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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Dominant Suppression of Inflammation via Targeted Mutation of the mRNA Destabilizing Protein Tristetraprolin
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Dominant Suppression of Inflammation via Targeted Mutation of the mRNA Destabilizing Protein Tristetraprolin

机译:通过靶向突变的失稳蛋白Tristetraprolin的突变显着抑制炎症。

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摘要

In myeloid cells, the mRNA-destabilizing protein tristetraprolin (TTP) is induced and extensively phosphorylated in response to LPS. To investigate the role of two specific phosphorylations, at serines 52 and 178, we created a mouse strain in which those residues were replaced by nonphosphorylatable alanine residues. The mutant form of TTP was constitutively degraded by the proteasome and therefore expressed at low levels, yet it functioned as a potent mRNA destabilizing factor and inhibitor of the expression of many inflammatory mediators. Mice expressing only the mutant form of TTP were healthy and fertile, and their systemic inflammatory responses to LPS were strongly attenuated. Adaptive immune responses and protection against infection by Salmonella typhimurium were spared. A single allele encoding the mutant form of TTP was sufficient for enhanced mRNA degradation and underexpression of inflammatory mediators. Therefore, the equilibrium between unphosphorylated and phosphorylated TTP is a critical determinant of the inflammatory response, and manipulation of this equilibrium may be a means of treating inflammatory pathologies.
机译:在髓样细胞中,响应LPS,会破坏mRNA的稳定蛋白tristetraprolin(TTP)并被广泛磷酸化。为了研究丝氨酸52和178的两个特定磷酸化的作用,我们创建了一个小鼠品系,其中那些残基被不可磷酸化的丙氨酸残基取代。 TTP的突变形式被蛋白酶体组成性降解,因此以低水平表达,但它却充当了有效的mRNA不稳定因子和许多炎症介质表达的抑制剂。仅表达TTP突变形式的小鼠是健康且可育的,并且它们对LPS的全身炎症反应被大大减弱。避免了适应性免疫反应和鼠伤寒沙门氏菌的保护。编码TTP突变形式的单个等位基因足以增强mRNA降解和炎症介质表达不足。因此,未磷酸化和磷酸化的TTP之间的平衡是炎症反应的关键决定因素,对该平衡的控制可能是治疗炎症病理的一种手段。

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