Identification of a novel polymorphism of estrogen receptor-a gene that is associated with calcium excretion in urine
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- 作者:Shinjiro Hoshino ; Takayuki Hosoi ; Mariko Miyao ; Masataka Shiraki ; Hajime Orimo ; Yasuyoshi Ouchi and Satoshi Inoue
- 关键词:Key words ; estrogen receptor ; polymorphism ; genetics ; calcium ; bone
- 刊名:Journal of Bone and Mineral Metabolism
- 出版时间:April 2000
- 出版年:2000
- 期刊代码:115_0914-8779
- 类别:med
- 卷:18
- 期:3
- 页码:153-157
- 数据来源:sp
摘要
A novel variation of the estrogen receptor-α (ERα) gene was identified by polymerase chain reaction–single-strand conformational polymorphism (PCR-SSCP). It is one base substitution in codon 325 (CCC [allele M] to CCG [allele m]) in exon 4 of the human ERα gene. This substitution did not cause an amino acid change. We categorized 306 unrelated Japanese postmenopausal women into three genotypes: MM, Mm, and mm; the frequency of each genotype was 26.5%, 43.1%, and 30.4%, respectively. Then, the association of this polymorphism with bone mineral density (BMD) of lumbar spine and bone–calcium metabolic markers was studied. There was no significant difference in BMD of the lumbar spine or most of the bone metabolic markers. However, the urinary calcium (Ca) excretion ratio (u-Ca/Cre) corrected by creatinine was significantly lower in the genotype mm group compared with the genotype MM group (MM vs mm, 0.247 卤 0.158 vs 0.200 卤 0.105; P < 0.05). We examined the relationship of restriction fragment length polymorphisms (RFLPs) (PvuII, XbaI) in intron 1 and the polymorphism in exon 4. The frequency of genotype MM was higher in the genotype PPxx, which was reported to be associated with lower BMD in the same population of Japanese postmenopausal women. The ER polymorphism identified in this study might be related to some biological mechanisms that regulate calcium metabolism.