Yohimbine enhances protection of berberine against LPS-induced mouse lethality through multiple mechanisms

Sepsis remains a major cause of mortality in intensive care units, better therapies are urgently needed. Gram-negative bacterial lipopolysaccharide (LPS) is an important trigger of sepsis. We have demonstrated that berberine (Ber) protects against lethality induced by LPS, which is enhanced by yohim...

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Bibliographic Details
Published in:PloS one 2012-12, Vol.7 (12), p.e52863
Main Authors: Li, Hui, Wang, Yiyang, Zhang, Haoqing, Jia, Baoyin, Wang, Daan, Li, Hongmei, Lu, Daxiang, Qi, Renbin, Yan, Yuxia, Wang, Huadong
Format: Article
Language:English
Subjects:
Activation
Animals
Bacteria
Berberine
Berberine - administration & dosage
Berberine - pharmacology
Biology
Cells, Cultured
Chinese medicine
Drug Synergism
Gene expression
Gram-negative bacteria
Health aspects
Hospitals
Infection
Injuries
Intensive care units
Interferon
Interferon regulatory factor 3
Interleukin 10
IP-10 protein
JNK protein
Kidneys
Kinases
Lethality
Lipopolysaccharides
Lipopolysaccharides - toxicity
Liver
Macrophages
Macrophages, Peritoneal - drug effects
Macrophages, Peritoneal - pathology
Macrophages, Peritoneal - physiology
Male
Medicine
Mice
Mice, Inbred BALB C
Mitogens
Mydriatics - administration & dosage
NF-κB protein
Nitric oxide
Peritoneum
Phosphorylation
Rodents
Sepsis
Sepsis - chemically induced
Sepsis - mortality
Sepsis - prevention & control
Signal Transduction - drug effects
Spleen
Stat1 protein
Tumor necrosis factor-TNF
Tumor necrosis factor-α
Tyk2 protein
Yohimbine
Yohimbine - administration & dosage
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Summary:Sepsis remains a major cause of mortality in intensive care units, better therapies are urgently needed. Gram-negative bacterial lipopolysaccharide (LPS) is an important trigger of sepsis. We have demonstrated that berberine (Ber) protects against lethality induced by LPS, which is enhanced by yohimbine (Y) pretreatment, and Ber combined with Y also improves survival in septic mice. However, the precise mechanisms by which Y enhances protection of Ber against LPS-induced lethality remain unclear. The present study confirmed that simultaneously administered Y also enhanced protection of Ber against LPS-induced lethality. Ber or/and Y attenuated liver injury, but not renal injury in LPS-challenged mice. Ber or/and Y all inhibited LPS-stimulated IκBα, JNK and ERK phosphorylation, NF-κB activation as well as TNF-α production. Ber also increased IL-10 production in LPS-challenged mice, which was enhanced by Y. Furthermore, Ber or/and Y all suppressed LPS-induced IRF3, TyK2 and STAT1 phosphorylation, as well as IFN-β and IP-10 mRNA expression in spleen of mice at 1 h after LPS challenge. Especially, Y enhanced the inhibitory effect of Ber on LPS-induced IP-10 mRNA expression. In vitro experiments further demonstrated that Y significantly enhanced the inhibitory effect of Ber on TNF-α production in LPS-treated peritoneal macrophages, Ber combined with Y promoted LPS-induced IL-10 production and LPS-stimulated IκBα, JNK, ERK and IRF3 phosphorylation and NF-κB activation were also suppressed by Ber or/and Y pretreatment in peritoneal macrophages. Taken together, these results demonstrate that Y enhances the protection of Ber against LPS-induced lethality in mice via attenuating liver injury, upregulating IL-10 production and suppressing IκBα, JNK, ERK and IRF3 phosphorylation. Ber combined with Y may be an effective immunomodulator agent for the prevention of sepsis.
ISSN:1932-6203
1932-6203
DOI:10.1371/journal.pone.0052863