Atovaquone efficacy in treating Lumefantrine resistant Plasmodium

Malaria affects 300-500 million people annually and kills more than 1 million, with majority of the clinical cases and deaths occurring in Sub-Saharan Africa. Drug resistance against Plasmodium falciparum remains a public health problem. Resistance is the result of two processes: drug selection of resistant parasites; and the spread of resistance. Strategies to overcome this problem require full understanding of the resistance mechanisms, besides the use of combined antimalarial therapies. Resistance to an antimalarial drug may however, be selected for by another drug in which the mechanism of resistance is similar. This study sought to establish cross-resistance patterns between four antimalarial namely atovaquone (ATQ), primaquine (PMQ), lumefantrine (LM) and piperaquine (PQ) using murine malaria models. Findings shows that PQ-resistance in Plasmodium berghei is associated with a significant resistance of PMQ and a slight, though not significant reduction in ATQ efficacy. Thus, ATQ can be a potential partner to artemisinin in combination therapy in places where there is widespread resistance towards PQ.

Autorentext

July 2012-Todate PhD student in Biochemistry, University of Nairobi 2009: MSc. in Medicinal Chemistry:1. Work Experience:(i) Dec. 2012-Todate: Lecturer Kabianga University, School of Nursing and Biomedical Sciences. Teaching Biomedical Sciences.(ii) Oct. 2010-Nov. 2012: Assistant Lecturer Great Lakes University of Kisumu, Faculty of Health sc.