Comparable outcomes in fracture reduction and bone properties with RANKL inhibition and alendronate treatment in a mouse model of osteogenesis imperfecta

Bargman, Renee; Posham, R.; Boskey, Adele L.; DiCarlo, Edward F.; Raggio, Cathleen; Pleshko, Nancy

doi:10.1007/s00198-011-1742-7

Cited by 47 publications

(52 citation statements)

References 46 publications

(45 reference statements)

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“…Treatment ended 12 weeks after the transition time point. Doses of RANK-Fc and ALN were based on results of previous studies that showed increased bone mineral density without side effects using the same dose [1][2][3]. Weaning was carried out between 3 and 4 weeks.…”

Section: Methodsmentioning

confidence: 99%

“…Our group has used the oim/oim mouse model as an analog for evaluating pharmaceutical therapies for moderate-to-severe OI [1-3, 9, 13, 27-29]. The oim/oim mice, as a result of an inappropriate stop codon in the collagen I alpha 2 chain's gene, have a aI(I) 3 triple helix instead of the expected aI(1) 2 aI(2) helix [11] and provide a reproducible model with a moderate-to-severe (Type III) form of OI [34], including the presence of spontaneous fractures. Both alendronate (a bisphosphonate) and RANKFc, an inhibitory antibody to RANKL (receptor activator of nuclear factor-jB ligand), tested in short-term (8-week) studies showed a comparable reduction in the number of fractures relative to saline-treated oim/oim mice [2].…”

Section: Introductionmentioning

confidence: 99%

“…The bone composition assessed by Fourier transform infrared (FTIR) imaging after short-term alendronate treatment of the oim/oim mouse, however, was unchanged relative to saline-treated mice [8]. RANK-Fc blocks the formation, activation, and survival of osteoclasts [2,3,13]. Because RANKL inhibitors have a shorter half-life in bone than do bisphosphonates, they are being investigated as an alternative therapy.…”

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Are Changes in Composition in Response to Treatment of a Mouse Model of Osteogenesis Imperfecta Sex-dependent?

Boskey

Marino

Spevak

et al. 2015

Clinical Orthopaedics &Amp; Related Research

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Background Osteogenesis imperfecta (OI) is a genetic disease characterized by skeletal fragility and deformity. There is extensive debate regarding treatment options in adults with OI. Antiresorptive treatment reduces the number of fractures in growing oim/oim mice, an animal model that reproducibly mimics the moderate-to-severe form of OI in humans. Effects of long-term treatments with antiresorptive agents, considered for treatment of older patients with OI with similar presentation (moderate-tosevere OI) are, to date, unknown. Questions/purposes Fourier transform infrared (FTIR) imaging, which produces a map of the spatial variation in chemical composition in thin sections of bone, was used to address the following questions: (1) do oim/oim mice show a sex dependence in compositional properties at 6.5 months of age; (2) is there a sex-dependent response to treatment with antiresorptive agents used in the treatment of OI in humans; and (3) are any compositional parameters in oim/oim mice corrected to wild-type (WT) values after treatment? Methods FTIR imaging data were collected from femurs from four to five mice per sex per genotype per treatment. Treatments were 24 weeks of saline, alendronate, or RANKFc; and 12 weeks of saline + 12 weeks RANK-Fc and 12 weeks of alendronate + RANK-Fc. FTIR imaging compositional parameters measured in cortical and cancellous bones were mineral-to-matrix ratio, carbonate-to-mineral ratio, crystal size/perfection, acid phosphate substitution, collagen maturity, and their respective distributions (heterogeneities). Because of the small sample size, nonparametric statistics (Mann-Whitney U-and Kruskal-Wallis tests with Bonferroni correction) were used to compare saline-treated male and female mice of different genotypes and treatment effects by sex and genotype, respectively. Statistical significance was defined as p \ 0.05.One or more of the authors (CLR) has received research funding from Amgen (Thousand Oaks, CA, USA) in partial support of this study in an amount less than USD 10,000. One or more of the authors (ALB) owns stock in Amgen (Thousand Oaks, CA) in an amount less than USD 10,000 and in Merck (Kenilworth, NJ, USA) in an amount less than USD 10,000. Results At 6.5 months, saline-treated male cortical oim/ oim bone had increased mineral-to-matrix ratio (p = 0.016), increased acid phosphate substitution (p = 0.032), and decreased carbonate-to-mineral ratio (p = 0.016) relative to WT. Cancellous bone in male oim/oim also had increased mineral-to-matrix ratio (p = 0.016) relative to male WT. Female oim/oim mouse bone composition for all cortical and cancellous bone parameters was comparable to WT (p [ 0.05). Only the female WT mice showed a response of mean compositional properties to treatment, increasing mineral-to-matrix after RANK-Fc treatment in cancellous bone (p = 0.036) compared with saline-treated mice. Male oim/oim increased mineral-to-matrix cortical and cancellous bone heterogeneity in response to all long-term treatments except for saline + RANK-Fc (p...

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Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Are Changes in Composition in Response to Treatment of a Mouse Model of Osteogenesis Imperfecta Sex-dependent?

Boskey

Marino

Spevak

et al. 2015

Clinical Orthopaedics &Amp; Related Research

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“…Among the bone structural parameters, cyclicCHAD was especially effective in preserving the trabecular number. This effect could be explained by the preferential remove of the thinnest trabeculae (PRETT) mechanism, (37,38) that relies on the fact that the thinnest metaphyseal trabeculae, which play a prominent metabolic role, are more prone to be resorbed by osteoclasts and have a shorter lifetime. Therefore, blocking osteoclast bone resorption prevents their disappearance and, as a consequence, their number is higher than in vehicle-treated animals.…”

Section: Discussionmentioning

confidence: 99%

The C-Terminal Domain of Chondroadherin: A New Regulator of Osteoclast Motility Counteracting Bone Loss

Capulli

Olstad

Önnerfjord

et al. 2014

Journal of Bone and Mineral Research

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Chondroadherin (CHAD) is a leucine-rich protein promoting cell attachment through binding to integrin a 2 b 1 and syndecans. We observed that CHAD mRNA and protein were lower in bone biopsies of 50-year-old to 65-year-old osteoporotic women and in bone samples of ovariectomized mice versus gender/age-matched controls, suggesting a role in bone metabolism. By the means of an internal cyclic peptide (cyclicCHAD), we observed that its integrin binding sequence impaired preosteoclast migration through a nitric oxide synthase 2-dependent mechanism, decreasing osteoclastogenesis and bone resorption in a concentration-dependent fashion, whereas it had no effect on osteoblasts. Consistently, cyclicCHAD reduced transcription of two nitric oxide downstream genes, migfilin and vasp, involved in cell motility. Furthermore, the nitric oxide donor, S-nitroso-N-acetyl-D,L-penicillamine, stimulated preosteoclast migration and prevented the inhibitory effect of cyclicCHAD. Conversely, the nitric oxide synthase 2 (NOS2) inhibitor, N5-(1-iminoethyl)-l-ornithine, decreased both preosteoclast migration and differentiation, confirming a role of the nitric oxide pathway in the mechanism of action triggered by cyclicCHAD. In vivo, administration of cyclicCHAD was well tolerated and increased bone volume in healthy mice, with no adverse effect. In ovariectomized mice cyclicCHAD improved bone mass by both a preventive and a curative treatment protocol, with an effect in line with that of the bisphosphonate alendronate, that was mimicked by the NOS2 inhibitor [L-N6-(1-Iminoethyl)-lysine.2 dihydrochloride]. In both mouse models, cyclicCHAD reduced osteoclast and bone resorption without affecting osteoblast parameters and bone formation. In conclusion, CHAD is a novel regulator of bone metabolism that, through its integrin binding domain, inhibits preosteoclast motility and bone resorption, with a potential translational impact for the treatment of osteoporosis.

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“…In preclinical study, Raggio and colleagues found that BPs and RANK-FC could decrease fractures in the mouse model of OI. (2,3) In OI patients, however, the effects of BPs on the fracture reduction in several randomized control trials are still inconsistent. (4,5) The second issue raised by Raggio and colleagues was that we compared the treatment effect of strontium ranelate on fracture reduction to the brtl/þ mice but not to the results that they reported.…”

mentioning

confidence: 99%

Response to Comment on Strontium Ranelate Reduces the Fracture Incidence in a Growing Mouse Model of Osteogenesis Imperfecta

Shi

Guo

et al. 2016

Journal of Bone and Mineral Research

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W e appreciate the kind words offered by Raggio and colleagues about our recent article.(1) Raggio and colleagues highlighted what they considered to be three problems with our discussion and reference. We address these three problems below.The first problem identified by Raggio and colleagues was in relation to our statement that "it is unclear whether treatment with bisphosphonates (BPs) can reduce the incidence of fracture and improve the clinical status in OI patients." In this sentence, we only emphasize the efficacy of BPs in the patients, not in the mice. In preclinical study, Raggio and colleagues found that BPs and RANK-FC could decrease fractures in the mouse model of OI. (2,3) In OI patients, however, the effects of BPs on the fracture reduction in several randomized control trials are still inconsistent. (4,5) The second issue raised by Raggio and colleagues was that we compared the treatment effect of strontium ranelate on fracture reduction to the brtl/þ mice but not to the results that they reported.(2) In fact, the reason why we cited the Brtl/þ mice (reference numbers 37 and 42 in the original study) was to explain some phenomena that we observed in our study, (6,7) not to compare the treatment effects on fracture. We do agree with Raggio and colleagues that the effect of strontium ranelate on fracture reduction in the oim/oim mice was comparable to what they reported (0.7 versus 0.9 fractures/mouse).(2) However, this is just an indirect comparison between these two drugs in two publications. Currently, a new study is underway in our laboratory to compare directly the effects of strontium ranelate and alendronate on fracture incidence in the oim/oim mice. We wish to share the works in future articles.In our study, we only chose the female mice for study. The first reason is that there may exist sex-dependent differences in response to pharmaceutical intervention in several mouse models of OI, which is what Raggio and colleagues mentioned. (8) Another reason why we did not include the male mice is that the male mice usually show more activity, sometimes even fighting and biting each other, which may cause fractures resulting from the bone fragility in this severe mouse model of OI. Because our primary goal was to evaluate the effect of strontium ranelate on the fracture reduction in OI, we thought that the male mice might not be suitable for the study.

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Comparable outcomes in fracture reduction and bone properties with RANKL inhibition and alendronate treatment in a mouse model of osteogenesis imperfecta

Cited by 47 publications

References 46 publications

Are Changes in Composition in Response to Treatment of a Mouse Model of Osteogenesis Imperfecta Sex-dependent?

Are Changes in Composition in Response to Treatment of a Mouse Model of Osteogenesis Imperfecta Sex-dependent?

The C-Terminal Domain of Chondroadherin: A New Regulator of Osteoclast Motility Counteracting Bone Loss

Response to Comment on Strontium Ranelate Reduces the Fracture Incidence in a Growing Mouse Model of Osteogenesis Imperfecta

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