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The Emerging Role of miR-223 in Platelet Reactivity: Implications in Antiplatelet Therapy

机译:miR-223在血小板反应性中的新兴作用:在抗血小板治疗中的意义。

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Platelets are anuclear cells and are devoid of genomic DNA, but they are capable ofde novoprotein synthesis from mRNA derived from their progenitor cells, megakaryocytes. There is mounting evidence that microRNA (miRNA) plays an important role in regulating gene expression in platelets. miR-223 is the most abundant miRNAs in megakaryocytes and platelets. One of the miR-223-regulated genes is ADP P2Y12, a key target for current antiplatelet drug therapy. Recent studies showed that a blunted response to P2Y12 antagonist, that is, high on-treatment platelet reactivity (HTPR), is a strong predictor of major cardiovascular events (MACEs) in coronary heart disease (CHD) patients receiving antiplatelet treatment. Recent clinical cohort study showed that the level of circulating miR-223 is inversely associated with MACE in CHD patients. In addition, our recent data demonstrated that the level of both intraplatelet and circulating miR-223 is an independent predictor for HTPR, thus providing a link between miR-223 and MACE. These lines of evidence indicate that miR-223 may serve as a potential regulatory target for HTPR, as well as a diagnostic tool for identification of HTPR in clinical settings.
机译:血小板是无核细胞,没有基因组DNA,但它们能够从其祖细胞巨核细胞衍生的mRNA中合成新蛋白。越来越多的证据表明,microRNA(miRNA)在调节血小板中的基因表达中起着重要作用。 miR-223是巨核细胞和血小板中最丰富的miRNA。 miR-223调控的基因之一是ADP P2Y12,它是当前抗血小板药物治疗的关键靶标。最近的研究表明,对P2Y12拮抗剂反应迟钝,即治疗中的高血小板反应性(HTPR),是接受抗血小板治疗的冠心病(CHD)患者主要心血管事件(MACE)的有力预测指标。最近的临床队列研究表明,在冠心病患者中,循环的miR-223的水平与MACE呈负相关。此外,我们最近的数据表明,血小板内和循环中的miR-223的水平都是HTPR的独立预测因子,因此提供了miR-223和MACE之间的联系。这些证据表明,miR-223可以作为HTPR的潜在调控靶标,并且可以作为在临床环境中鉴定HTPR的诊断工具。

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