Antitumor effects of citrinin in an animal model of Sarcoma 180 via cytogenetic mechanisms

Author:

Filho José Williams Gomes de Oliveira,Dos Santos Andrade Teresinha de Jesus Aguiar,De Lima Rosália Maria Tí´rres,Dos Reis Antonielly Campinho,Hameed Aneela,Santos José Victor de Oliveira,Afzal Muhammad Inam,De Menezes Ag-Anne Pereira Melo,De Alencar Marcus Viní­cius Oliveira Barros,Silva Dulce Helena Siqueira,Dias Ana Carolina Soares,Ferreira José Roberto de Oliveira,Islam Muhammad Torequl,Ferreira Paulo Michel Pinheiro,Salehi Bahare,Qamar Muhammad,Umer Muhammad,Imran Muhammad,Sharifi-Rad Javad,Martins Natália,De Castro e Sousa Joào Marcelo,Melo Cavalcante Ana Amélia de Carvalho

Abstract

Citrinin (CIT) is a cytotoxic, hepatotoxic, nephrotoxic and cardiotoxic metabolite obtained from Penicillium citrinum, that has been increasingly searched as an anticancer drug candidate. In this study, we assessed the antitumor effects of citrinin, using cytogenetic biomarkers for genotoxicity in Sarcoma 180 (S-180) ascitic fluid cells of mice. Citrinin, extracted from P. citrinum acetonitrile extract, was characterized by LC-MS. Cytotoxic assessment was done through using comet (alkaline version) and micronucleus assays. In S-180 cells, CI50 of CIT was 3.77 μg/mL, while at 12.5 and 100 μg/mL, CIT was as cytotoxic as doxorubicin (2 μg/mL). At 0.5, 1.0 and 2.0 μg/mL, it induced genotoxicity and mutagenicity in S-180 cells, especially at 2 μg/mL, triggering oxidative damage similar to hydrogen peroxide (10 mM). The antitumor effects were evidenced by a marked increase in S-180 cells apoptosis and necrosis due to clastogenic and/or aneugenic cytogenetic effects (micronucleus formation), as well as by induction of nucleoplasm bridges and nuclear buds, culminating in S-180 apoptosis and necrosis. CIT has potential as drug candidate for antitumor purposesbyinvolving cytogenetic mechanisms.

Publisher

CMB Association

Subject

General Medicine

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