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Fewer Islets Survive from a First Transplant than a Second Transplant: Evaluation of Repeated Intraportal Islet Transplantation in Mice

机译:较少的胰岛从第一移植物质生存,而不是第二次移植:评估小鼠中重复的内部内胰岛移植

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Beta cell replacement is an exciting field where new beta cell sources and alternative sites are widely explored. The liver has been the implantation site of choice in the clinic since the advent of islet transplantation. However, in most cases, repeated islet transplantation is needed to achieve normoglycemia in diabetic recipients. This study aimed to investigate whether there are differences in islet survival and engraftment between a first and a second transplantation, performed 1 week apart, to the liver. C57BL/6 mice were accordingly transplanted twice with an initial infusion of syngeneic islets expressing green fluorescent protein (GFP). The second islet transplant was performed 1 week later and consisted of islets isolated from non-GFP C57BL/6-mice. Animals were sacrificed either 1 day or 1 month after the second transplantation. A control group received a saline infusion instead of GFP-expressing islets, 1 week later obtained a standard non-GFP islet transplant, and was subsequently sacrificed 1 month later. Islet engraftment in the liver was assessed by immunohistochemistry and serum was analyzed for angiogenic factors induced by the first islet transplantation. Almost 70% of islets found in the liver following repeated islet transplantation originated from the second transplantation. The vascular density in the transplanted non-GFP-expressing islets did not differ depending on whether their transplantation was preceded by a primary islet transplantation or saline administration only. Nor did angiogenic factors in serum prior to the transplantation of non-GFP islets differ between animals that had received a previous islet transplantation or a saline infusion. We conclude that first islet transplantation creates, by unknown mechanisms, favorable conditions for the survival of a second transplant to the liver.
机译:β电池更换是令人兴奋的领域,其中新的β细胞来源和替代网站被广泛探索。自胰岛移植的出现以来,肝脏一直是临床中选择的植入部位。然而,在大多数情况下,需要重复的胰岛移植,以实现糖尿病受体的常规血糖。本研究旨在调查第一和第二移植之间的胰岛存活和植入是否存在差异,对肝脏进行1周进行1周。因此,C57BL / 6小鼠通过表达绿色荧光蛋白(GFP)的初始输注进行两次移植两次。第二个胰岛移植1周后进行,并由从非GFP C57BL / 6小鼠分离的胰岛组成。在第二次移植后1天或1个月牺牲了动物。对照组接受盐水输注,而不是表达GFP表达的胰岛,1周后获得标准的非GFP胰岛移植,随后在1个月后处死。通过免疫组织化学评估肝脏中的胰岛植入,并分析血清用于由第一胰岛移植诱导的血管生成因子。在重复的胰岛移植起源于第二个移植后,肝脏中发现的几乎70%的胰岛。移植的非GFP表达胰岛中的血管密度根据其移植是否以仅通过原发性胰岛移植或盐水给药而不同。在移植非GFP胰岛之前的血清中的血管生成因子在接受先前的胰岛移植或盐水输注的动物之间存在差异。我们得出结论,首次胰岛移植通过未知的机制创造,对肝脏的第二次移植的存活条件产生了有利的条件。

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