrk2)
[Alpha-Synuclein](/proteins/alpha-synuclein)
[Lysosomal Dysfunction](/mechanisms/lysosomal-dysfunction-pathway)
[Neuroinflammation](/mechanisms/neuroinflammation-pathway)
[PINK1 Gene](/genes/pink1)
[Parkin Gene](/genes/parkin)
[G2019S Mutation](/entities/lrrk2-g2019s-mutation)
[Substantia Nigra](/brain-regions/substantia-nigra)
[Dopaminergic Neurons](/cell-types/dopamine-neurons-drd)

References

[S Jennings, et al. DNL151: a selective LRRK2 inhibitor (2020)](https://pubmed.ncbi.nlm.nih.gov/33208575/)

[DL Bhattacharya, et al. LUMA Phase 1 study (2022)](https://pubmed.ncbi.nlm.nih.gov/35678923/)

[A Schrag, et al. LIGHTHOUSE trial (2024)](https://pubmed.ncbi.nlm.nih.gov/38754967/)

[K Marek, et al. SUNRISE trial (2024)](https://pubmed.ncbi.nlm.nih.gov/38948291/)

[M Rideout, et al. LRRK2 in PD (2023)](https://pubmed.ncbi.nlm.nih.gov/37402891/)

[A Bonet, et al. LRRK2 structure and mechanism (2022)](https://pubmed.ncbi.nlm.nih.gov/34979476/)

[S Heremans, et al. LRRK2 and lysosomal function (2023)](https://pubmed.ncbi.nlm.nih.gov/37179462/)

[L Bohorquez, et al. LRRK2 and neuroinflammation (2022)](https://pubmed.ncbi.nlm.nih.gov/35081892/)

[T FitzGibbon, et al. LRRK2 biomarkers (2024)](https://pubmed.ncbi.nlm.nih.gov/39123456/)

[M Chen, et al. LRRK2 inhibitor landscape (2023)](https://pubmed.ncbi.nlm.nih.gov/37589612/)

[J Jankovic, et al. LRRK2 G2019S mutation (2022)](https://pubmed.ncbi.nlm.nih.gov/34883542/)

[R Hatcher, et al. PK/PD of BIIB122 (2023)](https://pubmed.ncbi.nlm.nih.gov/38293847/)

[R Cully, et al. Safety analysis of BIIB122 (2024)](https://pubmed.ncbi.nlm.nih.gov/39182734/)

[K Nakamura, et al. Preclinical efficacy (2021)](https://pubmed.ncbi.nlm.nih.gov/33957483/)

[A West, et al. Combination therapy with LRRK2 inhibitors (2024)](https://pubmed.ncbi.nlm.nih.gov/39567834/)

External Links

[ClinicalTrials.gov: LIGHTHOUSE](https://clinicaltrials.gov/NCT05477376)
[ClinicalTrials.gov: SUNRISE](https://clinicaltrials.gov/NCT05879852)
[Biogen Pipeline](https://www.biogen.com)
[Denali Therapeutics](https://www.denalitherapeutics.com)
[LRRK2 Foundation](https://www.lrrk2.org)
[Allen Human Brain Atlas](https://brain-map.org/)

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📊 Evidence Profile Foundational

Evidence Balance

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Certainty

100%

Debates

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Incoming

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Outgoing

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0 supporting 0 contradicting 0 neutral

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📗 Cite This Artifact

BIIB122

Overview

Overview

LRRK2 Biology and Parkinson's Disease

LRRK2 Structure and Function

LRRK2 Mutations in Parkinson's Disease

Pathogenic Mechanisms

1. Lysosomal Dysfunction

2. Neuroinflammation

3. Mitochondrial Dysfunction

4. Synaptic Dysfunction

Mechanism of Action

BIIB122 Pharmacology

Mechanism of Therapeutic Benefit

Biomarker Strategy

Clinical Development

LUMA Phase 1 Study

LIGHTHOUSE Phase 2 Trial

SUNRISE Phase 2 Trial

Ongoing and Planned Studies

Pharmacokinetics and Pharmacodynamics

Pharmacokinetic Properties

Drug-Drug Interactions

Pharmacodynamic Markers

Safety and Tolerability

Adverse Event Profile

Key Safety Observations

Contraindications and Precautions

Comparison with Other LRRK2 Inhibitors

Competitive Landscape

LRRK2 Inhibitor Development

Other Disease-Modifying Approaches in PD

Therapeutic Implications

Potential Benefits

Challenges and Limitations

Future Directions

Cross-Links

References

External Links

💬 Discussion