Sitnicka Ewa, Brakebusch Cord, Martensson Inga-Lill, Svensson Marcus, Agace William W, Sigvardsson Mikael, Buza-Vidas Natalija, Bryder David, Cilio Corrado M, Ahlenius Henrik, Maraskovsky Eugene, Peschon Jacques J, Jacobsen Sten Eirik W
Hematopoietic Stem Cell Laboratory, Lund Strategic Research Center for Stem Cell Biology and Cell Therapy, Lund University Hospital, BMC 10, Klinikgatan 26, 221-84 Lund, Sweden.
J Exp Med. 2003 Nov 17;198(10):1495-506. doi: 10.1084/jem.20031152. Epub 2003 Nov 10.
Extensive studies of mice deficient in one or several cytokine receptors have failed to support an indispensable role of cytokines in development of multiple blood cell lineages. Whereas B1 B cells and Igs are sustained at normal levels throughout life of mice deficient in IL-7, IL-7Ralpha, common cytokine receptor gamma chain, or flt3 ligand (FL), we report here that adult mice double deficient in IL-7Ralpha and FL completely lack visible LNs, conventional IgM+ B cells, IgA+ plasma cells, and B1 cells, and consequently produce no Igs. All stages of committed B cell progenitors are undetectable in FL-/- x IL-7Ralpha-/- BM that also lacks expression of the B cell commitment factor Pax5 and its direct target genes. Furthermore, in contrast to IL-7Ralpha-/- mice, FL-/- x IL-7Ralpha-/- mice also lack mature B cells and detectable committed B cell progenitors during fetal development. Thus, signaling through the cytokine tyrosine kinase receptor flt3 and IL-7Ralpha are indispensable for fetal and adult B cell development.
对缺乏一种或几种细胞因子受体的小鼠进行的广泛研究未能支持细胞因子在多种血细胞谱系发育中起不可或缺的作用。虽然在缺乏白细胞介素7(IL-7)、IL-7受体α链(IL-7Rα)、共同细胞因子受体γ链或fms样酪氨酸激酶3配体(FL)的小鼠一生中,B1 B细胞和免疫球蛋白(Igs)维持在正常水平,但我们在此报告,IL-7Rα和FL双缺陷的成年小鼠完全缺乏可见的淋巴结、传统的IgM+B细胞、IgA+浆细胞和B1细胞,因此不产生Igs。在FL-/-×IL-7Rα-/-骨髓中无法检测到定向B细胞祖细胞的所有阶段,该骨髓也缺乏B细胞定向因子Pax5及其直接靶基因的表达。此外,与IL-7Rα-/-小鼠不同,FL-/-×IL-7Rα-/-小鼠在胎儿发育期间也缺乏成熟B细胞和可检测到的定向B细胞祖细胞。因此,通过细胞因子酪氨酸激酶受体flt3和IL-7Rα的信号传导对于胎儿和成年B细胞发育是不可或缺的。
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