Trypanocidal Structure-Activity Relationshipfor Cis- and Trans-methylpluviatolide

R. Silva; J. Saraiva; S. Albuquerque; C. Curti; P. M. Donate; T. N. C. Bianco; J. K. Bastos; M. L. A. Silva

doi:10.1055/s-2008-1075250

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Planta Med 2008; 74 - P-54
DOI: 10.1055/s-2008-1075250

Trypanocidal Structure-Activity Relationshipfor Cis- and Trans-methylpluviatolide

R Silva ¹, J Saraiva ², S Albuquerque ², C Curti ³, PM Donate ⁴, TNC Bianco ¹, JK Bastos ², MLA Silva ¹

¹Núcleo de Ciências Exatas e Tecnológicas – Universidade de Franca – Avenida Dr. Armando Salles de Oliveira, 2001, 14404-600, Franca, SP, Brazil
²Departamento de Análises Clínicas, Toxicológicas eBromatológicas da Faculdade de Ciências Farmacêuticas de Ribeirão Preto – Universidade de São Paulo – Avenida do Café, s/n, 14040-903 – Ribeirão Preto – SP, Brazil
³Departamento de Ciências Farmacêuticas da Faculdade de Ciências Farmacêuticas de Ribeirão Preto – Universidade de São Paulo – Avenida do Café, s/n, 14040-903 – Ribeirão Preto – SP, Brazil
⁴Departamento de Química da Faculdade de Filosofia,Ciências e Letras de Ribeirão Preto – Universidade de São Paulo – Avenida Bandeirantes, 3900, 14040-901 – Ribeirão Preto – SP, Brazil

Kongressbeitrag

The trypanocidal activity [1–3] of racemic mixtures of cis- and trans-methylpluviatolides (2) and (1), respectively was evaluated in vitro against Trypomastigote forms of two strains of T. Cruzi, and in the enzymatic assay of T. cruzi gGAPDH. The cytotoxicity of the compounds was assessed by the MTT method using LLC-MK2 cells. The effects of the compounds on peroxide and NO production were also investigated. The mixture of the trans stereoisomers displayed trypanocidal activity (IC₅₀ of 89.3 µM). Therefore, it was separated by chiral HPLC, furnishing the (+) and (−)-enantiomers. Only the (−)-enantiomer was active against the parasite (IC₅₀ of 18.7 µM) [4]. Despite being totally inactive, the (+)-enantiomer acted as an antagonistic competitor. Trans-methylpluviatolide displayed low toxicity for LLC-MK₂ cells, with IC₅₀ of 6.53 mM. Also, methylpluviatolide neither inhibit gGAPDH activity nor hinder peroxide and NO production at the evaluated concentrations. Acknowledgements: thanks to FAPESP for support for this research (Projects' 98/14956-7, 01/12006-6, 05/01550-8 and 06/60132-4). References: [1] Bastos JK, et al. (1999) Planta Med. 65: 541–544. [2] Souza VA, et al. (2005) Biorg Med Chem. 15: 303–307. [3] Da Silva Filho AA, et al. (2004) J Pharm Pharmacol. 56: 1195–1199. [4] Silva MLAE, et al. (2003) Patente WO 03080600.