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CD26-Related Serum Biomarkers: sCD26 Protein, DPP4 Activity, and Anti-CD26 Isotype Levels in a Colorectal Cancer-Screening Context

机译:CD26相关的血清生物标志物:SCD26蛋白,DPP4活性和抗CD26同种型水平在结肠直肠癌筛选背景下

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摘要

Current screening trials are showing reduction in colorectal cancer incidence and mortality. However, participation rates are often low, and blood-based tests could complement existing screening strategies. CD26 protein (sCD26) and its dipeptidyl peptidase IV (DPP4) enzymatic activity in circulation have been proposed as biomarkers for colorectal cancer and other diseases. However, changes in sCD26 and DPP4 levels show complex degrees of correlation, and their physiological or pathophysiological role is unclear. The aim of this study was to analyse if anti-CD26 autoantibodies are related to sCD26 and DPP4 and to determine their relevance in a context of colorectal cancer screening for complementing the value of sCD26 and DPP4 as biomarkers. These biomarkers were measured in a large prospective cohort (n=497, except the anti-CD26 antibodies, evaluated in 125 samples) that included a subgroup of individuals that were positive for the faecal immunological occult blood test (FIT) (n=86) and underwent a colonoscopy (n=47). We confirmed for the first time higher DPP4 activity in men compared to women (Student’s t test, p=0.002), though this difference between sexes was not seen for serum sCD26 protein. These biomarkers correlated (R=0.246, p=0.003) only in women. Correlations were found between anti-CD26 isotypes but not with DPP4 activity or sCD26 concentration, except for a negative correlation only in men between anti-CD26 IgA isotype and sCD26 (R=−0.232, p=0.044), and an almost significant negative correlation between anti-CD26 IgG and sCD26 limited to FIT-positive men. Interestingly, patients with advanced adenomas displayed the most elevated mean levels of anti-CD26 IgA, IgM, and particularly IgG (Mann-Whitney U test, p=0.030) in comparison with the other FIT positives without adenomas, and these levels did not correlate with sCD26 or its DPP4 activity. Our preliminary results suggest that the combination of these measures using sex as confounder could perhaps be used as biomarkers for colorectal disease. It also suggests that events affecting the gut influence the levels of anti-CD26 antibodies, which show little or no effect in antigen clearance. These findings should be confirmed in a larger cohort of individuals with colonoscopy. The physiological origin of the sex differences observed should be further addressed.
机译:目前的筛选试验显示结直肠癌发病率和死亡率降低。然而,参与率通常很低,血基的测试可以补充现有的筛选策略。已经提出了CD26蛋白(SCD26)及其二肽肽酶IV(DPP4)循环中的酶活性,作为结直肠癌和其他疾病的生物标志物。然而,SCD26和DPP4水平的变化显示复杂的相关程度,并且它们的生理或病理生理作用不明确。本研究的目的是分析抗CD26自身抗体与SCD26和DPP4有关,并在结直肠癌筛选中确定其相关性以将SCD26和DPP4的价值补充为生物标志物。这些生物标志物在大型前瞻性队列中测量(n = 497,除了在125个样品中评估的抗CD26抗体除外),其中包含粪便免疫血液检测(FIT)的阳性阳性的个体亚组(n = 86)并经历了结肠镜检查(n = 47)。与女性相比,我们在男性中第一次进行了更高的DPP4活性(学生的T试验,P = 0.002),但对于血清SCD26蛋白没有看到性别之间的这种差异。这些生物标志物仅在女性中相关(r = 0.246,p = 0.003)。在抗CD26同种型或不具有DPP4活性或SCD26浓度之间的相关性,除了仅在抗CD26 IGA同种型和SCD26之间的男性中的负相关性,以及对SCD26(R = -0.232,P = 0.044),以及几乎显着的负相关在抗CD26 IgG和SCD26之间限制适合阳性男性。有趣的是,高级腺瘤的患者均呈现出抗CD26 IgA,IgM和特别是IgG(Mann-Whitney U测试,P = 0.030)的最高平均水平相比没有腺瘤的其他粘性阳性,并且这些水平并不相关使用SCD26或其DPP4活动。我们的初步结果表明,这些措施的结合使用性行为混淆可能被用作结直肠疾病的生物标志物。它还表明,影响肠道的事件会影响抗CD26抗体的水平,这在抗原间隙中显示出很少或没有影响。这些发现应在具有结肠镜检查的较大的个体队列中确认。应进一步解决观察到性别差异的生理来源。

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