TY - JOUR
T1 - Genomic analysis of a parasite invasion
T2 - Colonization of the Americas by the blood fluke Schistosoma mansoni
AU - Platt, Roy N.
AU - Le Clec'h, Winka
AU - Chevalier, Frédéric D.
AU - McDew-White, Marina
AU - LoVerde, Philip T.
AU - Ramiro de Assis, Rafael
AU - Oliveira, Guilherme
AU - Kinung'hi, Safari
AU - Djirmay, Amadou Garba
AU - Steinauer, Michelle L.
AU - Gouvras, Anouk
AU - Rabone, Muriel
AU - Allan, Fiona
AU - Webster, Bonnie L.
AU - Webster, Joanne P.
AU - Emery, Aidan M.
AU - Rollinson, David
AU - Anderson, Timothy J.C.
N1 - Funding Information:
Sandra Smith and John M. Heaner (Texas Biomedical Research Institute) provided computational research support. Matthew Berriman provided the most recent genome sequence and annotation prior to publication. This research was funded by the National Institute of Allergy and Infectious Diseases (NIAD R01 AI097576‐01 and NIAD 5R21AI096277‐01), Texas Biomedical Research Institute Forum (award 0467). Sample acquisition was supported by funding from the Wellcome Trust (104958/Z/14/Z) for the SCAN project, the EU grant FP6 STREP contract no. 032203 for the CONTRAST project and the Gates Foundation coordinated by the University of Georgia Research Foundation Inc. (RR374‐053/5054146 and RR374‐053/4785426) for the SCORE project. S. mansoni
Publisher Copyright:
© 2022 The Authors. Molecular Ecology published by John Wiley & Sons Ltd.
PY - 2022/4
Y1 - 2022/4
N2 - Schistosoma mansoni, a snail-borne, blood fluke that infects humans, was introduced into the Americas from Africa during the Trans-Atlantic slave trade. As this parasite shows strong specificity to the snail intermediate host, we expected that adaptation to South American Biomphalaria spp. snails would result in population bottlenecks and strong signatures of selection. We scored 475,081 single nucleotide variants in 143 S. mansoni from the Americas (Brazil, Guadeloupe and Puerto Rico) and Africa (Cameroon, Niger, Senegal, Tanzania, and Uganda), and used these data to ask: (i) Was there a population bottleneck during colonization? (ii) Can we identify signatures of selection associated with colonization? (iii) What were the source populations for colonizing parasites? We found a 2.4- to 2.9-fold reduction in diversity and much slower decay in linkage disequilibrium (LD) in parasites from East to West Africa. However, we observed similar nuclear diversity and LD in West Africa and Brazil, suggesting no strong bottlenecks and limited barriers to colonization. We identified five genome regions showing selection in the Americas, compared with three in West Africa and none in East Africa, which we speculate may reflect adaptation during colonization. Finally, we infer that unsampled populations from central African regions between Benin and Angola, with contributions from Niger, are probably the major source(s) for Brazilian S. mansoni. The absence of a bottleneck suggests that this is a rare case of a serendipitous invasion, where S. mansoni parasites were pre-adapted to the Americas and able to establish with relative ease.
AB - Schistosoma mansoni, a snail-borne, blood fluke that infects humans, was introduced into the Americas from Africa during the Trans-Atlantic slave trade. As this parasite shows strong specificity to the snail intermediate host, we expected that adaptation to South American Biomphalaria spp. snails would result in population bottlenecks and strong signatures of selection. We scored 475,081 single nucleotide variants in 143 S. mansoni from the Americas (Brazil, Guadeloupe and Puerto Rico) and Africa (Cameroon, Niger, Senegal, Tanzania, and Uganda), and used these data to ask: (i) Was there a population bottleneck during colonization? (ii) Can we identify signatures of selection associated with colonization? (iii) What were the source populations for colonizing parasites? We found a 2.4- to 2.9-fold reduction in diversity and much slower decay in linkage disequilibrium (LD) in parasites from East to West Africa. However, we observed similar nuclear diversity and LD in West Africa and Brazil, suggesting no strong bottlenecks and limited barriers to colonization. We identified five genome regions showing selection in the Americas, compared with three in West Africa and none in East Africa, which we speculate may reflect adaptation during colonization. Finally, we infer that unsampled populations from central African regions between Benin and Angola, with contributions from Niger, are probably the major source(s) for Brazilian S. mansoni. The absence of a bottleneck suggests that this is a rare case of a serendipitous invasion, where S. mansoni parasites were pre-adapted to the Americas and able to establish with relative ease.
KW - Africa
KW - Brazil
KW - codispersal
KW - exome
KW - human parasite
KW - migration
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U2 - 10.1111/mec.16395
DO - 10.1111/mec.16395
M3 - Article
C2 - 35152493
AN - SCOPUS:85125166826
SN - 0962-1083
VL - 31
SP - 2242
EP - 2263
JO - Molecular Ecology
JF - Molecular Ecology
IS - 8
ER -