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Investigation of the cytotoxicity, genotoxicity and antioxidant prospects of JM-20 on human blood cells: A multi-target compound with potential therapeutic applications.
Silva, Fernanda D'Avila da; Galiciolli, Maria Eduarda de Andrade; Irioda, Ana Carolina; Oliveira, Cláudia Sirlene; Piccoli, Bruna Candia; Prestes, Alessandro de Souza; Borin, Bruna Cogo; Schuch, Andre Passaglia; Ochoa-Rodríguez, Estael; Nuñez-Figueredo, Yanier; Rocha, João Batista Teixeira da.
Affiliation
  • Silva FDD; Programa de Pós-graduação em Ciências Biológicas: Bioquímica Toxicológica, Universidade Federal de Santa Maria, 97105-900 Santa Maria, RS, Brazil.
  • Galiciolli MEA; Programa de Pós-Graduação Stricto Sensu em Biotecnologia Aplicada a Saúde da Criança e do Adolescente, Instituto de Pesquisa Pelé Pequeno Príncipe, Rua Silva Jardim, 1632 Curitiba, Paraná, Brazil; Faculdade Pequeno Príncipe, Avenida Iguaçu, 333 Curitiba, Paraná, Brazil.
  • Irioda AC; Programa de Pós-Graduação Stricto Sensu em Biotecnologia Aplicada a Saúde da Criança e do Adolescente, Instituto de Pesquisa Pelé Pequeno Príncipe, Rua Silva Jardim, 1632 Curitiba, Paraná, Brazil; Faculdade Pequeno Príncipe, Avenida Iguaçu, 333 Curitiba, Paraná, Brazil.
  • Oliveira CS; Programa de Pós-graduação em Ciências Biológicas: Bioquímica Toxicológica, Universidade Federal de Santa Maria, 97105-900 Santa Maria, RS, Brazil; Programa de Pós-Graduação Stricto Sensu em Biotecnologia Aplicada a Saúde da Criança e do Adolescente, Instituto de Pesquisa Pelé Pequeno Príncipe, Rua S
  • Piccoli BC; Programa de Pós-graduação em Ciências Biológicas: Bioquímica Toxicológica, Universidade Federal de Santa Maria, 97105-900 Santa Maria, RS, Brazil.
  • Prestes AS; Programa de Pós-graduação em Ciências Biológicas: Bioquímica Toxicológica, Universidade Federal de Santa Maria, 97105-900 Santa Maria, RS, Brazil.
  • Borin BC; Programa de Pós-graduação em Ciências Biológicas: Bioquímica Toxicológica, Universidade Federal de Santa Maria, 97105-900 Santa Maria, RS, Brazil.
  • Schuch AP; Programa de Pós-graduação em Ciências Biológicas: Bioquímica Toxicológica, Universidade Federal de Santa Maria, 97105-900 Santa Maria, RS, Brazil.
  • Ochoa-Rodríguez E; Centro de Investigación y Desarrollo de Medicamentos, Ave 26, N° 1605,e /Boyeros y Puentes Grandes, CP10600 La Habana, Cuba.
  • Nuñez-Figueredo Y; Centro de Investigación y Desarrollo de Medicamentos, Ave 26, N° 1605,e /Boyeros y Puentes Grandes, CP10600 La Habana, Cuba.
  • Rocha JBTD; Programa de Pós-graduação em Ciências Biológicas: Bioquímica Toxicológica, Universidade Federal de Santa Maria, 97105-900 Santa Maria, RS, Brazil. Electronic address: jbtrocha@yahoo.com.br.
Blood Cells Mol Dis ; 106: 102827, 2024 May.
Article in En | MEDLINE | ID: mdl-38301450
ABSTRACT
JM-20 is a 1,5-benzodiazepine compound fused to a dihydropyridine fraction with different pharmacological properties. However, its potential toxic effects on blood cells have not yet been reported. Thus, the present study aimed to investigate, for the first time, the possible cytotoxicity of JM-20 through cell viability, cell cycle, morphology changes, reactive species (RS) to DCFH-DA, and lipid peroxidation in human leukocytes, its hemolytic effect on human erythrocytes, and its potential DNA genotoxicity using plasmid DNA in vitro. Furthermore, the compound's ability to reduce the DPPH radical was also measured. Human blood was obtained from healthy volunteers (30 ± 10 years old), and the leukocytes or erythrocytes were immediately isolated and treated with different concentrations of JM-20. A cytoprotective effect was exhibited by 10 µM JM-20 against 1 mM tert-butyl hydroperoxide (t-but-OOH) in the leukocytes. However, the highest tested concentrations of the compound (20 and 50 µM) changed the morphology and caused a significant decrease in the cell viability of leukocytes (p < 0.05, in comparison with Control). All tested concentrations of JM-20 also resulted in a significant increase in intracellular RS as measured by DCFH-DA in these cells (p < 0.05, in comparison with Control). On the other hand, the results point out a potent antioxidant effect of JM-20, which was similar to the classical antioxidant α-tocopherol. The IC50 value of JM-20 against the lipid peroxidation induced by (FeII) was 1.051 µM ± 0.21, while the IC50 value of α-tocopherol in this parameter was 1.065 µM ± 0.34. Additionally, 50 and 100 µM JM-20 reduced the DPPH radical in a statistically similar way to the 100 µM α-tocopherol (p < 0.05, in comparison with the control). No significant hemolysis in erythrocytes, no cell cycle changes in leukocytes, and no genotoxic effects in plasmid DNA were induced by JM-20 at any tested concentration. The in silico pharmacokinetic and toxicological properties of JM-20, derivatives, and nifedipine were also studied. Here, our findings demonstrate that JM-20 and its putative metabolites exhibit similar characteristics to nifedipine, and the in vitro and in silico data support the low toxicity of JM-20 to mammals.
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Full text: 1 Collection: 01-internacional Database: MEDLINE Main subject: Alpha-Tocopherol / Fluoresceins / Antioxidants Limits: Adult / Animals / Humans Language: En Journal: Blood Cells Mol Dis Journal subject: HEMATOLOGIA Year: 2024 Document type: Article Affiliation country: Brasil Country of publication: Estados Unidos

Full text: 1 Collection: 01-internacional Database: MEDLINE Main subject: Alpha-Tocopherol / Fluoresceins / Antioxidants Limits: Adult / Animals / Humans Language: En Journal: Blood Cells Mol Dis Journal subject: HEMATOLOGIA Year: 2024 Document type: Article Affiliation country: Brasil Country of publication: Estados Unidos