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与CD31相比,通过CD105表达评估血管生成在905例乳腺癌中的预后意义:与患者长期预后的相关性

Prognostic significance of angiogenesis evaluated by CD105 expression compared to CD31 in 905 breast carcinomas: correlation with long-term patient outcome.

作者信息

Dales Jean-Philippe, Garcia Stephane, Andrac Lucile, Carpentier Severine, Ramuz Olivier, Lavaut Marie-Noëlle, Allasia Claude, Bonnier Pascal, Charpin Colette

机构信息

Service d'Anatomie et de Cytologie Pathologiques, Hôpital Nord, 13915 Marseille Cedex 20, France.

出版信息

Int J Oncol. 2004 May;24(5):1197-204.

Abstract

Our purpose was to determine the respective prognostic significance of CD105 and CD31 immunoexpression in node negative patients with breast carcinoma, since angiogenesis induces blood borne metastases and death in carcinomas. CD105 (endoglin) has been reported as expressed by activated endothelial cells and consequently should better reflect neoangiogenesis in malignant tumors. Comparison of CD31 and CD105 immunocytochemical expression was undertaken in a series of 905 breast carcinomas. Results were compared to patients' long-term (median = 11.3 years) outcome. Univariate (Kaplan-Meier) analysis showed that the number of CD105+ microvessels (cut-off 15 vessels) correlated significantly with poor overall survival (p=0.001). This correlation was less significant in node negative patients (p=0.035). The number of CD31+ microvessels (cut-off 25 vessels) similarly correlated with poor survival (p=0.032) but not in the subgroup of node negative patients. Marked CD105 expression also correlated with a high risk for metastasis in all patients (p=0.0002) and in the subset of node negative patients (p=0.001). Similarly metastasis risk in node negative patients correlated with marked CD31 immunocytochemical expression (p=0.02). Multivariate analysis (Cox model) identified CD105, but not CD31 immunoexpression, as an independent prognostic indicator. Our results suggest that: i) in breast carcinomas, immunoselection of microvessels containing activated CD105 labelled endothelial cells is endowed with a stronger prognostic significance, as compared to CD31 vessels labelling; ii) the CD105 immunoexpression may be considered as a potential tool for selecting node negative patients with a poorer outcome and higher metastasis risk; iii) in these patients specific antiangiogenic therapy targeted by anti-CD105 conjugates can be further developed.

摘要

我们的目的是确定CD105和CD31免疫表达在淋巴结阴性乳腺癌患者中的各自预后意义,因为血管生成会诱导癌症的血行转移和死亡。据报道,CD105(内皮糖蛋白)由活化的内皮细胞表达,因此应能更好地反映恶性肿瘤中的新生血管形成。我们对905例乳腺癌进行了CD31和CD105免疫细胞化学表达的比较。将结果与患者的长期(中位时间=11.3年)预后进行比较。单因素(Kaplan-Meier)分析显示,CD105+微血管数量(临界值为15个血管)与总体生存率差显著相关(p=0.001)。这种相关性在淋巴结阴性患者中不太显著(p=0.035)。CD31+微血管数量(临界值为25个血管)同样与生存率差相关(p=0.032),但在淋巴结阴性患者亚组中无此相关性。显著的CD105表达在所有患者(p=0.0002)和淋巴结阴性患者亚组(p=0.001)中也与高转移风险相关。同样,淋巴结阴性患者的转移风险与显著的CD31免疫细胞化学表达相关(p=0.02)。多因素分析(Cox模型)确定CD105免疫表达而非CD31免疫表达为独立的预后指标。我们的结果表明:i)在乳腺癌中,与标记CD31的血管相比,对含有活化的CD105标记内皮细胞的微血管进行免疫选择具有更强的预后意义;ii)CD105免疫表达可被视为选择预后较差和转移风险较高的淋巴结阴性患者的潜在工具;iii)在这些患者中,可进一步开发以抗CD105偶联物为靶点的特异性抗血管生成疗法。

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