Modifying Role of GSTP1 Polymorphism on the Association between Tea Fluoride Exposure and the Brick-Tea Type Fluorosis | Zendy

Junhua Wu | Zendy; Wei Wang | Zendy; Yang Liu | Zendy; Jing Sun | Zendy; Yan Ye | Zendy; Bingyun Li | Zendy; Xiaona Liu | Zendy; Hongxu Liu | Zendy; Zhenqi Sun | Zendy; Mang Li | Zendy; Jing Cui | Zendy; Dianjun Sun | Zendy; Yanmei Yang | Zendy; Yanhui Gao | Zendy

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Modifying Role of GSTP1 Polymorphism on the Association between Tea Fluoride Exposure and the Brick-Tea Type Fluorosis

Author(s) -

Junhua Wu,

Wei Wang,

Yang Liu,

Jing Sun,

Yan Ye,

Bingyun Li,

Xiaona Liu,

Hongxu Liu,

Zhenqi Sun,

Mang Li,

Jing Cui,

Dianjun Sun,

Yanmei Yang,

Yanhui Gao

Publication year - 2015

Publication title -

plos one

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 0.99

H-Index - 332

ISSN - 1932-6203

DOI - 10.1371/journal.pone.0128280

Subject(s) - skeletal fluorosis , single nucleotide polymorphism , medicine , genotype , gstp1 , dental fluorosis , gene polymorphism , allele , cross sectional study , fluoride , dentistry , genetics , biology , pathology , gene , chemistry , inorganic chemistry

Background Brick tea type fluorosis is a public health concern in the north-west area of China. The association between SNPs of genes influencing bone mass and fluorosis has attracted attention, but the association of SNPs with the risk of brick-tea type of fluorosis has not been reported. Objective To investigate the modifying roles of GSTP1 rs1695 polymorphisms on this association. Methods A cross-sectional study was conducted. Brick-tea water was tested by the standard of GB1996-2005 (China). Urinary fluoride was tested by the standard of WS/T 89-2006 (China). Skeletal fluorosis was diagnosed by X-ray, the part we scheduled was forearm, shank, and pelvic, then diagnosed the skeletal fluorosis by the standard of WS/192-2008 (China). Gene polymorphism was tested by Sequenom MassARRAY system. Result The prevalence rate in different ethnical participants was different: Tibetan individuals had the highest prevalence rate of skeletal fluorosis. There were significant differences in genotype frequencies of GSTP1 Rs1695 among different ethnical participants (p<0.001): Tibetan, Mongolian and Han subjects with homozygous wild type (GSTP1-AA) genotype were numerically higher than Kazakh and Russian subjects ( p <0.001). Compared to Tibetan participants who carried homozygous A allele of GSTP1 Rs1695, Tibetan participants who carried G allele had a significantly decreased risk of skeletal fluorosis (OR = 0.558 [95% CI, 0.326-0.955]). For Kazakh participants, a decreased risk of skeletal fluorosis among carriers of the G allele was limited to non high-loaded fluoride status (OR = 0. 166 [95% CI, 0.035–0.780] vs. OR = 1.478 [95% CI, 0.866–2.552] in participants with high-loaded fluoride status). Neither SNP-IF nor SNP-age for GSTP1 Rs1695 was observed. Conclusion The prevalence rate of the brick tea type fluorosis might have ethnic difference. For Tibetan individuals, who had the highest prevalence rate, G allele of GSTP1 Rs1695 might be a protective factor for brick tea type skeletal fluorosis.

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