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不同的血管生成模式与乳腺高级别导管原位癌相关。

Distinct angiogenic patterns are associated with high-grade in situ ductal carcinomas of the breast.

作者信息

Engels K, Fox S B, Whitehouse R M, Gatter K C, Harris A L

机构信息

Department of Cellular Science, John Radcliffe Hospital, University of Oxford, U.K.

出版信息

J Pathol. 1997 Feb;181(2):207-12. doi: 10.1002/(SICI)1096-9896(199702)181:2<207::AID-PATH758>3.0.CO;2-4.

Abstract

Angiogenesis, the formation of new blood vessels from the existing vascular network, has been demonstrated to be an important prognostic factor in invasive breast carcinoma. The switch to an angiogenic phenotype represents a growth-limiting step during carcinogenesis and might, in pre-invasive lesions, indicate the risk for developing an invasive phenotype. The discrepancy between modern therapy options for invasive breast carcinomas and the relatively aggressive treatment of in situ lesions underlines the need for such prognostic factors for ductal in situ breast carcinomas (DCIS). Patterns of vascularity were examined in 75 formalin-fixed, paraffin-embedded DCIS by immunohistochemical staining of vessels using antibodies against Factor VIII-related antigen. Histological classification was performed according to four different systems, based on architectural or cytonuclear features, or a combination of both. Two distinct vascular patterns were observed: a diffuse increase of stromal vascularity between duct lesions (pattern I), which was present alone in 8/75 (11 per cent), and a dense rim of microvessels adjacent to the basement membrane of individual ducts (pattern II), present alone in 12/75 (16 per cent). In total, 57 per cent (43/75) showed pattern 1 and 62 per cent (47/75) showed pattern II. There was a significant correlation between these patterns (P = 0.0001; chi 2 = 15.1), such that both were present in 35 (47 per cent). These different vascular patterns imply two angiogenic pathways: one pathway mediated by angiogenic factors released directly by tumour cells resulting in the rim of vessels and another generated indirectly via recruitment of accessory cells such as macrophage and endothelial cells, which themselves release other angiogenic factors, causing the increase of stromal vascularity. A significant increase in both stromal vascularity (pattern I) and the presence of a rim (pattern II) was observed in high-grade DCIS lesions (P = 0.005 and P = 0.037). Indeed, all the patient relapses occurred in these high-grade lesions, but due to the small number of patient events, no significant correlation of vascular pattern to survival was observed (P > 0.05). This study suggests that distinct patterns of vascularity in DCIS might be useful for identifying patients who are at risk of relapse.

摘要

血管生成是指从现有的血管网络形成新的血管,它已被证明是浸润性乳腺癌的一个重要预后因素。向血管生成表型的转变代表了致癌过程中的一个生长限制步骤,并且在癌前病变中可能预示着发展为浸润性表型的风险。浸润性乳腺癌的现代治疗方案与原位病变相对积极的治疗之间存在差异,这凸显了导管原位乳腺癌(DCIS)此类预后因素的必要性。通过使用抗VIII因子相关抗原的抗体对血管进行免疫组织化学染色,对75例福尔马林固定、石蜡包埋的DCIS的血管模式进行了检查。根据四种不同的系统进行组织学分类,这些系统基于结构或细胞核特征,或两者的组合。观察到两种不同的血管模式:导管病变之间间质血管的弥漫性增加(模式I),单独出现于8/75例(11%);以及单个导管基底膜附近微血管的致密边缘(模式II),单独出现于12/75例(16%)。总体而言,57%(43/75)表现为模式I,62%(47/75)表现为模式II。这些模式之间存在显著相关性(P = 0.0001;χ² = 15.1),两者同时存在于35例(47%)中。这些不同的血管模式意味着两条血管生成途径:一条途径由肿瘤细胞直接释放的血管生成因子介导,导致血管边缘形成;另一条途径通过招募辅助细胞如巨噬细胞和内皮细胞间接产生,这些细胞自身释放其他血管生成因子,导致间质血管增加。在高级别DCIS病变中观察到间质血管(模式I)和边缘的存在(模式II)均显著增加(P = 0.005和P = 0.037)。事实上,所有患者复发均发生在这些高级别病变中,但由于患者事件数量较少,未观察到血管模式与生存之间的显著相关性(P > 0.05)。这项研究表明,DCIS中不同的血管模式可能有助于识别有复发风险的患者。

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