tgf - β敲除和显性阴性受体转基因小鼠。

J J Letterio, E P Böttinger
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引用次数: 47

摘要

利用同源重组和转基因技术提供了小鼠模型来研究这三种哺乳动物tgf - β亚型的生理作用及其在完整动物环境下的调控。携带tgf - β同工型零突变的小鼠表明,它们在发育过程中发挥着离散的非重叠功能。tgf - β 1缺失小鼠揭示了该细胞因子在免疫系统调节中的关键作用,有证据表明各种免疫细胞群的发育、激活和功能发生了改变。将讨论在携带显性阴性突变tgf - β受体的转基因小鼠中组织和细胞限制性tgf - β信号通路中断的新方法。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
TGF-beta knockout and dominant-negative receptor transgenic mice.

Use of homologous recombination and transgenic technologies have provided mouse models to study the physiological roles of the three mammalian TGF-beta isoforms, and their regulation in the context of the intact animal. Mice harboring null mutations for TGF-beta isoforms demonstrate that each exerts discrete nonoverlapping functions during development. TGF-beta1 null mice reveal a crucial role for this cytokine in modulation of the immune system, with evidence for altered development, activation and function of various immune cell populations. New approaches to tissue- and cell-restricted disruption of TGF-beta signaling pathways in transgenic mice carrying dominant-negative mutant TGF-beta receptors will be discussed.

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