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Recently, the G191R variant in anionic trypsinogen (coded by PRSS2) was reported to be strongly associated with chronic pancreatitis (CP) (odds ratio (OR) = 0.37, p = 1.1×10−8) in European patients with CP1 and subsequently replicated in Hungarian and Japanese patients with CP.2 3 We and others have earlier shown that CP in tropical countries such as India and Bangladesh, especially tropical calcific pancreatitis (TCP), has a variable genetic basis compared to that in Europeans and rather than cationic trypsinogen (coded by PRSS1) mutations,3 4 variants in SPINK1 encoding the pancreatic secretory trypsin inhibitor or cathepsin B (CTSB) or chymotrypsin C predict susceptibility to TCP.3–7 We, therefore, investigated using a case–control approach whether G191R PRSS2 variant also confers protection against TCP.
We analysed the G191R variant in the PRSS2 gene by direct sequencing in 700 patients with CP including 500 patients with TCP, 155 patients having idiopathic chronic pancreatitis (ICP) and 45 with alcoholic pancreatitis (see supplementary material). On initial screening of 299 patients with TCP and 277 control subjects, the minor allele frequency (MAF) of the G191R variant was significantly lower compared to Europeans1 and was similar in both the groups (0.3%). Genotyping and pooled analysis of additional patients with CP and normal subjects showed comparable frequency of …
Footnotes
Competing interests: None.
Funding: The study was supported by funds from Council of Scientific and Industrial Research (CSIR), Ministry for Science and Technology, Government of India, India (NWP0032).
Ethics approval: The Institutional Ethics Committees of the respective institutions approved the study, as per the guidelines of the Indian Council of Medical Research for study on human subjects, on 7 June 2007.
▸ A supplementary table and additional details of the patients and methods are published online only at http://gut.bmj.com/content/vol58/issue6