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首页> 外文期刊>Experimental Hematology: Official Publication of the International Society for Experimental Hematology >Deep sequencing and proteomic analysis of the microRNA-induced silencing complex in human red blood cells
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Deep sequencing and proteomic analysis of the microRNA-induced silencing complex in human red blood cells

机译:人类红细胞中microRNA诱导的沉默复合物的深度测序和蛋白质组学分析

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摘要

During maturation, erythropoietic cells extrude their nuclei but retain their ability to respond to oxidant stress by tightly regulating protein translation. Several studies have reported microRNA-mediated regulation of translation during terminal stages of erythropoiesis, even after enucleation. In the present study, we performed a detailed examination of the endogenous microRNA machinery in human red blood cells using a combination of deep sequencing analysis of microRNAs and proteomic analysis of the microRNA-induced silencing complex. Among the 197 different microRNAs detected, miR-451a was the most abundant, representing more than 60% of all read sequences. In addition, miR-451a and its known target, 14-3-3 zeta mRNA, were bound to the microRNA-induced silencing complex, implying their direct interaction in red blood cells. The proteomic characterization of endogenous Argonaute 2-associated microRNA-induced silencing complex revealed 26 cofactor candidates. Among these cofactors, we identified several RNA-binding proteins, as well as motor proteins and vesicular trafficking proteins. Our results demonstrate that red blood cells contain complex microRNA machinery, which might enable immature red blood cells to control protein translation independent of de novo nuclei information. Copyright (C) 2015 ISEH - International Society for Experimental Hematology. Published by Elsevier Inc.
机译:在成熟过程中,促红细胞挤出其细胞核,但通过严格调节蛋白质翻译而保持其对氧化应激反应的能力。几项研究报道了在红细胞生成的最终阶段,甚至在去核后,microRNA介导的翻译调控。在本研究中,我们结合使用了microRNA的深度测序分析和microRNA诱导的沉默复合物的蛋白质组学,对人类红细胞中的内源性microRNA机制进行了详细的检查。在检测到的197种不同的microRNA中,miR-451a最丰富,占所有读取序列的60%以上。另外,miR-451a及其已知靶标14-3-3 zeta mRNA与microRNA诱导的沉默复合物结合,暗示它们在红细胞中的直接相互作用。内源性Argonaute 2相关的microRNA诱导的沉默复合物的蛋白质组学表征揭示了26个辅因子候选物。在这些辅助因子中,我们鉴定了几种RNA结合蛋白,以及运动蛋白和水泡运输蛋白。我们的结果表明,红细胞包含复杂的microRNA机制,这可能使未成熟的红细胞能够独立于新核信息而控制蛋白质翻译。版权所有(C)2015 ISEH-国际实验血液学会。由Elsevier Inc.发布

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