Analysis of phosphofructokinase and pyruvate kinase of leishmania, potential targets for new drugs

Obiettivo

The protozoan parasite Leishmania is responsible for several serious diseases of mankind, in tropical and subtropical areas of the world. The currently available drugs are not satisfactory. The aim of the proposed project is to contribute to the development of new drugs against these diseases, by a rational approach. Enzymes that play a key role in the metabolism of the parasite will be selected as targets for new drugs. The enzymes of the parasite will be studied in very great detail, to search for structural and kinetic differences with the enzymes of the mammalian host. Selective inhibitors will be designed that exploit these differences.
Glycolytic enzymes were chosen as targets for drugs to be designed, because glycolysis plays an essential role in the energy and carbohydrate metabolism of Leishmania. Phosphofructokinase (PFK) and pyruvate kinase (PK), key enzymes of the glycolytic pathway, are promising candidates for selective inhibition, because the parasite's enzymes have some unique structural and regulatory properties. It is, therefore, proposed to perform a thorough analysis of these two enzymes from Leishmania mexicana. The genes have already been cloned and are currently being characterized. The proteins will be overexpressed in E.coli and be used for kinetic studies. The primary structure of Leishmania PFK and PK will be modelled into a three-dimensional structure, using the available crystal structure of homologous proteins. Detailed information about enzyme-ligand interactions will be obtained by combining the results of the kinetic analysis, binding assays and molecular modelling. From this information hypotheses will be made as to how unique (sub)domains in the Leishmania proteins could be involved in specific kinetic features. The hypotheses will be tested by site-directed mutagenesis and subsequent analysis of the mutated proteins. Those domains conferring unique kinetic features to the proteins will be used for designing selective inhibitors that could be used as lead compounds for the development of chemotherapeutic agents. In parallel with the above described studies, we shall use the bacterially-overproduced PFK and PK in crystallization trials. If good crystals can be obtained, they will provide us with the most accurate information about the three-dimensional structures of the enzymes.

Campo scientifico (EuroSciVoc)

CORDIS classifica i progetti con EuroSciVoc, una tassonomia multilingue dei campi scientifici, attraverso un processo semi-automatico basato su tecniche NLP. Cfr.: Il Vocabolario Scientifico Europeo.

• ingegneria e tecnologia ingegneria dei materiali cristalli
• scienze naturali scienze biologiche biochimica biomolecole carboidrati
• scienze naturali scienze biologiche biochimica biomolecole proteine enzimi

Programma(i)

Programmi di finanziamento pluriennali che definiscono le priorità dell’UE in materia di ricerca e innovazione.

• FP3-STD 3 - Specific research and technological development programme (EEC) in the field of the life sciences and technologies for developing countries, 1990-1994

Argomento(i)

Gli inviti a presentare proposte sono suddivisi per argomenti. Un argomento definisce un’area o un tema specifico per il quale i candidati possono presentare proposte. La descrizione di un argomento comprende il suo ambito specifico e l’impatto previsto del progetto finanziato.

Invito a presentare proposte

Procedura per invitare i candidati a presentare proposte di progetti, con l’obiettivo di ricevere finanziamenti dall’UE.

Meccanismo di finanziamento

Meccanismo di finanziamento (o «Tipo di azione») all’interno di un programma con caratteristiche comuni. Specifica: l’ambito di ciò che viene finanziato; il tasso di rimborso; i criteri di valutazione specifici per qualificarsi per il finanziamento; l’uso di forme semplificate di costi come gli importi forfettari.

CSC - Cost-sharing contracts

Coordinatore

Partecipanti (2)