Gut mucosal T cell responses and gene expression correlate with protection against disease in long-term HIV-1-infected nonprogressors

Sankaran, Sumathi; Guadalupe, Moraima; Reay, Elizabeth; George, Michael; Flamm, Jason; Prindiville, Thomas P; Dandekar, Satya

doi:10.1073/pnas.0503463102

Cited by 140 publications

(142 citation statements)

References 23 publications

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“…In a smaller expression profiling study of GALT tissue, long-term nonprogressors had higher expression levels of many immune response genes, although the levels of expression of these genes were even greater in the noncontrollers. 19 It is possible that the controllers in our study have higher expression levels of immune response genes relative to HIV-negative healthy persons, but the levels are still relatively low with respect to the noncontrollers. Finally, it will be of interest to characterize the same set of parameters in HAART-suppressed patients who have undetectable viral loads as a result of drugmediated viral suppression as opposed to natural resistance.…”

Section: Cellular/molecular Signatures Of Hiv Progression E29mentioning

confidence: 79%

“…6,19,25 Our analysis has validated some parameters of such activation that are concordant between the peripheral blood and rectosigmoid biopsy tissue. Using several forms of analysis, we have also For personal use only.…”

Section: Cellular/molecular Signatures Of Hiv Progression E29mentioning

confidence: 98%

“…Whereas transcriptional profiling has been conducted on GALT tissue from long-term nonprogressors 19 and flow cytometric studies have been conducted on controllers, 6 this is the first time that gene expression patterns have been correlated with immune parameters in peripheral blood and in GALT of controllers and noncontrollers. By reducing the dimensions of our flow cytometry data through principal component analysis (PCA), 20 we were able to associate immune parameters with specific molecular markers that distinguish these 2 groups of subjects.…”

Section: Introductionmentioning

confidence: 99%

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Correlating cellular and molecular signatures of mucosal immunity that distinguish HIV controllers from noncontrollers

Loke

Favre

Hunt³

et al. 2010

Blood

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Section: Cellular/molecular Signatures Of Hiv Progression E29mentioning

confidence: 79%

Section: Cellular/molecular Signatures Of Hiv Progression E29mentioning

confidence: 98%

Section: Introductionmentioning

confidence: 99%

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Correlating cellular and molecular signatures of mucosal immunity that distinguish HIV controllers from noncontrollers

Loke

Favre

Hunt³

et al. 2010

Blood

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“…The persistence of HIV reservoirs in the gut-associated lymphoid tissue (GALT) has been well documented, and detectable levels of HIV replication (RNA, DNA, and p24 protein) have been reported in tissue biopsy specimens from the upper and lower intestinal tracts (3)(4)(5). Studies have shown that ART-naive or treated subjects with HIV show decreased intestinal tissue expression of genes involved in mucosal repair and regeneration, while expression of genes regulating inflammation and immune activation is increased (2,(5)(6)(7). In addition, the expression of genes involved in intestinal epithelial integrity and barrier function, such as tight junctional proteins, as well as in nutrient and xenobiotic absorptive and digestive functions, such as drug-metabolizing enzymes, is also decreased in HIV-infected subjects compared to HIV-negative healthy volunteers (6).…”

mentioning

confidence: 99%

“…Studies have shown that ART-naive or treated subjects with HIV show decreased intestinal tissue expression of genes involved in mucosal repair and regeneration, while expression of genes regulating inflammation and immune activation is increased (2,(5)(6)(7). In addition, the expression of genes involved in intestinal epithelial integrity and barrier function, such as tight junctional proteins, as well as in nutrient and xenobiotic absorptive and digestive functions, such as drug-metabolizing enzymes, is also decreased in HIV-infected subjects compared to HIV-negative healthy volunteers (6). Collectively, these data suggest that HIV infection leads to the disruption of the integrity of the intestinal epithelial barrier and alteration in nutrient and drug absorption.…”

mentioning

confidence: 99%

HIV-1 Alters Intestinal Expression of Drug Transporters and Metabolic Enzymes: Implications for Antiretroviral Drug Disposition

Kis

Sankaran-Walters

Hoque

et al. 2016

Antimicrob Agents Chemother

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؉ ART-naive group than in uninfected subjects. qPCR analysis confirmed significantly lower expression of ABCC2/MRP2 in ART-naive subjects than in the control group, while CYP3A4 and ABCG2/BCRP showed a trend toward decreased expression. Protein expression of MRP2 and BCRP was also significantly lower in the HIV ؉ naive group than in the control group and was partially restored to baseline levels in HIV ؉ subjects receiving ART. In contrast, gene and protein expression of ABCB1/Pgp was significantly increased in HIV ؉ subjects on ART relative to HIV ؉ ART-naive subjects. These data demonstrate that the expression of drug-metabolizing enzymes and efflux transporters is significantly altered in therapy-naive HIV ؉ subjects and in those receiving ART. Since CYP3A4, Pgp, MRPs, and BCRP metabolize or transport many antiretroviral drugs, their altered expression with HIV infection may negatively impact drug pharmacokinetics in HIV ؉ subjects. This has clinical implications when using data from healthy volunteers to guide ART.

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Strategies for optimizing targeting and delivery of mucosal HIV vaccines

Ahlers

Belyakov

2009

Eur J Immunol

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Effective frontline defenses against HIV-1 will require targeting vaccines to mucosal tissue in order to induce ab CD8 1 lymphocytes in mucosal effector sites (lamina propria and intraepithelial compartment) as well as antibody secreting plasma cells that can neutralize and limit free virus. A concerted second wave of assault against the virus will require the activation and recruitment of antigen specific memory CD4 1 and CD8 1 T cells in mesenteric lymph nodes and distal secondary lymphoid organs. New delivery strategies targeting the ''right'' DC subsets in combination with delivery of mucosal adjuvants and innate signals for activating DC will be essential for mucosal vaccines in order to circumvent the naturally tolerogenic environment and the induction of Tregs. Mucosal delivery of antigen in combination with inflammatory signals has been shown to empower systemic immunization by directing responses to mucosal sites for imprinting optimum mucosal memory. Here, we discuss novel vaccine strategies and adjuvants for optimizing mucosal delivery of HIV vaccines.

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Gut mucosal T cell responses and gene expression correlate with protection against disease in long-term HIV-1-infected nonprogressors

Cited by 140 publications

References 23 publications

Correlating cellular and molecular signatures of mucosal immunity that distinguish HIV controllers from noncontrollers

Correlating cellular and molecular signatures of mucosal immunity that distinguish HIV controllers from noncontrollers

HIV-1 Alters Intestinal Expression of Drug Transporters and Metabolic Enzymes: Implications for Antiretroviral Drug Disposition

Strategies for optimizing targeting and delivery of mucosal HIV vaccines

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