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Kidney Cell-Adapted Infectious Bronchitis Virus Arkansas Delmarva Poultry Industry Vaccine Confers Effective Protection Against Challenge

机译:适应肾脏细胞的传染性支气管炎病毒阿肯色州德尔马瓦家禽业疫苗赋予有效的保护以应对挑战

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We previously demonstrated that adaptation of an embryo-attenuated infectious bronchitis virus (IBV) Arkansas Delmarva Poultry Industry (ArkDPI)-derived vaccine to chicken embryo kidney (CEK) cells shifted the virus population towards homogeneity in spike (S) and nonstructural protein genes. Moreover, the typical Ark vaccine subpopulations emerging in chickens vaccinated with commercial Ark vaccines were not detected in chickens vaccinated with the CEK-adapted virus. In this study, chickens vaccinated with a low dose (1.6 x 3 10(3) EID50/bird, where EID50 is 50% embryo infectious dose) of CEK-adapted Ark vaccine at 5 days of age showed a significant reduction of IBV RNA in lachrymal fluids and decreased incidence of IBV RNA detection in tracheal swabs 5 days after challenge compared to unvaccinated challenged chickens. In a second experiment, 5-day-old chickens were vaccinated with 10(4) or 10(5) EID50/chicken of CEK-adapted Ark vaccine, and protection was compared to chickens vaccinated with 10(5) EID50/chicken of the commercial ArkDPI-derived vaccine from which the CEK-adapted virus originated. All vaccinated chicken groups showed a significant reduction of respiratory signs and viral load 5 days after Ark virulent challenge compared to unvaccinated challenged controls. No viral subpopulations different from the challenge virus were detected in chickens vaccinated with CEK-Ark after challenge. In contrast, IBV S1 sequences differing from the predominant population in the challenge virus were detected in several chickens vaccinated with the commercial Ark attenuated vaccine. From an applied perspective, the CEK-adapted IBV ArkDPI-derived vaccine is an improved and effective vaccine candidate with which to protect chickens against virulent Ark-type strains.
机译:先前我们证明了,对胚胎减毒的传染性支气管炎病毒(IBV)阿肯色州Delmarva家禽业(ArkDPI)衍生的疫苗对鸡胚肾(CEK)细胞的适应作用使病毒种群向着尖峰(S)和非结构蛋白基因的同质性转移。此外,在接种了商品Ark疫苗的鸡中出现的典型Ark疫苗亚群未在接种了CEK适应病毒的鸡中检出。在这项研究中,在5日龄时接种低剂量(1.6 x 3 10(3)EID50 /鸟,其中EID50是50%胚胎感染剂量)的CEK适应性方舟疫苗的鸡显示IBV RNA显着降低。与未接种疫苗的攻击鸡相比,攻击后5天气管拭子中的泪液和IBV RNA检测率降低。在第二个实验中,给5日龄的鸡接种适应CEK的Ark疫苗的10(4)或10(5)EID50 /鸡,并与接种10(5)EID50 /鸡的EID50 /鸡进行保护。源自商业的ArkDPI疫苗,源自CEK的病毒起源于该疫苗。与未接种疫苗的对照对照组相比,所有接种疫苗的鸡组在Ark毒性攻击后5天均显示出明显的呼吸道症状和病毒载量减少。在激发后用CEK-Ark疫苗接种的鸡中未检测到与激发病毒不同的病毒亚群。相反,在几只接种了商品Ark减毒疫苗的鸡中检测到了不同于挑战病毒中主要种群的IBV S1序列。从应用的角度来看,适应CEK的IBV ArkDPI衍生疫苗是一种改良且有效的候选疫苗,可用于保护鸡免受强毒Ark型毒株的侵害。

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