Code
3G017407
Duration
01 January 2007 → 30 December 2012
Funding
Research Foundation - Flanders (FWO)
Promotor
Research disciplines
-
Natural sciences
- Organic chemistry
-
Medical and health sciences
- Biomarker discovery and evaluation
- Drug discovery and development
- Medicinal products
- Pharmaceutics
- Pharmacognosy and phytochemistry
- Pharmacology
- Pharmacotherapy
- Toxicology and toxinology
- Other pharmaceutical sciences
Keywords
malaria
2C-methyl-D-erythritol 4-phophate pathway
DOXP reductoiomerase
Project description
A mevalonate independent pathway for isoprenoid biosynthesis, the so-called DOXP pathway, has been discovered recently and validated as new drug target. Fosmidomycin, a phosphonate that interferes with this pathway through inhibition of DOXP reductiosomerase, represents a promising antimalarial agent. This project aims at the development of alpha-substituted fosmidomycin analogues that are in vitro superior to fosmidomycin in inhibiting the growth of P. falciparum and other pathogens that use the non-mevalonate pathway.