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Urine Biomarkers of Risk in the Molecular Etiology of Breast Cancer

机译:尿液生物标志物在乳腺癌分子病因学中的风险

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Endogenous estrogens can be bio-activated to endogenous carcinogens via formation of estrogen quinones. Estrogen-3,4-quinones react with DNA to form mutagenic depurinating estrogen-DNA adducts. The carcinogenicity of endogenous estrogens is related to unbalanced estrogen metabolism leading to excess estrogen quinones and formation of depurinating DNA adducts. The present studies were initiated to confirm that relatively high levels of depurinating estrogen- DNA adducts are present in women at high risk for breast cancer or diagnosed with the disease. These adducts may be biomarkers for early detection of breast cancer risk. The estrogen metabolites, conjugates and depurinating DNA adducts were identified and quantified by using ultraperformance liquid chromatography/tandem mass spectrometry to analyze urine samples from 40 healthy control women, 40 high-risk women and 40 women with newly diagnosed breast cancer. Estrogen metabolism was shifted from protective methoxylation and conjugation pathways in healthy control women towards activating pathways leading to formation of depurinating DNA adducts in women at high risk or with breast cancer. These results support the hypothesis that breast cancer is initiated by mutations derived from depurination of estrogen-DNA adducts. Therefore, relative levels of depurinating estrogen-DNA adducts could become biomarkers for early detection of breast cancer risk and aid in determining preventive strategies.
机译:内源性雌激素可通过形成雌激素醌而被生物激活为内源性致癌物。雌激素3,4-醌与DNA反应形成诱变的脱嘌呤雌激素-DNA加合物。内源性雌激素的致癌性与雌激素代谢失衡有关,导致过量的雌激素醌和形成脱嘌呤的DNA加合物。发起本研究是为了确认在罹患乳腺癌高风险或被诊断出患有这种疾病的女性中,存在较高水平的嘌呤-雌激素-DNA脱嘌呤。这些加合物可能是早期发现乳腺癌风险的生物标志物。使用超高效液相色谱/串联质谱法对40例健康对照妇女,40例高危妇女和40例新诊断为乳腺癌的妇女的尿液样品进行分析,从而鉴定并定量了雌激素代谢物,缀合物和脱嘌呤的DNA加合物。雌激素的代谢已从健康对照妇女的保护性甲氧基化和结合途径转移到活化途径,从而导致高风险或患有乳腺癌的妇女形成脱嘌呤DNA加合物。这些结果支持以下假设:乳腺癌是由雌激素-DNA加合物的脱嘌呤引起的突变引发的。因此,相对水平的脱嘌呤雌激素-DNA加合物可能成为早期发现乳腺癌风险的生物标记,并有助于确定预防策略。

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