High glucose‑induced upregulation of CD36 promotes inflammation stress via NF‑κB in H9c2 cells

Cardiac inflammation serves an important role in the progression of diabetic cardiomyopathy. CD36 (cluster of differentiation 36) mediates inflammation stress in a variety of disease states. The present study investigated CD36 expression in high glucose (HG)‑induced H9c2 cells, whether CD36 upregula...

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Bibliographic Details
Published inMolecular medicine reports Vol. 24; no. 5
Main Authors Han, Baosheng, Wang, Jianzhong, Wu, Jiawei, Yan, Fang, Wang, Yaru, Li, Jun
Format Journal Article
LanguageEnglish
Published Greece Spandidos Publications UK Ltd 01.11.2021
D.A. Spandidos
Subjects
Acetylcysteine
Acidification
AMP-activated protein kinase
Animals
Antibodies
Apoptosis - drug effects
Cardiomyopathy
CD36 antigen
CD36 Antigens - physiology
Cell culture
Cell Line
Cell membranes
Diabetes
Diabetes mellitus
Diabetic Cardiomyopathies - metabolism
Fatty acids
Flow cytometry
Glucose
Glucose - metabolism
Hyperglycemia
IL-1β
Inflammation
Inflammation - metabolism
Kinases
Lipid metabolism
Metabolism
Myocytes, Cardiac
NF-kappa B - metabolism
NF-κB protein
Proteins
Rats
Reactive oxygen species
Reactive Oxygen Species - metabolism
Signal Transduction - drug effects
Thermal cycling
Tumor necrosis factor-TNF
Tumor necrosis factor-α
Up-regulation
CD36
diabetic cardiomyopathy
inflammation
reactive oxygen species
H9c2 cells
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Summary:Cardiac inflammation serves an important role in the progression of diabetic cardiomyopathy. CD36 (cluster of differentiation 36) mediates inflammation stress in a variety of disease states. The present study investigated CD36 expression in high glucose (HG)‑induced H9c2 cells, whether CD36 upregulation promotes inflammatory stress, and its potential mechanism. HG induced CD36 expression in a time‑dependent manner in cells, which was blocked following CD36 knockout or treatment with N‑acetylcysteine or MitoTEMPO. CD36 translocation to the cell membrane was increased at 72 h by HG stimulation of H9c2 cells. Moreover, CD36 knockout inhibited HG‑induced reactive oxygen species (ROS) generation, tumor necrosis factor‑α, interleukin (IL)‑6 and IL‑1β expression, and nuclear factor (NF)‑κB pathway activation. Further, CD36 knockout reversed metabolic reprogramming, lipid accumulation and AMP‑activated protein kinase activation caused by HG. The aforementioned data suggest that HG‑induced upregulation of CD36 promotes inflammatory stress via NF‑κB in H9c2 cells, mediated by metabolism reprogramming, lipid accumulation and enhanced ROS generation.
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ISSN:1791-2997
1791-3004
DOI:10.3892/mmr.2021.12404