| Literature DB >> 21225264 |
Paula A Abreu1, Viveca A G G da Silva, Fernanda C Santos, Helena C Castro, Cecília S Riscado, Mariana T de Souza, Camilly P Ribeiro, Juliana E Barbosa, Cláudio C C dos Santos, Carlos R Rodrigues, Viviane Lione, Bianca A M Correa, Anna C Cunha, Vitor F Ferreira, Maria C B V de Souza, Izabel C N P Paixão.
Abstract
Herpes simplex virus is an important human pathogen responsible for a range of diseases from mild uncomplicated mucocutaneous infections to life-threatening ones. Currently, the emergence of Herpes simplex virus resistant strains increased the need for more effective and less cytotoxic drugs for Herpes treatment. In this work, we synthesized a series of oxoquinoline derivatives and experimentally evaluated the antiviral activity against acyclovir resistant HSV-1 strain as well as their cytotoxity profile. The most active compound (3b), named here as Fluoroxaq-3b, showed a promising profile with a better cytotoxicity profile than acyclovir. The theoretical analysis of the structure-activity relationship of these compounds revealed some stereoelectronic properties such as lower LUMO energy and lipophilicity, besides a higher polar surface area and number of hydrogen bond acceptor groups as important parameters for the antiviral activity. Fluoroxaq-3b showed a good oral theoretical bioavailability, according to Lipinski rule of five, with a promising profile for further in vivo analysis.Entities:
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Year: 2011 PMID: 21225264 DOI: 10.1007/s00284-010-9860-6
Source DB: PubMed Journal: Curr Microbiol ISSN: 0343-8651 Impact factor: 2.188