AD Sigma-1 Receptor & Molecular Chaperone Therapy Companies

Alzheimer's Disease Sigma-1 Receptor & Molecular Chaperone Therapy Companies

Overview

Alzheimer's Disease Sigma-1 Receptor & Molecular Chaperone Therapy Companies

Overview

Sigma-1 Receptor (S1R) modulators and Molecular Chaperone therapies represent two complementary emerging approaches to Alzheimer's disease treatment that target fundamental cellular processes: endoplasmic reticulum (ER) stress, protein homeostasis, calcium dysregulation, and mitochondrial dysfunction.

Sigma-1 Receptor: The Sigma-1 Receptor is a unique chaperone protein localized to the ER membrane at mitochondria-associated membranes (MAMs). It serves as a calcium sensor and master regulator of cellular stress responses. S1R activation has been shown to protect against ER stress, maintain calcium homeostasis, improve mitochondrial function, and reduce neuroinflammation—all processes implicated in AD pathogenesis["@maurice2009"][@cai2020].

Molecular Chaperones: Heat shock proteins (Hsp90, Hsp70) and small molecule chaperones help maintain protein folding homeostasis. In AD, the accumulation of misfolded Abeta and tau overwhelms the cellular protein quality control system. Chaperone-based therapies aim to enhance this system to clear toxic protein aggregates.

This category page catalogs companies developing these approaches specifically for Alzheimer's disease.

Sigma-1 Receptor Agonists

Pridopidine (DNL458)

Developer: [Denki Kagaku Kogyo (Denka)](https://www.denka.co.jp/) (Japan)

| Attribute | Details |
|-----------|---------|
| Focus | Sigma-1 receptor agonist, dopaminergic stabilization |
| Lead Candidate | Pridopidine (DNL458) |
| Indication | Alzheimer's disease, Huntington's disease |
| Stage | Phase 2 (AD), Phase 3 (HD) |
| Mechanism | S1R agonist with D2 receptor modulation |

Scientific Rationale: Pridopidine has high affinity for Sigma-1 receptors and shows neuroprotective effects through:

• ER stress reduction
• Mitochondrial function improvement
• Calcium homeostasis restoration
• Anti-inflammatory effects in microglia

Astellas Pharma

Website: [Astellas](https://www.astellas.com/)

| Attribute | Details |
|-----------|---------|
| Focus | Multiple CNS targets including S1R |
| Lead Candidates | Various S1R modulators |
| Indication | Alzheimer's disease, Parkinson's disease |
| Stage | Discovery/Preclinical |
| Mechanism | Selective Sigma-1 receptor agonists |

Notes: Astellas has developed multiple Sigma-1 receptor modulators including ATA-221 (for PD) and continues to explore S1R targets for neurodegenerative diseases.

Relmada Therapeutics

Website: [Relmada Therapeutics](https://www.relmada.com/)

| Attribute | Details |
|-----------|---------|
| Focus | CNS drug development |
| Lead Candidate | REL-1017 (Esmethadone) |
| Indication | Major depressive disorder (not AD-specific) |
| Stage | Phase 3 |
| Mechanism | NMDA antagonist (not S1R-focused) |

Notes: While Relmada's lead candidate targets NMDA pathways, the company has explored CNS mechanisms relevant to neurodegeneration.

NeuroSearch A/S

Notes: Original developer of pridopidine, which was outlicensed to Denki/Denka for continued development.

AlgoTherapeutics

Notes: Emerging company focused on Sigma-1 receptor modulators for CNS disorders.

Molecular Chaperone Approaches

Hsp90 Inhibitors

Hsp90 inhibitors shift the protein folding equilibrium toward Hsp70, enhancing degradation of misfolded proteins.

| Company | Candidate | Stage | Notes |
|---------|-----------|-------|-------|
| Biohaven Pharmaceutical | Multiple Hsp90 inhibitors | Discovery | Exploring CNS applications |
| Synta Oncology (acquired) | Ganetespib (STA-9090) | Discontinued | Originally for cancer, explored in neurodegeneration |

Hsp70 Inducers

| Company | Candidate | Stage | Notes |
|---------|-----------|-------|-------|
| Retro Biosciences | RB-001 | Phase 1 | Senolytic + chaperone approach for aging |
| Calico (Alphabet) | Various | Discovery | Aging biology focus |

Small Molecule Chaperones

| Company | Candidate | Stage | Notes |
|---------|-----------|-------|-------|
| Trehalose developers | Trehalose | Preclinical | Sugar molecule with chaperone activity |
| TUDCA (Tauroursodeoxycholic acid) | Various | Phase 2/3 | Bile acid with protein stabilization properties |

Proteostasis Therapeutics

Website: [Proteostasis Therapeutics](https://www.proteostasis.com/)

| Attribute | Details |
|-----------|---------|
| Focus | Protein homeostasis modulation |
| Platform | UPRmt (mitochondrial unfolded protein response) modulators |
| Stage | Discovery/Preclinical |
| Mechanism | Small molecules enhancing cellular protein quality control |

Hsp90-Targeted Approaches

Companies exploring Hsp90 inhibition for neurodegenerative diseases:

• Targeting client proteins including tau, Aβ, α-synuclein
• Brain-penetrant inhibitors in development
• Combination with Hsp70 inducers

Scientific Rationale for AD

Sigma-1 Receptor in AD Pathogenesis

Molecular Chaperones in AD

Pipeline Summary

| Approach | Companies | Stage | Promise |
|----------|-----------|-------|---------|
| S1R Agonists | Denka, Astellas, others | Phase 2-3 | High (proven safety in HD) |
| Hsp90 Inhibitors | Various | Discovery/Preclinical | Moderate |
| Hsp70 Inducers | Retro Biosciences, Calico | Phase 1/Discovery | Moderate-High |
| Small Molecule Chaperones | Various academic/industry | Preclinical | Moderate |

Related Pages

• [Sigma-1 Receptor Agonists](/therapeutics/sigma-1-receptor-agonists) — Detailed mechanism and compounds
• [Molecular Chaperone Therapy](/therapeutics/molecular-chaperone-therapy) — Chaperone biology and therapeutic approaches
• [Sigma1 Receptor Protein](/proteins/sigma1r-protein) — Protein structure and biology
• [ER Stress in Neurodegeneration](/mechanisms/er-stress-neurodegeneration) — Pathway details
• [Protein Homeostasis](/mechanisms/protein-homeostasis) — Proteostasis mechanisms

References