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Potential Urinary Protein Biomarker Candidates for the Accurate Detection of Prostate Cancer among Benign Prostatic Hyperplasia Patients

机译:潜在的尿蛋白生物标志物候选人准确检测良性前列腺增生患者的前列腺癌

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摘要

Globally, Prostate cancer (PCa) is the most frequently occurring non-cutaneous cancer, and is the second highest cause of cancer mortality in men. Serum prostate specific antigen (PSA) has been the standard in PCa screening since its approval by the American Food & Drug Administration (FDA) in 1994. Currently, PSA is used as an indicator for PCa - patients with a serum PSA level above 4ng/mL will often undergo prostate biopsy to confirm cancer. Unfortunately fewer than similar to 30% of these men will biopsy positive for cancer, meaning that the majority of men undergo invasive biopsy with little benefit. Despite PSA's notoriously poor specificity (33%), there is still a significant lack of credible alternatives. Therefore an ideal biomarker that can specifically detect PCa at an early stage is urgently required. The aim of this study was to investigate the potential of using deregulation of urinary proteins in order to detect Prostate Cancer (PCa) among Benign Prostatic Hyperplasia (BPH). To identify the protein signatures specific for PCa, protein expression profiling of 8 PCa patients, 12 BPH patients and 10 healthy males was carried out using LC-MS/MS. This was followed by validating relative expression levels of proteins present in urine among all the patients using quantitative real time-PCR. This was followed by validating relative expression levels of proteins present in urine among all the patients using quantitative real time-PCR. This approach revealed that significant the down-regulation of Fibronectin and TP53INP2 was a characteristic event among PCa patients. Fibronectin mRNA down-regulation, was identified as offering improved specificity (50%) over PSA, albeit with a slightly lower although still acceptable sensitivity (75%) for detecting PCa. As for TP53INP2 on the other hand, its down-regulation was moderately sensitive (75%), identifying many patients with PCa, but was entirely non-specific (7%), designating many of the benign samples as malignant and being unable to accurately identify more than one negative.
机译:在全球范围内,前列腺癌(PCa)是最常见的非皮肤癌,并且是男性癌症死亡率第二高的原因。自1994年获得美国食品药品监督管理局(FDA)批准以来,血清前列腺特异性抗原(PSA)一直是PCa筛查的标准。目前,PSA用作PCa的指标-血清PSA水平高于4ng /毫升将经常进行前列腺穿刺活检以确认癌症。不幸的是,这些男性中活检阳性的少于30%,这意味着大多数男性接受侵入性活检几乎没有益处。尽管PSA的特异性很差(33%),但仍然严重缺乏可靠的替代方法。因此,迫切需要能够在早期特异性检测PCa的理想生物标志物。这项研究的目的是研究使用尿蛋白失调检测在良性前列腺增生(BPH)中检测前列腺癌(PCa)的潜力。为了鉴定对PCa特异的蛋白特征,使用LC-MS / MS对8位PCa患者,12位BPH患者和10位健康男性进行了蛋白表达谱分析。然后,使用定量实时PCR验证所有患者中尿液中蛋白质的相对表达水平。然后,使用定量实时PCR验证所有患者中尿液中蛋白质的相对表达水平。这种方法表明,纤连蛋白和TP53INP2的明显下调是PCa患者的特征性事件。纤连蛋白mRNA下调被认为与PSA相比具有更高的特异性(50%),尽管检测PCa的敏感性仍较低(75%),但特异性稍低。另一方面,对于TP53INP2,其下调是中等敏感的(75%),可识别许多PCa患者,但完全是非特异性的(7%),将许多良性样品指定为恶性且无法准确定位找出多个否定词。

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    Haj-Ahmad Yousef;

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  • 年度 2014
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  • 正文语种 en
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