首页> 外文期刊>Anticancer Research: International Journal of Cancer Research and Treatment >Revisiting the role of p53 in primary and secondary glioblastomas.
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Revisiting the role of p53 in primary and secondary glioblastomas.

机译:再次探讨p53在原发性和继发性胶质母细胞瘤中的作用。

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Glioblastoma multiforme (GBM) develops from astrocytes and is the most aggressive primary cancer in humans. Invading cells grow rapidly and form their own blood vessels making them difficult to surgically remove or treat. GBM may develop de novo (primary) or through progression from a low-grade or anaplastic astrocytoma (secondary). Mutational inactivation of the p53 gene and presence of aberrant p53 expression are reported in GBM, suggesting that p53 has a role in tumor progression. This study of seven de novo GBM and four secondary GBM patients, indicated that nine out of eleven (82%) had overexpression of p53. Our histopathological analysis showed that the expression of p53 in three out of four (75%) secondary GBM was confined to the nucleus and the p53 positive cells were randomly distributed throughout the tumor. The expression of p53 in four out of seven (57%) de novo GBM was cytoplasmic, diffusive, and confined to the perivascular region of the tumor. In two (29%) de novo samples both nuclear aswell as cytoplasmic staining that was not confined to the perivascular area was observed. The results suggest that cytoplasmic p53 may contribute to the formation and maintenance of de novo GBM by virtue of its control of the vasculature of tumors. Furthermore, cytoplasmic p53 may reflect an association of p53 with Cullin 7, PARC, or with the sequestering partner of p53, mortalin. These results underscore the significance of p53 in the tumorigenesis of de novo GBM.
机译:多形胶质母细胞瘤(GBM)由星形胶质细胞发育而成,是人类中最具侵略性的原发癌。侵袭性细胞迅速生长并形成自己的血管,使其难以通过外科手术切除或治疗。 GBM可能从头发展(原发性)或通过低度或间变性星形细胞瘤(继发性)进展。 GBM中报道了p53基因的突变失活和异常p53表达的存在,表明p53在肿瘤进展中起作用。这项针对7名从头开始的GBM和4名继发性GBM患者的研究表明,十一名患者中有九名(82%)过度表达了p53。我们的组织病理学分析表明,四分之三(75%)继发性GBM中有三分之三的p53表达局限于细胞核,而p53阳性细胞则随机分布在整个肿瘤中。在七个新的GBM中有四个(57%)中p53的表达是胞质的,扩散性的,并局限于肿瘤的血管周围区域。在两个(29%)新生样本中,观察到的核和细胞质染色均不局限于血管周围区域。结果表明,胞质p53可以通过控制肿瘤的脉管系统来促进从头GBM的形成和维持。此外,胞质p53可能反映p53与Cullin 7,PARC或p53的隔离伴侣mortalin的关联。这些结果强调了p53在新生GBM的肿瘤发生中的重要性。

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