CMTr mediated 2′-O-ribose methylation status of cap-adjacent nucleotides across animals

Author:

Dix Thomas C.,Haussmann Irmgard U.,Brivio Sarah,Nallasivan Mohannakarthik P.,HadzHiev Yavor,Müller Ferenc,Müller Berndt,Pettitt JonathanORCID,Soller MatthiasORCID

Abstract

Cap methyltransferases (CMTrs) O methylate the 2′ position of the ribose (cOMe) of cap-adjacent nucleotides of animal, protist, and viral mRNAs. Animals generally have two CMTrs, whereas trypanosomes have three, and many viruses encode one in their genome. In the splice leader of mRNAs in trypanosomes, the first four nucleotides contain cOMe, but little is known about the status of cOMe in animals. Here, we show that cOMe is prominently present on the first two cap-adjacent nucleotides with species- and tissue-specific variations in Caenorhabditis elegans, honeybees, zebrafish, mouse, and human cell lines. In contrast, Drosophila contains cOMe primarily on the first cap-adjacent nucleotide. De novo RoseTTA modeling of CMTrs reveals close similarities of the overall structure and near identity for the catalytic tetrad, and for cap and cofactor binding for human, Drosophila and C. elegans CMTrs. Although viral CMTrs maintain the overall structure and catalytic tetrad, they have diverged in cap and cofactor binding. Consistent with the structural similarity, both CMTrs from Drosophila and humans methylate the first cap-adjacent nucleotide of an AGU consensus start. Because the second nucleotide is also methylated upon heat stress in Drosophila, these findings argue for regulated cOMe important for gene expression regulation.

Funder

Leverhulme Trust and the Biotechnology and Biological Sciences Research Council

BBSRC

Wellcome Trust

Publisher

Cold Spring Harbor Laboratory

Subject

Molecular Biology

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