A complexPlasmodium falciparumcryptotype circulating at low frequency across the African continent

Author:

Miotto OlivoORCID,Amambua-Ngwa Alfred,Amenga-Etego Lucas,Abdel Hamid Muzamil M,Adam Ishag,Aninagyei Enoch,Apinjoh Tobias,Awandare Gordon A,Bejon Philip,Bertin Gwladys I,Bouyou-Akotet Marielle,Claessens Antoine,Conway David JORCID,D’Alessandro Umberto,Diakite Mahamadou,Djimdé AbdoulayeORCID,Dondorp Arjen M,Duffy Patrick,Fairhurst Rick M,Fanello Caterina I,Ghansah Anita,Ishengoma Deus,Lawniczak Mara,Maïga-Ascofaré Oumou,Auburn SarahORCID,Rosanas-Urgell Anna,Wasakul Varanya,White Nina FD,Almagro-Garcia Jacob,Pearson Richard D,Goncalves Sonia,Ariani Cristina,Bozdech Zbynek,Hamilton WilliamORCID,Simpson Victoria,Kwiatkowski Dominic P

Abstract

ABSTRACTThe population structure of the malaria parasitePlasmodium falciparumcan reveal underlying demographic and adaptive evolutionary processes. Here, we analyse population structure in 4,376P. falciparumgenomes from 21 countries across Africa. We identified a strongly differentiated cluster of parasites, comprising ∼1.2% of samples analysed, geographically distributed over 13 countries across the continent. Members of this cluster, named AF1, carry a genetic background consisting of a large number of highly differentiated variants, rarely observed outside this cluster, at a multitude of genomic loci distributed across most chromosomes. At these loci, the AF1 haplotypes appear to have common ancestry, irrespective of the sampling location; outside the shared loci, however, AF1 members are genetically similar to their sympatric parasites. AF1 parasites sharing up to 23 genomic co-inherited regions were found in all major regions of Africa, at locations over 7,000 km apart. We coined the termcryptotypeto describe a complex common background which is geographically widespread, but concealed by genomic regions of local origin. Most AF1 differentiated variants are functionally related, comprising structural variations and single nucleotide polymorphisms in components of the MSP1 complex and several other genes involved in interactions with red blood cells, including invasion and erythrocyte antigen export. We propose that AF1 parasites have adapted to some as yet unidentified evolutionary niche, by acquiring a complex compendium of interacting variants that rarely circulate separately in Africa. As the cryptotype spread across the continent, it appears to have been maintained mostly intact in spite of recombination events, suggesting a selective advantage. It is possible that other cryptotypes circulate in Africa, and new analysis methods may be needed to identify them.

Publisher

Cold Spring Harbor Laboratory

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