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唐氏综合征新生儿短暂性白血病中的爆裂细胞在体外向嗜碱性粒细胞/肥大细胞和巨核细胞谱系分化,同时伴有 GATA1 截断形式的下调。

Blasts in transient leukaemia in neonates with Down syndrome differentiate into basophil/mast-cell and megakaryocyte lineages in vitro in association with down-regulation of truncated form of GATA1.

机构信息

Department of Pathology and Laboratory Medicine, Tokyo Dental College Ichikawa General Hospital, 5-11-13 Sugano, Ichikawa, Chiba-ken, Japan.

出版信息

Br J Haematol. 2010 Mar;148(6):898-909. doi: 10.1111/j.1365-2141.2009.08038.x. Epub 2010 Jan 11.

DOI:10.1111/j.1365-2141.2009.08038.x
PMID:20064153
Abstract

Mutations of GATA1, leading to aberrant expression of a truncated form of GATA1 (called GATA1s), are present in transient leukaemia (TL) in neonates with Down syndrome. Using these molecular markers of TL, we investigated the growth and differentiation potential of TL blasts in the presence of hematopoietic growth factors (HGFs). Interleukin-3, stem cell factor and granulocyte-macrophage colony-stimulating factor potently stimulated the growth of TL blast progenitors and induced differentiation towards basophil/mast cell lineages, whereas thrombopoietin induced differentiation towards megakaryocytes. GATA1s was expressed in TL blasts in all five patients examined but was down-regulated during differentiation induced by these HGFs, while full-length GATA1 was not expressed throughout the culture. GATA1 mutations were detected in TL blasts in four patients, including one patient with two distinct mutations. The cells of this patient exhibited identical and only mutated sequences both before and after culture with HGFs, confirming the leukemic cell origin of these differentiated cells. Erythroid differentiation of TL blasts was not evident with any HGFs. These data indicate that TL blasts have the potential to grow and differentiate towards particular hematopoietic lineages in the presence of specific HGFs and that the down-regulation of GATA1s might be involved in blast cell differentiation.

摘要

GATA1 基因突变导致 GATA1 截断形式(称为 GATA1s)的异常表达,存在于唐氏综合征新生儿的短暂白血病(TL)中。使用这些 TL 的分子标志物,我们研究了在造血生长因子(HGFs)存在下 TL blasts 的生长和分化潜力。白细胞介素-3、干细胞因子和粒细胞-巨噬细胞集落刺激因子强烈刺激 TL blast 祖细胞的生长,并诱导向嗜碱性粒细胞/肥大细胞谱系分化,而血小板生成素诱导向巨核细胞分化。在所有检查的五名患者的 TL blasts 中均表达 GATA1s,但在这些 HGFs 诱导的分化过程中下调,而全长 GATA1 在整个培养过程中均不表达。在四名患者的 TL blasts 中检测到 GATA1 突变,包括一名患者有两个不同的突变。该患者的细胞在与 HGFs 培养前后均表现出相同且仅突变的序列,证实了这些分化细胞的白血病细胞起源。在任何 HGFs 存在下,TL blasts 的红细胞分化均不明显。这些数据表明,TL blasts 在特定 HGFs 的存在下具有向特定造血谱系生长和分化的潜力,并且 GATA1s 的下调可能参与了 blast 细胞分化。

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引用本文的文献

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GATA1s induces hyperproliferation of eosinophil precursors in Down syndrome transient leukemia.GATA1s 诱导唐氏综合征一过性白血病中嗜酸性粒细胞前体细胞过度增殖。
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Recurrent isochromosome 21 and multiple abnormalities in a patient suspected of having acute myeloid leukemia with eosinophilic differentiation -- a rare case from South India.一名疑似伴有嗜酸性分化的急性髓系白血病患者出现复发性21号等臂染色体及多种异常——来自印度南部的罕见病例
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