Oxytocin is an anabolic bone hormone

Tamma, Roberto; Colaianni, Graziana; Zhu, Ling; DiBenedetto, Adriana; Greco, Giovanni; Montemurro, Gabriella; Patano, Nicola; Strippoli, Maurizio; Vergari, Rosaria; Mancini, L.; Colucci, Silvia; Grano, Maria; Faccio, Roberta; Li, Xuan; Li, Jianhua; Usmani, Sabah; Bachar, Marilyn; Bab, Itai; Nishimori, Katsuhiko; Young, Larry J.; Buettner, Christoph; Iqbal, Jameel; Sun, Li; Zaidi, Mone; Zallone, Alberta

doi:10.1073/pnas.0901890106

Cited by 224 publications

(287 citation statements)

References 35 publications

(44 reference statements)

Supporting

Mentioning

275

Contrasting

Unclassified

Order By: Relevance

“…osteoporosis | osteoblast | skeleton O ver the past decade, we have described direct actions of anterior and posterior pituitary hormones on the skeleton (1)(2)(3)(4)(5)(6)(7)(8). We have shown that these actions are exerted via G protein-coupled receptors resident on both osteoblasts and osteoclasts.…”

mentioning

confidence: 99%

Functions of vasopressin and oxytocin in bone mass regulation

Sun

Tamma

Yuen

et al. 2015

Proc. Natl. Acad. Sci. U.S.A.

Self Cite

View full text Add to dashboard Cite

Prior studies show that oxytocin (Oxt) and vasopressin (Avp) have opposing actions on the skeleton exerted through high-affinity G protein-coupled receptors. We explored whether Avp and Oxtr can share their receptors in the regulation of bone formation by osteoblasts. We show that the Avp receptor 1α (Avpr1α) and the Oxt receptor (Oxtr) have opposing effects on bone mass: Oxtr −/− mice have osteopenia, and Avpr1α −/− mice display a high bone mass phenotype. More notably, this high bone mass phenotype is reversed by the deletion of Oxtr in Oxtr −/− :Avpr1α −/− doublemutant mice. However, although Oxtr is not indispensable for Avp action in inhibiting osteoblastogenesis and gene expression, Avpstimulated gene expression is inhibited when the Oxtr is deleted in Avpr1α −/− cells. In contrast, Oxt does not interact with Avprs in vivo in a model of lactation-induced bone loss in which Oxt levels are high. Immunofluorescence microscopy of isolated nucleoplasts and Western blotting and MALDI-TOF of nuclear extracts show that Avp triggers Avpr1α localization to the nucleus. Finally, a specific Avpr2 inhibitor, tolvaptan, does not affect bone formation or bone mass, suggesting that Avpr2, which primarily functions in the kidney, does not have a significant role in bone remodeling.O ver the past decade, we have described direct actions of anterior and posterior pituitary hormones on the skeleton (1-8). We have shown that these actions are exerted via G protein-coupled receptors resident on both osteoblasts and osteoclasts. We also find that the skeleton is highly sensitive to the action of posterior pituitary hormones; for example, mice haploinsufficient in oxytocin (Oxt) have osteopenic bones, but lactation is normal; lactation is impaired only in Oxt −/− mice (2). Likewise, Tshr haploinsufficient mice are completely euthyroid with normal thyroid follicles but display significant osteopenia (4). The exquisite sensitivity of the skeleton to pituitary hormones comes as no surprise, considering that the pituitary gland and the skeleton are both evolutionarily more primitive than target endocrine organs (7).Apart from the known actions of growth hormone on the skeleton, Tsh, Fsh, Acth, Oxt, and vasopressin (Avp) have all been shown to regulate the formation and/or function of both osteoblasts and osteoclasts and thus to control bone remodeling in vivo (2-4, 6-8). The two neurohypophyseal hormones Oxt and Avp have opposing functions (2, 3). Oxt stimulates and Avp inhibits osteoblast formation. Consequently, the genetic deletion of the Oxt receptor (Oxtr) and Avp receptor 1α (Avpr1α) yields opposing phenotypes, notably osteopenia in Oxtr −/− mice and high bone mass in Avpr1α −/− mice (2, 3). These findings may explain the rapid recovery of bone loss at weaning when plasma Oxt levels are high (9) and also the profound loss of bone noted in chronic hyponatremic states, such as the syndrome of inappropriate antidiuretic hormone secretion (SIADH), in which serum Avp levels are elevated (3).We find high levels of Oxtr expression on ...

show abstract

mentioning

confidence: 99%

Functions of vasopressin and oxytocin in bone mass regulation

Sun

Tamma

Yuen

et al. 2015

Proc. Natl. Acad. Sci. U.S.A.

Self Cite

View full text Add to dashboard Cite

show abstract

“…However, this effect is in contrast to uterine myocytes, wherein pErk is reduced in mice lacking either Arrb1 or Arrb2 (26). The intactness of the pErk response in osteoblasts could be explained by the known activation of MAPKs by G αi and G αq (28); this actin could account for the positive effect of Oxt on osteoblast viability that we have shown earlier (4).…”

Section: Discussionmentioning

confidence: 53%

“…We have shown previously that osteoblasts express abundant plasma membrane Oxtrs that drive cell differentiation to a mature, mineralizing phenotype in response to pituitary-and bone marrow-derived Oxt (4,6). However, the mechanism of this effect has remained uncertain.…”

Section: Discussionmentioning

confidence: 99%

“…Oxtrs are present on osteoclast precursors and osteoclasts (36), and their stimulation results in increased osteoclastogenesis but inhibited bone resorption (4). Rapid rises in Oxt during periods of calcium stress (1) might enable calcium mobilization followed by the rapid cessation of bone resorption through a brake on active osteoclasts (4).…”

Section: Discussionmentioning

confidence: 99%

“…More recently, we and others have shown that Oxt also stimulates bone formation directly by interacting with an osteoblastic Oxtr (3,4). The genetic deletion of Oxt or Oxtr in mice thus decreases osteoblast differentiation and bone formation, causing osteopenia (5,6).…”

mentioning

confidence: 99%

See 2 more Smart Citations

Osteoblast regulation via ligand-activated nuclear trafficking of the oxytocin receptor

Benedetto

Sun

Zambonin

et al. 2014

Proc. Natl. Acad. Sci. U.S.A.

Self Cite

View full text Add to dashboard Cite

We report that oxytocin (Oxt) receptors (Oxtrs), on stimulation by the ligand Oxt, translocate into the nucleus of osteoblasts, implicating this process in the action of Oxt on osteoblast maturation. Sequential immunocytochemistry of intact cells or isolated nucleoplasts stripped of the outer nuclear membrane showed progressive nuclear localization of the Oxtr; this nuclear translocation was confirmed by monitoring the movement of Oxtr-EGFP as well as by immunogold labeling. Nuclear Oxtr localization was conclusively shown by Western immunoblotting and MS of nuclear lysate proteins. We found that the passage of Oxtrs into the nucleus was facilitated by successive interactions with β-arrestins (Arrbs), the small GTPase Rab5, importin-β (Kpnb1), and transportin-1 (Tnpo1). siRNA-mediated knockdown of Arrb1, Arrb2, or Tnpo1 abrogated Oxt-induced expression of the osteoblast differentiation genes osterix (Sp7), Atf4, bone sialoprotein (Ibsp), and osteocalcin (Bglap) without affecting Erk phosphorylation. Likewise and again, without affecting pErk, inhibiting Arrb recruitment by mutating Ser rich clusters of the nuclear localization signal to Ala abolished nuclear import and Oxtr-induced gene expression. These studies define a previously unidentified mechanism for Oxtr action on bone and open possibilities for direct transcriptional modulation by nuclear G protein-coupled receptors. T he oxytocin (Oxt) receptor (Oxtr), a member of the rhodopsin-type (class I) family of G protein-coupled receptors (GPCRs), responds to the neurohypophyseal hormone Oxt to stimulate lactation and social bonding (1, 2). More recently, we and others have shown that Oxt also stimulates bone formation directly by interacting with an osteoblastic Oxtr (3, 4). The genetic deletion of Oxt or Oxtr in mice thus decreases osteoblast differentiation and bone formation, causing osteopenia (5, 6). We believe that this action supports maternal skeletal remineralization after the intergenerational transfer of calcium during pregnancy and lactation (5). However, the precise mechanism through which Oxtr activation translates into increased bone formation remains unclear.Oxt binding to Oxtrs is known to activate both G protein G αi -and G αq/11 -mediated phospholipase C pathways (7). However, in common with other GPCRs, prolonged or repetitive agonist stimulation by Oxt results in Oxtr internalization through β-arrestin (Arrb). GPCR internalization can activate signaling pathways quite distinct from those activated by the same receptors resident at the cell surface. Hence, desensitization of primary G protein-dependent signaling can be followed by a second wave of Arrb-mediated signaling (8). β-Arrestins can also recruit signaling proteins that connect GPCRs to various cytoplasmic effector pathways, such as mitogen-activated protein kinase (MAPK) and protein kinase B/phosphatidylinositol-4,5-bisphosphate 3-kinase (Akt/PI3K) (9, 10). Such mechanisms can elicit delayed genomic responses.After being internalized, GPCRs are either recycled back to the plasma m...

show abstract