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首页> 外文期刊>Bone marrow transplantation >Ex vivo expansion of enriched CD34+ cells from neonatal blood in the presence of thrombopoietin, a comparison with cord blood and bone marrow.
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Ex vivo expansion of enriched CD34+ cells from neonatal blood in the presence of thrombopoietin, a comparison with cord blood and bone marrow.

机译:在血小板生成素存在下从新生儿血液中富集的CD34 +细胞的离体扩增,与脐带血和骨髓的比较。

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摘要

Neonatal blood (NB) contains substantial numbers of stem and progenitor cells which decline rapidly after birth. Using a combination of cord blood (CB) and NB, we performed a successful, sibling transplant for a thalassaemia patient, leading to the proposal that NB could be used as an adjunct to CB for transplantation. This study was aimed at addressing the feasibility of expanding NB and thus minimizing the volume needed from a NB collection. In the presence of early acting cytokines interleukin-1beta (IL-1beta), IL-3, IL-6, stem cell factor (SCF), flt-3 ligand with and without thrombopoietin (Tpo), we compared the expansion capacity of CD34+ enriched cells from CB, NB and bone marrow (BM). Flow cytometry and colony-forming unit (CFU) analyses show that Tpo significantly increased the expansion of CD34+ cells from CB and NB to early and committed progenitors. No significant difference was observed between the expansion of CB and NB at 7, 14 or 21 days of culture in terms of CFU, CD34+ and CD61+ cell subsets. The expansion capacity of BM was significantly lower than that of NB or CB, possibly related to the low proportion of CD34+ CD38- cells observed at day 0. There was a relatively rapid expansion of NB which was evident at day 7 whilst the expansion of CB and BM remained low, suggesting a speedy maturation process in the postnatal infant. The expanded cells, being heterogeneous in their morphology and cell surface marker expression, were mostly of the myeloid lineage (CD45+, CD33+ and HLA-DR+). Our results showed that the expansion capacity of NB is comparable to that of CB and if transplanted, the expanded products of NB might contribute to the engraftment kinetics of the neutrophil and megakaryocyte lineage.
机译:新生儿血液(NB)包含大量的干细胞和祖细胞,它们在出生后迅速下降。使用脐带血(CB)和NB的组合,我们为地中海贫血患者成功完成了兄弟姐妹移植手术,从而提出了将NB用作CB的辅助移植的建议。这项研究旨在解决扩展NB的可行性,从而最大程度地减少NB收集所需的体积。在存在早期作用的细胞因子白介素-1β(IL-1beta),IL-3,IL-6,干细胞因子(SCF),含和不含血小板生成素(Tpo)的flt-3配体的情况下,我们比较了CD34 +的扩增能力富含来自CB,NB和骨髓(BM)的细胞。流式细胞仪和集落形成单位(CFU)分析表明,Tpo显着增加了CD34 +细胞从CB和NB到早期祖细胞的扩增。就CFU,CD34 +和CD61 +细胞亚群而言,在培养7、14或21天时CB和NB的扩增之间没有观察到显着差异。 BM的扩增能力明显低于NB或CB,这可能与在第0天观察到的CD34 + CD38-细胞比例较低有关。NB的扩增相对较快,这在第7天就很明显,而CB的扩增并且BM仍然很低,表明产后婴儿的成熟过程很快。扩增的细胞在形态和细胞表面标志物表达上是异质的,大部分是髓系(CD45 +,CD33 +和HLA-DR +)。我们的结果表明,NB的扩增能力与CB相当,如果移植,NB的扩增产物可能有助于嗜中性粒细胞和巨核细胞谱系的移植动力学。

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