Association between HLA Class I and Class II Alleles and the Outcome of West Nile Virus Infection: An Exploratory Study

Lanteri, Marion C; Kaidarova, Zhanna; Peterson, Trevor; Cate, Steven; Custer, Brian; Wu, Shiquan; Agapova, Maria; Law, Jacqueline P; Bielawny, Thomas; Plummer, Frank; Tobler, Leslie H; Loeb, Mark; Busch, Michael P; Bramson, Jonathan; Luo, Ma; Norris, Philip J

Association between HLA Class I and Class II Alleles and the Outcome of West Nile Virus Infection: An Exploratory Study

Marion C Lanteri, Zhanna Kaidarova, Trevor Peterson, Steven Cate, Brian Custer, Shiquan Wu, Maria Agapova, Jacqueline P Law, Thomas Bielawny, Frank Plummer, Leslie H Tobler, Mark Loeb, Michael P Busch, Jonathan Bramson, Ma Luo and Philip J Norris

PLOS ONE, 2011, vol. 6, issue 8, 1-10

Abstract: Background: West Nile virus (WNV) infection is asymptomatic in most individuals, with a minority developing symptoms ranging from WNV fever to serious neuroinvasive disease. This study investigated the impact of host HLA on the outcome of WNV disease. Methods: A cohort of 210 non-Hispanic mostly white WNV+ subjects from Canada and the U.S. were typed for HLA-A, B, C, DP, DQ, and DR. The study subjects were divided into three WNV infection outcome groups: asymptomatic (AS), symptomatic (S), and neuroinvasive disease (ND). Allele frequency distribution was compared pair-wise between the AS, S, and ND groups using χ2 and Fisher's exact tests and P values were corrected for multiple comparisons (Pc). Allele frequencies were compared between the groups and the North American population (NA) used as a control group. Logistic regression analysis was used to evaluate the potential synergistic effect of age and HLA allele phenotype on disease outcome. Results: The alleles HLA-A*68, C*08 and DQB*05 were more frequently associated with severe outcomes (ND vs. AS, PA*68 = 0.013/Pc = 0.26, PC*08 = 0.0075/Pc = 0.064, and PDQB1*05 = 0.029/Pc = 0.68), However the apparent DQB1*05 association was driven by age. The alleles HLA-B*40 and C*03 were more frequently associated with asymptomatic outcome (AS vs. S, PB*40 = 0.021/Pc = 0.58 and AS vs. ND PC*03 = 0.039/Pc = 0.64) and their frequencies were lower within WNV+ subjects with neuroinvasive disease than within the North American population (NA vs. S, PB*40 = 0.029 and NA vs. ND, PC*03 = 0.032). Conclusions: Host HLA may be associated with the outcome of WNV disease; HLA-A*68 and C*08 might function as “susceptible” alleles, whereas HLA-B*40 and C*03 might function as “protective” alleles.

Date: 2011
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Persistent link: https://EconPapers.repec.org/RePEc:plo:pone00:0022948

DOI: 10.1371/journal.pone.0022948

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