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Flow cytometric analysis of neoplastic nodules and hepatocellular carcinomas induced by ciprofibrate in the rat

机译:环丙贝特致大鼠肿瘤性结节和肝细胞癌的流式细胞仪分析

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Alterations in DNA ploidy accompany hepatocellular carcinoma (HCC). However, changes in DNA content are also seen in regenerating liver and with increasing age. Thus, to investigate the role of DNA ploidy changes in development of HCC, flow cytometric DNA content determinations were done in a rat model system of peroxisome proliferator-induced HCC. Paraffin blocks of liver isolated from 18 Fisher 344 male rats fed ciprofibrate for 20 weeks (4), 40 weeks (4) or 20 months (10) were examined. Livers from age-matched control rats were also examined. From the 20 month ciprofibrate group, nine neoplastic nodules (NNs), 27 HCCs and four non-tumorous surrounding tissue controls (NTCs) were examined. Significant DNA tetraploid populations were seen in both the NNs and NTCs. A significant increase in the percentage of DNA diploid cells was observed in the NN samples. No significant difference in the percentage S-phase cells was seen. Emergence of cell populations with new DNA ploidy classes (8c or DNA aneuploid) as compared with NTCs was only seen in HCCs (7 of 27), and five of these seven were DNA aneuploid, as distinct from DNA tetraploid, populations. A total of 16 of 24 HCC samples that were adequate for cell cycle analysis had average percent S-phase greater than the mean of the NTCs plus three standard deviations. Although a direct role cannot be inferred, these results support the hypothesis that increases in the fraction of diploid cells is an important early event in the development of rat HCC and that further alterations in DNA ploidy and increased proliferative fraction accompany the development of HCC.
机译:DNA倍性的改变伴随着肝细胞癌(HCC)。然而,DNA含量的变化在肝脏再生和年龄增长中也可见。因此,为了研究DNA倍数变化在HCC发生中的作用,在过氧化物酶体增殖物诱导的HCC大鼠模型系统中进行了流式细胞术DNA含量测定。检查了从18只Fisher 344雄性大鼠喂食环丙贝特20周(4),40周(4)或20个月(10)分离出的肝石蜡块。还检查了年龄匹配的对照大鼠的肝脏。在20个月的环丙贝特组中,检查了9个肿瘤结节(NNs),27个HCC和4个非肿瘤性周围组织对照(NTC)。在NNs和NTCs中都发现了重要的DNA四倍体种群。在NN样品中观察到DNA二倍体细胞百分比的显着增加。观察到S期细胞百分比没有显着差异。与NTC相比,具有新的DNA倍性类别(8c或DNA非整倍体)的细胞群的出现仅在HCC中可见(27个中的7个),这七个中的五个是DNA非整倍体,与DNA四倍体不同。在足以进行细胞周期分析的24个HCC样本中,共有16个样本的S相平均百分比大于NTC的平均值加三个标准差。尽管不能推断其直接作用,但这些结果支持以下假说:二倍体细胞分数的增加是大鼠肝癌发展中的重要早期事件,DNA倍性的进一步改变和增殖分数的增加伴随着肝癌的发展。

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