Toxicology International (Formerly Indian Journal of Toxicology)

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Effect of Sodium Valproate on the Toxicity of Cyclophosphamide in the Testes of Mice: Influence of Pre‑ and Post‑Treatment Schedule


Affiliations
  • National Institute of Pharmaceutical Education and Research, Department of Pharmacology and Toxicology, Facility for Risk Assessment and Intervention Studies, S.A.S. Nagar, India
     

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Recently, sodium valproate (VPA) has been proven as histone deacetylase (HDAC) inhibitor and potentiates the cytotoxicity of anticancer drugs, and also exhibit promising anti‑cancer activity. Present study aimed to investigate the influence of pre‑ and post‑treatment of VPA on cyclophosphamide (CP) induced genotoxicity and germ cell toxicity in mice. All the animals were treated with VPA at the dose of 500 mg/kg/day on alternate day thrice/week for a period of two weeks, CP at the dose of 200 mg/kg on 7th and 15th day and sacrificed 24 h after administration (i.p.) of the last dose. End point of evaluation includes sperm count, sperm head morphology, sperm comet assay and histology. VPA treatment significantly decreases CP induced sperm count, testes and epididymis weight; increased sperm head abnormality and sperm DNA damage. Both VPA pre‑ and post‑treatment augmented CP induced DNA damage and the germ cell toxicity; however, pre‑treatment induced more cytotoxicity and genotoxicity as compared to post‑treatment.

Keywords

Cyclophosphamide, DNA damage, histone deacetylase inhibitor, mice, sodium valproate
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  • Effect of Sodium Valproate on the Toxicity of Cyclophosphamide in the Testes of Mice: Influence of Pre‑ and Post‑Treatment Schedule

Abstract Views: 224  |  PDF Views: 0

Authors

S. Khan
, India
G. B. Jena
, India

Abstract


Recently, sodium valproate (VPA) has been proven as histone deacetylase (HDAC) inhibitor and potentiates the cytotoxicity of anticancer drugs, and also exhibit promising anti‑cancer activity. Present study aimed to investigate the influence of pre‑ and post‑treatment of VPA on cyclophosphamide (CP) induced genotoxicity and germ cell toxicity in mice. All the animals were treated with VPA at the dose of 500 mg/kg/day on alternate day thrice/week for a period of two weeks, CP at the dose of 200 mg/kg on 7th and 15th day and sacrificed 24 h after administration (i.p.) of the last dose. End point of evaluation includes sperm count, sperm head morphology, sperm comet assay and histology. VPA treatment significantly decreases CP induced sperm count, testes and epididymis weight; increased sperm head abnormality and sperm DNA damage. Both VPA pre‑ and post‑treatment augmented CP induced DNA damage and the germ cell toxicity; however, pre‑treatment induced more cytotoxicity and genotoxicity as compared to post‑treatment.

Keywords


Cyclophosphamide, DNA damage, histone deacetylase inhibitor, mice, sodium valproate