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一种检测单个T淋巴细胞产生集落刺激因子(CSF)的方法:评估T淋巴细胞克隆内产生粒细胞-巨噬细胞集落刺激因子和多谱系集落刺激因子的细胞频率。

An assay for colony-stimulating factor (CSF) production by single T lymphocytes: estimation of the frequency of cells producing granulocyte-macrophage CSF and multi-lineage CSF within a T lymphocyte clone.

作者信息

Kelso A

出版信息

J Immunol. 1986 Apr 15;136(8):2930-7.

PMID:3485676
Abstract

The frequency of cells producing hemopoietic colony-stimulating factors (CSF) in a murine T lymphocyte clone has been determined by using a simple microassay that does not require clonal expansion or the addition of accessory cells. When stimulated with concanavalin A (Con A), the clone LB3 produced both granulocyte-macrophage CSF (GM-CSF) and multi-lineage CSF (Multi-CSF), which could be detected by using the cell line FDC-P1, whose proliferation is dependent on the presence of either of these factors. Limiting dilution analysis of Con A-stimulated LB3 cells indicated a requirement for cell-cell contact for optimal production of CSF, which could be bypassed by preincubation of the cells at high density with Con A for 4 hr before dilution in the assay. Limiting dilution estimates of the frequency of CSF-producing cells among Con A-pretreated LB3 cells ranged from 20 to 50%. Direct measurement of CSF production by single Con A-pretreated cells isolated by micromanipulation revealed that 10 to 20% could secrete detectable CSF. However, when isolated Con A-pretreated two-cell and three-cell aggregates were assayed, 50 to 99% were positive, indicating that 30 to 80% of the cells in the aggregates secreted CSF. Assay of the supernatants from single cells and two-cell aggregates on both FDC-P1 cells and another cell line, 32D c13, which responds only to Multi-CSF, demonstrated that many cells produced GM-CSF only, and others varied in the relative quantities of GM-CSF and Multi-CSF produced.

摘要

通过使用一种简单的微量测定法,在不进行克隆扩增或添加辅助细胞的情况下,已确定了小鼠T淋巴细胞克隆中产生造血集落刺激因子(CSF)的细胞频率。用刀豆蛋白A(Con A)刺激时,克隆LB3产生粒细胞-巨噬细胞集落刺激因子(GM-CSF)和多谱系集落刺激因子(Multi-CSF),这可以通过使用细胞系FDC-P1检测到,该细胞系的增殖依赖于这些因子中的任何一种的存在。对Con A刺激的LB3细胞进行有限稀释分析表明,CSF的最佳产生需要细胞间接触,在测定中稀释前,通过将细胞在高密度下与Con A预孵育4小时可以绕过这一要求。对Con A预处理的LB3细胞中产生CSF的细胞频率的有限稀释估计范围为20%至50%。通过显微操作分离的单个Con A预处理细胞的CSF产生的直接测量显示,10%至20%的细胞可以分泌可检测到的CSF。然而,当对分离的Con A预处理的两细胞和三细胞聚集体进行测定时,50%至99%呈阳性,表明聚集体中30%至80%的细胞分泌CSF。在FDC-P1细胞和另一种仅对Multi-CSF有反应的细胞系32D c13上对单细胞和两细胞聚集体的上清液进行测定,结果表明许多细胞仅产生GM-CSF,其他细胞产生的GM-CSF和Multi-CSF的相对量各不相同。

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