Selective Migration of Subpopulations of Bone Marrow Cells along an SDF-1α and ATP Gradient.

Bone Marrow Research Pub Date : 2014-01-01 Epub Date: 2014-12-31 DOI:10.1155/2014/182645
Michael Laupheimer, Anna Skorska, Jana Große, Gudrun Tiedemann, Gustav Steinhoff, Robert David, Cornelia A Lux
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引用次数: 6

Abstract

Both stem cell chemokine stromal cell-derived factor-1α (SDF-1α) and extracellular nucleotides such as adenosine triphosphate (ATP) are increased in ischemic myocardium. Since ATP has been reported to influence cell migration, we analysed the migratory response of bone marrow cells towards a combination of SDF-1 and ATP. Total nucleated cells (BM-TNCs) were isolated from bone marrow of cardiac surgery patients. Migration assays were performed in vitro. Subsequently, migrated cells were subjected to multicolor flow cytometric analysis of CD133, CD34, CD117, CD184, CD309, and CD14 expression. BM-TNCs migrated significantly towards a combination of SDF-1 and ATP. The proportions of CD34+ cells as well as subpopulations coexpressing multiple stem cell markers were selectively enhanced after migration towards SDF-1 or SDF-1 + ATP. After spontaneous migration, significantly fewer stem cells and CD184+ cells were detected. Direct incubation with SDF-1 led to a reduction of CD184+ but not stem cell marker-positive cells, while incubation with ATP significantly increased CD14+ percentage. In summary, we found that while a combination of SDF-1 and ATP elicited strong migration of BM-TNCs in vitro, only SDF-1 was responsible for selective attraction of hematopoietic stem cells. Meanwhile, spontaneous migration of stem cells was lower compared to BM-TNCs or monocytes.

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骨髓细胞亚群沿SDF-1α和ATP梯度的选择性迁移。
干细胞趋化因子基质细胞衍生因子-1α (SDF-1α)和细胞外核苷酸如三磷酸腺苷(ATP)在缺血心肌中均升高。由于有报道称ATP会影响细胞迁移,我们分析了骨髓细胞对SDF-1和ATP结合的迁移反应。从心脏手术患者骨髓中分离总有核细胞(BM-TNCs)。进行体外迁移试验。随后,对迁移细胞进行CD133、CD34、CD117、CD184、CD309和CD14表达的多色流式细胞术分析。BM-TNCs向SDF-1和ATP的组合显著迁移。在向SDF-1或SDF-1 + ATP迁移后,CD34+细胞以及共表达多种干细胞标记物的亚群的比例选择性地增强。自发迁移后,检测到的干细胞和CD184+细胞明显减少。与SDF-1直接孵育导致CD184+减少,但未导致干细胞标记物阳性细胞减少,而与ATP孵育显著增加CD14+百分比。综上所述,我们发现虽然SDF-1和ATP的结合在体外诱导了BM-TNCs的强迁移,但只有SDF-1负责造血干细胞的选择性吸引。同时,与BM-TNCs或单核细胞相比,干细胞的自发迁移能力较低。
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