Nm-23, c-erbB-2, and progesterone receptor expression in invasive breast cancer: correlation with clinicopathologic parameters.

L L Nakopoulou, D Tsitsimelis, A C Lazaris, A Tzonou, H Gakiopoulou, C C Dicoglou, P S Davaris
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引用次数: 13

Abstract

Downregulation of nm-23 antimetastasis gene has been associated with disease progression in some human tumors. NPD kinase A is the product of the H1 isotype of the nm23 gene and its value as a marker of metastatic potential is well worth investigating. The expression of the nm23-H1 gene peptide was immunohistochemically evaluated in 191 primary mammary cancer tissues. A three-step immunoperoxidase staining procedure was performed and any association of our results with several classical clinicopathologic indicators, including hormonal status and c-erbB-2 oncoprotein membrane immunoexpression, was examined. NDP kinase A-positive cytoplasmic immunolabeling was noticed in 64% of all specimens (123/191) which frequently demonstrated positive progesterone receptor (PgR) status (p = 0.001) and were furthermore characterized by high PgR immunoreactivity rates. This association was significant by both univariate and multivariate statistical analysis. The double nm23-H1 (+)/PgR(+) phenotype was more frequently detected than any other combined phenotype of these markers. The nm23-H1 gene peptide was generally detected in a remarkable proportion of malignant cells, either in the invasive or the intraductal tumor components. Notably, large-cell ductal carcinomas in situ were characterized by lower nm23-H1 immunoreactivity rates when compared with other in situ cancer types. Quantitatively increased nm23-H1 immunopositive staining was more frequently observed in special histologic types of infiltrating cancers, in high nuclear grade tumors, as well as in carcinomas with high PgR levels (p = 0.05). The nm23-H1 (-)/c-erbB-2(+) phenotype was more often detected in the cancers of this study than the nm23-H1(+)/c-erbB-2(+) one. The former phenotype was correlated to postmenopausal ages as well as to extensive axillary nodal involvement by univariate statistical analysis. It is noteworthy that nm23-H1(-) status, on its own, was not statistically associated either with the presence or with a high number of involved lymph nodes. On the contrary, nm23-H1 immunopositivity was, paradoxically, more frequently observed in tumors of relatively increased TN tumor stage. Tumor progression is thus more likely to depend on the c-erbB-2 gene's overexpression. Possibly, any favorable outcome in nm23-H1(+) cases might be due to the fact that they also express PgR, which is a marker of a more functionally differentiated phenotype.
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浸润性乳腺癌中Nm-23、c-erbB-2和孕激素受体的表达:与临床病理参数的相关性
在一些人类肿瘤中,nm-23抗转移基因的下调与疾病进展有关。NPD激酶A是nm23基因H1同型的产物,其作为转移潜力标记物的价值值得研究。应用免疫组织化学方法检测了191例原发性乳腺癌组织中nm23-H1基因肽的表达。我们进行了三步免疫过氧化物酶染色,并检查了我们的结果与几个经典临床病理指标的关联,包括激素状态和c-erbB-2癌蛋白膜免疫表达。在所有标本中,有64%(123/191)的NDP激酶a阳性细胞质免疫标记显示为孕激素受体(PgR)阳性(p = 0.001),并且具有较高的PgR免疫反应率。单因素和多因素统计分析表明,这种关联是显著的。nm23-H1 (+)/PgR(+)双表型比这些标记的任何其他组合表型更常见。nm23-H1基因肽普遍在恶性细胞中检测到的比例显著,无论是浸润性肿瘤还是导管内肿瘤成分。值得注意的是,与其他原位癌类型相比,原位大细胞导管癌具有较低的nm23-H1免疫反应率。nm23-H1免疫阳性染色在特殊组织学类型的浸润性癌、高核级肿瘤以及高PgR水平的癌中更为常见(p = 0.05)。在本研究中,nm23-H1(-)/c-erbB-2(+)表型在癌症中比nm23-H1(+)/c-erbB-2(+)表型更常被检测到。通过单变量统计分析,前者表型与绝经后年龄以及广泛的腋窝淋巴结累及相关。值得注意的是,nm23-H1(-)状态本身与淋巴结的存在或受累淋巴结的数量均无统计学相关性。相反,nm23-H1免疫阳性在TN肿瘤分期相对增高的肿瘤中更为常见。因此,肿瘤的进展更可能取决于c-erbB-2基因的过度表达。nm23-H1(+)病例的任何有利结果可能是由于它们也表达PgR,这是功能分化表型的标志。
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