TY - JOUR
T1 - High Risk of Advanced Colorectal Neoplasia in Patients With Primary Sclerosing Cholangitis Associated With Inflammatory Bowel Disease
AU - Shah, Shailja C.
AU - ten Hove, Joren R.
AU - Castaneda, Daniel
AU - Palmela, Carolina
AU - Mooiweer, Erik
AU - Colombel, Jean Frédéric
AU - Harpaz, Noam
AU - Ullman, Thomas A.
AU - van Bodegraven, Ad A.
AU - Jansen, Jeroen M.
AU - Mahmmod, Nofel
AU - van der Meulen-de Jong, Andrea E.
AU - Ponsioen, Cyriel Y.
AU - van der Woude, Christine J.
AU - Oldenburg, Bas
AU - Itzkowitz, Steven H.
AU - Torres, Joana
N1 - Funding Information:
Conflicts of interest The authors disclose the following: J.–F.C. received research grants from AbbVie, Janssen Pharmaceuticals, and Takeda; speaking fees from AbbVie, Amgen, Ferring Pharmaceuticals, Shire, and Takeda; honoraria for advisory-board membership from AbbVie, Amgen, Boehringer Ingelheim, Celgene Corporation, Celltrion, Enterome, Ferring Pharmaceuticals, Genentech, Janssen Pharmaceuticals, Eli Lilly, Medimmune, Merck, Pfizer, Protagonist Therapeutics, Sandoz, Second Genome, Seres Therapeutics, Shire, Takeda, Theradiag, and Theravance Biopharma, and is a shareholder of Intestinal Biotech Development and Genfit. C.P. received consulting fees from Vitoria Laboratory, and travel support from Merck Sharp & Dohme and Abbvie. B.O. received research Grants from Dr. Falk Pharma, Takeda, Pfizer and Ferring; honoraria for advisory-board from Ferring, Pfizer, Janssen, Takeda, Abbvie, MSD, and speaker fees from MSD and Ferring. C.Y.P. received research grant and honoraria for advisory-board membership from Takeda and speaker's fees from Takeda, Abbvie Dr. Falk Pharma. J.M.J. received speaker fees from Janssen and advisory-board membership from MSD, Takeda, Janssen, Pfizer, Biogen, Fresenius, and Ferring. C.J.van der W. received research grants from Tramedico, Pfizer, and Takeda; speaker fees from Mundipharma, Celltrion, and Jansen and advisory-board membership from Pfizer, Takeda, MSD, Mundipharma, and Celltrion. J.T. received speaker fees from Takeda and consulting fees from Abbvie. The remaining authors disclose no conflicts.
Publisher Copyright:
© 2018 AGA Institute
PY - 2018/7
Y1 - 2018/7
N2 - Background & Aims: Patients with inflammatory bowel disease (IBD) and primary sclerosing cholangitis (PSC, termed PSC-IBD) are at increased risk for colorectal cancer, but their risk following a diagnosis of low-grade dysplasia (LGD) is not well described. We aimed to determine the rate of advanced colorectal neoplasia (aCRN), defined as high-grade dysplasia and/or colorectal cancer, following a diagnosis of indefinite dysplasia or LGD in this population. Methods: We performed a retrospective, longitudinal study of 1911 patients with colonic IBD (293 with PSC and 1618 without PSC) who underwent more than 2 surveillance colonoscopies from 2000 through 2015 in The Netherlands or the United States (9265 patient-years of follow-up evaluation). We collected data on clinical and demographic features of patients, as well as data from each surveillance colonoscopy and histologic report. For each surveillance colonoscopy, the severity of active inflammation was documented. The primary outcome was a diagnosis of aCRN during follow-up evaluation. We also investigated factors associated with aCRN in patients with or without a prior diagnosis of indefinite dysplasia or LGD. Results: Patients with PSC-IBD had a 2-fold higher risk of developing aCRN than patients with non-PSC IBD. Mean inflammation scores did not differ significantly between patients with PSC-IBD (0.55) vs patients with non-PSC IBD (0.56) (P =.89), nor did proportions of patients with LGD (21% of patients with PSC-IBD vs 18% of patients with non-PSC IBD) differ significantly (P =.37). However, the rate of aCRN following a diagnosis of LGD was significantly higher in patients with PSC-IBD (8.4 per 100 patient-years) than patients with non-PSC IBD (3.0 per 100 patient-years; P =.01). PSC (adjusted hazard ratio [aHR], 2.01; 95% CI, 1.09–3.71), increasing age (aHR 1.03; 95% CI, 1.01–1.05), and active inflammation (aHR, 2.39; 95% CI, 1.63–3.49) were independent risk factors for aCRN. Dysplasia was more often endoscopically invisible in patients with PSC-IBD than in patients with non-PSC IBD. Conclusions: In a longitudinal study of almost 2000 patients with colonic IBD, PSC remained a strong independent risk factor for aCRN. Once LGD is detected, aCRN develops at a higher rate in patients with PSC and is more often endoscopically invisible than in patients with only IBD. Our findings support recommendations for careful annual colonoscopic surveillance for patients with IBD and PSC, and consideration of colectomy once LGD is detected.
AB - Background & Aims: Patients with inflammatory bowel disease (IBD) and primary sclerosing cholangitis (PSC, termed PSC-IBD) are at increased risk for colorectal cancer, but their risk following a diagnosis of low-grade dysplasia (LGD) is not well described. We aimed to determine the rate of advanced colorectal neoplasia (aCRN), defined as high-grade dysplasia and/or colorectal cancer, following a diagnosis of indefinite dysplasia or LGD in this population. Methods: We performed a retrospective, longitudinal study of 1911 patients with colonic IBD (293 with PSC and 1618 without PSC) who underwent more than 2 surveillance colonoscopies from 2000 through 2015 in The Netherlands or the United States (9265 patient-years of follow-up evaluation). We collected data on clinical and demographic features of patients, as well as data from each surveillance colonoscopy and histologic report. For each surveillance colonoscopy, the severity of active inflammation was documented. The primary outcome was a diagnosis of aCRN during follow-up evaluation. We also investigated factors associated with aCRN in patients with or without a prior diagnosis of indefinite dysplasia or LGD. Results: Patients with PSC-IBD had a 2-fold higher risk of developing aCRN than patients with non-PSC IBD. Mean inflammation scores did not differ significantly between patients with PSC-IBD (0.55) vs patients with non-PSC IBD (0.56) (P =.89), nor did proportions of patients with LGD (21% of patients with PSC-IBD vs 18% of patients with non-PSC IBD) differ significantly (P =.37). However, the rate of aCRN following a diagnosis of LGD was significantly higher in patients with PSC-IBD (8.4 per 100 patient-years) than patients with non-PSC IBD (3.0 per 100 patient-years; P =.01). PSC (adjusted hazard ratio [aHR], 2.01; 95% CI, 1.09–3.71), increasing age (aHR 1.03; 95% CI, 1.01–1.05), and active inflammation (aHR, 2.39; 95% CI, 1.63–3.49) were independent risk factors for aCRN. Dysplasia was more often endoscopically invisible in patients with PSC-IBD than in patients with non-PSC IBD. Conclusions: In a longitudinal study of almost 2000 patients with colonic IBD, PSC remained a strong independent risk factor for aCRN. Once LGD is detected, aCRN develops at a higher rate in patients with PSC and is more often endoscopically invisible than in patients with only IBD. Our findings support recommendations for careful annual colonoscopic surveillance for patients with IBD and PSC, and consideration of colectomy once LGD is detected.
KW - Colon cancer
KW - Crohn's Disease
KW - Primary Sclerosing Cholangitis
KW - Surveillance
KW - Ulcerative Colitis
UR - http://www.scopus.com/inward/record.url?scp=85047333269&partnerID=8YFLogxK
U2 - 10.1016/j.cgh.2018.01.023
DO - 10.1016/j.cgh.2018.01.023
M3 - Article
C2 - 29378311
AN - SCOPUS:85047333269
SN - 1542-3565
VL - 16
SP - 1106-1113.e3
JO - Clinical Gastroenterology and Hepatology
JF - Clinical Gastroenterology and Hepatology
IS - 7
ER -