Origin and functional diversification of an amphian defense peptide arsenal

Roelants, Kim; Fry, Bryan; Ye, Lumeng; Stijlemans, Benoit; Brys, Lea; Kok, Philippe; Clynen, Elke; Schoofs, Liliane; Cornelis, Pierre; Bossuyt, Franky

doi:10.1371/journal.pgen.1003662

Origin and functional diversification of an amphian defense peptide arsenal

Author:

Roelants, Kim

Fry, Bryan ; Ye, Lumeng ; Stijlemans, Benoit ; Brys, Lea ; Kok, Philippe ; Clynen, Elke ; Schoofs, Liliane ; Cornelis, Pierre ; Bossuyt, Franky

Keywords:

Science & Technology, Life Sciences & Biomedicine, Genetics & Heredity, XENOPUS-MUELLERI PIPIDAE, ANTIMICROBIAL PEPTIDES, SKIN SECRETIONS, CLAWED FROGS, TRANSCRIPTIONAL REGULATION, SILURANA-EPITROPICALIS, ADAPTIVE EVOLUTION, CDNA SEQUENCE, PICKEREL FROG, NEUROMEDIN-N, Amino Acid Sequence, Animals, Antimicrobial Cationic Peptides, Anura, Evolution, Molecular, Gene Expression Profiling, Genetic Variation, Genome, Peptides, Phylogeny, Sequence Alignment, Skin, BATRACHOCHYTRIUM-DENDROBATIDIS, RANA-PALUSTRIS, 0604 Genetics, Developmental Biology, 3105 Genetics

Abstract:

The skin secretion of many amphibians contains an arsenal of bioactive molecules, including hormone-like peptides (HLPs) acting as defense toxins against predators, and antimicrobial peptides (AMPs) providing protection against infectious microorganisms. Several amphibian taxa seem to have independently acquired the genes to produce skin-secreted peptide arsenals, but it remains unknown how these originated from a non-defensive ancestral gene and evolved diverse defense functions against predators and pathogens. We conducted transcriptome, genome, peptidome and phylogenetic analyses to chart the full gene repertoire underlying the defense peptide arsenal of the frog Silurana tropicalis and reconstruct its evolutionary history. Our study uncovers a cluster of 13 transcriptionally active genes, together encoding up to 19 peptides, including diverse HLP homologues and AMPs. This gene cluster arose from a duplicated gastrointestinal hormone gene that attained a HLP-like defense function after major remodeling of its promoter region. Instead, new defense functions, including antimicrobial activity, arose by mutation of the precursor proteins, resulting in the proteolytic processing of secondary peptides alongside the original ones. Although gene duplication did not trigger functional innovation, it may have subsequently facilitated the convergent loss of the original function in multiple gene lineages (subfunctionalization), completing their transformation from HLP gene to AMP gene. The processing of multiple peptides from a single precursor entails a mechanism through which peptide-encoding genes may establish new functions without the need for gene duplication to avoid adaptive conflicts with older ones.