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首页> 外文期刊>Transplantation: Official Journal of the Transplantation Society >Reversal of diabetes by pancreatic islet transplantation into a subcutaneous, neovascularized device.
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Reversal of diabetes by pancreatic islet transplantation into a subcutaneous, neovascularized device.

机译:通过将胰岛移植到皮下的新血管化装置中来逆转糖尿病。

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BACKGROUND: Transplantation of pancreatic islets for the treatment of type 1 diabetes allows for physiologic glycemic control and insulin-independence when sufficient islets are implanted via the portal vein into the liver. Intrahepatic islet implantation requires specific infrastructure and expertise, and risks inherent to the procedure include bleeding, thrombosis, and elevation of portal pressure. Additionally, the relatively higher drug metabolite concentrations in the liver may contribute to the delayed loss of graft function of recent clinical trials. Identification of alternative implantation sites using biocompatible devices may be of assistance improving graft outcome. A desirable bioartificial pancreas should be easy to implant, biopsy, and retrieve, while allowing for sustained graft function. The subcutaneous (SC) site may require a minimally invasive procedure performed under local anesthesia, but its use has been hampered so far by lack of early vascularization, induction of local inflammation, and mechanical stress on the graft. METHODS: Chemically diabetic rats received syngeneic islets into the liver or SC into a novel biocompatible device consisting of a cylindrical stainless-steel mesh. The device was implanted 40 days prior to islet transplantation to allow embedding by connective tissue and neovascularization. Reversal of diabetes and glycemic control was monitored after islet transplantation. RESULTS: Syngeneic islets transplanted into a SC, neovascularized device restored euglycemia and sustained function long-term. Removal of graft-bearing devices resulted in hyperglycemia. Explanted grafts showed preserved islets and intense vascular networks. CONCLUSIONS: Ease of implantation, biocompatibility, and ability to maintain long-term graft function support the potential of our implantable device for cellular-based reparative therapies.
机译:背景:通过门静脉将足够的胰岛植入肝中时,胰岛的移植治疗1型糖尿病可实现生理性血糖控制和胰岛素独立性。肝内胰岛植入需要特定的基础设施和专业知识,并且该过程固有的风险包括出血,血栓形成和门脉压力升高。此外,肝脏中相对较高的药物代谢物浓度可能会导致近期临床试验中移植物功能的延迟丧失。使用生物相容性装置鉴定替代植入部位可能有助于改善移植物的结局。理想的生物人工胰腺应易于植入,活检和取出,同时允许持续的移植功能。皮下(SC)部位可能需要在局部麻醉下进行微创手术,但到目前为止,由于缺乏早期血管形成,局部炎症的诱导以及移植物的机械应力,其使用受到了阻碍。方法:化学性糖尿病大鼠将同种胰岛送入肝脏或将SC注入一种新型生物相容性装置中,该装置由圆柱形不锈钢网组成。在胰岛移植前40天植入该设备,以允许通过结缔组织包埋和新血管形成。胰岛移植后监测糖尿病的逆转和血糖控制。结果:同种异体胰岛移植到SC,新血管化装置中可恢复正常的血糖水平并长期维持功能。移除带有移植物的装置会导致高血糖症。外植移植物显示保留的胰岛和强烈的血管网络。结论:易于植入,生物相容性和维持长期移植功能的能力支持了我们的可植入设备用于基于细胞的修复疗法的潜力。

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