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流式细胞术与乳腺癌中Ki67标记指数的比较:181例病例的前瞻性评估

Flow cytometry vs. Ki67 labelling index in breast cancer: a prospective evaluation of 181 cases.

作者信息

Martínez-Arribas F, Núñez M J, Piqueras V, Lucas A R, Sánchez J, Tejerina A, Schneider J

机构信息

Fundación Tejerina, Centro de Patología de la Mama, Madrid, Spain.

出版信息

Anticancer Res. 2002 Jan-Feb;22(1A):295-8.

Abstract

BACKGROUND

Excessive proliferation is one of the first steps in oncogenic activation and one of the most important biological features defining the aggressiveness of tumors. Quantifying the proportion of tumor cells in S-phase by means of flow cytometry has shown, in the past, to be useful for defining high-risk subgroups in breast cancer. Several antigens closely associated with proliferation are also detectable by means of immunohistochemistry, offering in theory an easy to perform and cheap alternative to flow cytometry for measuring proliferation. To test this hypothesis, we compared both methods prospectively in a series of breast cancers.

MATERIALS AND METHODS

We studied the proliferation rate of 181 breast cancers (152 ductal infiltrating, 17 lobular infiltrating, 12 other histological varieties), operated upon at our institution, by means of flow cytometry and the Ki67 labelling index, using the MIBI antibody. Ploidy (expressed as DNA content or DNA-index), S-phase fraction and the Ki67 labelling index were the variables of the study. The S-phase fraction was considered separately for diploid and aneuploid tumors, following the 1992 Maine Consensus guidelines and was judged abnormally elevated if higher than the 75th percentile for each group. The Ki67 labelling index was expressed as percent positive tumor cells, positive cells being those showing specific nuclear staining.

RESULTS

DNA-ploidy and the Ki67 labelling index could be evaluated in all tumors. Of the total, 96 (53%) were diploid and 85 (47%) aneuploid. S-phase fraction could be measured in 172 out of the 181 tumors (95%). The 75th percentile cut-offs for diploid and aneuploid tumors were 9.9% and 15.8%, respectively. We found a significant correlation beween rising DNA content and increasing Ki67 index (r = 0.18; p = 0.022), as well as between the percentage of cells in S-phase of the whole tumor population and Ki67 (r = 0.22; p = 0.0055). A Ki67 cut-off of 50% or higher identified most aneuploid tumors, or a small group of diploid ones with a high S-phase fraction (specificity = 96.7%; positive predictive value 92.5%), however at the price of a very low sensitivity (62.6%). This was due to the presence of many aneuploid tumors with a low S-phase fraction.

CONCLUSION

The Ki67 labelling index and S-phase fraction are significantly correlated. However, flow cytometry provides additional indirect information on tumor aggressiveness associated with DNA-ploidy. Further studies are needed to determine whether Ki67 alone is sufficient as a routinely applicable method.

摘要

背景

过度增殖是致癌激活的首要步骤之一,也是定义肿瘤侵袭性的最重要生物学特征之一。过去,通过流式细胞术对S期肿瘤细胞比例进行定量分析,已被证明有助于确定乳腺癌的高危亚组。通过免疫组织化学也可检测到几种与增殖密切相关的抗原,理论上为测量增殖提供了一种易于操作且成本低廉的替代流式细胞术的方法。为验证这一假设,我们对一系列乳腺癌患者进行了这两种方法的前瞻性比较。

材料与方法

我们采用流式细胞术和Ki67标记指数(使用MIBI抗体),对在我院接受手术治疗的181例乳腺癌患者(152例导管浸润性癌、17例小叶浸润性癌、12例其他组织学类型)的增殖率进行了研究。倍体(以DNA含量或DNA指数表示)、S期分数和Ki67标记指数是研究变量。根据1992年缅因州共识指南,分别对二倍体和非整倍体肿瘤的S期分数进行分析,若高于每组的第75百分位数,则判定为异常升高。Ki67标记指数以肿瘤细胞阳性百分比表示,阳性细胞为显示特异性核染色的细胞。

结果

所有肿瘤均能评估DNA倍体和Ki67标记指数。其中,96例(53%)为二倍体,85例(47%)为非整倍体。181例肿瘤中有172例(95%)可测量S期分数。二倍体和非整倍体肿瘤的第75百分位数临界值分别为9.9%和15.8%。我们发现DNA含量增加与Ki67指数升高之间存在显著相关性(r = 0.18;p = 0.022),以及整个肿瘤群体S期细胞百分比与Ki67之间存在显著相关性(r = 0.22;p = 0.0055)。Ki67临界值为50%或更高时,可识别出大多数非整倍体肿瘤,或一小部分S期分数较高的二倍体肿瘤(特异性 = 96.7%;阳性预测值92.5%),然而代价是灵敏度非常低(62.6%)。这是由于存在许多S期分数较低的非整倍体肿瘤。

结论

Ki67标记指数与S期分数显著相关。然而,流式细胞术提供了与DNA倍体相关的肿瘤侵袭性的额外间接信息。需要进一步研究以确定单独使用Ki67作为常规适用方法是否足够。

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