Ten‐Year Simulation of the Effects of Denosumab on Bone Remodeling in Human Biopsies

Tourolle, Duncan C.; Dempster, David W.; Ledoux, Charles; Boaretti, Daniele; Aguilera, M. Safont; Saleem, Najma; Müller, Ralph

doi:10.1002/jbm4.10494

Cited by 15 publications

(17 citation statements)

References 34 publications

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“…This problem has been identified for in silico models of bone mechanobiology (Checa and Prendergast 2009), where simple approaches were adopted to overcome this lack of information (Perier-Metz et al 2020, 2022; Borgiani et al 2021). This limitation might be partially overcome by taking advantage of the mechanical environment as it was performed by Tourolle and colleagues (Tourolle et al 2021). A more synergistic study where the cytokines are experimentally obtained from the same site on a regular basis would help in the calibration of this micro-MPA in silico model.…”

Section: Discussionmentioning

confidence: 99%

Trabecular bone remodeling in the ageing mouse: a micro-multiphysics agent-basedin silicomodel using single-cell mechanomics

Boaretti

Marques

Ledoux

et al. 2022

Preprint

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Bone remodeling is regulated by the interaction between different cells and tissues across many spatial and temporal scales. In silico models have been of help to further understand the signaling pathways that regulate the spatial cellular interplay. We have established a 3D multiscale micro-multiphysics agent-based (micro-MPA)in silicomodel of trabecular bone remodeling using longitudinalin vivodata from the sixth caudal vertebra (CV6) of PolgA(D257A/D257A)mice, a mouse model of premature aging. Our model includes a variety of cells as single agents and receptor-ligand kinetics, mechanotransduction, diffusion and decay of cytokines which regulate the cells' behavior. The micro-MPA model was applied for simulating trabecular bone remodeling in the CV6 of 5 mice over 4 weeks and we evaluated the static and dynamic morphometry of the trabecular bone microarchitecture. We identified a configuration of the model parameters to simulate a homeostatic trabecular bone remodeling. Additionally, our simulations showed different anabolic, anti-anabolic, catabolic and anticatabolic responses with an increase or decrease by one standard deviation in the levels of osteoprotegerin (OPG), receptor activator of nuclear factor kB ligand (RANKL), and sclerostin (Scl) produced by the osteocytes. From these results, we concluded that OPG inhibits osteoclastic bone resorption by reducing the osteoclast recruitment, RANKL promotes bone resorption by enhancing the osteoclast recruitment and Scl blocks bone formation by inhibiting osteoblast differentiation. The variations in trabecular bone volume fraction and thickness (BV/TV and Tb.Th) were relatively higher with variations of one standard deviation in the levels of RANKL compared to OPG and Scl. This micro-MPA model will help us to better understand how cells respond to the mechanical signal by changing their activity in response to their local mechanical environment.

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Section: Discussionmentioning

confidence: 99%

Trabecular bone remodeling in the ageing mouse: a micro-multiphysics agent-basedin silicomodel using single-cell mechanomics

Boaretti

Marques

Ledoux

et al. 2022

Preprint

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“…In silico simulations have been proposed to provide fast, inexpensive and ethical alternatives to years of costly experimentation on animals and humans (Webster, 2020;Nikolova-Simons et al, 2021;Sarrami-Foroushani et al, 2021). Existing in silico models have been developed to study bone remodeling, its deregulation during metabolic bone diseases and the effect of therapeutics and exercise (Lemaire et al, 2004;Pivonka et al, 2008;Lerebours et al, 2015;Pastrama et al, 2018;Boaretti et al, 2019;Tourolle, 2019;Kameo et al, 2020;Martínez-Reina et al, 2021a;Tourolle et al, 2021).…”

Section: Introductionmentioning

confidence: 99%

“…β (RANK)-its ligand (RANKL) and Osteoprotegerin (OPG) (Boyce and Xing, 2008); mechanosensitivity via the Wingless and int-1 (Wnt) proteins, sclerostin and parathyroid hormone (PTH) (Jilka et al, 1999;Hadjidakis and Androulakis, 2006;Lewiecki, 2014;Kovács et al, 2019); osteoblastogenesis governed by levels of bone morphogenetic protein (BMP) and transforming growth factor-β (TGF-β) (Hanada et al, 1997;Zimmermann et al, 2005;Giannoudis et al, 2008); and interleukin-governed interplay between bone remodeling and immune reactions (Shaarawy et al, 2003;Pino et al, 2010;Sun et al, 2011;Giganti et al, 2012;Marques et al, 2013). Within the varied spectrum of in silico modeling techniques, only bone cell population dynamics models (Lemaire et al, 2004;Pivonka et al, 2008;Lerebours et al, 2015;Pastrama et al, 2018;Martínez-Reina et al, 2021a) and micro-multiphysics agentbased (micro-MPA) models (Boaretti et al, 2019;Tourolle, 2019;Kameo et al, 2020;Tourolle et al, 2021) explicitly incorporate the complex cellular and molecular mechanisms causing metabolic bone diseases and the pathways involved in their treatments.…”

Section: Introductionmentioning

confidence: 99%

“…To date, only micro-MPA models have the resolution to predict the effect of the complex cell-cytokine pathways in bone on the bone microarchitecture. Tourolle (Tourolle et al, 2021) and Kameo (Kameo et al, 2020) developed micro-MPA models of osteoporosis and its treatments with bisphosphonates and RANK ligand inhibitors, respectively, using microcomputed tomography (microCT) scans of iliac crest biopsies with resolutions on the order of 10 µm as input.…”

Section: Introductionmentioning

confidence: 99%

“…Despite the promise of such in silico models, extensive verification and validation are still needed, particularly using human data, for micro-MPA models or bone cell population dynamics models to be applied clinically. In these types of models, parameters for cell and cytokine behavior are set based on experimental values found in literature; however, the settings used vary from one research group to the next (Kameo et al, 2020;Tourolle et al, 2021) as well as from one model to another (Martínez-Reina et al, 2021a;Tourolle et al, 2021). The cellcytokine signaling pathways included in micro-MPA models of bone remodeling were based on earlier bone cell population dynamics models.…”

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Clinical Data for Parametrization of In Silico Bone Models Incorporating Cell-Cytokine Dynamics: A Systematic Review of Literature

Ledoux

Boaretti

Sachan

et al. 2022

Front. Bioeng. Biotechnol.

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In silico simulations aim to provide fast, inexpensive, and ethical alternatives to years of costly experimentation on animals and humans for studying bone remodeling, its deregulation during osteoporosis and the effect of therapeutics. Within the varied spectrum of in silico modeling techniques, bone cell population dynamics and agent-based multiphysics simulations have recently emerged as useful tools to simulate the effect of specific signaling pathways. In these models, parameters for cell and cytokine behavior are set based on experimental values found in literature; however, their use is currently limited by the lack of clinical in vivo data on cell numbers and their behavior as well as cytokine concentrations, diffusion, decay and reaction rates. Further, the settings used for these parameters vary across research groups, prohibiting effective cross-comparisons. This review summarizes and evaluates the clinical trial literature that can serve as input or validation for in silico models of bone remodeling incorporating cells and cytokine dynamics in post-menopausal women in treatment, and control scenarios. The GRADE system was used to determine the level of confidence in the reported data, and areas lacking in reported measures such as binding site occupancy, reaction rates and cell proliferation, differentiation and apoptosis rates were highlighted as targets for further research. We propose a consensus for the range of values that can be used for the cell and cytokine settings related to the RANKL-RANK-OPG, TGF-β and sclerostin pathways and a Levels of Evidence-based method to estimate parameters missing from clinical trial literature.

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Changes in RANKL and TRAcP 5b after discontinuation of denosumab suggest RANKL mediated formation of osteoclasts results in the increased bone resorption

et al. 2022

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Ten‐Year Simulation of the Effects of Denosumab on Bone Remodeling in Human Biopsies

Cited by 15 publications

References 34 publications

Trabecular bone remodeling in the ageing mouse: a micro-multiphysics agent-basedin silicomodel using single-cell mechanomics

Trabecular bone remodeling in the ageing mouse: a micro-multiphysics agent-basedin silicomodel using single-cell mechanomics

Clinical Data for Parametrization of In Silico Bone Models Incorporating Cell-Cytokine Dynamics: A Systematic Review of Literature

Changes in RANKL and TRAcP 5b after discontinuation of denosumab suggest RANKL mediated formation of osteoclasts results in the increased bone resorption

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