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Two approaches to discovering and developing new drugs for Chagas disease
McKerrow, J. H; Doyle, P. S; Engel, J. C; Podust, L. M; Robertson, S. A; Ferreira, R; Saxton, T; Arkin, M; Kerr, I. D; Brinen, L. S; Craik, C. S.
  • McKerrow, J. H; University of California. Sandler Center at Mission Bay. San Francisco. US
  • Doyle, P. S; University of California. Sandler Center at Mission Bay. San Francisco. US
  • Engel, J. C; University of California. Sandler Center at Mission Bay. San Francisco. US
  • Podust, L. M; University of California. Sandler Center at Mission Bay. San Francisco. US
  • Robertson, S. A; University of California. Sandler Center at Mission Bay. San Francisco. US
  • Ferreira, R; University of California. Sandler Center at Mission Bay. San Francisco. US
  • Saxton, T; University of California. Sandler Center at Mission Bay. San Francisco. US
  • Arkin, M; University of California. Sandler Center at Mission Bay. San Francisco. US
  • Kerr, I. D; University of California. Sandler Center at Mission Bay. San Francisco. US
  • Brinen, L. S; University of California. Sandler Center at Mission Bay. San Francisco. US
  • Craik, C. S; University of California. Sandler Center at Mission Bay. San Francisco. US
Mem. Inst. Oswaldo Cruz ; 104(supl.1): 263-269, July 2009. tab
Artículo en Inglés | LILACS | ID: lil-520888
ABSTRACT
This review will focus on two general approaches carried out at the Sandler Center, University of California, San Francisco, to address the challenge of developing new drugs for the treatment of Chagas disease. The first approach is target-based drug discovery, and two specific targets, cytochrome P450 CYP51 and cruzain (aka cruzipain), are discussed. A "proof of concept" molecule, the vinyl sulfone inhibitor K777, is now a clinical candidate. The preclinical assessment compliance for filing as an Investigational New Drug with the United States Food and Drug Administration (FDA) is presented, and an outline of potential clinical trials is given. The second approach to identifying new drug leads is parasite phenotypic screens in culture. The development of an assay allowing high throughput screening of Trypanosoma cruzi amastigotes in skeletal muscle cells is presented. This screen has the advantage of not requiring specific strains of parasites, so it could be used with field isolates, drug resistant strains or laboratory strains. It is optimized for robotic liquid handling and has been validated through a screen of a library of FDA-approved drugs identifying 65 hits.
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Texto completo: Disponible Índice: LILACS (Américas) Asunto principal: Tripanocidas / Compuestos de Vinilo / Diseño de Fármacos / Inhibidores de Cisteína Proteinasa / Enfermedad de Chagas / Dipéptidos Límite: Animales / Humanos País/Región como asunto: America del Norte Idioma: Inglés Revista: Mem. Inst. Oswaldo Cruz Asunto de la revista: Medicina Tropical / Parasitología Año: 2009 Tipo del documento: Artículo / Documento de proyecto País de afiliación: Estados Unidos Institución/País de afiliación: University of California/US

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Texto completo: Disponible Índice: LILACS (Américas) Asunto principal: Tripanocidas / Compuestos de Vinilo / Diseño de Fármacos / Inhibidores de Cisteína Proteinasa / Enfermedad de Chagas / Dipéptidos Límite: Animales / Humanos País/Región como asunto: America del Norte Idioma: Inglés Revista: Mem. Inst. Oswaldo Cruz Asunto de la revista: Medicina Tropical / Parasitología Año: 2009 Tipo del documento: Artículo / Documento de proyecto País de afiliación: Estados Unidos Institución/País de afiliación: University of California/US