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nm23、血管生成与淋巴结阴性乳腺癌转移倾向之间的关系。

The relationship between nm23, angiogenesis, and the metastatic proclivity of node-negative breast cancer.

作者信息

Heimann R, Ferguson D J, Hellman S

机构信息

Department of Radiation and Cellular Oncology, The Pritzker School of Medicine, The University of Chicago, Illinois 60637, USA.

出版信息

Cancer Res. 1998 Jul 1;58(13):2766-71.

PMID:9661889
Abstract

Distant metastases are the major cause of morbidity and mortality in women with breast cancer. The prediction of this metastatic proclivity is essential in determining prognosis and should allow an appropriate choice of therapy. A critical look at the metastatic process and its phenotypic expression offers an opportunity to identify some of the important events in the process that may relate to prognosis, with the goal of identifying those patients with occult metastases and also sparing systemic treatment in those patients whose tumors have not developed the capacity for distant spread. To evaluate the significance of nm23 and angiogenesis in the metastatic cascade, we used archival material from 163 node-negative breast cancer patients who had a median follow-up of 14 years. All patients underwent mastectomy and received no adjuvant chemotherapy or hormone or radiation therapy. Immunohistochemistry was used to detect nm23-H1 expression, whereas angiogenesis was determined by microvessel count (MVC). We found the 15-year disease-free survival (DFS) to be significantly better in patients with high nm23 compared with low nm23 (91% compared with 70%, P = 0.008). Low MVC is associated with excellent (92%) long-term DFS. In those patients with high MVC, high nm23 allows the identification of a subgroup with significantly higher DFS (90% compared with 66%, P = 0.02). Among high nuclear grade tumors, if nm23 is high, the DFS is significantly better (89% compared with 68%, P = 0.03). Thus, nm23 is still associated with excellent survival, even when there is unfavorable angiogenesis or nuclear grade. Multivariate analysis confirms that nm23 and MVC are important prognostic factors. High MVC appears necessary but not sufficient for metastasis to occur, whereas low nm23 may further contribute to metastatic progression. Both nm23 and MVC contribute valuable information in characterizing the malignant phenotype.

摘要

远处转移是乳腺癌女性发病和死亡的主要原因。预测这种转移倾向对于确定预后至关重要,并且应有助于做出合适的治疗选择。深入研究转移过程及其表型表达,为识别该过程中一些可能与预后相关的重要事件提供了机会,目的是识别那些有隐匿性转移的患者,并避免对那些肿瘤尚未发展出远处扩散能力的患者进行全身治疗。为了评估nm23和血管生成在转移级联反应中的意义,我们使用了163例淋巴结阴性乳腺癌患者的存档材料,这些患者的中位随访时间为14年。所有患者均接受了乳房切除术,未接受辅助化疗、激素治疗或放射治疗。采用免疫组织化学检测nm23-H1表达,而通过微血管计数(MVC)确定血管生成情况。我们发现,nm23高表达的患者15年无病生存率(DFS)显著高于nm23低表达的患者(分别为91%和70%,P = 0.008)。低MVC与出色的(92%)长期DFS相关。在MVC高的患者中,nm23高表达可识别出DFS显著更高的亚组(分别为90%和66%,P = 0.02)。在高核分级肿瘤中,如果nm23高表达,DFS显著更好(分别为89%和68%,P = 0.03)。因此,即使存在不利的血管生成或核分级,nm23仍与良好的生存率相关。多因素分析证实nm23和MVC是重要的预后因素。高MVC似乎是转移发生的必要但非充分条件,而低nm23可能进一步促进转移进展。nm23和MVC在表征恶性表型方面都提供了有价值的信息。

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