| Literature DB >> 33887183 |
Shabnam Mohammadi1, Lu Yang2, Arbel Harpak3, Santiago Herrera-Álvarez4, María Del Pilar Rodríguez-Ordoñez4, Julie Peng5, Karen Zhang2, Jay F Storz1, Susanne Dobler6, Andrew J Crawford7, Peter Andolfatto8.
Abstract
Although gene duplication is an important source of evolutionary innovation, the functional divergence of duplicates can be opposed by ongoing gene conversion between them. Here, we report on the evolution of a tandem duplication of Na+,K+-ATPase subunit α1 (ATP1A1) shared by frogs in the genus Leptodactylus, a group of species that feeds on toxic toads. One ATP1A1 paralog evolved resistance to toad toxins although the other retained ancestral susceptibility. Within species, frequent non-allelic gene conversion homogenized most of the sequence between the two copies but was counteracted by strong selection on 12 amino acid substitutions that distinguish the two paralogs. Protein-engineering experiments show that two of these substitutions substantially increase toxin resistance, whereas the additional 10 mitigate their deleterious effects on ATPase activity. Our results reveal how examination of neo-functionalized gene duplicate evolution can help pinpoint key functional substitutions and interactions with the genetic backgrounds on which they arise.Entities:
Keywords: ATP-alpha subunit; cardiotonic steroids; epistasis; gene duplication; molecular evolution; natural selection; neofunctionalization; non-allelic gene conversion; potassium ATPase; sodium; toxin resistance
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Year: 2021 PMID: 33887183 PMCID: PMC8281379 DOI: 10.1016/j.cub.2021.03.089
Source DB: PubMed Journal: Curr Biol ISSN: 0960-9822 Impact factor: 10.900