Humanized mouse model of HIV-1 latency with enrichment of latent virus in PD-1+ and TIGIT+ CD4 T cells

George N. Llewellyn; Eduardo Seclén; Stephen W Wietgrefe; Siyu Liu; Morgan Chateau; Hua Pei; Katherine Perkey; Matthew D. Marsden; Sarah J. Hinkley; David E. Paschon; Michael C. Holmes; Jerome A. Zack; Stan G. Louie; Ashley T Haase; Paula M. Cannona

doi:10.1128/JVI.02086-18

Humanized mouse model of HIV-1 latency with enrichment of latent virus in PD-1⁺ and TIGIT⁺ CD4 T cells

George N. Llewellyn, Eduardo Seclén, Stephen W Wietgrefe, Siyu Liu, Morgan Chateau, Hua Pei, Katherine Perkey, Matthew D. Marsden, Sarah J. Hinkley, David E. Paschon, Michael C. Holmes, Jerome A. Zack, Stan G. Louie, Ashley T Haase, Paula M. Cannona

Microbiology

Research output: Contribution to journal › Article › peer-review

20 Scopus citations

Abstract

Combination anti-retroviral drug therapy (ART) potently suppresses HIV-1 replication but does not result in virus eradication or a cure. A major contributing factor is the long-term persistence of a reservoir of latently infected cells. To study this reservoir, we established a humanized mouse model of HIV-1 infection and ART suppression based on an oral ART regimen. Similar to humans, HIV-1 levels in the blood of ART-treated animals were frequently suppressed below the limits of detection. However, the limited timeframe of the mouse model and the small volume of available samples makes it a challenging model with which to achieve full viral suppression and to investigate the latent reservoir. We therefore used an ex vivo latency reactivation assay that allows a semiquantitative measure of the latent reservoir that establishes in individual animals, regardless of whether they are treated with ART. Using this assay, we found that latently infected human CD4 T cells can be readily detected in mouse lymphoid tissues and that latent HIV-1 was enriched in populations expressing markers of T cell exhaustion, PD-1 and TIGIT. In addition, we were able to use the ex vivo latency reactivation assay to demonstrate that HIV-specific TALENs can reduce the fraction of reactivatable virus in the latently infected cell population that establishes in vivo, supporting the use of targeted nuclease-based approaches for an HIV-1 cure. IMPORTANCE HIV-1 can establish latent infections that are not cleared by current antiretroviral drugs or the body’s immune responses and therefore represent a major barrier to curing HIV-infected individuals. However, the lack of expression of viral antigens on latently infected cells makes them difficult to identify or study. Here, we describe a humanized mouse model that can be used to detect latent but reactivatable HIV-1 in both untreated mice and those on ART and therefore provides a simple system with which to study the latent HIV-1 reservoir and the impact of interventions aimed at reducing it.

Original language	English (US)
Article number	e02086-18
Journal	Journal of virology
Volume	93
Issue number	10
DOIs	https://doi.org/10.1128/JVI.02086-18
State	Published - May 1 2019

Bibliographical note

Funding Information:
This study was supported by NIH grants AI110149 and HL129902 to P.M.C.

Publisher Copyright:
© 2019 American Society for Microbiology. All Rights Reserved.

Keywords

HIV-1
Humanized mice
Latency
PD-1
TALEN
TIGIT

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Llewellyn, G. N., Seclén, E., Wietgrefe, S. W., Liu, S., Chateau, M., Pei, H., Perkey, K., Marsden, M. D., Hinkley, S. J., Paschon, D. E., Holmes, M. C., Zack, J. A., Louie, S. G., Haase, A. T., & Cannona, P. M. (2019). Humanized mouse model of HIV-1 latency with enrichment of latent virus in PD-1⁺ and TIGIT⁺ CD4 T cells. Journal of virology, 93(10), Article e02086-18. https://doi.org/10.1128/JVI.02086-18

Llewellyn, GN, Seclén, E, Wietgrefe, SW, Liu, S, Chateau, M, Pei, H, Perkey, K, Marsden, MD, Hinkley, SJ, Paschon, DE, Holmes, MC, Zack, JA, Louie, SG, Haase, AT & Cannona, PM 2019, 'Humanized mouse model of HIV-1 latency with enrichment of latent virus in PD-1⁺ and TIGIT⁺ CD4 T cells', Journal of virology, vol. 93, no. 10, e02086-18. https://doi.org/10.1128/JVI.02086-18

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