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用多糖疫苗对人类进行免疫接种可诱导全身性、主要是聚合型IgA2亚类抗体反应。

Immunization of humans with polysaccharide vaccines induces systemic, predominantly polymeric IgA2-subclass antibody responses.

作者信息

Tarkowski A, Lue C, Moldoveanu Z, Kiyono H, McGhee J R, Mestecky J

机构信息

Department of Microbiology, University of Alabama, Birmingham 35294.

出版信息

J Immunol. 1990 May 15;144(10):3770-8.

PMID:2110213
Abstract

Ig class- and IgA subclass-specific immune responses to protein and polysaccharide Ag were studied in serum, external secretions, and at the single cell level in peripheral blood of systemically immunized adults. Immunization with tetanus toxoid induced predominantly IgG antibody responses in serum and in the PBMC. The IgA antibody response was low, and was mostly of the IgA1 subclass. In contrast, immunization with polysaccharide Ag (Haemophilus influenzae type b, Neisseria meningitidis serogroup A, C, Y, W-135, and Streptococcus pneumoniae capsular polysaccharides) elicited a major IgA response predominantly of the IgA2 isotype. Analysis of the molecular forms of secreted IgA antibodies indicated that polymers were produced early after immunization, irrespective of the nature of the Ag. When compared with serum antibody and to PBMC cell responses, systemic immunization with polysaccharides induced a minor salivary response dominated by IgG and IgM antibodies. In contrast, the presence of antipolysaccharide antibodies in bile, irrespective of their isotype, paralleled the serum response 14 days after the immunization with polysaccharide Ag. These results suggest that biliary Ig were mostly derived from serum. Different patterns of the expression of MHC class II Ag on T cells, B cells, and monocytes during the course of immunization with protein or polysaccharide Ag were observed: whereas protein Ag induced a high frequency of HLA-DP- and HLA-DR-expressing cells early in the course of immunization, polysaccharide vaccines elicited low and protracted increases of HLA-DP+ T cells. Polysaccharide vaccine covalently coupled to a protein carrier induced a higher frequency of antipolysaccharide antibody-secreting cells in peripheral blood and increased the IgG to IgA ratio among polysaccharide-specific antibody-secreting cells.

摘要

在全身免疫的成年人的血清、外分泌液以及外周血单细胞水平上,研究了针对蛋白质和多糖抗原的Ig类别及IgA亚类特异性免疫反应。用破伤风类毒素免疫主要诱导血清和外周血单个核细胞(PBMC)产生IgG抗体反应。IgA抗体反应较低,且大多为IgA1亚类。相比之下,用多糖抗原(b型流感嗜血杆菌、A、C、Y、W-135群脑膜炎奈瑟菌以及肺炎链球菌荚膜多糖)免疫引发了主要的IgA反应,主要为IgA2同种型。对分泌型IgA抗体分子形式的分析表明,无论抗原性质如何,免疫后早期都会产生聚合物。与血清抗体和PBMC细胞反应相比,用多糖进行全身免疫诱导的唾液反应较弱,以IgG和IgM抗体为主。相反,无论同种型如何,多糖抗原免疫14天后胆汁中抗多糖抗体的存在与血清反应相似。这些结果表明胆汁中的Ig大多源自血清。在用蛋白质或多糖抗原免疫过程中,观察到T细胞、B细胞和单核细胞上MHC II类抗原表达的不同模式:蛋白质抗原在免疫早期诱导高频率表达HLA-DP和HLA-DR的细胞,而多糖疫苗则引起HLA-DP+ T细胞低水平且持续时间较长的增加。与蛋白质载体共价偶联的多糖疫苗在外周血中诱导产生更高频率的抗多糖抗体分泌细胞,并增加了多糖特异性抗体分泌细胞中IgG与IgA的比例。

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