The Parent-into-F1 Model of Graft-vs-Host Disease as a Model of In Vivo T Cell Function and Immunomodulation.

Current medicinal chemistry. Immunology, endocrine & metabolic agents Pub Date : 2005-12-01 DOI:10.2174/156801305774962204

R A Puliaev, I A Puliaeva, A E Ryan, C S Via

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引用次数: 23

Abstract

Since its description roughly 30 years ago, the parent-into-F1 model of graft-vs.-host disease has provided insights into the mechanisms of in vivo T cell activation and the pathogenesis of autoimmune conditions. A new and emerging role for the P-->F1 model is one of identifying agents with immunomodulatory activity and defining in vivo mechanisms that promote cell mediated or antibody mediated immune responses. Because F1 mice are not irradiated prior to donor cell transfer, the P-->F1 model has in the past not been strictly analogous to human hematopoetic stem cell transplantation. However with the advent of newer non-myeloablative conditioning regimens, the model may assume more relevance. In this article, we first provide a review of relevant earlier fundamental observations followed by a summary of recent work from our laboratory in which acute and chronic GVHD in this model have been used not only to study normal T cell responses in vivo but also to define mechanisms important in the pathogenesis of autoimmunity and immunomodulation.

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移植物抗宿主病亲代转入f1模型作为体内T细胞功能和免疫调节的模型。

自大约30年前被描述以来，“亲代到f1”的移植物vs。-宿主病为体内T细胞活化机制和自身免疫性疾病的发病机制提供了见解。P- >F1模型的一个新作用是识别具有免疫调节活性的药物，并确定促进细胞介导或抗体介导的免疫反应的体内机制。由于F1小鼠在供体细胞移植之前没有经过照射，因此P- >F1模型过去并没有严格类比于人类造血干细胞移植。然而，随着新的非清髓调节疗法的出现，该模型可能具有更大的相关性。在本文中，我们首先回顾了相关的早期基本观察结果，然后总结了我们实验室最近的工作，其中急性和慢性GVHD在该模型中不仅用于研究体内正常T细胞反应，而且还用于定义自身免疫和免疫调节发病机制中的重要机制。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Current medicinal chemistry. Immunology, endocrine & metabolic agents

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