High Glucose Induces Autophagy through PPARγ-Dependent Pathway in Human Nucleus Pulposus Cells.

IF 3.5 3区 医学 Q2 MEDICINE, RESEARCH & EXPERIMENTAL
PPAR Research Pub Date : 2018-03-01 eCollection Date: 2018-01-01 DOI:10.1155/2018/8512745
Chang Jiang, Shuhao Liu, Yuanwu Cao, Hongping Shan
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引用次数: 8

Abstract

Diabetes mellitus is a multiorgan disorder affecting many types of connective tissues, including bone and cartilage. High glucose could accelerate the autophagy in nucleus pulposus (NP) cells. In our present study, we investigated whether peroxisome proliferator-activated receptor γ (PPAR-γ) pathway is involved into autophagy regulation in NP cells under high glucose condition. After NP cells were treated with different high glucose concentrations for 72 hours, the rate of autophagy increased. Moreover, the levels of PPARγ, Beclin-1, and LC3II were significantly increased and p62 was significantly decreased compared to control group. Then, NP cells were treated with high glucose plus PPARγ agonist or PPARγ antagonist, respectively. The rate of autophagy and the levels of Beclin-1 and LC3II increased, but p62 decreased when PPARγ agonist was used. On the contrary, the rate of autophagy and the levels of Beclin-1 and LC3II decreased, while p62 increased when PPARγ antagonist was added. These results suggested that autophagy induced by high glucose in NP cells was through PPARγ-dependent pathway.

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高糖通过ppar γ依赖途径诱导人髓核细胞自噬。
糖尿病是一种多器官疾病,影响多种结缔组织,包括骨和软骨。高糖可促进髓核细胞的自噬。在本研究中,我们研究了过氧化物酶体增殖激活受体γ (PPAR-γ)途径是否参与高糖条件下NP细胞的自噬调节。不同高浓度葡萄糖处理NP细胞72小时后,细胞自噬率升高。与对照组相比,PPARγ、Beclin-1、LC3II水平显著升高,p62水平显著降低。然后,分别用高糖加PPARγ激动剂或PPARγ拮抗剂处理NP细胞。使用PPARγ激动剂后,细胞自噬率升高,Beclin-1和LC3II水平升高,p62水平降低。相反,加入PPARγ拮抗剂后,自噬率降低,Beclin-1和LC3II水平降低,p62水平升高。提示高糖诱导NP细胞自噬是通过ppar γ依赖途径进行的。
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来源期刊
PPAR Research
PPAR Research MEDICINE, RESEARCH & EXPERIMENTAL-
CiteScore
6.20
自引率
3.40%
发文量
17
审稿时长
12 months
期刊介绍: PPAR Research is a peer-reviewed, Open Access journal that publishes original research and review articles on advances in basic research focusing on mechanisms involved in the activation of peroxisome proliferator-activated receptors (PPARs), as well as their role in the regulation of cellular differentiation, development, energy homeostasis and metabolic function. The journal also welcomes preclinical and clinical trials of drugs that can modulate PPAR activity, with a view to treating chronic diseases and disorders such as dyslipidemia, diabetes, adipocyte differentiation, inflammation, cancer, lung diseases, neurodegenerative disorders, and obesity.
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