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单链小干扰RNA比双链小干扰RNA更具免疫刺激性:2'-羟基尿苷在免疫反应中的核心作用。

Single-stranded small interfering RNA are more immunostimulatory than their double-stranded counterparts: a central role for 2'-hydroxyl uridines in immune responses.

作者信息

Sioud Mouldy

机构信息

The Norwegian Radium Hospital, Department of Immunology, Molecular Medicine Group Montebello, Oslo, Norway.

出版信息

Eur J Immunol. 2006 May;36(5):1222-30. doi: 10.1002/eji.200535708.

DOI:10.1002/eji.200535708
PMID:16609928
Abstract

It has recently become apparent that certain small interfering RNA (siRNA) sequences stimulate the innate immunity through endosomal Toll-like receptors (TLR), particularly TLR7 and TLR8. However, it remains unclear whether siRNA duplexes act as specific ligands for these receptors. To address this question and to overcome the problem of immune activation by siRNA, several RNA sequences were chemically synthesized and their effects were investigated. Results indicate that human peripheral blood mononuclear cells (PBMC) recognize and respond to a large number of sense or antisense single-stranded (ss) siRNA. In most cases immunostimulatory RNA motifs are more effectively recognized by innate immunity in the context of ss siRNA as compared to siRNA duplexes. Novel immunostimulatory RNA motifs were identified and their replacement with adenosines abrogated immune activation. Most notably, replacement of the 2'-hydroxyl uridines with either 2'-fluoro, 2'-deoxy or 2'-O-methyl uridines abrogated immune activation. Thus, immune recognition of RNA by TLR can be evaded by 2'-ribose modifications of only uridines. Collectively, the data should facilitate the development of siRNA therapeutics and expand the understanding of how RNA is sensed by innate immunity.

摘要

最近已明显发现,某些小干扰RNA(siRNA)序列通过内体Toll样受体(TLR),特别是TLR7和TLR8刺激先天免疫。然而,尚不清楚siRNA双链体是否作为这些受体的特异性配体。为了解决这个问题并克服siRNA引起的免疫激活问题,化学合成了几种RNA序列并研究了它们的作用。结果表明,人外周血单核细胞(PBMC)识别并对大量有义或反义单链(ss)siRNA作出反应。在大多数情况下,与siRNA双链体相比,免疫刺激RNA基序在ss siRNA背景下更有效地被先天免疫识别。鉴定了新的免疫刺激RNA基序,并用腺苷替代它们消除了免疫激活。最值得注意的是,用2'-氟、2'-脱氧或2'-O-甲基尿苷替代2'-羟基尿苷消除了免疫激活。因此,仅通过尿苷的2'-核糖修饰就可以规避TLR对RNA的免疫识别。总体而言,这些数据应有助于siRNA治疗药物的开发,并扩大对先天免疫如何感知RNA的理解。

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