血浆钙保护蛋白和髓过氧化物酶作为炎症性肠病的生物标志物。

IF 4.5 3区 医学 Q1 GASTROENTEROLOGY & HEPATOLOGY
Duo Hou, Akhilesh Swaminathan, Grace M Borichevsky, Chris M Frampton, Antony J Kettle, Richard B Gearry
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引用次数: 0

摘要

背景:炎症性肠病(IBD)是一种复发缓解型疾病,需要积极监测肠道炎症。我们的目的是确定血浆髓过氧化物酶(pMPO)和钙保护蛋白(pCal)这两种中性粒细胞蛋白与现有疾病活动性指标的相关性。方法:前瞻性招募接受回肠结肠镜检查的成年IBD患者。基线评估包括血液检查(pMPO、pCal和c反应蛋白[CRP])、症状问卷和内窥镜指标(CD简单内窥镜评分[SES-CD]和UC内窥镜严重程度指数[UCEIS])。活动期IBD定义为SES-CD≥2,UCEIS≥2。Spearman等级相关性评估血液标记物与内镜活动之间的关系。受试者工作特征曲线下面积(AUROC)和单变量logistic回归评估了血液标志物(在最佳阈值下)识别活动性疾病的能力。结果:共纳入170名受试者(女性,n = 92;克罗恩病[CD], n = 99;中位年龄46岁,IQR 35-58岁)。血浆生物标志物更准确地识别UC患者的活动性IBD (AUROCpMPO = 0.76, P .05;AUROCpCal = 0.65, P 13.86 ng/mL(比值比[OR] = 10.13, 3.4-30.16)和pcalbb0 961.72 ng/mL (OR = 3.38, 1.21-9.4)与内窥镜下活动性UC的发生率增加相关。结论:血浆MPO有望作为IBD活性的潜在血液生物标志物,特别是UC。联合使用pMPO和CRP增加了区分活动性和静止性IBD的诊断效用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Plasma Calprotectin and Myeloperoxidase as Biomarkers in Inflammatory Bowel Disease.

Background: Inflammatory bowel disease (IBD) is a relapsing-remitting illness requiring proactive monitoring of gut inflammation. We aimed to determine the correlations of plasma myeloperoxidase (pMPO) and calprotectin (pCal), two neutrophil proteins, with existing measures of disease activity.

Methods: Adults with IBD undergoing ileocolonoscopy were recruited prospectively. Baseline assessments included blood tests (pMPO, pCal, and C-reactive protein ([CRP]), symptom questionnaires, and endoscopic indices (simple endoscopic score for CD [SES-CD] and UC endoscopic index of severity [UCEIS]). Active IBD was defined as SES-CD > 2 and UCEIS ≥ 2. Spearman's rank correlations assessed the associations between blood markers and endoscopic activity. The area under the receiver operating characteristics curves (AUROC) and univariable logistic regression assessed the ability of blood markers (at optimal thresholds) to identify active disease.

Results: In total, 170 participants were included (female, n = 92; Crohn's disease [CD], n = 99; median age 46 years, IQR 35-58). Plasma biomarkers more accurately identified active IBD in individuals with UC (AUROCpMPO = 0.76, P < .001; AUROCpCal = 0.66, P < .05; AUROCCRP = 0.73, P < .001) than in CD (AUROCpMPO = 0.62, P > .05; AUROCpCal = 0.65, P < .01; AUROCCRP = 0.66, P < .01). In all patients with IBD, the addition of pCal (AUROC = 0.73, P < .001) and pMPO (AUROC = 0.73, P < .001) to CRP added benefit compared to CRP (AUROC = 0.70, P < .001) alone. Plasma myeloperoxidase > 13.86 ng/mL (odds ratio [OR] = 10.13, 3.4-30.16) and pCal > 961.72 ng/mL (OR = 3.38, 1.21-9.4) were associated with an increased odds of having endoscopically active UC.

Conclusions: Plasma MPO shows promise as a potential blood-based biomarker of IBD activity, especially in UC. The combined use of pMPO and CRP adds diagnostic utility in discriminating between active versus quiescent IBD.

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来源期刊
Inflammatory Bowel Diseases
Inflammatory Bowel Diseases 医学-胃肠肝病学
CiteScore
9.70
自引率
6.10%
发文量
462
审稿时长
1 months
期刊介绍: Inflammatory Bowel Diseases® supports the mission of the Crohn''s & Colitis Foundation by bringing the most impactful and cutting edge clinical topics and research findings related to inflammatory bowel diseases to clinicians and researchers working in IBD and related fields. The Journal is committed to publishing on innovative topics that influence the future of clinical care, treatment, and research.
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