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Investigation of the Ovarian and Prostate Cancer Peptidome for Candidate Early Detection Markers Using a Novel Nanoparticle Biomarker Capture Technology

机译:使用新型纳米颗粒生物标志物捕获技术研究卵巢癌和前列腺癌肽组作为候选早期检测标志物的研究

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摘要

Current efforts to identify protein biomarkers of disease use mainly mass spectrometry (MS) to analyze tissue and blood specimens. The low-molecular-weight “peptidome” is an attractive information archive because of the facile nature by which the low-molecular-weight information freely crosses the endothelial cell barrier of the vasculature, which provides opportunity to measure disease microenvironment-associated protein analytes secreted or shed into the extracellular interstitium and from there into the circulation. However, identifying useful protein biomarkers (peptidomic or not) which could be useful to detect early detection/monitoring of disease, toxicity, doping, or drug abuse has been severely hampered because even the most sophisticated, high-resolution MS technologies have lower sensitivities than those of the immunoassays technologies now routinely used in clinical practice. Identification of novel low abundance biomarkers that are indicative of early-stage events that likely exist in the sub-nanogram per milliliter concentration range of known markers, such as prostate-specific antigen, cannot be readily detected by current MS technologies. We have developed a new nanoparticle technology that can, in one step, capture, concentrate, and separate the peptidome from high-abundance blood proteins. Herein, we describe an initial pilot study whereby the peptidome content of ovarian and prostate cancer patients is investigated with this method. Differentially abundant candidate peptidome biomarkers that appear to be specific for early-stage ovarian and prostate cancer have been identified and reveal the potential utility for this new methodology
机译:当前识别疾病的蛋白质生物标记物的努力主要使用质谱(MS)分析组织和血液样本。低分子量的“肽组”是一个有吸引力的信息档案库,因为低分子量的信息可以轻松穿越血管系统的内皮细胞屏障,从而提供了测量与疾病微环境相关的蛋白质分析物的机会或掉入细胞外间质并从那里进入循环系统。但是,由于可以用来检测疾病,毒性,兴奋剂或药物滥用的早期检测/监测,鉴定有用的蛋白质生物标记物(无论是否为肽类)已受到严重阻碍,因为即使是最先进的高分辨率MS技术,其敏感性也低于目前在临床实践中通常使用的免疫测定技术的那些。新的低丰度生物标志物的鉴定表明早期事件,这些事件可能存在于已知标志物(例如前列腺特异性抗原)的每毫升亚纳克浓度范围内,目前的质谱技术无法轻易检测到。我们已经开发出一种新的纳米粒子技术,该技术可以一步捕获,浓缩和分离高丰度血液蛋白中的肽组。在这里,我们描述了一个初步的初步研究,其中卵巢和前列腺癌患者的肽组含量用这种方法进行了调查。已鉴定出似乎对早期卵巢癌和前列腺癌特异的差异丰富的候选肽组生物标记物,并揭示了这种新方法的潜在用途

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