ABSTRACT
Colonic polyps are very common in the general population. Some polyps present a cancerization risk and their screening and management by endoscopy reduce the risk of colorectal cancer. Other polyps do not need specific follow-up. There are different types of polyps whose classification has been updated over the last ten years. Serrated polyps now intersect hyperplastic polyps, sessile serrated adenomas and traditional serrated adenomas. Current recommendations are to resect and histologically analyze each colonic polyp to define a personalized endoscopic surveillance strategy. Some colonic polyposis syndromes require management in a specialized center.
Les polypes coliques sont très fréquents dans la population générale. Certains sont à risque de cancérisation et leurs dépistage et prise en charge par le biais de l'endoscopie permettent une diminution du risque de cancer colorectal. D'autres ne nécessitent pas de surveillance. La classification des polypes a été remise à jour au cours de ces dix dernières années et, à côté des adénomes conventionnels, on reconnaît à présent les festonnés ou dentelés qui regroupent les polypes hyperplasiques, les adénomes dentelés sessiles et les dentelés traditionnels. Les recommandations actuelles sont de réséquer et d'analyser histologiquement chaque polype colique afin de définir une stratégie de surveillance endoscopique personnalisée. Certains syndromes dits de polypose colique nécessitent une prise en charge en centre spécialisé.
Subject(s)
Colonic Polyps , Adenoma/pathology , Colonic Polyps/pathology , Colonic Polyps/surgery , HumansABSTRACT
Not fully defined pathophysiologic mechanisms of inflammatory bowel disease (IBD) involve an array of genetic, epigenetic, infectious, physiological and immunological factors. Nowadays, an inadequate activation of the innate immune system to a luminal factor occurring in genetically predisposed subjects is the most widely accepted today. Micro-autoimmune diseases, a group of small, single-stranded, non-coding RNA molecules act as potent negative gene regulators. Beyond cancer and various autoimmune diseases, their impact on IBD has recently been the focus of research. Differential expression of various micro-RNAs has been documented in active and inactive ulcerative colitis, while micro-RNA profile appears to differ between ileal and colonic Crohn's disease. Except for tissue samples, attempts have been made to estimate similar differences at patients' blood samples. Apart from offering new directions in related research, these molecules arise as useful diagnostic tools and potential therapeutic targets. This review focuses on micro-RNA alterations in IBD and their potential implication on immunologic deregulation.