Oxindole-Based Compounds Are Selective Inhibitors of Plasmodium f alciparum Cyclin Dependent Protein Kinases

Artigo Revisado por pares

Oxindole-Based Compounds Are Selective Inhibitors of Plasmodium f alciparum Cyclin Dependent Protein Kinases

2003; American Chemical Society; Volume: 46; Issue: 18 Linguagem: Inglês

10.1021/jm0300983

ISSN

1520-4804

Autores

Cassandra L. Woodard, Zhiyu Li, April K. Kathcart, James R. Terrell, Lucia Gerena, Miriam Lopez-Sanchez, Dennis E. Kyle, Apurba K. Bhattacharjee, Daniel A. Nichols, William Y. Ellis, Sean T. Prigge, Jeanne A. Geyer, Norman C. Waters,

Tópico(s)

HIV/AIDS drug development and treatment

Resumo

Cyclin dependent protein kinases (CDKs) have become attractive drug targets in an effort to identify effective inhibitors of the parasite Plasmodium falciparum, the causative agent of the most severe form of human malaria. We tested known CDK inhibitors for their ability to inhibit two malarial CDKs: Pfmrk and PfPK5. Many broad spectrum CDK inhibitors failed to inhibit Pfmrk suggesting that the active site differs from other CDKs in important ways. By screening compounds in the Walter Reed chemical database, we identified oxindole-based compounds as effective inhibitors of Pfmrk (IC(50) = 1.5 microM). These compounds have low cross-reactivity against PfPK5 and human CDK1 demonstrating selectivity for Pfmrk. Amino acid comparison of the active sites of Pfmrk and PfPK5 identified unique amino acid differences that may explain this selectivity and be exploited for further drug development efforts.

Ver no editor

Altmetric

PlumX

Entrar

Lembrar minha senha

Receber meu e-mail de confirmação

Oxindole-Based Compounds Are Selective Inhibitors of Plasmodium f alciparum Cyclin Dependent Protein Kinases