Estrogen Prevents Bone Loss via Estrogen Receptor α and Induction of Fas Ligand in Osteoclasts

Nakamura, Takashi; Imai, Yuuki; Μatsumoto, Takahiro; Sato, Shingo; Takeuchi, Kazusane; Igarashi, Katsuhide; Harada, Yoshifumi; Azuma, Yoshiaki; Krust, Andrée; Yamamoto, Yasutake; Nishina, Hiroshi; Takeda, Satoshi; Takayanagi, Hiroshi; Metzger, Daniel; Kanno, Jun; Takaoka, Kunio; Martın, Thomas; Chambon, Pierre; Kato, Shigeaki

doi:10.1016/j.cell.2007.07.025

Cited by 901 publications

(841 citation statements)

References 52 publications

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“…But, there still remains the possibility that signaling linked to ER would be altered even though the immunolocalization of ER was unchanged. Recently, the proapoptotic effect of estrogens on osteoclasts was reported to be mediated by an increase in Fas ligand production by osteoclasts [44], and in vitro studies showed that estrogens stimulate Fas ligand expression in osteoblastic cells which are precusors of osteocytes [43]. However, we showed no obvious difference in the number of TUNEL-positive osteoblasts and osteocytes even after the OVX.…”

Section: Immunolocalization Of Er and Tunel-positive Osteocytes In Tcontrasting

confidence: 51%

“…Thus, reduced-sclerostin did not appear to be associated with diminished ER in osteocytes in the mesial region. Other studies suggested a proapoptotic effect of estrogens on osteoclasts and osteoblasts [43,44], and therefore, it was necessary to confirm whether the reduced amount of sclerostin would be It is well known that OVX stimulates osteoclastic differentiation and subsequent bone resorption in long bones, and also shows the similar effects in alveolar bone [16][17][18][19][20][21][22].…”

Section: Immunolocalization Of Er and Tunel-positive Osteocytes In Tmentioning

confidence: 99%

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Immunolocalization of sclerostin synthesized by osteocytes in relation to bone remodeling in the interradicular septa of ovariectomized rats

Guo

Liu

et al. 2012

Journal of Electron Microscopy

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This study aimed to elucidate whether estrogen deficiency would affect the synthesis of an osteocyte-derived factor, sclerostin, in the mesial region of alveolar bone. Eight 9-week-old Wister female rats were ovariectomized (OVX), and the other eight rats were Sham-operated (Sham). After 4 weeks, the interradicular septa of mandibular first molar were embedded in paraffin, and then, were histochemically examined. Sclerostin-positive osteocytes were located in a superficial layer of the mesial region of Sham bone, while the OVX mesial region showed a lesser presence of the sclerostin-reactive osteocytes. There was no significant difference in the distribution of estrogen receptor  and TUNEL-positive cells in either Sham or OVX groups. Meanwhile, the Sham mesial region demonstrated many osteoclasts, but the OVX specimens showed numerous osteoclasts in association with intense immunolabeling of the receptor activator of the nuclear factor kB ligand. Complex meshwork of cement lines was seen consistent with irregularly-distributed osteocytic lacunar-canalicular system in the OVX mesial region, compared with those of the Sham specimens. In conclusion, estrogen deficiency appears to inhibit osteocytes for sclerostin synthesis in the mesial region of the interradicular septum, mediated by accelerated bone remodeling, rather than by directly effecting osteocytes. words

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Section: Immunolocalization Of Er and Tunel-positive Osteocytes In Tcontrasting

confidence: 51%

Section: Immunolocalization Of Er and Tunel-positive Osteocytes In Tmentioning

confidence: 99%

Immunolocalization of sclerostin synthesized by osteocytes in relation to bone remodeling in the interradicular septa of ovariectomized rats

Guo

Liu

et al. 2012

Journal of Electron Microscopy

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“…We generated mice doubly deficient in p85a and p85b, which are dominantly expressed in the osteoclast lineage. Because homozygous deletion of Pik3r1, which encodes p85a, p55a, and p50a, results in perinatal lethality, (34) we crossed Pik3r1 F/À mice (25) with Ctsk Cre/þ mice (27) to obtain osteoclast-specific Pik3r1 knockout (Pik3r1 DOc/À ) mice. We mated Pik3r1 DOc/À mice with Pik3r2 À/À mice (26) to generate mice deficient in both p85a and b (Pik3r1 DOc/À Pik3r2 À/À mice).…”

Section: Resultsmentioning

confidence: 99%

“…Mice and the in vivo analysis of bone tissues Pik3r1 F/F , (25) Pik3r2 À/À , (26) CtsKCre transgenic, (27) and Akt pleckstrin homology domain-green fluorescent protein (AktPH-GFP) transgenic mice (28) were previously generated and are described elsewhere. Because a small population of osteoclasts from CtsKCrePik3r1 F/F mice still expressed p85a, CtsKCrePik3r1 F/F we mated mice to Pik3r1 þ/À mice to generate CtsKCrePik3r1 F/À (Pik3r1 Doc/À ) mice.…”

Section: Methodsmentioning

confidence: 99%

Class IA phosphatidylinositol 3-kinase regulates osteoclastic bone resorption through protein kinase B–mediated vesicle transport

Shirakawa

Nakamura

Masuda

et al. 2012

Journal of Bone and Mineral Research

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Class IA phosphatidylinositol 3-kinases (PI3Ks) are activated by growth factor receptors and regulate a wide range of cellular processes. In osteoclasts, they are activated downstream of a v b 3 integrin and colony-stimulating factor-1 receptor (c-Fms), which are involved in the regulation of bone-resorbing activity. The physiological relevance of the in vitro studies using PI3K inhibitors has been of limited value, because they inhibit all classes of PI3K. Here, we show that the osteoclast-specific deletion of the p85 genes encoding the regulatory subunit of the class IA PI3K results in an osteopetrotic phenotype caused by a defect in the bone-resorbing activity of osteoclasts. Class IA PI3K is required for the ruffled border formation and vesicular transport, but not for the formation of the sealing zone. p85a/b doubly deficient osteoclasts had a defect in macrophage colony-stimulating factor (M-CSF)-induced protein kinase B (Akt) activation and the introduction of constitutively active Akt recovered the bone-resorbing activity. Thus, the class IA PI3K-Akt pathway regulates the cellular machinery crucial for osteoclastic bone resorption, and may provide a molecular basis for therapeutic strategies against bone diseases. ß

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“…Estrogen has been shown to inhibit osteoclastogenesis via ER␣ (Nakamura et al, 2007), and kaempferol and quercetin also shows potent inhibitory effect on in vitro osteoclastic bone resorption (Wattel et al, 2003). Thus, kaempferol and quercetin in TSZ may also exert their antiosteoporotic effect not only by promoting osteoblastogenesis but also by inhibiting osteoclastogenesis.…”

Section: Discussionmentioning

confidence: 99%

Antiosteoporotic compounds from seeds of Cuscuta chinensis

Yang

Chen

Wang

et al. 2011

Journal of Ethnopharmacology

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Estrogen Prevents Bone Loss via Estrogen Receptor α and Induction of Fas Ligand in Osteoclasts

Cited by 901 publications

References 52 publications

Immunolocalization of sclerostin synthesized by osteocytes in relation to bone remodeling in the interradicular septa of ovariectomized rats

Immunolocalization of sclerostin synthesized by osteocytes in relation to bone remodeling in the interradicular septa of ovariectomized rats

Class IA phosphatidylinositol 3-kinase regulates osteoclastic bone resorption through protein kinase B–mediated vesicle transport

Antiosteoporotic compounds from seeds of Cuscuta chinensis

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