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核仁大小及活性与人类乳腺癌中的视网膜母细胞瘤蛋白(pRb)和p53状态相关。

Nucleolar size and activity are related to pRb and p53 status in human breast cancer.

作者信息

Treré Davide, Ceccarelli Claudio, Montanaro Lorenzo, Tosti Elena, Derenzini Massimo

机构信息

Department of Experimental Pathology, Unit of Clinical Pathology, University of Bologna, Bologna, Italy.

出版信息

J Histochem Cytochem. 2004 Dec;52(12):1601-7. doi: 10.1369/jhc.4A6454.2004.

Abstract

Cell proliferation is tightly coordinated with cell growth. The oncosuppressor proteins pRb and p53 may exert a key role in coupling growth and proliferation by controlling both ribosome biogenesis and cell cycle progression. In the present study we evaluated the relationship between the pRb and p53 status and rRNA transcriptional activity in histological sections of 343 human primary breast carcinomas. Ribosomal biogenesis was quantified by morphometric analysis of silver-stained interphase nucleolar organizer regions (AgNORs). pRb and p53 status was assessed by immunohistochemistry. Twenty-four tumors were considered to be pRb deleted, 260 tumors showed a phosphorylated-pRb labeling index (LI) up to 25%, and 55 tumors an LI >25%. Tumors with deleted pRb or phosphorylated-pRb-LI > or =25% were characterized by significantly greater mean AgNOR area values than those with unaltered pRb (p<0.001). In the 71 tumors with mutated p53 the NOR area mean value was greater than in the 272 tumors with normal p53 (p<0.001). Our results demonstrate, for the first time in vivo, that pRb and p53 status is related to the ribosome biogenesis rate and suggest that in tumors with altered pRb and p53 function the up-regulation of rRNA synthesis may always assure an adequate growth to cancer cells with uncontrolled cell cycle progression.

摘要

细胞增殖与细胞生长紧密协调。肿瘤抑制蛋白pRb和p53可能通过控制核糖体生物合成和细胞周期进程,在连接生长与增殖过程中发挥关键作用。在本研究中,我们评估了343例人原发性乳腺癌组织切片中pRb和p53状态与rRNA转录活性之间的关系。通过对银染间期核仁组织区(AgNORs)进行形态计量分析来量化核糖体生物合成。通过免疫组织化学评估pRb和p53状态。24例肿瘤被认为pRb缺失,260例肿瘤的磷酸化pRb标记指数(LI)高达25%,55例肿瘤的LI>25%。pRb缺失或磷酸化pRb-LI>或=25%的肿瘤,其平均AgNOR面积值显著大于pRb未改变的肿瘤(p<0.001)。在71例p53突变的肿瘤中,NOR面积平均值大于272例p53正常的肿瘤(p<0.001)。我们的结果首次在体内证明,pRb和p53状态与核糖体生物合成速率相关,并表明在pRb和p53功能改变的肿瘤中,rRNA合成的上调可能始终确保癌细胞在细胞周期进程不受控制的情况下有足够的生长。

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