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半胱天冬酶抑制剂 IDN6556 促进猪胰岛自体移植模型中边缘质量胰岛的植入。

Caspase inhibitor IDN6556 facilitates marginal mass islet engraftment in a porcine islet autotransplant model.

机构信息

Department of Surgery, University of Alberta, Edmonton, Alberta, Canada.

出版信息

Transplantation. 2012 Jul 15;94(1):30-5. doi: 10.1097/TP.0b013e318257745d.

Abstract

BACKGROUND

Large numbers of islets are lost in the early phase after clinical islet transplantation, through apoptosis, necrosis, or innate inflammatory injury. We previously demonstrated the efficacy of a series of caspase inhibitors in mouse models on islet engraftment through reduction in early posttransplant apoptosis. We studied IDN6556, a caspase inhibitor with a first-pass effect, in a large animal (pig) intraportal marginal mass islet autotransplant model.

METHODS

Total pancreatectomy and marginal mass islet autotransplantation were carried out in Yucatan miniature swine to explore the effects of IDN6556 on islet engraftment. Pigs were treated with IDN6556 at a dose of 20 mg/kg orally twice daily (n=7) or phosphate-buffered saline control (n=6) orally for 7 days, and blood glucose was monitored for 1 month. Glucose tolerance and acute insulin release were determined at 1 month.

RESULTS

There were no differences in islet procurement, isolation, or islet functional parameters between the two groups. Pigs receiving IDN6556 had lower fasting blood glucose level after transplantation and a higher percentage (100% vs. 33.3%) showed fasting blood glucose levels less than 11 mM. This translated into an enhanced metabolic reserve and acute insulin release for pigs in the treatment group.

CONCLUSIONS

IDN6556 led to enhanced islet engraftment in this large animal islet transplant model. Although this study has limitations including a short interval of study (1 month) and the use of unpurified islets, the results justify early clinical trials of IDN6556 in islet transplantation.

摘要

背景

大量胰岛在临床胰岛移植后的早期阶段通过细胞凋亡、坏死或固有炎症损伤而丢失。我们之前的研究表明,通过减少移植后早期细胞凋亡,一系列细胞凋亡抑制剂在胰岛移植的小鼠模型中具有疗效。我们在大型动物(猪)门静脉边缘质量胰岛自体移植模型中研究了具有首过效应的细胞凋亡抑制剂 IDN6556。

方法

在尤卡坦微型猪中进行全胰切除术和边缘质量胰岛自体移植,以探讨 IDN6556 对胰岛移植的影响。猪口服 IDN6556 20mg/kg,每日两次(n=7)或口服磷酸盐缓冲液对照(n=6),连续 7 天,并监测 1 个月的血糖。在 1 个月时测定葡萄糖耐量和急性胰岛素释放。

结果

两组间胰岛采集、分离或胰岛功能参数无差异。接受 IDN6556 治疗的猪在移植后空腹血糖水平较低,空腹血糖水平低于 11mM 的比例(100% vs. 33.3%)更高。这转化为治疗组猪的代谢储备和急性胰岛素释放增强。

结论

IDN6556 导致这种大型动物胰岛移植模型中的胰岛移植增强。尽管该研究存在局限性,包括研究时间短(1 个月)和使用未纯化的胰岛,但结果证明 IDN6556 在胰岛移植中的早期临床试验是合理的。

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