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首页> 外文期刊>Analytical cellular pathology: the journal of the European Society for Analytical Cellular Pathology >Evaluation of tumor heterogeneity of prostate carcinoma by flow- and image DNA cytometry and histopathological grading.
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Evaluation of tumor heterogeneity of prostate carcinoma by flow- and image DNA cytometry and histopathological grading.

机译:通过流式和图像DNA细胞计数法和组织病理学分级评估前列腺癌的肿瘤异质性。

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BACKGROUND: Heterogeneity of prostate carcinoma is one of the reasons for pretreatment underestimation of tumor aggressiveness. We studied tumor heterogeneity and the probability of finding the highest tumor grade and DNA aneuploidy with relation to the number of biopsies. MATERIAL AND METHODS: Specimens simulating core biopsies from five randomly selected tumor areas from each of 16 Bocking's grade II and 23 grade III prostate carcinomas were analyzed for tumor grade and DNA ploidy by flow- and fluorescence image cytometry (FCM, FICM). Cell cycle composition was measured by FCM. RESULTS: By determination of ploidy and cell cycle composition, morphologically defined tumors can further be subdivided. Heterogeneity of tumor grade and DNA ploidy (FCM) was 54% and 50%. Coexistence of diploid tumor cells in aneuploid specimens represents another form of tumor heterogeneity. The proportion of diploid tumor cells decreased significantly with tumor grade and with increase in the fraction of proliferating cell of the aneuploid tumor part. The probability of estimating the highest tumor grade or aneuploidy increased from 40% for one biopsy to 95% for 5 biopsies studied. By combining the tumor grade with DNA ploidy, the probability of detecting a highly aggressive tumor increased from 40% to 70% and 90% for one and two biopsies, respectively. CONCLUSION: Specimens of the size of core biopsies can be used for evaluation of DNA ploidy and cell cycle composition. Underestimation of aggressiveness of prostate carcinoma due to tumor heterogeneity is minimized by simultaneous study of the tumor grade and DNA ploidy more than by increasing the number of biopsies. The biological significance of coexistent diploid tumor cell in aneuploid lesions remains to be evaluated.
机译:背景:前列腺癌的异质性是治疗前低估了肿瘤侵袭性的原因之一。我们研究了肿瘤异质性以及发现最高肿瘤等级和DNA非整倍性与活检次数相关的可能性。材料与方法:通过流式和荧光图像细胞术(FCM,FICM)分析了16个博克II级和23级III级前列腺癌中每个随机选择的5个肿瘤区域的核心活检样本,以分析其肿瘤等级和DNA倍性。通过FCM测量细胞周期组成。结果:通过确定倍性和细胞周期组成,可以进一步细分形态学明确的肿瘤。肿瘤等级和DNA倍性(FCM)的异质性分别为54%和50%。非整倍体标本中二倍体肿瘤细胞的共存代表了肿瘤异质性的另一种形式。二倍体肿瘤细胞的比例随肿瘤等级和非整倍体肿瘤部分的增殖细胞比例的增加而显着降低。估计最高肿瘤等级或非整倍性的可能性从一项活检的40%增加到五项活检的95%。通过将肿瘤等级与DNA倍性相结合,对于一次活检和两次活检,检测到高度侵袭性肿瘤的可能性分别从40%增加到70%和90%。结论:核心活检标本的大小可用于评估DNA倍性和细胞周期组成。通过同时研究肿瘤等级和DNA倍体性,而不是通过增加活检数量,可以将因肿瘤异质性而引起的前列腺癌侵略性低估降至最低。非整倍性病变中共存的二倍体肿瘤细胞的生物学意义尚待评估。

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