Allelic variation at the interleukin 1β gene is associated with decreased bone mass in patients with inflammatory bowel diseases

Background-Interleukin 1 beta (IL-1 beta) and its natural antagonist have been implicated in the pathogenesis of inflammatory bowel disease (IBD). Both cytokines influence bone formation. IL-1 beta stimulates osteoclast activity while interleukin I receptor antagonist (IL-1ra) enhances bone formation. Aims-To determine whether the decreased bone mass in IBD is related to gene polymorphisms coding for IL-1 beta and IL-1ra, and thus identify patients with an increased risk. Methods-Bone mineral densitometry was performed at the femoral neck, lumbar spine, and the distal third of the radius in 75 IBD patients (34 men/41 women; 40.3 (1.6) years) and in 58 healthy controls (HC; 28 men/30 women; 32.4 (1.2) years). Values were correlated with the TaqI and Aval gene polymorphisms in the IL1B and the variable number of tandem repeats gene polymorphism in the IL1RN gene. Results-In IBD patients, but not in HC, carriers of allele 2 at the Aval gene polymorphism (IL1B-511*2) had significantly lower Z scores at the lumbar spine (-0.82 (0.13) v -0.29 (0.21) p = 0.03) and the femoral neck (-0.59 (0.14) v 0.15 (0.19); p = 0.003) than non-carriers.. These patients also had a higher risk for osteopenia or osteoporosis at the femoral neck (odds ratio 3.63 (95% confidence interval 0.95-13.93)). No association was found between bone mass and the other gene polymorphisms analysed in IBD patients or in HC. Conclusions-Our results suggest that genetic variability may be a major determinant of bone loss in IBD. Carriers of IL1B-511*2, who are hypersecretors of IL-1 beta, have a higher risk of presenting with low bone mass in IBD. Screening for this allele may contribute to determination of the risk of bone loss at the time of disease onset.