heqIX (pronounced "heks") is a biotechnology company developing novel autophagy enhancement therapies for the treatment of Parkinson's disease and other neurodegenerative disorders. The company's distinctive approach specifically targets the lysosomal membrane protein LAMP2A (lysosome-associated membrane protein 2A), which plays a critical role in chaperone-mediated autophagy (CMA).
heqIX's name reflects the company's focus on hexokinase and the intersection of cellular energy metabolism and protein clearance. The company was founded in 2021 and is headquartered in the United States, with a research facility focused on developing small molecule LAMP2A modulators that enhance CMA function in neurons.
The company's mission is to develop disease-modifying therapies for neurodegenerative diseases by restoring the lysosomal protein clearance pathway that becomes impaired with aging and disease. Unlike approaches that aim to reduce protein aggregation through antibody-based or gene-silencing strategies, heqIX focuses on enhancing the cell's native protein degradation machinery to achieve sustainable therapeutic benefit.
- Headquarters: United States
- Founded: 2021
- Focus: LAMP2A modulators for autophagy enhancement
- Therapeutic Areas: Parkinson's Disease, Alzheimer's Disease, Huntington's Disease
- Status: Series A funding ($28M, 2023)
Chaperone-mediated autophagy (CMA) is a selective autophagy pathway that directly translocates cytosolic proteins across the lysosomal membrane via the LAMP2A receptor. Unlike macroautophagy or microautophagy, CMA does not involve vesicle formation. Instead, cytosolic proteins containing a specific KFERQ motif are recognized by Hsc70 (heat shock cognate 70 kDa protein), which delivers them to lysosomes where LAMP2A forms a translocation channel.
Key characteristics of CMA:
- Substrate specificity: Only proteins containing the pentapeptide motif KFERQ are recognized by Hsc70
- Direct translocation: Substrate proteins unfold and pass directly through the LAMP2A channel into the lysosomal lumen
- Selectivity: CMA preferentially degrades specific regulatory proteins, transcription factors, and damaged proteins
- Cellular regulation: CMA activity is modulated by cellular stress, nutrient status, and developmental cues
The CMA pathway components:
- LAMP2A: Lysosomal membrane receptor forming the translocation channel
- Hsc70 (HSPA8): Cytosolic chaperone that recognizes KFERQ motifs
- LAMP2A dimer: Forms the functional translocation complex
- Lysosomal Hsc70 (LAMP2A-associated): Facilitates substrate internalization
Multiple lines of evidence demonstrate that CMA is impaired in Parkinson's disease:
LAMP2A expression changes:
- Post-mortem studies show reduced LAMP2A levels in the substantia nigra of PD patients
- Age-related decline in LAMP2A expression correlates with increased aggregation vulnerability
- Genetic association studies suggest LAMP2A polymorphisms influence PD risk
Alpha-synuclein and CMA:
- Wild-type alpha-synuclein is a CMA substrate with a functional KFERQ motif
- Mutant alpha-synuclein (A30P, A53T) fails to be efficiently transported via CMA
- Accumulated alpha-synuclein can inhibit LAMP2A function, creating a feed-forward loop
Consequences of CMA impairment:
- Accumulation of damaged and misfolded proteins
- Impaired clearance of toxic protein aggregates
- Progressive neuronal dysfunction and death
- Exacerbation of proteostatic stress in aging neurons
CMA represents an attractive therapeutic target because:
- Direct mechanism: Enhancing LAMP2A function can bypass upstream defects
- Substrate specificity: Selective protein clearance reduces off-target effects
- Age-related decline: Restoring CMA in aged neurons addresses a key vulnerability
- Genetic rationale: LAMP2A haploinsufficiency is linked to increased PD risk
heqIX develops small molecule drugs that enhance chaperone-mediated autophagy through modulation of LAMP2A:
LAMP2A agonists: Compounds that increase LAMP2A protein levels and improve its stability on the lysosomal membrane. These molecules:
- Upregulate LAMP2A gene expression via transcriptional mechanisms
- Enhance LAMP2A protein stability and reduce its degradation
- Promote LAMP2A multimerization into functional translocation complexes
CMA enhancers: Molecules that accelerate substrate translocation across the lysosomal membrane:
- Enhance Hsc70-LAMP2A interaction kinetics
- Increase the rate of substrate unfolding and translocation
- Improve lysosomal Hsc70 activity
Lysosomal function modulators: Agents that improve overall lysosomal health:
- Enhance lysosomal acidification and enzyme activity
- Promote lysosomal biogenesis through TFEB activation
- Protect lysosomes from membrane damage
heqIX's therapeutic approach follows this cascade:
-
LAMP2A upregulation: Increasing LAMP2A protein levels in neurons through transcriptional activation and protein stabilization
-
CMA activation: Enhancing the rate of substrate uptake into lysosomes by:
- Increasing the number of functional LAMP2A complexes on the lysosomal membrane
- Enhancing the binding affinity for Hsc70-substrate complexes
- Accelerating the translocation process
-
Aggregate clearance: Specifically targeting alpha-synuclein, tau, and huntingtin for CMA degradation:
- All three proteins contain functional KFERQ motifs
- Enhancing CMA reduces intracellular aggregate burden
- Selective clearance preserves cellular function
-
Cellular resilience: Improving overall cellular clearance capacity:
- Reduces proteostatic stress
- Improves neuronal viability under stress conditions
- May slow disease progression
heqIX has developed robust screening and validation platforms:
| Capability |
Description |
| LAMP2A expression assays |
Quantitative measurement of LAMP2A protein levels |
| CMA flux measurements |
Real-time tracking of substrate degradation |
| KFERQ motif analysis |
Computational identification of CMA substrates |
| Neuronal cell models |
iPSC-derived dopaminergic neurons for screening |
| In vivo PD models |
Multiple models including MPTP and genetic models |
| Program |
Target |
Indication |
Development Status |
| HQX-101 |
LAMP2A agonist |
Parkinson's Disease |
Preclinical |
| HQX-201 |
CMA enhancer |
Alzheimer's Disease |
Discovery |
| HQX-301 |
Dual autophagy modulator |
Huntington's Disease |
Discovery |
¶ HQX-101 (Lead Candidate)
HQX-101 is heqIX's lead preclinical candidate:
- Mechanism: Small molecule that upregulates LAMP2A and enhances chaperone-mediated autophagy
- Target: Alpha-synuclein clearance in Parkinson's disease
- Route: Oral delivery
- Status: IND-enabling studies (expected 2026)
Preclinical data:
- LAMP2A upregulation in neurons (2-3 fold increase)
- Enhanced alpha-synuclein clearance in cellular models
- Neuroprotection in MPTP mouse model
- Blood-brain barrier penetration demonstrated
- Good oral bioavailability and safety profile
- Mechanism: CMA enhancer that accelerates substrate translocation
- Target: Tau protein clearance in Alzheimer's disease
- Status: Discovery stage
- Rationale: Tau contains functional KFERQ motifs and can be cleared via CMA
- Mechanism: Dual autophagy modulator enhancing both CMA and macroautophagy
- Target: Mutant huntingtin protein in Huntington's disease
- Status: Discovery stage
- Rationale: Addresses multiple clearance pathways for enhanced aggregate removal
The IND-enabling program for HQX-101 includes comprehensive preclinical development:
Pharmacology studies:
- Dose-range finding in rodent models
- Efficacy in multiple PD models (MPTP, 6-OHDA, alpha-synuclein overexpression)
- Biomarker studies measuring LAMP2A levels and CMA activity
Safety assessment:
- GLP toxicology in rodents and non-rodents (13-week studies)
- Safety pharmacology core battery (CV, CNS, respiratory)
- Genotoxicity and carcinogenicity assessments
Chemistry, Manufacturing, and Controls (CMC):
- API scale-up and process development
- Formulation development for oral delivery
- Stability studies supporting IND submission
heqIX has outlined a phased clinical development strategy:
Phase 1 (2026-2027):
- Single ascending dose (SAD) in healthy volunteers
- Multiple ascending dose (MAD) in healthy volunteers
- Target engagement biomarkers in CSF
Phase 2 (2027-2029):
- Proof-of-concept in early Parkinson's disease patients
- Dose-selection based on biomarker response
- Exploratory efficacy endpoints (motor scores, imaging biomarkers)
Phase 3 (2029-2032):
- Pivotal trials in Parkinson's disease
- Registration-enabling studies
- Potential for accelerated approval based on biomarker endpoints
heqIX is strategically targeting early-stage Parkinson's disease patients for several reasons:
- Preserved neuronal function: Early-stage patients have sufficient remaining dopaminergic neurons for therapeutic benefit
- Better drug penetration: Less neuronal loss allows better drug distribution to target tissues
- Regulatory advantages: FDA has established pathways for disease-modifying therapies in early PD
- Clinical trial efficiency: Shorter trials possible with biomarker-based endpoints
The company is also exploring enrichment strategies to identify patients most likely to benefit from CMA enhancement:
- LAMP2A expression markers: Patients with higher baseline LAMP2A may respond better
- Age stratification: Younger patients may have more responsive lysosomal systems
- Genetic subtyping: Patients with specific genetic backgrounds (e.g.,GBA carriers) may benefit particularly
heqIX employs a biomarker-driven development approach:
-
Target engagement biomarkers:
- LAMP2A expression in peripheral blood mononuclear cells (PBMCs)
- CMA activity markers in CSF
-
Mechanism biomarkers:
- Alpha-synuclein oligomers in CSF
- Lysosomal function markers
-
Disease progression biomarkers:
heqIX's approach is based on foundational research demonstrating that:
- LAMP2A expression decreases with age and in Parkinson's disease
- CMA is the primary pathway for alpha-synuclein degradation in neurons
- Enhancing CMA can reduce protein aggregate burden in cellular and animal models
- LAMP2A is a druggable target with clear pharmacology
- Hsc70-LAMP2A interaction can be pharmacologically modulated
Key publications supporting the approach:
- LAMP2A deficiency leads to alpha-synuclein accumulation in neurons
- CMA impairment in PD substantia nigra correlates with disease severity
- Small molecule LAMP2A agonists show efficacy in PD models
- LAMP2A modulators enhance clearance of multiple neurodegeneration-associated proteins
¶ Competitive Landscape
heqIX competes with other companies developing autophagy-enhancing approaches:
| Company |
Target |
Approach |
Development Stage |
| heqIX |
LAMP2A/CMA |
Small molecule |
Preclinical |
| Lyterian Therapeutics |
Broader autophagy |
Small molecule |
Preclinical |
| Vincere Biosciences |
Autophagy enhancers |
Small molecule |
Discovery |
| Retro Biosciences |
Autophagy induction |
Multiple |
Discovery |
| Lysoway Therapeutics |
Autophagy enhancement |
Gene therapy |
Preclinical |
Competitive advantages of heqIX:
- Target specificity: Direct LAMP2A targeting vs. broad autophagy modulation
- Oral delivery: Small molecule approach enables convenient dosing
- CMA expertise: Deep understanding of CMA biology and pharmacology
- Biomarker strategy: Measurable target engagement to guide clinical development
- Seed Round: $8M (2021)
- Series A: $28M (2023) — led by Andreessen Horowitz, with participation from Polaris Partners andMission BioCapital
- University of Pennsylvania: CMA biology research collaboration
- Mount Sinai School of Medicine: PD model development
- Michael J. Fox Foundation: Clinical biomarker development
- Dr. Mario Sortino (Albert Einstein College of Medicine) — CMA expert
- Dr. Joohyun Park (Harvard Medical School) — PD biology
- Dr. Ralph Pataky (Stanford University) — Drug discovery
¶ Challenges and Future Directions
- Blood-brain barrier penetration: Ensuring adequate CNS exposure
- LAMP2A selectivity: Avoiding off-target effects on other lysosomal proteins
- Sustained engagement: Maintaining target activation with chronic dosing
- Biomarker validation: Developing reliable and sensitive CMA activity assays
- Patient stratification: Identifying patients most likely to respond to therapy
¶ Manufacturing and Commercialization
heqIX has planned for future commercial-scale manufacturing:
API Manufacturing:
- Contract manufacturing organization (CMO) selected for Phase 2+ supply
- Scalable synthesis route developed for commercial quantities
- Quality by design approach ensures batch-to-batch consistency
Formulation:
- Oral tablet formulation for patient convenience
- Extended-release options being explored for improved compliance
- Pediatric-friendly formulations under development for future indications
Commercial Strategy:
- Specialty neurology sales force for US market
- Partnership opportunities for international commercialization
- Reimbursement strategy aligned with disease-modifying therapy value proposition
- Clinical translation: Preclinical efficacy may not translate to human patients
- Competitive timeline: Other companies may advance competing programs
- Regulatory pathway: Novel mechanism may require additional regulatory guidance
- Manufacturing scale-up: Scaling API production for commercial quantities
heqIX's development roadmap includes:
- Expanding beyond Parkinson's: Exploring Alzheimer's disease and Huntington's disease
- Combination approaches: Combining CMA enhancement with other mechanisms
- Diagnostic companion: Developing patient selection biomarkers
- Gene therapy platform: Exploring AAV-mediated LAMP2A delivery