Does rapid sequence divergence preclude RNA structure conservation in vertebrates?

Author:

Seemann Stefan E12ORCID,Mirza Aashiq H13,Bang-Berthelsen Claus H14,Garde Christian1,Christensen-Dalsgaard Mikkel1,Workman Christopher T15ORCID,Pociot Flemming13,Tommerup Niels16,Gorodkin Jan12ORCID,Ruzzo Walter L178ORCID

Affiliation:

1. Center for non-coding RNA in Technology and Health (RTH), University of Copenhagen, Denmark

2. Department of Veterinary and Animal Sciences, University of Copenhagen, Denmark

3. Steno Diabetes Center Copenhagen, Gentofte, Denmark

4. National Food Institute, Technical University of Denmark, Kgs. Lyngby, Denmark

5. Center for Biological Sequence Analysis, Technical University of Denmark, Denmark

6. Department of Cellular and Molecular Medicine (ICMM), University of Copenhagen, Denmark

7. Computer Science and Engineering and Genome Sciences, University of Washington, USA

8. Fred Hutchinson Cancer Research Center, Seattle, USA

Abstract

Abstract Accelerated evolution of any portion of the genome is of significant interest, potentially signaling positive selection of phenotypic traits and adaptation. Accelerated evolution remains understudied for structured RNAs, despite the fact that an RNA’s structure is often key to its function. RNA structures are typically characterized by compensatory (structure-preserving) basepair changes that are unexpected given the underlying sequence variation, i.e., they have evolved through negative selection on structure. We address the question of how fast the primary sequence of an RNA can change through evolution while conserving its structure. Specifically, we consider predicted and known structures in vertebrate genomes. After careful control of false discovery rates, we obtain 13 de novo structures (and three known Rfam structures) that we predict to have rapidly evolving sequences—defined as structures where the primary sequences of human and mouse have diverged at least twice as fast (1.5 times for Rfam) as nearby neutrally evolving sequences. Two of the three known structures function in translation inhibition related to infection and immune response. We conclude that rapid sequence divergence does not preclude RNA structure conservation in vertebrates, although these events are relatively rare.

Funder

Innovation Fund Denmark

University of Copenhagen

Publisher

Oxford University Press (OUP)

Subject

Genetics

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