Discrimination of pediatric cryptogenic multifocal ulcerous stenosing enteritis from small bowel Crohn’s disease and gastrointestinal tuberculosis: A retrospective study (with videos)

Introduction Cryptogenic multifocal ulcerous stenosing enteritis (CMUSE) is a rare entity that mimics various inflammatory strictures of the small intestine. Pediatric literature is scarce. We analyzed the clinical, radiological, endoscopic and histopathological features of children with CMUSE that...

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Veröffentlicht in:Indian journal of gastroenterology 2024-12, Vol.43 (6), p.1144-1155
Hauptverfasser: Samanta, Arghya, Sen Sarma, Moinak, Singh, Sumit Kumar, Srivastava, Anshu, Poddar, Ujjal, Mandelia, Ankur, Agrawal, Vinita, Yachha, Surendra Kumar, Lal, Richa
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Sprache:eng
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Zusammenfassung:Introduction Cryptogenic multifocal ulcerous stenosing enteritis (CMUSE) is a rare entity that mimics various inflammatory strictures of the small intestine. Pediatric literature is scarce. We analyzed the clinical, radiological, endoscopic and histopathological features of children with CMUSE that differentiate it from small bowel Crohn’s disease (SBCD) and gastrointestinal tuberculosis (GITB). Methods CMUSE was diagnosed by the following criteria: (1) unexplained small bowel strictures with superficial ulcers, (2) chronic/relapsing ulcers of small bowel after resection, (3) no signs of systemic inflammation, (4) absence of other known etiologies of small bowel ulcers. SBCD and GITB were diagnosed based on standard criteria. The clinical features, laboratory parameters, radioimaging, endoscopy (including video capsule endoscopy [VCE], intra-operative endoscopy), histopathological features and treatment outcome were noted. Results Out of 48, CMUSE was diagnosed in 13 (27%) isolated small bowel and ileocecal strictures, while GITB and SBCD accounted for 41% and 21% cases, respectively. Common presentations were sub-acute obstruction (46%), obscure gastrointestinal bleeding (38%) and protein-losing enteropathy (38%). CMUSE patients had significantly longer disease duration compared to SBCD and GITB ( p  
ISSN:0254-8860
0975-0711
0975-0711
DOI:10.1007/s12664-024-01604-3