Adipsin promotes bone marrow adiposity by priming mesenchymal stem cells

BACKGROUND: Marrow adipose tissue (MAT) has been shown to be vital for regulating metabolism and maintaining skeletal homeostasis in the bone marrow (BM) niche. As a reflection of BM remodeling, MAT is highly responsive to nutrient fluctuations, hormonal changes, and metabolic disturbances such as o...

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Autores principales: Aaron, Nicole, Kraakman, Michael J, Zhou, Qiuzhong, Liu, Qiongming, Costa, Samantha, Yang, Jing, Liu, Longhua, Yu, Lexiang, Wang, Liheng, He, Ying, Fan, Lihong, Hirakawa, Hiroyuki, Ding, Lei, Lo, James, Wang, Weidong, Zhao, Baohong, Guo, Edward, Sun, Lei, Rosen, Cliff J, Qiang, Li
Formato: Online Artículo Texto
Lenguaje:English
Publicado: eLife Sciences Publications, Ltd 2021
Materias:
Medicine
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8219379/
https://www.ncbi.nlm.nih.gov/pubmed/34155972
http://dx.doi.org/10.7554/eLife.69209
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author Aaron, Nicole
Kraakman, Michael J
Zhou, Qiuzhong
Liu, Qiongming
Costa, Samantha
Yang, Jing
Liu, Longhua
Yu, Lexiang
Wang, Liheng
He, Ying
Fan, Lihong
Hirakawa, Hiroyuki
Ding, Lei
Lo, James
Wang, Weidong
Zhao, Baohong
Guo, Edward
Sun, Lei
Rosen, Cliff J
Qiang, Li
author_facet Aaron, Nicole
Kraakman, Michael J
Zhou, Qiuzhong
Liu, Qiongming
Costa, Samantha
Yang, Jing
Liu, Longhua
Yu, Lexiang
Wang, Liheng
He, Ying
Fan, Lihong
Hirakawa, Hiroyuki
Ding, Lei
Lo, James
Wang, Weidong
Zhao, Baohong
Guo, Edward
Sun, Lei
Rosen, Cliff J
Qiang, Li
author_sort Aaron, Nicole
collection PubMed
description BACKGROUND: Marrow adipose tissue (MAT) has been shown to be vital for regulating metabolism and maintaining skeletal homeostasis in the bone marrow (BM) niche. As a reflection of BM remodeling, MAT is highly responsive to nutrient fluctuations, hormonal changes, and metabolic disturbances such as obesity and diabetes mellitus. Expansion of MAT has also been strongly associated with bone loss in mice and humans. However, the regulation of BM plasticity remains poorly understood, as does the mechanism that links changes in marrow adiposity with bone remodeling. METHODS: We studied deletion of Adipsin, and its downstream effector, C3, in C57BL/6 mice as well as the bone-protected PPARγ constitutive deacetylation 2KR mice to assess BM plasticity. The mice were challenged with thiazolidinedione treatment, calorie restriction, or aging to induce bone loss and MAT expansion. Analysis of bone mineral density and marrow adiposity was performed using a μCT scanner and by RNA analysis to assess adipocyte and osteoblast markers. For in vitro studies, primary bone marrow stromal cells were isolated and subjected to osteoblastogenic or adipogenic differentiation or chemical treatment followed by morphological and molecular analyses. Clinical data was obtained from samples of a previous clinical trial of fasting and high-calorie diet in healthy human volunteers. RESULTS: We show that Adipsin is the most upregulated adipokine during MAT expansion in mice and humans in a PPARγ acetylation-dependent manner. Genetic ablation of Adipsin in mice specifically inhibited MAT expansion but not peripheral adipose depots, and improved bone mass during calorie restriction, thiazolidinedione treatment, and aging. These effects were mediated through its downstream effector, complement component C3, to prime common progenitor cells toward adipogenesis rather than osteoblastogenesis through inhibiting Wnt/β-catenin signaling. CONCLUSIONS: Adipsin promotes new adipocyte formation and affects skeletal remodeling in the BM niche. Our study reveals a novel mechanism whereby the BM sustains its own plasticity through paracrine and endocrine actions of a unique adipokine. FUNDING: This work was supported by the National Institutes of Health T32DK007328 (NA), F31DK124926 (NA), R01DK121140 (JCL), R01AR068970 (BZ), R01AR071463 (BZ), R01DK112943 (LQ), R24DK092759 (CJR), and P01HL087123 (LQ).
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spelling pubmed-82193792021-06-23 Adipsin promotes bone marrow adiposity by priming mesenchymal stem cells Aaron, Nicole Kraakman, Michael J Zhou, Qiuzhong Liu, Qiongming Costa, Samantha Yang, Jing Liu, Longhua Yu, Lexiang Wang, Liheng He, Ying Fan, Lihong Hirakawa, Hiroyuki Ding, Lei Lo, James Wang, Weidong Zhao, Baohong Guo, Edward Sun, Lei Rosen, Cliff J Qiang, Li eLife Medicine BACKGROUND: Marrow adipose tissue (MAT) has been shown to be vital for regulating metabolism and maintaining skeletal homeostasis in the bone marrow (BM) niche. As a reflection of BM remodeling, MAT is highly responsive to nutrient fluctuations, hormonal changes, and metabolic disturbances such as obesity and diabetes mellitus. Expansion of MAT has also been strongly associated with bone loss in mice and humans. However, the regulation of BM plasticity remains poorly understood, as does the mechanism that links changes in marrow adiposity with bone remodeling. METHODS: We studied deletion of Adipsin, and its downstream effector, C3, in C57BL/6 mice as well as the bone-protected PPARγ constitutive deacetylation 2KR mice to assess BM plasticity. The mice were challenged with thiazolidinedione treatment, calorie restriction, or aging to induce bone loss and MAT expansion. Analysis of bone mineral density and marrow adiposity was performed using a μCT scanner and by RNA analysis to assess adipocyte and osteoblast markers. For in vitro studies, primary bone marrow stromal cells were isolated and subjected to osteoblastogenic or adipogenic differentiation or chemical treatment followed by morphological and molecular analyses. Clinical data was obtained from samples of a previous clinical trial of fasting and high-calorie diet in healthy human volunteers. RESULTS: We show that Adipsin is the most upregulated adipokine during MAT expansion in mice and humans in a PPARγ acetylation-dependent manner. Genetic ablation of Adipsin in mice specifically inhibited MAT expansion but not peripheral adipose depots, and improved bone mass during calorie restriction, thiazolidinedione treatment, and aging. These effects were mediated through its downstream effector, complement component C3, to prime common progenitor cells toward adipogenesis rather than osteoblastogenesis through inhibiting Wnt/β-catenin signaling. CONCLUSIONS: Adipsin promotes new adipocyte formation and affects skeletal remodeling in the BM niche. Our study reveals a novel mechanism whereby the BM sustains its own plasticity through paracrine and endocrine actions of a unique adipokine. FUNDING: This work was supported by the National Institutes of Health T32DK007328 (NA), F31DK124926 (NA), R01DK121140 (JCL), R01AR068970 (BZ), R01AR071463 (BZ), R01DK112943 (LQ), R24DK092759 (CJR), and P01HL087123 (LQ). eLife Sciences Publications, Ltd 2021-06-22 /pmc/articles/PMC8219379/ /pubmed/34155972 http://dx.doi.org/10.7554/eLife.69209 Text en © 2021, Aaron et al https://creativecommons.org/licenses/by/4.0/This article is distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use and redistribution provided that the original author and source are credited.
spellingShingle Medicine
Aaron, Nicole
Kraakman, Michael J
Zhou, Qiuzhong
Liu, Qiongming
Costa, Samantha
Yang, Jing
Liu, Longhua
Yu, Lexiang
Wang, Liheng
He, Ying
Fan, Lihong
Hirakawa, Hiroyuki
Ding, Lei
Lo, James
Wang, Weidong
Zhao, Baohong
Guo, Edward
Sun, Lei
Rosen, Cliff J
Qiang, Li
Adipsin promotes bone marrow adiposity by priming mesenchymal stem cells
title Adipsin promotes bone marrow adiposity by priming mesenchymal stem cells
title_full Adipsin promotes bone marrow adiposity by priming mesenchymal stem cells
title_fullStr Adipsin promotes bone marrow adiposity by priming mesenchymal stem cells
title_full_unstemmed Adipsin promotes bone marrow adiposity by priming mesenchymal stem cells
title_short Adipsin promotes bone marrow adiposity by priming mesenchymal stem cells
title_sort adipsin promotes bone marrow adiposity by priming mesenchymal stem cells
topic Medicine
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8219379/
https://www.ncbi.nlm.nih.gov/pubmed/34155972
http://dx.doi.org/10.7554/eLife.69209
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