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Hepatocellular carcinomas with a high proliferation index and a low degree of apoptosis and necrosis are associated with a shortened survival

机译:高增殖指数,低凋亡和坏死程度的肝细胞癌与生存期缩短有关

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In this study we investigated tumour growth in relation to the immunohistochemical expression of p53 and bcl-2 and to patient survival data in 33 operated hepatocellular carcinomas (HCCs). In order to estimate the growth, a growth index, based on the degree of cell proliferation, apoptosis and necrosis, was calculated for each tumour. Cell proliferation was determined immunohistochemically by the number of proliferating cell nuclear antigen (PCNA)-positive cells in tumours, the extent of apoptosis was determined by counting the number of cells labelled by the in situ 3'-end labelling technique and tumour necrosis was estimated as the percentage of necrotic areas in haematoxylin--eosin-stained tissue sections. In our analysis we found that the survival of patients with HCCs showing a high growth index (i.e. tumours showing a high proliferation and simultaneously a low degree of apoptosis and necrosis) was significantly shorter than with other patients (P = 0.004, log-rank test). When analysed separately, cell proliferation, apoptosis or necrosis did not show any significant association with survival. p53 positivity was found in 8/33 (24%) of tumours. There were significantly more p53-positive cases in tumours with a high growth index (P = 0.01, Fisher's exact test) suggesting that dysfunction of the p53 gene may affect tumour growth. p53-positive cases did not, however, have a significantly shorter survival time than p53-negative cases (P = 0.3, log-rank test). bcl-2 positivity was found in only 1/33 (3%) of the HCCs. Thus bcl-2 overexpression does not seem to play an important role in hepatocellular carcinogenesis. In summary, our results suggest that in HCCs a compound score based on the evaluation of the degree of cell proliferation, apoptosis and necrosis is a biologically more relevant prognostic indicator than any of its composite parameters alone.
机译:在这项研究中,我们调查了p53和bcl-2的免疫组织化学表达与33例手术肝细胞癌(HCC)患者生存数据相关的肿瘤生长情况。为了估计生长,针对每个肿瘤计算基于细胞增殖,凋亡和坏死的程度的生长指数。免疫组织化学方法根据肿瘤中增殖细胞核抗原(PCNA)阳性细胞的数量确定细胞增殖,通过计数用原位3'末端标记技术标记的细胞数量确定凋亡程度,并评估肿瘤坏死以苏木精-伊红染色的组织切片中坏死面积的百分比表示。在我们的分析中,我们发现具有高生长指数(即,肿瘤表现出高增殖,同时凋亡和坏死程度低)的肝癌患者的生存期明显短于其他患者(P = 0.004,对数秩检验) )。单独分析时,细胞增殖,凋亡或坏死与存活率无明显关系。在8/33(24%)的肿瘤中发现p53阳性。在具有高生长指数的肿瘤中,有明显更多的p53阳性病例(P = 0.01,Fisher精确检验),表明p53基因功能异常可能影响肿瘤的生长。然而,p53阳性病例的生存时间没有比p53阴性病例明显短(P = 0.3,对数秩检验)。在只有1/33(3%)的HCC中发现bcl-2阳性。因此,bcl-2的过度表达似乎在肝细胞癌变中不发挥重要作用。总而言之,我们的结果表明,在肝癌中,基于细胞增殖,凋亡和坏死程度评估的综合评分是生物学上比单独的任何复合指标更相关的预后指标。

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