Decline in calcitonin receptor expression in osteocytes with age

Gooi, Julian; Chia, Ling Yeong; Walsh, Nicole C.; Karsdal, Morten A.; Quinn, J; Martın, Thomas; Sims, Natalie A.

doi:10.1530/joe-13-0524

Cited by 21 publications

(21 citation statements)

References 53 publications

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“…This has been assessed using both biochemical markers and histomorphometry and implies that the induced formation is taking place predominantly on quiescent surfaces. (49)(50)(51)(52)(53)(54)(55)(56)(57) The same outcome is reported by Varela and colleagues, (48) where aged osteopenic rats were treated with three doses of abaloparatide (1, 5, and 25 mg/kg), resulting in substantial doseresponsive increases in BMD and bone formation, assessed by histomorphometry, without any significant increase in resorption parameters. It is interesting that such low doses of abaloparatide were used in this study, given the choice in the clinical trial of a dose 4 times higher than that of teriparatide, and the known very much higher dose of PTHrP(1-36) required in mice and in human subjects.…”

Section: Abaloparatide Is An Anabolic Agent But Is It Relatively Ressupporting

confidence: 68%

“…(49)(50)(51)(52)(53)(54)(55)(56)(57) The same outcome is reported by Varela and colleagues, (48) where aged osteopenic rats were treated with three doses of abaloparatide (1, 5, and 25 mg/kg), resulting in substantial doseresponsive increases in BMD and bone formation, assessed by histomorphometry, without any significant increase in resorption parameters. It is interesting that such low doses of abaloparatide were used in this study, given the choice in the clinical trial of a dose 4 times higher than that of teriparatide, and the known very much higher dose of PTHrP(1-36) required in mice and in human subjects.These doses of abaloparatide are in the same range of dosedependent effects observed in studies of PTH(1-34) in aged osteopenic rats, where similar dose-responsive anabolic effects with PTH(1-34) were achieved at 0.1, 0.3, 3, and 30 mg/kg (49) and with 5 and 15 mg/kg.(50) In these latter two studies and many other studies in aged ovariectomized (OVX) rats, some using low PTH doses, others using relatively high doses (100 mg/kg), (51)(52)(53)(54)(55)(56)(57) the anabolic effect was achieved without any increase in osteoclast surface or resorption markers. …”

supporting

confidence: 68%

“…(50) In these latter two studies and many other studies in aged ovariectomized (OVX) rats, some using low PTH doses, others using relatively high doses (100 mg/kg), (51)(52)(53)(54)(55)(56)(57) the anabolic effect was achieved without any increase in osteoclast surface or resorption markers.…”

Section: Abaloparatide Is An Anabolic Agent But Is It Relatively Resmentioning

confidence: 99%

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Abaloparatide Is an Anabolic, but Does It Spare Resorption?

Martın

Seeman

2016

Journal of Bone and Mineral Research

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L ongevity is increasing the burden of fractures. Although antiresorptive therapy slows remodeling, it does not prevent or repair microstructural deterioration. The challenge is to reconstruct the skeleton. The more advanced the patient's age, the more likely that microstructural deterioration is severe and so the more rational the choice of an anabolic agent as first-line therapy. PTH(1-34) (teriparatide) reduces vertebral and nonvertebral fracture risk, in part, by increasing bone matrix volume. Abaloparatide has also recently been reported to reduce morphometric vertebral fracture risk (1,2) and is thus a most welcome addition to the therapeutics of bone fragility. Abaloparatide is claimed to produce its anabolic effect with a much lesser effect on bone resorption than occurs with teriparatide. In this Commentary, we query the latter proposition, which we suggest contains two misconceptions: first, that with teriparatide treatment an anabolic window exists during which bone formation predominates but then is offset by bone resorption, which follows later, and second that less bone resorption occurs with abaloparatide, leaving the "window" open longer and allowing more bone formation. Anabolic Therapy With Parathyroid Hormone (PTH) and AbaloparatideTo understand the fallacies in these two notions, the mythical anabolic window and the purported lesser resorptive effect of abaloparatide, it is necessary first to discuss the mechanisms of action of PTH. The idea that intermittent injection of PTH might promote bone formation was proposed more than 80 years ago by Albright (3) and shown in rats by Selye.Progress was slow, with no attempt to study PTH treatment clinically until the 1970s. The first clinical trial was published in 2001 (5) and was stopped after 18 months because of a toxicity study that showed dose-dependent development of osteosarcoma in rats treated throughout their lives. (6) With the total number of subjects in the clinical trial reduced to 1600 and the duration of treatment being only 18 months, no potential antihip fracture efficacy could be demonstrated, but vertebral and nonvertebral fracture risk was reduced and bone mineral density (BMD) increased.The efficacy of teriparatide as an anabolic therapy depends on intermittent injections, each achieving a sharp peak of PTH in the blood.(7) When teriparatide therapy is begun, circulating bone formation markers increase rapidly, with a delayed appearance of resorption markers, giving rise to the concept of the "anabolic window." (8,9) This was based on the idea that the initial period of increased anabolic markers reflects an early period of bone formation relatively "unopposed" by resorption but then superseded by subsequent increases in bone resorption. This theory was not based on histomorphometric evidence of changing volumes of bone formation and resorption but rather inferred from finding an early increase in bone "formation" markers, followed by a later increase in bone "resorption" markers.Abaloparatide is a 34-amino acid peptide acting u...

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Section: Abaloparatide Is An Anabolic Agent But Is It Relatively Ressupporting

confidence: 68%

supporting

confidence: 68%

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Abaloparatide Is an Anabolic, but Does It Spare Resorption?

Martın

Seeman

2016

Journal of Bone and Mineral Research

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“…Collagen II-positive staining in the annulus fibrosis was much weaker in the OVX+V group than that in the sham and OVX+CT and groups. MMP-1-and MMP-13-positive staining in the annulus fibrosis was stronger in the OVX+V group than in the sham and OVX+CT groups reduced as rodents age, the CT-receptor (CTR) was identified in bone-matrix-embedded osteocytes [25,26]. Moreover, articular cartilage chondrocytes from osteoarthritis (OA) patients do indeed express CTR, which makes articular cartilage a pharmacological target for salmon CT [27].…”

Section: Discussionmentioning

confidence: 99%

Calcitonin suppresses intervertebral disk degeneration and preserves lumbar vertebral bone mineral density and bone strength in ovariectomized rats

et al. 2015

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“…Some osteoclasts can have low activity, including those derived from RAW264.7 cells, which leads to inconclusive results. CTR is highly specific in the myelomonocytic lineage for osteoclasts, although osteocytes as well as some cell types not found in bone can express CTR (Gooi et al, 2014;Nicholson et al, 1986). This has led us previously to investigate the use of anti-CTR antibodies to identify murine osteoclasts in culture (peptides derived from human CTR seem to be poorly immunogenic in rabbits); we therefore have employed this approach with IL-33 + TGFβ-treated RAW264.7 cells.…”

Section: Discussionmentioning

confidence: 99%