Paucity of CD4+CCR5+ T cells is a typical feature of natural SIV hosts

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255

267

HIV-infected humans and SIV-infected rhesus macaques experience a rapid and dramatic loss of mucosal CD4+ T cells that is considered to be a key determinant of AIDS pathogenesis. In this study, we show that nonpathogenic SIV infection of sooty mangabeys (SMs), a natural host species for SIV, is also associated with an early, severe, and persistent depletion of memory CD4+ T cells from the intestinal and respiratory mucosa. Importantly, the kinetics of the loss of mucosal CD4+ T cells in SMs is similar to that of SIVmac239-infected rhesus macaques. Although the nonpathogenic SIV infection of SMs induces the same pattern of mucosal target cell depletion observed during pathogenic HIV/SIV infections, the depletion in SMs occurs in the context of limited local and systemic immune activation and can be reverted if virus replication is suppressed by antiretroviral treatment. These results indicate that a profound depletion of mucosal CD4+ T cells is not sufficient per se to induce loss of mucosal immunity and disease progression during a primate lentiviral infection. We propose that, in the disease-resistant SIV-infected SMs, evolutionary adaptation to both preserve immune function with fewer mucosal CD4+ T cells and attenuate the immune activation that follows acute viral infection protect these animals from progressing to AIDS.

Section: Discussionmentioning

confidence: 71%

Severe Depletion of Mucosal CD4+ T Cells in AIDS-Free Simian Immunodeficiency Virus-Infected Sooty Mangabeys

Gordon

Klatt

Bosinger

et al. 2007

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255

267

“…These polymorphisms result in the inability to produce CCR5A in chimpanzees and CCR5B in AGM (11). The relevance of these polymorphic sequences and their potential impact on reduced expression of exon 1-containing transcripts and CCR5 surface expression is illustrated by the recent findings of Pandrea et al (57) who showed that natural hosts for SIV infection express remarkably low levels of CCR5 on CD4 ϩ T cells from gut. Thus, taken together, we propose that in some natural hosts of SIV, polymorphic sequences that affect the Oct-1/2 cis-binding site in Pr2 or splicing patterns of CCR5 mRNA might result in the reduced CCR5 expression (57).…”

Section: Discussionmentioning

confidence: 90%

“…This might provide a possible species-specific mechanism by which primate populations modulate CCR5 gene expression. It is conceivable that loss of the Oct site and other polymorphisms may be responsible for lower levels of CCR5 expression observed in natural primate hosts of SIV infection (e.g., Sooty mangabey) that do not progress to AIDS compared with hosts in which SIV or HIV infection leads to AIDS (57). Extending this notion, the results of our current and previous studies (11) suggest that sequences that influence the production of exon 1-containing transcripts are targets for selection.…”

Section: Discussionmentioning

confidence: 99%

Production of Specific mRNA Transcripts, Usage of an Alternate Promoter, and Octamer-Binding Transcription Factors Influence the Surface Expression Levels of the HIV Coreceptor CCR5 on Primary T Cells

Mummidi

Adams

VanCompernolle

et al. 2007

Surface levels of CCR5 on memory CD4+ T cells influence HIV-1/AIDS susceptibility. Alternative promoter usage results in the generation of CCR5 mRNA isoforms that differ based on whether they contain or lack the untranslated exon 1. The impact of exon 1-containing transcripts on CCR5 surface expression is unknown. In this study, we show that the increased cell surface expression of CCR5 on primary T cells is associated with selective enrichment of exon 1-containing transcripts. The promoter that drives exon 1-containing transcripts is highly active in primary human T cells but not in transformed T cell lines. The transcription factors Oct-1 and -2 inhibit and enhance, respectively, the expression of exon 1-containing transcripts and CCR5 surface levels. However, polymorphisms at homologous octamer-binding sites in the CCR5 promoter of nonhuman primates abrogate the binding of these transcription factors. These results identify exon 1-containing transcripts, and the cis-trans factors that regulate the expression levels of these mRNA isoforms as key parameters that affect CCR5 surface expression levels, and by extension, susceptibility to HIV/AIDS among humans, and possibly, the observed interspecies differences in susceptibility to lentiviral infection.

“…Blood and tissue samples (superficial lymph nodes (LNs), bronchoalveolar lavage (BAL), intestinal biopsy, and intestinal resections) were collected as reported (3,23,47). Plasma and PBMC and mononuclear cells from the intestine, BAL, and LNs were isolated as described previously (3,23).…”

Section: Tissue Samplingmentioning

confidence: 99%

Acute Loss of Intestinal CD4+ T Cells Is Not Predictive of Simian Immunodeficiency Virus Virulence

Pandrea

Gautam

Ribeiro

et al. 2007

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249

402

The predictive value of acute gut-associated lymphoid tissue (GALT) CD4+ T cell depletion in lentiviral infections was assessed by comparing three animal models illustrative of the outcomes of SIV infection: pathogenic infection (SIVsmm infection of rhesus macaques (Rh)), persistent nonprogressive infection (SIVagm infection of African green monkeys (AGM)), and transient, controlled infection (SIVagm infection of Rh). Massive acute depletion of GALT CD4+ T cells was a common feature of acute SIV infection in all three models. The outcome of this mucosal CD4+ T cell depletion, however, differed substantially between the three models: in SIVsmm-infected Rh, the acute GALT CD4+ T cell depletion was persistent and continued with disease progression; in SIVagm, intestinal CD4+ T cells were partially restored during chronic infection in the context of normal levels of apoptosis and immune activation and absence of damage to the mucosal immunologic barrier; in SIVagm-infected Rh, complete control of viral replication resulted in restoration of the mucosal barrier and immune restoration. Therefore, our data support a revised paradigm wherein severe GALT CD4+ T cell depletion during acute pathogenic HIV and SIV infections of humans and Rh is necessary but neither sufficient nor predictive of disease progression, with levels of immune activation, proliferation and apoptosis being key factors involved in determining progression to AIDS.