ANTI-RANKL TREATMENT ENHANCES MUSCLE STRENGTH THROUGH MACROPHAGE MODULATION MECHANISM IN SARCOPENIC MICE

C. Cui; Y. Long; C. Liu; R.M.Y. Wong; S.K. Chow; W. Cheung

doi:10.1302/1358-992X.2023.7.089

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ANTI-RANKL TREATMENT ENHANCES MUSCLE STRENGTH THROUGH MACROPHAGE MODULATION MECHANISM IN SARCOPENIC MICE

The International Combined Orthopaedic Research Societies (ICORS), World Congress of Orthopaedic Research, Edinburgh, Scotland, 7–9 September 2022. Part 1 of 3.

C. Cui
Y. Long
C. Liu
R.M.Y. Wong
S.K. Chow
W. Cheung

ANTI-RANKL TREATMENT ENHANCES MUSCLE STRENGTH THROUGH MACROPHAGE MODULATION MECHANISM IN SARCOPENIC MICE

Cui C, Long Y, Liu C, Wong R, Chow S, Cheung W. ANTI-RANKL TREATMENT ENHANCES MUSCLE STRENGTH THROUGH MACROPHAGE MODULATION MECHANISM IN SARCOPENIC MICE. Orthop Procs. 2023;105-B(SUPP_7):89-89. doi:10.1302/1358-992X.2023.7.089

Cui, C., et al. “ANTI-RANKL TREATMENT ENHANCES MUSCLE STRENGTH THROUGH MACROPHAGE MODULATION MECHANISM IN SARCOPENIC MICE.” Orthopaedic Proceedings, vol. 105-B, no. SUPP_7, 2023, pp. 89-89., https://doi.org/10.1302/1358-992X.2023.7.089

Cui, C., Long, Y., Liu, C., Wong, R., Chow, S., & Cheung, W. (2023). ANTI-RANKL TREATMENT ENHANCES MUSCLE STRENGTH THROUGH MACROPHAGE MODULATION MECHANISM IN SARCOPENIC MICE. Orthopaedic Proceedings, 105-B(SUPP_7), 89-89. https://doi.org/10.1302/1358-992X.2023.7.089

Cui, C., Long, Y., Liu, C., Wong, R., Chow, S. and Cheung, W. (2023) “ANTI-RANKL TREATMENT ENHANCES MUSCLE STRENGTH THROUGH MACROPHAGE MODULATION MECHANISM IN SARCOPENIC MICE.” Orthopaedic Proceedings, 105-B(SUPP_7), pp. 89-89. Available at: https://doi.org/10.1302/1358-992X.2023.7.089

Cui, C., Y. Long, C. Liu, R.M.Y. Wong, S.K. Chow, and W. Cheung. “ANTI-RANKL TREATMENT ENHANCES MUSCLE STRENGTH THROUGH MACROPHAGE MODULATION MECHANISM IN SARCOPENIC MICE.” Orthopaedic Proceedings 105-B, no. SUPP_7 (2023): 89-89. https://doi.org/10.1302/1358-992X.2023.7.089

Cui C, Long Y, Liu C, Wong R, Chow S, Cheung W. ANTI-RANKL TREATMENT ENHANCES MUSCLE STRENGTH THROUGH MACROPHAGE MODULATION MECHANISM IN SARCOPENIC MICE. Orthop Procs. 2023 Apr 4;105-B(SUPP_7):89-89. https://doi.org/10.1302/1358-992X.2023.7.089

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Abstract

Sarcopenia is an age-related geriatric syndrome which is associated with subsequent disability and morbidity. Currently there is no promising therapy approved for the treatment of sarcopenia. The receptor activator of nuclear factor NF-κB ligand (RANKL) and its receptor (RANK) are expressed in bone and skeletal muscle. Activation of the NF-κB pathway mainly inhibits myogenic differentiation, which leads to skeletal muscle dysfunction and loss. LYVE1 and CD206 positive macrophage has been reported to be associated with progressive impairment of skeletal muscle function with aging. The study aims to investigate the effects of an anti-RANKL treatment on sarcopenic skeletal muscle and explore the related mechanisms on muscle inflammation and the polarization status of macrophages.

Sarcopenic senescence-accelerated mouse P8 (SAMP8) mice at month 8 were treated intraperitoneally with 5mg/kg anti-RANKL (IK22/5) or isotype control (2A3; Bio X Cell) antibody every 4 weeks and harvested at month 10. Senescence accelerated mouse resistant-1 (SAMR1) were collected at month 10 as the age-matched non-sarcopenic group. Ex-vivo functional assessment, grip strength and immunostaining of C/EBPa, CD206, F4/80, LYVE1 and PAX7 were performed. Data analysis was done with one-way ANOVA, and the significant level was set at p≤0.05.

At month 10, tetanic force/specific tetanic force, twitch force/specific twitch force in anti-RANKL group were significantly higher than control group (all p<0.01). The mice in the anti-RANKL treatment group also showed significantly higher grip strength than Con group (p<0.001). The SAMP8 mice at month 10 expressed significantly more C/EBPa, CD206 and LYVE1 positive area than in SAMR1, while anti-RANKL treatment significantly decreased C/EBPa, CD206 and LYVE1 positive area.

The anti-RANKL treatment protected against skeletal muscle dysfunctions through suppressing muscle inflammation and modulating M2 macrophages, which may represent a novel therapeutic approach for sarcopenia.

Acknowledgment: Collaborative Research Fund (CRF, Ref: C4032-21GF)

*Email: 1155072350@link.cuhk.edu.hk