Osteoblast–Osteoclast Coculture Amplifies Inhibitory Effects of FG‐4592 on Human Osteoclastogenesis and Reduces Bone Resorption

Osteoblast–Osteoclast Coculture Amplifies Inhibitory Effects of FG‐4592 on Human Osteoclastogenesis and Reduces Bone Resorption

ABSTRACT The link between bone and blood vessels is regulated by hypoxia and the hypoxia‐inducible transcription factor, HIF, which drives both osteogenesis and angiogenesis. The recent clinical approval of PHD enzyme inhibitors, which stabilize HIF protein, introduces the potential for a new clinic...

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Main Authors: Philippa A Hulley, Ioanna Papadimitriou‐Olivgeri, Helen J Knowles
Format: Article
Language:English
Published: Wiley 2020-07-01
Series:JBMR Plus
Subjects:
3D MODELS
COCULTURE
OSTEOBLASTS
OSTEOCLASTS
PHD ENZYME INHIBITOR
Online Access:https://doi.org/10.1002/jbm4.10370
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spelling doaj-082fbd51b4234adc899730448deb2dfe2021-05-02T22:42:33ZengWileyJBMR Plus2473-40392020-07-0147n/an/a10.1002/jbm4.10370Osteoblast–Osteoclast Coculture Amplifies Inhibitory Effects of FG‐4592 on Human Osteoclastogenesis and Reduces Bone ResorptionPhilippa A Hulley0Ioanna Papadimitriou‐Olivgeri1Helen J Knowles2Nuffield Department of Orthopaedics Rheumatology & Musculoskeletal Sciences University of Oxford Oxford UKNuffield Department of Orthopaedics Rheumatology & Musculoskeletal Sciences University of Oxford Oxford UKNuffield Department of Orthopaedics Rheumatology & Musculoskeletal Sciences University of Oxford Oxford UKABSTRACT The link between bone and blood vessels is regulated by hypoxia and the hypoxia‐inducible transcription factor, HIF, which drives both osteogenesis and angiogenesis. The recent clinical approval of PHD enzyme inhibitors, which stabilize HIF protein, introduces the potential for a new clinical strategy to treat osteolytic conditions such as osteoporosis, osteonecrosis, and skeletal fracture and nonunion. However, bone‐resorbing osteoclasts also play a central role in bone remodeling and pathological osteolysis, and HIF promotes osteoclast activation and bone loss in vitro. It is therefore likely that the result of PHD enzyme inhibition in vivo would be mediated by a balance between increased bone formation and increased bone resorption. It is essential that we improve our understanding of the effects of HIF on osteoclast formation and function and consider the potential contribution of inhibitory interactions with other musculoskeletal cells. The PHD enzyme inhibitor FG‐4592 stabilized HIF protein and stimulated osteoclast‐mediated bone resorption, but inhibited differentiation of human CD14+ monocytes into osteoclasts. Formation of osteoclasts in a more physiologically relevant 3D collagen gel did not affect the sensitivity of osteoclastogenesis to FG‐4592, but increased sensitivity to reduced concentrations of RANKL. Coculture with osteoblasts amplified inhibition of osteoclastogenesis by FG‐4592, whether the osteoblasts were proliferating, differentiating, or in the presence of exogenous M‐CSF and RANKL. Osteoblast coculture dampened the ability of high concentrations of FG‐4592 to increase bone resorption. These data provide support for the therapeutic use of PHD enzyme inhibitors to improve bone formation and/or reduce bone loss for the treatment of osteolytic pathologies and indicate that FG‐4592 might act in vivo to inhibit the formation and activity of the osteoclasts that drive osteolysis. © 2020 The Authors. JBMR Plus published by Wiley Periodicals, Inc. on behalf of American Society for Bone and Mineral Research.https://doi.org/10.1002/jbm4.103703D MODELSCOCULTUREOSTEOBLASTSOSTEOCLASTSPHD ENZYME INHIBITOR
collection DOAJ
language English
format Article
sources DOAJ
author Philippa A Hulley
Ioanna Papadimitriou‐Olivgeri
Helen J Knowles
spellingShingle Philippa A Hulley
Ioanna Papadimitriou‐Olivgeri
Helen J Knowles
Osteoblast–Osteoclast Coculture Amplifies Inhibitory Effects of FG‐4592 on Human Osteoclastogenesis and Reduces Bone Resorption
JBMR Plus
3D MODELS
COCULTURE
OSTEOBLASTS
OSTEOCLASTS
PHD ENZYME INHIBITOR
author_facet Philippa A Hulley
Ioanna Papadimitriou‐Olivgeri
Helen J Knowles
author_sort Philippa A Hulley
title Osteoblast–Osteoclast Coculture Amplifies Inhibitory Effects of FG‐4592 on Human Osteoclastogenesis and Reduces Bone Resorption
title_short Osteoblast–Osteoclast Coculture Amplifies Inhibitory Effects of FG‐4592 on Human Osteoclastogenesis and Reduces Bone Resorption
title_full Osteoblast–Osteoclast Coculture Amplifies Inhibitory Effects of FG‐4592 on Human Osteoclastogenesis and Reduces Bone Resorption
title_fullStr Osteoblast–Osteoclast Coculture Amplifies Inhibitory Effects of FG‐4592 on Human Osteoclastogenesis and Reduces Bone Resorption
title_full_unstemmed Osteoblast–Osteoclast Coculture Amplifies Inhibitory Effects of FG‐4592 on Human Osteoclastogenesis and Reduces Bone Resorption
title_sort osteoblast–osteoclast coculture amplifies inhibitory effects of fg‐4592 on human osteoclastogenesis and reduces bone resorption
publisher Wiley
series JBMR Plus
issn 2473-4039
publishDate 2020-07-01
description ABSTRACT The link between bone and blood vessels is regulated by hypoxia and the hypoxia‐inducible transcription factor, HIF, which drives both osteogenesis and angiogenesis. The recent clinical approval of PHD enzyme inhibitors, which stabilize HIF protein, introduces the potential for a new clinical strategy to treat osteolytic conditions such as osteoporosis, osteonecrosis, and skeletal fracture and nonunion. However, bone‐resorbing osteoclasts also play a central role in bone remodeling and pathological osteolysis, and HIF promotes osteoclast activation and bone loss in vitro. It is therefore likely that the result of PHD enzyme inhibition in vivo would be mediated by a balance between increased bone formation and increased bone resorption. It is essential that we improve our understanding of the effects of HIF on osteoclast formation and function and consider the potential contribution of inhibitory interactions with other musculoskeletal cells. The PHD enzyme inhibitor FG‐4592 stabilized HIF protein and stimulated osteoclast‐mediated bone resorption, but inhibited differentiation of human CD14+ monocytes into osteoclasts. Formation of osteoclasts in a more physiologically relevant 3D collagen gel did not affect the sensitivity of osteoclastogenesis to FG‐4592, but increased sensitivity to reduced concentrations of RANKL. Coculture with osteoblasts amplified inhibition of osteoclastogenesis by FG‐4592, whether the osteoblasts were proliferating, differentiating, or in the presence of exogenous M‐CSF and RANKL. Osteoblast coculture dampened the ability of high concentrations of FG‐4592 to increase bone resorption. These data provide support for the therapeutic use of PHD enzyme inhibitors to improve bone formation and/or reduce bone loss for the treatment of osteolytic pathologies and indicate that FG‐4592 might act in vivo to inhibit the formation and activity of the osteoclasts that drive osteolysis. © 2020 The Authors. JBMR Plus published by Wiley Periodicals, Inc. on behalf of American Society for Bone and Mineral Research.
topic 3D MODELS
COCULTURE
OSTEOBLASTS
OSTEOCLASTS
PHD ENZYME INHIBITOR
url https://doi.org/10.1002/jbm4.10370
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AT ioannapapadimitriouolivgeri osteoblastosteoclastcocultureamplifiesinhibitoryeffectsoffg4592onhumanosteoclastogenesisandreducesboneresorption
AT helenjknowles osteoblastosteoclastcocultureamplifiesinhibitoryeffectsoffg4592onhumanosteoclastogenesisandreducesboneresorption
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