Expansion and Neofunctionalization of Actinoporin-like Genes in Mediterranean Mussel (Mytilus galloprovincialis)

Author:

Koritnik Neža1,Gerdol Marco2,Šolinc Gašper1,Švigelj Tomaž1,Caserman Simon1,Merzel Franci3,Holden Ellie45,Benesch Justin L P45,Trenti Francesco6,Guella Graziano6,Pallavicini Alberto27ORCID,Modica Maria Vittoria8,Podobnik Marjetka1,Anderluh Gregor1ORCID

Affiliation:

1. Department of Molecular Biology and Nanobiotechnology, National Institute of Chemistry , Ljubljana , Slovenia

2. Department of Life Sciences, University of Trieste , Trieste , Italy

3. Theory Department, National Institute of Chemistry , Ljubljana , Slovenia

4. Department of Chemistry, Oxford University , Oxford , UK

5. Kavli Institute for Nanoscience Discovery, University of Oxford , Oxford , UK

6. Bioorganic Chemistry Lab, Department of Physics, University of Trento , Via Sommarive 14, 38123 Povo , Italy

7. Division of Oceanography, National Institute of Oceanography and Applied Geophysics , Trieste , Italy

8. Department of Biology and Evolution of Marine Organisms, Stazione Zoologica Anton Dohrn , Napoli , Italy

Abstract

Abstract Pore-forming toxins are an important component of the venom of many animals. Actinoporins are potent cytolysins that were first detected in the venom of sea anemones; however, they are occasionally found in animals other than cnidarians and are expanded in a few predatory gastropods. Here, we report the presence of 27 unique actinoporin-like genes with monophyletic origin in Mytilus galloprovincialis, which we have termed mytiporins. These mytiporins exhibited a remarkable level of molecular diversity and gene presence–absence variation, which warranted further studies aimed at elucidating their functional role. We structurally and functionally characterized mytiporin-1 and found significant differences from the archetypal actinoporin fragaceatoxin C. Mytiporin-1 showed weaker permeabilization activity, no specificity towards sphingomyelin, and weak activity in model lipid systems with negatively charged lipids. In contrast to fragaceatoxin C, which forms octameric pores, functional mytiporin-1 pores on negatively charged lipid membranes were hexameric. Similar hexameric pores were observed for coluporin-26 from Cumia reticulata and a conoporin from Conus andremenezi. This indicates that also other molluscan actinoporin-like proteins differ from fragaceatoxin C. Although the functional role of mytiporins in the context of molluscan physiology remains to be elucidated, the lineage-specific gene family expansion event that characterizes mytiporins indicates that strong selective forces acted on their molecular diversification. Given the tissue distribution of mytiporins, this process may have broadened the taxonomic breadth of their biological targets, which would have important implications for digestive processes or mucosal immunity.

Publisher

Oxford University Press (OUP)

Subject

Genetics,Ecology, Evolution, Behavior and Systematics

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