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Association study of anti-Mllerian hormone and anti-Mllerian hormone type II receptor polymorphisms with idiopathic primary ovarian insufficiencyopen access

Authors
Yoon, S. H.Choi, Y. M.Hong, M. A.Kim, J. J.Lee, G. H.Hwang, K. R.Moon, S. Y.
Issue Date
Dec-2013
Publisher
OXFORD UNIV PRESS
Keywords
AMH; AMHR2; polymorphism; primary ovarian insufficiency
Citation
HUMAN REPRODUCTION, v.28, no.12, pp 3301 - 3305
Pages
5
Indexed
SCI
SCIE
SCOPUS
Journal Title
HUMAN REPRODUCTION
Volume
28
Number
12
Start Page
3301
End Page
3305
URI
https://scholarworks.dongguk.edu/handle/sw.dongguk/17454
DOI
10.1093/humrep/det384
ISSN
0268-1161
1460-2350
Abstract
Are the genetic polymorphisms of the anti-Mllerian hormone (AMH) and anti-Mllerian hormone type II receptor (AMHR2) genes associated with idiopathic primary ovarian insufficiency (POI) in a Korean population? The distribution of the AMH and the AMHR2 polymorphisms in a Korean POI population was not significantly different from controls. AMH plays an important role in regulating both the primordial follicle recruitment and the cyclic selection of the antral follicles. The AMHR2 -482AG polymorphism was associated with an earlier menopause and nulliparous women with the GG genotype had a 2.6 years earlier onset of menopause compared with the AA genotype women. Therefore, genetic variants in the AMH signal transduction pathway might affect the ovarian function of women. Casecontrol study. The subjects consisted of 211 idiopathic POI patients and 233 post-menopausal controls. The frequency of the AMH Ile(49)Ser and AMHR2 -482AG polymorphisms was analyzed in 211 patients with idiopathic POI and in 233 post-menopausal controls, and we also analyzed clinical characteristics, such as age at the time of POI and LH, FSHas well as estradiol levels according to the specific genotype. Genotyping for the AMH Ile(49)Ser and the AMHR2 -482AG polymorphisms was performed by a minor groove binder primer/probe Taqman assay. The genotype distributions and allele frequencies for the AMH Ile(49)Ser and the AMHR2 -482AG polymorphisms were similar between the POI patients and the controls. Within POI population, the AMH Ile(49)Ser and the AMHR2 -482AG polymorphisms were not associated with age at the time of POI and LH, FSH as well as estradiol levels. Haplotype analysis also showed no significant difference between groups. Study is limited to a Korean population. Our findings suggest that genetic variants in the AMH signal transduction pathway may not influence the susceptibility of idiopathic POI. This is the first report on the association between the AMH and AMHR2 polymorphisms and idiopathic POI.
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