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人浆细胞的高IgE分泌能力。

High IgE secretion capacity of human plasma cells.

作者信息

Werner-Favre C, Matthes T, Barnet M, Zubler R H

机构信息

Department of Medicine, Hôpital Cantonal Universitaire, Geneva, Switzerland.

出版信息

Eur J Immunol. 1993 Aug;23(8):2038-40. doi: 10.1002/eji.1830230849.

Abstract

In accordance with results obtained in another culture system, it has previously been shown that human B cells frequently switch to immunoglobulin E (IgE) when they are co-cultured with irradiated mutant EL4 thymoma cells (which provide a CD40 ligand-mediated B cell activation signal), T cell supernatant and recombinant interleukin (IL)-4. However, because of the potentially severe side effects of IgE, such as anaphylaxis, B cells could have a limited capacity to produce this isotype. The IgE secretion rate of plasma cells is not known. In the present study, we compared the secretion rates for different Ig classes by means of limiting dilution analysis of plasmocytic cells that were harvested after 8 to 9 days from primary EL4/B cell cultures and titrated into secondary cultures in the presence of a cell proliferation-blocking concentration of hydroxyurea. These cells secreted Ig at constant rates for periods of up to 2 weeks; IgE secretion was IL-4 independent. The mean cellular secretion rates were similarly high for IgE (150 pg/cell/24 h) and other isotypes (IgM 273 pg, IgG 112 pg, IgA 136 pg/cell/24 h). In terms of molecules per min this represents 3.3 x 10(5) for IgE versus 1.2 x 10(5) for IgM, 3.1 x 10(5) for IgG and 3.6 x 10(5) for IgA. The relative frequency of IgE-secreting cells was only 0.3% of the total number of Ig-secreting cells, suggesting a small size of IgE-producing clones in this in vitro system. Whether this is relevant regarding an in vivo response is not known. Clearly, the Ig secretion capacity of plasma cells would not limit an IgE response in the absence of extrinsic control.

摘要

根据在另一种培养系统中获得的结果,先前已表明,当人类B细胞与经辐照的突变EL4胸腺瘤细胞(其提供CD40配体介导的B细胞活化信号)、T细胞上清液和重组白细胞介素(IL)-4共培养时,它们经常转换为免疫球蛋白E(IgE)。然而,由于IgE可能具有严重的副作用,如过敏反应,B细胞产生这种同种型的能力可能有限。浆细胞的IgE分泌率尚不清楚。在本研究中,我们通过对从原发性EL4/B细胞培养物中收获8至9天后的浆细胞进行有限稀释分析,比较了不同Ig类别的分泌率,并在存在细胞增殖阻断浓度的羟基脲的情况下将其滴定到二级培养物中。这些细胞在长达2周的时间内以恒定速率分泌Ig;IgE分泌不依赖于IL-4。IgE(150 pg/细胞/24小时)和其他同种型(IgM 273 pg、IgG 112 pg、IgA 136 pg/细胞/24小时)的平均细胞分泌率同样高。以每分钟分子数计算,这代表IgE为3.3×10⁵,而IgM为1.2×10⁵,IgG为3.1×10⁵,IgA为3.6×10⁵。分泌IgE的细胞的相对频率仅为分泌Ig的细胞总数的0.3%,表明在该体外系统中产生IgE的克隆规模较小。这是否与体内反应相关尚不清楚。显然,在没有外在控制的情况下,浆细胞的Ig分泌能力不会限制IgE反应。

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