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Antibody cross-reactivity accounts for widespread appearance of m1A in 5'UTRs.


ABSTRACT: N1-methyladenosine (m1A) was proposed to be a highly prevalent modification in mRNA 5'UTRs based on mapping studies using an m1A-binding antibody. We developed a bioinformatic approach to discover m1A and other modifications in mRNA throughout the transcriptome by analyzing preexisting ultra-deep RNA-Seq data for modification-induced misincorporations. Using this approach, we detected appreciable levels of m1A only in one mRNA: the mitochondrial MT-ND5 transcript. As an alternative approach, we also developed an antibody-based m1A-mapping approach to detect m1A at single-nucleotide resolution, and confirmed that the commonly used m1A antibody maps sites to the transcription-start site in mRNA 5'UTRs. However, further analysis revealed that these were false-positives caused by binding of the antibody to the m7G-cap. A different m1A antibody that lacks cap-binding cross-reactivity does not show enriched binding in 5'UTRs. These results demonstrate that high-stoichiometry m1A sites are exceedingly rare in mRNAs and that previous mappings of m1A to 5'UTRs were the result of antibody cross-reactivity to the 5' cap.

SUBMITTER: Grozhik AV 

PROVIDER: S-EPMC6851129 | biostudies-literature | 2019 Nov

REPOSITORIES: biostudies-literature

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Antibody cross-reactivity accounts for widespread appearance of m<sup>1</sup>A in 5'UTRs.

Grozhik Anya V AV   Olarerin-George Anthony O AO   Sindelar Miriam M   Li Xing X   Gross Steven S SS   Jaffrey Samie R SR  

Nature communications 20191112 1


N<sup>1</sup>-methyladenosine (m<sup>1</sup>A) was proposed to be a highly prevalent modification in mRNA 5'UTRs based on mapping studies using an m<sup>1</sup>A-binding antibody. We developed a bioinformatic approach to discover m<sup>1</sup>A and other modifications in mRNA throughout the transcriptome by analyzing preexisting ultra-deep RNA-Seq data for modification-induced misincorporations. Using this approach, we detected appreciable levels of m<sup>1</sup>A only in one mRNA: the mitochond  ...[more]

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