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通过选择性渗透休克而非酶消化法分离有活力的猪胰岛。

Isolation of viable porcine islets by selective osmotic shock without enzymatic digestion.

作者信息

Atwater I, Guajardo M, Caviedes P, Jeffs S, Parrau D, Valencia M, Romero C, Arriagada C, Caamaño E, Salas A, Olguin F, Atlagich M, Maas R, Mears D, Rojas E

机构信息

Institute of Biomedical Sciences, University of Chile, Santiago, Chile.

出版信息

Transplant Proc. 2010 Jan-Feb;42(1):381-6. doi: 10.1016/j.transproceed.2009.11.030.

Abstract

Islet transplantation is a potential cure for type 1 diabetes, but clinical results have been disappointing. Currently, islet isolation is by enzymatic digestion of the pancreas which has significant pitfalls: warm ischemia exposure, collagenase-induced damage to the islet mass and viability, poor reproducibility, high cost, a relatively low number of islets obtained per whole pancreas, and selection of islets for collagenase resistance rather than for glucose responsiveness. In the present study we performed a series of experiments in a porcine model to demonstrate the feasibility of a new isolation method based on selective osmotic shock (SOS) using very high glucose solutions, doubling or tripling physiological osmotic strength. The SOS method can be carried out at room temperature or in the cold eliminating warm ischemia time which damages the islets. The SOS method does not depend on the texture of the pancreas so all pancreases can be processed identically and the process can be fully automated. The SOS method isolates all the islets of the pancreas regardless of size and shape allowing a greater number of islets to be harvested. The SOS method avoids exposure to toxins in collagenase solutions, is inexpensive and selects for islets with high concentrations of Glut 2 transporters, representing the best glucose responding islets. The SOS method showed a comparable recovery of islets from young pig pancreas and the islets showed improved viability. We conclude that the selective osmotic shock (SOS) method of separating islets from the pancreatic tissue is superior to the collagenase method.

摘要

胰岛移植是1型糖尿病的一种潜在治疗方法,但临床结果却令人失望。目前,胰岛分离是通过对胰腺进行酶消化来实现的,这种方法存在诸多严重缺陷:热缺血暴露、胶原酶对胰岛团块和活力造成的损伤、可重复性差、成本高、每个全胰腺获得的胰岛数量相对较少,以及选择抗胶原酶而非对葡萄糖有反应性的胰岛。在本研究中,我们在猪模型上进行了一系列实验,以证明一种基于选择性渗透休克(SOS)的新分离方法的可行性,该方法使用葡萄糖浓度为生理渗透压两倍或三倍的高糖溶液。SOS方法可在室温或低温下进行,消除了损害胰岛的热缺血时间。SOS方法不依赖于胰腺的质地,因此所有胰腺都可以以相同方式处理,并且该过程可以完全自动化。SOS方法能分离出胰腺的所有胰岛,无论其大小和形状如何,从而可收获更多数量的胰岛。SOS方法避免了接触胶原酶溶液中的毒素,成本低廉,且选择具有高浓度Glut 2转运蛋白的胰岛,这些胰岛代表了对葡萄糖反应最佳的胰岛。SOS方法从幼猪胰腺中分离出的胰岛回收率相当,且这些胰岛的活力有所提高。我们得出结论,从胰腺组织中分离胰岛的选择性渗透休克(SOS)方法优于胶原酶方法。

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