Xenotransplantation of embryonic pig pancreas for treatment of diabetes mellitus in non-human primates.

Marc R Hammerman
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引用次数: 9

Abstract

Transplantation therapy for diabetes in humans is limited by the low availability of human donor whole pancreas or islets. Outcomes are complicated by immunosuppressive drug toxicity. Xenotransplantation is a strategy to overcome supply problems. Implantation of tissue obtained early during embryogenesis is a way to reduce transplant immunogenicity. Pig insulin is biologically active in humans. In that regard the pig is an appropriate xenogeneic organ donor. Insulin-producing cells originating from embryonic pig pancreas obtained very early following pancreatic primordium formation [embryonic day 28 (E28)] engraft long-term in rhesus macaques. Endocrine cells originating from embryonic pig pancreas transplanted in host mesentery migrate to mesenteric lymph nodes, engraft, differentiate and improve glucose tolerance in rhesus macaques without the need for immune suppression. Transplantation of embryonic pig pancreas is a novel approach towards beta cell replacement therapy that could be applicable to humans.

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猪胚胎胰腺异种移植治疗非人类灵长类动物糖尿病。
人类糖尿病的移植治疗受到人类供体全胰腺或胰岛的低可用性的限制。结果因免疫抑制药物毒性而复杂化。异种移植是克服供应问题的一种策略。植入胚胎发生早期获得的组织是降低移植免疫原性的一种方法。猪胰岛素在人体内具有生物活性。在这方面,猪是一种合适的异种器官供体。来源于猪胚胎胰腺的产胰岛素细胞在恒河猴胰腺原基形成[胚胎第28天(E28)]后很早就获得。移植于宿主肠系膜的猪胚胎胰腺内分泌细胞在恒河猴体内无需免疫抑制即可迁移至肠系膜淋巴结并植入、分化和改善葡萄糖耐量。猪胚胎胰腺移植是一种适用于人类的β细胞替代疗法的新方法。
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