首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Leukemogenic mechanisms and targets of a NUP98/HHEX fusion in acute myeloid leukemia.
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Leukemogenic mechanisms and targets of a NUP98/HHEX fusion in acute myeloid leukemia.

机译:NUP98 / HHEX融合在急性髓细胞白血病中的致白血病机制和靶标。

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摘要

We have studied a patient with acute myeloid leukemia (AML) and t(10;11)(q23;p15) as the sole cytogenetic abnormality. Molecular analysis revealed a translocation involving nucleoporin 98 (NUP98) fused to the DNA-binding domain of the hematopoietically expressed homeobox gene (HHEX). Expression of NUP98/HHEX in murine bone marrow cells leads to aberrant self-renewal and a block in normal differentiation that depends on the integrity of the NUP98 GFLG repeats and the HHEX homeodomain. Transplantation of bone marrow cells expressing NUP98/HHEX leads to transplantable acute leukemia characterized by extensive infiltration of leukemic blasts expressing myeloid markers (Gr1(+)) as well as markers of the B-cell lineage (B220(+)). A latency period of 9 months and its clonal character suggest that NUP98/HHEX is necessary but not sufficient for disease induction. Expression of EGFP-NUP98/HHEX fusions showed a highly similar nuclear localization pattern as for other NUP98/homeodomain fusions, such as NUP98/HOXA9. Comparative gene expression profiling in primary bone marrow cells provided evidence for the presence of common targets in cells expressing NUP98/HOXA9 or NUP98/HHEX. Some of these genes (Hoxa5, Hoxa9, Flt3) are deregulated in NUP98/HHEX-induced murine leukemia as well as in human blasts carrying this fusion and might represent bona fide therapeutic targets.
机译:我们研究了急性髓细胞性白血病(AML)和t(10; 11)(q23; p15)作为唯一的细胞遗传学异常的患者。分子分析显示涉及核孔蛋白98(NUP98)的易位,融合到造血表达的同源盒基因(HHEX)的DNA结合域上。 NUP98 / HHEX在鼠骨髓细胞中的表达导致异常的自我更新和正常分化的障碍,这取决于NUP98 GFLG重复序列和HHEX同源域的完整性。表达NUP98 / HHEX的骨髓细胞移植导致可移植性急性白血病,其特征是表达髓样标记物(Gr1(+))和B细胞谱系标记物(B220(+))的白血病母细胞广泛浸润。 9个月的潜伏期及其克隆特性表明NUP98 / HHEX对疾病的诱导是必要的,但还不足。 EGFP-NUP98 / HHEX融合蛋白的表达显示出与其他NUP98 / homeodomain融合蛋白(例如NUP98 / HOXA9)高度相似的核定位模式。在原代骨髓细胞中比较基因表达谱提供了在表达NUP98 / HOXA9或NUP98 / HHEX的细胞中存在共同靶标的证据。其中一些基因(Hoxa5,Hoxa9,Flt3)在NUP98 / HHEX诱导的鼠类白血病以及携带这种融合蛋白的人类胚细胞中被失调,可能代表了真正的治疗靶标。

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