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多指标分析血管生成和淋巴管生成因子可预测非小细胞肺癌患者的预后。

Multiplexed analysis of angiogenesis and lymphangiogenesis factors predicts outcome for non-small cell lung cancer patients.

机构信息

Third Department of Medicine, Sotiria General Hospital, Athens, Greece.

出版信息

Virchows Arch. 2011 Mar;458(3):331-40. doi: 10.1007/s00428-010-1015-4. Epub 2010 Dec 14.

DOI:10.1007/s00428-010-1015-4
PMID:21161269
Abstract

Angiogenesis and lymphangiogenesis are key components of non-small cell lung cancer (NSCLC) tumor growth and metastatic spread; however, the prognostic and predictive role of angiogenic and lymphangiogenic biomarkers remains controversial for NSCLC patients. We assessed VEGF, VEGFC, VEGFD, VEGFR3 protein expression, tumor microvessel, and lymphatic vessel (LmVD) density by immunohistochemistry in 103 NSCLC; biomarkers were analyzed individually as well as multiplexed with each other. No correlations were identified between VEGF, VEGFC, VEGFD, or LmVD and clinical characteristics. VEGFR3 was correlated with VEGFC (p = 0.03), VEGFD (p < 0.0001), and intratumor LmVD (p = 0.03). Tumors that did not express VEGFR3 had a worse prognosis (log rank p = 0.03). VEGF was significantly correlated with survival in adenocarcinomas (log rank p = 0.014) but not in squamous cell carcinomas (log rank p = 0.5). Multivariate Cox regression analysis confirmed the independent prognostic potential of VEGFR3 (hazard ratio (HR) = 0.05; 95% confidence intervals (CI) = 0.008-0.32, p = 0.002) for all patients and VEGF (HR = 8.69, 95% CI = 1.4-53.69, p = 0.02) for adenocarcinomas. When biomarkers were multiplexed, only stage and VEGFC expression were independent predictors of survival for all patients. Weighted expression of VEGFC, VEGFR3, and stage was used to build a prognostic classifier for stage I-IIIA patients; patients in the low risk group had prolonged survival compared with high risk patients (log rank p = 0.02). There was no association between biomarkers and early recurrence or response to treatment. Angiogenic and lymphangiogenic biomarkers studied define subgroups of patients at high risk and may be useful for prognostic stratification of NSCLC patients especially those with early stage disease.

摘要

血管生成和淋巴管生成是非小细胞肺癌 (NSCLC) 肿瘤生长和转移扩散的关键组成部分;然而,血管生成和淋巴管生成生物标志物对 NSCLC 患者的预后和预测作用仍存在争议。我们通过免疫组织化学方法评估了 103 例 NSCLC 中的 VEGF、VEGFC、VEGFD、VEGFR3 蛋白表达、肿瘤微血管和淋巴管 (LmVD) 密度;生物标志物单独进行分析,并相互组合进行分析。VEGF、VEGFC、VEGFD 或 LmVD 与临床特征之间均无相关性。VEGFR3 与 VEGFC(p=0.03)、VEGFD(p<0.0001)和肿瘤内 LmVD(p=0.03)相关。不表达 VEGFR3 的肿瘤预后更差(对数秩检验 p=0.03)。VEGF 在腺癌中与生存显著相关(对数秩检验 p=0.014),但在鳞癌中无相关性(对数秩检验 p=0.5)。多变量 Cox 回归分析证实 VEGFR3(危险比 (HR)=0.05;95%置信区间 (CI)=0.008-0.32,p=0.002)对所有患者和 VEGF(HR=8.69,95% CI=1.4-53.69,p=0.02)对腺癌有独立的预后预测能力。当生物标志物组合时,只有分期和 VEGFC 表达是所有患者生存的独立预测因素。VEGFC、VEGFR3 和分期的加权表达用于构建 I-IIIA 期患者的预后分类器;低危组患者的生存时间长于高危患者(对数秩检验 p=0.02)。生物标志物与早期复发或治疗反应之间无关联。研究中的血管生成和淋巴管生成生物标志物定义了高危患者亚组,可能对 NSCLC 患者,特别是早期疾病患者的预后分层有用。

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本文引用的文献

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Maspin 表达降低合并血管内皮生长因子 C 升高与非小细胞肺癌不良预后相关。
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