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首页> 外文期刊>American Journal of Pathology: Official Publication of the American Association of Pathologists >MYCN promotes the expansion of Phox2B-positive neuronal progenitors to drive neuroblastoma development.
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MYCN promotes the expansion of Phox2B-positive neuronal progenitors to drive neuroblastoma development.

机译:MYCN促进Phox2B阳性神经元祖细胞的扩增,以驱动神经母细胞瘤的发展。

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摘要

Amplification of the oncogene MYCN is a tumorigenic event in the development of a subset of neuroblastomas that commonly consist of undifferentiated or poorly differentiated neuroblasts with unfavorable clinical outcome. The cellular origin of these neuroblasts is unknown. Additionally, the cellular functions and target cells of MYCN in neuroblastoma development remain undefined. Here we examine the cell types that drive neuroblastoma development in TH-MYCN transgenic mice, an animal model of the human disease. Neuroblastoma development in these mice begins with hyperplastic lesions in early postnatal sympathetic ganglia. We show that both hyperplasia and primary tumors are composed predominantly of highly proliferative Phox2B(+) neuronal progenitors. MYCN induces the expansion of these progenitors by both promoting their proliferation and preventing their differentiation. We further identify a minor population of undifferentiated nestin(+) cells in both hyperplastic lesions and primary tumors that may serve as precursors of Phox2B(+) neuronal progenitors. These findings establish the identity of neuroblasts that characterize the tumor phenotype and suggest a cellular pathway by which MYCN can promote neuroblastoma development.
机译:致癌基因MYCN的扩增是神经母细胞瘤子集发展中的致瘤事件,通常由未分化或分化差的神经母细胞组成,临床效果不佳。这些成神经细胞的细胞起源是未知的。另外,在神经母细胞瘤发展中MYCN的细胞功能和靶细胞仍然不确定。在这里,我们检查了驱动TH-MYCN转基因小鼠(人类疾病的动物模型)中神经母细胞瘤发展的细胞类型。这些小鼠的神经母细胞瘤发展始于出生后早期交感神经节的增生性病变。我们显示增生和原发性肿瘤主要由高度增殖的Phox2B(+)神经元祖细胞组成。 MYCN通过促进它们的增殖和阻止其分化来诱导这些祖细胞的扩增。我们进一步确定增生性病变和原发性肿瘤中未分化的Nestin(+)细胞的少数群体,它们可以作为Phox2B(+)神经元祖细胞的前体。这些发现建立了表征肿瘤表型的成神经细胞的身份,并提出了MYCN可以促进成神经细胞瘤发展的细胞途径。

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