Literature DB >> 29603369

Clinical and genetic risk factors for decreased bone mineral density in Japanese patients with inflammatory bowel disease.

Takeo Naito1, Naonobu Yokoyama1, Yoichi Kakuta1, Kazuko Ueno2, Yosuke Kawai2, Motoyuki Onodera1, Rintaro Moroi1, Masatake Kuroha1, Yoshitake Kanazawa1, Tomoya Kimura1, Hisashi Shiga1, Katsuya Endo1, Masao Nagasaki2, Atsushi Masamune1, Yoshitaka Kinouchi3, Tooru Shimosegawa1.   

Abstract

BACKGROUND AND AIM: Patients with inflammatory bowel disease (IBD) are at a high risk of low bone mineral density (BMD). Reportedly, clinical and genetic factors cause low BMD in Caucasians; however, studies in non-Caucasian populations remain scarce.
METHODS: Clinical risk factors for low BMD were investigated in 266 Japanese patients with IBD, and a genome-wide association analysis (GWAS) was performed using linear regression with associated clinical factors as covariates. Genotyping was performed using a population-optimized genotyping array (Japonica array® ). After quality control, the genotype data of 4 384 682 single-nucleotide polymorphisms (SNPs) from 254 patients with IBD were used for GWAS.
RESULTS: Body mass index, age, and disease duration were independently associated with the BMD of the femoral neck (P = 1.41E - 13, 1.04E - 5, and 1.58E - 3, respectively), and body mass index and sex were associated with the BMD of the lumbar spine (P = 6.90E - 10 and 6.84E - 3, respectively). In GWAS, 118 and 42 candidate SNPs of the femoral neck and lumbar spine, respectively, were identified. Among 118, 111 candidate SNPs of the femoral neck were located within the SLC22A23 gene, which is a known IBD susceptibility gene (minimum P = 1.42E - 07). Among 42, 18 candidate SNPs of the lumbar spine were located within the MECOM gene, which is associated with osteopenia (minimum P = 5.86E - 07). Interestingly, none of the known loci showed a significant association with BMD.
CONCLUSIONS: Although clinical risk factors for low BMD in IBD were similar to those in the general population, genetic risk factors were rather different.
© 2018 Journal of Gastroenterology and Hepatology Foundation and John Wiley & Sons Australia, Ltd.

Entities:  

Keywords:  genome-wide association analysis; inflammatory bowel disease genetics; osteoporosis

Mesh:

Substances:

Year:  2018        PMID: 29603369     DOI: 10.1111/jgh.14149

Source DB:  PubMed          Journal:  J Gastroenterol Hepatol        ISSN: 0815-9319            Impact factor:   4.029


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