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Unleashing TIGER on small RNAs
admin
2018-09-07
发布年2018
语种英语
国家美国
领域地球科学
正文(英文)
Credit: CC0 Public Domain

Efforts to explore the landscape of small RNAs (sRNAs)—short RNA molecules that are poorly understood—often use high-throughput sequencing (sRNA-seq). These efforts are hampered by a lack of tools to identify, quantify and analyze all the different sRNAs in sRNA-seq datasets.

Kasey Vickers, PhD, and colleagues have now developed a new analytical method called TIGER (Tools for Integrative Genome analysis of Extracellular sRNAs). To demonstrate the power of this , they performed sRNA-seq on mouse , bile, urine and livers. In the resulting datasets, TIGER was able to identify approximately 60 percent of sRNAs on lipoproteins and more than 85 percent of sRNAs in bile, urine and liver.

The researchers found that the majority of sRNAs on lipoproteins are non-host sRNAs derived from bacterial sources in the microbiome and environment.

The study, reported in the Journal of Extracellular Vesicles, revealed novel lipoprotein and biofluid sRNAs and showed that TIGER is well-suited to the study of sRNAs.

Explore further: Battling bubbles: How plants protect themselves from killer fungus

More information: Ryan M. Allen et al. Bioinformatic analysis of endogenous and exogenous small RNAs on lipoproteins, Journal of Extracellular Vesicles (2018). DOI: 10.1080/20013078.2018.1506198

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来源平台Science X network
文献类型新闻
条目标识符http://119.78.100.173/C666/handle/2XK7JSWQ/124688
专题地球科学
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admin. Unleashing TIGER on small RNAs. 2018.
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