免疫抑制
医学
小岛
糖尿病
移植
胰岛
人性化鼠标
免疫学
自身免疫
内科学
内分泌学
抗体
免疫系统
作者
Xiaomeng Hu,Corie Gattis,Ari G. Olroyd,Annabelle M. Friera,Kathy White,Chi Young,Ron Basco,Meghan Lamba,Frank Wells,Ramya Ankala,William E. Dowdle,August Lin,Kyla Egenberger,J. Michael Rukstalis,Jeffrey R. Millman,Andrew J. Connolly,T. Deuse,Sonja Schrepfer
出处
期刊:Science Translational Medicine
[American Association for the Advancement of Science (AAAS)]
日期:2023-04-12
卷期号:15 (691)
被引量:35
标识
DOI:10.1126/scitranslmed.adg5794
摘要
Transplantation of allogeneic pancreatic donor islets has successfully been performed in selected patients with difficult-to-control insulin-dependent diabetes and impaired awareness of hypoglycemia (IAH). However, the required systemic immunosuppression associated with this procedure prevents this cell replacement therapy from more widespread adoption in larger patient populations. We report the editing of primary human islet cells to the hypoimmune HLA class I- and class II-negative and CD47-overexpressing phenotype and their reaggregation into human HIP pseudoislets (p-islets). Human HIP p-islets were shown to survive, engraft, and ameliorate diabetes in immunocompetent, allogeneic, diabetic humanized mice. HIP p-islet cells were further shown to avoid autoimmune killing in autologous, diabetic humanized autoimmune mice. The survival and endocrine function of HIP p-islet cells were not impaired by contamination of unedited or partially edited cells within the p-islets. HIP p-islet cells were eliminated quickly and reliably in this model using a CD47-targeting antibody, thus providing a safety strategy in case HIP cells exert toxicity in a future clinical setting. Transplantation of human HIP p-islets for which no immunosuppression is required has the potential to lead to wider adoption of this therapy and help more diabetes patients with IAH and history of severe hypoglycemic events to achieve insulin independence.
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