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编码T细胞替代因子的互补DNA的克隆及其与B细胞生长因子II的同一性

Cloning of complementary DNA encoding T-cell replacing factor and identity with B-cell growth factor II.

作者信息

Kinashi T, Harada N, Severinson E, Tanabe T, Sideras P, Konishi M, Azuma C, Tominaga A, Bergstedt-Lindqvist S, Takahashi M

出版信息

Nature. 1986;324(6092):70-3. doi: 10.1038/324070a0.

Abstract

Proliferation and maturation of antigen-stimulated B cells are regulated by several soluble factors derived from macrophages and T cells. These soluble factors are functionally divided into two groups: B-cell growth factor (BCGF), thought to be involved in B-cell proliferation; and B-cell differentiation factor (BCDF), responsible for maturation of activated B cells into immunoglobulin-secreting cells. This classification needs to be re-examined in the light of the recent cloning of complementary DNA encoding IgG1 induction factor (interleukin-4, IL-4) from the 2.19 mouse T-cell line. Recombinant IL-4 has BCGF and BCDF activities and affects B cells, T cells and mast cells (refs 7, 8; our unpublished data). Another well-characterized B-cell factor is T-cell replacing factor (TRF), which, when secreted by the murine T-cell hybridoma B151K12, is defined by two activities: induction of IgM secretion by BCL1 leukaemic B-cell line; and induction of secondary anti-dinitrophenol (DNP) immunoglobulin G (IgG) synthesis in vitro by DNP-prime B cells. Although TRF from B151K12 was classified as BCDF, purified TRF has BCGF-II activity. To elucidate the molecular properties of TRF we isolated cDNA encoding TRF from the 2.19 T-cell line and report here the structure and multiple activities of this lymphokine.

摘要

抗原刺激的B细胞的增殖和成熟受源自巨噬细胞和T细胞的几种可溶性因子调控。这些可溶性因子在功能上分为两类:B细胞生长因子(BCGF),被认为参与B细胞增殖;以及B细胞分化因子(BCDF),负责将活化的B细胞成熟为分泌免疫球蛋白的细胞。鉴于最近从小鼠2.19 T细胞系中克隆出编码IgG1诱导因子(白细胞介素-4,IL-4)的互补DNA,这一分类需要重新审视。重组IL-4具有BCGF和BCDF活性,并影响B细胞、T细胞和肥大细胞(参考文献7、8;我们未发表的数据)。另一种特征明确的B细胞因子是T细胞替代因子(TRF),当由小鼠T细胞杂交瘤B151K12分泌时,它具有两种活性:诱导BCL1白血病B细胞系分泌IgM;以及在体外由二硝基苯酚(DNP)致敏的B细胞诱导二次抗DNP免疫球蛋白G(IgG)合成。尽管来自B151K12的TRF被归类为BCDF,但纯化的TRF具有BCGF-II活性。为了阐明TRF的分子特性,我们从2.19 T细胞系中分离出编码TRF的cDNA,并在此报告这种淋巴因子的结构和多种活性。

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