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. 2018 Jul 17;32(11):1389-1401.
doi: 10.1097/QAD.0000000000001824.

Monotypic low-level HIV viremias during antiretroviral therapy are associated with disproportionate production of X4 virions and systemic immune activation

Marta E Bull  1   2 Caroline Mitchell  3 Jaime Soria  4 Sheila Styrchak  2 Corey Williams-Wietzikoski  2 Jillian Legard  2 Jennifer McKernan-Mullin  2 Kelli Kraft  2 Frankline Onchiri  2 Joshua Stern  5 Sarah Holte  5   6 Kevin J Ryan  7 Edward P Acosta  7 Alberto La Rosa  8 Robert W Coombs  9   10 Eduardo Ticona  4   11 Lisa M Frenkel  1   2   10
Affiliations

Monotypic low-level HIV viremias during antiretroviral therapy are associated with disproportionate production of X4 virions and systemic immune activation

Marta E Bull et al. AIDS. .

Abstract

Objective: During effective antiretroviral therapy (ART), low-level plasma viremias (LLV) (HIV RNA >30-1000 copies/ml) can be detected intermittently. We hypothesized that systemic inflammation is associated with LLV either as the cause or result of the production of virions from clonally expanded cells.

Methods: Prospective cohort study of HIV-infected ART-naive Peruvians enrolled prior to ART and followed for 2 years. Plasma HIV RNA and peripheral blood mononuclear cell (PBMC) HIV DNA concentrations were quantified pre-ART from individuals whose plasma HIV RNA was ART-suppressed. Inflammatory biomarker concentrations were measured pre and during ART. Single-genome amplification (SGA) derived HIV env and pol genotypes from pre-ART and LLV specimens. Antiretroviral levels during ART assessed adherence. Statistical associations and phylogenetic relationships were examined.

Results: Among 82 participants with median plasma HIV RNA less than 30 copies/ml, LLV were detected in 33 of 82 (40%), with a LLV median HIV RNA of 73 copies/ml. Participants with vs. without LLV had significantly higher pre-ART plasma HIV RNA (P < 0.001) and PBMC HIV DNA (P < 0.007); but, during ART, their antiretroviral drug levels were similar. LLV env sequences were monotypic in 17 of 28 (61%) and diverse in 11 of 28 (39%) participants. Those with the monotypic vs. diverse LLV pattern had elevated hsCRP and sCD163 (P = 0.004) and LLV with more X4 variants (P = 0.02).

Conclusion: In individuals with monotypic LLV sequences, higher levels of pre-ART HIV DNA and RNA, systemic inflammation and X4 viruses suggest an interaction between inflammation and the production of virions from proliferating infected cells, and that naïve T cells may be a source of LLV.

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Figures

Fig. 1
Fig. 1
Study schema of 126 HIV-infected antiretroviral therapy-naive adult participants with AIDS-defining illness or a CD4+ T-lymphocytes less than 250 cells/μl enrolled in this observational cohort study in Lima, Peru.
Fig. 2
Fig. 2
Representative phylogenetic trees, divergence, and plasma HIV RNA plots from four of 28 participants who had sequences generated from plasma low-level viremias (a–c) or viremias below the limit of quantification (d) (month specimens collected, in parenthesis).
Fig. 2 (Continued)
Fig. 2 (Continued)
Representative phylogenetic trees, divergence, and plasma HIV RNA plots from four of 28 participants who had sequences generated from plasma low-level viremias (a–c) or viremias below the limit of quantification (d) (month specimens collected, in parenthesis).
Fig. 2 (Continued)
Fig. 2 (Continued)
Representative phylogenetic trees, divergence, and plasma HIV RNA plots from four of 28 participants who had sequences generated from plasma low-level viremias (a–c) or viremias below the limit of quantification (d) (month specimens collected, in parenthesis).
Fig. 2 (Continued)
Fig. 2 (Continued)
Representative phylogenetic trees, divergence, and plasma HIV RNA plots from four of 28 participants who had sequences generated from plasma low-level viremias (a–c) or viremias below the limit of quantification (d) (month specimens collected, in parenthesis).
Fig. 3
Fig. 3
Concentrations of biomarkers of inflammation and cellular determined before and during antiretroviral therapy, including comparisons between participants with monotypic low-level viremia compared with those with diverse low-level viremia.
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References

    1. Havlir DV, Bassett R, Levitan D, Gilbert P, Tebas P, Collier AC, et al. Prevalence and predictive value of intermittent viremia with combination HIV therapy. JAMA 2001; 286:171–179. - PubMed
    1. Karlsson AC, Younger SR, Martin JN, Grossman Z, Sinclair E, Hunt PW, et al. Immunologic and virologic evolution during periods of intermittent and persistent low-level viremia. AIDS 2004; 18:981–989. - PubMed
    1. Nettles RE, Kieffer TL, Kwon P, Monie D, Han Y, Parsons T, et al. Intermittent HIV-1 viremia (Blips) and drug resistance in patients receiving HAART. JAMA 2005; 293:817–829. - PubMed
    1. Hofstra LM, Mudrikova T, Stam AJ, Otto S, Tesselaar K, Nijhuis M, et al. Residual viremia is preceding viral blips and persistent low-level viremia in treated HIV-1 patients. PLoS One 2014; 9:e110749. - PMC - PubMed
    1. Mavigner M, Delobel P, Cazabat M, Dubois M, L’Faqihi-Olive FE, Raymond S, et al. HIV-1 residual viremia correlates with persistent T-cell activation in poor immunological responders to combination antiretroviral therapy. PLoS One 2009; 4:e7658. - PMC - PubMed

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