Association of bone mineral density with a dinucleotide repeat polymorphism at the calcitonin (CT) locus

被引:0
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作者
M. Miyao
T. Hosoi
M. Emi
T. Nakajima
S. Inoue
S. Hoshino
M. Shiraki
H. Orimo
Y. Ouchi
机构
[1] Department of Geriatric Medicine,
[2] Graduate School of Medicine,undefined
[3] The University of Tokyo,undefined
[4] Tokyo,undefined
[5] Japan,undefined
[6] Department of Molecular Biology,undefined
[7] Institute of Gerontology,undefined
[8] Nippon Medical School,undefined
[9] 1-396 Kosugi-cho,undefined
[10] Nakahara-ku,undefined
[11] Kawasaki 211-8533,undefined
[12] Japan Tel. +81-44-733-5230; Fax +81-44-733-5192 e-mail: memi@nms.ac.jp,undefined
[13] Research Institute and Practice for Involutional Diseases,undefined
[14] Nagano,undefined
[15] Japan,undefined
[16] Department of Endocrinology,undefined
[17] Tokyo Metropolitan Geriatric Hospital,undefined
[18] Tokyo,undefined
[19] Japan,undefined
来源
Journal of Human Genetics | 2000年 / 45卷
关键词
Key words Calcitonin gene; Bone mineral density; Osteoporosis; Microsatellite polymorphism; Risk factors;
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摘要
Calcitonin (CT), a calcium-regulating hormone, lowers the calcium level in serum by inhibiting bone resorption. Because CT may play a role in the pathogenesis of osteoporosis, genetic variations in or adjacent to the CT gene may be associated with variations in bone mineral density (BMD). The present study examined the correlation between a dinucleotide (cytosine-adenine; CA) repeat polymorphism at the CT locus and BMD in 311 Japanese postmenopausal women (mean age, 64.1 years). Seven alleles were present in this population; each allele contained 10, 11, 16, 17, 18, 19, or 20 CA repeats. Thus, we designated the respective genotypes A10, A11, A16, A17, A18, A19, and A20. The A10 and A17 alleles were the predominant alleles in the population studied. Z scores (a parameter representing deviation from the age-specific weight-adjusted average BMD) were compared between individuals that possessed one or two alleles of each genotype and those that did not possess the allele. Subjects who possessed one or two A10 alleles had lower BMD Z scores than those who did not (lumbar 2–4 BMD Z score; −0.148 ± 1.23 vs 0.182 ± 1.54; P = 0.04). No significant relationships were observed between allelic status and background data or biochemical parameters. The significant association observed between BMD and genetic variations at the CT locus implies that polymorphism at this locus may be a useful marker for the genetic study of osteoporosis.
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页码:346 / 350
页数:4
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