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The relationship between clinics and the venom of the causative Amazon pit viper (Bothrops atrox)

机译:诊所与致病亚马逊坑毒蛇(Bothrops Atrox)之间的关系

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摘要

Snake venoms are complex mixtures of proteins with toxic activities, with many distinct isoforms, affecting different physiological targets, comprised in a few protein families. It is currently accepted that this diversity in venom composition is an adaptive advantage for venom efficacy on a wide range of prey. However, on the other side, variability on isoforms expression has implications in the clinics of human victims of snakebites and in the efficacy of antivenoms. B. atrox snakes are responsible for most of the human accidents in Brazilian Amazon and the type and abundance of protein families on their venoms present individual variability. Thus, in this study we attempted to correlate the individual venom proteome of the snake brought to the hospital by the patient seeking for medical assistance with the clinical signs observed in the same patient. Individual variability was confirmed in venoms of the 14 snakes selected for the study. The abundance of each protein family was quite similar among the venom samples, while the isoforms composition was highly variable. Considering the protein families, the SVMP group presented the best correlation with bleeding disorders and edema. Considering individual isoforms, some isoforms of venom metalloproteinase (SVMP), C-type lectin-like toxins (CTL) and snake venom serine proteinases (SVSP) presented expression levels that with statistically significant positive correlation to signs and symptoms presented by the patients as bleeding disorders, edema, ecchymosis and blister formation. However, some unexpected data were also observed as the correlation between a CTL, CRISP or LAAO isoforms with blister formation, still to be confirmed with a larger number of samples. Although this is still a small number of patient samples, we were able to indicate that venom composition modulates clinical manifestations of snakebites, to confirm at the bedside the prominent role of SVMPs and to include new possible toxin candidates for the development of toxin inhibitors or to improve antivenom selectiveness, important actions for the next generation treatments of snakebites.
机译:蛇毒液是具有毒性活动的复杂蛋白质混合物,具有许多不同的同种型,影响了几种蛋白质家族的不同生理靶标。目前已接受毒液组成的这种多样性是毒液效力对各种猎物的适应性优势。然而,在另一方面,同种型表达的可变性在蛇咬的人类受害者和抗静电子的疗效中具有影响。 B. Atrox Snakes负责巴西亚马逊的大部分人类事故以及毒液上的蛋白质家庭的类型和丰度目的是个性变异性。因此,在这项研究中,我们试图通过寻求在同一患者中观察到的临床症状的患者将蛇的个体毒液蛋白质组相关联。在为研究选择的14个蛇的毒液中证实了个体变异性。在毒液样品中,每种蛋白质家族的丰度非常相似,而同种型组合物是高度可变的。考虑到蛋白质家族,SVMP组呈现出与出血障碍和水肿的最佳相关性。考虑单个同种型,一些异构素(SVMP),C型凝集素样毒素(CTL)和蛇毒丝氨酸丝氨酸(SVSP)的异构体呈现表达水平,其表达水平与患者呈现出血的症状和症状的统计学显着呈阳性相关性病症,水肿,瘀斑和泡罩形成。然而,也观察到一些意外数据作为具有泡罩形成的CTL,清脆或Laao同种型之间的相关性,仍然用更多数量的样品确认。虽然这仍然是少数患者样品,但我们能够表明毒液组合物调节蛇咬的临床表现,以确认SVMP的突出作用,并包括用于开发毒素抑制剂的新可能毒素候选者改善抗静电子选择性,对蛇咬伤的下一代治疗的重要行为。

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