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中华乳腺病杂志(电子版)

中华乳腺病杂志(电子版) ›› 2015, Vol. 09 ›› Issue (06) : 380 -386. doi: 10.3877/cma. j. issn.1674-0807.2015.06.007

论著

CK5/6 和Ki67 表达与乳腺癌分子病理特征关系的临床分析
邓淼1, 刘江波1,(), 刘起鹏1, 张婷1, 田燕晓2, 陈登庭1, 邢鲁奇2   
  1. 1.471003 洛阳,河南科技大学第一附属医院乳腺外科
    2.471003 洛阳,河南科技大学第一附属医院病理科
  • 收稿日期:2015-07-09 出版日期:2015-12-01
  • 通信作者: 刘江波
  • 基金资助:
    洛阳市应用技术研究与开发基金(0802021A)河南科技大学第一附属医院博士科研启动基金(0801-2014)

Correlation of CK5/6 and Ki67 expression with molecular pathological features of breast cancer

Miao Deng1, Jiangbo Liu1,(), Qipeng Liu1, Ting Zhang1, Yanxiao Tian2, Dengting Chen1, Luqi Xing2   

  1. 1.Department of Breast Surgery
    2.Department of Pathology, the First Affiliated Hospital, Henan University of Science and Technology, Luoyang 471003, China.
  • Received:2015-07-09 Published:2015-12-01
  • Corresponding author: Jiangbo Liu
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引用本文:

邓淼, 刘江波, 刘起鹏, 张婷, 田燕晓, 陈登庭, 邢鲁奇. CK5/6 和Ki67 表达与乳腺癌分子病理特征关系的临床分析[J/OL]. 中华乳腺病杂志(电子版), 2015, 09(06): 380-386.

Miao Deng, Jiangbo Liu, Qipeng Liu, Ting Zhang, Yanxiao Tian, Dengting Chen, Luqi Xing. Correlation of CK5/6 and Ki67 expression with molecular pathological features of breast cancer[J/OL]. Chinese Journal of Breast Disease(Electronic Edition), 2015, 09(06): 380-386.

目的

研究CK 5/6 和Ki67 在乳腺癌组织中的表达及其临床意义。

方法

回顾性收集2011 年2 月至2014 年7 月在河南科技大学第一附属医院接受改良根治术的乳腺癌患者109 例,用免疫组织化学法检测癌组织CK5/6 和Ki67 表达,分析其与乳腺癌分子病理特征的关系。 计数资料采用χ2检验或Fisher 确切概率法,相关性分析采用Spearman 相关分析,并用Logistic 回归分析CK5/6 表达的独立影响因素。

结果

109 例乳腺癌组织中CK5/6 和Ki67 表达率分别为22.02%(24/109)、62.04%(67/108,1 例表达未能判断);三阴性乳腺癌(TNBC)中CK5/6 表达率为62.2%(23/37),显著高于非TNBC的4.6%(3/66)(χ2=41.708,P<0.001);Ki67 表达在分子分型间差异无统计学意义(χ2 =0.147,P<0.001)。 CK5/6 表达与ER、PR 及E-钙黏蛋白表达负相关(r=-0.505、-0.417、-0.239,P 均<0.050),而ER 缺失是影响CK5/6 表达的独立因素(OR=0.099,95%CI=0.023 ~0.424)。 基底样型乳腺癌(BLBC)(TNBC-CK5/6+)的E-钙黏蛋白表达显著低于非BLBC(χ2=6.669,P=0.010)。 在TNBC,仅Ki67 与组织学分级正相关外(r=0.354,P=0.043)。

结论

CK5/6 表达标记的BLBC 易发生侵袭转移的特性可能与E-钙黏蛋白表达缺失有关,而Ki67 表达可能不是识别BLBC 生物学特性的分子标记。

关键词: 乳腺肿瘤, 角蛋白质类, Ki-67 抗原, 分子分型

Objective

To study the expression of cytokeratin 5/6 (CK5/6) and Ki67 in breast cancer and clinical significance.

Methods

The clinical data of 109 breast cancer patients treated with modified radical mastectomy in the First Affiliated Hospital of Henan University of Science and Technology from February 2011 to July 2014 were retrospectively collected. The expressions of CK5/6 and Ki67 in breast cancer tissues were detected by immunohistochemical staining, and their association with molecular pathological features of breast cancer was analyzed. Numeration data was processed using χ2 test or Fisher's exact test, correlation analysis was performed using Spearman method, and Logistic regression was used for analyzing the independent factors in CK5/6 expression.

Results

The positive rates of CK5/6 and Ki67 expression in breast cancer tissue were 22.02% (24/109) and 62.04% (67/108, one case was not detected) respectively. The positive rate of CK5/6 expression was 62.2% (23/37) in triple negative breast cancer (TNBC), significantly higher than that in non-TNBC (χ2 =41.708, P<0.001); while the expression of Ki67 presented no statistical difference in different molecular subtypes of breast cancer(χ2 = 0.147,P <0.001). CK5/6 expression was negatively correlated with ER, PR, and E-cadherin expression in breast cancer (r=-0.505, -0.417, -0.239,all P <0.050). Moreover, the deficiency of ER expression was an independent factor influencing CK5/6 expression(OR=0.099,95% CI=0.023-0.424). Ki67 expression was not correlated with other molecular markers including ER, PR, HER-2 and E-cadherin. The expression of E-cadherin in basal-like breast cancer (BLBC)was significantly lower than that in non-BLBC (χ2=6.669,P=0.010). In TNBC, the expressions of CK5/6 and Ki67 were positively associated with Ki67 and histological grade (r=0.354, P=0.043).

Conclusion

The malignant biological features of invasion and metastasis in BLBC with CK5/6 positive expression may be related with E-cadherin expression deficiency, while Ki67 expression may not be a molecular marker to identify BLBC.

Key words: Breast neoplasms, Keratins, Ki-67 antigen, Molecular typing
表1 影响乳腺癌CK5/6 表达的分子指标Logistic 回归变量赋值表
变量 变量分类及赋值
CK5/6 阴性=1,阳性=2
Ki67 阴性=1,阳性=2
HER-2 阴性=1,阳性=2
ER 阴性=1,阳性=2
PR 阴性=1,阳性=2
E-钙黏蛋白 阴性=1,阳性=2
表2 109 例乳腺癌组织中CK5/6 和Ki67 表达与乳腺癌临床病理特征之间的关系
临床病理特征 例数 CK5/6(例) χ2 P Ki67(例) χ2 P
阴性 阳性 阴性 阳性
组织学分级a
1、2级 69 55 14 0.779 0.377 27 42 2.781 0.095
3级 28 20 8 6 22
肿瘤直径b
≤2 cm 28 23 5 0.192 0.661 11 17 0.064 0.800
>2 cm 64 50 14 23 40
TNM分期c
Ⅰ期+Ⅱ期 58 47 11 0.272 0.602 24 33 1.466 0.226
Ⅲ期+Ⅳ期 34 26 8 10 24
腋窝淋巴结转移
阴性 50 36 14 0.517 0.472 21 30 0.424 0.515
阳性 59 46 13 20 37
表3 109 例乳腺癌组织中CK5/6 和Ki67 表达与肿瘤分子指标的关系
分子指标 例数 CK5/6(例) r P Ki67a(例) r P
阴性 阳性 阴性 阳性
Ki67a
阴性 41 34 7 0.128 0.186
阳性 67 48 19
ERb
阴性 49 25 24 -0.505 <0.001 16 32 0.076 0.440
阳性 59 56 3 24 35
PRc
阴性 71 44 27 -0.417 <0.001 25 45 -0.046 0.627
阳性 37 37 0 15 22
HER-2
阴性 100 73 27 -0.172 0.073 40 59 0.167 0.084
阳性 9 9 0 1 8
E-钙黏蛋白
阴性 50 32 18 -0.239 0.012 18 31 -0.023 0.813
阳性 59 50 9 23 36
表4 乳腺癌CK5/6 表达与分子指标关系的Logistic 回归分析(n=107)
因素 回归系数 标准误 Wald P OR 95%CI
ER -2.310 0.742 9.708 0.002 0.099 0.023~0.424
常量 43.241 13794.080 0.000 0.997 6.018
表5 CK5/6 和Ki67 在不同分子分型乳腺癌中的表达(例)
分子分型 例数 CK5/6 Ki67
阴性 阳性 阴性 阳性
非TNBC
luminal Aa 12 12 0
luminal Bb 47 44 3 12 35
HER-2过表达c 7 7 0 0 7
TNBCde 37 14 23 13 24
χ2 42.000 <0.001
P 3.831 0.147
表6 38 例TNBC 中CK5/6 和Ki67 表达与肿瘤分子病理特征的相关性关系
分子病理特征 例数 CK5/6 r P Ki67 r P
阴性 阳性 阴性 阳性
Ki67a
阴性 13 6 7 0.126 0.457
阳性 24 8 16
E-钙黏蛋白
阴性 24 8 16 -0.126 0.457 9 15 0.067 0.692
阳性 13 6 7 4 9
组织学分级b
2级 20 9 11 0.065 0.721 8 12 0.354 0.043
3级 13 5 8 1 12
肿瘤直径c
≤2 cm 6 1 5 -0.224 0.243 2 4 -0.026 0.896
>2 cm 23 10 13 8 14
TNM分期d
Ⅰ期+Ⅱ期 18 7 11 0.025 0.897 6 11 -0.011 0.956
Ⅲ期+Ⅳ期 11 4 7 4 7
腋窝淋巴结转移
阴性 20 9 11 0.160 0.344 8 12 0.111 0.515
阳性 17 5 12 5 12
表7 CK5/6 表达标记的BLBC 与非BLBC 的分子病理特征比较
分子病理特征 例数 非BLBC BLBC χ2 P
Ki67
阴性 40 33 7 0.604 0.437
阳性 67 51 16
E-钙黏蛋白
阴性 49 33 16 6.669 0.010
阳性 58 51 7
组织学分级a
1+2级 68 57 11 1.919 0.166
3级 28 20 8
肿瘤直径b
≤2 cm 27 22 5 0.003 0.953
>2 cm 63 51 12
TNM分期c
Ⅰ期+Ⅱ期 56 46 10 0.103 0.748
Ⅲ期+Ⅳ期 34 27 7
腋窝淋巴结转移
阴性 48 37 11 0.104 0.747
阳性 59 47 12
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