Robust and persistent reactivation of SIV and HIV by N-803 and depletion of CD8+ cells

Julia Bergild McBrien; Maud Mavigner; Lavinia Franchitti; S. Abigail Smith; Erick White; Gregory K. Tharp; Hasse Walum; Kathleen Busman-Sahay; Christian R. Aguilera-Sandoval; William O. Thayer; Rae Ann Spagnuolo; Martina Kovarova; Angela Wahl; Barbara Cervasi; David M. Margolis; Thomas H. Vanderford; Diane G. Carnathan; Mirko Paiardini; Jeffrey D. Lifson; John H. Lee; Jeffrey T. Safrit; Steven E. Bosinger; Jacob D. Estes; Cynthia A. Derdeyn; J. Victor Garcia; Deanna A. Kulpa; Ann Chahroudi; Guido Silvestri

doi:10.1038/s41586-020-1946-0

Robust and persistent reactivation of SIV and HIV by N-803 and depletion of CD8⁺ cells

Julia Bergild McBrien, Maud Mavigner, Lavinia Franchitti, S. Abigail Smith, Erick White, Gregory K. Tharp, Hasse Walum, Kathleen Busman-Sahay, Christian R. Aguilera-Sandoval, William O. Thayer, Rae Ann Spagnuolo, Martina Kovarova, Angela Wahl, Barbara Cervasi, David M. Margolis, Thomas H. Vanderford, Diane G. Carnathan, Mirko Paiardini, Jeffrey D. Lifson, John H. LeeJeffrey T. Safrit, Steven E. Bosinger, Jacob D. Estes, Cynthia A. Derdeyn, J. Victor Garcia, Deanna A. Kulpa, Ann Chahroudi, Guido Silvestri

Vaccine and Gene Therapy Institute

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94 Scopus citations

Abstract

Human immunodeficiency virus (HIV) persists indefinitely in individuals with HIV who receive antiretroviral therapy (ART) owing to a reservoir of latently infected cells that contain replication-competent virus^1–4. Here, to better understand the mechanisms responsible for latency persistence and reversal, we used the interleukin-15 superagonist N-803 in conjunction with the depletion of CD8⁺ lymphocytes in ART-treated macaques infected with simian immunodeficiency virus (SIV). Although N-803 alone did not reactivate virus production, its administration after the depletion of CD8⁺ lymphocytes in conjunction with ART treatment induced robust and persistent reactivation of the virus in vivo. We found viraemia of more than 60 copies per ml in all macaques (n = 14; 100%) and in 41 out of a total of 56 samples (73.2%) that were collected each week after N-803 administration. Notably, concordant results were obtained in ART-treated HIV-infected humanized mice. In addition, we observed that co-culture with CD8⁺ T cells blocked the in vitro latency-reversing effect of N-803 on primary human CD4⁺ T cells that were latently infected with HIV. These results advance our understanding of the mechanisms responsible for latency reversal and lentivirus reactivation during ART-suppressed infection.

Original language	English (US)
Pages (from-to)	154-159
Number of pages	6
Journal	Nature
Volume	578
Issue number	7793
DOIs	https://doi.org/10.1038/s41586-020-1946-0
State	Published - Feb 6 2020

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McBrien, J. B., Mavigner, M., Franchitti, L., Smith, S. A., White, E., Tharp, G. K., Walum, H., Busman-Sahay, K., Aguilera-Sandoval, C. R., Thayer, W. O., Spagnuolo, R. A., Kovarova, M., Wahl, A., Cervasi, B., Margolis, D. M., Vanderford, T. H., Carnathan, D. G., Paiardini, M., Lifson, J. D., ... Silvestri, G. (2020). Robust and persistent reactivation of SIV and HIV by N-803 and depletion of CD8⁺ cells. Nature, 578(7793), 154-159. https://doi.org/10.1038/s41586-020-1946-0

McBrien, JB, Mavigner, M, Franchitti, L, Smith, SA, White, E, Tharp, GK, Walum, H, Busman-Sahay, K, Aguilera-Sandoval, CR, Thayer, WO, Spagnuolo, RA, Kovarova, M, Wahl, A, Cervasi, B, Margolis, DM, Vanderford, TH, Carnathan, DG, Paiardini, M, Lifson, JD, Lee, JH, Safrit, JT, Bosinger, SE, Estes, JD, Derdeyn, CA, Garcia, JV, Kulpa, DA, Chahroudi, A & Silvestri, G 2020, 'Robust and persistent reactivation of SIV and HIV by N-803 and depletion of CD8⁺ cells', Nature, vol. 578, no. 7793, pp. 154-159. https://doi.org/10.1038/s41586-020-1946-0

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title = "Robust and persistent reactivation of SIV and HIV by N-803 and depletion of CD8+ cells",

abstract = "Human immunodeficiency virus (HIV) persists indefinitely in individuals with HIV who receive antiretroviral therapy (ART) owing to a reservoir of latently infected cells that contain replication-competent virus1–4. Here, to better understand the mechanisms responsible for latency persistence and reversal, we used the interleukin-15 superagonist N-803 in conjunction with the depletion of CD8+ lymphocytes in ART-treated macaques infected with simian immunodeficiency virus (SIV). Although N-803 alone did not reactivate virus production, its administration after the depletion of CD8+ lymphocytes in conjunction with ART treatment induced robust and persistent reactivation of the virus in vivo. We found viraemia of more than 60 copies per ml in all macaques (n = 14; 100%) and in 41 out of a total of 56 samples (73.2%) that were collected each week after N-803 administration. Notably, concordant results were obtained in ART-treated HIV-infected humanized mice. In addition, we observed that co-culture with CD8+ T cells blocked the in vitro latency-reversing effect of N-803 on primary human CD4+ T cells that were latently infected with HIV. These results advance our understanding of the mechanisms responsible for latency reversal and lentivirus reactivation during ART-suppressed infection.",

author = "McBrien, {Julia Bergild} and Maud Mavigner and Lavinia Franchitti and Smith, {S. Abigail} and Erick White and Tharp, {Gregory K.} and Hasse Walum and Kathleen Busman-Sahay and Aguilera-Sandoval, {Christian R.} and Thayer, {William O.} and Spagnuolo, {Rae Ann} and Martina Kovarova and Angela Wahl and Barbara Cervasi and Margolis, {David M.} and Vanderford, {Thomas H.} and Carnathan, {Diane G.} and Mirko Paiardini and Lifson, {Jeffrey D.} and Lee, {John H.} and Safrit, {Jeffrey T.} and Bosinger, {Steven E.} and Estes, {Jacob D.} and Derdeyn, {Cynthia A.} and Garcia, {J. Victor} and Kulpa, {Deanna A.} and Ann Chahroudi and Guido Silvestri",

note = "Funding Information: Acknowledgements This work was supported by NIH grants R01-AI125064 and UM1-AI124436 (to G.S. and A.C.); R01-AI143414 (to G.S. and D.A.K.); R01-MH108179 and R01-AI111899 (to J.V.G.); UM1-AI126619 (to D.M.M.); R01-AI123010 (to A.W.); P30 AI050409 (Emory Center for AIDS Research); P51 OD011092 (Oregon National Primate Research Center base grant); the National Institutes of Health{\textquoteright}s Office of the Director, Office of Research Infrastructure Programs P51OD011132 (Yerkes National Primate Research Center base grant); and supported in part by federal funds from the National Cancer Institute, National Institutes of Health, under contracts HHSN261200800001E and 75N91019D00024 (J.D.L.). We thank B. Jones, S. O{\textquoteright}Connor and J. Sacha for discussions; S. Ehnert, S. Jean and all of the animal care and veterinary staff at the Yerkes National Primate Research Center; B. Cervasi and K. Gill at the Emory University Flow Cytometry Core; Emory and Pediatric{\textquoteright}s/Winship Flow Cytometry Core; the Translational Virology and Reservoir Cores of the Emory CFAR, the Emory Nonhuman Primate Genomics Core for RNA sequencing and analysis and the Quantitative Molecular Diagnostics Core of the AIDS and Cancer Virus Program, Frederick National Laboratory, for high-sensitivity plasma viral-load testing; NantKwest for providing N-803, K. Reimann and the NHP Reagent Resources for the MT807R1 antibody, R. Geleziunas and Gilead Pharmaceuticals for providing tenofovir and emtricitabine, D. Hazuda and B. Howell from Merck for providing raltegravir and J. Demarest and ViiV Healthcare for providing dolutegravir for this study. Publisher Copyright: {\textcopyright} 2020, The Author(s), under exclusive licence to Springer Nature Limited.",

year = "2020",

month = feb,

day = "6",

doi = "10.1038/s41586-020-1946-0",

language = "English (US)",

volume = "578",

pages = "154--159",

journal = "Nature",

issn = "0028-0836",

publisher = "Nature Publishing Group",

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TY - JOUR

T1 - Robust and persistent reactivation of SIV and HIV by N-803 and depletion of CD8+ cells

AU - McBrien, Julia Bergild

AU - Mavigner, Maud

AU - Franchitti, Lavinia

AU - Smith, S. Abigail

AU - White, Erick

AU - Tharp, Gregory K.

AU - Walum, Hasse

AU - Busman-Sahay, Kathleen

AU - Aguilera-Sandoval, Christian R.

AU - Thayer, William O.

AU - Spagnuolo, Rae Ann

AU - Kovarova, Martina

AU - Wahl, Angela

AU - Cervasi, Barbara

AU - Margolis, David M.

AU - Vanderford, Thomas H.

AU - Carnathan, Diane G.

AU - Paiardini, Mirko

AU - Lifson, Jeffrey D.

AU - Lee, John H.

AU - Safrit, Jeffrey T.

AU - Bosinger, Steven E.

AU - Estes, Jacob D.

AU - Derdeyn, Cynthia A.

AU - Garcia, J. Victor

AU - Kulpa, Deanna A.

AU - Chahroudi, Ann

AU - Silvestri, Guido

N1 - Funding Information: Acknowledgements This work was supported by NIH grants R01-AI125064 and UM1-AI124436 (to G.S. and A.C.); R01-AI143414 (to G.S. and D.A.K.); R01-MH108179 and R01-AI111899 (to J.V.G.); UM1-AI126619 (to D.M.M.); R01-AI123010 (to A.W.); P30 AI050409 (Emory Center for AIDS Research); P51 OD011092 (Oregon National Primate Research Center base grant); the National Institutes of Health’s Office of the Director, Office of Research Infrastructure Programs P51OD011132 (Yerkes National Primate Research Center base grant); and supported in part by federal funds from the National Cancer Institute, National Institutes of Health, under contracts HHSN261200800001E and 75N91019D00024 (J.D.L.). We thank B. Jones, S. O’Connor and J. Sacha for discussions; S. Ehnert, S. Jean and all of the animal care and veterinary staff at the Yerkes National Primate Research Center; B. Cervasi and K. Gill at the Emory University Flow Cytometry Core; Emory and Pediatric’s/Winship Flow Cytometry Core; the Translational Virology and Reservoir Cores of the Emory CFAR, the Emory Nonhuman Primate Genomics Core for RNA sequencing and analysis and the Quantitative Molecular Diagnostics Core of the AIDS and Cancer Virus Program, Frederick National Laboratory, for high-sensitivity plasma viral-load testing; NantKwest for providing N-803, K. Reimann and the NHP Reagent Resources for the MT807R1 antibody, R. Geleziunas and Gilead Pharmaceuticals for providing tenofovir and emtricitabine, D. Hazuda and B. Howell from Merck for providing raltegravir and J. Demarest and ViiV Healthcare for providing dolutegravir for this study. Publisher Copyright: © 2020, The Author(s), under exclusive licence to Springer Nature Limited.

PY - 2020/2/6

Y1 - 2020/2/6

N2 - Human immunodeficiency virus (HIV) persists indefinitely in individuals with HIV who receive antiretroviral therapy (ART) owing to a reservoir of latently infected cells that contain replication-competent virus1–4. Here, to better understand the mechanisms responsible for latency persistence and reversal, we used the interleukin-15 superagonist N-803 in conjunction with the depletion of CD8+ lymphocytes in ART-treated macaques infected with simian immunodeficiency virus (SIV). Although N-803 alone did not reactivate virus production, its administration after the depletion of CD8+ lymphocytes in conjunction with ART treatment induced robust and persistent reactivation of the virus in vivo. We found viraemia of more than 60 copies per ml in all macaques (n = 14; 100%) and in 41 out of a total of 56 samples (73.2%) that were collected each week after N-803 administration. Notably, concordant results were obtained in ART-treated HIV-infected humanized mice. In addition, we observed that co-culture with CD8+ T cells blocked the in vitro latency-reversing effect of N-803 on primary human CD4+ T cells that were latently infected with HIV. These results advance our understanding of the mechanisms responsible for latency reversal and lentivirus reactivation during ART-suppressed infection.

AB - Human immunodeficiency virus (HIV) persists indefinitely in individuals with HIV who receive antiretroviral therapy (ART) owing to a reservoir of latently infected cells that contain replication-competent virus1–4. Here, to better understand the mechanisms responsible for latency persistence and reversal, we used the interleukin-15 superagonist N-803 in conjunction with the depletion of CD8+ lymphocytes in ART-treated macaques infected with simian immunodeficiency virus (SIV). Although N-803 alone did not reactivate virus production, its administration after the depletion of CD8+ lymphocytes in conjunction with ART treatment induced robust and persistent reactivation of the virus in vivo. We found viraemia of more than 60 copies per ml in all macaques (n = 14; 100%) and in 41 out of a total of 56 samples (73.2%) that were collected each week after N-803 administration. Notably, concordant results were obtained in ART-treated HIV-infected humanized mice. In addition, we observed that co-culture with CD8+ T cells blocked the in vitro latency-reversing effect of N-803 on primary human CD4+ T cells that were latently infected with HIV. These results advance our understanding of the mechanisms responsible for latency reversal and lentivirus reactivation during ART-suppressed infection.

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Robust and persistent reactivation of SIV and HIV by N-803 and depletion of CD8⁺ cells

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