Sage Journals: Discover world-class research

Abstract

Ex vivo mucosal explants have become a mainstay of HIV-1 studies using human tissue. In this study, we examine the baseline phenotypic and virologic differences between biopsies derived from the small intestine (SI) and large intestine (LI) for use in ex vivo explant studies. To do this, we collected endoscopic mucosal biopsies from both SI and LI from the same healthy, HIV-seronegative participants. Mucosal mononuclear cell phenotypes and quantity were compared using flow cytometry. Comparative HIV-1 infectibility of the explants was assessed using an ex vivo explant HIV-1 infection assay. We found that all biopsies had similar numbers of T cells per biopsy. While the percentage of CD4⁺ T cells from SI biopsies expressed significantly more activation markers (CD38, HLA-DR) and HIV coreceptors (CXCR4, CCR5), the absolute numbers of activated CD4⁺ T cells were similar between both sites. LI explants, however, supported more efficient HIV-1 infection, as evidenced by earlier rise in p24 accumulation and greater percent of infected explants at limiting infectious doses. These results suggest that explants from LI biopsies support more efficient HIV-1 infection than SI biopsies, despite similar numbers of available, activated HIV-1 target cells. These findings highlight important differences in LI and SI explants, which must be considered in designing and interpreting ex vivo HIV-1 infection studies, and suggest that factors within the tissue other than target cell number and activation state may play a role in regulating HIV-1 infection.

Get full access to this article

View all access options for this article.

References

Patel

, Borkowf

, Brooks

, Lasry

, Lansky

, Mermin

: Estimating per-act HIV transmission risk: A systematic review. AIDS, 2014; 28:1509–1519.

Veazey

, DeMaria

, Chalifoux

, et al.: Gastrointestinal tract as a major site of CD4+ T cell depletion and viral replication in SIV infection. Science, 1998; 280:427–431.

Mattapallil

, Douek

, Hill

, Nishimura

, Martin

, Roederer

: Massive infection and loss of memory CD4+ T cells in multiple tissues during acute SIV infection. Nature, 2005; 434:1093–1097.

, Duan

, Estes

, et al.: Peak SIV replication in resting memory CD4+ T cells depletes gut lamina propria CD4+ T cells. Nature, 2005; 434:1148–1152.

Mehandru

, Poles

, Tenner-Racz

, et al.: Primary HIV-1 infection is associated with preferential depletion of CD4+ T lymphocytes from effector sites in the gastrointestinal tract. J Exp Med, 2004; 200:761–770.

Voigt

, Keshavarzian

, Losurdo

, et al.: HIV-associated mucosal gene expression: Region-specific alterations. AIDS, 2015; 29:537–546.

Donaldson

, Lee

, Mazmanian

: Gut biogeography of the bacterial microbiota. Nat Rev Micro, 2016; 14:20–32.

Abner

, Guenthner

, Guarner

, et al.: A human colorectal explant culture to evaluate topical microbicides for the prevention of HIV infection. J Infect Dis, 2005; 192:1545–1556.

Fletcher

, Elliott

, Grivel

, et al.: Ex vivo culture of human colorectal tissue for the evaluation of candidate microbicides. AIDS, 2006; 20:1237–1245.

10.

Richardson-Harman

, Lackman-Smith

, Fletcher

, et al.: Multisite comparison of anti-human immunodeficiency virus microbicide activity in explant assays using a novel endpoint analysis. J Clin Microbiol, 2009; 47:3530–3539.

11.

Shacklett

, Yang

, Hausner

, et al.: Optimization of methods to assess human mucosal T-cell responses to HIV infection. J Immunol Methods, 2003; 279:17–31.

12.

Miller

, Li

, Abel

, et al.: Propagation and dissemination of infection after vaginal transmission of simian immunodeficiency virus. J Virol, 2005; 79:9217–9227.

13.

Zhang

, Schuler

, Zupancic

, et al.: Sexual transmission and propagation of SIV and HIV in resting and activated CD4+ T cells. Science, 1999; 286:1353–1357.

14.

Zhang

, Wietgrefe

, Li

, et al.: Roles of substrate availability and infection of resting and activated CD4+ T cells in transmission and acute simian immunodeficiency virus infection. Proc Natl Acad Sci U S A, 2004; 101:5640–5645.

15.

Richardson-Harman

, Mauck

, McGowan

, Anton

: Dose-response relationship between tissue concentrations of UC781 and explant infectibility with HIV type 1 in the RMP-01 rectal safety study. AIDS Res Hum Retroviruses, 2012; 28:1422–1433.

16.

Richardson-Harman

, Hendrix

, Bumpus

, et al.: Correlation between compartmental tenofovir concentrations and an ex vivo rectal biopsy model of tissue infectibility in the RMP-02/MTN-006 phase 1 study. PLoS One, 2014; 9:e111507.

17.

Anton

, Saunders

, Elliott

, et al.: First phase 1 double-blind, placebo-controlled, randomized rectal microbicide trial using UC781 gel with a novel index of ex vivo efficacy. PLoS One, 2011; 6:e23243.

18.

Bunge

AKE

, Dezzutti

, Rohan

, et al.: A Phase 1 trial to assess the safety, acceptability, pharmacokinetics and pharmacodynamics of a novel dapivirine vaginal film. J Acquir Immune Defic Syndr (1999), 2016; 71:498–505.

19.

Dezzutti

, Russo

, Wang

, et al.: Development of HIV-1 rectal-specific microbicides and colonic tissue evaluation. PLoS One, 2014; 9:e102585.

20.

Herrera

, Cranage

, McGowan

, Anton

, Shattock

: Colorectal microbicide design: Triple combinations of reverse transcriptase inhibitors are optimal against HIV-1 in tissue explants. AIDS, 2011; 25:1971–1979.

21.

Scott

, Park

, Dezzutti

: Broadly neutralizing anti-HIV antibodies prevent HIV infection of mucosal tissue ex vivo. Antimicrob Agents Chemother, 2016; 60:904–912.

22.

Boullé

, Müller

, Dähling

, et al.: HIV cell-to-cell spread results in earlier onset of viral gene expression by multiple infections per cell. PLoS Pathog, 2016; 12:e1005964.

23.

Iwami

, Takeuchi

, Nakaoka

, et al.: Cell-to-cell infection by HIV contributes over half of virus infection. Elife, 2015; 4.

24.

Sigal

, Kim

, Balazs

, et al.: Cell-to-cell spread of HIV permits ongoing replication despite antiretroviral therapy. Nature, 2011; 477:95–98.

25.

Cameron

, Freudenthal

, Barker

, Gezelter

, Inaba

, Steinman

: Dendritic cells exposed to human immunodeficiency virus type-1 transmit a vigorous cytopathic infection to CD4+ T cells. Science, 1992; 257:383–387.

26.

Gurney

, Elliott

, Nassanian

, et al.: Binding and transfer of human immunodeficiency virus by DC-SIGN+ cells in human rectal mucosa. J Virol, 2005; 79:5762–5773.

27.

Meng

, Sellers

, Mosteller-Barnum

, Rogers

, Shaw

, Smith

: Lamina propria lymphocytes, not macrophages, express CCR5 and CXCR4 and are the likely target cell for human immunodeficiency virus type 1 in the intestinal mucosa. J Infect Dis, 2000; 182:785–791.

28.

, Meng

, Graham

, Shaw

, Smith

: Intestinal macrophages display reduced permissiveness to human immunodeficiency virus 1 and decreased surface CCR5. Gastroenterology, 1999; 116:1043–1053.

29.

Preza

, Yang

, Elliott

, Anton

, Ochoa

: T lymphocyte density and distribution in human colorectal mucosa, and inefficiency of current cell isolation protocols. PLoS One, 2015; 10:e0122723.

Supplementary Material

Please find the following supplemental material available below.

For Open Access articles published under a Creative Commons License, all supplemental material carries the same license as the article it is associated with.

For non-Open Access articles published, all supplemental material carries a non-exclusive license, and permission requests for re-use of supplemental material or any part of supplemental material shall be sent directly to the copyright owner as specified in the copyright notice associated with the article.

0.00 MB

0.34 MB

Comparative Assessment of Small and Large Intestine Biopsies for Ex Vivo HIV-1 Pathogenesis Studies

Abstract

Get full access to this article

References

Supplementary Material