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Featured researches published by Bingwei Sun.


Acta Pharmacologica Sinica | 2008

Suppression of inflammatory cytokine production and oxidative stress by CO-releasing molecules—liberated CO in the small intestine of thermally-injured mice

Dongming Liu; Bingwei Sun; Zhiwei Sun; Qin Jin; Yan Sun; Xi Chen

AbstractAim:To determine whether carbon monoxide (CO)-releasing molecules-liberated CO suppress inflammatory cytokine production and oxidative stress in the small intestine of burnt mice.Methods:Twenty-eight mice were assigned to 4 groups. The mice in the sham group (n=7) underwent sham thermal injury, whereas the mice in the burn group (n=7) received 15% total body surface area full-thickness thermal injury, the mice in the burn+CO-releasing molecules (CORM)-2 group (n=7) underwent the same injury with immediate administration of CORM-2 (8 mg/kg, iv), and the mice in the burn+inactivated CORM (iCORM)-2 group (n=7) underwent the same injury with immediate administration of iCORM-2. The levels of inflammatory cytokines in the tissue homogenates were measured by ELISA. The levels of malondialdehyde (MDA), nitric oxide (NO) and the expression of inducible nitric oxide synthase (iNOS) in the small intestine were also assessed. In the in vitro experiment, Caco-2 cells were stimulated by experimental mouse sera (50%, v/v) for 4 h. Subsequently, the levels of interleukin (IL)-8 and NO in the supernatants were assessed. Reactive oxygen species (ROS) generation in Caco-2 cells was also measured.Results:The treatment of burnt mice with CORM-2 significantly attenuated the levels of IL-1β, TNF-α, MDA, and NO in tissue homogenates. This was accompanied by a decrease of iNOS expression. In parallel, the levels of IL-8, NO, and intracellular ROS generation in the supernatants of Caco-2 stimulated by the CORM-2-treated burnt mouse sera was markedly decreased.Conclusion:CORM-released CO attenuates the production of inflammatory cytokines, prevents burn-induced ROS generation, and suppresses the oxidative stress in the small intestine of burnt mice by interfering with the protein expression of iNOS.


International Journal of Biological Sciences | 2008

CO-releasing molecules (CORM-2)-liberated CO attenuates leukocytes infiltration in the renal tissue of thermally injured mice.

Bingwei Sun; Zhiwei Sun; Qin Jin; Xi Chen


World Journal of Gastroenterology | 2008

CO liberated from CORM-2 modulates the inflammatory response in the liver of thermally injured mice

Bingwei Sun; Yan Sun; Zhiwei Sun; Xi Chen


World Journal of Gastroenterology | 2007

Carbon liberated from CO-releasing molecules attenuates leukocyte infiltration in the small intestine of thermally injured mice

Bingwei Sun; Qin Jin; Yan Sun; Zhiwei Sun; Xi Chen; Zhao-Yong Chen; Gediminas Cepinskas


National Medical Journal of China | 2007

[Molecular mechanism of inhibition of early pulmonary injury and inflammatory response by exogenous carbon monoxide: experiment with mice].

Bingwei Sun; Xuling Chen; Chen Zy; Katada K; Cepinskas G


Archive | 2009

Application of carbon monoxide release molecules in preparing medicament for treating early sepsis

Bingwei Sun; Dongming Liu; Xi Chen


Archive | 2012

Application of carbon monoxide molecules in inhibition on acute rejection after skin grafting

Bingwei Sun; Zhiwei Sun; Yan Sun


Archive | 2009

Use of carbon monoxide released substance in preparing medicine for treating pyemia

Bingwei Sun; Dongming Liu; Xi Chen


The FASEB Journal | 2007

Carbon monoxide (CO)-releasing molecule (CORM)-liberated CO attenuates inflammatory response in the liver of thermally-injured mice

Bingwei Sun; Aurelia Bihari; Xi Chen; Zhao-Yong Chen; Ningzheng Tai; Richard F. Potter; Gediminas Cepinskas


Archive | 2010

Application of carbon monoxide-releasing molecules and heparin in preparing medicament for treating sepsis

Bingwei Sun; Dongming Liu; Xi Chen

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Aurelia Bihari

University of Western Ontario

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Richard F. Potter

University of Western Ontario

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Xuling Chen

Central South University

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