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자료유형
학술저널
저자정보
Hwang, Joo-Yeon (Center for Genome Science, National Institute of Health, Osong Health Technology Administration Complex) Lee, Seung-Hun (Division of Endocrinology and Metabolism, Asan Medical Center, University of Ulsan College of Medicine) Go, Min-Jin (Center for Genome Science, National Institute of Health, Osong Health Technology Administration Complex) Kim, Beom-Jun (Division of Endocrinology and Metabolism, Asan Medical Center, University of Ulsan College of Medicine) Kim, Young-Jin (Center for Genome Science, National Institute of Health, Osong Health Technology Administration Complex) Kim, Dong-Joon (Center for Genome Science, National Institute of Health, Osong Health Technology Administration Complex) Oh, Ji-Hee (Center for Genome Science, National Institute of Health, Osong Health Technology Administration Complex) Koo, Hee-Jo (Center for Genome Science, National Institute of Health, Osong Health Technology Administration Complex) Cha, My-Jung (Center for Genome Science, National Institute of Health, Osong Health Technology Administration Complex) Lee, Min-Hye (Center for Genome Science, National Institute of) Yun, Ji-Young Yoo, Hye-Sook Kang, Young-Ah Oh, Ki-Won Kang, Moo-Il Son, Ho-Young Kim, Shin-Yoon Kim, Ghi-Su Han, Bok-Ghee Cho, Yoon-Shin Koh, Jung-Min Lee, Jong-Young
저널정보
한국유전체학회 Genomics & informatics Genomics & informatics 제9권 제2호
발행연도
2011.1
수록면
52 - 58 (7page)

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Osteoporotic fracture (OF), along with bone mineral density (BMD), is an important diagnostic parameter and a clinical predictive risk factor in the assessment of osteoporosis in the elderly population. However, a genome-wide association study (GWAS) on OF has not yet been clarified sufficiently. To identify OF-associated genetic variants and candidate genes, we conducted a GWAS in a population-based cohort (Korean Association Resource [KARE], n=1,427 [case: 288 and control: 1139]) and performed a de novo replication study in hospital-based individuals (Asan and Catholic Medical Center [ACMC], n=1,082 [case: 272 and control: 810]). In a combined meta-analysis, a newly identified genetic locus in an intergenic region at 10p11.2 (near genes FZD8 and ANKRD30A ) showed the most significant association (odd ratio [OR] = 2.00, 95% confidence interval [CI] = 1.47~2.74, p=$1.27{\times}10^{-6}$) in the same direction. We provide the first evidence for a common genetic variant influencing OF and genetic information for further investigation in bone metabolism.

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