4.7 Article

Andiroba oil and nanoemulsion (Carapa guianensis Aublet) reduce lesion severity caused by the antineoplastic agent doxorubicin in mice

Journal

BIOMEDICINE & PHARMACOTHERAPY
Volume 138, Issue -, Pages -

Publisher

ELSEVIER FRANCE-EDITIONS SCIENTIFIQUES MEDICALES ELSEVIER
DOI: 10.1016/j.biopha.2021.111505

Keywords

Crabwood; Histopathology; Immunohistochemistry; Apoptosis

Funding

  1. Coordination for the Improvement of Higher Education Personnel (CAPES) [047/2012]
  2. National Bank for Economic and Social Development - BNDES [2.318.697.0001]
  3. CAPES

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This study investigated the potential of andiroba oil (AO) and a nanoemulsion of andiroba oil (AN) to reduce the side effects of Doxorubicin (DOX) in treating cancer. It was found that andiroba oil reduced the severity of lesions caused by DOX, decreasing hematotoxicity and histological changes, while also reducing apoptotic cell death. In some cases, the nanoemulsion AN showed greater efficacy than AO alone, highlighting the potential of nanotechnology to improve the pharmacokinetics of lipid compounds in the body.
Doxorubicin (DOX) is an anthracycline antibiotic used in the fight against many types of cancer. Although it is quite effective for this purpose, its clinical use is limited by its severe side effects, highlighting the relevance of efforts to identify substances that act to minimize these effects. In this work, we sought to verify the ability of andiroba oil (AO) and a nanoemulsion of andiroba oil (AN) to lessen the side effects of DOX. The animals were separated into 7 groups with 6 animals each: mice treated with AO (2000 mg/kg), AN (2000 mg/kg), the antineoplastic agent DOX (40 mg/kg), AO+DOX, AN+DOX and solvent controls was used of negative control (corn oil and nanoemulsion surfactant). AO and AN were administered for 14 consecutive days orally by gavage and on the 13th day, applied DOX by intraperitoneal route (i.p.), in order to evaluate the protective potential of andiroba. The animals were euthanized on the 15th day. Hematological, biochemical, histological, and immunohistochemical parameters were analyzed. Andiroba reduced several aspects of the severity of lesions caused by DOX, decreasing hematotoxicity and the severity of histological changes in the liver and kidneys, and reducing the frequency of apoptotic cell death. In many cases, AN showed greater efficacy than AO alone, reflecting the feasibility of using this nanotechnology to improve the pharmacokinetics of lipid compounds in the body. The study sheds new light on the therapeutic benefits of andiroba and suggests new ways for investigating how the quantity and quality of lipid compounds affect exposed organisms.

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