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预防胰岛移植中β细胞凋亡的干预策略。

Interventional strategies to prevent beta-cell apoptosis in islet transplantation.

作者信息

Emamaullee Juliet A, Shapiro A M James

机构信息

Surgical Medical Research Institute, University of Alberta, Edmonton, AB T6G 2N8.

出版信息

Diabetes. 2006 Jul;55(7):1907-14. doi: 10.2337/db05-1254.

Abstract

A substantial proportion of the transplanted islet mass fails to engraft due to death by apoptosis, and a number of strategies have been explored to inhibit beta-cell loss. Inhibition of extrinsic signals of apoptosis (i.e., cFLIP or A20) have been explored in experimental islet transplantation but have only shown limited impact. Similarly, strategies targeted at intrinsic signal inhibition (i.e., BCL-2) have not yet provided substantial improvement in islet engraftment. Recently, investigation of downstream apoptosis inhibitors that block the final common pathway (i.e., X-linked inhibitor of apoptosis protein [XIAP]) have demonstrated promise in both human and rodent models of engraftment. In addition, XIAP has enhanced long-term murine islet allograft survival. The complexities of both intrinsic and extrinsic apoptotic pathway inhibition are discussed in depth.

摘要

相当一部分移植的胰岛团块因凋亡死亡而未能成功植入,人们已经探索了多种策略来抑制β细胞损失。在实验性胰岛移植中已探索了抑制凋亡的外在信号(即cFLIP或A20),但仅显示出有限的影响。同样,针对内在信号抑制的策略(即BCL-2)尚未在胰岛植入方面带来实质性改善。最近,对阻断最终共同途径的下游凋亡抑制剂(即X连锁凋亡抑制蛋白[XIAP])的研究已在人类和啮齿动物植入模型中显示出前景。此外,XIAP提高了小鼠胰岛同种异体移植的长期存活率。本文深入讨论了内在和外在凋亡途径抑制的复杂性。

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