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Promise and Challenge: Markers of Prostate Cancer Detection Diagnosis and Prognosis

机译:承诺与挑战:前列腺癌检测诊断和预后的标志

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摘要

Approximately 1 man in 6 will be diagnosed with prostate cancer during his life lifetime, and over 200,000 men in the U.S. are diagnosed with prostate cancer annually. Since the widespread adoption of PSA testing, about 60–70% of men at risk in the U.S. have had a blood test for prostate cancer. With this, prostate cancer death rates have decreased, yet only slightly. Thirty thousand men still die each year from this disease. PSA testing fails to identify a small but significant proportion of aggressive cancers, and only about 30% of men with a “positive” PSA have a positive biopsy. Additionally, of men who are treated for prostate cancer, about 25% require additional treatment, presumably due to disease recurrence. Also of concern is the growing evidence that there are some prostate cancers for which treatment may not be necessary. Very long-term studies from the U.S. and Europe, following men with prostate cancer have found that some tumors do not progress over time. In these individuals, prostate cancer treatment is unnecessary and harmful as these men do not benefit from treatment but will be at risk of treatment-related side effects and complications. They suggest a fundamental problem with prostate cancer: it is not possible, at this time, to predict the natural history of the disease. It is for these reasons that the most important challenge in prostate cancer today is the inability to predict the behavior of an individual tumor in an individual patient. Here we review issues related to performance and validation of biomarkers with a focus on “doing no harm”, and bearing in mind that it is the ultimate goal of early detection to save lives. Improved diagnostic and prognostic biomarkers are needed for prostate cancer, and the use of these markers should ultimately translate into increased life span and quality of life. The ultimate goal would be to not only have accurate biomarkers suitable for early diagnosis, but also biomarkers that identify men at greatest risk of developing aggressive disease. Technology has been brought to bear on this problem, and the major approaches are genomics, expression analysis, and proteomics. Proteomics and DNA methylation assays may soon be used in sensitive and specific diagnostic testing of serum and tissues for cancer. Expression arrays may be used to establish both a more specific diagnosis and prognosis for a particular tumor. The proteome is only beginning to be understood, and alternative splicing and post-translational modifications of proteins such as glycosylation and phosphorylation are challenging areas of study. Finally, risk assessment and prognosis are being pursued through analysis of genomic polymorphisms (single nucleotide polymorphisms, SNPs). This huge task is only beginning, and requires the combined expertise of molecular epidemiologists, oncologists, surgeons, pathologists, and basic scientists.
机译:在其一生中,大约有六分之一的人将被诊断出患有前列腺癌,并且在美国,每年有超过200,000的男性被诊断出患有前列腺癌。自从广泛采用PSA测试以来,美国大约60-70%的高危男性已经对前列腺癌进行了血液测试。这样,前列腺癌的死亡率下降了,但仅略有下降。每年仍有三万人死于这种疾病。 PSA测试无法识别出一小部分但占很大比例的侵袭性癌症,只有约30%的PSA“阳性”男性活检阳性。另外,在接受前列腺癌治疗的男性中,大概25%可能由于疾病复发而需要额外的治疗。同样令人关注的是,越来越多的证据表明有些前列腺癌可能不需要治疗。继患有前列腺癌的男性之后,来自美国和欧洲的长期研究发现,某些肿瘤不会随着时间的推移而发展。在这些个体中,前列腺癌的治疗是不必要的且有害的,因为这些男性无法从治疗中受益,但将面临与治疗相关的副作用和并发症的风险。他们提出了前列腺癌的一个基本问题:目前无法预测这种疾病的自然病史。由于这些原因,当今前列腺癌中最重要的挑战是无法预测单个患者中单个肿瘤的行为。在这里,我们以“无害”为重点,回顾与生物标志物的性能和验证有关的问题,并牢记这是早期发现以挽救生命的最终目标。前列腺癌需要改进的诊断和预后生物标志物,这些标志物的使用最终应转化为延长的寿命和生活质量。最终目标不仅是要有适合早期诊断的准确生物标志物,而且还要有识别出罹患侵略性疾病风险最大的男人的生物标志物。已经为解决这个问题采用了技术,主要方法是基因组学,表达分析和蛋白质组学。蛋白质组学和DNA甲基化测定可能很快将用于血清和组织的敏感性和特异性诊断测试,以检测癌症。表达阵列可用于建立针对特定肿瘤的更具体的诊断和预后。蛋白质组学才刚刚开始被理解,蛋白质的其他剪接和翻译后修饰(例如糖基化和磷酸化)是具有挑战性的研究领域。最后,通过分析基因组多态性(单核苷酸多态性,SNP)来进行风险评估和预后评估。这项艰巨的任务才刚刚开始,需要分子流行病学家,肿瘤学家,外科医生,病理学家和基础科学家的共同专业知识。

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