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西罗莫司与胰岛植入减少和β细胞功能受损有关。

Sirolimus is associated with reduced islet engraftment and impaired beta-cell function.

作者信息

Zhang Nan, Su Dongming, Qu Shen, Tse Tonia, Bottino Rita, Balamurugan A N, Xu Jing, Bromberg Jonathan S, Dong H Henry

机构信息

Department of Gene and Cell Medicine, Mount Sinai School of Medicine, New York, NY, USA.

出版信息

Diabetes. 2006 Sep;55(9):2429-36. doi: 10.2337/db06-0173.

Abstract

Successful islet transplantation depends on the infusion of sufficiently large quantities of islets, but only a fraction of transplanted islets can survive and become engrafted, and yet the underlying mechanism remains unclear. In this study, we examined the effect of sirolimus, a key component of the immunosuppressive regimen in clinical islet transplantation, on islet engraftment and function. To distinguish the effect of sirolimus on immune rejection from its effect on islet engraftment, we used a syngeneic model. Diabetic mice were transplanted with 250 islets under the renal capsule, followed by treatment with sirolimus or vehicle for 14 days. Thirty days posttransplantation, islet grafts were retrieved for the determination of insulin content and vascular density. Compared with mock-treated controls, diabetic recipient mice receiving sirolimus exhibited impaired blood glucose profiles and reduced glucose-stimulated insulin secretion, correlating with reduced intragraft insulin content and decreased vascular density. Islets exposed to sirolimus for 24 h in culture displayed significantly diminished glucose-stimulated insulin release, coinciding with decreased pancreas duodenum homeobox-1 and GLUT2 expression in cultured islets. Furthermore, sirolimus-treated diabetic recipient mice, as opposed to mock-treated controls, were associated with dyslipidemia. These data suggest that sirolimus, administered in the early posttransplantation phase, is a confounding factor for reduced islet engraftment and impaired beta-cell function in transplants.

摘要

成功的胰岛移植依赖于输注足够大量的胰岛,但只有一小部分移植的胰岛能够存活并实现植入,然而其潜在机制仍不清楚。在本研究中,我们研究了西罗莫司(临床胰岛移植免疫抑制方案的关键成分)对胰岛植入和功能的影响。为了区分西罗莫司对免疫排斥的影响与其对胰岛植入的影响,我们使用了同基因模型。将糖尿病小鼠在肾被膜下移植250个胰岛,随后用西罗莫司或赋形剂治疗14天。移植后30天,取出胰岛移植物以测定胰岛素含量和血管密度。与模拟治疗的对照组相比,接受西罗莫司治疗的糖尿病受体小鼠血糖水平受损,葡萄糖刺激的胰岛素分泌减少,这与移植物内胰岛素含量降低和血管密度下降相关。在培养中暴露于西罗莫司24小时的胰岛显示葡萄糖刺激的胰岛素释放显著减少,这与培养的胰岛中胰腺十二指肠同源盒-1和葡萄糖转运蛋白2表达降低一致。此外,与模拟治疗的对照组相反,接受西罗莫司治疗的糖尿病受体小鼠伴有血脂异常。这些数据表明,在移植后早期给予西罗莫司是移植中胰岛植入减少和β细胞功能受损的一个混杂因素。

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