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目前用于测量乳腺癌及其他实体瘤瘤内微血管密度的病理方法。

Current pathologic methods for measuring intratumoral microvessel density within breast carcinoma and other solid tumors.

作者信息

Weidner N

机构信息

Department of Pathology, University of California, San Francisco 94143-0102, USA.

出版信息

Breast Cancer Res Treat. 1995;36(2):169-80. doi: 10.1007/BF00666038.

Abstract

Abundant evidence has shown that tumor growth and metastasis are dependent upon tumor angiogenesis (TA). TA refers to the growth of new vessels toward and within the tumor. Until TA occurs, tumors grow no larger than 2-4 mm in diameter. Also, TA is necessary at the beginning and at the end of the metastatic cascade of events. Thus, it seems reasonable that increasing intratumoral microvascular density (iMVD) might correlate with greater tumor aggressiveness, such as a higher frequency of metastases and/or decreased survival. Indeed, in 1991 my colleagues and I reported a statistically significant association between greater incidence of metastases in patients with breast carcinoma and increasing iMVD. Microvessel density was measured with a light microscope in a single area of invasive tumor (200x field or 0.74 mm2) representative of the highest microvessel density (neovascular "hot spot"). This was done after endothelial cells, lining the microvessels, had been highlighted with anti-factor VIII-related antigen/von Willebrand's factor (F8RA/vWF). Subsequent studies by other investigators, using either anti-F8RA/vWF or other relatively vessel-specific reagents such as anti-CD31, have shown that the association of greater tumor aggressiveness with increasing iMVD exists not only in breast carcinoma, but also in other solid tumors. This article reviews the methods of highlighting intratumoral vessels and describes the techniques for counting these vessels for assessing iMVD.

摘要

大量证据表明,肿瘤生长和转移依赖于肿瘤血管生成(TA)。TA是指新血管向肿瘤内部生长。在TA发生之前,肿瘤直径不会超过2 - 4毫米。此外,TA在转移级联反应的起始和终末阶段都是必需的。因此,肿瘤内微血管密度(iMVD)增加可能与更高的肿瘤侵袭性相关,如转移频率更高和/或生存率降低,这似乎是合理的。事实上,1991年我和我的同事报告了乳腺癌患者转移发生率增加与iMVD升高之间存在统计学显著关联。微血管密度是在代表最高微血管密度(新生血管“热点”)的侵袭性肿瘤单一区域(200倍视野或0.74平方毫米)用光学显微镜测量的。这是在用抗因子VIII相关抗原/血管性血友病因子(F8RA/vWF)突出显示微血管内衬的内皮细胞后进行的。其他研究者随后使用抗F8RA/vWF或其他相对血管特异性试剂(如抗CD31)进行的研究表明,更高的肿瘤侵袭性与iMVD增加之间的关联不仅存在于乳腺癌中,也存在于其他实体瘤中。本文回顾了突出肿瘤内血管的方法,并描述了计数这些血管以评估iMVD的技术。

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