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Improving Pathological Assessment of Breast Cancer by Employing Array-Based Transcriptome Analysis

机译:利用基于阵列的转录组分析改善乳腺癌的病理学评估

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Breast cancer research has paved the way of personalized oncology with the introduction of hormonal therapy and the measurement of estrogen receptor as the first widely accepted clinical biomarker. The expression of another receptor—HER2/ERBB2eu—was initially a sign of worse prognosis, but targeted therapy has granted improved outcome for these patients so that today HER2 positive patients have better prognosis than HER2 negative patients. Later, the introduction of multigene assays provided the pathologists with an unbiased assessment of the tumors’ molecular fingerprint. The recent FDA approval of complete microarray pipelines has opened new possibilities for the objective classification of breast cancer samples. Here we review the applications of microarrays for determining ER and HER2 status, molecular subtypes as well as predicting prognosis and grade for breast cancer patients. An open question remains the role of single genes within such signatures. Openly available microarray datasets enable the execution of an independent cross-validation of new marker and signature candidates. In summary, we review the current state regarding clinical applications of microarrays in breast cancer molecular pathology.
机译:乳腺癌研究为激素疗法的发展铺平了道路,激素疗法的引入和雌激素受体的测定是第一个被广泛接受的临床生物标志物。另一种受体HER2 / ERBB2 / neu的表达最初是预后不良的迹象,但靶向治疗已使这些患者的预后得到改善,因此如今HER2阳性患者比HER2阴性患者的预后更好。后来,多基因测定法的引入为病理学家提供了对肿瘤分子指纹的公正评估。 FDA最近批准了完整的微阵列管线,为乳腺癌样品的客观分类开辟了新的可能性。在这里,我们回顾了微阵列在确定ER和HER2状态,分子亚型以及预测乳腺癌患者的预后和等级方面的应用。一个悬而未决的问题仍然是单个基因在此类签名中的作用。公开可用的微阵列数据集可以执行新标记和签名候选者的独立交叉验证。总之,我们回顾了有关微阵列在乳腺癌分子病理学中的临床应用的当前状态。

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