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TOXICOLOGICAL EVALUATION AND IN SILICO PHARMACOKINETICS OF CEFTIOFUR IN HUMAN AND ENVIRONMENTAL HEALTH

Correa GV;
Rosa JFLF;
Cezário SPS;
Araujo LF;
Prates LLCM;
Nobre SAM;
Motta LF

Gabriel Veloso Correa

José Felipe Leite Ferreira Rosa

Stephanie Priscila de Sousa Cezário

Laura Faria Araujo

Ludmilla Louise Cerqueira Maia Prates

Sérgio Avelino Mota Nobre

Luiz Frederico Motta


Keywords

Antibiotic
Ceftiofur
Environmental in silico toxicology
Human in silico toxicology and human in silico pharmacokinetics

Abstract

Ceftiofur is a broad-spectrum cephalosporin, effective against Gram-positive and Gram-negative pathogens. This antibiotic works by inhibiting the synthesis of the bacterial cell wall. Antibiotics, used in both human and veterinary medicine, are drugs of concern when found in the environment. This is due to the fact that, even at low concentrations, prolonged exposure to these residues can lead to the emergence of resistant bacteria, compromising human health and environmental balance. Direct or indirect contact, whether through the food chain, water resources or animal excreta, represent the main routes of contamination. In the present study, in silico methodologies were employed  to predict the molecular properties of the antibiotic Ceftiofur. The in silico environmental toxicology study  showed that Ceftiofur is not toxic to bees, but is toxic to fish and crustaceans, and its chemical structure does not degrade in the environment. ADME in silico analysis  indicated that the antibiotic does not present a favorable prediction for oral bioavailability, due to violations of the Lipinski criteria and has a moderate intestinal absorption rate and absence of permeability across the blood-brain barrier. In addition, the in silico pharmacokinetic study  revealed that Ceftiofur has no inhibitory capacity on any of the five hepatic isoenzymes of cytochrome P450 complex (CYP450). The  human in silico toxicology study  showed promising results, demonstrating that the antibiotic is non-toxic (non-mutagenic) in the AMES test, has no carcinogenic properties, and is classified in category IV for acute oral toxicity, indicating low toxicity.

 

DOI:https://doi.org/10.56238/sevened2024.037-107


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This work is licensed under a Creative Commons Attribution-NonCommercial 4.0 International License.

Copyright (c) 2024 Gabriel Veloso Correa , José Felipe Leite Ferreira Rosa, Stephanie Priscila de Sousa Cezário, Laura Faria Araujo, Ludmilla Louise Cerqueira Maia Prates, Sérgio Avelino Mota Nobre, Luiz Frederico Motta

Author(s)

  • Gabriel Veloso Correa
  • José Felipe Leite Ferreira Rosa
  • Stephanie Priscila de Sousa Cezário
  • Laura Faria Araujo
  • Ludmilla Louise Cerqueira Maia Prates
  • Sérgio Avelino Mota Nobre
  • Luiz Frederico Motta