Genotoxic and Mutagenic Assessment of PT-31, a Molecule with Antipsychotic Potential

Author:

Bigolin Cassiana1,Veiverberg Andriele1,Prado Rodrigues Gabriela Zimmermann1ORCID,Hilario Garcia Ana Letícia2,Machado Kayser Juliana1ORCID,Bertoldi Fernando1,Dutra Arbo Marcelo3ORCID,Galdino Pitta Marina4ORCID,da Rocha Pitta Ivan4,Gehlen Günther1ORCID,Heemann Betti Andresa1ORCID

Affiliation:

1. Institute of Health Sciences, Feevale University, Novo Hamburgo, Rio Grande do Sul, Brazil

2. Department of Cellular and Molecular Biology Applied to Health, Universidade Luterana do Brasil, ULBRA, Rio Grande do Sul, Brazil

3. Federal University of Rio Grande do Sul, Porto Alegre, Rio Grande do Sul, Brazil

4. Research Centre for Therapeutic Innovation, Federal University of Pernambuco, Recife, Pernambuco, Brazil

Abstract

Abstract: The PT-31 molecule, a potential antipsychotic, has demonstrated promising results when orally administrated to in vivo models. A recent study suggested the genotoxic and mutagenic po-tential of PT-31 after acute treatment by intraperitoneal route. This study aimed to evaluate PT-31 potential of inducing genotoxic or mutagenic damage after acute oral administration. For that, adult males and females Balb/C mice were treated acutely by oral administration with vehicle or PT-31 in three different doses (10, 20, and 40 mg kg-1). After 24 hours from PT-31 administration, animals were euthanized for performing the comet and micronucleus assays. None of the tested groups of PT-31 presented a significant increase in damage index and MN frequency. However, they presen-ted the following tendency on damage index: females presented a tendency at 40 mg kg-1 and males at 20 mg kg-1. Regarding the MN assay, male mice at the highest dose of 40 mg kg-1 presented a tendency of increased MN frequency. Also, there was a significant increase in PCE/NCE ratio in male mice. Results suggest that the male mice group presented higher susceptibility to damage. The tendency of increased damage to DNA and MN frequency suggests that the molecule PT-31 may induce reparable damage to DNA, and these DNA strand repairs may have originated from the MN. However, significant genotoxic and mutagenic effects were not observed. This study reinforces the atypical profile of the molecule as much as its safety by oral route administration.

Publisher

Bentham Science Publishers Ltd.

Subject

General Earth and Planetary Sciences,General Environmental Science

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