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Flk2/Flt3配体是原始B细胞祖细胞生长的一种有效辅助因子。

flk2/flt3 ligand is a potent cofactor for the growth of primitive B cell progenitors.

作者信息

Hunte B E, Hudak S, Campbell D, Xu Y, Rennick D

机构信息

Department of Immunology, DNAX Research Institute of Molecular and Cellular Biology, Palo Alto, CA 94304, USA.

出版信息

J Immunol. 1996 Jan 15;156(2):489-96.

PMID:8543798
Abstract

We have investigated the role of flk2/flt3 ligand (FL) in B cell lymphopoiesis. The ability of FL to stimulate the growth of immature B cells was assessed using distinct populations: CD43lowB220+ pre-B cells, CD43+B220+ pro-B cells, and CD43+B220low progenitors. FL failed to affect the growth of the pro-B or pre-B cells whether used alone or in combination with stem cell factor (SCF) or IL-7. In striking contrast, FL was a potent cofactor for the CD43+B220low progenitor cells, interacting with either IL-7 and/or SCF to stimulate their growth. The combination of FL with IL-7 plus SCF stimulated maximum expansion of these cells, albeit, less than that stimulated in stromal cell cultures. When the CD43+B220low progenitors were divided based on expression of heat stable Ag (CD24) into a CD24- and a CD24+ subset, the FL-responsive cells were contained only within the CD24- subset. FL interacted with SCF or with IL-7 to stimulate their growth resulting in a 20- and 50-fold increase in cellularity, respectively. Since the CD24- subset was the most immature of the B cell populations studied, our data suggest that FL costimulates the expansion of very primitive B cell progenitors.

摘要

我们研究了flk2/flt3配体(FL)在B淋巴细胞生成中的作用。使用不同细胞群体评估FL刺激未成熟B细胞生长的能力:CD43lowB220+前B细胞、CD43+B220+原B细胞和CD43+B220low祖细胞。无论单独使用还是与干细胞因子(SCF)或白细胞介素-7(IL-7)联合使用,FL均未能影响原B细胞或前B细胞的生长。与之形成显著对比的是,FL是CD43+B220low祖细胞的有效辅因子,可与IL-7和/或SCF相互作用以刺激其生长。FL与IL-7加SCF的组合刺激了这些细胞的最大程度扩增,尽管低于基质细胞培养中所刺激的程度。当根据热稳定抗原(CD24)的表达将CD43+B220low祖细胞分为CD24-和CD24+亚群时,对FL有反应的细胞仅包含在CD24-亚群内。FL与SCF或IL-7相互作用以刺激它们的生长,分别导致细胞数量增加20倍和50倍。由于CD24-亚群是所研究的B细胞群体中最不成熟的,我们的数据表明FL共刺激非常原始的B细胞祖细胞的扩增。

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