2011
DOI: 10.1128/jvi.01921-10
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Cell-Associated Viral Burden Provides Evidence of Ongoing Viral Replication in Aviremic HIV-2-Infected Patients

Abstract: Viremia is significantly lower in HIV-2 than in HIV-1 infection, irrespective of disease stage. Nevertheless, the comparable proviral DNA burdens observed for these two infections indicate similar numbers of infected cells. Here we investigated this apparent paradox by assessing cell-associated viral replication. We found that untreated HIV-1-positive (HIV-1 ؉ ) and HIV-2 ؉ individuals, matched for CD4 T cell depletion, exhibited similar gag mRNA levels, indicating that significant viral transcription is occur… Show more

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Cited by 45 publications
(42 citation statements)
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“…Compared to data for HIV-1-infected individuals, less data are available about the relationship between the progression toward overt disease and the presence of an IFN state in HIV-2-infected individuals at different stages of the disease. However, in marked contrast to HIV-1-infected individuals, HIV-2-infected individuals do generally display low viral loads (44)(45)(46)(47). The reasons for these differences are unknown at present.…”
Section: A Lpha and Beta Interferons (Ifn-␣ And Ifn-␤) Collectively mentioning
confidence: 85%
See 1 more Smart Citation
“…Compared to data for HIV-1-infected individuals, less data are available about the relationship between the progression toward overt disease and the presence of an IFN state in HIV-2-infected individuals at different stages of the disease. However, in marked contrast to HIV-1-infected individuals, HIV-2-infected individuals do generally display low viral loads (44)(45)(46)(47). The reasons for these differences are unknown at present.…”
Section: A Lpha and Beta Interferons (Ifn-␣ And Ifn-␤) Collectively mentioning
confidence: 85%
“…One of the major differences that exists between HIV-1 and HIV-2 infections in vivo is that while the former is characterized by high viral loads in the majority of untreated patients, a high proportion of HIV-2-infected patients present with relatively low viral loads for decades (44)(45)(46)(47). In light of the results presented here, it would be tempting to speculate that the higher susceptibility of HIV-2 to IFN-␣ is at least in part responsible for the presence of lower viral loads, while the partial resistance displayed by HIV-1 allows the virus to replicate despite the presence of chronic type I interferon responses.…”
Section: Discussionmentioning
confidence: 99%
“…In antiretroviral-treated adults, total HIV DNA in resting CD4 T cells is strongly associated with CD4 and CD8 T cell activation, whereas there is no association between cell activation and integrated DNA or IUPM coculture results (254). Cell-associated HIV RNA load, which reflects the level of viral transcription, including abortive transcription, also correlates with immune activation in untreated patients, patients on cART, and natural controllers (204,255,256,257). In patients on cART with undetectable viremia, HIV transcript loads correlate negatively with the CD4 T cell count (257) and positively with lymphoproliferative responses to HIV p24 antigen (258).…”
Section: Discussionmentioning
confidence: 99%
“…If the former is true, it is necessary to develop quantitative virological biomarkers to monitor these effects. Further studies are warranted to establish whether CA HIV-1 RNA can be used as a reliable surrogate marker of such effects, but several reports already point to a direct correlation of CA HIV RNA levels with markers of immune activation in untreated patients, natural controllers, and patients on ART [127-129]. …”
Section: Reviewmentioning
confidence: 99%