Effect of calcineurin inhibitors on myotoxic activity of crotoxin and Bothrops asper phospholipase A2 myotoxins in vivo and in vitro

Miyabara, Elen Haruka; Baptista, Igor L.; Lomonte, Bruno; Selistre-de-Araújo, Heloísa Sobreiro; Gutiérrez, José Marı́a; Moriscot, Anselmo Sigari

doi:10.1016/j.cbpc.2006.03.002

Cited by 7 publications

(6 citation statements)

References 56 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Receptors for myotoxins isolated from the venom of Oxyuranus scutellatus have been identified [15,16] and it has been suggested that the receptor of the Lys49 myotoxin is the VEGF (vascular endothelial growth factor) receptor itself [17,18]. The presence of specific plasma membrane receptors is also supported by the selectivity of some myotoxins for type I muscle fibers [19,20]. The finding that various snake myotoxins are more toxic to differentiated myotubes than to undifferentiated myoblasts [21,22] may indeed suggest the presence of specific toxin receptors in the differentiated, but not in the undifferentiated, cells.…”

Section: Introductionmentioning

confidence: 83%

Calcium imaging of muscle cells treated with snake myotoxins reveals toxin synergism and presence of acceptors

Cintra-Francischinelli

Pizzo

Rodrigues‐Simioni

et al. 2009

Cell. Mol. Life Sci.

Self Cite

View full text Add to dashboard Cite

Snake myotoxins have a great impact on human health worldwide. Most of them adopt a phospholipase A2 fold and occur in two forms which often co-exist in the same venom: the Asp49 toxins hydrolyse phospholipids, whilst Lys49 toxins are enzymatically inactive. To gain insights into their mechanism of action, muscle cells were exposed to Bothrops myotoxins, and cytosolic Ca(2+) and cytotoxicity were measured. In both myoblasts and myotubes, the myotoxins induced a rapid and transient rise in cytosolic [Ca(2+)], derived from intracellular stores, followed, only in myotubes, by a large Ca(2+) influx and extensive cell death. Myoblast viability was unaffected. Notably, in myotubes Asp49 and Lys49 myotoxins acted synergistically to increase the plasma membrane Ca(2+) permeability, inducing cell death. Therefore, these myotoxins may bind to acceptor(s) coupled to intracellular Ca(2+) mobilization in both myoblasts and myotubes. However, in myotubes only, the toxins alter plasma membrane permeability, leading to death.

show abstract

Section: Introductionmentioning

confidence: 83%

Calcium imaging of muscle cells treated with snake myotoxins reveals toxin synergism and presence of acceptors

Cintra-Francischinelli

Pizzo

Rodrigues‐Simioni

et al. 2009

Cell. Mol. Life Sci.

Self Cite

View full text Add to dashboard Cite

show abstract

“…Moreover, BaV myotoxins are able to affect types I, IIA and IIB muscle fibers, whereas crotoxin is more selective towards oxidative types I and IIA fibers [36]; since tibialis anterior muscle is predominantly constituted by type II fibers [59] such difference might have implications in the mtDNA release. Differences in the mechanism of action of crotoxin and BaV myotoxins were shown by their different myotoxic response to the pretreatment of animals with calcineurin [60], an observation that might be related to the variable specificity towards different muscle fiber types.…”

Section: Discussionmentioning

confidence: 99%

Envenomations by Bothrops and Crotalus Snakes Induce the Release of Mitochondrial Alarmins

et al. 2012

View full text Add to dashboard Cite

Skeletal muscle necrosis is a common manifestation of viperid snakebite envenomations. Venoms from snakes of the genus Bothrops, such as that of B. asper, induce muscle tissue damage at the site of venom injection, provoking severe local pathology which often results in permanent sequelae. In contrast, the venom of the South American rattlesnake Crotalus durissus terrificus, induces a clinical picture of systemic myotoxicity, i.e., rhabdomyolysis, together with neurotoxicity. It is known that molecules released from damaged muscle might act as ‘danger’ signals. These are known as ‘alarmins’, and contribute to the inflammatory reaction by activating the innate immune system. Here we show that the venoms of B. asper and C. d. terrificus release the mitochondrial markers mtDNA (from the matrix) and cytochrome c (Cyt c) from the intermembrane space, from ex vivo mouse tibialis anterior muscles. Cyt c was released to a similar extent by the two venoms whereas B. asper venom induced the release of higher amounts of mtDNA, thus reflecting hitherto some differences in their pathological action on muscle mitochondria. At variance, injection of these venoms in mice resulted in a different time-course of mtDNA release, with B. asper venom inducing an early onset increment in plasma levels and C. d. terrificus venom provoking a delayed release. We suggest that the release of mitochondrial ‘alarmins’ might contribute to the local and systemic inflammatory events characteristic of snakebite envenomations.

show abstract

“…c) An important consequence in muscles is that the damaged mitochondria release cell death mediators through the opening of the permeability transition pore [114]. This is suggested by the ability of cyclosporin A to abrogate myotoxicity induced by crotoxin [38] because cyclosporin A inhibits the opening of the permeability transition pore. If Ca 2+ -induced mitochondrial alterations and loss of function are relatively simple to detect in vivo, this may not be the case for other less-prominent intracellular organelles.…”

Section: Membrane Damagementioning

confidence: 97%

“…The binding of notexin to muscle cell plasma membrane has been documented by immunoelectron microscopy [37]. Furthermore, the ability of cyclosporin A, an inhibitor of calcineurin, to suppress the myotoxic action of crotoxin can be interpreted on the basis of the calcineurininduced shift of muscle fiber type to crotoxinsusceptible type I, slow oxidative fibers [38]. However, the identity of receptors remains elusive.…”

Section: Cell Bindingmentioning

confidence: 98%

Cellular pathology induced by snake venom phospholipase A2 myotoxins and neurotoxins: common aspects of their mechanisms of action

Montecucco

Gutiérrez

Lomonte

2008

Cell. Mol. Life Sci.

Self Cite

250

148

View full text Add to dashboard Cite

A large variety of snake toxins evolved from PLA(2) digestive enzymes through a process of 'accelerated evolution'. These toxins have different tissue targets, membrane receptors and mechanisms of alteration of the cell plasma membrane. Two of the most commonly induced effects by venom PLA(2)s are neurotoxicity and myotoxicity. Here, we will discuss how these snake toxins achieve a similar cellular lesion, which is evolutionarily highly conserved, despite the differences listed above. They cause an initial plasma membrane perturbation which promotes a large increase of the cytosolic Ca(2+) concentration leading to cell degeneration, following modes that we discuss in detail for muscle cells and for the neuromuscular junction. The different systemic pathophysiological consequences caused by these toxins are not due to different mechanisms of cell toxicity, but to the intrinsic anatomical and physiological properties of the targeted tissues and cells.

show abstract

Effect of calcineurin inhibitors on myotoxic activity of crotoxin and Bothrops asper phospholipase A2 myotoxins in vivo and in vitro

Cited by 7 publications

References 56 publications

Calcium imaging of muscle cells treated with snake myotoxins reveals toxin synergism and presence of acceptors

Calcium imaging of muscle cells treated with snake myotoxins reveals toxin synergism and presence of acceptors

Envenomations by Bothrops and Crotalus Snakes Induce the Release of Mitochondrial Alarmins

Cellular pathology induced by snake venom phospholipase A2 myotoxins and neurotoxins: common aspects of their mechanisms of action

Contact Info

Product

Resources

About