Endoscopic Diagnosis and Differentiation of Inflammatory Bowel Disease

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REVIEW Clin Endosc 2016;49:370-375 http://dx.doi.org/10.5946/ce.2016.090 Print ISSN 2234-2400 On-line ISSN 2234-2443 Open Access Endoscopic Diagnosis and Differentiation of Inflammatory Bowel Disease Ji Min Lee and Kang-Moon Lee Department of Internal Medicine, St. Vincent's Hospital, College of Medicine, The Catholic University of Korea, Suwon, Korea Patients with inflammatory bowel disease have significantly increased in recent decades in Korea. Intestinal tuberculosis (ITB) and intestinal Behcet s disease (BD), which should be differentiated from Crohn s disease (CD), are more frequent in Korea than in the West. Thus, the accurate diagnosis of these inflammatory diseases is problematic in Korea and clinicians should fully understand their clinical and endoscopic characteristics. Ulcerative colitis mostly presents with rectal inflammation and continuous lesions, while CD presents with discontinuous inflammatory lesions and frequently involves the ileocecal area. Involvement of fewer than four segments, a patulous ileocecal valve, transverse ulcers, and scars or pseudopolyps are more frequently seen in ITB than in CD. A few ulcers with discrete margins are a typical endoscopic finding of intestinal BD. However, the differential diagnosis is difficult in many clinical situations because typical endoscopic findings are not always observed. Therefore, clinicians should also consider symptoms and laboratory, pathological, and radiological findings, in addition to endoscopic findings. Clin Endosc 2016;49:370-375 Key Words: Inflammatory bowel diseases; Colitis, ulcerative; Crohn disease; Endoscopy; Diagnosis, differential INTRODUCTION Inflammatory bowel disease (IBD) is a chronic and idiopathic inflammatory disease of the digestive tract showing a remitting and relapsing disease course. Ulcerative colitis (UC) and Crohn s disease (CD) are two major forms of IBD. The number of patients with IBD has rapidly increased in recent years and is increasingly prominent in Korea. 1 However, many clinicians do not yet fully understand the clinical and endoscopic characteristics of IBD so that diagnosis is frequently delayed or incorrect in many cases. Accurate diagnosis of IBD is an important problem in Korea due to the higher prevalence of intestinal tuberculosis (ITB) and intestinal Behcet s Received: June 28, 2016 Revised: July 18, 2016 Accepted: July 20, 2016 Correspondence: Kang-Moon Lee Department of Internal Medicine, St. Vincent s Hospital, College of Medicine, The Catholic University of Korea, 93 Jungbu-daero, Paldal-gu, Suwon 16247, Korea Tel: +82-31-249-8151, Fax: +82-31-253-8898, E-mail: drmaloman@catholic.ac.kr cc This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License (http://creativecommons.org/ licenses/by-nc/3.0) which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited. disease (BD) than in the West. 2,3 Guidelines for diagnosis of IBD were established by the IBD Study Group of the Korean Association for the Study of Intestinal Diseases in 2009. 3-6 In this review, we delineate typical endoscopic findings and the differential diagnostic features of UC, CD, ITB, and intestinal BD based on these guidelines. TYPICAL ENDOSCOPIC FINDINGS OF INFLAMMATORY BOWEL DISEASE Ulcerative colitis The inflammation involves the rectum in most cases and spreads proximally. The typical endoscopic findings in patients with UC include edematous mucosa, erythema, loss of vascular markings, and mucosal friability. 4 More severe cases may be associated with erosions, ulcers, and spontaneous bleeding. Luminal narrowing and pseudopolyps may occur due to chronic inflammation, which results in mucosal atrophy (Fig. 1). 7-9 Focal inflammation around the appendiceal orifice is observed in up to 75% of patients with UC. 10 However, these typical findings are not always present. A 370 Copyright 2016 Korean Society of Gastrointestinal Endoscopy

Lee JM et al. Endoscopy in Inflammatory Bowel Disease A B D E C Fig. 1. Typical endoscopic features of ulcerative colitis. (A) Mild: mucosal erythema, fine granularity, decreased vascular marking. (B) Moderate: marked erythema, loss of vascular marking, erosions. (C) Severe: ulcers. (D) Severe: spontaneous bleeding. (E) Luminal narrowing with pseudopolyps. A B C Fig. 2. Typical endoscopic features of Crohn s disease. (A) Longitudinal ulcers, (B) cobblestone appearance, (C) aphthous ulcers showing longitudinal array. Korean study revealed that atypical distribution of inflammation was seen in 20% of newly diagnosed UC patients during initial colonoscopy: 3.3% had segmental UC with rectal sparing and 15.8% presented with segmental skip lesions without appendiceal orifice inflammation.11 Although inflammation in UC patients is mostly limited to the colon, ileal inflammation (backwash ileitis) may infrequently be observed.12 In this case, physicians should consider small bowel evaluation to differentiate CD from UC.13 Crohn s disease Typical endoscopic findings in CD include discontinuous distribution of longitudinal ulcers (defined as 4 to 5 cm ulcers in the Japanese criteria), cobblestone appearance, and/or small aphthous ulcerations arranged in a longitudinal fashion (Fig. 2).5,14 A Korean study reported longitudinal ulcers in 37.2%, cobblestone appearance in 23.9%, and aphthous ulcers in 59.3% of newly diagnosed CD cases. Non-caseating granuloma, a biopsy feature suggestive of CD, may be noted in only 13% to 36% of patients with CD so that sensitivity of biopsy is low.15 Esophagogastroduodenoscopy is not routinely recommended in CD patients unless upper gastrointestinal symptoms are present.5 Gastroduodenal CD presents with nonspecific 371

A B C Fig. 3. Typical endoscopic features of intestinal tuberculosis. (A) Transverse ulcers, (B) deformed and patulous ileocecal valve, (C) pseudopolyps. fewer than 50% of patients.20,21 Therefore, acquisition of more than three biopsy samples from the margin and base of ulcers is recommended to increase the diagnostic yield.3 Intestinal Behcet s disease Typical endoscopic findings in intestinal BD are a few, large, round, deep, and discrete ulcers with elevated margins in the ileocecal area (Fig. 4). Other atypical findings such as aphthous ulcers, irregular/geographic-shaped ulcers with focal distribution, and diffuse ulceration can be present in patients with intestinal BD.6,22 DIFFERENTIAL DIAGNOSIS OF INFLAMMATORY BOWEL DISEASE Ulcerative colitis and other causes of enterocolitis Fig. 4. Typical endoscopic feature of intestinal Behcet s disease. A large, round, deep, and discrete ulcer in the terminal ileum. lesions such as erosions, erythema, or ulcers.16 A bamboo joint-like appearance can be seen on endoscopy, characterized by swollen, longitudinal folds traversed by erosive fissures or linear furrows on the lesser curvature of the gastric body and cardia.17 Intestinal tuberculosis ITB frequently involves the ileocecal area and ascending colon. Endoscopic findings of ITB may include transverse ulcers, nodules with inflammatory changes of surrounding mucosa, pseudopolyps, and/or distorted and strictured ileocecal valves (Fig. 3).3,18,19 Although the typical histologic feature of caseating granuloma, positive acid-fast staining, and/or isolation of Mycobacterium tuberculosis from the culture of biopsy specimens can confirm ITB, these findings are present in 372 The differential diagnosis of UC includes infectious colitis, ischemic colitis, colitis due to drugs, radiation colitis, and solitary rectal ulcer syndrome.4,23 A history of preceding abdominal pain, medication use, radiation therapy, or straining during defecation can be helpful.4 Clinicians should always keep in mind that there is no specific endoscopic finding of UC. Infectious colitis can present with endoscopic features similar to those of UC. Thus, to make the correct diagnosis, onset and duration of symptoms should be considered together. Microbiological culture can also be helpful for differentiating UC from infectious colitis. Indeed, in a multinational web-based survey conducted by the Asian Organization for Crohn s and Colitis, more than half of Asian gastroenterologists reported always or usually performing microbiological culture for suspected UC.24 Ulcerative colitis and Crohn s disease UC mostly presents with rectal inflammation and continu-

Lee JM et al. Endoscopy in Inflammatory Bowel Disease Table 1. Differential Diagnosis of UC and CD Characteristic UC CD Rectal involvement Almost always Frequent Small bowel involvement Rare Frequent Continuous lesions Always Infrequent Depth of ulceration Mucosa Deeper than mucosa Cobblestone appearance No Yes Stricture Rare Frequent Fistula No Frequent Perianal lesions No Frequent panca ++ + ASCA + ++ UC, ulcerative colitis; CD, Crohn s disease; panca, perinuclear antineutrophil cytoplasmic antibodies; ASCA, anti-saccharomyces cerevisiae antibodies. Table 2. Endoscopic Characteristics of CD and ITB Characteristic CD ITB Involvement of ICV Common Usually, strictured and patulous ICV Involvement of colon 4 Segments, especially terminal ileum and ICV <4 Segments, especially ICV and ascending colon Ulcers Longitudinal Transverse Cobblestone appearance Frequent Rare Aphtous lesions Frequent Rare Perianal lesions Frequent Rare Scars/pseudopolyps + ++ CD, Crohn s disease; ITB, intestinal tuberculosis; ICV, ileocecal valve. ous lesions, while CD presents with discontinuous inflammatory lesions that frequently involve the ileocecal area. Shallow and indiscrete ulcers that involve only the mucosa, with edematous and erythematous changes in the surrounding area may suggest UC. 22 CD can involve not only the colon but also the small bowel, and frequently presents with deep ulcers. The deep ulcers with a longitudinal array create a cobblestone appearance. Sparing of the rectum, presence of perianal disease, and occurrence of strictures and fistulas suggest CD. Use of serologic markers may help in the differential diagnosis of UC and CD. 25,26 Anti-Saccharomyces cerevisiae antibodies (ASCA) can be detected in 35% to 50% of CD patients, but in only 1% of patients with UC. 26 On the other hand, perinuclear antineutrophil cytoplasmic antibodies (panca) are detected more frequently in patients with UC. The sensitivity of panca+ for UC was reportedly 55.3%, and ASCA+ in combination with panca resulted in 54.6% sensitivity for detection of CD. 25 Considering the relatively low sensitivity, serologic test can be the adjunctive tool when differentiation between CD and UC is clinically difficult (Table 1). Crohn s disease and intestinal tuberculosis The presence of longitudinal ulcers is a typical endoscopic finding in CD, whereas transverse ulcers are common in ITB (Table 2). However, since these typical findings are not always present, it is often difficult to differentiate between the two diseases. 23 In a Korean study that assessed the diagnostic value of various colonoscopic findings in CD and ITB, anorectal lesions, longitudinal ulcers, aphthous ulcers, and cobblestone appearance were seen frequently in CD, whereas involvement of fewer than four segments, a patulous ileocecal valve, transverse ulcers, and scars or pseudopolyps were observed commonly in ITB. 27 Using these parameters, the correct diagnosis was made in 87.5% of patients, with a positive predictive value of 94.9% for CD and 88.9% for ITB, respectively. However, this analysis method is still not validated, and further studies are needed. The typical histologic finding of caseating granuloma and positive acid-fast staining are seen in fewer than 30% of ITB patients, 28 but chest X-ray and interferon-γ assay may aid in the diagnosis of ITB. In fact, 67% of ITB patients had active pulmonary TB in a Korean study. 29 Therefore, chest X-ray is 373

an essential test in ITB. Interferon-γ assay may also be useful as a supplementary diagnostic tool for ITB. A recent Korean study reported that 66% of patients with ITB had a positive interferon-γ assay (QuantiFERON-TB Gold test), compared to 9.7% of patients with CD. 30 If accurate diagnosis of the two diseases remains unclear despite the above methods, performing follow-up colonoscopy after empirical anti-tb therapy can be helpful. 3 Crohn s disease and intestinal Behcet s disease A Korean study suggested an algorithm for the differential diagnosis of CD and intestinal BD according to endoscopic features. Ulcer shape, distribution, number, margins, and border contours, and the presence of aphthous, cobblestone, perianal, and strictured lesions enabled correct diagnosis of intestinal BD or CD in 92% of a study population. 31 Among these parameters, the most sensitive finding indicative of intestinal BD was the absence of a cobblestone appearance, and the most specific was a round ulcer shape. In addition, distribution patterns in patients with intestinal BD are more focal than in patients with CD. Therefore, a round ulcer or focally distributed lesions in the intestinal tract can suggest intestinal BD. Another Korean study proposed simple criteria for the diagnosis of intestinal BD using systemic and colonoscopic features. Five or fewer lesions, oval shape, deep penetration, discrete border, and ileocecal location were regarded as typical ulcerations in BD. Overall, the positive predictive value and diagnostic accuracy using these criteria were 86.1% and 91.1%, respectively. 32 CONCLUSIONS Colonoscopy is the principal test for diagnosing IBD. Clinicians can accurately diagnose most cases by fully understanding the typical endoscopic findings. In some cases, however, it is difficult to differentiate IBD due to an atypical presentation. Therefore, not only endoscopic features but also clinical symptoms, as well as laboratory, pathological, and radiological findings should be considered. Conflicts of Interest The authors have no financial conflicts of interest. REFERENCES 1. Yang SK, Yun S, Kim JH, et al. Epidemiology of inflammatory bowel disease in the Songpa-Kangdong district, Seoul, Korea, 1986-2005: a KASID study. Inflamm Bowel Dis 2008;14:542-549. 2. Suzuki Kurokawa M, Suzuki N. Behcet s disease. Clin Exp Med 2004;4:10-20. 3. 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