首页> 美国卫生研究院文献>Journal of Virology >Sensitization of mice with wild-type and cold-adapted influenza virus variants: immune response to two H1N1 and H3N2 viruses.
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Sensitization of mice with wild-type and cold-adapted influenza virus variants: immune response to two H1N1 and H3N2 viruses.

机译:用野生型和冷适应型流感病毒变异株敏化小鼠:对两种H1N1和H3N2病毒的免疫应答。

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摘要

Two A strain influenza viruses, A/Hong Kong/123/77 (A/HK/123/77) (H1N1) and A/Queensland/6/72 (A/Qld/6/72) (H3N2), and the two cold-adapted reassortants which possess the surface antigens of these strains (CR35 and CR6, respectively) were tested for their ability both to induce primary cytotoxic T-cell (Tc cell) responses in mice and to sensitize mice for a second Tc cell response when challenged with a distantly related A strain virus, A/Shearwater/72 (H6N5). After intranasal inoculation, A/Qld/6/72 replicated to higher titers in the lung (1 to 2 log10 50% egg infective doses) than did A/HK/123/77 or either of the reassortants. A/Qld/6/72 induced higher Tc cell responses in the lung than did CR6, and both were more effective than either A/HK/123/77 or CR35 in this respect. When similar doses (10 or 10(3) hemagglutinin units) of each virus were injected intravenously into mice and the spleens were tested for Tc cell activity 6 days later, both A/Qld/6/72 and CR6 were ca. 100-fold better at inducing a primary Tc cell response than A/HK/123/77 or CR35. In contrast, the H1N1 and H3N2 viruses gave rather similar anti-hemagglutinin antibody titers (after intravenous injection) and delayed-type hypersensitivity reactions (after subcutaneous injection). If mice were primed with a low dose of these viruses (10(4) 50% egg infective doses intranasally), A/Qld/6/72 and CR6 were more effective than A/HK/123/77 or CR35 at sensitizing for a secondary Tc cell response when challenged with A/Shearwater/72, but if larger doses were given either intranasally (10(6) 50% egg infective doses) or intravenously (10 to 10(3) hemagglutinin units), all viruses sensitized the mice equally well, despite the fact the A/Shearwater/72 gives a poor primary Tc cell response in mice. Thus, the viral glycoprotein antigens can be important in determining the immunogenicity of the virus and, particularly, the class I antigen-restricted Tc cell response of the host.
机译:两种A株流感病毒A / Hong Kong / 123/77(A / HK / 123/77)(H1N1)和A / Queensland / 6/72(A / Qld / 6/72)(H3N2)测试了具有这些菌株的表面抗原(分别为CR35和CR6)的冷适应重配子的诱导小鼠原代细胞毒性T细胞(Tc细胞)反应以及使小鼠对第二种Tc细胞反应敏感的能力。感染了远缘相关的A株病毒A / Shearwater / 72(H6N5)。鼻内接种后,与A / HK / 123/77或任一重组子相比,A / Qld / 6/72在肺中的滴度更高(1至2 log10 50%卵感染剂量)。与CR6相比,A / Qld / 6/72在肺中诱导的Tc细胞应答更高,在这方面,两者均比A / HK / 123/77或CR35更有效。当将每种病毒的相似剂量(10或10(3)血凝素单位)静脉注射到小鼠中并在6天后测试脾脏的Tc细胞活性时,A / Qld / 6/72和CR6均为ca。诱导原发性Tc细胞应答的能力比A / HK / 123/77或CR35高100倍。相反,H1N1和H3N2病毒的抗血凝素抗体滴度(静脉注射后)和迟发型超敏反应(皮下注射后)相似。如果小鼠接受低剂量的这些病毒(鼻内10(4)50%鸡蛋感染剂量)致敏,则A / Qld / 6/72和CR6比A / HK / 123/77或CR35更有效地致敏当用A / Shearwater / 72攻击时,继发性Tc细胞应答,但是如果通过鼻内(10(6)50%鸡蛋感染剂量)或静脉内(10至10(3)血凝素单位)给予较大剂量,则所有病毒都会使小鼠敏感尽管事实证明A / Shearwater / 72在小鼠中的原代Tc细胞反应较差,但效果同样好。因此,病毒糖蛋白抗原在确定病毒的免疫原性,尤其是确定宿主的I类抗原限制的Tc细胞应答方面可能是重要的。

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