Anti-bacterial specificities in the human fetal B cell repertoire.

U. Settmacher, A. Delvig, S. Jahn
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引用次数: 2

Abstract

To study the human fetal B cell repertoire, liver and spleen lymphocytes were fused with the human x mouse heteromyeloma line CB-F7. Initially, 2310 IgM and 181 IgG producing hybridoma lines were established. Culture supernatants were analysed for binding activity to antigens from both the exogeneous and the endogeneous environments. For IgG secreting cell lines no antigenetic specificity has been detected. However, independently from the gestational age, monoclonal IgM antibodies binding to bacterial antigens (tetanus toxoid, lipid A, N. meningitidis antigens) were found. In particular, nearly 10% of the hybridomas obtained from fetal liver produced antibodies binding to lipid A (endotoxin). Among the IgM antibodies with anti-bacterial specificities approximately 30% were found to be polyspecific, i.e. these antibodies recognized auto-antigens of different molecular origin as well (ssDNA, keratin, myosin, actin). We conclude that polyreactive natural IgM antibodies may be generated during fetal life, which may take part in the formation of a humoral anti-infectious first line defense barrier in the neonate.
人胎儿B细胞库的抗菌特异性。
为了研究人胎儿B细胞库,将肝脏和脾脏淋巴细胞与人x小鼠异骨髓瘤细胞系CB-F7融合。初步建立了2310株产生IgM和181株产生IgG的杂交瘤细胞株。分析了培养上清液与外源和内源环境抗原的结合活性。IgG分泌细胞系未检测到抗原性。然而,独立于胎龄,发现单克隆IgM抗体结合细菌抗原(破伤风类毒素,脂质A,脑膜炎奈塞菌抗原)。特别是,近10%的从胎儿肝脏获得的杂交瘤产生结合脂质A(内毒素)的抗体。在具有抗菌特异性的IgM抗体中,约30%被发现是多特异性的,即这些抗体也识别不同分子来源的自身抗原(ssDNA、角蛋白、肌球蛋白、肌动蛋白)。我们的结论是,多反应性天然IgM抗体可能在胎儿时期产生,这可能参与了新生儿体液抗感染第一道防御屏障的形成。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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