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Citations to this article

Excess glucocorticoids inhibit murine bone turnover via modulating the immunometabolism of the skeletal microenvironment
Xu Li, … , Jiankun Xu, Ling Qin
Xu Li, … , Jiankun Xu, Ling Qin
Published March 21, 2024
Citation Information: J Clin Invest. 2024;134(10):e166795. https://doi.org/10.1172/JCI166795.
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Research Article Bone biology Article has an altmetric score of 1

Excess glucocorticoids inhibit murine bone turnover via modulating the immunometabolism of the skeletal microenvironment

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Abstract

Elevated bone resorption and diminished bone formation have been recognized as the primary features of glucocorticoid-associated skeletal disorders. However, the direct effects of excess glucocorticoids on bone turnover remain unclear. Here, we explored the outcomes of exogenous glucocorticoid treatment on bone loss and delayed fracture healing in mice and found that reduced bone turnover was a dominant feature, resulting in a net loss of bone mass. The primary effect of glucocorticoids on osteogenic differentiation was not inhibitory; instead, they cooperated with macrophages to facilitate osteogenesis. Impaired local nutrient status — notably, obstructed fatty acid transportation — was a key factor contributing to glucocorticoid-induced impairment of bone turnover in vivo. Furthermore, fatty acid oxidation in macrophages fueled the ability of glucocorticoid-liganded receptors to enter the nucleus and then promoted the expression of BMP2, a key cytokine that facilitates osteogenesis. Metabolic reprogramming by localized fatty acid delivery partly rescued glucocorticoid-induced pathology by restoring a healthier immune-metabolic milieu. These data provide insights into the multifactorial metabolic mechanisms by which glucocorticoids generate skeletal disorders, thus suggesting possible therapeutic avenues.

Authors

Xu Li, Tongzhou Liang, Bingyang Dai, Liang Chang, Yuan Zhang, Shiwen Hu, Jiaxin Guo, Shunxiang Xu, Lizhen Zheng, Hao Yao, Hong Lian, Yu Nie, Ye Li, Xuan He, Zhi Yao, Wenxue Tong, Xinluan Wang, Dick Ho Kiu Chow, Jiankun Xu, Ling Qin

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Total citations by year

Year: 2025 2024 Total
Citations: 5 2 7
Citation information
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Citations to this article (7)

Title and authors Publication Year
Targeting the central and peripheral nervous system to regulate bone homeostasis: mechanisms and potential therapies
Liang TZ, Jin ZY, Lin YJ, Chen ZY, Li Y, Xu JK, Yang F, Qin L
Military Medical Research 2025
Conductive Hydrogel Inspires Neutrophil Extracellular Traps to Combat Bacterial Infections in Wounds
OuYang L, Lin Z, He X, Sun J, Liao J, Liao Y, Xie X, Hu W, Zeng R, Tao R, Liu M, Sun Y, Mi B, Liu G
ACS Nano 2025
PDGF-BB improves cortical bone quality through restoring the osteogenic microenvironment in the steroid-associated osteonecrosis of rabbits
Cao H, Shi K, Long J, Liu Y, Meng X, Huang C, Hao J, Li L, Zhao Y, Ye T, Lai Y, Qin L, Wang X
Journal of Orthopaedic Translation 2025
Matrix Viscoelasticity Orchestrates Osteogenesis via Mechanotransduction Mediated Metabolic Switch in Macrophages
Tao D, Wang H, Chang S, Cheng J, Da N, Zhang L, Yang J, Wang W, Xu F, Li B
Advanced Healthcare Materials 2025
Progress of research on the gut microbiome and its metabolite short-chain fatty acids in postmenopausal osteoporosis: a literature review.
Chen Y, Xie Y, Yu X
Frontiers of medicine 2025
Knockdown of SMYD3 by RNA Interference Regulates the Expression of Autophagy-Related Proteins and Inhibits Bone Formation in Fluoride-Exposed Osteoblasts.
Deng J, Zeng X, Zhang K, Zhang T, Dong Y, Zou J, Wu C, Li Y, Li F, Guan Z
Biological Trace Element Research 2024
Reduced graphene oxide loaded with tetrahedral framework nucleic acids for combating orthodontically induced root resorption
Yuan W, Huang M, Chen W, Chen S, Cai J, Chen L, Lin H, He K, Chen H, Jiang W, Ou Y, Chen J
Journal of Nanobiotechnology 2024

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