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Senescent macrophages in the human adipose tissue as a source of inflammaging
Giulia Matacchione, Jessica Perugini, Eleonora Di Mercurio, Jacopo Sabbatinelli, Francesco Prattichizzo, Martina Senzacqua, Gianluca Storci, Christian Dani, Giovanni Lezoche, Mario Guerrieri, Antonio Giordano, Massimiliano Bonafè, Fabiola Olivieri
GeroScience · 2022 · ▲ 68 citations
Deregulated nutrient-sensing
Cellular senescence
Altered intercellular communication
Chronic inflammation
Cell culture / in vitro
Human
In vitro
Abstract
Obesity is a major risk factor for type 2 diabetes and a trigger of chronic and systemic inflammation. Recent evidence suggests that an increased burden of senescent cells (SCs) in the adipose tissue of obese/diabetic animal models might underlie such pro-inflammatory phenotype. However, the role of macrophages as candidate SCs, their phenotype, the distribution of SCs among fat depots, and clinical relevance are debated. The senescence(definition) marker β-galactosidase and the macrophage marker CD68 were scored in visceral (vWAT) and subcutaneous (scWAT) adipose tissue from obese patients (n=17) undergoing bariatric surgery and control patients (n=4) subjected to cholecystectomy. A correlation was made between the number of SCs and BMI, serum insulin, and the insulin resistance (IR) index HOMA. The monocyte cell line (THP-1) was cultured in vitro in high glucose milieu (60 mM D-glucose) and subsequently co-cultured with human adipocytes (hMADS) to investigate the reciprocal inflammatory activation. In obese patients, a significantly higher number of SCs was observed in vWAT compared to scWAT; about 70% of these cells expressed the macrophage marker CD68; and the number of SCs in vWAT, but not in scWAT, positively correlated with BMI, HOMA-IR, and insulin. THP-1 cultured in vitro in high glucose milieu acquired a senescent-like phenotype (HgSMs), characterized by a polarization toward a mixed M1/M2-like secretory phenotype. Co-culturing HgSMs with hMADS elicited pro-inflammatory cytokine expression in both cell types, and defective insulin signaling in hMADS. In morbid obesity, expansion of visceral adipose depots involves an increased burden of macrophages with senescent-like phenotype that may promote a pro-inflammatory profile and impair insulin signaling in adipocytes, supporting a framework where senescent macrophages fuel obesity-induced systemic inflammation and possibly contribute to the development of IR.
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- DOI
- 10.1007/s11357-022-00536-0
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- 2026-06-11 MST
Cite this
APA
Matacchione, G., Perugini, J., Mercurio, E.D., Sabbatinelli, J., Prattichizzo, F., Senzacqua, M., Storci, G., Dani, C., Lezoche, G., Guerrieri, M., Giordano, A., Bonafè, M., & Olivieri, F. (2022). Senescent macrophages in the human adipose tissue as a source of inflammaging. <em>GeroScience</em>. https://doi.org/10.1007/s11357-022-00536-0
Vancouver
Matacchione G, Perugini J, Mercurio ED, Sabbatinelli J, Prattichizzo F, Senzacqua M, et al. Senescent macrophages in the human adipose tissue as a source of inflammaging. GeroScience. 2022. doi:10.1007/s11357-022-00536-0.
BibTeX
@article{giulia2022Senesc,
title = {Senescent macrophages in the human adipose tissue as a source of inflammaging},
author = {Giulia Matacchione and Jessica Perugini and Eleonora Di Mercurio and Jacopo Sabbatinelli and Francesco Prattichizzo and Martina Senzacqua and Gianluca Storci and Christian Dani and Giovanni Lezoche and Mario Guerrieri and Antonio Giordano and Massimiliano Bonafè and Fabiola Olivieri},
journal = {GeroScience},
year = {2022},
doi = {10.1007/s11357-022-00536-0},
}
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