Pharmaceuticals (Jan 2023)

Cytotoxic and Antileishmanial Effects of the Monoterpene β-Ocimene

  • Julyanne Maria Saraiva de Sousa,
  • Thaís Amanda de Lima Nunes,
  • Raiza Raianne Luz Rodrigues,
  • João Paulo Araújo de Sousa,
  • Maria da Conceição Albuquerque Val,
  • Francisco Alex da Rocha Coelho,
  • Airton Lucas Sousa dos Santos,
  • Nicolle Barreira Maciel,
  • Vanessa Maria Rodrigues de Souza,
  • Yasmim Alves Aires Machado,
  • Paulo Sérgio de Araújo Sousa,
  • Alyne Rodrigues de Araújo,
  • Jefferson Almeida Rocha,
  • Damião Pergentino de Sousa,
  • Marcos Vinicius da Silva,
  • Daniel Dias Rufino Arcanjo,
  • Klinger Antônio da Franca Rodrigues

DOI
https://doi.org/10.3390/ph16020183
Journal volume & issue
Vol. 16, no. 2
p. 183

Abstract

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Leishmaniasis is a group of infectious-parasitic diseases with high mortality rates, and endemic in many regions of the globe. The currently available drugs present serious problems such as high toxicity, costs, and the emergence of drug resistance. This has stimulated research into new antileishmania drugs based on natural products and their derivatives. β-Ocimene is a monoterpene found naturally in the essential oils of many plant species which presents antileishmanial activity, and which has not yet been evaluated for its potential to inhibit the etiological agent of leishmaniasis. The aim of this work was to evaluate the activity of β-ocimene against Leishmania amazonensis, its cytotoxicity, and potential mechanisms of action. β-Ocimene presented direct activity against the parasite, with excellent growth inhibition of promastigotes (IC50 = 2.78 μM) and axenic amastigotes (EC50 = 1.12 μM) at concentrations non-toxic to RAW 264.7 macrophages (CC50 = 114.5 µM). The effect is related to changes in membrane permeability and resulting abnormalities in the parasitic cell shape. These were, respectively, observed in membrane integrity and atomic force microscopy assays. β-Ocimene was also shown to act indirectly, with greater activity against intra-macrophagic amastigotes (EC50 = 0.89 μM), increasing TNF-α, nitric oxide (NO), and reactive oxygen species (ROS), with lysosomal effects, as well as promoting decreases in IL-10 and IL-6. Against intra-macrophagic amastigote forms the selectivity index was higher than the reference drugs, being 469.52 times more selective than meglumine antimoniate, and 42.88 times more selective than amphotericin B. Our results suggest that β-ocimene possesses promising in vitro antileishmania activity and is a potential candidate for investigation in in vivo assays.

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