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Toxinology of venoms from five Australian lesser known elapid snakes

机译:五条澳大利亚鲜为人知的蛇形蛇毒液的毒理学

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摘要

Research into Australian elapid venoms has mainly focused on the seven genera of greatest clinical significance: Acanthophis, Hoplocephalus, Notechis, Oxyuranus, Pseudechis, Pseudonaja and Tropidechis. However, even small species represent a potential for causing severe clinical envenoming. Further, owing to taxonomic distinctiveness, these species are a potential source of novel toxins for use in drug design and development. This is the first study to characterize the venoms of Cryptophis boschmai, Denisonia devisi, Echiopsis curta, Hemiaspis signata and Vermicella annulata. MALDI analysis of each venom, over the range of 4–40 kDa, indicated components in the weight range for three finger toxins (6–8 kDa) and phospholipase A₂ (PLA₂; 12–14 kDA). Interestingly, C. boschmai venom was the only venom, which contained components > 25 kDa. All venoms (10 μg/ml) demonstrated in vitro neurotoxicity in the chick biventer cervicis nerve-muscle preparation, with a relative rank order of: H. signata ≥ D. devisi ≥ V. annulata = E. curta > C. boschmai. CSL polyvalent antivenom neutralized the inhibitory effects of C. boschmai venom but only delayed the inhibitory effect of the other venoms. All venoms displayed PLA2 activity but over a wide range (i.e. 1–621 μmol/min./mg). The venoms of C. boschmai (60 μg/kg, i.v.), D. devisi (60 μg/kg, i.v.) and H. signata (60 μg/kg, i.v.) produced hypotensive effects in vivo in an anaesthetized rat preparation. H. signata displayed moderate pro-coagulant activity while the other venoms were weakly pro-coagulant. This study demonstrated that these understudied Australian elapids have varying pharmacological activity, with notable in vitro neurotoxicity for four of the venoms, and may produce mild to moderate effects following systemic envenoming.
机译:对澳大利亚蛇毒的毒液的研究主要集中在具有最大临床意义的七个属上:棘皮动物,蛇脑,Notechis,Oxyuranus,Pseudechis,Pseudonaja和Tropidechis。但是,即使很小的物种也可能导致严重的临床毒害。此外,由于分类学上的独特性,这些物种是用于药物设计和开发的新型毒素的潜在来源。这是第一个表征博氏隐孢子虫,Denisonia devisi,Echiopsis curta,Hemiaspis signata和Vermicella annulata毒液特征的研究。每种毒液的MALDI分析在4–40 kDa范围内,表明三种手指毒素(6–8 kDa)和磷脂酶A 2(PLA 2; 12–14 kDA)的重量范围内的成分。有趣的是,博氏梭菌毒液是唯一的毒液,其成分> 25 kDa。所有毒液(10μg/ ml)在雏鸡颈静脉神经肌肉制剂中均表现出体外神经毒性,其相对等级顺序为:H. signata≥D. devisi≥V. annulata = E. curta> C. boschmai。 CSL多价抗蛇毒中和了博世脉络膜蛇毒的抑制作用,但仅延迟了其他蛇毒的抑制作用。所有毒液均具有PLA2活性,但作用范围很广(即1–621μmol/ min。/ mg)。在麻醉的大鼠制剂中,博世梭菌(60μg/ kg,腹腔注射),D。devisi(60μg/ kg,腹腔注射)和Sign。H. signata(60μg/ kg,腹腔注射)的毒液在体内产生了降压作用。 H. signata表现出中等的促凝活性,而其他毒液则弱促凝。这项研究表明,这些未被充分研究的澳大利亚卵磷脂具有不同的药理活性,对四种毒液具有明显的体外神经毒性,并且在全身性毒液作用后可能产生轻度至中度的作用。

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