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Quantitative Proteomics of Breast Tumors: Tissue Quality Assessment to Clinical Biomarkers

机译:乳腺肿瘤的定量蛋白质组学:对临床生物标志物的组织质量评估。

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摘要

Liquid chromatography-selected reaction monitoring mass spectrometry (LC-SRM) is not only a proven tool for clinical chemistry, but also a versatile method to enhance the capability to quantify biomarkers for tumor biology research. As the treatment of cancer continues to evolve, the ability to assess multiple biomarkers to assign cancer phenotypes based on the genetic background and the signaling of the individual tumor becomes paramount to our ability to treat the patient. In breast cancer, the American Society of Clinical Oncology (ASCO) has defined biomarkers for patient assessment to guide selection of therapy: estrogen receptor, progesterone receptor, and the HER2/Neu receptor tyrosine kinase; therefore, these proteins were selected for LC-SRM assay development. Detailed molecular characterization of these proteins is necessary for patient treatment, so expression and phosphorylation assays have been developed and applied. In addition, other LC-SRM assays were developed to further evaluate tumor biology (e.g. Ki-67 for proliferation and vimentin for tumor aggressiveness related to the epithelial-to-mesenchymal transition). These measurements combined with biomarkers for tissue quality and histological content are implemented in a three tier multiplexed assay platform, which is translated from cell line models into frozen tumor tissues banked from breast cancer patients.
机译:液相色谱选择的反应监测质谱仪(LC-SRM)不仅是临床化学中行之有效的工具,而且还是一种增强肿瘤生物学研究生物标志物定量能力的通用方法。随着癌症治疗方法的不断发展,基于遗传背景和单个肿瘤信号评估多种生物标志物以分配癌症表型的能力对于我们治疗患者的能力至关重要。在乳腺癌中,美国临床肿瘤学会(ASCO)为患者评估定义了生物标志物,以指导治疗选择:雌激素受体,孕激素受体和HER2 / Neu受体酪氨酸激酶;因此,选择了这些蛋白质用于LC-SRM分析开发。这些蛋白质的详细分子表征对于患者治疗是必需的,因此表达和磷酸化测定已得到开发和应用。此外,还开发了其他LC-SRM分析方法以进一步评估肿瘤生物学(例如Ki-67的增殖和波形蛋白的与上皮间质转化相关的肿瘤侵袭性)。这些测量值与生物标志物的组织质量和组织学含量相结合,可在三层多重测定平台中实施,该平台可从细胞系模型转换为乳腺癌患者的冷冻肿瘤组织。

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