Abstract
Scorpion envenomation is a leading cause of morbidity and mortality among accidents caused by venomous animals. Major clinical manifestations that precede death after scorpion envenomation include heart failure and pulmonary edema. Here, we demonstrate that cardiac dysfunction and fatal outcomes caused by lethal scorpion envenomation in mice are mediated by a neuro-immune interaction linking IL-1 receptor signaling, prostaglandin E2, and acetylcholine release. IL-1R deficiency, the treatment with a high dose of dexamethasone or blockage of parasympathetic signaling using atropine or vagotomy, abolished heart failure and mortality of envenomed mice. Therefore, we propose the use of dexamethasone administration very early after envenomation, even before antiserum, to inhibit the production of inflammatory mediators and acetylcholine release, and to reduce the risk of death.
Publication types
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Research Support, Non-U.S. Gov't
MeSH terms
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Acetylcholine / metabolism*
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Animals
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Antivenins / administration & dosage
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Atropine / pharmacology
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Dexamethasone / administration & dosage
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Dinoprostone / biosynthesis*
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Disease Models, Animal
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Heart Failure / drug therapy
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Heart Failure / etiology*
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Heart Failure / physiopathology
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Humans
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Inflammation Mediators / metabolism
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Male
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Mice
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Mice, Inbred C57BL
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Mice, Knockout
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Models, Cardiovascular
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Neuroimmunomodulation / drug effects
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Receptors, Interleukin-1 Type I / deficiency
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Receptors, Interleukin-1 Type I / genetics
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Receptors, Interleukin-1 Type I / metabolism*
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Scorpion Stings / complications
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Scorpion Venoms / toxicity*
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Scorpions
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Signal Transduction
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Vagotomy
Substances
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Antivenins
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IL1R1 protein, mouse
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Inflammation Mediators
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Receptors, Interleukin-1 Type I
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Scorpion Venoms
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Atropine
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Dexamethasone
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Dinoprostone
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Acetylcholine