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首页> 外文期刊>OMICS: A journal of integrative biology >Comparative Serum Proteome Analysis of Human Lymph Node Negative/Positive Invasive Ductal Carcinoma of the Breast and Benign Breast Disease Controls via Label-Free Semiquantitative Shotgun Technology
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Comparative Serum Proteome Analysis of Human Lymph Node Negative/Positive Invasive Ductal Carcinoma of the Breast and Benign Breast Disease Controls via Label-Free Semiquantitative Shotgun Technology

机译:人类淋巴的比较血清蛋白质组分析节点消极/积极的浸润性导管癌乳房和良性乳房疾病的控制通过Label-Free半定量的猎枪技术

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Serum proteomics provides a useful tool to identify potential biomarkers associated with cancer progression. In the present study, a two-dimensional liquid chromatography-tandem mass spectrometry (2D-LC-MS=MS) on a linear ion trap was utilized to identify and compare serum proteins from breast cancer patients. Three groups of 21 human sera, 7 from patients with lymph node-negative invasive ductal carcinoma (IDCB), 7 from patients with lymph node-positive IDCB, and 7 controls from patients with benign breast diseases, were analyzed. Through proteomic analysis, a total of 2,078 proteins were identified with at least two unique peptide hits. By quantification with label-free spectral counting, a fruitful list of serum proteins with significant differences in abundance accompanying the progression of breast cancer was found. Through hierarchical cluster analysis based on the differently expressed proteins in selection, we found that different groups of sera could be distinguished. Among the selected proteins, tenascin-XB (TNXB) was further validated by the ELISA method in 131 serum samples as a promising biomarker for early metastasis of breast cancer. These experiments revealed the valuable potential of label-free quantitative 2D-LC-MS=MS for identification of novel biomarkers for disease progression.
机译:血清蛋白质组学提供了一个有用的工具识别潜在的相关生物标志物癌症的发展。二维液相chromatography-tandem质光谱法(2 d-lc-ms = MS)在一个线性离子阱是用来识别和比较血清从乳腺癌患者蛋白质。人类血清组21,从患者7淋巴淋巴结阴性浸润性导管癌(IDCB),从患者淋巴node-positive 7从良性患者IDCB和7控制乳腺疾病,进行了分析。蛋白质分析,共有2078名确定至少有两个独特的肽。通过量化label-free光谱计数、血清蛋白质的卓有成效的列表显著差异的陪同发现乳腺癌的进展。通过分层聚类分析的基础上蛋白质表达的不同选择,我们发现,不同组的血清杰出的。tenascin-XB (TNXB)进一步验证了ELISA方法在131年作为一个有前途的血清样本生物标志物早期乳腺癌的转移。这些实验揭示了价值的潜力label-free量化2 d-lc-ms =女士识别疾病的生物标记进展。

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