Up-rerglation of SIRT1 induced by 17beta-estradiol promotes autophagy and inhibits apoptosis in osteoblasts

被引:0
|
作者
Wang, Yu [1 ]
Mei, Runhong [1 ,2 ]
Hao, Shimin [1 ]
Luo, Peng [1 ]
Wang, Penghao [1 ]
Almatari, Yaser [1 ]
Guo, Lei [1 ]
Guo, Lan [1 ]
机构
[1] China Med Univ, Dept Orthoped, Hosp 1, Shenyang 110001, Liaoning, Peoples R China
[2] Nanchang Univ, Affiliated Hosp 4, Med Coll, Dept Orthopaed, Nanchang 330006, Jiangxi, Peoples R China
来源
AGING-US | 2021年 / 13卷 / 20期
基金
中国国家自然科学基金;
关键词
SIRT1; autophagy; apoptosis; AMPK-mTOR; FOXO3a; MESENCHYMAL STEM-CELLS; ALPHA ER-ALPHA; SIGNALING PATHWAY; OXIDATIVE STRESS; MICRONIZED; 17-BETA-ESTRADIOL; OSTEOPROTEGERIN SYNTHESIS; INDUCED OSTEOPOROSIS; BONE; PROTECTS; RECEPTOR;
D O I
暂无
中图分类号
Q2 [细胞生物学];
学科分类号
071009 ; 090102 ;
摘要
Osteoporosis is a common systemic skeletal metabolism disorder resulting in bone fragility and increased fracture risk. Silent information regulator factor 2 homolog 1 (SIRT1) is crucial in the regulation of several biological processes, including bone metabolism, autophagy, apoptosis, and aging. This study aimed to assess whether the up-regulation of SIRT1 induced by 17beta-estradiol (17 beta-E2) could promote autophagy and inhibit apoptosis in osteoblasts via the AMPK-mTOR and FOXO3a pathways, respectively. The study found that 17 beta-E2 (10 -6 M) administration induced the up-regulation of SIRT1 in osteoblasts. Up-regulation of SIRT1 induced by 17 beta-E2 increased the expression level of LC3, Beclin-1, Bcl-2, p-AMPK, FOXO3a but decreased caspase-3 and p-mTOR expression, and then promoted autophagy and inhibited apoptosis. More autophagosomes were observed under a transmission electron microscope (TEM) in 17 beta-E2 and SRT1720 (a selective SIRT1 activator) co-treated group. When Ex527 (a SIRT1-specific inhibitor) was pretreated, the reversed changes were observed. Taken together, our findings demonstrated that the up-regulation of SIRT1 induced by 17 beta-E2 could promote autophagy via the AMPK-mTOR pathway and inhibit apoptosis via the FOXO3a activation in osteoblasts, and SIRT1 might become a more significant target in osteoporosis treatment.
引用
收藏
页码:23652 / 23671
页数:20
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