Abstract
Objectives: Pancreas divisum (PD) as a cause of pancreatitis has been debated. In this study, we report the association of multiple gene polymorphisms on the risk of RAP in the presence of PD. Design: We enrolled 687 individuals (167 IRAP, 276 ICP, and 244 unrelated healthy controls) from May 2015 to September 2016. Patients were divided into those with/without PD. Associations between the significantly prevalent SNPs and IRAP/ICP in the presence of PD were evaluated. Clinical data were analyzed using Mann–Whitney U/Chi-square test. Effect size of association of SNPs with IRAP/ICP was expressed as odds ratio (OR) (95% CI). Gene–gene interaction was assessed by transheterozygosity analyses. Bonferroni-corrected two-tailed “p” value of ≤ 0.01 was considered statistically significant. Results: Thirty-three (19.8%) and 82 (29.7%) patients with IRAP and ICP, respectively, had PD. Among the patients with IRAP, duration of disease was significantly shorter in those with PD compared to those without (mean [95% CI] duration: 1.6 (1.3–1.9) vs 2.7 (2.3–3.1) years; p = 0.005). There were no differences in gender, race, and diabetes among patients with/without PD in IRAP/ICP groups. Mean (95% CI) pancreatic duct diameter (mm) was significantly higher in the presence of PD in patients with both IRAP [1.6 (1.4–1.9) v/s 1.29 (1.2–1.4); p = 0.03)] and ICP [5.2 (4.5–5.9) v/s 4.5 (3.9–5.1); p = 0.02]. CTSB (rs12338) polymorphisms were significantly associated with IRAP [OR (95% CI) 2.44 (1.41–4.22); p = 0.001] among patients with PD. No association was observed with ICP. Transheterozygosity analysis did not show any significant associations of combination of SNPs with IRAP in the presence of PD. Conclusion: Risk of RAP due to PD increases in patients with rs12338 polymorphism in the cathepsin B gene.
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Talukdar, R., Aslam, M., Reddy, D. N., Nabi, Z., Shava, U., Ravikanth, V. V., … Govardhan, B. (2021). Pancreas Divisum Increases the Risk of Recurrent Acute Pancreatitis in Patients with rs12338 Polymorphism in the Cathepsin B Gene. Digestive Diseases and Sciences, 66(7), 2283–2290. https://doi.org/10.1007/s10620-020-06517-7
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