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门静脉内胰岛移植中的血栓形成与炎症:病理生理学及新兴治疗方法综述

Thrombosis and inflammation in intraportal islet transplantation: a review of pathophysiology and emerging therapeutics.

作者信息

Wilson John T, Chaikof Elliot L

机构信息

Department of Biomedical Engineering, Georgia Institute of Technology, Atlanta, Georgia, USA.

出版信息

J Diabetes Sci Technol. 2008 Sep;2(5):746-59. doi: 10.1177/193229680800200502.

DOI:10.1177/193229680800200502
PMID:19885257
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2769789/
Abstract

With the inception of the Edmonton Protocol, intraportal islet transplantation (IPIT) has re-emerged as a promising cell-based therapy for type 1 diabetes. However, current clinical islet transplantation remains limited, in part, by the need to transplant islets from 2-4 donor organs, often through several separate infusions, to reverse diabetes in a single patient. Results from clinical islet transplantation and experimental animal models now indicate that the majority of transplanted islets are destroyed in the immediate post-transplant period, a process largely facilitated by deleterious inflammatory responses triggered by islet-derived procoagulant and proinflammatory mediators. Herein, mechanisms that underlie the pathophysiology of thrombosis and inflammation in IPIT are reviewed, and emerging approaches to improve islet engraftment through attenuation of inflammatory responses are discussed.

摘要

随着埃德蒙顿方案的启动,门静脉内胰岛移植(IPIT)已再度成为一种有前景的1型糖尿病细胞疗法。然而,目前的临床胰岛移植仍受到限制,部分原因是需要从2至4个供体器官移植胰岛,通常要通过几次单独输注,才能使单一患者的糖尿病得到逆转。临床胰岛移植和实验动物模型的结果表明,大多数移植的胰岛在移植后即刻被破坏,这一过程在很大程度上是由胰岛衍生的促凝和促炎介质引发的有害炎症反应所推动的。本文综述了IPIT中血栓形成和炎症病理生理学的潜在机制,并讨论了通过减轻炎症反应来改善胰岛植入的新方法。

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