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Immune responses and protection in different strains of aged mice immunized intranasally with an adjuvant-combined influenza vaccine

机译:佐剂联合流感疫苗经鼻内免疫的不同年龄小鼠的免疫应答和保护

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Immune responses and protection against influenza virus infection were compared between young (2 months) and aged (18 months) BALB/c, C3H and C57BL/6 (B6) mice after intranasal vaccination. The mice were immunized with 2.5 mug protein of A/PR/8/34 (PRs) (H1N1) virus vaccine containing a cholera toxin adjuvant. In both the young and aged BALB/c mice, high levels of PR8-specific antibody-forming cell (AFC) responses were induced in the nasal-associated lymphoid tissue (NALT) 7 days after immunization. Nasal wash IgA and serum IgG antibody (Ab) responses to the PR8 haemagglutinin (HA) 4 weeks after immunization were slightly higher in the young mice than in the aged mice. The young mice showed complete protection against challenge infection, while the aged mice showed only a partial protection. In the C3H mice, NALT-AFC, and IgA and IgG Ab responses were higher in the young mice than those in the aged mice in pallarel with the more efficient protection in the young mice than in the aged mice. Both the young and aged B6 mice showed no NALT-AFC responses, scarce IgA and IgG Ab responses and no protection. In the BALB/c mice, IgG1 and IgG2a levels were significantly lower in the aged mice. On the other hand, in the C3H mice, only IgG2a level was significantly lower in the aged mice. Similar results were obtained in terms of immune responses and protection between the young and aged mice of three different strains of mice after intra-nasal immunization with 0.1 mug of PR8 vaccine containing the adjuvant, two-times at 4-week intervals. In the B6 mice, the immune response was improved by immunization with a higher dose of the adjuvant-combined vaccine. These results suggest that local Ab responses, as well as systemic Ab responses, are downregulated in aged mice, although the degree of the downregulation of immune responses differs from strain to strain.
机译:在鼻内接种疫苗后,对年轻(2个月)和年龄大(18个月)的BALB / c,C3H和C57BL / 6(B6)小鼠的免疫应答和对流感病毒感染的防护进行了比较。用含有霍乱毒素佐剂的2.5杯A / PR / 8/34(PRs)(H1N1)病毒疫苗对小鼠进行免疫。在年轻和年老的BALB / c小鼠中,免疫7天后,在与鼻相关的淋巴样组织(NALT)中都诱导了高水平的PR8特异性抗体形成细胞(AFC)反应。免疫后4周,鼻洗IgA和血清IgG抗体(Ab)对PR8血凝素(HA)的反应在老年小鼠中略高于老年小鼠。幼鼠对攻击性感染表现出完全的保护作用,而老年小鼠只表现出部分保护作用。在C3H小鼠中,年轻小鼠的NALT-AFC以及IgA和IgG Ab反应高于老年小鼠的pallarel,而年轻小鼠的保护作用比老年小鼠更高。 B6幼鼠和老年鼠均未显示NALT-AFC反应,稀缺的IgA和IgG Ab反应且无保护作用。在BALB / c小鼠中,老年小鼠的IgG1和IgG2a水平显着降低。另一方面,在C3H小鼠中,只有IgG2a水平在老年小鼠中显着降低。在用0.1杯含佐剂的PR8疫苗鼻内免疫后,每4周间隔两次,在三种不同品系的小鼠的年轻小鼠和老年小鼠之间的免疫应答和保护方面获得了相似的结果。在B6小鼠中,通过使用更高剂量的佐剂组合疫苗进行免疫可以改善免疫反应。这些结果表明,尽管免疫应答的下调程度因品系而异,但在衰老小鼠中局部Ab应答以及全身性Ab应答均被下调。

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