Falk Roni T, Staff Annetine Cathrine, Bradwin Gary, Karumanchi S Ananth, Troisi Rebecca
Metabolic Epidemiology Branch, Division of Cancer Epidemiology and Genetics, NCI, 9609 Medical Center Drive, Bethesda, MD, 20852, USA.
Women and Children's Division, Department of Gynecology and Obstetrics, Oslo University Hospital, Ullevål, 0424, Oslo, Norway.
Cancer Causes Control. 2016 Aug;27(8):1009-17. doi: 10.1007/s10552-016-0779-5. Epub 2016 Jun 29.
Pro-angiogenic factors are positively associated with breast tumor staging and poorer prognosis, but their role in the etiology of breast cancer has not been assessed.
We measured serum levels of the pro-angiogenic vascular endothelial growth factor A (VEGF), and placental growth factor (PlGF) and anti-angiogenic soluble fms-like tyrosine kinase-1 (sFlt-1) in 352 incident breast cancer cases [mean age at diagnosis 67 (range 55-83)] and 352 non-cases in the prostate, lung, colorectal, and ovarian screening trial (women enrolled 1993-2001, followed through 2005) matched on age and date of enrollment. Cases were followed on average 4.2 years from blood draw to diagnosis, range 3.9-12.8 years; 53 % were estrogen receptor positive/progesterone receptor positive (ER+/PR+), and 13 % were ER-/PR-. Quartile-specific hazard ratios (HR) and 95 % confidence intervals (CI) were estimated using weighted Cox proportional hazards regression models adjusted for known breast cancer risk factors. An ordinal variable for the angiogenic markers was used to test for trend in the HR.
Comparing the highest to lowest quartile, multivariable HR were 0.90 for VEGF (95 % CI 0.33-2.43, p trend = 0.88), 1.38 for sFlt-1 (95 % CI 0.63-3.04, p trend = 0.63), and 0.62 for PlGF (95 % CI 0.19-2.00, p trend = 0.73). Risk patterns were not altered when all angiogenic markers were included in the model simultaneously, or by restricting analyses to invasive breast cancers, to cases diagnosed two or more years after blood collection or to ER+ tumors.
There was no evidence of an increased breast cancer risk associated with circulating levels of pro-angiogenic markers VEGF and PlGF or a reduced risk with circulating levels of anti-angiogenic marker sFlt-1.
促血管生成因子与乳腺肿瘤分期及较差预后呈正相关,但其在乳腺癌病因学中的作用尚未得到评估。
我们检测了352例新发乳腺癌病例[诊断时的平均年龄为67岁(范围55 - 83岁)]以及前列腺、肺、结肠和卵巢筛查试验中的352例非病例(1993 - 2001年入组女性,随访至2005年)血清中促血管生成的血管内皮生长因子A(VEGF)、胎盘生长因子(PlGF)以及抗血管生成的可溶性fms样酪氨酸激酶-1(sFlt-1)的水平,这些非病例在年龄和入组日期上与病例相匹配。病例从采血到诊断平均随访4.2年,范围3.9 - 12.8年;53%为雌激素受体阳性/孕激素受体阳性(ER+/PR+),13%为ER-/PR-。使用针对已知乳腺癌风险因素进行调整的加权Cox比例风险回归模型估计四分位数特异性风险比(HR)和95%置信区间(CI)。使用血管生成标志物的有序变量来检验HR中的趋势。
将最高四分位数与最低四分位数进行比较,多变量分析中VEGF的HR为0.90(95% CI 0.33 - 2.43,p趋势 = 0.88),sFlt-1的HR为1.38(95% CI 0.63 - 3.04,p趋势 = 0.63),PlGF的HR为0.62(95% CI 0.19 - 2.00,p趋势 = 0.73)。当所有血管生成标志物同时纳入模型时,或者将分析限制在浸润性乳腺癌、采血两年或更长时间后诊断的病例或ER+肿瘤时,风险模式没有改变。
没有证据表明循环中促血管生成标志物VEGF和PlGF的水平升高与乳腺癌风险增加相关,也没有证据表明循环中抗血管生成标志物sFlt-1的水平降低与乳腺癌风险降低相关。
