Mitoribosome structure with cofactors and modifications reveals mechanism of ligand binding and interactions with L1 stalk

Author:

Singh VivekORCID,Itoh YuzuruORCID,Del’Olio Samuel,Hassan AsemORCID,Naschberger Andreas,Flygaard Rasmus Kock,Nobe YukoORCID,Izumikawa Keiichi,Aibara ShintaroORCID,Andréll JuniORCID,Whitford Paul C.ORCID,Barrientos AntoniORCID,Taoka MasatoORCID,Amunts AlexeyORCID

Abstract

AbstractThe mitoribosome translates mitochondrial mRNAs and regulates energy conversion that is a signature of aerobic life forms. We present a 2.2 Å resolution structure of human mitoribosome together with validated mitoribosomal RNA (rRNA) modifications, including aminoacylated CP-tRNAVal. The structure shows how mitoribosomal proteins stabilise binding of mRNA and tRNA helping to align it in the decoding center, whereas the GDP-bound mS29 stabilizes intersubunit communication. Comparison between different states, with respect to tRNA position, allowed us to characterize a non-canonical L1 stalk, and molecular dynamics simulations revealed how it facilitates tRNA transitions in a way that does not require interactions with rRNA. We also report functionally important polyamines that are depleted when cells are subjected to an antibiotic treatment. The structural, biochemical, and computational data illuminate the principal functional components of the translation mechanism in mitochondria and provide a description of the structure and function of the human mitoribosome.

Funder

Stiftelsen för Strategisk Forskning

Ragnar Söderbergs stiftelse

Knut och Alice Wallenbergs Stiftelse

EC | Horizon 2020 Framework Programme

MEXT | Japan Science and Technology Agency

DH | NIHR | Health Services Research Programme

United States Department of Defense | Missile Defense Agency

Publisher

Springer Science and Business Media LLC

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