Emergency granulopoiesis refers to the increased production of neutrophils in bone marrow and their release into circulation induced by severe infection. Several studies point to a critical role for G-CSF as the main mediator of emergency granulopoiesis. However, the consequences of G-CSF stimulation on the transcriptome of neutrophils and their precursors have not yet been investigated in humans. In this work, we examine the changes in mRNA expression induced by administration of G-CSF in vivo, as a model of emergency granulopoiesis in humans. Blood samples were collected from healthy individuals after 5 d of G-CSF administration. Neutrophil precursors were sorted into discrete stages of maturation by flow cytometry, and RNA was subjected to microarray analysis. mRNA levels were compared with previously published expression levels in corresponding populations of neutrophil precursors isolated from bone marrow of untreated, healthy individuals. One thousand one hundred and ten mRNAs were differentially expressed >2-fold throughout terminal granulopoiesis. Major changes were seen in pathways involved in apoptosis, cytokine signaling, and TLR pathways. In addition, G-CSF treatment reduced the levels of four of five measured granule proteins in mature neutrophils, including the proantibacterial protein hCAP-18, which was completely deficient in neutrophils from G-CSF-treated donors. These results indicate that multiple biological processes are altered to satisfy the increased demand for neutrophils during G-CSF-induced emergency granulopoiesis in humans.

译文

紧急粒细胞生成是指严重感染引起的骨髓中性粒细胞生成增加并释放到循环中。多项研究指出,g-csf作为紧急粒细胞生成的主要介质的关键作用。然而,尚未在人类中研究g-csf刺激对嗜中性粒细胞及其前体转录组的影响。在这项工作中,我们检查了体内使用g-csf诱导的mRNA表达的变化,作为人类紧急粒细胞生成的模型。给予g-csf 5天后,从健康个体收集血液样本。通过流式细胞仪将中性粒细胞前体分为成熟的离散阶段,并对RNA进行微阵列分析。将mRNA水平与先前发表的从未经治疗的健康个体的骨髓中分离出的中性粒细胞前体的相应群体中的表达水平进行了比较。一千个110 mrna在整个末端粒化过程中差异表达> 2倍。在涉及凋亡,细胞因子信号传导和TLR途径的途径中观察到主要变化。此外,g-csf处理降低了成熟嗜中性粒细胞 (包括前抗菌蛋白hCAP-18) 中五种测量的颗粒蛋白中的四种的水平,后者在来自g-csf处理的供体的嗜中性粒细胞中完全缺乏。这些结果表明,在g-csf诱导的人类紧急粒细胞生成过程中,多种生物学过程发生了变化,以满足对嗜中性粒细胞的需求增加。

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