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首页> 外文期刊>Vaccine >Intranasal proteosome-based respiratory syncytial virus (RSV) vaccines protect BALB/c mice against challenge without eosinophilia or enhanced pathology
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Intranasal proteosome-based respiratory syncytial virus (RSV) vaccines protect BALB/c mice against challenge without eosinophilia or enhanced pathology

机译:基于鼻内蛋白体的呼吸道合胞病毒(RSV)疫苗可保护BALB / c小鼠免受挑战,而不会出现嗜酸性粒细胞增多或病理改变

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摘要

A safe and effective vaccine against respiratory syncytial virus (RSV) is still unavailable. Proteosome-based adjuvants are derived from the outer membrane proteins (OMP) of Neisseria species and are potent inducers of both mucosal and systemic immunity in humans and animals. Candidate RSV subunit vaccines comprising enriched RSV proteins (eRSV) formulated with proteosomes alone or with LPS (Protollin) were produced. Administered intranasally in BALB/c mice, both vaccines elicited long-lasting systemic and mucosal RSV-specific antibodies and fully protected against challenge. In vitro restimulation of lymphocytes from the Protollin-eRSV immunized mice with F (MHC-I) and G (MHC-II) peptides elicited F peptide-specific CD8(+) T cells and supernatant IFNgamma, TNFalpha, IL-2 and IL-10 while the formalin-inactivated RSV (FI-RSV) vaccine elicited predominantly IL-5. Pulmonary eosinophilia did not develop following immunization with either proteosome-based vaccine following challenge compared to mice immunized with FI-RSV. Proteosome-based eRSV vaccines can therefore protect against RSV challenge in mice without increasing the risk of pulmonary immunopathologic responses.
机译:仍然没有针对呼吸道合胞病毒(RSV)的安全有效疫苗。基于蛋白体的佐剂衍生自奈瑟氏球菌属的外膜蛋白(OMP),是人类和动物黏膜和全身免疫的有效诱导剂。制备了包含富集的RSV蛋白(eRSV)的候选RSV亚单位疫苗,该蛋白由单独的蛋白体或与LPS(Protollin)配制而成。两种疫苗都通过鼻腔内给药于BALB / c小鼠体内,可引起持久的全身性和粘膜RSV特异性抗体,并能完全抵抗攻击。用F(MHC-I)和G(MHC-II)肽对Protollin-eRSV免疫小鼠的淋巴细胞进行体外再刺激,引起F肽特异性CD8(+)T细胞和上清IFNgamma,TNFalpha,IL-2和IL- 10而福尔马林灭活的RSV(FI-RSV)疫苗主要诱发IL-5。与用FI-RSV免疫的小鼠相比,在攻击后用任一基于蛋白体的疫苗免疫后,肺嗜酸性粒细胞增多都没有发生。因此,基于蛋白质体的eRSV疫苗可以保护小鼠免受RSV攻击,而不会增加肺部免疫病理反应的风险。

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