首页> 外文期刊>Biologicals: Journal of the International Association of Biological Standardization >Development of novel strategies to control foot-and-mouth disease: marker vaccines and antivirals.
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Development of novel strategies to control foot-and-mouth disease: marker vaccines and antivirals.

机译:控制口蹄疫的新策略的发展:标记疫苗和抗病毒药。

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摘要

Foot-and-mouth disease (FMD) is economically the most important viral-induced livestock disease worldwide. The disease is highly contagious and FMD virus (FMDV) replicates and spreads extremely rapidly. Outbreaks in previously FMD-free countries, including Taiwan, the United Kingdom, and Uruguay, and the potential use of FMDV by terrorist groups have demonstrated the vulnerability of countries and the need to develop control strategies that can rapidly inhibit or limit disease spread. The current vaccine, an inactivated whole virus preparation, has a number of limitations for use in outbreaks in disease-free countries. We have developed an alternative approach using a genetically engineered FMD subunit vaccine that only contains the portions of the viral genome required for virus capsid assembly and lacks the coding region for most of the viral nonstructural (NS) proteins including the highly immunogenic 3D protein. Thus, animals inoculated with this marker vaccine can readily be differentiated from infected animals using diagnostic assays employing the NS proteins not present in the vaccine and production of this vaccine, which does not contain infectious FMDV, does not require expensive high-containment manufacturing facilities. One inoculation of this subunit vaccine delivered in a replication-defective human adenovirus vector can induce rapid, within 7 days, and relatively long-lasting protection in swine. Similarly cattle inoculated with one dose of this recombinant vector are rapidly protected from direct and contact exposure to virulent virus. Furthermore, cattle given two doses of this vaccine developed high levels of FMDV-specific neutralizing antibodies, but did not develop antibodies against viral NS proteins demonstrating the ability of FMD subunit vaccinated animals to be differentiated from infected animals. To stimulate early protection prior to the vaccine-induced adaptive immune response we inoculated swine with the antiviral agent, type I interferon, and induced complete protection within 1 day. Protection can last for 3-5 days. The combination of the FMD marker vaccine and type I interferon can induce immediate, within 1 day, and long-lasting protection against FMD. Thus, this combination approach successfully addresses a number of concerns of FMD-free countries with the current disease control plan. By rapidly limiting virus replication and spread this strategy may reduce the number of animals that need to be slaughtered during an outbreak.
机译:口蹄疫(FMD)在经济上是全球范围内最重要的病毒引起的家畜疾病。该疾病具有高度传染性,FMD病毒(FMDV)复制和传播极快。台湾,英国和乌拉圭等以前没有口蹄疫的国家暴发,恐怖组织可能利用口蹄疫病毒证明了各国的脆弱性,并需要制定能够迅速抑制或限制疾病传播的控制策略。目前的疫苗是一种灭活的全病毒制剂,在无病国家的暴发中使用有许多限制。我们已经开发了一种使用基因工程FMD亚单位疫苗的替代方法,该疫苗仅包含病毒衣壳装配所需的病毒基因组部分,并且缺少大多数病毒非结构(NS)蛋白质(包括高度免疫原性3D蛋白质)的编码区。因此,使用该疫苗中不存在的NS蛋白的诊断测定可以容易地将接种了这种标志疫苗的动物与受感染的动物区分开,并且该疫苗的生产不含传染性FMDV,不需要昂贵的高含量制造设施。复制缺陷型人腺病毒载体中接种的这种亚单位疫苗的一次接种可在猪中诱导迅速,7天内和相对长期的保护。类似地,用一剂这种重组载体接种的牛被迅速保护免于直接和接触强毒病毒的接触。此外,给予两次该疫苗剂量的牛产生了高水平的FMDV特异性中和抗体,但未产生针对病毒NS蛋白的抗体,证明了FMD亚基接种的动物有能力与感染的动物区分开。为了在疫苗诱导的适应性免疫应答之前刺激早期保护,我们在猪中接种了抗病毒剂,I型干扰素,并在1天内诱导了完全保护。保护可以持续3-5天。 FMD标记疫苗和I型干扰素的组合可在1天内立即诱导出针对FMD的持久保护。因此,这种结合方法通过当前的疾病控制计划成功解决了无口蹄疫国家的许多关切。通过快速限制病毒的复制和传播,该策略可以减少爆发期间需要宰杀的动物数量。

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