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IgE expression on the surface of B1 and B2 lymphocytes in experimental murine schistosomiasis

机译:实验性小鼠血吸虫病B1和B2淋巴细胞表面IgE表达

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In a previous study we monitored the distribution and phenotype expression of B1 cells during the evolution of experimental murine schistosomiasis mansoni and we proposed that the B1 cells were heterogeneous: a fraction which originated in the spleen and followed the migratory pathway to mesenteric ganglia, while the other was the resident peritoneal B1-cell pool. In the present study, we have addressed the question of whether these two B1-lymphocyte populations are involved in the production of the late Ig isotype IgE, which is present in high levels in schistosomal infection. Lymphocyte expression of surface markers and immunoglobulins were monitored by immunofluorescence flow cytometry. Both in the spleen and mesenteric ganglia, the B1 and B2 cells were induced to switch from IgM to IgE in the early Th2-dominated phase of the disease, with an increase of IgE in its later phases. Conversely, peritoneal B1-IgM+ switched to the remaining IgE+ present in high numbers in the peritoneal cavity throughout the disease. We correlated the efficient induction of the expression of late Ig isotypes by B1 cells with high levels of inflammatory cytokines due to the intense host response to the presence of worms and their eggs in the abdominal cavity. In conclusion, B1 cells have a different switch behavior from IgM to IgE indicating that these cell sub-populations depend on the microenvironment.
机译:在先前的研究中,我们监测了实验性曼氏血吸虫病的演化过程中B1细胞的分布和表型表达,我们提出B1细胞是异质性的:一部分起源于脾脏,并沿着迁移途径进入肠系膜神经节,而另一个是常驻腹膜B1细胞池。在本研究中,我们已经解决了这两个B1淋巴细胞群体是否参与晚期Ig同种型IgE的生产的问题,后者在血吸虫病感染中呈高水平存在。通过免疫荧光流式细胞术监测表面标志物和免疫球蛋白的淋巴细胞表达。在脾和肠系膜神经节中,B1和B2细胞在该疾病早期以Th2为主的阶段均被诱导从IgM转换为IgE,而在其后期则增加。相反,在整个疾病期间,腹膜B1-IgM +转换为大量存在于腹膜腔中的剩余IgE +。我们将B1细胞与高水平的炎性细胞因子有效诱导了晚期Ig亚型的表达,这归因于宿主对蠕虫及其卵在腹腔中的强烈宿主反应。总之,B1细胞具有从IgM到IgE的不同转换行为,表明这些细胞亚群取决于微环境。

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