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A Simple and Novel Strategy for the Production of a Pan-specific Antiserum against Elapid Snakes of Asia

机译:一种简单新颖的制备针对亚洲Elapid蛇的泛特异性抗血清的策略

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摘要

Snakebite envenomation is a serious medical problem in many tropical developing countries and was considered by WHO as a neglected tropical disease. Antivenom (AV), the rational and most effective treatment modality, is either unaffordable and/or unavailable in many affected countries. Moreover, each AV is specific to only one (monospecific) or a few (polyspecific) snake venoms. This demands that each country to prepare AV against its local snake venoms, which is often not feasible. Preparation of a ‘pan-specific’ AV against many snakes over a wide geographical area in some countries/regions has not been possible. If a ‘pan-specific’ AV effective against a variety of snakes from many countries could be prepared, it could be produced economically in large volume for use in many countries and save many lives. The aim of this study was to produce a pan-specific antiserum effective against major medically important elapids in Asia. The strategy was to use toxin fractions (TFs) of the venoms in place of crude venoms in order to reduce the number of antigens the horses were exposed to. This enabled inclusion of a greater variety of elapid venoms in the immunogen mix, thus exposing the horse immune system to a diverse repertoire of toxin epitopes, and gave rise to antiserum with wide paraspecificity against elapid venoms. Twelve venom samples from six medically important elapid snakes (4 Naja spp. and 2 Bungarus spp.) were collected from 12 regions/countries in Asia. Nine of these 12 venoms were ultra-filtered to remove high molecular weight, non-toxic and highly immunogenic proteins. The remaining 3 venoms were not ultra-filtered due to limited amounts available. The 9 toxin fractions (TFs) together with the 3 crude venoms were emulsified in complete Freund’s adjuvant and used to immunize 3 horses using a low dose, low volume, multisite immunization protocol. The horse antisera were assayed by ELISA and by in vivo lethality neutralization in mice. The findings were: a) The 9 TFs were shown to contain all of the venom toxins but were devoid of high MW proteins. When these TFs, together with the 3 crude venoms, were used as the immunogen, satisfactory ELISA antibody titers against homologous/heterologous venoms were obtained. b) The horse antiserum immunologically reacted with and neutralized the lethal effects of both the homologous and the 16 heterologous Asian/African elapid venoms tested. Thus, the use of TFs in place of crude venoms and the inclusion of a variety of elapid venoms in the immunogen mix resulted in antiserum with wide paraspecificity against elapid venoms from distant geographic areas. The antivenom prepared from this antiserum would be expected to be pan-specific and effective in treating envenomations by most elapids in many Asian countries. Due to economies of scale, the antivenom could be produced inexpensively and save many lives. This simple strategy and procedure could be readily adapted for the production of pan-specific antisera against elapids of other continents.
机译:蛇咬咬毒在许多热带发展中国家是一个严重的医学问题,被世界卫生组织认为是一种被忽视的热带病。抗毒液(AV)是一种合理且最有效的治疗方式,在许多受影响的国家中要么无法负担和/或无法获得。而且,每个AV仅针对一个(单特异性)或几个(多特异性)蛇毒。这就要求每个国家准备针对当地蛇毒的抗病毒药物,这通常是不可行的。在某些国家/地区,无法针对广泛范围内的许多蛇准备“特定于锅的” AV。如果准备针对多种国家的各种蛇有效的“锅具专用”抗病毒药,就可以经济地大量生产,以供许多国家使用并挽救许多生命。这项研究的目的是产生一种针对亚洲主要医学上重要的弹性蛋白的泛特异性抗血清。策略是使用毒液的毒素级分(TFs)代替粗毒液,以减少马所接触的抗原数量。这使得能够在免疫原混合物中包含更多种弹性蛋白毒液,从而使马免疫系统暴露于多种毒素表位,并产生了针对弹性毒液具有广泛亚特异性的抗血清。从亚洲的12个地区/国家收集了12条毒蛇样品,这些毒蛇样品来自6条具有医学重要性的长形蛇(4条眼镜蛇和2条邦加勒斯蛇)。对这12种毒液中的9种进行了超滤,以去除高分子量,无毒和高度免疫原性的蛋白质。由于可用量有限,其余3种毒液未进行超滤。将9种毒素级分(TFs)与3种粗毒液一起在完全的弗氏佐剂中乳化,并使用低剂量,小体积,多部位免疫方案对3匹马进行免疫。通过ELISA和通过在小鼠中体内致死中和来测定马抗血清。研究结果是:a)9个TF被证明含有所有毒毒素,但不含高分子量蛋白。当将这些TF与3种粗毒液一起用作免疫原时,可获得令人满意的针对同源/异源毒液的ELISA抗体效价。 b)马的抗血清与被测试的同种和16种异源亚洲/非洲弹性毒液发生免疫反应并中和其致死作用。因此,使用TFs代替粗毒液并在免疫原混合物中包含多种弹性毒液导致了抗血清,该血清具有针对来自遥远地理区域的弹性毒液的超亚特异性。在许多亚洲国家,大多数人用这种抗血清制备的抗蛇毒血清应具有泛特异性并能有效治疗蛇毒。由于规模经济,抗蛇毒血清可以廉价生产并挽救许多生命。这种简单的策略和程序可以很容易地适用于生产针对其他大陆的的泛特异性抗血清。

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