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      Potent anti-inflammatory activity of betulinic acid treatment in a model of lethal endotoxemia.

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          Abstract

          Betulinic acid (BA) is a lupane-type triterpene with a number of biological activities already reported. While potent anti-HIV and antitumoral activities were attributed to BA, it is considered to have a moderate anti-inflammatory activity. Here we evaluated the effects of BA in a mouse model of endotoxic shock. Endotoxemia was induced through intraperitoneally LPS administration, nitric oxide (NO) and cytokines were assessed by Griess method and ELISA, respectively. Treatment of BALB/c mice with BA at 67 mg/kg caused a 100% survival against a lethal dose of lipopolysaccharide (LPS). BA treatment caused a reduction in TNF-α production induced by LPS but did not alter IL-6 production. Moreover, BA treatment increased significantly the serum levels of IL-10 compared to vehicle-treated, LPS-challenged mice. To investigate the role of IL-10 in BA-induced protection, wild-type and IL-10(-/-) mice were studied. In contrast to the observations in IL-10(+/+) mice, BA did not protect IL-10(-/-) mice against a lethal LPS challenge. Addition of BA inhibited the production of pro-inflammatory mediators by macrophages stimulated with LPS, while promoting a significant increase in IL-10 production. BA-treated peritoneal exudate macrophages produced lower concentrations of TNF-α and NO and higher concentrations of IL-10 upon LPS stimulation. Similarly, macrophages obtained from BA-treated mice produced less pro-inflammatory mediators and increased IL-10 when compared to non-stimulated macrophages obtained from vehicle-treated mice. In conclusion, we have shown that BA has a potent anti-inflammatory activity in vivo, protecting mice against LPS by modulating TNF-α production by macrophages in vivo through a mechanism dependent on IL-10.

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          Author and article information

          Journal
          Int. Immunopharmacol.
          International immunopharmacology
          Elsevier BV
          1878-1705
          1567-5769
          Dec 2014
          : 23
          : 2
          Affiliations
          [1 ] Laboratory of Tissue Engineering and Immunopharmacology Gonçalo Moniz Research Center, Oswaldo Cruz Foundation, Rua Waldemar Falcão, 121, 40296-750, Salvador, Bahia, Brazil.
          [2 ] Laboratory of Pharmaceutical Technology, Federal University of Paraíba, João Pessoa, Cidade Universitária, s/n, 58051-900, João Pessoa, PB, Brazil.
          [3 ] Laboratory of Tissue Engineering and Immunopharmacology Gonçalo Moniz Research Center, Oswaldo Cruz Foundation, Rua Waldemar Falcão, 121, 40296-750, Salvador, Bahia, Brazil; Department of Life Sciences, State University of Bahia, Rua Silveira Martins, 2555, 41150-000, Salvador, BA, Brazil.
          [4 ] Laboratory of Tissue Engineering and Immunopharmacology Gonçalo Moniz Research Center, Oswaldo Cruz Foundation, Rua Waldemar Falcão, 121, 40296-750, Salvador, Bahia, Brazil; Center of Biotecnology and Cell Therapy, São Rafael Hospital, Av. São Rafael, 2152. São Marcos 41253-190, Salvador, BA, Brazil.
          [5 ] Laboratory of Tissue Engineering and Immunopharmacology Gonçalo Moniz Research Center, Oswaldo Cruz Foundation, Rua Waldemar Falcão, 121, 40296-750, Salvador, Bahia, Brazil; Center of Biotecnology and Cell Therapy, São Rafael Hospital, Av. São Rafael, 2152. São Marcos 41253-190, Salvador, BA, Brazil. Electronic address: milena@bahia.fiocruz.br.
          Article
          S1567-5769(14)00373-7
          10.1016/j.intimp.2014.09.021
          25281393
          5e1bdc07-e0b9-45c8-9654-9de665bd6b1a
          History

          Betulinic acid,Endotoxemia,Macrophages,Anti-inflammatory activity,Cytokines

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