Clinicopathological and Molecular Characterisation of Crohn’s Disease-associated Small Bowel Adenocarcinomas

Author:

Liao Xiaoyan12,Li Guangyuan2,McBride Russel2,Houldsworth Jane2,Harpaz Noam2,Polydorides Alexandros D2

Affiliation:

1. Department of Pathology and Laboratory Medicine, University of Rochester Medical Center, Rochester, NY, USA

2. Department of Pathology, Mount Sinai Hospital, New York, NY, USA

Abstract

Abstract Background and Aims Small bowel adenocarcinoma [SBA] is a recognised complication of Crohn’s disease [CD], but its low absolute prevalence limits opportunities for clinicopathological characterisation. Methods We compared the clinical, pathological, and molecular features of 48 SBA from patients with CD [CDSBA] and 29 SBAs from patients without CD [NSBA] who underwent treatment at our tertiary care centre between 2000 and 2018. Results Patients with CDSBA were younger than those with NSBA [mean age, 56 vs 64; p = 0.02]. Males predominated in both groups. Most CDSBA [69%] occurred in the ileum, whereas most NSBA occurred in the duodenum [38%] and jejunum [31%; p < 0.001]. Stage I tumours were more prevalent in the CDSBA [33% vs 3%; p = 0.002], although the rates of Stage IV disease and disease-specific mortality were similar in both groups. CDSBA were less likely to present a discrete mass [35% vs 93%; p < 0.001] and were more often stricturing or fistulising [75% vs 10%, respectively, p < 0.001] than NSBA. Microscopically, CDSBA were relatively heterogeneous, exhibiting at least three distinct growth patterns in 39% compared with 1% of NSBA [p = 0.01]. Low-grade tubuloglandular adenocarcinoma was the predominant pattern in 19% of CDSBA compared with 0% of NSBA [p = 0.003]. CDSBA were more frequently DNA mismatch repair proficient [90% vs 62%; p = 0.04] and exhibited profiles of frequently mutated genes similar to those of NSBA, except for IDH1 [18%] and SMAD4 [12%] mutations that occurred uniquely in CDSBA. Conclusions These observations, based on the largest single-centre series described hitherto, establish that CDSBA is a distinct clinical, pathological, and molecular entity.

Funder

Department of Pathology at Mount Sinai Hospital

Publisher

Oxford University Press (OUP)

Subject

Gastroenterology,General Medicine

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