Gene fragmentation and RNA editing without borders: eccentric mitochondrial genomes of diplonemids

Author:

Kaur Binnypreet12ORCID,Záhonová Kristína13ORCID,Valach Matus4ORCID,Faktorová Drahomíra12ORCID,Prokopchuk Galina1ORCID,Burger Gertraud4ORCID,Lukeš Julius12ORCID

Affiliation:

1. Institute of Parasitology, Biology Centre, Czech Academy of Sciences, 37005 České Budějovice (Budweis), Czech Republic

2. Faculty of Sciences, University of South Bohemia, 37005 České Budějovice (Budweis), Czech Republic

3. Faculty of Science, Charles University, BIOCEV, 25250 Vestec, Czech Republic

4. Department of Biochemistry and Robert-Cedergren Centre for Bioinformatics and Genomics, Université de Montréal, H3T 1J4 Montreal, Canada

Abstract

AbstractDiplonemids are highly abundant heterotrophic marine protists. Previous studies showed that their strikingly bloated mitochondrial genome is unique because of systematic gene fragmentation and manifold RNA editing. Here we report a comparative study of mitochondrial genome architecture, gene structure and RNA editing of six recently isolated, phylogenetically diverse diplonemid species. Mitochondrial gene fragmentation and modes of RNA editing, which include cytidine-to-uridine (C-to-U) and adenosine-to-inosine (A-to-I) substitutions and 3′ uridine additions (U-appendage), are conserved across diplonemids. Yet as we show here, all these features have been pushed to their extremes in the Hemistasiidae lineage. For example, Namystynia karyoxenos has its genes fragmented into more than twice as many modules than other diplonemids, with modules as short as four nucleotides. Furthermore, we detected in this group multiple A-appendage and guanosine-to-adenosine (G-to-A) substitution editing events not observed before in diplonemids and found very rarely elsewhere. With >1,000 sites, C-to-U and A-to-I editing in Namystynia is nearly 10 times more frequent than in other diplonemids. The editing density of 12% in coding regions makes Namystynia’s the most extensively edited transcriptome described so far. Diplonemid mitochondrial genome architecture, gene structure and post-transcriptional processes display such high complexity that they challenge all other currently known systems.

Funder

ERC

Czech Ministry of Education

Gordon and Betty Moore Foundation

Natural Sciences and Engineering Research Council of Canada

University of South Bohemia

Publisher

Oxford University Press (OUP)

Subject

Genetics

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