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首页> 外文期刊>Oligonucleotides >Sequence and Structural Features of RNA Aptamer Against Myasthenic Autoantibodies
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Sequence and Structural Features of RNA Aptamer Against Myasthenic Autoantibodies

机译:抗肌无力自身抗体的RNA适体的序列和结构特征

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摘要

Myasthenia gravis (MG) is mainly caused by autoantibodies to postsynaptic nicotinic acetylcholine receptors (AChRs). Previously, we isolated an RNA aptamer with 2′-amino pyrimidines that inhibited both a rat monoclonal antibody, which recognizes the main immunogenic region on the AChR, and MG patient autoantibodies from down-modulating AChRs on human cells. In this study, secondary configuration and binding motif of the aptamer were characterized, and moreover, various mutant aptamer forms were generated to figure out sequence and structure requirements of the aptamer. Then, we found that intrinsic structure formation and sequence composition of the selected RNA aptamer specific to the antibody are required for the aptamer activity to inhibit the myasthenic autoantibody-mediated destruction of cell surface AChRs. Noticeably, we identified 47-mer minimized aptamer version, which can efficiently protect cells from the effects of the autoantibodies and could be optimally applicable for MG therapy.
机译:重症肌无力(MG)主要是由对突触后烟碱型乙酰胆碱受体(AChRs)的自身抗体引起的。以前,我们分离了一种具有2'-氨基嘧啶的RNA适体,该适体可抑制大鼠单克隆抗体(该抗体识别AChR上的主要免疫原性区域)和MG患者自身抗体,从而抑制人类细胞上AChR的下调。在这项研究中,适体的二级构型和结合基序进行了表征,此外,产生了多种突变体适体形式,以找出适体的序列和结构要求。然后,我们发现选择的特异性针对抗体的RNA适体的内在结构形成和序列组成是适体活性抑制肌无力自身抗体介导的细胞表面AChRs破坏所需的。值得注意的是,我们确定了47-mer最小化适体形式,它可以有效保护细胞免受自身抗体的影响,并且可以最佳地应用于MG治疗。

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  • 来源
    《Oligonucleotides 》 |2009年第3期| 273-280| 共8页
  • 作者

    Jung-Sun Cho; Seong-Wook Lee;

  • 作者单位

    Department of Molecular Biology, Institute of Nanosensor and Biotechnology, Dankook University, Yongin, Republic of Korea.;

    Department of Molecular Biology, Institute of Nanosensor and Biotechnology, Dankook University, Yongin, Republic of Korea.;

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