Habermann Jens K, Roblick Uwe J, Luke Brian T, Prieto Darue A, Finlay William J J, Podust Vladimir N, Roman John M, Oevermann Elisabeth, Schiedeck Thomas, Homann Nils, Duchrow Michael, Conrads Thomas P, Veenstra Timothy D, Burt Stanley K, Bruch Hans-Peter, Auer Gert, Ried Thomas
Genetics Branch, National Cancer Institute, National Institutes of Health, 50 South Drive, Bethesda, MD 20892, USA.
Gastroenterology. 2006 Oct;131(4):1020-9; quiz 1284. doi: 10.1053/j.gastro.2006.07.011.
BACKGROUND & AIMS: Late diagnosis of colorectal carcinoma results in a significant reduction of average survival times. Yet despite screening programs, about 70% of tumors are detected at advanced stages (International Union Against Cancer stages III/IV). We explored whether detection of malignant disease would be possible through identification of tumor-specific protein biomarkers in serum samples.
A discovery set of sera from patients with colorectal malignancy (n = 58) and healthy control individuals (n = 32) were screened for potential differences using surface-enhanced laser desorption/ionization time-of-flight mass spectrometry. Candidate proteins were identified and their expression levels were validated in independent sample sets using a specific immunoassay (enzyme-linked immunosorbent assay).
By using class comparison and custom-developed algorithms we identified several m/z values that were expressed differentially between the malignant samples and the healthy controls of the discovery set. Characterization of the most prominent m/z values revealed a member of the complement system, the stable form of C3a anaphylatoxin (ie, C3a-desArg). Based on a specific enzyme-linked immunosorbent assay, serum levels of complement C3a-desArg predicted the presence of colorectal malignancy in a blinded validation set (n = 59) with a sensitivity of 96.8% and a specificity of 96.2%. Increased serum levels were also detected in 86.1% of independently collected sera from patients with colorectal adenomas (n = 36), whereas only 5.6% were classified as normal.
Complement C3a-desArg is present at significantly higher levels in serum from patients with colorectal adenomas (P < .0001) and carcinomas (P < .0001) than in healthy individuals. This suggests that quantification of C3a-desArg levels could ameliorate existing screening tests for colorectal cancer.
结直肠癌的晚期诊断会导致平均生存时间显著缩短。然而,尽管有筛查项目,仍有大约70%的肿瘤在晚期(国际抗癌联盟III/IV期)被发现。我们探讨了通过鉴定血清样本中的肿瘤特异性蛋白质生物标志物来检测恶性疾病是否可行。
使用表面增强激光解吸/电离飞行时间质谱对一组来自结直肠恶性肿瘤患者(n = 58)和健康对照个体(n = 32)的血清进行筛查,以寻找潜在差异。鉴定出候选蛋白质,并使用特异性免疫测定法(酶联免疫吸附测定)在独立样本集中验证其表达水平。
通过类别比较和定制开发的算法,我们确定了几个在发现组的恶性样本和健康对照之间差异表达的m/z值。对最显著的m/z值进行表征后发现是补体系统的一个成员,即C3a过敏毒素的稳定形式(即C3a-去精氨酸)。基于特异性酶联免疫吸附测定,补体C3a-去精氨酸的血清水平在一个盲法验证集(n = 59)中预测结直肠恶性肿瘤的存在,敏感性为96.8%,特异性为96.2%。在86.1%独立收集的结直肠腺瘤患者血清(n = 36)中也检测到血清水平升高,而只有5.6%被分类为正常。
结直肠腺瘤患者(P <.0001)和癌患者(P <.0001)血清中的补体C3a-去精氨酸水平显著高于健康个体。这表明对C3a-去精氨酸水平进行定量可以改善现有的结直肠癌筛查试验。