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对霍奇金病患者连续淋巴结样本进行流式细胞术分析:一次活检内结果可重复吗?

Flow cytometric analysis of consecutive lymph node samples from patients with Hodgkin's disease: reproducible within one biopsy?

作者信息

Pasman P C, Erdkamp F L, Breed W P, Janssen W C, Hoffmann J J, Schutte B, Vrints L W, Schouten H C

机构信息

University Hospital Maastricht, Department of Internal Medicine, The Netherlands.

出版信息

Leuk Lymphoma. 1996 Jul;22(3-4):339-44. doi: 10.3109/10428199609051766.

Abstract

In Hodgkin's disease DNA aneuploidy is not a prognostic factor. However, the prognostic significance of DNA content in Hodgkin's disease may be missed by either intratumor DNA heterogeneity or DNA analysis of limited samples. For flow cytometry usually one section of 40-60 microns is used for the analysis. In breast cancer this proved to be insufficient. In Hodgkin's disease no data are available. Therefore, we examined if analysis of more sections does increase the yield of aneuploidy. Archival, formalin-fixed, parafin embedded tissues were used. From 13 patients four sections of 50 microns could be analysed for DNA content. In 12 of 13 patients the results were consistent in all four sections of one patient case; seven diploid, four aneuploid and one multiploid. In one case ploidy status changed: two sections were diploid and two were aneuploid. The DNA-index of the aneuploid samples ranged from 0.75 to 1.38 and varied from 0.02 to 0.14 within one case. The S-phase fraction remained constant within all evaluable cases (sd: 0.5-1.5%), except for one (sd: 4.7%). In conclusion, in Hodgkin's disease the ploidy status of the first section can be regarded to represent the whole tissue sample. Therefore, the absence of prognostic value of ploidy status is not explained by sampling errors in tissues analysed.

摘要

在霍奇金病中,DNA非整倍体不是一个预后因素。然而,霍奇金病中DNA含量的预后意义可能会因肿瘤内DNA异质性或有限样本的DNA分析而被忽视。对于流式细胞术,通常使用40 - 60微米的一个切片进行分析。在乳腺癌中,这已被证明是不够的。在霍奇金病中尚无相关数据。因此,我们研究了分析更多切片是否确实能提高非整倍体的检出率。使用了存档的、福尔马林固定、石蜡包埋的组织。对13例患者的四个50微米切片进行了DNA含量分析。在13例患者中的12例,一个病例的所有四个切片结果一致;7例二倍体,4例非整倍体,1例多倍体。在一个病例中,倍体状态发生了变化:两个切片为二倍体,两个为非整倍体。非整倍体样本的DNA指数范围为0.75至1.38,在一个病例中变化范围为0.02至0.14。除了一个病例(标准差:4.7%)外,所有可评估病例中的S期分数保持恒定(标准差:0.5 - 1.5%)。总之,在霍奇金病中,第一个切片的倍体状态可被视为代表整个组织样本。因此,倍体状态缺乏预后价值不能用所分析组织的抽样误差来解释。

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