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首页> 外文期刊>American Journal of Translational Research >4-Hydroxy estrogen metabolite, causing genomic instability by attenuating the function of spindle-assembly checkpoint, can serve as a biomarker for breast cancer
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4-Hydroxy estrogen metabolite, causing genomic instability by attenuating the function of spindle-assembly checkpoint, can serve as a biomarker for breast cancer

机译:4-羟基雌激素代谢物,通过衰减主轴组件检查点的功能引起基因组不稳定性,可以作为乳腺癌的生物标志物

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摘要

Sex hormone metabolism is altered during mammary gland tumorigenesis, and different metabolites may have different effects on mammary epithelial cells. This study aimed to evaluate associations between urinary sexual metabolite levels and breast cancer risk among premenopausal women of Mainland China. The molecular metabolism of the cancer-related metabolites was also explored based on the clinical data. The sex hormone metabolites in the urine samples of patients with breast cancer versus normal healthy women were analyzed comprehensively. Among many alterations of sex hormone metabolisms, 4-hydroxy estrogen (4-OH-E) metabolite was found to be significantly increased in the urine samples of patients with breast cancer compared with the normal healthy controls. This was the most important risk factor for breast cancer. Several experiments were conducted in vitro and in vivo to probe this mechanism. 4-Hydroxyestradiol (4-OH-E 2 ) was found to induce malignant transformation of breast cells and tumorigenesis in nude mice. At the molecular level, 4-OH-E 2 compromised the function of spindle-assembly checkpoint and rendered resistance to the anti-microtubule drug. Further, transgenic mice with high expression of CYP1B1, a key enzyme of 4-hydroxy metabolites, were established and stimulated with estrogen. Cancerous tissue was found to appear in the mammary gland of transgenic mice.
机译:性激素代谢在乳腺肿瘤肿瘤中改变,不同的代谢物可能对乳腺上皮细胞产生不同的影响。本研究旨在评估尿性交代谢物水平与乳腺癌风险与中国大陆前辈妇女的关联。还根据临床数据探索癌症相关代谢物的分子代谢。全面分析了乳腺癌患者患者尿液样本中的性激素代谢物。在与正常健康对照相比,乳腺癌患者的尿液样本中发现4-羟基雌激素(4-OH-E)代谢物中发现了4-羟基雌激素的改变。这是乳腺癌最重要的危险因素。在体外进行几个实验,体内进行探测该机制。发现4-羟基雌二醇(4-OH-E 2)被发现诱导裸鼠中乳腺细胞和肿瘤发生的恶性转化。在分子水平下,4-OH-E 2损害主轴组件检查点的功能,并呈现对抗微管药物的抗性。此外,具有高表达CYP1B1的转基因小鼠,确定并用雌激素刺激4-羟基代谢物的关键酶。发现癌组织出现在转基因小鼠的乳腺中。

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