低浓度的肝素可作为抗蛇毒血清,对抗鼠血蛇毒和鼠血蛇毒- 1的神经毒性和肌毒性作用。

Journal of Venom Research Pub Date : 2010-10-15
Sandro Rostelato-Ferreira, Gildo Bernardo Leite, Adélia Cristina Oliveira Cintra, Maria Alice da Cruz-Höfling, Léa Rodrigues-Simioni, Yoko Oshima-Franco
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引用次数: 0

摘要

肝素已被证明可以对抗蛇毒毒液的肌毒作用。在体外神经-肌肉制剂和小鼠腓肠肌中,研究了极低肝素浓度(LHC)拮抗黄颡鱼毒液及其磷脂酶a(2)肌毒素(BthTX-I)的神经毒性/肌毒性作用的能力。用商用抗蛇毒血清(CBA)进行归一化检测。LHC (1IU/ml)对神经肌肉麻痹的影响分别降低了4倍和4.5倍(CBA为2.8倍和2.5倍),对纤维损伤的影响分别降低了5.4倍和4.4倍(CBA为2.5倍和13.3倍),对jararacussu和BthTX-I诱导的CK活性分别降低了6倍和1.7倍(CBA为30倍和1.6倍)。在LHC+毒液孵育15min后加入硫酸鱼精蛋白,避免了LHC对毒液神经毒性的中和作用。这有力地证明,鉴于鱼精蛋白的多阳离子性质,它可能与多阴离子肝素络合,使其无法与毒液的基本成分结合,从而降低毒性。由于肝素对毒液的拮抗作用通常比肌毒素更强,我们讨论了bthtx - 1以外的其他毒液成分可能是多阴离子肝素促进拮抗作用的靶点。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Heparin at low concentration acts as antivenom against Bothrops jararacussu venom and bothropstoxin-I neurotoxic and myotoxic actions.

Heparin has been shown to antagonize myotoxic effects of crotaline venoms. Here a very low heparin concentration (LHC) was examined in its ability to antagonize the neurotoxic/myotoxic effects of Bothrops jararacussu venom and its phospholipase A(2) myotoxin, bothropstoxin-I (BthTX-I), in an in vitroz nerve-muscle preparation and in mice gastrocnemius. Normalization of results was done by assays with commercial antibothropic antivenom (CBA). LHC (1IU/ml) added to the incubation bath reduced by 4- and 4.5-fold (vs 2.8- and 2.5-fold by CBA) the neuromuscular paralysis, by 5.4 and 4.4-fold (vs 2.5- and 13.3-fold by CBA) the percentage of fibers damaged and by 6- and 1.7-fold (vs 30- and 1.6-fold by CBA) the CK activity induced by B. jararacussu and BthTX-I, respectively. Protamine sulphate added 15min after the incubation of the preparation with LHC+venom, avoided the LHC neutralizing effect against venom neurotoxicity. This strongly attests that given the polycationic nature of protamine, it probably complexed with the polyanionic heparin making it unattainable for binding to basic components of venom, reducing toxicity. Since heparin antagonism is generally stronger against venom effects than is myotoxin we discuss that other venom components than the BthTX-I are likely target for the antagonism promoted by the polyanionic heparin.

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