Long-term glycemic control using polymer-encapsulated human stem cell–derived beta cells in immune-competent mice

免疫系统 移植 免疫抑制 血糖性 胰岛素 医学 细胞疗法 糖尿病 干细胞 免疫学 生物 内科学 内分泌学 细胞生物学
作者
Arturo J. Vegas,Omid Veiseh,Mads Gürtler,Jeffrey R. Millman,Felicia W. Pagliuca,Andrew Bader,Joshua C. Doloff,Jie Li,Michael Chen,Karsten Olejnik,Hok Hei Tam,Siddharth Jhunjhunwala,Erin Langan,Stephanie Aresta-Dasilva,Srujan Gandham,James J. McGarrigle,Matthew A. Bochenek,Jennifer Hollister‐Lock,José Oberholzer,Dale L. Greiner,Gordon C. Weir,Douglas A. Melton,Róbert Langer,Daniel G. Anderson
出处
期刊:Nature Medicine [Nature Portfolio]
卷期号:22 (3): 306-311 被引量:622
标识
DOI:10.1038/nm.4030
摘要

The transplantation of glucose-responsive, insulin-producing cells offers the potential for restoring glycemic control in individuals with diabetes. Pancreas transplantation and the infusion of cadaveric islets are currently implemented clinically, but these approaches are limited by the adverse effects of immunosuppressive therapy over the lifetime of the recipient and the limited supply of donor tissue. The latter concern may be addressed by recently described glucose-responsive mature beta cells that are derived from human embryonic stem cells (referred to as SC-β cells), which may represent an unlimited source of human cells for pancreas replacement therapy. Strategies to address the immunosuppression concerns include immunoisolation of insulin-producing cells with porous biomaterials that function as an immune barrier. However, clinical implementation has been challenging because of host immune responses to the implant materials. Here we report the first long-term glycemic correction of a diabetic, immunocompetent animal model using human SC-β cells. SC-β cells were encapsulated with alginate derivatives capable of mitigating foreign-body responses in vivo and implanted into the intraperitoneal space of C57BL/6J mice treated with streptozotocin, which is an animal model for chemically induced type 1 diabetes. These implants induced glycemic correction without any immunosuppression until their removal at 174 d after implantation. Human C-peptide concentrations and in vivo glucose responsiveness demonstrated therapeutically relevant glycemic control. Implants retrieved after 174 d contained viable insulin-producing cells.
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