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http://dx.doi.org/10.5142/JGR.2008.32.4.315

Compound K Rich Fractions Regulate NF-κB-dependent Inflammatory Responses and Protect Mice from Endotoxin-induced Lethal Shock  

Yang, Chul-Su (Department of Microbiology and Infection Signaling Network Research Center)
Yuk, Jae-Min (Department of Microbiology and Infection Signaling Network Research Center)
Ko, Sung-Ryong (Ginseng Research Group, KT&G Central Research Institute)
Cho, Byung-Goo (Ginseng Research Group, KT&G Central Research Institute)
Sohn, Hyun-Joo (Ginseng Research Group, KT&G Central Research Institute)
Kim, Young-Sook (Ginseng Research Group, KT&G Central Research Institute)
Wee, Jae-Joon (Ginseng Research Group, KT&G Central Research Institute)
Do, Jae-Ho (Ginseng Research Group, KT&G Central Research Institute)
Jo, Eun-Kyeong (Department of Microbiology and Infection Signaling Network Research Center)
Publication Information
Journal of Ginseng Research / v.32, no.4, 2008 , pp. 315-323 More about this Journal
Abstract
In the previous studies, we isolated the compound K rich fractions (CKRF) and showed that CKRF inhibited Toll-like receptor (TLR) 4- or TLR9-induced inflammatory signaling. To extend our previous studies,1) we investigated the molecular mechanisms of CKRF in the TLR4-associated signaling via nuclear factor (NF)-${\kappa}B$, and in vivo role of CKRF for induction of tolerance in lipopolysaccharide (LPS)-induced septic shock. In murine bone marrow-dervied macrophages, CKRF significantly inhibited the induction of mRNA expression of proinflammatory mediators such as tumor necrosis factor-${\alpha}$, interleukin-6, cyclooxygenase-2, and inducible nitric oxide synthase. In addition, CKRF significantly attenuated the transcriptional activities of TLR4/LPS-induced NF-${\kappa}B$. Nuclear translocation of NF-${\kappa}B$ in response to LPS stimulation was significantly abrogated by pre-treatment with CKRF. Furthermore, CKRF inhibited the recruitment of p65 to the interferon-sensitive response element flanking region in response to LPS. Finally, oral administration of CKRF significantly protected mice from Gram-negative bacterial LPS-induced lethal shock and inhibited systemic inflammatory cytokine levels. Together, these results demonstrate that CKRF modulates the TLR4-dependent NF-${\kappa}B$ activation, and suggest a therapeutic role for Gram-negative septic shock.
Keywords
Compound K rich fractions; Toll-like receptor 4; nuclear factor ${\kappa}B$; endotoxemia;
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