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首页> 外文期刊>Gastroenterology >Approaches to Integrating Biomarkers Into Clinical Trials and Care Pathways as Targets for the Treatment of Inflammatory Bowel Diseases
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Approaches to Integrating Biomarkers Into Clinical Trials and Care Pathways as Targets for the Treatment of Inflammatory Bowel Diseases

机译:将生物标志物纳入临床试验和护理途径的方法,作为治疗炎症性肠病的靶标

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BACKGROUND & AIMS: There is no consensus on the best way to integrate biomarkers into inflammatory bowel disease (IBD) research and clinical practice. The International Organization for the Study of Inflammatory Bowel Disease aimed to outline biomarker definitions, categories, and operating properties required for their use in registration trials and clinical practice. Using fecal calprotectin as an example, we provide a framework for biomarker development and validation in patients with IBD. METHODS: We reviewed international society guidelines, regulatory agency guidance documents, and standardized reporting guidelines for biomarkers, in combination with publications on fecal calprotectin levels in patients with IBD. We assessed the validity of fecal calprotectin to serve as a surrogate biomarker of IBD activity and outlined a framework for further validation and development of biomarkers. RESULTS: No endpoints have been fully validated as surrogates of risk of disease complications; mucosal healing is the most valid endpoint used to determine risk of disease complications. Fecal level of calprotectin has not been validated as a biomarker for IBD activity because of lack of technical and clinical reliability, assessment of performance when used as a replacement for endoscopy, and assessment of responsiveness to changes in disease states. The level of fecal calprotectin can be used only as a prognostic factor for disease recurrence in patients in remission after medical or surgical treatment. CONCLUSIONS: We reviewed guidelines, regulatory documents, and publications to identify properties required for the development of biomarkers of IBD activity and areas in need of clarification from regulatory agencies and societies. We propose a path forward for research of biomarkers for IBD.
机译:背景和目标:将生物标志物整合到炎症性肠病(IBD)研究和临床实践中没有达成共识。国际炎症性肠病研究旨在概述对注册试验和临床实践所需的生物标志物定义,类别和操作性能。用粪便钙抗菌素为例,我们为IBD患者提供了一种生物标志物开发和验证的框架。方法:我们审查了国际社会指导方针,监管机构指导文件和标准化的生物标志物报告指南,与IBD患者患者粪便冲突素水平的出版物组合。我们评估了粪便CalProtectin的有效性,作为IBD活动的替代生物标志物,并概述了进一步验证和发展生物标志物的框架。结果:没有完全验证终点作为疾病并发症风险的替代品;粘膜治疗是最有效的终点用于确定疾病并发症的风险。由于缺乏技术和临床可靠性,缺乏技术和临床可靠性,当用作内窥镜检查时的替代品,以及对疾病状态的变化评估时,粪便抑制素的粪便水平尚未被验证为IBD活动的生物标志物。粪便水平的水平可以仅作为医疗或手术治疗后缓解患者疾病复发的预后因素。结论:我们审查了指导方针,监管文件和出版物,以确定制定IBD活动生物标志物和需要澄清监管机构和社会的地区所需的财产。我们提出了一条向前推进IBD生物标志物的道路。

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