生物
转移RNA
计算生物学
基因组
遗传学
互补DNA
基因
模式生物
核糖核酸
作者
Andrew Behrens,Geraldine Rodschinka,Danny D. Nedialkova
出处
期刊:Molecular Cell
[Elsevier BV]
日期:2021-02-15
卷期号:81 (8): 1802-1815.e7
被引量:254
标识
DOI:10.1016/j.molcel.2021.01.028
摘要
Measurements of cellular tRNA abundance are hampered by pervasive blocks to cDNA synthesis at modified nucleosides and the extensive similarity among tRNA genes. We overcome these limitations with modification-induced misincorporation tRNA sequencing (mim-tRNAseq), which combines a workflow for full-length cDNA library construction from endogenously modified tRNA with a comprehensive and user-friendly computational analysis toolkit. Our method accurately captures tRNA abundance and modification status in yeast, fly, and human cells and is applicable to any organism with a known genome. We applied mim-tRNAseq to discover a dramatic heterogeneity of tRNA isodecoder pools among diverse human cell lines and a surprising interdependence of modifications at distinct sites within the same tRNA transcript.
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