Kabore J. W., Ilboudo H., Noyes H., Camara O., Kabore J., Camara M., Koffi M., Lejon Veerle, Jamonneau Vincent, MacLeod A., Hertz-Fowler C., Marie A., Belem G., Matovu E., Bucheton Bruno, Sidibe I., Trypano G. E. N. Res Grp. (2017). Candidate gene polymorphisms study between human African trypanosomiasis clinical phenotypes in Guinea. PLOS Neglected Tropical Diseases, 11 (8), p. e0005833 [13 p.]. ISSN 1935-2735.
Titre du document
Candidate gene polymorphisms study between human African trypanosomiasis clinical phenotypes in Guinea
Année de publication
2017
Auteurs
Kabore J. W., Ilboudo H., Noyes H., Camara O., Kabore J., Camara M., Koffi M., Lejon Veerle, Jamonneau Vincent, MacLeod A., Hertz-Fowler C., Marie A., Belem G., Matovu E., Bucheton Bruno, Sidibe I., Trypano G. E. N. Res Grp
Source
PLOS Neglected Tropical Diseases, 2017,
11 (8), p. e0005833 [13 p.] ISSN 1935-2735
Background Human African trypanosomiasis (HAT), a lethal disease induced by Trypanosoma brucei gambiense, has a range of clinical outcomes in its human host in West Africa: an acute form progressing rapidly to second stage, spontaneous self-cure and individuals able to regulate parasitaemia at very low levels, have all been reported from endemic foci. In order to test if this clinical diversity is influenced by host genetic determinants, the association between candidate gene polymorphisms and HAT outcome was investigated in populations from HAT active foci in Guinea. Methodology and results Samples were collected from 425 individuals; comprising of 232 HAT cases, 79 subjects with long lasting positive and specific serology but negative parasitology and 114 endemic controls. Genotypes of 28 SNPs in eight genes passed quality control and were used for an association analysis. IL6 rs1818879 allele A (p = 0.0001, OR = 0.39, CI95 = [0.24-0.63], BONF = 0.0034) was associated with a lower risk of progressing from latent infection to active disease. MIF rs36086171 allele G seemed to be associated with an increased risk (p = 0.0239, OR = 1.65, CI95 = [1.07-2.53], BONF = 0.6697) but did not remain significant after Bonferroni correction. Similarly MIF rs12483859 C allele seems be associated with latent infections (p = 0.0077, OR = 1.86, CI95 = [1.18-2.95], BONF = 0.2157). We confirmed earlier observations that APOL1 G2 allele (DEL) (p = 0.0011, OR = 2.70, CI95 = [1.49-4.91], BONF = 0.0301) is associated with a higher risk and APOL1 G1 polymorphism (p = 0.0005, OR = 0.45, CI95 = [0.29-0.70], BONF = 0.0129) with a lower risk of developing HAT. No associations were found with other candidate genes. Conclusion Our data show that host genes are involved in modulating Trypanosoma brucei gambiense infection outcome in infected individuals from Guinea with IL6 rs1818879 being associated with a lower risk of progressing to active HAT. These results enhance our understanding of host-parasite interactions and, ultimately, may lead to the development of new control tools.
Plan de classement
Entomologie médicale / Parasitologie / Virologie [052]
Description Géographique
GUINEE
Localisation
Fonds IRD [F B010071057]
Identifiant IRD
fdi:010071057
