[化疗对乳腺癌患者循环血管生成因子水平的影响]
[Effects of chemotherapy on circulating angiogenic factor levels in patients with breast cancer].
作者信息
Tang Jin-hai, Zhao Jian-hua, Gong Jian-ping, Qin Jian-wei, Pan Li-qun, Xu Zhi-yin
机构信息
Department of Surgery, Jiangsu Tumor Hospital, Nanjing 210009, China.
出版信息
Zhonghua Zhong Liu Za Zhi. 2007 Mar;29(3):210-4.
OBJECTIVE
To study the changes in circulating VEGF and endostatin (ES) levels during chemotherapy for patients with breast cancer, and their correlation with efficacy of chemotherapy.
METHODS
40 breast cancer patients with metastases were included in this study. They received TAC/TEC, CAF/CEF, NP, CAP, CMF, TFP, TA or TC regime chemotherapy, respectively. Totally 120 serum samples were collected from the patients at three time points: before chemotherapy, the end of 1 and 5-6 chemotherapy cycles, and analyzed for VEGF and ES levels using ELISA. Tumor agiogenesis activity was evaluated by serum soluble vascular cell adhesion molecule (VCAM - 1) measured by ELISA as a surrogate marker.
RESULTS
(1) Before chemotherapy, the median level of VEGF in patients with breast cancer was 496.6 pg/ml, 4.7 times higher than that of healthy controls (P <0.001). The median level of ES was 95.5 ng/ml, 18.3% lower than that of healthy controls (P = 0.183). VCAM-1 was 1077.1 ng/ml and higher than that of controls (P <0.001). The serum VEGF levels correlated with VCAM-1 levels, tumor staging and metastatic sites (P <0.05). (2) At the end of 1 cycle of chemotherapy, the serum VEGF level (median 524.8 pg/ml) was higher than the pretreatment values (P = 0.047), whereas the levels of ES and VCAM-1 were not significantly altered (110.5 ng/ml, P = 0.055; and 975.6 ng/ml, P = 0.27). (3) At the end of 5-6 cycles, the changes in VEGF correlated with the response to chemotherapy. Serum VEGF levels in 27 patients with chemotherapy-responsive and stable disease showed a significant decrease (median 287.4 pg/ml) , but not observed in 13 patients with progressive disease. VCAM-1 also showed a treatment-related change like VEGF. However, chemotherapy might only have a minor effect on ES, because there was no significant difference in the ES levels among 5-6 cycle patients, 1 cycle patients and healthy controls, and neither between therapy-responsive patients.
CONCLUSION
Intensive chemotherapy for breast cancer results in a significant decrease of serum VEGF level, which might be an indicator of the controlled disease status, and following the treatment-induced response or stabilization, the tumor angiogenesis seems to change into an anti-angiogenesis direction.
目的
研究乳腺癌患者化疗期间循环血管内皮生长因子(VEGF)和内皮抑素(ES)水平的变化及其与化疗疗效的相关性。
方法
本研究纳入40例有转移的乳腺癌患者。他们分别接受TAC/TEC、CAF/CEF、NP、CAP、CMF、TFP、TA或TC方案化疗。在化疗前、化疗第1周期结束时以及第5 - 6周期结束时这三个时间点从患者身上共采集120份血清样本,采用酶联免疫吸附测定法(ELISA)分析VEGF和ES水平。通过ELISA检测血清可溶性血管细胞黏附分子(VCAM - 1)作为替代标志物来评估肿瘤血管生成活性。
结果
(1)化疗前,乳腺癌患者VEGF的中位水平为496.6 pg/ml,比健康对照者高4.7倍(P <0.001)。ES的中位水平为95.5 ng/ml,比健康对照者低18.3%(P = 0.183)。VCAM - 1为1077.1 ng/ml,高于对照者(P <0.001)。血清VEGF水平与VCAM - 1水平、肿瘤分期及转移部位相关(P <0.05)。(2)化疗第1周期结束时,血清VEGF水平(中位值524.8 pg/ml)高于治疗前水平(P = 0.047),而ES和VCAM - 1水平无显著变化(分别为110.5 ng/ml,P = 0.055;975.6 ng/ml,P = 0.27)。(3)在第5 - 6周期结束时,VEGF的变化与化疗反应相关。27例化疗敏感且病情稳定患者的血清VEGF水平显著下降(中位值287.4 pg/ml),而13例病情进展患者未观察到这种下降。VCAM - 1也呈现出与VEGF类似的与治疗相关的变化。然而,化疗对ES可能仅有轻微影响,因为第5 - 6周期患者、第1周期患者和健康对照者之间的ES水平无显著差异,治疗敏感患者之间也无差异。
结论
乳腺癌强化化疗导致血清VEGF水平显著下降,这可能是疾病得到控制的一个指标,并且在治疗引起反应或病情稳定后,肿瘤血管生成似乎转变为抗血管生成方向。
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