Autophagy in osteoblasts is involved in mineralization and bone homeostasis

被引:404
作者
Nollet, Marie [1 ]
Santucci-Darmanin, Sabine [1 ]
Breuil, Veronique [1 ,2 ]
Al-Sahlanee, Rasha [1 ]
Cros, Chantal [1 ]
Topi, Majlinda [1 ]
Momier, David [1 ]
Samson, Michel [1 ]
Pagnotta, Sophie [3 ]
Cailleteau, Laurence [4 ]
Battaglia, Severine [5 ]
Farlay, Delphine [6 ]
Dacquin, Romain [7 ]
Barois, Nicolas [8 ]
Jurdic, Pierre [7 ]
Boivin, Georges [6 ]
Heymann, Dominique [5 ]
Lafont, Frank [8 ,9 ]
Lu, Shi Shou [10 ]
Dempster, David W. [10 ]
Carle, Georges F. [1 ]
Pierrefite-Carle, Valerie [1 ]
机构
[1] Univ Nice Sophia Antipolis, Fac Med, UMR MATOs CEA iBEB SBTN CAL E 4320, F-06189 Nice, France
[2] CHU Nice, Serv Rhumatol, F-06202 Nice, France
[3] Univ Nice Sophia Antipolis, Ctr Commun Microscopie Appl, F-06189 Nice, France
[4] Univ Nice Sophia Antipolis, Fac Med, Plateforme Imagerie IRCAN, F-06189 Nice, France
[5] Univ Nantes, INSERM UMR 957, Equipe Labellisee Ligue Natl Canc 2012, Nantes, France
[6] Univ Lyon, INSERM UMR 1033, Lyon, France
[7] Univ Lyon, CNRS, Inst Genom Fonct Lyon, Ecole Normale Super Lyon, Lyon, France
[8] Inst Pasteur, Plate Forme BICeL IFR142, F-59019 Lille, France
[9] Univ Lille Nord France, Inst Pasteur Lille, CNRS UMR 8204, INSERM U1019, Lille, France
[10] Helen Hayes Hosp, Reg Bone Ctr, West Havertsraw, NY USA
关键词
autophagy; bone remodeling; mineralization; osteoblast; INTRACELLULAR CALCIUM-PHOSPHATE; OXIDATIVE STRESS; UNCONVENTIONAL SECRETION; HYDROGEN-PEROXIDE; PATHWAY; DISEASE; PROTEIN; APOPTOSIS; VESICLES; GENDER;
D O I
10.4161/auto.36182
中图分类号
Q2 [细胞生物学];
学科分类号
071009 ; 090102 ;
摘要
Bone remodeling is a tightly controlled mechanism in which osteoblasts (OB), the cells responsible for bone formation, osteoclasts (OC), the cells specialized for bone resorption, and osteocytes, the multifunctional mechanosensing cells embedded in the bone matrix, are the main actors. Increased oxidative stress in OB, the cells producing and mineralizing bone matrix, has been associated with osteoporosis development but the role of autophagy in OB has not yet been addressed. This is the goal of the present study. We first show that the autophagic process is induced in OB during mineralization. Then, using knockdown of autophagy-essential genes and OB-specific autophagy-deficient mice, we demonstrate that autophagy deficiency reduces mineralization capacity. Moreover, our data suggest that autophagic vacuoles could be used as vehicles in OB to secrete apatite crystals. In addition, autophagy-deficient OB exhibit increased oxidative stress and secretion of the receptor activator of NFKB1 (TNFSF11/RANKL), favoring generation of OC, the cells specialized in bone resorption. In vivo, we observed a 50% reduction in trabecular bone mass in OB-specific autophagy-deficient mice. Taken together, our results show for the first time that autophagy in OB is involved both in the mineralization process and in bone homeostasis. These findings are of importance for mineralized tissues which extend from corals to vertebrates and uncover new therapeutic targets for calcified tissue-related metabolic pathologies.
引用
收藏
页码:1965 / 1977
页数:13
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