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首页> 外文期刊>Molecular & cellular proteomics: MCP >Identification of Candidate Plasma Protein Biomarkers for Cervical Cancer Using the Multiplex Proximity Extension Assay
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Identification of Candidate Plasma Protein Biomarkers for Cervical Cancer Using the Multiplex Proximity Extension Assay

机译:利用多路复用近距离分析鉴定宫颈癌候选血浆蛋白生物标志物

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摘要

Human papillomavirus (HPV) is recommended as the primary test in cervical cancer screening, with co-testing by cytology for HPV-positive women to identify cervical lesions. Cytology has low sensitivity and there is a need to identify biomarkers that could identify dysplasia that are likely to progress to cancer. We searched for plasma proteins that could identify women with cervical cancer using the multiplex proximity extension assay (PEA). The abundance of 100 proteins were measured in plasma collected at the time of diagnosis of patients with invasive cervical cancer and in population controls using the Olink Multiplex panels CVD II, INF I, and ONC II. Eighty proteins showed increased levels in cases compared with controls. We identified a signature of 11 proteins (PTX3, ITGB1BP2, AXIN1, STAMPB, SRC, SIRT2, 4E-BP1, PAPPA, HB-EGF, NEMO and IL27) that distinguished cases and controls with a sensitivity of 0.96 at a specificity of 1.0. This signature was evaluated in a prospective replication cohort with samples collected before, at or after diagnosis and achieved a sensitivity of 0.78 and a specificity 0.56 separating samples collected at the time of diagnosis of invasive cancer from samples collected prior to diagnosis. No difference in abundance was seen between samples collected prior to diagnosis or after treatment as compared with population controls, indicating that this protein signature is mainly informative close to time of diagnosis. Further studies are needed to determine the optimal window in time prior to diagnosis for these biomarker candidates.
机译:推荐人乳头瘤病毒(HPV)作为宫颈癌筛查中的主要试验,通过细胞学进行Cytology进行HPV阳性妇女识别宫颈病变。细胞学敏感性低,需要鉴定可以识别可能对癌症进行的发育不良的生物标志物。我们搜索了血浆蛋白,可以使用多路复用接近延伸测定(豌豆)鉴定宫颈癌的妇女。使用Olink Multiplex CVD II,INF I和ONC II在诊断侵入性宫颈癌患者和人口控制时收集的血浆中100种蛋白质的丰度。与对照相比,八十蛋白在病例中显示出增加的水平。我们鉴定了11种蛋白质(PTX3,ITGB1BP2,AXIN1,StampB,SRC,SIRT2,4E-BP1,PAPPA,HB-EGF,NEMO和IL27)的特征,其特异性和对照在1.0的特异性下的灵敏度为0.96。该签名在预期复制队列中评估了在诊断前,处于或之后收集的样品,并达到0.78的敏感性,并且在诊断诊断到诊断前的样品时收集的特异性0.56分离样品。在诊断之前或与人口对照相比,在治疗之前收集的样品之间没有看到丰度的差异,表明该蛋白质签名主要是诊断时间接近的信息。需要进一步的研究来在诊断这些生物标志物候选者之前及时确定最佳窗口。

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    Uppsala Univ Biomed Ctr Dept Immunol Genet &

    Pathol Sci Life Lab SciLifeLab Uppsala Box 815 SE;

    Uppsala Univ Biomed Ctr Dept Immunol Genet &

    Pathol Sci Life Lab SciLifeLab Uppsala Box 815 SE;

    OLINK Prote Uppsala Sci Pk SE-75183 Uppsala Sweden;

    OLINK Prote Uppsala Sci Pk SE-75183 Uppsala Sweden;

    Uppsala Univ Dept Womens &

    Childrens Hlth S-75185 Uppsala Sweden;

    Umea Univ Dept Radiat Sci SE-90187 Umea Sweden;

    Umea Univ Dept Publ Hlth &

    Clin Med Nutr Res SE-90187 Umea Sweden;

    Umea Univ Dept Med Biosci Clin Chem SE-90187 Umea Sweden;

    Uppsala Univ Dept Womens &

    Childrens Hlth S-75185 Uppsala Sweden;

    Uppsala Univ Biomed Ctr Dept Immunol Genet &

    Pathol Sci Life Lab SciLifeLab Uppsala Box 815 SE;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 生物化学;
  • 关键词

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