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首页> 外文期刊>Gut and Liver >Fecal Immunochemical Test and Fecal Calprotectin Measurement Are Noninvasive Monitoring Tools for Predicting Endoscopic Activity in Patients with Ulcerative Colitis
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Fecal Immunochemical Test and Fecal Calprotectin Measurement Are Noninvasive Monitoring Tools for Predicting Endoscopic Activity in Patients with Ulcerative Colitis

机译:粪便免疫化学测试和粪便钙卫蛋白测量是预测溃疡性结肠炎患者内镜活动的无创监测工具

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Mucosal healing (MH) has been considered as the target in the treatment of inflammatory bowel disease (IBD) based on the observation that MH is associated with improved clinical outcomes reducing the risk of surgery, hospitalization, and steroid dependency. 1 , 2 However, endoscopic assessment, the gold standard for evaluating MH has several limitations in its clinical use because of its inconvenience, invasiveness, and high-cost, while symptom-based disease activity score has a quite discordance with MH. 3 Thus, need for reliable, noninvasive, surrogate markers precisely reflecting the mucosal status has fuelled interests in the use of fecal immunochemical test (FIT) and fecal calprotectin (Fcal) measurement. Although several IBD clinicians have used these markers as assistant tools for diagnosis, monitoring, and decision making for further invasive tests for years, there still remain controversies regarding “how to use fecal markers” in routine clinical practice. In this issue of Gut and Liver, the article entitled “Fecal immunochemical test and fecal calprotectin results show different profiles in disease monitoring for ulcerative colitis” 4 sought to determine the best choice of fecal markers in real clinical practice by evaluating changes in the values of each marker based on the findings of consecutive colonoscopies in patients with ulcerative colitis (UC). A total of 110 colonoscopy intervals from 84 patients were identified and the data of fecal samples which were collected within 2 days before colonoscopy were evaluated. This study adopted cutoff values of FIT and Fcal as 100 ng/mL, and 180 μg/g, respectively, and defined MH as Mayo endoscopic subscore of 0 throughout the entire colon. Interestingly, changes of fecal marker levels were found to have different patterns according to the presence or absence of mucosal inflammation in the precedent colonoscopy. FIT had an advantage in predicting the results of subsequent colonoscopic examinations in patients with MH and a negative FIT result at the precedent examination showed 93% of the overall accuracy compared with Fcal showing 79% of accuracy. On the other hand, Fcal measurement was superior in terms of reflecting the change in endoscopic activity than FIT (r=0.59, p<0.0001 vs r=0.30, p=0.054) in patients with a persistent high endoscopic activity. In addition, FIT was useful in predicting the achievement of MH after therapy in patients with active endoscopic inflammation at the precedent colonoscopy. The ratios of negative conversion of Fcal and FIT in these patients were 92% and 62%, respectively. Fecal markers have been shown to be associated with endoscopic disease activity, treatment response, and prediction for relapse. Ma et al . 5 reported similar performance of FIT and Fcal in identifying MH in IBD patients by showing that positive predictive value (PPV) for FIT <100 ng/mL and Fcal ≤250 μg/g were 0.78 and 0.77, respectively, but better performance were observed in patients with UC, particularly for FIT (area under the curve, 0.88 vs 0.69, p=0.05). Ryu et al . 6 reported a positively correlation of FIT with endoscopic activity (r=0.626, p<0.01) and clinical activity (r=0.496, p<0.01) in patients with UC. Furthermore, Mooiweer et al . 7 confirmed the added value of Fcal over MH for predicting clinical relapse and Molander et al . 8 found a precedent increase of Fcal 6 months before clinical relapse in patients who discontinued anti-tumor necrosis factor therapy after achieving deep remission. In accordance with previous studies, this study 4 enlarged our knowledge about the appropriate choice of fecal markers for disease monitoring at specific clinical situations of UC, and confirmed different values of the two markers, namely FIT as a surrogate measure of bleeding from mucosal ulceration, and Fcal as a surrogate measure of mucosal inflammation per se. 5 Based on these results, the authors proposed an algorithm for using fecal markers in specific situations. Fcal was recommended for the monitoring of treatment efficacy after induction therapy. On the other hand, FIT was recommended to monitor endoscopic disease activity after symptom improvement following induction therapy, and repetitively after achieving MH confirmed by colonoscopy due to its higher PPV for MH and low cost. A positive conversion of FIT during monitoring of stable patients aids in deciding further colonoscopy or additional treatment. However, there are several limitations in using fecal markers in real practice. One of the major concerns regarding Fcal is its large variations in day-to-day, by time of day, and within the same bowel movement. Moreover, the ideal cutoff value has not yet been determined 9 and discrepancies between different Fcal kits are another problems. 10 Finally, high false positive rates of FIT require caution in the interpretation of results. Examinations of multiple samples in a serial manner are thought to reduce possible errors and could be more ben
机译:粘膜愈合(MH)被认为是治疗炎症性肠病(IBD)的目标,原因是观察到MH与改善临床结局相关,从而降低了手术,住院和类固醇依赖的风险。 [1,2]然而,在内窥镜评估中,评估MH的金标准由于其不便,侵入性和高成本而在其临床应用中存在一些局限性,而基于症状的疾病活动性评分与MH却存在很大差异。 3因此,对可靠,无创,能准确反映粘膜状态的替代标志物的需求,激发了人们对粪便免疫化学测试(FIT)和粪便钙卫蛋白(Fcal)测量的兴趣。尽管数年来,IBD临床医生一直将这些标志物用作诊断,监测和决策的辅助工具,以进行进一步的侵入性检查,但在常规临床实践中仍存在关于“如何使用粪便标志物”的争议。在本期《肠道与肝脏》杂志上,题为“粪便免疫化学测试和粪便钙卫蛋白的结果显示了在溃疡性结肠炎疾病监测中的不同情况”的文章4试图通过评估Bcl值的变化来确定实际临床实践中粪便标记物的最佳选择。每个标记都是基于溃疡性结肠炎(UC)患者连续结肠镜检查的发现。确定了总共84位患者的110次结肠镜检查间隔,并评估了在结肠镜检查之前2天内收集的粪便样本数据。这项研究采用FIT和Fcal的截断值分别为100 ng / mL和180μg/ g,并将MH定义为整个结肠的Mayo内镜下评分为0。有趣的是,根据结肠镜检查中是否存在粘膜炎症,粪便标志物水平的变化具有不同的模式。 FIT在预测MH患者随后的结肠镜检查结果方面具有优势,而先前检查的FIT结果阴性显示总体准确度为93%,而Fcal显示准确度为79%。另一方面,在持续高内镜活动的患者中,Fcal测量在反映内窥镜活动的变化方面优于FIT(r = 0.59,p <0.0001 vs r = 0.30,p = 0.054)。另外,FIT可用于预测结肠镜检查前活动性内镜发炎患者的治疗后MH的实现情况。这些患者中Fcal和FIT的阴性转化率分别为92%和62%。粪便标记物已显示与内窥镜疾病活动,治疗反应和复发预测有关。 Ma等。 5报告显示FIT <100 ng / mL和Fcal≤250μg/ g的阳性预测值(PPV)分别为0.78和0.77,但在IBD患者中MH的FIT和Fcal表现相似。 UC患者,尤其是FIT患者(曲线下面积,0.88 vs 0.69,p = 0.05)。 Ryu等。 6报道了UC患者的FIT与内镜活动(r = 0.626,p <0.01)和临床活动(r = 0.496,p <0.01)呈正相关。此外,Mooiweer等人。 7证实了Fcal比MH在预测临床复发方面的附加价值和Molander等人。 8发现在达到深层缓解后停止抗肿瘤坏死因子治疗的患者中,临床复发前6个月Fcal有所增加。根据以往的研究,该研究4扩大我们的知识有关的疾病,在UC的特定临床情况监测粪便标记的合适的选择,并确认了两个标记的不同值,即散客从粘膜溃疡出血的替代措施, Fcal是粘膜炎症本身的替代指标。 5基于这些结果,作者提出了一种在特定情况下使用粪便标记物的算法。建议使用Fcal监测诱导治疗后的治疗效果。另一方面,建议FIT监测诱导治疗后症状改善后的内窥镜疾病活动,并且由于其对MH的更高的PPV和低成本,因此在结肠镜检查证实的MH后反复进行监测。在监测稳定患者期间,FIT的阳性转化有助于决定进一步的结肠镜检查或其他治疗。但是,在实际操作中使用粪便标记物存在一些限制。有关Fcal的主要问题之一是它在每天,每天的不同时间以及同一排便中的变化很大。而且,理想的临界值尚未确定9,而不同Fcal套件之间的差异是另一个问题。 10最后,FIT的高假阳性率在解释结果时需要谨慎。以串行方式检查多个样本被认为可以减少可能的错误,并且可能会更有益

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