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首页> 外文期刊>Cell transplantation >Donor Pretreatment With IL-1 Receptor Antagonist Attenuates Inflammation and Improves Functional Potency in Islets From Brain-Dead Nonhuman Primates
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Donor Pretreatment With IL-1 Receptor Antagonist Attenuates Inflammation and Improves Functional Potency in Islets From Brain-Dead Nonhuman Primates

机译:用IL-1受体拮抗剂预处理供体可减轻炎症,并改善脑死亡的非人灵长类动物胰岛的功能潜能。

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摘要

Most pancreas and islet grafts are recovered from brain-dead (BD) donors. In this study we characterized the early inflammatory response induced by brain death in pancreata and islets from nonhuman primate donors and evaluated the effect of targeted anti-inflammatory intervention in the protection of pancreatic islets prior to transplantation. BD donors were monitored for 6 h and assigned to three experimental groups: group 1: BD-untreated donors (BD-UT) (n=7), group 2: BD + donor pretreatment with IL-1ra (n=6), and group 3: non-BD animals serving as controls (n=7). We observed an IL-1ra-dependent reduction in the mobilization and activation of neutrophils from bone marrow and a significantly reduced accumulation of CD68(+) leukocytes in the pancreas and islets after brain death induction. Donor treatment with IL-1ra significantly decreased chemoldne mRNA expression (MCP-1, IL-8, and MIP-1a) and attenuated the activation of circulating neutrophils and intraislet macrophages as demonstrated by a reduction in intracellular IL-1 beta, IL-6, MCP-1, and MIP-1 alpha expression. As a result, IL-1ra dramatically improved viability, mitochondrial membrane polarity, and islet engraftment in mice transplanted using a minimal islet mass. These results suggest that early immunomodulation targeting inflammation in the BD donor may represent an effective therapeutic strategy to improve islet quality and function prior to transplantation.
机译:大多数胰腺和胰岛移植物均来自脑死亡(BD)供体。在这项研究中,我们表征了胰腺和非人类灵长类动物供体的胰岛中脑死亡引起的早期炎症反应,并评估了靶向抗炎干预在移植前保护胰岛中的作用。监测BD供体6小时,并分为三个实验组:第1组:未经BD治疗的供体(BD-UT)(n = 7),第2组:BD + IL-1ra预处理供体(n = 6),以及第3组:非BD动物作为对照(n = 7)。我们观察到IL-1ra依赖性减少中性粒细胞从骨髓的动员和激活,并显着减少诱导脑死亡的胰腺和胰岛中CD68(+)白细胞的积累。用IL-1ra进行的供体治疗可显着降低chemoldne mRNA表达(MCP-1,IL-8和MIP-1a),并减弱循环中的中性粒细胞和胰岛内巨噬细胞的活化,这可通过降低细胞内IL-1β,IL-6来证明,MCP-1和MIP-1 alpha表达式。结果,IL-1ra显着改善了使用最小胰岛质量移植的小鼠的生存力,线粒体膜极性和胰岛植入。这些结果表明,针对BD供体中炎症的早期免疫调节可能代表了改善胰岛质量和移植前功能的有效治疗策略。

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