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Efficacy of a Replikin Peptide Vaccine Against Low-Pathogenicity Avian Influenza H5 Virus

机译:复制蛋白肽疫苗对低致病性禽流感H5病毒的功效

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In this study, the sequence of the H5 and PB1 genes of the low-pathogenic avian influenza virus (LPAI) A/Black Duck/NC/674-964/06 isolate were determined for replikin peptides and used to design and chemically synthesize a vaccine. The vaccine was used to immunize specific-pathogen-free (SPF) leghorn chickens held in Horsfall isolation units, by the upper respiratory route, at 1, 7, and 14 days of age. The birds were challenged at 28 days of age with 1 c 106 50% embryo infective dose of the LPAI Black Duck/NC/674-964/06 H5N1 virus per bird. Oropharyngeal and cloacal swabs were collected at 2, 4, and 7 days postinoculation (PI) for virus detection by real-time RT-PCR. Serum was collected at 7, 14, and 21 days PI and examined for antibodies against avian influenza virus by the enzyme-linked immunosorbent assay and hemagglutination inhibition (HI) tests. Tissue samples for histopathology were collected from three birds per group at 3 days PI. The experimental design consisted of a negative control group (not vaccinated and not challenged) and a vaccinated group, a vaccinated and challenged group, and a positive control group (challenged only). None of the nonchallenged birds, the vaccinated birds, or the vaccinated and challenged birds showed overt clinical signs of disease during the study. A slight depression was observed in the nonvaccinated challenged birds on day 2 postchallenge. Although the numbers of birds per group are small, no shedding of the challenge virus was detected in the vaccinated and challenged birds, whereas oropharyngeal and cloacal shedding was detected in the nonvaccinated and challenged birds. HI antibodies were detected in the vaccinated and nonchallenged group as well as in the vaccinated and challenged group, but rising antibody titers, indicating infection with the LPAI challenge virus, were not detected. Rising HI titers were observed in the nonvaccinated and challenged group. In addition, no antibodies were detected in the nonchallenged birds. Noteworthy microscopic lesions were not observed in the vaccinated and challenged birds, whereas nonvaccinated-challenged birds had microscopic lesions consistent with infection with LPAI viruses. Taken together, these data indicate that a replikin peptide vaccine, specifically made against the H5N1 Black Duck/NC/674-964/06 isolate, and administered three times to the upper respiratory tract, was capable of protecting chickens from infection and from shedding of the homologous virus, which is extremely important because reduced virus shedding and transmission decreases the potential for H5 LPAI viruses to become HPAI viruses. The study is also important because it shows that the vaccine can be effectively mass-delivered to the upper respiratory tract.
机译:在这项研究中,确定了低致病性禽流感病毒(LPAI)A / Black Duck / NC / 674-964 / 06分离株的H5和PB1基因序列,以用于复制素肽,并用于设计和化学合成疫苗。该疫苗用于通过上呼吸道对分别在1、7和14天龄的Horsfall隔离单元中饲养的无特定病原(SPF)来亨鸡进行免疫。用每只鸟1 c 106 50%胚胎感染剂量的LPAI黑鸭/ NC / 674-964 / 06 H5N1病毒对这些鸟进行攻击。接种后第2、4和7天收集口咽和泄殖腔拭子,通过实时RT-PCR检测病毒。在感染后第7、14和21天收集血清,并通过酶联免疫吸附试验和血凝抑制(HI)试验检查抗禽流感病毒的抗体。在感染后第3天从每组三只鸟收集组织病理学的组织样品。实验设计包括阴性对照组(未接种疫苗且未挑战)和接种组,接种和挑战组以及阳性对照组(仅接受挑战)。在研究过程中,未受攻击的鸟类,接种疫苗的鸟类或经免疫接种和挑战的鸟类均未显示明显的疾病临床症状。攻击后第2天,未接种疫苗的受攻击鸡只观察到轻微的压抑。尽管每组的禽鸟数量很少,但在接种疫苗和受攻击的鸟类中未检测到挑战病毒脱落,而在未接种疫苗和受攻击的鸟类中未检测到口咽和泄殖腔脱落。在接种和未攻击组以及接种和攻击组中均检测到HI抗体,但未检测到抗体滴度上升,表明已感染LPAI攻击病毒。在未接种疫苗和攻击的组中,HI滴度升高。此外,在非挑战性鸟类中未检测到抗体。在接种疫苗和攻击的鸟类中未观察到明显的微观损伤,而未接种疫苗的挑战性鸟类具有与LPAI病毒感染一致的微观损伤。综上所述,这些数据表明,针对H5N1黑鸭/ NC / 674-964 / 06分离株专门制成的复制素肽疫苗,已对上呼吸道进行了3次给药,能够保护鸡免受感染和脱落。同源病毒,这一点极为重要,因为减少的病毒脱落和传播会降低H5 LPAI病毒成为HPAI病毒的可能性。该研究也很重要,因为它表明该疫苗可以有效地大量递送到上呼吸道。

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