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Present and future cell therapies for pancreatic beta cell replenishment 被引量:3

Present and future cell therapies for pancreatic beta cell replenishment
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摘要 If only at a small scale,islet transplantation has successfully addressed what ought to be the primary endpoint of any cell therapy:the functional replenishment of damaged tissue in patients.After years of less-thanoptimal approaches to immunosuppression,recent advances consistently yield long-term graft survival rates comparable to those of whole pancreas transplantation.Limited organ availability is the main hurdle that stands in the way of the widespread clinical utilization of this pioneering intervention.Progress in stem cell research over the past decade,coupled with our decades-long experience with islet transplantation,is shaping the future of cell therapies for the treatment of diabetes.Here we review the most promising avenues of research aimed at generating an inexhaustible supply of insulin-producing cells for islet regeneration,including the differentiation of pluripotent and multipotent stem cells of embryonic and adult origin along the beta cell lineage and the direct reprogramming of non-endocrine tissues into insulin-producing cells. If only at a small scale,islet transplantation has successfully addressed what ought to be the primary endpoint of any cell therapy:the functional replenishment of damaged tissue in patients.After years of less-thanoptimal approaches to immunosuppression,recent advances consistently yield long-term graft survival rates comparable to those of whole pancreas transplantation.Limited organ availability is the main hurdle that stands in the way of the widespread clinical utilization of this pioneering intervention.Progress in stem cell research over the past decade,coupled with our decades-long experience with islet transplantation,is shaping the future of cell therapies for the treatment of diabetes.Here we review the most promising avenues of research aimed at generating an inexhaustible supply of insulin-producing cells for islet regeneration,including the differentiation of pluripotent and multipotent stem cells of embryonic and adult origin along the beta cell lineage and the direct reprogramming of non-endocrine tissues into insulin-producing cells.
出处 《World Journal of Gastroenterology》 SCIE CAS CSCD 2012年第47期6876-6884,共9页 世界胃肠病学杂志(英文版)
基金 Supported by Funding of the National Institutes of Health the Juvenile Diabetes Research Foundation the American Diabetes Association the Foundation for Diabetes Research the Diabetes Research Institute Foundation
关键词 细胞治疗 胰岛β细胞 多能干细胞 胰岛移植 免疫抑制 临床应用 细胞再生 重新编程 Human embryonic stem cells Induced pluripotent stem cells Mesenchymal stem cells Beta cell differentiation Reprogramming Islet transplantation
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