Data from: A chromosome 5q31.1 locus associates with tuberculin skin test reactivity in HIV-positive individuals from tuberculosis hyper-endemic regions in east Africa
One in three people has been infected with Mycobacterium tuberculosis (MTB), and the risk for MTB infection in HIV-infected individuals is even higher. We hypothesized that HIV-positive individuals living in tuberculosis-endemic regions who do not get infected by Mycobacterium tuberculosis are genet...
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Zusammenfassung: | One in three people has been infected with Mycobacterium tuberculosis
(MTB), and the risk for MTB infection in HIV-infected individuals is even
higher. We hypothesized that HIV-positive individuals living in
tuberculosis-endemic regions who do not get infected by Mycobacterium
tuberculosis are genetically resistant. Using an "experiment of
nature" design that proved successful in our previous work, we
performed a genome-wide association study of tuberculin skin test
positivity using 469 HIV-positive patients from prospective study cohorts
of tuberculosis from Tanzania and Uganda to identify genetic loci
associated with MTB infection in the context of HIV-infection. Among these
individuals, 244 tested were tuberculin skin test (TST) positive either at
enrollment or during the >8 year follow up, while 225 were not. We
identified a genome-wide significant association between the dominant
model of rs877356 and binary TST status in the combined cohort (OR=0.2671,
p=1.22x10-8). Association was replicated with similar significance when
examining TST induration as a continuous trait. The variant lies in the
5q31.1 region, 57kb downstream from IL9. Two-locus analyses of association
of variants near rs877356 showed a haplotype comprised of rs877356 and an
IL9 missense variant rs2069885 had the most significant association
(p=1.59x10-12). We also replicated previously linked loci on chromosomes
2, 5, and 11. IL9 is a cytokine produced by mast cells and T¬H2 cells
during inflammatory responses, providing a possible link between airway
inflammation and protection from MTB infection. Our results indicate that
studying uninfected participants with extensive exposure increases the
power to detect associations in complex infectious disease. |
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DOI: | 10.5061/dryad.cq183 |