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用于检测结肠癌的尿液蛋白质组分析

Proteomic profiling of urine for the detection of colon cancer.

作者信息

Ward Douglas G, Nyangoma Stephen, Joy Howard, Hamilton Emma, Wei Wenbin, Tselepis Chris, Steven Neil, Wakelam Michael J O, Johnson Philip J, Ismail Tariq, Martin Ashley

机构信息

Cancer Research UK Institute for Cancer Studies, University of Birmingham, Edgbaston, UK.

出版信息

Proteome Sci. 2008 Jun 16;6:19. doi: 10.1186/1477-5956-6-19.

Abstract

BACKGROUND

Colorectal cancer is the second most common cause of cancer related death in the developed world. To date, no blood or stool biomarkers with both high sensitivity and specificity for potentially curable early stage disease have been validated for clinical use. SELDI and MALDI profiling are being used increasingly to search for biomarkers in both blood and urine. Both techniques provide information predominantly on the low molecular weight proteome (<15 kDa). There have been several reports that colorectal cancer is associated with changes in the serum proteome that are detectable by SELDI and we hypothesised that proteomic changes would also be detectable in urine.

RESULTS

We collected urine from 67 patients with colorectal cancer and 72 non-cancer control subjects, diluted to a constant protein concentration and generated MALDI and SELDI spectra. The intensities of 19 peaks differed significantly between cancer and non-cancer patients by both t-tests and after adjusting for confounders using multiple linear regressions. Logistic regression classifiers based on peak intensities identified colorectal cancer with up to 78% sensitivity at 87% specificity. We identified and independently quantified 3 of the discriminatory peaks using synthetic stable isotope peptides (an 1885 Da fragment of fibrinogen and hepcidin-20) or ELISA (beta2-microglobulin).

CONCLUSION

Changes in the urine proteome may aid in the early detection of colorectal cancer.

摘要

背景

在发达国家,结直肠癌是癌症相关死亡的第二大常见原因。迄今为止,尚无对潜在可治愈的早期疾病具有高敏感性和特异性的血液或粪便生物标志物被证实可用于临床。表面增强激光解吸电离(SELDI)和基质辅助激光解吸电离(MALDI)图谱分析越来越多地用于在血液和尿液中寻找生物标志物。这两种技术主要提供有关低分子量蛋白质组(<15 kDa)的信息。有几份报告称,结直肠癌与血清蛋白质组的变化有关,这些变化可通过SELDI检测到,我们推测蛋白质组的变化在尿液中也可检测到。

结果

我们收集了67例结直肠癌患者和72例非癌症对照受试者的尿液,将其稀释至恒定蛋白质浓度,并生成MALDI和SELDI光谱。通过t检验以及使用多元线性回归调整混杂因素后,癌症患者和非癌症患者之间19个峰的强度存在显著差异。基于峰强度的逻辑回归分类器在87%的特异性下识别结直肠癌的敏感性高达78%。我们使用合成稳定同位素肽(纤维蛋白原的1885 Da片段和铁调素-20)或酶联免疫吸附测定(β2-微球蛋白)对3个鉴别峰进行了鉴定和独立定量。

结论

尿液蛋白质组的变化可能有助于结直肠癌的早期检测。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a7e9/2440369/434796373553/1477-5956-6-19-1.jpg

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