Vitamin D Receptor in Osteoblasts Is a Negative Regulator of Bone Mass Control

Yamamoto, Yasutake; Yoshizawa, Tatsuya; Fukuda, Tsuyoshi; Shirode-Fukuda, Yuko; Yu, Taiyong; Sekine, Keisuke; Satō, Takashi; Kawano, Hirotaka; Aihara, Ken‐ichi; Nakamichi, Yuko; Watanabe, Tomoyuki; Shindo, Masayo; Inoue, Kenzo; Inoue, Erina; Tsuji, Naoya; Hoshino, Maiko; Karsenty, G.; Metzger, Daniel; Chambon, Pierre; Kato, Shigeaki; Imai, Yuuki

doi:10.1210/en.2012-1542

Cited by 152 publications

(104 citation statements)

References 45 publications

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“…With a few exceptions (27,28), most of the previous histomorphometric studies have shown increased bone resorption among hypercalciuric patients (3,5,7,8). Vitamin D-induced osteoclastogenesis seems to be accomplished through a VDR-mediated increase in RANKL expression in osteoblasts (36).…”

Section: Discussionmentioning

confidence: 97%

Expression of Fibroblast Growth Factor 23, Vitamin D Receptor, and Sclerostin in Bone Tissue from Hypercalciuric Stone Formers

Menon

Moysés

Gomes

et al. 2014

Clinical Journal of the American Society of Nephrology

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Background and objectives Increased bone resorption, low bone formation, and abnormal mineralization have been described in stone formers with idiopathic hypercalciuria. It has been previously shown that the receptor activator of NF-kB ligand mediates bone resorption in idiopathic hypercalciuria (IH). The present study aimed to determine the expression of fibroblast growth factor 23 (FGF-23), vitamin D receptor (VDR), and sclerostin in bone tissue from IH stone formers.Design, setting, participants, & measurements Immunohistochemical analysis was performed in undecalcified bone samples previously obtained for histomorphometry from 30 transiliac bone biopsies of idiopathic hypercalciuria stone-forming patients between 1992 and 2002 and 33 healthy individuals (controls). Serum parameters were obtained from their medical records.Results Histomorphometry disclosed 21 IH patients with high and 9 IH patients with normal bone resorption. Importantly, eroded surfaces (ES/BS) from IH patients but not controls were significantly correlated with VDR immunostaining in osteoblasts (r=0.51; P=0.004), sclerostin immunostaining in osteocytes (r=0.41; P=0.02), and serum 1,25-dihydroxyvitamin D (r=0.55; P,0.01). Of note, both VDR and sclerostin immunostaining were significantly correlated with serum 1,25-dihydroxyvitamin D in IH patients (r=0.52; P=0.01 and r=0.53; P=0.02, respectively), although VDR and sclerostin expression did not differ between IH and controls. IH patients with high bone resorption exhibited a significantly stronger sclerostin immunostaining than IH patients with normal bone resorption. FGF-23 expression in osteocytes from IH patients did not differ from controls and was not correlated with any histomorphometric parameter.Conclusions These findings suggest the contribution of VDR and sclerostin, as well as 1,25-dihydroxyvitamin D, to increase bone resorption in idiopathic hypercalciuria but do not implicate FGF-23 in the bone alterations seen in these patients.

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Section: Discussionmentioning

confidence: 97%

Expression of Fibroblast Growth Factor 23, Vitamin D Receptor, and Sclerostin in Bone Tissue from Hypercalciuric Stone Formers

Menon

Moysés

Gomes

et al. 2014

Clinical Journal of the American Society of Nephrology

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“…The role of VDR signaling in bone cells during a positive calcium balance is still not fully elucidated, but the specific effects likely depend on the osteoblast differentiation stage (FIGURE 6). VDR signaling in osteoprogenitors and osteoblasts has a positive effect on osteoclast formation and bone resorption and thus negatively regulates bone mass, as shown by Vdr inactivation in mice using the collagen type I promoter which resulted in increased bone mass (501). On the other hand, VDR activity in more mature osteoblasts has anabolic and anticatabolic activity and increases bone mass, as evidenced by Vdr overexpression using the osteocalcin promotor (29, 157).…”

Section: Role Of Osteoblastic/osteocytic Vdr Signaling In Bone Homeosmentioning

confidence: 99%

Vitamin D: Metabolism, Molecular Mechanism of Action, and Pleiotropic Effects

Christakos

Dhawan

Verstuyf

et al. 2016

Physiological Reviews

1,470

1,234

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, [1,25(OH) 2 D 3 ] is the hormonally active form of vitamin D. The genomic mechanism of 1,25(OH) 2 D 3 action involves the direct binding of the 1,25(OH) 2 D 3 activated vitamin D receptor/retinoic X receptor (VDR/RXR) heterodimeric complex to specific DNA sequences. Numerous VDR co-regulatory proteins have been identified, and genome-wide studies have shown that the actions of 1,25(OH) 2 D 3 involve regulation of gene activity at a range of locations many kilobases from the transcription start site. The structure of the liganded VDR/RXR complex was recently characterized using cryoelectron microscopy, X-ray scattering, and hydrogen deuterium exchange. These recent technological advances will result in a more complete understanding of VDR coactivator interactions, thus facilitating cell and gene specific clinical applications. Although the identification of mechanisms mediating VDR-regulated transcription has been one focus of recent research in the field, other topics of fundamental importance include the identification and functional significance of proteins involved in the metabolism of vitamin D. CYP2R1 has been identified as the most important 25-hydroxylase, and a critical role for CYP24A1 in humans was noted in studies showing that inactivating mutations in CYP24A1 are a probable cause of idiopathic infantile hypercalcemia. In addition, studies using knockout and transgenic mice have provided new insight on the physiological role of vitamin D in classical target tissues as well as evidence of extraskeletal effects of 1,25(OH) 2 D 3 including inhibition of cancer progression, effects on the cardiovascular system, and immunomodulatory effects in certain autoimmune diseases. Some of the mechanistic findings in mouse models have also been observed in humans. The identification of similar pathways in humans could lead to the development of new therapies to prevent and treat disease.

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“…Moreover, ablating Vdr or Cyp27b1 from cells within the skeleton does not cause rickets either. The skeleton is normal if Vdr is selectively ablated from chondrocytes, mature osteoblasts, or osteocytes (375,421), and a high bone mass phenotype with reduced resorptive surfaces occurs when Vdr is ablated from osteoblasts (750). Ablating Cyp27b1 from chondrocytes does not reproduce the rachitic growth plate, whereas low phosphorus will cause the widened, irregular growth plate (466).…”

Section: Role In the Neonatementioning

confidence: 99%

Bone Development and Mineral Homeostasis in the Fetus and Neonate: Roles of the Calciotropic and Phosphotropic Hormones

Kovacs

2014

Physiological Reviews

211

188

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Mineral and bone metabolism are regulated differently in utero compared with the adult. The fetal kidneys, intestines, and skeleton are not dominant sources of mineral supply for the fetus. Instead, the placenta meets the fetal need for mineral by actively transporting calcium, phosphorus, and magnesium from the maternal circulation. These minerals are maintained in the fetal circulation at higher concentrations than in the mother and normal adult, and such high levels appear necessary for the developing skeleton to accrete a normal amount of mineral by term. Parathyroid hormone (PTH) and calcitriol circulate at low concentrations in the fetal circulation. Fetal bone development and the regulation of serum minerals are critically dependent on PTH and PTH-related protein, but not vitamin D/calcitriol, fibroblast growth factor-23, calcitonin, or the sex steroids. After birth, the serum calcium falls and phosphorus rises before gradually reaching adult values over the subsequent 24 -48 h. The intestines are the main source of mineral for the neonate, while the kidneys reabsorb mineral, and bone turnover contributes mineral to the circulation. This switch in the regulation of mineral homeostasis is triggered by loss of the placenta and a postnatal fall in serum calcium, and is followed in sequence by a rise in PTH and then an increase in calcitriol. Intestinal calcium absorption is initially a passive process facilitated by lactose, but later becomes active and calcitriol-dependent. However, calcitriol's role can be bypassed by increasing the calcium content of the diet, or by parenteral administration of calcium.

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Vitamin D Receptor in Osteoblasts Is a Negative Regulator of Bone Mass Control

Cited by 152 publications

References 45 publications

Expression of Fibroblast Growth Factor 23, Vitamin D Receptor, and Sclerostin in Bone Tissue from Hypercalciuric Stone Formers

Expression of Fibroblast Growth Factor 23, Vitamin D Receptor, and Sclerostin in Bone Tissue from Hypercalciuric Stone Formers

Vitamin D: Metabolism, Molecular Mechanism of Action, and Pleiotropic Effects

Bone Development and Mineral Homeostasis in the Fetus and Neonate: Roles of the Calciotropic and Phosphotropic Hormones

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