YKL-40 Anti-Inflammatory Cycling

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YKL-40 Anti-Inflammatory Cycling

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Rank: 23 | Score: 78/100

Overview

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Rank: 23 | Score: 78/100

Overview

Mermaid diagram (expand to render)

YKL-40 Anti-Inflammatory Cycling Therapy is a biomarker-guided approach that uses YKL-40 (chitinase-3-like protein 1) as a dynamic marker of neuroinflammation to guide pulsed anti-inflammatory treatment. Rather than continuous immunosuppression, this approach synchronizes therapy with inflammatory peaks, potentially reducing toxicity while maximizing efficacy["@olsson2013"][@baldacci2015].

Biological Background

YKL-40 as an Inflammatory Biomarker

YKL-40 is a chitinase-like protein produced by activated [microglia](/cell-types/microglia-neuroinflammation), [astrocytes](/entities/astrocytes), and neutrophils:

Pro-inflammatory association: Elevated in conditions with active neuroinflammation
Disease correlation: Levels correlate with disease severity in AD, PD, and MS
Dynamic range: Changes in response to disease progression and treatment
Cellular source: Primarily from activated microglia and astrocytes in the brain

Rationale for Cycling Therapy

Continuous anti-inflammatory treatment faces challenges:

Tolerance: Long-term use can lead to reduced efficacy
Immunosuppression risks: Increased infection susceptibility
Target engagement: Constant blockade may not match inflammatory dynamics

Cyclic therapy offers advantages:

Rhythm matching: Synchronize with natural inflammatory oscillations
Drug holidays: Reduce cumulative exposure and side effects
Mechanism cycling: Alternate between different anti-inflammatory pathways

Evidence in Neurodegeneration

YKL-40 is elevated in CSF and plasma of AD patients compared to controls[@olsson2013]
Higher YKL-40 correlates with faster cognitive decline in AD[@baldacci2015]
YKL-40 response to anti-inflammatory treatment has been observed in clinical trials

Scoring (10-Dimension Rubric)

| Dimension | Score | Rationale |
|-----------|-------|-----------|
| Novelty | 8 | YKL-40-guided cycling is an emerging concept; not yet in clinical practice |
| Mechanistic Rationale | 8 | Biological basis for inflammatory cycling is well-established |
| Root-Cause Coverage | 7 | Addresses neuroinflammation as a contributor to pathology |
| Delivery Feasibility | 8 | Uses existing anti-inflammatory agents; biomarker is available |
| Safety Plausibility | 8 | Cycling approach may reduce safety concerns vs. continuous use |
| Combinability | 8 | Can be combined with disease-modifying therapies |
| Biomarker Availability | 8 | YKL-40 ELISA assays are commercially available |
| De-risking Path | 7 | Clear pathway using established anti-inflammatory compounds |
| Multi-disease Potential | 8 | Applicable to AD, PD, ALS, and other neuroinflammatory conditions |
| Patient Impact | 7 | Improved safety profile could expand the patient population |

Implementation Strategy

Patient Selection

Elevated baseline YKL-40 in CSF or plasma
Confirmed neuroinflammation through additional markers (IL-6, TNF-α)
Exclusion of active infections or autoimmune conditions

Treatment Protocol

Phase 1: Establish Baseline

Measure YKL-40 at screening, baseline, and weeks 4, 8
Define individual inflammatory signature

Phase 2: Initiate Cycling

Active treatment period: 4-8 weeks of anti-inflammatory therapy
Drug holiday: 2-4 weeks without anti-inflammatory treatment
Cycle repeat: Monitor YKL-40 to guide cycle timing

Anti-inflammatory Agents to Cycle

Minocycline: Antibiotic with anti-inflammatory properties
NSAIDs: Low-dose aspirin, celecoxib (selective COX-2)
Natural compounds: Curcumin, omega-3 fatty acids
Experimental: [NLRP3](/entities/nlrp3-inflammasome) inhibitors, [TREM2](/proteins/trem2) agonists

Biomarker Monitoring

YKL-40 every 2-4 weeks during active treatment
Track trends: rising YKL-40 = resume therapy; declining = extend holiday
Secondary markers: IL-6, TNF-α, CRP

De-risking Path

Clinical Validation

Establish YKL-40 response patterns in neurodegenerative diseases

Test cycling vs. continuous dosing in proof-of-concept trials

Identify optimal cycle length and drug selection

Regulatory Path

Pursue biomarker-guided indication for existing compounds

Use YKL-40 as endpoint in early-phase trials

Seek combination therapy approvals with disease-modifying agents

Commercial Strategy

Position as precision anti-inflammatory approach

Develop monitoring kit for YKL-40 cycling

Partner with companies owning anti-inflammatory assets

External Links

[PubMed](https://pubmed.ncbi.nlm.nih.gov/)
[KEGG Pathways](https://www.genome.jp/kegg/pathway.html)

Actionable Next Steps

Lab Experiments

YKL-40 assay standardization: Compare YKL-40 ELISA kits from multiple vendors (Quanterix, R&D Systems, BioLegend) in 200+ AD/PD patient samples to establish assay interchangeability and correlation with CSF YKL-40.

Inflammatory cycling proof-of-concept: Test pulsed minocycline vs. continuous dosing in LPS-challenged mouse primary microglia. Measure YKL-40, IL-6, TNF-alpha at each cycle phase to define optimal on/off timing.

Biomarker correlation study: Establish correlation between plasma YKL-40 and CSF YKL-40, and validate against neuroinflammation PET ligands (e.g., TSPO) in tauopathy mouse models.

Drug candidate screening: Screen NSAIDs (aspirin, celecoxib), natural compounds (curcumin, omega-3), and experimental NLRP3 inhibitors for YKL-40 suppression in iPSC-derived microglia.

Clinical Protocol Design

Observational cohort: Enroll 200 participants with elevated baseline YKL-40 (AD, PD, FTD). Track YKL-40 trajectories over 24 months with standardized sampling protocol.

Cycling vs. continuous RCT: "CYCLAD" - randomized controlled trial comparing 4-weeks-on/2-weeks-off minocycline vs. continuous minocycline vs. placebo in YKL-40 elevated participants. Primary: YKL-40 change at 24 weeks.

Adaptive cycle optimization: Use Bayesian adaptive design to optimize cycle length and drug selection based on YKL-40 response trajectories.

Combination trial: Add YKL-40 cycling to standard-of-care (anti-amyloid, anti-tau) to test additive benefit on cognitive endpoints.

Company Partnership Opportunities

Quanterix: Leader in ultra-sensitive biomarker testing; partner for YKL-40 assay development and clinical trial biomarker infrastructure.

AC Immune: Their anti-inflammatory pipeline (NLRP3 inhibitor) could be combined with YKL-40 cycling protocol.

AbbVie/Eli Lilly: Large CNS portfolios with anti-inflammatory assets; potential for combination therapy trials.

Alzheimer's Drug Discovery Foundation: Funder alignment for biomarker-guided anti-inflammatory trials.

Grant Targets

| Grant | Agency | Focus | Amount | Fit |
|-------|--------|-------|--------|-----|
| R01 | NIH/NIA | AD biomarker therapeutics | $1.5M/5yr | High - YKL-40 as endpoint |
| R21 | NIH/NINDS | Early-phase PD therapeutics | $275K/2yr | High - PD-YKL-40 correlation |
| U01 | NIH/NIA | Target validation consortium | $3M/5yr | Medium |
| AACSF | Alzheimer's Association | Precision anti-inflammatory | $150-400K | High |
| MJFF | Michael J. Fox Foundation | Neuroinflammation biomarkers | $150-300K | High |

Priority: Start with MJFF to establish YKL-40 as PD inflammation biomarker, then expand to AD.

Implementation Roadmap

Phase 1: Biomarker Validation & Dosing Protocol (Months 1-15)

Cost: $2-3.5M

| Milestone | Timeline | Cost | Risk |
|-----------|----------|------|------|
| YKL-40 assay standardization across labs | Months 1-6 | $800K | Low |
| Dose-ranging preclinical in mouse neuroinflammation model | Months 4-10 | $1M | Medium |
| GLP toxicology (90-day) | Months 6-12 | $700K | Low |
| Pre-IND meeting | Month 12 | $150K | Low |
| Phase 1 protocol finalization | Months 12-15 | $350K | Low |

Key Risks:

YKL-40 variability may require assay standardization (mitigation: use central lab)
Optimal cycling schedule may need iteration

Phase 2: Phase 2 Adaptive Cycling Trial (Months 14-30)

Cost: $7-12M

| Milestone | Timeline | Cost | Risk |
|-----------|----------|------|------|
| Phase 2a: dose-finding (n=80) | Months 14-22 | $4M | Medium |
| Biomarker analysis: YKL-40, IL-6, TNF-alpha | Months 16-24 | $1.5M | Low |
| Interim analysis | Month 20 | $400K | Medium |
| Phase 2b: optimal cycling schedule (n=100) | Months 22-30 | $4M | Medium |

Key Risks:

Off periods may lead to rebound inflammation
Patient adherence to cycling protocol

Phase 3: Registration Program (Months 28-54)

Cost: $30-50M

| Milestone | Timeline | Cost | Risk |
|-----------|----------|------|------|
| Phase 3 protocol design | Months 28-32 | $2M | Low |
| Global enrollment (n=600) | Months 32-44 | $22M | Medium |
| Phase 3 readout | Month 50 | $4M | Medium |
| Regulatory filings | Months 50-54 | $8M | Low |

Total Program Cost: $39-65.5M over 54 months

Risk-Adjusted Scenarios

| Scenario | Probability | Cost Impact |
|----------|-------------|-------------|
| Best case | 15% | $35M |
| Base case | 50% | $50M |
| Slow enrollment | 25% | $68M |
| Safety signal | 10% | +$25M |

Academic Center Recommendations

US: Stanford (inflammation biomarkers), UCSF (ADRC), Mount Sinai (neuroinflammation)

EU: University of Bonn (Azheimer's research), Karolinska, Cambridge

Key Academic Collaborators: Dr. Tony Wyss-Coray (inflammation), Dr. Eric Kandel (neuroprotection)

Decision Gates

| Gate | Criteria | Go/No-Go |
|------|----------|----------|
| Phase 1→2 | Positive safety + biomarker response | Go if YKL-40 reduction >20% |
| Phase 2→3 | Clinical signal in cognition | Go if ADAS-Cog slowing >20% |
| Registration | Phase 3 confirmatory | Go if p<0.025 |

Potential Pharmaceutical Partners

Tier 1 - Large Pharma (Inflammation/Neuroscience Focus)

Biogen — Existing AD portfolio ( Aduhelm), inflammation partnerships; ideal for Phase 3

Eli Lilly — Strong neurodegeneration pipeline, [tau](/proteins/tau) programs

Roche/Genentech — Neuroscience division, gantenerumab program

AbbVie — Immunology-neuroscience crossover, UCB partnership

Tier 2 - Specialized Biotech

AC Immune — Anti-tau, anti-amyloid antibodies, Swiss precision

ProMIS Neurosciences — Amyloid target, antibody platform

Cognition Therapeutics — Sigma-2 receptor modulators

Alnylam — siRNA delivery, neuroinflammation applications

Tier 3 - Diagnostic/Companion Partners

Roche Diagnostics — Biomarker assay development

Quanterix — Ultra-sensitive Simoa platform for YKL-40

C2N Diagnostics — CSF biomarker specialization

Partnership Structure Recommendations:

Phase 1-2: Academic-led, small biotech COGS partnership
Phase 2b: Co-development with Tier 1 pharma (50/50 costs)
Phase 3: Full acquisition or licensing deal (00-200M upfront)

Cross-Links

[YKL-40 Biomarker](/mechanisms/ykl40-biomarker)
[Microglia in Neurodegeneration](/cell-types/microglia)
[Neuroinflammation](/mechanisms/neuroinflammation)
[Biomarkers for Neurodegeneration](/mechanisms/neurodegeneration-biomarkers)

Rubric Score

| Dimension | Score | Rationale |
|-----------|-------|-----------|
| Novelty | 7/10/10 | YKL-40 biomarker is established; cycling-based treatment is innovative |
| Mechanistic Rationale | 6/10/10 | Uses YKL-40 to guide anti-inflammatory treatment cycles |
| Addresses Root Cause | 6/10/10 | Addresses neuroinflammation dynamically; biomarker-driven adjustment |
| Delivery Feasibility | 7/10/10 | Standard drug delivery; biomarker guides timing |
| Safety Plausibility | 7/10/10 | Cycling may reduce chronic drug exposure; safety monitoring enhanced |
| Combinability | 7/10/10 | Compatible with multiple anti-inflammatory approaches |
| Biomarker Availability | 8/10/10 | YKL-40 well-established; accessible via blood |
| De-risking Path | 7/10/10 | Cycling approach can be validated in clinical trials |
| Multi-disease Potential | 7/10/10 | Relevant for AD, PD, ALS, MS, autoimmune conditions |
| Patient Impact | 7/10/10 | Could optimize anti-inflammatory therapy while minimizing side effects |
| Total | 69/100 | |

References

[Olsson et al, YKL-40 in cerebrospinal fluid in Alzheimer's disease (2013)](https://pubmed.ncbi.nlm.nih.gov/23935827/)

[Baldacci et al, YKL-40: a promising biomarker for Alzheimer's disease? (2015)](https://pubmed.ncbi.nlm.nih.gov/25876989/)

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📊 Evidence Profile Foundational

Evidence Balance

+0%

Certainty

85%

Debates

0

Incoming

17

Outgoing

26

0 supporting 0 contradicting 0 neutral

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📗 Cite This Artifact

YKL-40 Anti-Inflammatory Cycling

Overview

Overview

Biological Background

YKL-40 as an Inflammatory Biomarker

Rationale for Cycling Therapy

Evidence in Neurodegeneration

Scoring (10-Dimension Rubric)

Implementation Strategy

Patient Selection

Treatment Protocol

Biomarker Monitoring

De-risking Path

Clinical Validation

Regulatory Path

Commercial Strategy

See Also

External Links

Actionable Next Steps

Lab Experiments

Clinical Protocol Design

Company Partnership Opportunities

Grant Targets

Implementation Roadmap

Phase 1: Biomarker Validation & Dosing Protocol (Months 1-15)

Phase 2: Phase 2 Adaptive Cycling Trial (Months 14-30)

Phase 3: Registration Program (Months 28-54)

Total Program Cost: $39-65.5M over 54 months

Risk-Adjusted Scenarios

Academic Center Recommendations

Decision Gates

Potential Pharmaceutical Partners

Cross-Links

Rubric Score

References

💬 Discussion