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Título: Discovery of Entamoeba histolytica hexokinase 1 inhibitors through homology modeling and virtual screening
Autor(es): SAUCEDO MENDIOLA, MARIA LETICIA
SALAS PACHECO, JOSE MANUEL
NAJERA PEÑA, HUGO
ROJO DOMINGUEZ, ARTURO
YEPEZ MULIA, LILIAN
AVITIA DOMINGUEZ, CLAUDIA ISELA
TELLEZ VALENCIA, ALFREDO
Temas: Entamoeba histolytica - Investigaciones
Homología (Biología)
Detección de microorganismo
Fecha: 2014
Editorial: United Kingdom : Taylos & Francis
Citation: Journal of Enzyme Inhibition and Medicinal Chemistry, vol. 29, núm. 3, mar, 2014
Resumen: Entamoeba histolytica, the parasite which causes amebiasis is responsible for 110 000 deaths a year. Entamoeba histolytica depends on glycolysis to obtain ATP for cellular work. According to metabolic flux studies, hexokinase exerts the highest flux control of this metabolic pathway; therefore, it is an excellent target in the search of new antiamebic drugs. To this end, a tridimensional model of E. histolytica hexokinase 1 (EhHK1) was constructed and validated by homology modeling. After virtual screening of 14 400 small molecules, the 100 with the best docking scores were selected, purchased and assessed in their inhibitory capacity. The results showed that three molecules (compounds 2921, 11275 and 2755) inhibited EhHK1 with an I50 of 48, 91 and 96 mM, respectively. Thus, we found the first inhibitors of EhHK1 that can be used in the search of new chemotherapeutic agents against amebiasis.
URI: http://ilitia.cua.uam.mx:8080/jspui/handle/123456789/609
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