Rapid diagnostic tests (RDTs) have transformed malaria diagnosis. The most prevalent P. falciparum RDTs detect histidine-rich protein 2 (PfHRP2). However, pfhrp2 gene deletions yielding false-negative RDTs, first reported in South America in 2010, have been confirmed in Africa and Asia. We developed a mathematical model to explore the potential for RDT-led diagnosis to drive selection of pfhrp2 -deleted parasites. Low malaria prevalence and high frequencies of people seeking treatment resulted in the greatest selection pressure. Calibrating our model against confirmed pfhrp2 -deletions in the Democratic Republic of Congo, we estimate a starting frequency of 6% pfhrp2 -deletion prior to RDT introduction. Furthermore, the patterns observed necessitate a degree of selection driven by the introduction of PfHRP2-based RDT-guided treatment. Combining this with parasite prevalence and treatment coverage estimates, we map the model-predicted spread of pfhrp2 -deletion, and identify the geographic regions in which surveillance for pfhrp2 -deletion should be prioritised. eLife digest Since the turn of the millennium, a large increase in international funding has helped to reduce the public health impact of malaria. The introduction of rapid diagnostic tests has played a central role in these efforts, particularly in remote areas that are heavily affected by the disease. These tests analyse human blood samples for specific proteins that are produced by malaria parasites. The most common rapid diagnostic tests for malaria detect a protein called HRP2, which is produced by the deadliest malaria parasite, Plasmodium falciparum . Recently, however, cases have emerged where the tests have failed to detect these malaria infections. The first occurred in South America, and were found to be because some malaria parasites no longer possessed the gene that produces HRP2. Since then, malaria parasites that lack this gene have been found in several locations in Africa. This raises the question of whether using the tests favours the survival and spread of parasites that cannot produce the HRP2 protein. Using mathematical modelling techniques, Watson et al. now present evidence that suggests that the use of HRP2-detecting rapid diagnostic tests over the past 10 years could have favoured the evolution of malaria parasites that lack this protein. Furthermore, the models suggest that the conditions that are most likely to cause such selection are places where malaria infections are not common but people seek treatment at high rates. Using this information, Watson et al. created a map of 160 locations in Africa most at risk of rapid diagnostic test-driven selection against the gene that produces HRP2. Public health authorities could use these maps to determine where they should more closely monitor malaria parasites to see if they lack this gene. Future genetic investigations will be required in the high-risk areas to confirm and refine the predictions. The development of rapid diagnostic tests that detect other malaria proteins will also be essential if malaria parasites that lack HRP2 continue to spread.
【저자키워드】 Rapid diagnostic tests, Mathematical modelling, P. falciparum, mapping, pfhrp2-deletion,