Ex vivo rectal explant model reveals potential opposing roles of Natural Killer cells and Marginal Zone-like B cells in HIV-1 infection

Smith, S Abigail; Murray, Phillip M.; Amancha, Praveen Kumar; Ackerley, Cassie Grimsley; Hu, Yi‐Juan; Amara, Rama Rao; Kelley, Colleen F.

doi:10.1038/s41598-020-76976-5

Cited by 4 publications

(7 citation statements)

References 58 publications

(62 reference statements)

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“…Additional significant Reactome pathways included antigen-presenting cell (APC)/B-cell pathways and cytokine/chemokine pathways (Table 1). Previous studies within our lab identified B cells within the gut, specifically CD1c+ B cells, as being associated with p24 production in the rectal explant model [17], and CD1C was also associated with p24 here (log 2 fold = 1.10, P adj = 0.003). Additional DEGs of interest included genes necessary for B-cell–T-cell interactions, such as CD40 (log 2 fold = 0.72, P adj = 0.0004), CD83 (log 2 fold = 0.93, P adj = 0.003), and IL4I1 (log 2 fold = 0.96, P adj = 0.001).…”

Section: Resultsmentioning

confidence: 66%

“…For the explant challenge, three biopsies from each participant were weighed and challenged with 10 2.8 TCID 50 HIV-1 BaL for 2 h (37 8C, 5% CO 2 ), placed on a collagen raft, and sampled longitudinally, as previously described [17]. Supernatants were collected on days 3, 7, 10, 14, and 18 post-challenge, and stored at À30 8C until p24 was quantified via ELISA (ABL, Inc., Rockville, Maryland, USA; #5447), and normalized to biopsy weight.…”

Section: Methodsmentioning

confidence: 99%

“…As an alternative strategy to identify signatures within the rectal mucosa associated with support or restriction of HIV replication, we utilized the ex-vivo human rectal explant model of HIV infection. This system was developed to interrogate the earliest immune responses within rectal mucosal tissues after HIVexposure, to evaluate novel anti-HIV therapeutics, and, within our lab, to identify immune cell subsets associated with support or suppression of HIV production [11][12][13][14][15][16][17]. Here, we performed bulk RNAseq transcriptomic analyses on rectal biopsies donated by HIV-negative men (Fig.…”

Section: Introductionmentioning

confidence: 99%

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T-cell activation and B-cell interaction signatures in rectal tissues are associated with HIV replication in ex-vivo model of infection

Smith

Murray

Amancha

et al. 2022

Aids

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Objective: The rectal mucosa is a critical site of HIV vulnerability. We sought to identify transcriptomic features of rectal mucosal tissue prior to exposure associated with support or restriction of HIV replication.Design: Rectal tissue from HIV-negative cisgender men (n ¼ 57) underwent concurrent RNAseq transcriptomic analyses (two biopsies/participant) and challenge with HIV in the ex-vivo explant model of infection (three biopsies challenged/participant) as part of a larger cohort study to understand the rectal mucosal immune environment among MSM.Methods: P24 was quantified in the explant supernatants over a culture period of 18 days via ELISA. Participant median p24 log area under the curve was correlated with bulk transcriptomic data (Illumina HiSeq3000) to identify associations between gene expression and p24 production. Significant differentially expressed genes (DEGs) were identified via DESeq2 analysis and analyzed with Reactome to identify pathways of interest.Results: In total, 183 DEG (181 upregulated, two downregulated) were associated with higher p24 accumulation in the ex-vivo challenge model, including T-cell activation, Bcell function, and chemokine DEG. Reactome analysis of the upregulated genes identified 'Adaptive Immune System', 'Cytokine Signaling in Immune System', and 'Innate Immune System' as significantly upregulated pathways. Conclusion:For the first time, we identified rectal tissue transcriptomic signatures associated with increased p24 production utilizing an ex-vivo model. Our findings are highly relevant to HIV transmission and the early establishment of HIV reservoirs in humans, and future studies should examine the identified pathways as targets for new or improved biomedical prevention or treatment interventions.

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Section: Resultsmentioning

confidence: 66%

Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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T-cell activation and B-cell interaction signatures in rectal tissues are associated with HIV replication in ex-vivo model of infection

Smith

Murray

Amancha

et al. 2022

Aids

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“…Three fresh rectal biopsy specimens from each participant were exposed to HIV-1 BaL (10 2.8 TCID 50 in a volume of 250 µL media) for 2 hours, washed extensively, and placed on collagen rafts for the 18-day incubation period, as described in detail previously ( 22 ). Culture supernatant was collected from each well at days 3, 7, 10, 14, and 18 for p24 concentration analysis, and the well was replenished with 700 μl of fresh complete media.…”

Section: Methodsmentioning

confidence: 99%

The rectal mucosal immune environment and HIV susceptibility among young men who have sex with men

et al. 2022

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Young men who have sex with men (YMSM) represent a particularly high-risk group for HIV acquisition in the US, despite similarly reported rates of sexual activity as older, adult MSM (AMSM). Increased rates of HIV infection among YMSM compared to AMSM could be partially attributable to differences within the rectal mucosal (RM) immune environment associated with earlier sexual debut and less lifetime exposure to receptive anal intercourse. Using an ex vivo explant HIV challenge model, we found that rectal tissues from YMSM supported higher levels of p24 at peak viral replication timepoints compared to AMSM. Among YMSM, the RM was characterized by increased CD4+ T cell proliferation, as well as lower frequencies of tissue resident CD8+ T cells and pro-inflammatory cytokine producing CD4+ and CD8+ T cells. In addition, the microbiome composition of YMSM was enriched for anaerobic taxa that have previously been associated with HIV acquisition risk, including Prevotella, Peptostreptococcus, and Peptoniphilus. These distinct immunologic and microbiome characteristics were found to be associated with higher HIV replication following ex vivo challenge of rectal explants, suggesting the RM microenvironment of YMSM may be uniquely conducive to HIV infection.

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“…NK cells also seem to play a role in the rectal immunity to HIV. A higher frequency of NK cells in rectal mucosa (which resembles that of the FGT, with the lower expression of CD16 and a higher expression of CD56 compared to their blood counterparts) seem to correlate negatively with HIV-1 replication in this tissue, as opposed to MZ B-cells, which frequencies correlate positively with viral replication [ 190 , 197 ]. It was suggested that MZ could contribute to trans-infection of HIV given that as mentioned earlier, these cells can bind to virus particles via surface lectins such as α4β7 and DC-SIGN [ 152 ].…”

Section: Natural Killer Cellsmentioning

confidence: 99%

The Importance of Regulation in Natural Immunity to HIV

et al. 2021

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Worldwide, most Human Immunodeficiency Virus (HIV) infections are acquired through heterosexual intercourse, and in sub-Saharan Africa, 59% of new HIV infections affect women. Vaccines and microbicides hold promise for preventing the acquisition of HIV. To this end, the study of HIV highly exposed seronegative (HESN) female commercial sex workers (CSWs), who constitute a model of natural immunity to HIV, provides an exceptional opportunity to determine important clues for the development of preventive strategies. Studies using both female genital tract (FGT) and peripheral blood samples of HESN CSWs, have allowed identifying distinct features, notably low-inflammatory patterns associated with resistance to infection. How this seemingly regulated response is achieved at the initial site of HIV infection remains unknown. One hypothesis is that populations presenting regulatory profiles contribute to the orchestration of potent anti-viral and low-inflammatory responses at the initial site of HIV transmission. Here, we view to update our knowledge regarding this issue.

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Ex vivo rectal explant model reveals potential opposing roles of Natural Killer cells and Marginal Zone-like B cells in HIV-1 infection

Cited by 4 publications

References 58 publications

T-cell activation and B-cell interaction signatures in rectal tissues are associated with HIV replication in ex-vivo model of infection

T-cell activation and B-cell interaction signatures in rectal tissues are associated with HIV replication in ex-vivo model of infection

The rectal mucosal immune environment and HIV susceptibility among young men who have sex with men

The Importance of Regulation in Natural Immunity to HIV

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