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Hematopoietic stem cells express multiple myeloid markers: implications for the origin and targeted therapy of acute myeloid leukemia

机译:造血干细胞表达多种髓系标记物:对急性髓系白血病的起源和靶向治疗的意义

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摘要

Human hematopoietic stem cells (HSCs) are generally regarded as being devoid of the markers expressed by differentiated blood cells, the lineage-specific antigens. However, recent work suggests that genes associated with the myeloid lineage are transcribed in mouse HSCs. Here, we explore whether myeloid genes are actually translated in human HSCs. We show that CD33, CD13, and CD123, well-established myeloid markers, are expressed on human long-term repopulating cells from cord blood and bone marrow. In addition, we demonstrate that nonobese diabetic/severe combined immunodeficiency (NOD/SCID) leukemia-initiating cells (SL-ICs) are restricted to the CD33+ fraction in 11 of 12 acute myeloid leukemia (AML) samples studied, indicating that leukemic stem cells (LSCs) express this antigen. This study changes our view of HSCs and the process of differentiation. Furthermore, based on the phenotypic similarity of HSCs and LSCs, our data provide support for the hypothesis that AML derives from an HSC. Our findings also provide a challenge to contemporary attempts to improve the outcome of AML using myeloid antigen-targeted therapies, given the potential for HSC killing.
机译:人类造血干细胞(HSC)通常被认为缺乏分化血细胞表达的标记,即谱系特异性抗原。但是,最近的研究表明与髓系谱系相关的基因在小鼠HSC中被转录。在这里,我们探讨了髓样基因是否在人类HSC中实际翻译。我们显示,CD33,CD13和CD123(已建立的骨髓标记)在从脐带血和骨髓的人类长期繁殖细胞上表达。此外,我们证明了非肥胖型糖尿病/重症联合免疫缺陷症(NOD / SCID)白血病起始细胞(SL-ICs)在12种急性髓细胞性白血病(AML)中的11种中仅局限于CD33 + 组分样本进行了研究,表明白血病干细胞(LSC)表达了这种抗原。这项研究改变了我们对HSC和分化过程的看法。此外,基于HSC和LSC的表型相似性,我们的数据为AML来自HSC的假设提供了支持。考虑到HSC杀伤的潜力,我们的发现也对当代尝试使用髓样抗原靶向疗法改善AML的结果提出了挑战。

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