The evolution of snake venoms resulted in multigene toxin families that code for structurally similar isoforms eventually harboring distinct functions. PLAs are dominant toxins in viper venoms, and little is known about the impact of their diversity on human envenomings and neutralization by antivenoms. Here, we show the isolation of three distinct PLAs from venom. FA1 is a Lys-49 homologue, and FA3 and FA4 are catalytic Asp-49 PLAs. FA1 and FA3 are basic myotoxic proteins, while FA4 is an acid non-myotoxic PLA. FA3 was the most potent toxin, inducing higher levels of edema, inflammatory nociception, indirect hemolysis, and anticoagulant activity on human, rat, and chicken plasmas. FA4 presented lower anticoagulant activity, and FA1 had only a slight effect on human and rat plasmas. PLAs presented differential reactivities with antivenoms, with an emphasis on FA3, which was not recognized or neutralized by the antivenoms used in this study. Our findings reveal the functional and antigenic diversity among PLAs from venom, highlighting the importance of assessing venom variability for understanding human envenomations and treatment with antivenoms, particularly evident here as the antivenom fails to recognize FA3, the most active multifunctional toxin described.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9414272PMC
http://dx.doi.org/10.3390/toxins14080543DOI Listing

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