Author:
Mulindwa Julius,Kimuda Magambo Phillip,Noyes Harry,Ilboudo Hamidou,Koffi Mathurin,Ahouty Bernadin,Nyangiri Oscar,Cooper Anneli,Clucas Caroline,Nambala Peter,Musaya Janelisa,Ngoyi Dieudonne ́ Mumba,Karume Kevin,Fataki Olivier,Simo Gustave,Ofon Elvis,Enyaru John,Nerima Barbara,Tait Andy,Marcello Lucio,Chisi John,Kabore Jacques,Kabore Justin Windingoudi,Kamoto Kelita,Simuunza Martin,Alibu Vincent P.,Jamonneau Vincent,Camera Marianne,Camara Mamadou,Bucheton Bruno,Hertz-Fowler Christiane,Macleod Annette,Matovu Enock,
Abstract
AbstractTrypanosoma brucei gambienseandTrypanosoma brucei rhodesiensecause human African trypanosomiasis (HAT), a neglected tropical disease that constitutes an important public health issue in sub-Saharan Africa. In the absence of a vaccine, only chemotherapy and vector control has been used to combat the disease. Environmental factors, such as exposure to infected tsetse files, and genetic factors such as variants in theAPOL1gene have been shown to contribute to the risk of developing HAT. However, the known factors only explain a small part of the risk of developing trypanosomiasis. We have undertaken a genome wide association study (GWAS) using 3813 samples fromT. b. gambienseandT.b. rhodesienseHAT foci in Guinea, Côte d’Ivoire, Cameroon, DRC, Malawi and Uganda. 2141 samples were genotyped on the H3Africa SNP chip followed by a genotyping a validation cohort of an additional 1,627 samples at candidate loci. After the primary and validation studies we identified a novel locus nearSMOC2with genome-wide significance. We also identified suggestive associations nearNXN, NTNG1andNCKAP5that have stronger associations with disease susceptibility than theAPOL1loci that has been previously identified by hypothesis driven approaches. These genes offer new entry points for future studies of the underlying genetic mechanisms of HAT.
Publisher
Cold Spring Harbor Laboratory