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Thymocyte-targeted overexpression of xiap transgene disrupts T lymphoid apoptosis and maturation

机译:胸腺细胞靶向过表达xiap 转基因破坏T淋巴样细胞凋亡和成熟

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摘要

The X-linked inhibitor of apoptosis (XIAP) and other members of the inhibitor of apoptosis (IAP) family can suppress apoptosis induced by a diverse variety of triggers. Functional studies done to date have focused on tissue culture models and adenovirus overexpression of XIAP and other IAP proteins. Here we report the phenotype of an engineered transgenic mouse overexpressing a human IAP, as well as assessing the long-term consequence of IAP overexpression. We document the relative protein expression levels of the endogenous mouse homologue to XIAP, mouse inhibitor of apoptosis (MIAP 3), within thymocyte and T cell subpopulations. The consequence of lymphoid-targeted overexpression of XIAP in transgenic mice suggests a physiological role for the endogenous protein, MIAP3. Xiap-transgenic mice accumulated thymocytes and/or T cells in primary and secondary lymphoid tissue, T cell maturation was perturbed, and transgenic thymocytes resisted a variety of apoptotic triggers both in vitro and in vivo. These observations imply a possible key function for the intrinsic cellular inhibitor XIAP in maintaining the homeostasis of the immune system.
机译:X连锁的凋亡抑制剂(XIAP)和凋亡抑制剂(IAP)家族的其他成员可以抑制由多种触发因素诱导的凋亡。迄今为止完成的功能性研究集中在组织培养模型以及XIAP和其他IAP蛋白的腺病毒过度表达上。在这里,我们报告了过表达人IAP的工程化转基因小鼠的表型,并评估了IAP过表达的长期后果。我们记录了胸腺细胞和T细胞亚群内XIAP,小鼠凋亡的抑制因子(MIAP 3)的内源性小鼠同源物的相对蛋白表达水平。在转基因小鼠中以淋巴样靶向的XIAP过表达的结果表明内源性蛋白质MIAP3具有生理作用。 Xiap转基因小鼠在原发性和继发性淋巴组织中积累了胸腺细胞和/或T细胞,扰动了T细胞的成熟,转基因胸腺细胞在体外和体内均能抵抗多种凋亡触发。这些观察 暗示内在细胞抑制剂XIAP可能具有关键功能 维持免疫系统的动态平衡。

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