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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >GPR56 identifies primary human acute myeloid leukemia cells with high repopulating potential in vivo
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GPR56 identifies primary human acute myeloid leukemia cells with high repopulating potential in vivo

机译:GPR56鉴定了具有高重新迁移潜力的原发性人急性髓性白血病细胞

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摘要

Acute myeloid leukemia (AML) is a genetically heterogeneous hematologic malignancy, which is initiated and driven by a rare fraction of leukemia stem cells (LSCs). Despite the difficulties of identifying a common LSC phenotype, there is increasing evidence that high expression of stem cell gene signatures is associated with poor clinical outcome. Identification of functionally distinct subpopulations in this disease is therefore crucial to dissecting the molecular machinery underlying LSC self-renewal. Here, we combined next-generation sequencing technology with in vivo assessment of LSC frequencies and identified the adhesion G protein-coupled receptor 56 (GPR56) as a novel and stable marker for human LSCs for the majority of AML samples. High GPR56 expression was significantly associated with high-risk genetic subgroups and poor outcome. Analysis of GPR56 in combination with CD34 expression revealed engraftment potential of GPR56(+) cells in both the CD34(-) and CD34(+) fractions, thus defining a novel LSC compartment independent of the CD34(+) CD38(-) LSC phenotype.
机译:急性髓性白血病(AML)是一种遗传异质血液学恶性肿瘤,其被白血病干细胞(LSCs)的罕见部分引发和驱动。尽管识别常见的LSC表型难度,但越来越多的证据表明干细胞基因特征的高表达与临床结果不良有关。因此,鉴定该疾病中功能明显的亚群对解剖底层LSC自我更新的分子机制来说是至关重要的。这里,我们将下一代测序技术组合在LSC频率的体内评估中,并将粘附G蛋白偶联受体56(GPR56)鉴定为用于大多数AML样品的人LSC的新颖且稳定的标志物。高GPR56表达与高危遗传亚组和差的结果显着相关。 GPR56与CD34表达组合的分析显示了CD34( - )和CD34(+)级分中GPR56(+)细胞的植入电位,从而定义了独立于CD34(+)CD38( - )LSC表型的新型LSC盒。

著录项

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  • 作者单位

    Univ Montreal Inst Res Immunol &

    Canc Lab Mol Genet Stem Cells Montreal PQ Canada;

    CHU Laval Ctr Rech Infectiol CHU Quebec Ctr Rech 2705 Blvd Laurier Quebec City PQ G1V 4G2;

    Univ Montreal Inst Res Immunol &

    Canc Lab Mol Genet Stem Cells Montreal PQ Canada;

    Univ Montreal Inst Res Immunol &

    Canc Lab Mol Genet Stem Cells Montreal PQ Canada;

    Univ Montreal Inst Res Immunol &

    Canc Montreal PQ Canada;

    British Columbia Canc Agcy Terry Fox Lab 601 W 10th Ave Vancouver BC V5Z 1L3 Canada;

    Univ Montreal Inst Res Immunol &

    Canc Lab Mol Genet Stem Cells Montreal PQ Canada;

    Univ Montreal Inst Res Immunol &

    Canc Lab Mol Genet Stem Cells Montreal PQ Canada;

    Univ Montreal Inst Res Immunol &

    Canc Lab Mol Genet Stem Cells Montreal PQ Canada;

    CHU Laval Ctr Rech Infectiol CHU Quebec Ctr Rech 2705 Blvd Laurier Quebec City PQ G1V 4G2;

    British Columbia Canc Agcy Terry Fox Lab 601 W 10th Ave Vancouver BC V5Z 1L3 Canada;

    Univ Montreal Inst Res Immunol &

    Canc Montreal PQ Canada;

    McGill Univ Montreal Childrens Hosp McGill Univ Hlth Ctr Dept Pediat Res Inst Montreal PQ H3H;

    Univ Munich Univ Hosp Grosshadern Dept Internal Med 3 Munich Germany;

    Univ Auckland Dept Mol Med &

    Pathol Auckland 1 New Zealand;

    British Columbia Canc Agcy Terry Fox Lab 601 W 10th Ave Vancouver BC V5Z 1L3 Canada;

    Univ Montreal Inst Res Immunol &

    Canc Montreal PQ Canada;

    Maisonneuve Rosemont Hosp Div Hematol Oncol Montreal PQ Canada;

    Univ Montreal Inst Res Immunol &

    Canc Lab Mol Genet Stem Cells Montreal PQ Canada;

    CHU Laval Ctr Rech Infectiol CHU Quebec Ctr Rech 2705 Blvd Laurier Quebec City PQ G1V 4G2;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 血液及淋巴系疾病;
  • 关键词

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