Evolution and dosage compensation of nucleolar organizing regions (NORs) mediated by mobile elements in turtles with female (ZZ/ZW) but not with male (XX/XY) heterogamety

Eugenia E Montiel; Daleen Badenhorst; LingSze Lee; Nicole Valenzuela

doi:10.1111/jeb.14064

Evolution and dosage compensation of nucleolar organizing regions (NORs) mediated by mobile elements in turtles with female (ZZ/ZW) but not with male (XX/XY) heterogamety

J Evol Biol. 2022 Dec;35(12):1709-1720. doi: 10.1111/jeb.14064. Epub 2022 Jul 25.

Authors

Eugenia E Montiel^{1

2}, Daleen Badenhorst¹, LingSze Lee¹, Nicole Valenzuela¹

Affiliations

¹ Department of Ecology, Evolution, and Organismal Biology, Iowa State University, Ames, Iowa, USA.
² Department of Experimental Biology (Genetics Area), University of Jaén, Jaén, Spain.

Abstract

Understanding the evolution and regulation of nucleolar organizing regions (NORs) is important to elucidate genome structure and function. This is because ribosomal gene (rDNA) copy number and activity mediate protein biosynthesis, stress response, ageing, disease, dosage compensation and genome stability. Here, we found contrasting dosage compensation of sex-linked NORs in turtles with male and female heterogamety. Most taxa examined exhibit homomorphic rRNA gene clusters in a single autosome pair (determined by 28S rDNA fluorescence in situ hybridization), whereas NORs are sex-linked in Apalone spinifera, Pelodiscus sinensis and Staurotypus triporcatus. Full-dosage compensation upregulates the male X-NOR (determined via silver staining-AgNOR) in Staurotypus (who lacks Y-NOR) compared with female X-AgNORs. In softshell Apalone and Pelodiscus, who share homologous ZZ/ZW micro-chromosomes, their enlarged W-NOR is partially active (due to 28S rDNA invasion by R2 retroelements), whereas their smaller Z-NOR is silent in females but active in both male-Zs (presumably because the W-NOR meets cellular demands and excessive NOR activity is costly). We hypothesize that R2 disruption favoured W enlargement to add intact 28S-units, perhaps facilitated by reduced recombination during sex chromosome evolution. The molecular basis of the potentially adaptive female Z-silencing is likely intricate and perhaps epigenetic, as non-ribosomal Z genes are active in Apalone females. Yet, Emydura maquarii exhibit identical heteromorphism in their autosomal NOR (R2 invaded 28S-units and the small-autosome NOR is silent), suggesting that the softshell turtle pattern can evolve independent of sex chromosome evolution. Our study illuminates the complex sex chromosome evolution and dosage compensation of non-model systems that challenges classic paradigms.

Keywords: 18S/28S repetitive DNA; R2 retrotransposon retroelement transposable element; adaptive evolution of sex chromosome dosage compensation; gene regulation silencing; nucleolar organizing region; ribosomal RNA genes (rRNA, rDNA); silver-staining AgNOR; temperature-dependent (TSD) and ZZ/ZW XX/XY genotypic sex determination (GSD); turtle reptile vertebrates.

Publication types

Research Support, U.S. Gov't, Non-P.H.S.
Research Support, Non-U.S. Gov't

MeSH terms

Animals
DNA, Ribosomal
Dosage Compensation, Genetic
Evolution, Molecular
Female
In Situ Hybridization, Fluorescence
Male
Sex Chromosomes / genetics
Turtles* / genetics

Substances

DNA, Ribosomal