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Dual-function biomarkers for detection of breast cancer and its cancer type: Invasive versus non-invasive

机译:用于检测乳腺癌及其癌症类型的双功能生物标志物:有创与无创

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Improved methods to assess an individual's risk of developing cancer, to detect cancers at early stages when they can be treated more effectively, to distinguish between invasive and non-invasive cancers, and to monitor recurrence and response to therapy are required to help doctor treat cancer more effectively. Traditional mammography and DNA Microarrays have been studied for early cancer detection and invasive cancer prediction. However, there is still challenging for detecting early cancer and cancer invasiveness simultaneously. In the paper, we presented a method to discover breast cancer dual-function biomarkers from LC/MS/MS plasma proteome which can discriminate not only cancer from normal breast but also invasive cancer from noninvasive cancer. The training set (Study A) and testing set (Study B) are each from plasma samples of 40 healthy women and 40 women diagnosed with breast cancer. Study A contains 30 invasive cancer samples and 10 non-invasive cancer samples, and Study B contains 23 invasive cancer samples, 8 non-invasive cancer samples, and 9 cancer samples with unknown type. First, we identified from Study A 21 differentially express biomarkers between normal and cancer. Then, we trained a Support Vector Machine with five-fold cross-validation for each combination of 5 out of the 21 biomarkers in the training set. Lastly, we found the optimal combination as best dual-function five biomarker panel. Further pathway analysis showed that the five biomarkers have strong connection with the complement and coagulation cascades pathway. This method can be extended to other cancers for dual-function marker identification. In the future, Multiple Reaction Monitoring (MRM) is planned for validation of these potential dual-function biomarkers.
机译:评估个人发展癌症风险的改进方法,在早期阶段检测癌症,以区分侵入性和无侵入性癌症,并需要监测治疗的复发和反应,以帮助医生治疗癌症更有效地。已经研究了传统的乳房爆炸和DNA微阵列用于早期癌症检测和侵袭性癌症预测。然而,同时检测早期癌症和癌症侵犯性仍然有挑战性。在本文中,我们提出了一种从LC / MS / MS血浆蛋白质中发现乳腺癌双功能生物标志物的方法,其不仅可以区分来自正常乳腺癌的癌症,而且来自非侵入性癌症。训练集(研究A)和测试集(研究B)各自来自40名健康妇女的血浆样本和40名患有乳腺癌的女性。研究A包含30个侵入性癌症样本和10个无侵入性癌症样本,研究B包含23个侵入性癌症样本,8个非侵入性癌症样本和9种癌症样品,具有未知类型。首先,我们从研究中确定了正常和癌症之间的21个差异表达生物标志物。然后,我们训练了一个支持向量机,为训练集中的21个生物标志物中的每个组合5倍的交叉验证。最后,我们发现最佳组合作为最佳双功能五个生物标志物面板。进一步的途径分析表明,五种生物标志物与补体和凝固级联途径有强关系。该方法可以扩展到其他癌症以进行双函数标记识别。未来,计划多次反应监测(MRM)用于验证这些潜在的双功能生物标志物。

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