Adipose-derived leptin and complement factor D mediate osteoarthritis severity and pain

Kelsey H. Collins; Kristin L. Lenz; Hope D. Welhaven; Erica Ely; Luke E. Springer; Sophie Paradi; Ruhang Tang; Lauryn Braxton; Antonina Akk; Huimin Yan; Bo Zhang; Xiaobo Wu; John P. Atkinson; Arin K. Oestreich; Ron K. June; Christine T.N. Pham; Farshid Guilak

doi:10.1126/sciadv.adt5915

Adipose-derived leptin and complement factor D mediate osteoarthritis severity and pain

Kelsey H. Collins, Kristin L. Lenz, Hope D. Welhaven, Erica Ely, Luke E. Springer, Sophie Paradi, Ruhang Tang, Lauryn Braxton, Antonina Akk, Huimin Yan, Bo Zhang, Xiaobo Wu, John P. Atkinson, Arin K. Oestreich, Ron K. June, Christine T.N. Pham, Farshid Guilak

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Abstract

Obesity is a risk factor for osteoarthritis (OA), and leptin is among the adipokines implicated in obesity-induced OA. However, the specific role of leptin in OA severity and pain is not known. Using lipodystrophic (LD) mice, we show that fat-secreted factors are required for knee OA development, implicating a fat-cartilage cross-talk. Fat pad implantation or systemic leptin restoration in LD mice reintroduced structural OA and pain, whereas implantation of leptin-deficient fat pad did not change OA susceptibility. Isochronic parabiosis and spatial transcriptomics confirmed that a fat-joint cross-talk likely occurred via soluble mediators. Global unsupervised multiomics of conditioned media from fat implants revealed that leptin exerts a regulatory effect on adipsin (or complement factor D), the activity of which modulates the contrastive OA structural and pain phenotype. These findings suggest that adipokines influence OA pathogenesis, providing conclusive evidence of a fat-joint cross-talk and implicating OA as a systemic disease of adipose tissue.

Original language	English
Article number	eadt5915
Journal	Science Advances
Volume	11
Issue number	17
DOIs	https://doi.org/10.1126/sciadv.adt5915
State	Published - Apr 25 2025

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Collins, K. H., Lenz, K. L., Welhaven, H. D., Ely, E., Springer, L. E., Paradi, S., Tang, R., Braxton, L., Akk, A., Yan, H., Zhang, B., Wu, X., Atkinson, J. P., Oestreich, A. K., June, R. K., Pham, C. T. N., & Guilak, F. (2025). Adipose-derived leptin and complement factor D mediate osteoarthritis severity and pain. Science Advances, 11(17), Article eadt5915. https://doi.org/10.1126/sciadv.adt5915

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title = "Adipose-derived leptin and complement factor D mediate osteoarthritis severity and pain",

abstract = "Obesity is a risk factor for osteoarthritis (OA), and leptin is among the adipokines implicated in obesity-induced OA. However, the specific role of leptin in OA severity and pain is not known. Using lipodystrophic (LD) mice, we show that fat-secreted factors are required for knee OA development, implicating a fat-cartilage cross-talk. Fat pad implantation or systemic leptin restoration in LD mice reintroduced structural OA and pain, whereas implantation of leptin-deficient fat pad did not change OA susceptibility. Isochronic parabiosis and spatial transcriptomics confirmed that a fat-joint cross-talk likely occurred via soluble mediators. Global unsupervised multiomics of conditioned media from fat implants revealed that leptin exerts a regulatory effect on adipsin (or complement factor D), the activity of which modulates the contrastive OA structural and pain phenotype. These findings suggest that adipokines influence OA pathogenesis, providing conclusive evidence of a fat-joint cross-talk and implicating OA as a systemic disease of adipose tissue.",

author = "Collins, {Kelsey H.} and Lenz, {Kristin L.} and Welhaven, {Hope D.} and Erica Ely and Springer, {Luke E.} and Sophie Paradi and Ruhang Tang and Lauryn Braxton and Antonina Akk and Huimin Yan and Bo Zhang and Xiaobo Wu and Atkinson, {John P.} and Oestreich, {Arin K.} and June, {Ron K.} and Pham, {Christine T.N.} and Farshid Guilak",

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doi = "10.1126/sciadv.adt5915",

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AU - Collins, Kelsey H.

AU - Lenz, Kristin L.

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AU - Ely, Erica

AU - Springer, Luke E.

AU - Paradi, Sophie

AU - Tang, Ruhang

AU - Braxton, Lauryn

AU - Akk, Antonina

AU - Yan, Huimin

AU - Zhang, Bo

AU - Wu, Xiaobo

AU - Atkinson, John P.

AU - Oestreich, Arin K.

AU - June, Ron K.

AU - Pham, Christine T.N.

AU - Guilak, Farshid

N1 - Publisher Copyright: © 2025 The Authors, some rights reserved; exclusive licensee American Association for the Advancement of Science. No claim to original U.S. Government Works. Distributed under a Creative Commons Attribution NonCommercial License 4.0 (CC BY-N C).

PY - 2025/4/25

Y1 - 2025/4/25

N2 - Obesity is a risk factor for osteoarthritis (OA), and leptin is among the adipokines implicated in obesity-induced OA. However, the specific role of leptin in OA severity and pain is not known. Using lipodystrophic (LD) mice, we show that fat-secreted factors are required for knee OA development, implicating a fat-cartilage cross-talk. Fat pad implantation or systemic leptin restoration in LD mice reintroduced structural OA and pain, whereas implantation of leptin-deficient fat pad did not change OA susceptibility. Isochronic parabiosis and spatial transcriptomics confirmed that a fat-joint cross-talk likely occurred via soluble mediators. Global unsupervised multiomics of conditioned media from fat implants revealed that leptin exerts a regulatory effect on adipsin (or complement factor D), the activity of which modulates the contrastive OA structural and pain phenotype. These findings suggest that adipokines influence OA pathogenesis, providing conclusive evidence of a fat-joint cross-talk and implicating OA as a systemic disease of adipose tissue.

AB - Obesity is a risk factor for osteoarthritis (OA), and leptin is among the adipokines implicated in obesity-induced OA. However, the specific role of leptin in OA severity and pain is not known. Using lipodystrophic (LD) mice, we show that fat-secreted factors are required for knee OA development, implicating a fat-cartilage cross-talk. Fat pad implantation or systemic leptin restoration in LD mice reintroduced structural OA and pain, whereas implantation of leptin-deficient fat pad did not change OA susceptibility. Isochronic parabiosis and spatial transcriptomics confirmed that a fat-joint cross-talk likely occurred via soluble mediators. Global unsupervised multiomics of conditioned media from fat implants revealed that leptin exerts a regulatory effect on adipsin (or complement factor D), the activity of which modulates the contrastive OA structural and pain phenotype. These findings suggest that adipokines influence OA pathogenesis, providing conclusive evidence of a fat-joint cross-talk and implicating OA as a systemic disease of adipose tissue.

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Adipose-derived leptin and complement factor D mediate osteoarthritis severity and pain

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