HIV-1 RNA Dysregulates the natural TLR response to subclinical endotoxemia in Kenyan female sex-workers
Date
2009Author
Lester, Richard T.
Yao, Xiao-Dan
Ball, T. Blake
McKinnon, Lyle R.
Omange, Were R.
Kaul, Rupert
Wachihi, Charles
Jaoko Walter G.
Rosenthal, Kenneth L.
Plummer, Francis A.
Type
ArticleLanguage
enMetadata
Show full item recordAbstract
Subclinical endotoxemia has been reported in HIV-1 infected persons and may drive systemic immune
activation and pathogenesis. Proinflammatory responsiveness to endotoxin (LPS) is mediated by Toll-like receptor 4 (TLR4).
We therefore examined the association between plasma LPS levels, HIV RNA, and TLR4 expression and cytokine responses in
the blood of HIV infected and uninfected participants in a cohort of female sex-workers in Kenya.
Methodology/Principal Findings: Ex vivo plasma and peripheral blood mononuclear cells (PBMC) were assessed for LPS
and TLR mRNA, respectively. The effects of HIV single stranded RNA, a TLR8 ligand, on TLR4 and LPS signaling were further
assessed in short term PBMC culture. Both HIV uninfected and infected subjects frequently had low detectable LPS levels in
their plasmas. Significantly increased LPS levels were associated with chronic HIV-1 infection, both treated and untreated,
but not with other acute or semi-chronic conditions reported. In HIV-uninfected subjects, TLR4 mRNA expression levels
correlated inversely with plasma LPS levels, suggesting chronic endotoxin ‘tolerance’ in vivo. A similar effect of reduced
TLR4 mRNA was seen in short term PBMC culture after stimulation with LPS. Interestingly, the apparent in vivo tolerance
effect was diminished in subjects with HIV infection. Additionally, pre-stimulation of PBMC with LPS lead to proinflammatory
(TNF-a) tolerance to subsequent LPS stimulation; however, pre-treatment of PBMC with HIV single-stranded RNA40, could
enhance TLR4-mediated LPS responsiveness in vitro.
Conclusions/Significance: Thus, dysregulation of endotoxin tolerance by HIV-1 RNA may exacerbate HIV chronic immune
activation and pathogenesis.
URI
http://www.ncbi.nlm.nih.gov/pubmed/19461969http://erepository.uonbi.ac.ke:8080/xmlui/handle/123456789/10079
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2680984/
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- Faculty of Health Sciences (FHS) [10377]