Associations between Vitamin D-Binding Protein (DBP) Gene Polymorphism (TAAA)n and Development of Osteoporosis in the Volga-Ural Region of Russia

Хусаинова, Р. И.; Seleznyova, L. I.; Maltsev, Andrey V.; Shakirova, R. Ya.; Nurlygayanov, R. Z.; Надыршина, Д. Д.; Хуснутдинова, Э. К.

doi:10.1007/s10517-014-2538-5

Cited by 3 publications

(1 citation statement)

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“…Genotyping based on rs4588 of the GC gene showed that total hip-bone mineral content was associated with GC genotype (p = 0.05, ANCOVA) in boys [ 116 ]. In women of postmenopausal age, DBP ∗ 10 (with 10 repeats of TAAA) is associated with lower incidence of bone fracture compared with relevant controls, while DBP ∗ 11 is related to higher incidence [ 117 ]. Another study showed that DBP ∗ 10 and DBP ∗ 11 are both associated with lower risks of osteoporosis [ 118 ].…”

Section: Peripheral Oscillators In Bonementioning

confidence: 99%

Insights into the Role of Circadian Rhythms in Bone Metabolism: A Promising Intervention Target?

Song

Wang

Kim

et al. 2018

BioMed Research International

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Numerous physiological processes of mammals, including bone metabolism, are regulated by the circadian clock system, which consists of a central regulator, the suprachiasmatic nucleus (SCN), and the peripheral oscillators of the BMAL1/CLOCK-PERs/CRYs system. Various bone turnover markers and bone metabolism-regulating hormones such as melatonin and parathyroid hormone (PTH) display diurnal rhythmicity. According to previous research, disruption of the circadian clock due to shift work, sleep restriction, or clock gene knockout is associated with osteoporosis or other abnormal bone metabolism, showing the importance of the circadian clock system for maintaining homeostasis of bone metabolism. Moreover, common causes of osteoporosis, including postmenopausal status and aging, are associated with changes in the circadian clock. In our previous research, we found that agonism of the circadian regulators REV-ERBs inhibits osteoclast differentiation and ameliorates ovariectomy-induced bone loss in mice, suggesting that clock genes may be promising intervention targets for abnormal bone metabolism. Moreover, osteoporosis interventions at different time points can provide varying degrees of bone protection, showing the importance of accounting for circadian rhythms for optimal curative effects in clinical treatment of osteoporosis. In this review, we summarize current knowledge about circadian rhythms and bone metabolism.

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Section: Peripheral Oscillators In Bonementioning

confidence: 99%