MHC matching fails to prevent long-term rejection of iPSC-derived neurons in non-human primates.
Romina Aron BadinAurore BugiSusannah WilliamsMarta VadoriMarie MichaelCaroline JanAlberto NassiSophie LecourtoisAntoine BlancherEmanuele CozziPhilippe HantrayeAnselme L PerrierPublished in: Nature communications (2019)
Cell therapy products (CTP) derived from pluripotent stem cells (iPSCs) may constitute a renewable, specifically differentiated source of cells to potentially cure patients with neurodegenerative disorders. However, the immunogenicity of CTP remains a major issue for therapeutic approaches based on transplantation of non-autologous stem cell-derived neural grafts. Despite its considerable side-effects, long-term immunosuppression, appears indispensable to mitigate neuro-inflammation and prevent rejection of allogeneic CTP. Matching iPSC donors' and patients' HLA haplotypes has been proposed as a way to access CTP with enhanced immunological compatibility, ultimately reducing the need for immunosuppression. In the present work, we challenge this paradigm by grafting autologous, MHC-matched and mis-matched neuronal grafts in a primate model of Huntington's disease. Unlike previous reports in unlesioned hosts, we show that in the absence of immunosuppression MHC matching alone is insufficient to grant long-term survival of neuronal grafts in the lesioned brain.
Keyphrases
- cell therapy
- pluripotent stem cells
- induced pluripotent stem cells
- stem cells
- end stage renal disease
- bone marrow
- mesenchymal stem cells
- ejection fraction
- induced apoptosis
- chronic kidney disease
- cerebral ischemia
- endothelial cells
- stem cell transplantation
- peritoneal dialysis
- blood brain barrier
- low dose
- endoplasmic reticulum stress
- white matter
- high dose
- spinal cord injury
- cell proliferation
- brain injury
- drug induced
- patient reported