首页> 美国卫生研究院文献>Epidemiology and Infection >The effects of humoral cellular and non-specific immunity on intracerebral Bordetella pertussis infections in mice.
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The effects of humoral cellular and non-specific immunity on intracerebral Bordetella pertussis infections in mice.

机译:体液免疫细胞免疫和非特异性免疫对小鼠脑内百日咳博德特氏菌感染的影响。

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摘要

When mice were injected intracerebrally with doses of Bordetella pertussis vaccine greater than 5 ImD 50 and challenged intracerebrally 14 days later with virulent B. pertussis there was an immediate reduction in the numbers of organisms. An analysis of this in vivo bactericidal effect has shown that large doses of an unrelated vaccine, Salmonella typhosa, equivalent in cell mass to about 50 ImD 50 of B. pertussis vaccine can achieve this effect, so for such doses the effect must be partly non-specific. This action is not maintained and so is not ultimately protective. Local immunoglobulin was also demonstrable 14 days after 300 ImD 50 of B. pertussis vaccine but following smaller doses of 10-20 ImD 50 it could not be found until after the mice had been infected and the blood-brain barrier impaired. A similar immediate reduction in the numbers of infecting organisms inoculated 1 day after vaccination has been shown to follow very small, non-protective doses of vaccines unrelated to B. pertussis and to be achieved with lipopolysaccharide and endotoxin isolated from B. pertussis. Brains were not sterilized and only in mice receiving protective B. pertussis vaccine was the lowering of infection maintained beyond 2 days and the brains eventually sterilized. The antibody passively protecting mice against intracerebral infection was found in the 19S and 11 S globulin fractions of the serum of once-vaccinated mice and in the 11 S and 7 S fractions of the serum of rabbits and ascitic fluid of mice receiving repeated doses of vaccine. The IgM probably eliminated infections by immediate sterilization but had to be present locally to do so since it was unable to pass from the circulation into the brain, and was therefore inactive when injected intraperitoneally. The IgA and IgG were not so restricted and both the 11 S and 7 S globulins were capable of exerting an immediate suppressive effect on infecting organisms. The 7 S globulin was also capable of a maintained or delayed suppressive effect. Lymphocytes from fully protected once-vaccinated mice, transferred 2-3 weeks after intraperitoneal vaccination, were able to confer some protection when injected intraperitoneally or intracerebrally into recipient mice infected 2 weeks after transfer. Homologous, non-concentrated antiserum from once-vaccinated mice, injected intraperitoneally 1 hr. before infection sometimes augmented the transferred immunity, whereas alone it was inactive.
机译:当给小鼠脑内注射剂量大于5 ImD 50的百日咳博德特氏杆菌疫苗,并在14天后向脑内用强毒百日咳博德特氏菌攻击时,细菌数量立即减少。对这种体内杀菌作用的分析表明,大剂量的无关疫苗,鼠伤寒沙门氏菌,相当于百日咳百日咳博德特氏菌疫苗的细胞质量约为50 ImD 50,可以达到这种效果,因此,对于这种剂量,效果必须部分是非-具体。无法保持此操作,因此最终也不能起到保护作用。在百日咳百日咳博德特氏菌疫苗300 ImD 50后14天也证实了局部免疫球蛋白,但是在较小剂量的10-20 ImD 50后,直到小鼠被感染并且血脑屏障受损后才发现。接种后1天接种的感染性生物数量迅速减少,已显示出与百日咳博德特氏菌无关的非常小剂量的非保护性疫苗,并使用从百日咳博德特氏菌中分离出的脂多糖和内毒素来实现。未对大脑进行灭菌,仅在接受保护性百日咳博德特氏菌疫苗的小鼠中,感染的降低得以维持超过2天,并且最终对大脑进行了灭菌。在一次接种过的小鼠血清的19S和11 S球蛋白级分以及兔子和接受重复剂量疫苗的腹水的11 S和7 S组分中发现了一种被动保护小鼠免于脑内感染的抗体。 IgM可能通过立即灭菌消除了感染,但由于它无法从循环系统传递到大脑,因此必须局部存在,因此腹膜内注射时无活性。 IgA和IgG不受此限制,11 S和7 S球蛋白均能够对感染生物产生即时抑制作用。 7S球蛋白还能够维持或延迟抑制作用。腹膜内接种疫苗后2-3周转移的经过完全保护的曾经接种过疫苗的小鼠的淋巴细胞,当腹膜内或脑内注射到转移后2周感染的受体小鼠体内时,能够提供一定的保护。曾经接种过疫苗的小鼠的同源,非浓缩抗血清腹膜内注射1小时。在感染之前,有时可以增强转移的免疫力,而在单独使用时则没有活性。

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