Abstract

The high medical importance of Crotalus snakes is unquestionable, as this genus is the second in frequency of ophidian accidents in many countries, including Brazil. With a relative less complex composition compared to other genera venoms, as those from the Bothrops genus, the Crotalus genus venom from South America is composed basically by the neurotoxin crotoxin (a phospholipase A2), the thrombin-like gyroxin (a serinoprotease), a very potent aggregating protein convulxin, and a myotoxic polypeptide named crotamine. Interestingly not all Crotalus snakes express crotamine, which was first described in early 50s due to its ability to immobilize animal hind limbs, contributing therefore to the physical immobilization of preys and representing an important advantage for the envenoming efficacy, and consequently, for the feeding and survival of these snakes in nature. Representing about 10–25% of the dry weight of the crude venom of crotamine-positive rattlesnakes, the polypeptide crotamine is also suggested to be of importance for antivenom therapy, although the contribution of this toxin to the main symptoms of envenoming process remains far unknown until now. Herein, we concomitantly performed in vitro and in vivo assays to show for the first time the dose-dependent response of crotamine-triggered hind limbs paralysis syndrome, up to now believed to be observable only at high (sub-lethal) concentrations of crotamine. In addition, ex vivo assay performed with isolated skeletal muscles allowed us to suggest here that compounds active on voltage-sensitive sodium and/or potassium ion channels could both affect the positive inotropic effect elicited by crotamine in isolated diaphragm, besides also affecting the hind limbs paralysis syndrome imposed by crotamine in vivo. By identifying the potential molecular targets of this toxin, our data may contribute to open new roads for translational studies aiming to improve the snakebite envenoming treatment in human. Interestingly, we also demonstrate that the intraplantal or intraperitoneal (ip) injections of crotamine in mice do not promote pain. Therefore, this work may also suggest the profitable utility of non-toxic analogs of crotamine as a potential tool for targeting voltage-gated ion channels in skeletal muscles, aiming its potential use in the therapy of neuromuscular dysfunctions and envenoming therapy.

Highlights

  • Ophidian accident by Crotalus genus is mainly characterized by the myasthenic face with eventual paralysis of ocular muscles, and few reports of respiratory difficulties

  • We report that compounds active on voltage-sensitive sodium and/or potassium ion channels can affect the positive inotropic effect elicited by crotamine in vitro in isolated diaphragm and in the hind limbs paralysis syndrome triggered by crotamine in vivo

  • Nociceptive threshold evaluation demonstrated that crotamine does not trigger pain, and we suggest crotamine as a potential tool for targeting voltage-gated ion channels present in skeletal muscles, with potential to be used as a lead compound to develop drugs for neuromuscular dysfunctions therapy

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Summary

Introduction

Ophidian accident by Crotalus genus is mainly characterized by the myasthenic face with eventual paralysis of ocular muscles, and few reports of respiratory difficulties. The main known components of South American Crotalus genus venom are the neurotoxin phospholipase A2 (namely crotoxin), the thrombin-like serinoprotease (namely gyroxin), a very potent aggregating protein (namely convulxin), and a small myotoxic polypeptide (namely crotamine). Crotalus venom is relatively less complex compared to other snake genus venoms as those from Bothrops [1]. Most of the described myotoxic effects is believed to be determined by the phospholipase A2 crotoxin (the most abundant toxin), while the contribution of crotamine (the second more abundant toxin in the venom of crotamine-positive rattlesnakes) and other toxins present in the Crotalus venom seems to be marginal to the main symptoms of envenoming, and still remains little explored [1]. The presence of crotamine in the venom is considered of high importance for antivenom vaccine production [1], and for pharmacotherapeutic interventions

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