十二指肠克罗恩病:病例报告和系统回顾

Muniratu Amadu, Jonathan Soldera
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摘要

背景炎症性肠病,包括溃疡性结肠炎、微小结肠炎和克罗恩病(CD),具有全球性影响。本综述侧重于十二指肠 CD(DCD),这是一种影响十二指肠的罕见亚型。DCD 的罕见性和无症状性给诊断带来了挑战,影响了预后和患者的健康。延迟诊断会恶化 DCD 的预后。目的 报告一例罕见的 DCD 病例,讨论诊断难题及其对预后的影响。方法 按照 PRISMA 声明进行了系统的文献检索。使用 PubMed/MEDLINE、《美国胃肠病学杂志》和南威尔士大学数据库中的特定医学主题词 (MeSH) 对相关研究进行了识别和分析。数据收集包括放射学扫描、内窥镜检查、活检和组织病理学结果等信息。结果 该综述考虑了 8 个病例报告和 1 个观察性研究,涉及 44 名被诊断为 DCD 的患者,其中一些患者因诊断延误而出现并发症。由于 DCD 尚无金标准检查方法,因此采用了多种诊断方法。这些方法包括放射扫描(磁共振成像(MRI)、计算机断层扫描(CT)和上消化道 X 光)、内窥镜检查(结肠镜检查和食管胃十二指肠镜检查)、活组织检查和临床怀疑。结论 本综述讨论了 DCD 诊断的挑战以及 CT、MRI 和透视的作用。它指出了它们的局限性,并将研究结果与内窥镜检查和组织病理学研究进行了比较。需要进一步开展研究以改进诊断,强调扫描解读、内窥镜检查程序和活检,尤其是在常规内窥镜检查期间对高危患者的诊断。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Duodenal Crohn’s disease: Case report and systematic review
BACKGROUND Inflammatory bowel disease, including ulcerative colitis, microscopic colitis, and Crohn’s disease (CD), has a global impact. This review focuses on duodenal CD (DCD), a rare subtype affecting the duodenum. DCD’s rarity and asymptomatic nature create diagnostic challenges, impacting prognosis and patient well-being. Delayed diagnosis can worsen DCD outcomes. AIM To report a rare case of DCD and to discuss the diagnostic challenges and its implications on prognosis. METHODS A systematic literature search, following the PRISMA statement, was conducted. Relevant studies were identified and analysed using specific Medical Subject Terms (MeSH) from PubMed/MEDLINE, American Journal of Gastroenterology, and the University of South Wales database. Data collection included information from radiology scans, endoscopy procedures, biopsies, and histopathology results. RESULTS The review considered 8 case reports and 1 observational study, involving 44 participants diagnosed with DCD, some of whom developed complications due to delayed diagnosis. Various diagnostic methods were employed, as there is no gold standard workup for DCD. Radiology scans [magnetic resonance imaging (MRI), computed tomography (CT), and upper gastrointestinal X-ray], endoscopy procedures (colonoscopy and esophagogastroduodenoscopy), biopsies, and clinical suspicions were utilized. CONCLUSION This review discusses DCD diagnosis challenges and the roles of CT, MRI, and fluoroscopy. It notes their limitations and compares findings with endoscopy and histopathology studies. Further research is needed to improve diagnosis, emphasizing scan interpretation, endoscopy procedures, and biopsies, especially in high-risk patients during routine endoscopy.
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