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Hypoimmune islets achieve insulin independence after allogeneic transplantation in a fully immunocompetent non-human primate

50

Citations

25

References

2024

Year

Abstract

Allogeneic transplantation of pancreatic islets for patients with difficult-to-control diabetes mellitus is severely hampered by the requirement for continuous immunosuppression and its associated morbidity. We report that allogeneic transplantation of genetically engineered (B2M<sup>-/-</sup>, CIITA<sup>-/-</sup>, CD47<sup>+</sup>), primary, hypoimmune, pseudo-islets (p-islets) results in their engraftment into a fully immunocompetent, diabetic non-human primate wherein they provide stable endocrine function and enable insulin independence without inducing any detectable immune response in the absence of immunosuppression. Hypoimmune primary p-islets may provide a curative cell therapy for type 1 diabetes mellitus.

References

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