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与HOXB4相比,HOXA4赋予短期再增殖细胞更强的植入潜力。

HOXA4 provides stronger engraftment potential to short-term repopulating cells than HOXB4.

作者信息

Fournier Marilaine, Lebert-Ghali Charles-Étienne, Bijl Janetta J

机构信息

1 Centre de Recherche de l'Hôpital Maisonneuve-Rosemont , Montréal, Québec, Canada .

2 Départment de Microbiologie et Immunologie et, Université de Montréal , Montréal, Québec, Canada .

出版信息

Stem Cells Dev. 2015 Oct 15;24(20):2413-22. doi: 10.1089/scd.2015.0063. Epub 2015 Aug 12.

Abstract

Genes of the HOX4 paralog group have been shown to expand hematopoietic stem cells (HSCs). Endogenous expression of HOXA4 is 10-fold higher than HOXB4 in embryonic primitive hematopoietic cells undergoing self-renewal suggesting a more potent capacity of HOXA4 to expand HSC. In this study, we provide evidence by direct competitive bone marrow cultures that HOXA4 and HOXB4 induce self-renewal of primitive hematopoietic cells with identical kinetics. Transplantation assays show that short-term repopulation by HOXA4-overexpressing multilineage progenitors was significantly greater than HOXB4-overexpressing progenitors in vivo, indicating differences in the sensitivity of the cells to external signals. Small array gene expression analysis showed an increase in multiple Notch and Wnt signaling -associated genes, including receptors and ligands, as well as pluripotency genes, for both HOXA4- and HOXB4-overexpressing cells, which was more pronounced for HOXA4, suggesting that both HOX proteins may assert their affects through intrinsic and extrinsic pathways to induce self-renewal of primitive hematopoietic cells. Thus, HOXA4 increases short-term repopulation to higher levels than HOXB4, which may involve Notch signaling.

摘要

HOX4旁系同源基因家族的基因已被证明可扩增造血干细胞(HSC)。在进行自我更新的胚胎原始造血细胞中,HOXA4的内源性表达比HOXB4高10倍,这表明HOXA4扩增造血干细胞的能力更强。在本研究中,我们通过直接竞争性骨髓培养提供证据表明,HOXA4和HOXB4以相同的动力学诱导原始造血细胞的自我更新。移植试验表明,在体内,过表达HOXA4的多谱系祖细胞的短期重建能力明显强于过表达HOXB4的祖细胞,这表明细胞对外部信号的敏感性存在差异。小阵列基因表达分析显示,过表达HOXA4和HOXB4的细胞中,多个与Notch和Wnt信号相关的基因(包括受体和配体)以及多能性基因均有增加,HOXA4的这种增加更为明显,这表明两种HOX蛋白可能通过内在和外在途径发挥作用,以诱导原始造血细胞的自我更新。因此,HOXA4比HOXB4能将短期重建提高到更高水平,这可能涉及Notch信号传导。

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