首页> 美国政府科技报告 >Induction of In Vivo Antipolysaccharide Immunoglobulin Responses to Intact Streptococcus pneumoniae Is More Heavily Dependent on Btk-Mediated B- Cell Receptor Signaling than Antiprotein Responses
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Induction of In Vivo Antipolysaccharide Immunoglobulin Responses to Intact Streptococcus pneumoniae Is More Heavily Dependent on Btk-Mediated B- Cell Receptor Signaling than Antiprotein Responses

机译:体内抗多糖免疫球蛋白对完整肺炎链球菌的反应比Btk介导的B细胞受体信号更强烈依赖于抗蛋白反应

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The relative role of Btk-dependent B-cell receptor (BCR) signaling in the induction of antipolysaccharide (anti-PS) and antiprotein immunoglobulin (Ig) responses to an intact extracellular bacterium in vivo is unknown. Btk(exp low) mice exhibit reduced BCR signaling but largely restore B-cell development. Btk(exp low) mice immunized with intact Streptococcus pneumoniae elicit reduced anti-PS but normal antiprotein Ig responses. Immunization of Btk(exp low) mice with PS-protein conjugate in saline results in an even more profound defect in the anti-PS but not antiprotein response, which is largely restored by use of a CpG-containing oligodeoxynucleotide as an adjuvant. These data demonstrate a greater dependence on Btk-mediated BCR signaling for physiologic anti-PS relative to antiprotein responses, as well as the existence of a compensatory Toll-like receptor-mediated signaling pathway naturally triggered in response to intact bacterial pathogens.

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