Evolution of New Hormone Function: Loss and Gain of a Receptor

doi:10.1093/jhered/esi024

Journal of Heredity Advance Access published online on January 13, 2005
Journal of Heredity, doi:10.1093/jhered/esi024

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Evolution of New Hormone Function: Loss and Gain of a Receptor

D. M. Irwin ¹^* and K. Wong ¹

¹ From the Department of Laboratory Medicine and Pathobiology, Banting and Best Diabetes Centre, University of Toronto, 100 College St., Toronto, Ontario, Canada M5G lL5

^* To whom correspondence should be addressed.
D. M. Irwin, E-mail: david.irwin{at}utoronto.ca

Abstract

The vertebrate proglucagon gene encodes three glucagon-likesequences (glucagon, glucagon-like peptide-1 [GLP-1], and glucagon-likepeptide 2 [GLP-2]) that have distinct functions in regulatingmetabolism in mammals. In contrast, glucagon and GLP-1 havesimilar physiological actions in fish, that of mammalian glucagon.We have identified sequences similar to receptors for proglucagon-derivedpeptides from the genomes of two fish (pufferfish and zebrafish),a frog (Xenopus tropicalis), and a bird (chicken). Phylogeneticanalysis of the receptor sequences suggested an explanationfor the divergent function of GLP-1 in fish and mammals. Thephylogeny of our predicted and characterized receptors for proglucagon-derivedpeptides demonstrate that receptors for glucagon, GLP-1, andGLP-2 have an origin before the divergence of fish and mammals;however, fish have lost the gene encoding the GLP-1 class ofreceptors, and likely the incretin action of GLP-1. Receptorsthat bind GLP-1, but yield glucagon-like action, have been characterizedin goldfish and zebrafish, and these sequences are most closelyrelated to glucagon receptors. Both pufferfish and zebrafishhave a second glucagon receptor-like gene that is most closelyrelated to the characterized goldfish glucagon receptor. Thephylogeny of glucagon receptor-like genes in fish indicatesthat a duplication of the glucagon receptor gene occurred onthe ancestral fish lineage, and could explain the shared actionof glucagon and GLP-1. We suggest that the binding specificityof one of the duplicated glucagon receptors has diverged, yieldingreceptors for GLP-1 and glucagon, but that ancestral downstreamsignaling has been maintained, resulting in both receptors retainingglucagon-stimulated downstream effects.

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Journal of Heredity

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Evolution of New Hormone Function: Loss and Gain of a Receptor