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首页> 外文期刊>The journal of clinical investigation >microRNA-142–mediated repression of phosphodiesterase 3B critically regulates peripheral immune tolerance
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microRNA-142–mediated repression of phosphodiesterase 3B critically regulates peripheral immune tolerance

机译:microRNA-142介导的磷酸二酯酶3B的抑制关键调节外周免疫耐受

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Tregs play a fundamental role in immune tolerance via control of self-reactive effector T cells (Teffs). This function is dependent on maintenance of a high intracellular cAMP concentration. A number of microRNAs are implicated in the maintenance of Tregs. In this study, we demonstrate that peripheral immune tolerance is critically dependent on posttranscriptional repression of the cAMP-hydrolyzing enzyme phosphodiesterase-3b ( Pde3b ) by microRNA-142-5p (miR-142-5p). In this manner, miR-142-5p acts as an immunometabolic regulator of intracellular cAMP, controlling Treg suppressive function. Mir142 was associated with a super enhancer bound by the Treg lineage–determining transcription factor forkhead box P3 (FOXP3), and Treg-specific deletion of miR-142 in mice (Treg ~(Δ142)) resulted in spontaneous, lethal, multisystem autoimmunity, despite preserved numbers of phenotypically normal Tregs. Pharmacological inhibition and genetic ablation of PDE3B prevented autoimmune disease and reversed the impaired suppressive function of Tregs in Treg ~(Δ142) animals. These findings reveal a critical molecular switch, specifying Treg function through the modulation of a highly conserved, cell-intrinsic metabolic pathway. Modulation of this pathway has direct relevance to the pathogenesis and treatment of autoimmunity and cancer.
机译:Treg通过控制自我反应性效应T细胞(Teffs)在免疫耐受中起重要作用。该功能取决于维持高细胞内cAMP浓度。许多微RNA与Treg的维持有关。在这项研究中,我们证明了外周免疫耐受关键取决于microRNA-142-5p(miR-142-5p)对cAMP水解酶磷酸二酯酶3b(Pde3b)的转录后抑制。以这种方式,miR-142-5p充当细胞内cAMP的免疫代谢调节剂,控制Treg抑制功能。 Mir142与受Treg谱系决定的转录因子叉头盒P3(FOXP3)结合的超级增强子有关,小鼠中Treg特异性缺失miR-142(Treg〜(Δ142))导致自发,致命的多系统自身免疫,尽管保留了大量表型正常的Treg。 PDE3B的药理抑制和遗传消除可预防自身免疫性疾病,并逆转Treg〜(Δ142)动物中Treg的抑制功能受损。这些发现揭示了关键的分子开关,通过高度保守的细胞内源性代谢途径的调节来指定Treg功能。该途径的调节与自身免疫和癌症的发病机理和治疗直接相关。

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