Peptide-Based Wnt Signal Activation Enables Scalable Production of Clinical-Grade Patient-Derived Intestinal Organoids for Regenerative Cell Therapy
Sugihara HY, Nagata S, Kawasaki S, Takahashi J, Hiraguri Y, Fukuda M, et al.
Summary
Researchers at Institute of Science Tokyo developed a GMP-compliant protocol using the Wnt-activating peptide PG-008 to grow patient-derived colonic organoids for regenerative therapy. The peptide-based approach produced remarkably pure cultures of intestinal stem cells and transit-amplifying cells, achieving 82% organoid establishment rate from 60 patients. PG-008 organoid cultures outperformed conventional recombinant WNT3A in consistency and scalability.
Clinical Significance
This work represents a major step toward clinical-grade intestinal organoid production for autologous transplantation in GI diseases. The peptide-based Wnt activation eliminates the need for expensive recombinant proteins while improving culture purity — a critical advance for bringing regenerative GI therapies from bench to bedside.
Key Findings:
- GMP-compliant protocol using PG-008 peptide for colonic organoid expansion
- 82% establishment rate across 60 patients
- PG-008 enriched LGR5+ intestinal stem cells and injury-induced regenerative ISCs
- Single-cell RNA sequencing showed PG-008 cultures were more homogeneous than WNT3A
- Collagen-cultured organoids performed comparably to Matrigel
Clinical Takeaway: Peptide-based Wnt activation is a scalable, cost-effective alternative to recombinant protein for growing patient-derived intestinal organoids — paving the way for autologous cell therapies in conditions like IBD and short bowel syndrome.
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