Gene Amplification and Functional Diversification of Melanocortin 4 Receptor at an Extremely Polymorphic Locus Controlling Sexual Maturation in the Platyfish

Author:

Volff Jean-Nicolas12,Selz Yvonne2,Hoffmann Carsten3,Froschauer Alexander2,Schultheis Christina12,Schmidt Cornelia2,Zhou Qingchun2,Bernhardt Wolfgang2,Hanel Reinhold2,Böhne Astrid12,Brunet Frédéric1,Ségurens Béatrice4,Couloux Arnaud4,Bernard-Samain Sylvie4,Barbe Valérie4,Ozouf-Costaz Catherine5,Galiana Delphine1,Lohse Martin J3,Schartl Manfred2

Affiliation:

1. Institut de Génomique Fonctionnelle de Lyon, Ecole Normale Supérieure de Lyon-Centre National de la Recherche Scientifique UMR5242-Université Claude Bernard Lyon I, F-69364 Lyon Cedex 07, France

2. Physiologische Chemie I, Biozentrum, University of Würzburg, D-97074 Würzburg, Germany

3. Department of Pharmacology and Toxicology, University of Würzburg, D-97078 Würzburg, Germany

4. Commissariat à l'Energie Atomique/Direction des Sciences du Vivant/Institut de Génomique/Genoscope, F-91057 Evry Cedex, France

5. Centre National de la Recherche Scientifique Unité Mixte de Recherche 7138, Département Systématique et Evolution, Muséum National d’Histoire Naturelle, F-75231 Paris Cedex 5, France

Abstract

Abstract In two swordtail species of the genus Xiphophorus, the onset of puberty has been shown to be modulated at the P locus by sequence polymorphism and gene copy-number variation affecting the type 4 melanocortin hormone receptor Mc4r. The system works through the interaction of two allelic types, one encoding wild type and the other dominant-negative receptors. We have analyzed the structure and evolution of the P locus in the platyfish Xiphophorus maculatus, where as many as nine alleles of P determining the onset of sexual maturity in males and females, fecundity in females, and adult size in males are located on both the X and Y chromosomes in a region linked to the master sex-determining locus. In this species, mc4r has been amplified to up to 10 copies on both the X and Y chromosomes through recent large serial duplications. Subsequently, mc4r paralogues have diverged considerably into many different subtypes. Certain copies have acquired new untranslated regions through genomic rearrangements, and transposable element insertions and other mutations have accumulated in promoter regions, possibly explaining observed deviations from the classical mc4r transcriptional pattern. In the mc4r-coding sequence, in-frame insertions and deletions as well as nonsense and missense mutations have generated a high diversity of Mc4r-predicted proteins. Most of these variants are expressed in embryos, adults, and/or tumors. Functional receptor characterization demonstrated major divergence in pharmacological behavior for Mc4r receptors encoded by different copies of platyfish mc4r, with differences in constitutive activity as well as binding and stimulation by hormones. The high degree of allelic and copy-number variation observed between individuals can explain the high level of polymorphism for sexual maturation, fecundity, and body size in the platyfish: multiple combinations of Mc4r variants with different biochemical properties might interact to modulate the melanocortin signaling that regulates the hypothalamus–pituitary–gonadal axis.

Publisher

Oxford University Press (OUP)

Subject

Genetics

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