Attenuation of Proinflammatory Responses by S-[6]-Gingerol via Inhibition of ROS/NF-Kappa B/COX2 Activation in HuH7 Cells

Attenuation of Proinflammatory Responses by S-[6]-Gingerol via Inhibition of ROS/NF-Kappa B/COX2 Activation in HuH7 Cells

Introduction. Hepatic inflammation underlies the pathogenesis of chronic diseases such as insulin resistance and type 2 diabetes mellitus. S-[6]-Gingerol has been shown to have anti-inflammatory properties. Important inflammatory mediators of interleukins include nuclear factor κB (NFκB) and cycloox...

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Published in:Evidence-based complementary and alternative medicine Vol. 2013; no. 2013; pp. 1 - 8
Main Authors: McGrath, Kristine C. Y., Li, Yi-Ming, Li, Xiao-Hong, Heather, Alison K., Roufogalis, Basil D., Duke, Colin C., Tran, Van H.
Format: Journal Article
Language:English
Published: Cairo, Egypt Hindawi Puplishing Corporation 01-01-2013
Hindawi Publishing Corporation
Hindawi Limited
Subjects:
Anti-inflammatory agents
Apoptosis
Cell culture
Chemokines
Chronic illnesses
Cyclooxygenase-2
Cytokines
Diabetes mellitus
Diabetes mellitus (non-insulin dependent)
Disease
Gene expression
Gingerol
Hepatocytes
Inflammation
Inflammatory response
Inhibition
Insulin
Insulin resistance
Interleukin 1
Interleukin 6
Interleukin 8
Liver
mRNA
NF-κB protein
Oxidative stress
Pathogenesis
Phosphorylation
Transcription factors
Tumor necrosis factor-TNF
Australia
United States > US
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Summary:Introduction. Hepatic inflammation underlies the pathogenesis of chronic diseases such as insulin resistance and type 2 diabetes mellitus. S-[6]-Gingerol has been shown to have anti-inflammatory properties. Important inflammatory mediators of interleukins include nuclear factor κB (NFκB) and cyclooxygenase 2 (COX2). We now explore the mechanism of anti-inflammatory effects of S-[6]-gingerol in liver cells. Methods. HuH7 cells were stimulated with IL1β to establish an in vitro hepatic inflammatory model. Results. S-[6]-Gingerol attenuated IL1β-induced inflammation and oxidative stress in HuH7 cells, as evidenced by decreasing mRNA levels of inflammatory factor IL6, IL8, and SAA1, suppression of ROS generation, and increasing mRNA levels of DHCR24. In addition, S-[6]-gingerol reduced IL1β-induced COX2 upregulation as well as NFκB activity. Similar to the protective effects of S-[6]-gingerol, both NS-398 (a selective COX2 inhibitor) and PDTC (a selective NFκB inhibitor) suppressed mRNA levels of IL6, IL8, and SAA1. Importantly, PDTC attenuated IL1β-induced overexpression of COX2. Of particular note, the protective effect of S-[6]-gingerol against the IL1β-induced inflammatory response was similar to that of BHT, an ROS scavenger. Conclusions. The findings of this study demonstrate that S-[6]-gingerol protects HuH7 cells against IL1β-induced inflammatory insults through inhibition of the ROS/NFκB/COX2 pathway.
Bibliography:ObjectType-Article-1
SourceType-Scholarly Journals-1
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Academic Editor: Ke Ren
ISSN:1741-427X
1741-4288
DOI:10.1155/2013/146142