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诱导产生IgM、IgG和IgA的人B细胞诱导因子:不依赖白细胞介素2

Human B cell-inducing factor(s) for production of IgM, IgG and IgA: independence from IL 2.

作者信息

Ralph P, Welte K, Levi E, Nakoinz I, Litcofsky P B, Mertelsmann R H, Moore M A

出版信息

J Immunol. 1984 Apr;132(4):1858-62.

PMID:6607950
Abstract

Human peripheral blood B cells are stimulated into proliferation by killed Staphylococcus aureus bacteria strain Cowan I (Sac). T lymphocytes in the presence of a T cell mitogen induce high numbers of immunoglobulin-secreting cells (ISC) in these Sac-stimulated B cells. The T cells can be largely replaced by a lymphokine factor. We describe here the 11000-fold purification of this B cell-inducing factor (BIF). BIF preparations that are free of IL 2 do not require IL 2 for optimal induction of ISC. This was shown by the lack of effect of IL 2 alone or with suboptimal or optimal concentrations of BIF on the induction of ISC and by the absence of IL 2 production in the purified B cell population which, with other controls, excludes significant T cell contamination. BIF, purified through four fractionation steps and free of IL 2, induces IgM, IgG, and IgA-ISC in approximately the same ratio as unfractionated lymphokine. Because we have not yet attained a pure BIF preparation, the possibility of separate factors for the production of each immunoglobulin isotype cannot be ruled out.

摘要

人外周血B细胞可被灭活的金黄色葡萄球菌考恩I株(Sac)刺激而增殖。在T细胞有丝分裂原存在的情况下,T淋巴细胞可在这些经Sac刺激的B细胞中诱导产生大量免疫球蛋白分泌细胞(ISC)。T细胞在很大程度上可被一种淋巴因子所替代。我们在此描述了这种B细胞诱导因子(BIF)的11000倍纯化过程。不含白细胞介素2(IL 2)的BIF制剂在最佳诱导ISC时不需要IL 2。单独的IL 2或与次优或最佳浓度的BIF共同作用对ISC诱导均无影响,且纯化的B细胞群体中不产生IL 2,与其他对照一起排除了显著的T细胞污染,这些均表明了这一点。经四个分级分离步骤纯化且不含IL 2的BIF诱导产生IgM、IgG和IgA-ISC的比例与未分级分离的淋巴因子大致相同。由于我们尚未获得纯的BIF制剂,因此不能排除存在分别用于产生每种免疫球蛋白同种型的单独因子的可能性。

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