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Diversity and Molecular Evolution of Antimicrobial Peptides in Caecilian Amphibians

Citation

Benítez-Prián, M.; Lorente-Martínez, H.; Agorreta, A.; Gower, D.J.; Wilkinson, M.; Roelants, K.; San Mauro, D. Diversity and Molecular Evolution of Antimicrobial Peptides in Caecilian Amphibians. Toxins 2024, 16, 150. https://doi.org/10.3390/toxins16030150

Abstract

Antimicrobial peptides (AMPs) are key molecules in the innate immune defence of vertebrates with rapid action, broad antimicrobial spectrum, and ability to evade pathogen resistance mechanisms. To date, amphibians are the major group of vertebrates from which most AMPs have been characterised, but most studies have focused on the bioactive skin secretions of anurans (frogs and toads). In this study, we have analysed the complete genomes and/or transcriptomes of eight species of caecilian amphibians (order Gymnophiona) and characterised the diversity, molecular evolution, and antimicrobial potential of the AMP repertoire of this order of amphibians. We have identified 477 candidate AMPs within the studied caecilian genome and transcriptome datasets. These candidates are grouped into 29 AMP families, with four corresponding to peptides primarily exhibiting antimicrobial activity and 25 potentially serving as AMPs in a secondary function, either in their entirety or after cleavage. In silico prediction methods were used to identify 62 of those AMPs as peptides with promising antimicrobial activity potential. Signatures of directional selection were detected for five candidate AMPs, which may indicate adaptation to the different selective pressures imposed by evolutionary arms races with specific pathogens. These findings provide encouraging support for the expectation that caecilians, being one of the least-studied groups of vertebrates, and with ~300 million years of separate evolution, are an underexplored resource of great pharmaceutical potential that could help to contest antibiotic resistance and contribute to biomedical advance.

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Funding This research received no direct external funding. M.B.-P. was sponsored by a predoctoral contract of the Complutense University of Madrid. H.L-M. was sponsored by a predoctoral contract of the Complutense University of Madrid in partnership with the Real Colegio Complutense at Harvard University (RCC-UCM) Acknowledgments We thank Bin Lu for the selfless provision of transcriptomic data for Ichthyophis kohtaoensis. Six anonymous reviewers provided insightful comments on an earlier version of the manuscript. Support was provided by the Spanish network of research laboratories working on adaptation genomics (AdaptNET).

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