A majority of m 6 A residues are in the last exons, allowing the potential for 3′ UTR regulation

Ke, Shengdong; Alemu, Endalkachew A.; Mertens, Claudia; Gantman, Emily C.; Fak, John J.; Mele, Aldo; Haripal, Bhagwattie; Zucker-Scharff, Ilana; Moore, Michael J.; Park, Christopher Y.; Vågbø, Cathrine Broberg; Kusśnierczyk, Anna; Klungland, Arne; Darnell, James; Darnell, Robert B.

doi:10.1101/gad.269415.115

articleGenes & DevelopmentSep 24, 2015DIAMOND OA

A majority of m 6 A residues are in the last exons, allowing the potential for 3′ UTR regulation

SKShengdong Ke EAEndalkachew A. Alemu CMClaudia Mertens ECEmily C. Gantman JJJohn J. Fak

Howard Hughes Medical Institute · Rockefeller University · +4 more institutions

PubMed

Indexed incrossrefpubmed

Abstract

We adapted UV CLIP (cross-linking immunoprecipitation) to accurately locate tens of thousands of m(6)A residues in mammalian mRNA with single-nucleotide resolution. More than 70% of these residues are present in the 3'-most (last) exons, with a very sharp rise (sixfold) within 150-400 nucleotides of the start of the last exon. Two-thirds of last exon m(6)A and >40% of all m(6)A in mRNA are present in 3' untranslated regions (UTRs); contrary to earlier suggestions, there is no preference for location of m(6)A sites around stop codons. Moreover, m(6)A is significantly higher in noncoding last exons than in next-to-last exons harboring stop codons. We found that m(6)A density peaks early in the 3' UTR and that,…

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Keywords

Exon
Biology
Untranslated region
Exon trapping
Genetics
Messenger RNA
Exon shuffling
Intron

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