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Genetic Engineering of Immune Evasive Stem Cell-Derived Islets

Sara Dutton Sackett, Samuel J. Kaplan, Samantha A. Mitchell, Matthew E. Brown, Adam L. Burrack, Shane T. Grey, Danwei Huangfu, Jon S. Odorico

2022Transplant International28 citationsDOIOpen Access PDF

Abstract

Genome editing has the potential to revolutionize many investigative and therapeutic strategies in biology and medicine. In the field of regenerative medicine, one of the leading applications of genome engineering technology is the generation of immune evasive pluripotent stem cell-derived somatic cells for transplantation. In particular, as more functional and therapeutically relevant human pluripotent stem cell-derived islets (SCDI) are produced in many labs and studied in clinical trials, there is keen interest in studying the immunogenicity of these cells and modulating allogeneic and autoimmune immune responses for therapeutic benefit. Significant experimental work has already suggested that elimination of Human Leukocytes Antigen (HLA) expression and overexpression of immunomodulatory genes can impact survival of a variety of pluripotent stem cell-derived somatic cell types. Limited work published to date focuses on stem cell-derived islets and work in a number of labs is ongoing. Rapid progress is occurring in the genome editing of human pluripotent stem cells and their progeny focused on evading destruction by the immune system in transplantation models, and while much research is still needed, there is no doubt the combined technologies of genome editing and stem cell therapy will profoundly impact transplantation medicine in the future.

Topics & Concepts

Induced pluripotent stem cellRegenerative medicineStem cellGenome editingImmune systemTransplantationSomatic cellCell therapyMedicineBiologyImmunologyImmunogenicityComputational biologyEmbryonic stem cellGenomeGeneticsGeneInternal medicinePancreatic function and diabetesCRISPR and Genetic EngineeringPluripotent Stem Cells Research