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首页> 外文期刊>Clinical and vaccine immunology: CVI >Analysis of heavy-chain antibody responses and resistance to Parelaphostrongylus tenuis in experimentally infected alpacas
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Analysis of heavy-chain antibody responses and resistance to Parelaphostrongylus tenuis in experimentally infected alpacas

机译:重链抗体反应和分析抵抗Parelaphostrongylus清塞音实验感染羊驼

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The parasitic nematode Parelaphostrongylus tenuis is an important cause of neurologic disease of camelids in central and eastern North America. The aim of this study was to determine whether alpacas develop resistance to disease caused by P. tenuis in response to a previous infection or a combination of controlled infection and immunization. Alpacas were immunized with a homogenate of third-stage larvae (L3) and simultaneously implanted subcutaneously with diffusion chambers containing 20 live L3. Sham-treated animals received adjuvant alone and empty chambers. The protocol was not effective in inducing resistance to oral challenge with 10 L3, and disease developed between 60 and 71 days following infection. Immediately following the onset of neurologic disease, affected animals were treated with a regimen of anthelmintic and anti-inflammatory drugs, and all recovered. One year later, a subset of alpacas from this experiment was challenged with 20 L3 and the results showed that prior infection induced resistance to disease. Primary and secondary infections induced production of conventional and heavy-chain IgGs that reacted with soluble antigens in L3 homogenates but did not consistently recognize a recombinant form of a parasite-derived aspartyl protease inhibitor. Thus, the latter antigen may not be a good candidate for serology-based diagnostic tests. Antibody responses to parasite antigens occurred in the absence of overt disease, demonstrating that P. tenuis infection can be subclinical in a host that has been considered to be highly susceptible to disease. The potential for immunoprophylaxis to be effective in preventing disease caused by P. tenuis was supported by evidence of resistance to reinfection.
机译:寄生线虫Parelaphostrongylus清塞音神经系统疾病的一个重要原因吗骆驼科在北美中部和东部。本研究的目的是确定羊驼产生耐药性疾病所致p .清塞音在回答之前感染或控制感染和的组合免疫接种。三级幼虫(L3)和匀浆同时植入皮下注射,扩散室包含20 L3生活。仅接受辅助和Sham-treated动物空腔。诱导阻力口服10 L3,挑战和疾病发展60至71天后感染。神经系统疾病的发病,影响动物治疗方案的驱虫剂和抗炎药,恢复。年之后,一个子集的羊驼实验是20 L3和挑战结果表明,前感染引起抵抗疾病。感染诱导生产常规和重链免疫球蛋白与可溶性反应在L3匀浆抗原,但没有一直承认的重组形式parasite-derived天门冬氨酰蛋白酶抑制剂。因此,后者抗原可能不是一个好候选人serology-based诊断测试。抗体反应寄生虫抗原发生没有明显的疾病,展示, p .清塞音可以亚临床感染主机被认为是高度容易感染疾病。有效预防接种免疫疾病引起的p .清塞音是支持的抵抗再感染的证据。

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