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首页> 外文期刊>Pediatric Research >Vaccine-Induced Human Antibody Responses to the Haemophilus influenzae b Polysaccharide in Severe Combined Immunodeficient Mice Engrafted with Human Leukocytes
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Vaccine-Induced Human Antibody Responses to the Haemophilus influenzae b Polysaccharide in Severe Combined Immunodeficient Mice Engrafted with Human Leukocytes

机译:接种人白细胞的严重联合免疫缺陷小鼠中疫苗诱导的人类对流感嗜血杆菌b多糖的抗体应答。

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We examined the ability of severe combined immunodeficient (SCID) mice-human peripheral blood leukocyte (PBL) chimeras to respond to immunization with Haemophilus influenzae b polysaccharide (Hib PS) vaccines. Two to 3 wk after PBL engraftment, human-PBL-SCID mice, prepared with PBL from one of five adult donors, were immunized with free or protein-conjugated Hib PS. Antibody to Hib PS was quantitated in preimmunization and postimmunization sera. Before immunization, anti-Hib PS antibody was detectable (>10 ng/mL) in three of 40 mice. Of the 37 human-PBL-SCID mice not having detectable serum antibody before immunization, 31 produced ≥20 ng/mL (≥2-fold increase) anti-Hib PS antibody 2 to 3 wk after immunization. Both free and protein-conjugated forms of Hib PS were immunogenic. Geometric mean anti-Hib PS antibody levels ranged from 50 to 139 ng/mL. Vaccine-induced anti-Hib PS antibodies frequently expressed Hibld-1, a cross-reactive idiotype that predominates the in vivo human antibody response to Hib PS. However, among mice engrafted with PBL from a single donor, the Hibld-1 distribution was highly skewed, suggesting that clonally distinct B cells were being stimulated in individual mice. These findings indicate that human PBL transplanted into SCID mice are functionally responsive to Hib PS antigenic challenge. This system may serve as a useful model for studying the regulation and cellular requirements for human polysaccharide immunity.
机译:我们检查了严重的联合免疫缺陷(SCID)小鼠-人外周血白细胞(PBL)嵌合体对流感嗜血杆菌b多糖(Hib PS)疫苗免疫反应的能力。 PBL植入后2至3 wk,用游离的或结合蛋白的Hib PS免疫从五个成年供体之一的PBL制备的人PBL-SCID小鼠。在免疫前和免疫后血清中对Hib PS抗体进行定量。免疫前,在40只小鼠中的3只中可检测到抗Hib PS抗体(> 10 ng / mL)。在免疫前没有可检测的血清抗体的37只人PBL-SCID小鼠中,有31只在免疫后2至3周产生了≥20 ng / mL(≥2倍增加)的抗Hib PS抗体。游离形式和蛋白质结合形式的Hib PS均具有免疫原性。抗Hib PS抗体的几何平均水平为50到139 ng / mL。疫苗诱导的抗Hib PS抗体经常表达Hibld-1,这是一种交叉反应的独特型,在体内人类抗体对Hib PS的反应中占主导地位。但是,在从单个供体移植了PBL的小鼠中,Hibld-1的分布高度偏斜,这表明单个小鼠的克隆性B细胞受到刺激。这些发现表明,移植到SCID小鼠中的人PBL对Hib PS抗原性攻击具有功能性应答。该系统可以用作研究人类多糖免疫的调节和细胞需求的有用模型。

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