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Identification of potential serum biomarkers for breast cancer using a functional proteomics technology

机译:使用功能蛋白质组学技术鉴定乳腺癌潜在的血清生物标志物

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BackgroundCancer is a genetic disease; its development and metastasis depend on the function of many proteins. Human serum contains thousands of proteins; it is a window for the homeostasis of individual’s health. Many of the proteins found in the human serum could be potential biomarkers for cancer early detection and drug efficacy evaluation. MethodsIn this study, a functional proteomics technology was used to systematically monitor metabolic enzyme and protease activities from resolved serum proteins produced by a modified 2-D gel separation and subsequent Protein Elution Plate, a method collectively called PEP. All the experiments were repeated at least twice to ensure the validity of the findings. ResultsFor the first time, significant differences were found between breast cancer patient serum and normal serum in two families of enzymes known to be involved in cancer development and metastasis: metabolic enzymes and proteases. Multiple enzyme species were identified in the serum assayed directly or after enrichment. Both qualitative and quantitative differences in the metabolic enzyme and protease activity were detected between breast cancer patient and control group, providing excellent biomarker candidates for breast cancer diagnosis and drug development. ConclusionsThis study identified several potential functional protein biomarkers from breast cancer patient serum. It also demonstrated that the functional proteomics technology, PEP, can be applied to the analysis of any functional proteins in human serum which contains thousands of proteins. The study indicated that the functional domain of the human serum could be unlocked with the PEP technology, pointing to a novel alternative for the development of diagnosis biomarkers for breast cancer and other diseases.
机译:背景癌症是一种遗传疾病。其发展和转移取决于许多蛋白质的功能。人血清中含有数千种蛋白质。它是个人健康平衡的窗口。人血清中发现的许多蛋白质可能是癌症早期检测和药物功效评估的潜在生物标记。方法在这项研究中,使用功能蛋白质组学技术来系统监测通过改良的2-D凝胶分离和随后的蛋白洗脱板(统称为PEP)产生的分离的血清蛋白的代谢酶和蛋白酶活性。所有实验至少重复两次以确保发现的有效性。结果首次在乳腺癌患者血清和正常血清之间发现了两个已知与癌症发展和转移有关的酶家族:代谢酶和蛋白酶,两者之间存在显着差异。直接或富集测定的血清中鉴定出多种酶。在乳腺癌患者和对照组之间均检测到代谢酶和蛋白酶活性的定性和定量差异,为乳腺癌的诊断和药物开发提供了极好的生物标志物候选物。结论本研究从乳腺癌患者血清中鉴定出几种潜在的功能性蛋白质生物标志物。它还证明了功能蛋白质组学技术PEP可用于分析人血清中包含数千种蛋白质的任何功能蛋白质。研究表明,PEP技术可以解锁人血清的功能域,为开发乳腺癌和其他疾病的诊断生物标记物提供了一种新的选择。

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