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Limited Protection Conferred by Recombinant Newcastle Disease Virus Expressing Infectious Bronchitis Spike Protein

机译:通过重组新城疫病毒表达传染性支气管炎穗蛋白的有限保护赋予了有限的保护

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Recombinant Newcastle disease virus (NDV) LaSota (LS) expressing secreted trimeric spike (S)-ectodomain (Se) of infectious bronchitis virus (IBV) (rLS/IBV.Se) was developed and evaluated for protection conferred against IBV challenge. The IBV S-ectodomain protein, which is S excluding the transmembrane anchor and short cytoplasmic domain of S2, expressed from recombinant LS corresponds to an Arkansas (Ark)-type IBV. In a first experiment, chickens were primed at 1 day of age or primed at 1 day of age and boosted at 14 days of age with 10(4) 50% embryo infectious doses (EID50)/bird of rLS/IBV.Se and challenged with a virulent Ark strain. A single vaccination proved completely ineffective at protecting chickens against challenge, whereas priming and boosting reduced clinical signs and tracheal lesions but did not reduce viral load in lachrymal fluids. In experiment 2, the vaccine dose was increased to 10(7) EID50/bird and a different virulent Ark strain was used for challenge. In addition, chickens were singly immunized on either day 1 or day 10 after hatch. NDV antibody levels detected in vaccinated chickens were moderate, with hemagglutination inhibition titers varying between 4 and 5 log(2). Slightly higher antibody levels to NDV were observed in chickens vaccinated on day 10 versus day 1 but without the difference achieving statistical significance. In contrast, antibody responses measured using recombinant IBV S1 protein-coated ELISA plates were significantly greater in chickens vaccinated on day 10 than on day 1. The use of a higher rLS/IBV.Se dose substantially enhanced the success of a single vaccination compared to experiment 1. Signs and tracheal lesions were reduced more effectively in chickens vaccinated at day 10 after hatch. However, as in experiment 1, vaccination did not reduce the viral loads in tear fluids of challenged chickens. Similar results, in which no reduction in viral load in the trachea was apparent from rLS/IBV.S vaccination, have been obtained by others. Further work is needed to understand the immune responses induced by this recombinant virus that seems to provide some protection against the disease but does not reduce viral loads in the upper respiratory tract.
机译:制定并评估表达分泌的三聚体峰值(IB)的分泌的三聚体钉(IBV)(RLS / IBV.SE)的分泌的三聚体钉(SE)的重组新宫疾病病毒(LS),并评估赋予IBV挑战的保护。 IBV S-Octodomain蛋白,其不包括S2的跨膜锚和S2的短细胞质结构域,对应于阿肯色州(ARK)-Type IBV。在第一个实验中,鸡在1天的1天或在1天的时候灌注,并在14天的14天内提升,10(4)50%的胚胎传染病(Eid50)/鸟类/ IBV .SE和挑战用毒性的方舟菌株。在保护鸡对抗攻击中,单一疫苗接种被证明是完全无效的,而引发和促进临床症状和气管病变,但并未降低纳米液体中的病毒载量。在实验2中,将疫苗剂量增加到10(7)eid50 /鸟类,并且使用不同的毒力ARK菌株用于攻击。此外,鸡在孵化后1天或第10天在孵化中单独免疫鸡。在接种疫苗的鸡中检测到的NDV抗体水平是中等的,血凝抑制滴度在4至5的log(2)之间变化。在第10天接种的鸡与第1天接种的鸡中观察到NDV略高的抗体水平,但没有差异达到统计学意义。相反,使用重组IBV S1蛋白涂覆的ELISA板在第10天接种的鸡蛋白涂覆的ELISA板测量的抗体应答显着大于1天的鸡。使用更高的RLS / IBV.SE剂量,与...相比实验1.在孵化后第10天接种疫苗的鸡症和气管病变更有效地减少。然而,如在实验1中,疫苗接种没有减少挑战性鸡的撕裂液中的病毒载量。类似的结果,其中气管中的病毒载量没有从RLS / IBV.S疫苗接种中显而易见,已经通过他人获得。需要进一步的工作来了解这种重组病毒诱导的免疫应答,似乎为疾病提供了一些保护,但不会减少上呼吸道中的病毒载量。

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