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引导 2'--甲基化的分泌性小核仁 RNA 的长程功能。

Long-range function of secreted small nucleolar RNAs that direct 2'--methylation.

机构信息

From the Department of Medicine.

Mallinckrodt Institute of Radiology, and.

出版信息

J Biol Chem. 2018 Aug 24;293(34):13284-13296. doi: 10.1074/jbc.RA118.003410. Epub 2018 Jul 6.

Abstract

Small nucleolar RNAs (snoRNAs) are noncoding RNAs that guide chemical modifications of structural RNAs. Whereas snoRNAs primarily localize in the nucleolus, where their canonical function is to target nascent ribosomal RNAs for 2'--methylation, recent studies provide evidence that snoRNAs traffic out of the nucleus. Furthermore, RNA-Seq data indicate that extracellular vesicles released from cells contain snoRNAs. However, it is not known whether snoRNA secretion is regulated or whether secreted snoRNAs are functional. Here, we show that inflammation stimulates secretion of snoRNAs U32a (SNORD32a), U33 (SNORD33), U34 (SNORD34), and U35a (SNORD35a) from cultured macrophages, in mice, and in human subjects. Secreted snoRNAs co-fractionate with extracellular vesicles and are taken up by recipient cells. In a murine parabiosis model, we demonstrate that snoRNAs travel through the circulation to function in distant tissues. These findings support a previously unappreciated link between inflammation and snoRNA secretion in mice and humans and uncover a potential role for secreted snoRNAs in cell-cell communication.

摘要

小核仁 RNA(snoRNAs)是一类非编码 RNA,可指导结构 RNA 的化学修饰。尽管 snoRNAs 主要定位于核仁,其典型功能是靶向新生核糖体 RNA 进行 2'-甲基化,但最近的研究提供了证据表明 snoRNAs 会从核内输出。此外,RNA-Seq 数据表明,细胞释放的细胞外囊泡中含有 snoRNAs。然而,尚不清楚 snoRNA 的分泌是否受到调控,或者分泌的 snoRNAs 是否具有功能。在这里,我们发现炎症刺激培养的巨噬细胞、小鼠和人类来源的 snoRNA U32a(SNORD32a)、U33(SNORD33)、U34(SNORD34)和 U35a(SNORD35a)的分泌。分泌的 snoRNAs 与细胞外囊泡共分离,并被受体细胞摄取。在小鼠联体共生模型中,我们证明 snoRNAs 通过血液循环到达远处的组织发挥作用。这些发现支持了以前未被认识到的炎症与小鼠和人类 snoRNA 分泌之间的联系,并揭示了分泌 snoRNAs 在细胞间通讯中的潜在作用。

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