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Novel Molecular Markers for Breast Cancer:

机译:乳腺癌的新型分子标记:

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The use of molecular biomarkers assures that breast cancer (BC) patients receive optimal treatment. Established biomarkers, such as estrogen receptor, progesterone receptor, HER2, and Ki67, have been playing significant roles in the subcategorization of BC to predict the prognosis and decide the specific therapy to each patient. Antihormonal therapy using 4-hydroxytamoxifen or aromatase inhibitors have been employed in patients whose tumor cells express hormone receptors, while monoclonal antibody to HER2 has been administered to HER2-positive BCs. Although new therapeutic agents have been developed in the past few decades, many patients still die of the disease due to relapse; thus, novel molecular markers that predict therapeutic failure and those that can be targets for specific therapy are expected. We have chosen four of such molecules by reviewing recent publications, which are cyclin E, B-Myb, Twist, and DMP1β. The oncogenicity of these molecules has been demonstrated in vivo and/or in vitro through studies using transgenic mice or siRNAs, and their expressions have been shown to be associated with shortened overall or disease-free survival of BC patients. The former three molecules have been shown to accelerate epithelial-mesenchymal transition that is often associated with cancer stem cell-ness and metastasis; all these four can be novel therapeutic targets as well. Thus, large prospective studies employing immunohistochemistry will be needed to establish the predictive values of these molecules in patients with BC.
机译:分子生物标志物的使用可确保乳腺癌(BC)患者得到最佳治疗。已建立的生物标志物,例如雌激素受体,孕激素受体,HER2和Ki67,在BC的亚分类中可发挥重要作用,以预测预后并确定针对每个患者的具体治疗方法。对于肿瘤细胞表达激素受体的患者,已采用使用4-羟基他莫昔芬或芳香酶抑制剂的抗激素疗法,而针对HER2阳性的BCs已给予HER2单克隆抗体。尽管在过去的几十年中已经开发出新的治疗剂,但许多患者仍因复发而死于疾病。因此,预期可以预测治疗失败的新型分子标记以及可以作为特定治疗靶点的分子标记。通过回顾最近的出版物,我们选择了四个这样的分子,即细胞周期蛋白E,B-Myb,Twist和DMP1β。这些分子的致癌性已经通过使用转基因小鼠或siRNA的研究在体内和/或体外得到证实,并且它们的表达已证明与BC患者的总体生存时间缩短或无病生存有关。前三种分子已被证明可加速上皮-间质转化,这通常与癌症干细胞和转移有关。所有这四个也可以是新颖的治疗靶标。因此,需要大量采用免疫组织化学的前瞻性研究来确定这些分子在BC患者中的预测价值。

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