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DOWNREGULATION OF INFLAMMATORY MICRORNAS BY ILT3

机译:ILT3对发炎微RNA的下调

摘要

It has been discovered that inhibition of two or more specific inflammatory miRs (30b, 21, 146a, and 155) suppresses T cell proliferation, promotes T cell anergy or induces the formation of suppressor T cells, thereby providing a focused therapy with minimal toxicity for disorders associated with abnormally high immune responses. The corollary involves increasing the level of certain proinflammatory miRs thereby providing methods for immuno stimulation. It has also been discovered that significant increases of serum miR21 which occur in heart allograft rejection can be used to identify patients that have this disorder without requiring a biopsy.
机译:已经发现抑制两个或多个特定的炎性miRs(30b,21、146a和155)可抑制T细胞增殖,促进T细胞无反应性或诱导抑制性T细胞的形成,从而提供针对毒性最小的集中疗法与异常高免疫反应有关的疾病。结果涉及增加某些促炎性miR的水平,从而提供免疫刺激的方法。还已经发现,在心脏同种异体移植排斥反应中出现的血清miR21的显着增加可用于鉴定患有这种疾病的患者而无需活检。

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