Use este identificador para citar ou linkar para este item: http://sgc.anlis.gob.ar/handle/123456789/1355
Título: Major Kinds of Drug Targets in Chagas Disease or American Trypanosomiasis
Autor(es): Duschak, Vilma G 
Palavras-chave: Trypanosoma cruzi;Enfermedad de Chagas;Vías Biosintéticas;Enzimas;Orgánulos
Data do documento: 22-Jul-2019
Jornal: Current drug targets 
Resumo: 
American Trypanosomiasis, a parasitic infection commonly named Chagas disease, affects millions of people all over Latin American countries. Presently, the World Health Organization (WHO) predicts that the number of international infected individuals extends to 7 to 8 million, assuming that more than 10,000 deaths occur annually. The transmission of the etiologic agent, Trypanosoma cruzi, through people migrating to non-endemic world nations makes it an emergent disease. The best promising targets for trypanocidal drugs may be classified into three main groups: Group I includes the main molecular targets that are considered among specific enzymes involved in the essential processes for parasite survival, principally Cruzipain, the major antigenic parasite cysteine proteinase. Group II involves biological pathways and their key specific enzymes, such as Sterol biosynthesis pathway, among others, specific antioxidant defense mechanisms, and bioenergetics ones. Group III includes the atypical organelles /structures present in the parasite relevant clinical forms, which are absent or considerably different from those present in mammals and biological processes related to them. These can be considered potential targets to develop drugs with extra effectiveness and fewer secondary effects than the currently used therapeutics. An improved distinction between the host and the parasite targets will help fight against this neglected disease.
Descrição: 
Fil: Duschak, Vilma G. ANLIS Dr. C. G. Malbrán. Instituto Nacional de Parasitología Dr. Mario Fatala Chaben; Argentina.
URI: http://sgc.anlis.gob.ar/handle/123456789/1355
DOI: 10.2174/1389450120666190423160804
Direitos: Closed Access
Aparece nas Coleções:Publicaciones INP

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