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Altered p16 and Bcl-2 Expression Reflects Pathologic Development in Hydatidiform Moles and Choriocarcinoma

机译:p16和Bcl-2表达的改变反映了葡萄胎和绒癌的病理发展。

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Abnormal trophoblast differentiation is the main cause of gestational trophoblast diseases in the case of hydatidiform moles and choriocarcinomas. Here we investigated the expression patterns of two gene products, p16 and Bcl-2, implicated in cell cycle regulation and apoptosis, respectively, using immunohistochemistry during normal placenta differentiation, hydatidiform moles (partial, complete and invasive) and post-molar choriocarcinomas. The p16 protein shows a gradual expression in cytotrophoblast of normal villous, from a p16 weak proliferative phenotype to a p16 strong invasive phenotype reaching a maximum around 17?weeks of gestation. The expression pattern in cytotrophoblast was similar in moles in contrast to the villous mesenchyme of invasive moles where p16 was strongly expressed. Bcl-2 expression was syncytiotrophoblast specific in normal placenta and moles and increased gradually during normal differentiation. The results explain the persistence of normal and molar villous fragments during their development and their dramatic invasion in the uterine arteries in case of invasive moles. In choriocarcinomas the weak Bcl-2 expression is associated with weak p16 expression indicating a great apoptotic and proliferative potentials. The results suggest that strong p16 expression in the villous mesenchyme may be responsible in part of the morbidity of the moles, and the key of cancer progression in the choriocarcinomas would be a fast cell-cycle turnover.
机译:在葡萄胎和绒毛膜癌的情况下,滋养细胞异常分化是妊娠滋养细胞疾病的主要原因。在这里,我们研究了正常胎盘分化,葡萄胎(部分,完全和浸润)和磨牙后绒毛膜上皮癌中免疫组织化学检测的两种基因产物p16和Bcl-2的表达模式,分别涉及细胞周期调控和凋亡。 p16蛋白在正常绒毛的细胞滋养细胞中逐渐表达,从p16弱增殖表型到p16强侵袭性表型,在妊娠17周左右达到最大值。与滋养性痣的绒毛间充质相比,成纤维细胞中的表达模式在痣中是相似的,后者强烈表达p16。 Bcl-2表达是正常胎盘和痣中的合体滋养层细胞特异性表达,并在正常分化过程中逐渐增加。结果解释了正常和臼齿绒毛碎片在其发育过程中的持久性以及在侵入性痣的情况下它们在子宫动脉中的剧烈侵袭。在绒癌中,弱的Bcl-2表达与弱的p16表达相关,表明其具有巨大的凋亡和增殖潜能。结果表明,绒毛间充质中p16的强表达可能是部分痣的发病原因,绒毛膜癌中癌症进展的关键是细胞周期的快速更新。

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