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Extracellular vesicle associated long non-coding RNAs functionally enhance cell viability

机译:细胞外小泡相关的长非编码RNA功能增强细胞活力

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摘要

Cells communicate with one another to create microenvironments and share resources. One avenue by which cells communicate is through the action of exosomes. Exosomes are extracellular vesicles that are released by one cell and taken up by neighbouring cells. But how exosomes instigate communication between cells has remained largely unknown. We present evidence here that particular long non-coding RNA molecules are preferentially packaged into exosomes. We also find that a specific class of these exosome associated non-coding RNAs functionally modulate cell viability by direct interactions with l-lactate dehydrogenase B (LDHB), high-mobility group protein 17 (HMG-17), and CSF2RB, proteins involved in metabolism, nucleosomal architecture and cell signalling respectively. Knowledge of this endogenous cell to cell pathway, those proteins interacting with exosome associated non-coding transcripts and their interacting domains, could lead to a better understanding of not only cell to cell interactions but also the development of exosome targeted approaches in patient specific cell-based therapies.
机译:单元之间相互通信以创建微环境并共享资源。细胞交流的一种途径是通过外来体的作用。外泌体是由一个细胞释放并被邻近细胞吸收的细胞外囊泡。但是,外泌体如何促进细胞之间的通讯仍然是未知的。我们在这里提供证据,特别长的非编码RNA分子优先包装到外来体中。我们还发现,这些外泌体相关的非编码RNA的特定类别通过与l-乳酸脱氢酶B(LDHB),高迁移率族蛋白17(HMG-17)和CSF2RB(与参与的蛋白)直接相互作用来功能性地调节细胞活力。代谢,核小体结构和细胞信号转导。了解这种内源性细胞间通路,与外泌体相关的非编码转录物及其相互作用域相互作用的蛋白质,不仅可以更好地理解细胞间相互作用,还可以开发针对患者特异性细胞的外泌体靶向方法。基础疗法。

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