Structural bias in T4 RNA ligase-mediated 3'-adapter ligation

T4 RNA ligases are commonly used to attach adapters to RNAs, but large differences in ligation efficiency make detection and quantitation problematic. We developed a ligation selection strategy using random RNAs in combination with high-throughput sequencing to gain insight into the differences in e...

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Veröffentlicht in:	Nucleic acids research 2012-04, Vol.40 (7), p.e54-e54
Hauptverfasser:	Zhuang, Fanglei, Fuchs, Ryan T, Sun, Zhiyi, Zheng, Yu, Robb, G Brett
Format:	Artikel
Sprache:	eng
Schlagworte:	Animals DNA DNA sequencing High-Throughput Nucleotide Sequencing Methods Online Mice MicroRNAs - chemistry MicroRNAs - metabolism miRNA Nucleic Acid Conformation Nucleotide sequence Nucleotides Oligonucleotides - chemistry Protein structure Quantitation RNA - chemistry RNA - metabolism RNA Folding RNA ligase RNA Ligase (ATP) - metabolism Secondary structure Sequence Analysis, RNA Viral Proteins - metabolism
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container_title	Nucleic acids research
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creator	Zhuang, Fanglei Fuchs, Ryan T Sun, Zhiyi Zheng, Yu Robb, G Brett
description	T4 RNA ligases are commonly used to attach adapters to RNAs, but large differences in ligation efficiency make detection and quantitation problematic. We developed a ligation selection strategy using random RNAs in combination with high-throughput sequencing to gain insight into the differences in efficiency of ligating pre-adenylated DNA adapters to RNA 3'-ends. After analyzing biases in RNA sequence, secondary structure and RNA-adapter cofold structure, we conclude that T4 RNA ligases do not show significant primary sequence preference in RNA substrates, but are biased against structural features within RNAs and adapters. Specifically, RNAs with less than three unstructured nucleotides at the 3'-end and RNAs that are predicted to cofold with an adapter in unfavorable structures are likely to be poorly ligated. The effect of RNA-adapter cofold structures on ligation is supported by experiments where the ligation efficiency of specific miRNAs was changed by designing adapters to alter cofold structure. In addition, we show that using adapters with randomized regions results in higher ligation efficiency and reduced ligation bias. We propose that using randomized adapters may improve RNA representation in experiments that include a 3'-adapter ligation step.
doi_str_mv	10.1093/nar/gkr1263
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subjects	Animals DNA DNA sequencing High-Throughput Nucleotide Sequencing Methods Online Mice MicroRNAs - chemistry MicroRNAs - metabolism miRNA Nucleic Acid Conformation Nucleotide sequence Nucleotides Oligonucleotides - chemistry Protein structure Quantitation RNA - chemistry RNA - metabolism RNA Folding RNA ligase RNA Ligase (ATP) - metabolism Secondary structure Sequence Analysis, RNA Viral Proteins - metabolism
title	Structural bias in T4 RNA ligase-mediated 3'-adapter ligation
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