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N-myc基因扩增作为神经母细胞瘤患者的预后标志物。

Amplification of N-myc as a prognostic marker for patients with neuroblastoma.

作者信息

Schwab M

机构信息

Deutsches Krebs Forschungszentrum, Institut für Experimentelle Pathologie, Heidelberg, Germany.

出版信息

Semin Cancer Biol. 1993 Feb;4(1):13-8.

PMID:8448374
Abstract

N-myc is amplified between 5 and several hundred-fold frequently in neuroblastomas and, at lower frequency, in other human cancers with neuronal qualities, including retinoblastomas, gliomas, astrocytomas and small cell lung cancers. In neuroblastomas N-myc amplification is significantly correlated with poor prognosis; for other types of tumors such a correlation is difficult to make, due to low incidence of amplification. Amplification is associated with elevated expression, both of mRNA and protein. N-myc encodes two polypeptides of relative masses of 62 and 64 kDa, which are phosphorylated, at least in vitro, by casein kinase II and that are localized in the nucleus. There they can associate in vivo with another protein, Max, through a C-terminal dimerization motif, the leucine zipper. An N-terminal portion of N-myc, referred to as 'Myc-boxes', can substitute for the transcription-activating function of the yeast transcription factor Gal 4, thus raising the possibility that N-myc itself may act as a transcription factor, either alone or in association with other factors.

摘要

N-myc在神经母细胞瘤中常扩增5至数百倍,在其他具有神经细胞特性的人类癌症中扩增频率较低,这些癌症包括视网膜母细胞瘤、神经胶质瘤、星形细胞瘤和小细胞肺癌。在神经母细胞瘤中,N-myc扩增与预后不良显著相关;对于其他类型的肿瘤,由于扩增发生率低,很难得出这样的相关性。扩增与mRNA和蛋白质的表达升高有关。N-myc编码两种相对分子质量分别为62 kDa和64 kDa的多肽,至少在体外,它们可被酪蛋白激酶II磷酸化,且定位于细胞核。在细胞核中,它们可通过C端二聚化基序亮氨酸拉链在体内与另一种蛋白Max结合。N-myc的N端部分被称为“Myc盒”,可替代酵母转录因子Gal 4的转录激活功能,因此增加了N-myc本身可能单独或与其他因子联合作为转录因子发挥作用的可能性。

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