Abstract

Gallbladder disease (GBD) has an overall prevalence of 10–40% depending on factors such as age, gender, population, obesity and diabetes, and represents a major economic burden. Although gallstones are composed of cholesterol by-products and are associated with obesity, presumed causal pathways remain unproven, although BMI reduction is typically recommended. We performed genetic studies to discover candidate genes and define pathways involved in GBD. We genotyped 15 241 women of European ancestry from three cohorts, including 3216 with GBD, using the Human cardiovascular disease (HumanCVD) BeadChip containing up to ~53 000 single-nucleotide polymorphisms (SNPs). Effect sizes with P-values for development of GBD were generated. We identify two new loci associated with GBD, GCKR rs1260326:T>C (P=5.88 × 10−7, ß=−0.146) and TTC39B rs686030:C>A (P=6.95x10−7, ß=0.271) and detect four independent SNP effects in ABCG8 rs4953023:G>A (P=7.41 × 10−47, ß=0.734), ABCG8 rs4299376:G>T (P=2.40 × 10−18, ß=0.278), ABCG5 rs6544718:T>C (P=2.08 × 10−14, ß=0.044) and ABCG5 rs6720173:G>C (P=3.81 × 10−12, ß=0.262) in conditional analyses taking genotypes of rs4953023:G>A as a covariate. We also delineate the risk effects among many genotypes known to influence lipids. These data, from the largest GBD genetic study to date, show that specific, mainly hepatocyte-centred, components of lipid metabolism are important to GBD risk in women. We discuss the potential pharmaceutical implications of our findings.

Highlights

  • Gallbladder disease (GBD) is a major cause of morbidity, hospital admission, surgical intervention and economic burden and is caused by gallstones.[1]

  • The resource comprises nine cohort studies funded by the NHLBI including: Atherosclerosis Risk in Communities (ARIC), Cardiovascular Health Study (CHS), Cleveland Family Study (CFS), Coronary Artery Risk Development in Young Adults (CARDIA), Framingham Heart Study (FHS), Jackson Heart Study (JHS), Multi-Ethnic Study of Atherosclerosis (MESA) and the Sleep Heart Health Study (SHHS)

  • single-nucleotide polymorphism (SNP) with P-value o1 × − 4 (37 SNPs in total) explain 0.0808 of the variance in ARIC, while they explain 0.0917 of the variance in WHI

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Summary

Introduction

Gallbladder disease (GBD) is a major cause of morbidity, hospital admission, surgical intervention and economic burden and is caused by gallstones.[1] Gallstones occur in 10–40% of adults in developed countries,[2] predominantly in women.[3] The incidence increases with age and other factors such as obesity and diabetes, there are differences between men and women in the determinants of GBD.[4]. These differences make advisable the analysis of the genetic basis of GBD separate by sex. Large genetic studies have shown that the additive genetic heritability of symptomatic gallstones ranges from 25 to 29%.7,8

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