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人B淋巴细胞体内和体外的IgE同种型转换:主要存在直接从IgM到IgE类别转换程序的证据

In vivo and in vitro IgE isotype switching in human B lymphocytes: evidence for a predominantly direct IgM to IgE class switch program.

作者信息

van der Stoep N, Korver W, Logtenberg T

机构信息

Department of Immunology, University Hospital Utrecht, The Netherlands.

出版信息

Eur J Immunol. 1994 Jun;24(6):1307-11. doi: 10.1002/eji.1830240610.

Abstract

Molecular analysis of circular excision products and composite genomic switch regions has demonstrated that in mice, immunoglobulin (Ig) isotype switching from IgM to IgE often proceeds sequentially via IgG1. Based on analysis of Ig production in cell cultures, it has been suggested that human B cells may switch to IgE via IgG4, whereas limited molecular data from in vitro switched B cells suggest a direct IgM to IgE switch program. To obtain a quantitative assessment of direct versus sequential IgE switching in humans, we have analyzed the nucleotide sequences of 29 composite S mu/S epsilon switch regions from freshly isolated human B lymphocytes from patients with atopic dermatitis and from B lymphocytes induced to switch to IgE synthesis in vitro. The data show that in these B cells IgE isotype switching progressed directly from IgM to IgE. We conclude that, in contrast to the murine IgM/IgE switch program, the IgM to IgE switch in B lymphocytes from patients with atopic dermatitis as well as in vitro stimulated B cells from healthy donors preferentially proceeds via direct S mu to S epsilon switch recombination.

摘要

对环状切除产物和复合基因组开关区域的分子分析表明,在小鼠中,免疫球蛋白(Ig)同种型从IgM转换为IgE通常通过IgG1依次进行。基于对细胞培养物中Ig产生的分析,有人提出人类B细胞可能通过IgG4转换为IgE,而来自体外转换B细胞的有限分子数据表明存在直接从IgM到IgE的转换程序。为了对人类中直接与顺序性IgE转换进行定量评估,我们分析了来自特应性皮炎患者新鲜分离的人类B淋巴细胞以及体外诱导转换为IgE合成的B淋巴细胞的29个复合Sμ/Sε开关区域的核苷酸序列。数据表明,在这些B细胞中,IgE同种型转换直接从IgM进展到IgE。我们得出结论,与小鼠IgM/IgE转换程序不同,特应性皮炎患者的B淋巴细胞以及健康供体的体外刺激B细胞中的IgM到IgE转换优先通过直接的Sμ到Sε开关重组进行。

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