Last Updated: 01/09/2025

Design and synthesis of Inhibitors of PfDHODH: Towards a new treatment for malaria

Objectives

The main goal of this project is to apply structure-based drug design and synthesis to produce drug-like DHODH inhibitors as potential new antimalarial drug leads, which will then be evaluated biologically.

Principal Institution

University of Leeds, United Kingdom

Principal Investigators / Focal Persons

Rowan Katrine Taylor

Rationale and Abstract

An estimated 3.3 billion people are at risk of malaria, with populations living in sub-Saharan Africa having the highest infection rates, resulting in ~219 million documented cases of malaria and in excess of 660,000 deaths in 2010. The treatment and control of malaria is increasingly difficult due to the spread of resistance to antimalarial drugs. This is a concern even for artemisinin-based combination therapies (ACTs)- the first-line of treatment, where there is evidence of altered parasite sensitivity in a number of countries. In order to eradicate malaria it is clear that the new classes of antimalarial with novel mechanisms of action and defined pharmacological profile would be needed. It is reassuring that several potential drugs are entering clinical trials but their success or longevity is unknown, necessitating development of new inhibitors operating on novel targets. Work at Leeds and elsewhere has identified the enzyme DHODH as an attractive target for the development of new antimalarial drugs.

Themes

Basic Science
Drug Resistance
Drug-based Strategies

Date

Jul 2016 — Sep 2016

Total Project Funding

$2,701

Funding Details

Wellcome Trust, United Kingdom

Grant ID: 202071/Z/16/Z

GBP 2,000

Project Site

United Kingdom