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接种疫苗及感染疾病后针对白细胞增多促进因子、丝状血凝素、脂多糖以及百日咳期间诱导产生的与补体结合抗体结合的一种蛋白质的抗体反应。

Antibody responses after vaccination and disease against leukocytosis promoting factor, filamentous hemagglutinin, lipopolysaccharide and a protein binding to complement-fixing antibodies induced during whooping cough.

作者信息

Winsnes R, Lønnes T, Møgster B, Berdal B P

出版信息

Dev Biol Stand. 1985;61:353-65.

PMID:2872124
Abstract

The serum antibody responses of vaccinated children and whooping cough patients to the highly purified Bordetella pertussis antigens, leukocytosis-promoting factor (LPF), lipopolysaccharide (LPS), a protein binding to complement-fixing antibodies induced during whooping cough (PBCA) and to a partly purified filamentous hemagglutinin fraction (FHA) were analysed in enzyme-linked immunosorbent assay. Of the IgG antibodies, those to FHA and LPS were often persistent both after infection and vaccination. The mean titers were about six to ten times higher after disease than after vaccination in corresponding age groups. IgG antibodies to LPF were frequently detected in high titers in patients (mean arbitrary units = 1723), but seldom in low titers (mean units = 20), after vaccination. IgG antibodies to PBCA disappeared some years after vaccination. IgM antibodies to PBCA, FHA and LPS were present in almost 100% after vaccination and disease. IgM antibodies to LPF were detected in 23% of the vaccinated and in 83% of the patients. The respective mean IgM units to PBCA, FHA, LPS and LPF were 14, 13, 16 and 134 times higher in patients than in vaccinated children. None of the vaccinated children and 20% of the patients had IgA antibodies to LPF. No pronounced differences in the percentage of the respective IgA responses to PBCA, the FHA fraction and LPS were found between the two groups. The striking differences in the immune response of vaccinated children and patients were to LPF. Since whooping cough protects better than vaccination against B. pertussis infection, the present study indicates that immunogenic LPF should be included in an acellular vaccine. Also addition of FHA, PBCA and possibly even of LPS, if it can be prepared in an immunogenic and atoxic form, might be necessary in order to prepare a highly effective acellular vaccine.

摘要

在酶联免疫吸附试验中分析了接种疫苗的儿童和百日咳患者对高度纯化的百日咳博德特氏菌抗原、白细胞增多促进因子(LPF)、脂多糖(LPS)、一种与百日咳期间诱导的补体结合抗体结合的蛋白质(PBCA)以及部分纯化的丝状血凝素组分(FHA)的血清抗体反应。在IgG抗体中,针对FHA和LPS的抗体在感染和接种疫苗后通常持续存在。在相应年龄组中,患病后的平均滴度比接种疫苗后高约六至十倍。接种疫苗后,患者中经常检测到高滴度的针对LPF的IgG抗体(平均任意单位=1723),但很少检测到低滴度的(平均单位=20)。接种疫苗后数年,针对PBCA的IgG抗体消失。接种疫苗和患病后,几乎100%的人存在针对PBCA、FHA和LPS的IgM抗体。在23%的接种疫苗者和83%的患者中检测到针对LPF的IgM抗体。患者中针对PBCA、FHA、LPS和LPF的各自平均IgM单位比接种疫苗的儿童高14、13、16和134倍。没有接种疫苗的儿童和20%的患者有针对LPF的IgA抗体。两组之间在针对PBCA、FHA组分和LPS的各自IgA反应百分比方面没有发现明显差异。接种疫苗的儿童和患者的免疫反应的显著差异在于LPF。由于百日咳比接种疫苗预防百日咳博德特氏菌感染的效果更好,本研究表明免疫原性LPF应包含在无细胞疫苗中。此外,如果LPS能够以免疫原性和无毒形式制备,添加FHA、PBCA甚至LPS可能对于制备高效无细胞疫苗是必要的。

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