Your search keyword '"Jeffrey D. Lifson"' showing total 525 results

1. Administration of anti-HIV-1 broadly neutralizing monoclonal antibodies with increased affinity to Fcγ receptors during acute SHIVAD8-EO infection

Author

Joana Dias, Giulia Fabozzi, Slim Fourati, Xuejun Chen, Cuiping Liu, David R. Ambrozak, Amy Ransier, Farida Laboune, Jianfei Hu, Wei Shi, Kylie March, Anna A. Maximova, Stephen D. Schmidt, Jakob Samsel, Chloe A. Talana, Keenan Ernste, Sung Hee Ko, Margaret E. Lucas, Pierce E. Radecki, Kristin L. Boswell, Yoshiaki Nishimura, John-Paul Todd, Malcolm A. Martin, Constantinos Petrovas, Eli A. Boritz, Nicole A. Doria-Rose, Daniel C. Douek, Rafick-Pierre Sékaly, Jeffrey D. Lifson, Mangaiarkarasi Asokan, Lucio Gama, John R. Mascola, Amarendra Pegu, and Richard A. Koup

Subjects

Science

Abstract

Abstract Anti-HIV-1 broadly neutralizing antibodies (bNAbs) have the dual potential of mediating virus neutralization and antiviral effector functions through their Fab and Fc domains, respectively. So far, bNAbs with enhanced Fc effector functions in vitro have only been tested in NHPs during chronic simian-HIV (SHIV) infection. Here, we investigate the effects of administering in acute SHIVAD8-EO infection either wild-type (WT) bNAbs or bNAbs carrying the S239D/I332E/A330L (DEL) mutation, which increases binding to FcγRs. Emergence of virus in plasma and lymph nodes (LNs) was delayed by bNAb treatment and occurred earlier in monkeys given DEL bNAbs than in those given WT bNAbs, consistent with faster clearance of DEL bNAbs from plasma. DEL bNAb-treated monkeys had higher levels of circulating virus-specific IFNγ single-producing CD8+ CD69+ T cells than the other groups. In LNs, WT bNAbs were evenly distributed between follicular and extrafollicular areas, but DEL bNAbs predominated in the latter. At week 8 post-challenge, LN monocytes and NK cells from DEL bNAb-treated monkeys upregulated proinflammatory signaling pathways and LN T cells downregulated TNF signaling via NF-κB. Overall, bNAbs with increased affinity to FcγRs shape innate and adaptive cellular immunity, which may be important to consider in future strategies of passive bNAb therapy.

Published

2024

2. No evidence for ongoing replication on ART in SIV-infected macaques

Author

Taina T. Immonen, Christine M. Fennessey, Leslie Lipkey, Laura Newman, Agatha Macairan, Marjorie Bosche, Nora Waltz, Gregory Q. Del Prete, Jeffrey D. Lifson, and Brandon F. Keele

Subjects

Science

Abstract

Abstract The capacity of HIV-1 to replicate during optimal antiretroviral therapy (ART) is challenging to assess directly. To gain greater sensitivity to detect evolution on ART, we used a nonhuman primate (NHP) model providing precise control over the level of pre-ART evolution and more comprehensive analyses than are possible with clinical samples. We infected 21 rhesus macaques (RMs) with the barcoded virus SIVmac239M and initiated ART early to minimize baseline genetic diversity. RMs were treated for 285–1200 days. We used several tests of molecular evolution to compare 1352 near-full-length (nFL) SIV DNA single genome sequences from PBMCs, lymph nodes, and spleen obtained near the time of ART initiation and those present after long-term ART, none of which showed significant changes to the SIV DNA population during ART in any animal. To investigate the possibility of ongoing replication in unsampled putative tissue sanctuaries during ART, we discontinued treatment in four animals and confirmed that none of the 336 nFL SIV RNA sequences obtained from rebound plasma viremia showed evidence of evolution. The rigorous nature of our analyses reinforced the emerging consensus of a lack of appreciable ongoing replication on effective ART and validates the relevance of this NHP model for cure studies.

Published

2024

3. Acute-phase innate immune responses in SIVmac239-infected Mamu-B*08+ Indian rhesus macaques may contribute to the establishment of elite control

Author

Brandon C. Rosen, Kaitlin Sawatzki, Michael J. Ricciardi, Elise Smith, Inah Golez, Jack T. Mauter, Núria Pedreño-López, Aaron Yrizarry-Medina, Kim L. Weisgrau, Logan J. Vosler, Thomas B. Voigt, Johan J. Louw, Jennifer Tisoncik-Go, Leanne S. Whitmore, Christakis Panayiotou, Noor Ghosh, Jessica R. Furlott, Christopher L. Parks, Ronald C. Desrosiers, Jeffrey D. Lifson, Eva G. Rakasz, David I. Watkins, and Michael Gale

Subjects

simian immunodeficiency virus (SIV), cytotoxic T lymphocytes (CTLs), human immunodeficiency virus (HIV), vaccines, acquired immunodeficiency syndrome (AIDS), Immunologic diseases. Allergy, RC581-607

Abstract

IntroductionSpontaneous control of chronic-phase HIV/SIV viremia is often associated with the expression of specific MHC class I allotypes. HIV/SIV-specific CD8+ cytotoxic T lymphocytes (CTLs) restricted by these MHC class I allotypes appear to be critical for viremic control. Establishment of the elite controller (EC) phenotype is predictable in SIVmac239-infected Indian rhesus macaques (RMs), with approximately 50% of Mamu-B*08+ RMs and 20% of Mamu-B*17+ RMs becoming ECs. Despite extensive characterization of EC-associated CTLs in HIV/SIV-infected individuals, the precise mechanistic basis of elite control remains unknown. Because EC and non-EC viral load trajectories begin diverging by day 14 post-infection, we hypothesized that hyperacute innate immune responses may contribute to viremic control.MethodsTo gain insight into the immunological factors involved in the determination of EC status, we vaccinated 16 Mamu-B*08+ RMs with Vif and Nef to elicit EC-associated CTLs, then subjected these 16 vaccinees and an additional 16 unvaccinated Mamu-B*08+ controls to repeated intrarectal SIVmac239 challenges. We then performed whole-blood transcriptomic analysis of all 32 SIVmac239-infected Mamu-B*08+ RMs and eight SIVmac239-infected Mamu-B*08– RMs during the first 14 days of infection.ResultsVaccination did not provide protection against acquisition, but peak and setpoint viremia were significantly lower in vaccinees relative to controls. We did not identify any meaningful correlations between vaccine-induced CTL parameters and SIVmac239 acquisition rate or chronic-phase viral loads. Ultimately, 13 of 16 vaccinees (81%) and 7 of 16 controls (44%) became ECs (viremia ≤ 10,000 vRNA copies/mL plasma for ≥ 4 weeks). We identified subsets of immunomodulatory genes differentially expressed (DE) between RM groupings based on vaccination status, EC status, and MHC class I genotype. These DE genes function in multiple innate immune processes, including the complement system, cytokine/chemokine signaling, pattern recognition receptors, and interferon-mediated responses.DiscussionA striking difference in the kinetics of differential gene expression among our RM groups suggests that Mamu-B*08-associated elite control is characterized by a robust, rapid innate immune response that quickly resolves. These findings indicate that, despite the association between MHC class I genotype and elite control, innate immune factors in hyperacute SIV infection preceding CTL response development may facilitate the establishment of the EC phenotype.

Published

2024

4. Viral escape mutations do not account for non-protection from SIVmac239 challenge in RhCMV/SIV vaccinated rhesus macaques

Author

Benjamin N. Bimber, Justine Sunshine, G. W. McElfresh, Jason S. Reed, Reese Pathak, Katherine B. Bateman, Colette M. Hughes, Roxanne M. Gilbride, Julia C. Ford, David Morrow, Jeffrey D. Lifson, Jonah B. Sacha, Scott G. Hansen, and Louis J. Picker

Subjects

SIV, viral escape, CMV vaccine vector, viral sequence analysis, HIV/SIV, Immunologic diseases. Allergy, RC581-607

Abstract

Simian immunodeficiency virus (SIV) vaccines based upon 68-1 Rhesus Cytomegalovirus (RhCMV) vectors show remarkable protection against pathogenic SIVmac239 challenge. Across multiple independent rhesus macaque (RM) challenge studies, nearly 60% of vaccinated RM show early, complete arrest of SIVmac239 replication after effective challenge, whereas the remainder show progressive infection similar to controls. Here, we performed viral sequencing to determine whether the failure to control viral replication in non-protected RMs is associated with the acquisition of viral escape mutations. While low level viral mutations accumulated in all animals by 28 days-post-challenge, which is after the establishment of viral control in protected animals, the dominant circulating virus in virtually all unprotected RMs was nearly identical to the challenge stock, and there was no difference in mutation patterns between this cohort and unvaccinated controls. These data definitively demonstrate that viral mutation does not explain lack of viral control in RMs not protected by RhCMV/SIV vaccination. We further demonstrate that during chronic infection RhCMV/SIV vaccinated RMs do not acquire escape mutation in epitopes targeted by RhCMV/SIV, but instead display mutation in canonical MHC-Ia epitopes similar to unvaccinated RMs. This suggests that after the initial failure of viral control, unconventional T cell responses induced by 68-1 RhCMV/SIV vaccination do not exert strong selective pressure on systemically replicating SIV.

Published

2024

5. Early antiretroviral therapy in SIV-infected rhesus macaques reveals a multiphasic, saturable dynamic accumulation of the rebound competent viral reservoir

Author

Brandon F. Keele, Afam A. Okoye, Christine M. Fennessey, Benjamin Varco-Merth, Taina T. Immonen, Emek Kose, Andrew Conchas, Mykola Pinkevych, Leslie Lipkey, Laura Newman, Agatha Macairan, Marjorie Bosche, William J. Bosche, Brian Berkemeier, Randy Fast, Mike Hull, Kelli Oswald, Rebecca Shoemaker, Lorna Silipino, Robert J. Gorelick, Derick Duell, Alejandra Marenco, William Brantley, Jeremy Smedley, Michael Axthelm, Miles P. Davenport, Jeffrey D. Lifson, and Louis J. Picker

Subjects

Immunologic diseases. Allergy, RC581-607, Biology (General), QH301-705.5

Published

2024

6. Long-acting lenacapavir protects macaques against intravenous challenge with simian-tropic HIVResearch in context

Author

Adrienne E. Swanstrom, Robert J. Gorelick, Jorden L. Welker, Fabian Schmidt, Bing Lu, Kelly Wang, William Rowe, Matthew W. Breed, Kristin E. Killoran, Joshua A. Kramer, Duncan Donohue, James D. Roser, Paul D. Bieniasz, Theodora Hatziioannou, Cathi Pyle, James A. Thomas, Charles M. Trubey, Jim Zheng, Wade Blair, Stephen R. Yant, Jeffrey D. Lifson, and Gregory Q. Del Prete

Subjects

HIV, Pre-exposure prophylaxis, PrEP, Nonhuman primate, Macaque, Capsid, Medicine, Medicine (General), R5-920

Abstract

Summary: Background: Long-acting subcutaneous lenacapavir (LEN), a first-in-class HIV capsid inhibitor approved by the US FDA for the treatment of multidrug-resistant HIV-1 with twice yearly dosing, is under investigation for HIV-1 pre-exposure prophylaxis (PrEP). We previously derived a simian-tropic HIV-1 clone (stHIV-A19) that encodes an HIV-1 capsid and replicates to high titres in pigtail macaques (PTM), resulting in a nonhuman primate model well-suited for evaluating LEN PrEP in vivo. Methods: Lenacapavir potency against stHIV-A19 in PTM peripheral blood mononuclear cells in vitro was determined and subcutaneous LEN pharmacokinetics were evaluated in naïve PTMs in vivo. To evaluate the protective efficacy of LEN PrEP, naïve PTMs received either a single subcutaneous injection of LEN (25 mg/kg, N = 3) or vehicle (N = 4) 30 days before a high-dose intravenous challenge with stHIV-A19, or 7 daily subcutaneous injections of a 3-drug control PrEP regimen starting 3 days before stHIV-A19 challenge (N = 3). Findings: In vitro, LEN showed potent antiviral activity against stHIV-A19, comparable to its potency against HIV-1. In vivo, subcutaneous LEN displayed sustained plasma drug exposures in PTMs. Following stHIV-A19 challenge, while all vehicle control animals became productively infected, all LEN and 3-drug control PrEP animals were protected from infection. Interpretation: These findings highlight the utility of the stHIV-A19/PTM model and support the clinical development of long-acting LEN for PrEP in humans. Funding: Gilead Sciences as part of a Cooperative Research and Development Agreement between Gilead Sciences and Frederick National Lab; federal funds from the National Cancer Institute, National Institutes of Health, under Contract No. 75N91019D00024/HHSN261201500003I; NIH grant R01AI078788.

Published

2023

7. Molecular insights into antibody-mediated protection against the prototypic simian immunodeficiency virus

Author

Fangzhu Zhao, Zachary T. Berndsen, Nuria Pedreño-Lopez, Alison Burns, Joel D. Allen, Shawn Barman, Wen-Hsin Lee, Srirupa Chakraborty, Sandrasegaram Gnanakaran, Leigh M. Sewall, Gabriel Ozorowski, Oliver Limbo, Ge Song, Peter Yong, Sean Callaghan, Jessica Coppola, Kim L. Weisgrau, Jeffrey D. Lifson, Rebecca Nedellec, Thomas B. Voigt, Fernanda Laurino, Johan Louw, Brandon C. Rosen, Michael Ricciardi, Max Crispin, Ronald C. Desrosiers, Eva G. Rakasz, David I. Watkins, Raiees Andrabi, Andrew B. Ward, Dennis R. Burton, and Devin Sok

Subjects

Science

Abstract

SIVmac239 infection of macaques is a favored model of human HIV infection, but antibody-mediated protection for SIVmac239 is insufficiently understood. Here, Zhao and Berndsen et al isolated nAbs and confirmed protection against SIVmac239 infection in passive transfer studies in macaques. The nAb was used to provide the first high-resolution structure of a rhesus SIV trimer by CryoEM. Analysis of the glycosylation pattern of this SIV trimer suggests a denser glycan shield on Env for rhesus SIV compared to chimpanzee SIV or HIV-1, which partially explains the poor nAb response of rhesus macaques to SIVmac239 infection.

Published

2022

8. Limited impact of fingolimod treatment during the initial weeks of ART in SIV-infected rhesus macaques

Author

Maria Pino, Amélie Pagliuzza, M. Betina Pampena, Claire Deleage, Elise G. Viox, Kevin Nguyen, Inbo Shim, Adam Zhang, Justin L. Harper, Sadia Samer, Colin T. King, Barbara Cervasi, Kiran P. Gill, Stephanie Ehnert, Sherrie M. Jean, Michael L. Freeman, Jeffrey D. Lifson, Deanna Kulpa, Michael R. Betts, Nicolas Chomont, Michael M. Lederman, and Mirko Paiardini

Subjects

Science

Abstract

Although antiretroviral therapy (ART) is able to successfully suppress plasma viremia in most people living with HIV, ART withdrawal typically results in viral replication and rebound. Authors investigate the effect, in terms of delay in viral replication, and immune cell dynamics in lymphoid tissue, of fingolimod (FTY720) administration at the time of ART initiation in SIV-infected rhesus macaques.

Published

2022

9. Rapamycin limits CD4+ T cell proliferation in simian immunodeficiency virus–infected rhesus macaques on antiretroviral therapy

Author

Benjamin D. Varco-Merth, William Brantley, Alejandra Marenco, Derick D. Duell, Devin N. Fachko, Brian Richardson, Kathleen Busman-Sahay, Danica Shao, Walter Flores, Kathleen Engelman, Yoshinori Fukazawa, Scott W. Wong, Rebecca L. Skalsky, Jeremy Smedley, Michael K. Axthelm, Jeffrey D. Lifson, Jacob D. Estes, Paul T. Edlefsen, Louis J. Picker, Cheryl M.A. Cameron, Timothy J. Henrich, and Afam A. Okoye

Subjects

AIDS/HIV, Medicine

Abstract

Proliferation of latently infected CD4+ T cells with replication-competent proviruses is an important mechanism contributing to HIV persistence during antiretroviral therapy (ART). One approach to targeting this latent cell expansion is to inhibit mTOR, a regulatory kinase involved with cell growth, metabolism, and proliferation. Here, we determined the effects of chronic mTOR inhibition with rapamycin with or without T cell activation in SIV-infected rhesus macaques (RMs) on ART. Rapamycin perturbed the expression of multiple genes and signaling pathways important for cellular proliferation and substantially decreased the frequency of proliferating CD4+ memory T cells (TM cells) in blood and tissues. However, levels of cell-associated SIV DNA and SIV RNA were not markedly different between rapamycin-treated RMs and controls during ART. T cell activation with an anti-CD3LALA antibody induced increases in SIV RNA in plasma of RMs on rapamycin, consistent with SIV production. However, upon ART cessation, both rapamycin and CD3LALA–treated and control-treated RMs rebounded in less than 12 days, with no difference in the time to viral rebound or post-ART viral load set points. These results indicate that, while rapamycin can decrease the proliferation of CD4+ TM cells, chronic mTOR inhibition alone or in combination with T cell activation was not sufficient to disrupt the stability of the SIV reservoir.

Published

2022

10. Highly Efficient Autologous HIV-1 Isolation by Coculturing Macrophage With Enriched CD4+ T Cells From HIV-1 Patients

Author

Cristina Xufré, Tanía González, Lorna Leal, Charles M. Trubey, Jeffrey D. Lifson, José María Gatell, José Alcamí, Núria Climent, Felipe García, and Sonsoles Sánchez-Palomino

Subjects

autologous HIV immunogen, HIV isolation, HIV therapeutic vaccine, CD4+ T cells, coculture, monocyte-derived macrophages (MDM), Microbiology, QR1-502

Abstract

We described a novel HIV autologous isolation method based in coculturing macrophages and CD4+T-cell-enriched fractions from peripheral blood collected from antiretroviral-treated (ART) HIV patients. This method allows the isolation of high viral titers of autologous viruses, over 1010HIV RNA copies/ml, and reduces the time required to produce necessary amounts for virus for use as antigens presented by monocyte-derived myeloid cells in HIV therapeutic vaccine approaches. By applying these high titer and autologous virus produced in the patient-derived cells, we intended to elicit a boost of the immunological system response in HIV therapeutic vaccines in clinical trials.

Published

2022

11. Induction of Transient Virus Replication Facilitates Antigen-Independent Isolation of SIV-Specific Monoclonal Antibodies

Author

Nuria Pedreño-Lopez, Christine M. Dang, Brandon C. Rosen, Michael J. Ricciardi, Varian K. Bailey, Martin J. Gutman, Lucas Gonzalez-Nieto, Matthias G. Pauthner, Khoa Le, Ge Song, Raiees Andrabi, Kim L. Weisgrau, Nicholas Pomplun, José M. Martinez-Navio, Sebastian P. Fuchs, Jens Wrammert, Eva G. Rakasz, Jeffrey D. Lifson, Mauricio A. Martins, Dennis R. Burton, David I. Watkins, and Diogo M. Magnani

Subjects

Genetics, QH426-470, Cytology, QH573-671

Abstract

Structural characterization of the HIV-1 Envelope (Env) glycoprotein has facilitated the development of Env probes to isolate HIV-specific monoclonal antibodies (mAbs). However, preclinical studies have largely evaluated these virus-specific mAbs against chimeric viruses, which do not naturally infect non-human primates, in contrast to the unconstrained simian immunodeficiency virus (SIV)mac239 clone. Given the paucity of native-like reagents for the isolation of SIV-specific B cells, we examined a method to isolate SIVmac239-specific mAbs without using Env probes. We first activated virus-specific B cells by inducing viral replication after the infusion of a CD8β-depleting mAb or withdrawal of antiretroviral therapy in SIVmac239-infected rhesus macaques. Following the rise in viremia, we observed 2- to 4-fold increases in the number of SIVmac239 Env-reactive plasmablasts in circulation. We then sorted these activated B cells and obtained 206 paired Ab sequences. After expressing 122 mAbs, we identified 14 Env-specific mAbs. While these Env-specific mAbs bound to both the SIVmac239 SOSIP.664 trimer and to infected primary rhesus CD4+ T cells, five also neutralized SIVmac316. Unfortunately, none of these mAbs neutralized SIVmac239. Our data show that this method can be used to isolate virus-specific mAbs without antigenic probes by inducing bursts of contemporary replicating viruses in vivo. Keywords: SIV, monoclonal antibodies, rhesus macaques, CD8b depletion, antiretroviral therapy interruption

Published

2020

12. Low-level alternative tRNA priming of reverse transcription of HIV-1 and SIV in vivo

Author

Christine M. Fennessey, Celine Camus, Taina T. Immonen, Carolyn Reid, Frank Maldarelli, Jeffrey D. Lifson, and Brandon F. Keele

Subjects

SIV, HIV, Primer binding site, tRNA, Next-generation deep-sequencing, Immunologic diseases. Allergy, RC581-607

Abstract

Abstract Background Reverse transcription (RT) of HIV and SIV is initiated by the binding of the acceptor stem of tRNALys3 to the primer binding site (PBS) of the viral RNA genome. Previous studies have suggested that this tRNALys3 is not the only molecule capable of priming reverse transcription, and that at least one other lysyl tRNA, tRNALys5, which has an acceptor stem sequence varying from tRNALys3 by only a single transition mutation resulting in the integration of a thymine (T) at position 8 of the PBS in the viral genome, can prime reverse transcription. Results We undertook an unbiased approach, evaluating the primer binding site by deep-sequencing of HIV and SIV directly from the plasma of 15 humans and 11 macaques. We found that in humans there are low but measurable levels of viral RNA genomes harboring a PBS containing the noncanonical T at position 8 (PBS-Lys5) corresponding to the tRNAlys5 sequence and representing an average of 0.52% (range 0.07–1.6%) of the total viral population. This value is remarkably consistent with the proportion of PBS-Lys5 we identified in a cross-sectional assessment of the LANL HIV database (0.51%). In macaques chronically infected with SIVmac239, the PBS-Lys5 was also detected but at a frequency 1-log less than seen for HIV, with an average of 0.056% (range 0.01–0.09%). At this proportion, PBS-Lys5 was comparable to other transition mutations, making it impossible to determine whether the mutation observed is a result of use of tRNALys5 as an RT primer at very low levels or merely the product of in vitro cDNA synthesis/PCR error. We also identified two novel PBS sequences in HIV and SIV at low levels in vivo corresponding to tRNALys6 and tRNALys1,2, suggesting that these tRNAs may rarely also be used to prime RT. In vivo reversion of the PBS-Lys5 found in SIVmac239 was rapid and reached background levels by 30 days post-infection. Conclusions We conclude that while alternative tRNAs can initiate reverse transcription of HIV and SIV in vivo, their overall contributions to the replicating viral population are small.

Published

2019

13. Non-neutralizing Antibodies May Contribute to Suppression of SIVmac239 Viremia in Indian Rhesus Macaques

Author

Nuria Pedreño-Lopez, Brandon C. Rosen, Walter J. Flores, Matthew J. Gorman, Thomas B. Voigt, Michael J. Ricciardi, Kristin Crosno, Kim L. Weisgrau, Christopher L. Parks, Jeffrey D. Lifson, Galit Alter, Eva G. Rakasz, Diogo M. Magnani, Mauricio A. Martins, and David I. Watkins

Subjects

non-neutralizing antibodies, SIV, rhesus macaques (Macaca mulatta), immunoadsorption, anti-FcRn Ab, adoptive transfer, Immunologic diseases. Allergy, RC581-607

Abstract

The antiviral properties of broadly neutralizing antibodies against HIV are well-documented but no vaccine is currently able to elicit protective titers of these responses in primates. While current vaccine modalities can readily induce non-neutralizing antibodies against simian immunodeficiency virus (SIV) and HIV, the ability of these responses to restrict lentivirus transmission and replication remains controversial. Here, we investigated the antiviral properties of non-neutralizing antibodies in a group of Indian rhesus macaques (RMs) that were vaccinated with vif, rev, tat, nef, and env, as part of a previous study conducted by our group. These animals manifested rapid and durable control of viral replication to below detection limits shortly after SIVmac239 infection. Although these animals had no serological neutralizing activity against SIVmac239 prior to infection, their pre-challenge titers of Env-binding antibodies correlated with control of viral replication. To assess the contribution of anti-Env humoral immune responses to virologic control in two of these animals, we transiently depleted their circulating antibodies via extracorporeal plasma immunoadsorption and inhibition of IgG recycling through antibody-mediated blockade of the neonatal Fc receptor. These procedures reduced Ig serum concentrations by up to 80% and temporarily induced SIVmac239 replication in these animals. Next, we transferred purified total Ig from the rapid controllers into six vaccinated RMs one day before intrarectal challenge with SIVmac239. Although recipients of the hyperimmune anti-SIV Ig fraction were not protected from infection, their peak and chronic phase viral loads were significantly lower than those in concurrent unvaccinated control animals. Together, our results suggest that non-neutralizing Abs may play a role in the suppression of SIVmac239 viremia.

Published

2021

14. Long-Term Delivery of an Anti-SIV Monoclonal Antibody With AAV

Author

José M. Martinez-Navio, Sebastian P. Fuchs, Desiree E. Mendes, Eva G. Rakasz, Guangping Gao, Jeffrey D. Lifson, and Ronald C. Desrosiers

Subjects

gene therapy, AAV vector, long-term expression, broadly neutralizing antibodies, HIV/SIV cure, immunotherapy, Immunologic diseases. Allergy, RC581-607

Abstract

Long-term delivery of anti-HIV monoclonal antibodies using adeno-associated virus (AAV) holds promise for the prevention and treatment of HIV infection. We previously reported that after receiving a single administration of AAV vector coding for anti-SIV antibody 5L7, monkey 84-05 achieved high levels of AAV-delivered 5L7 IgG1 in vivo which conferred sterile protection against six successive, escalating dose, intravenous challenges with highly infectious, highly pathogenic SIVmac239, including a final challenge with 10 animal infectious doses (1). Here we report that monkey 84-05 has successfully maintained 240–350 μg/ml of anti-SIV antibody 5L7 for over 6 years. Approximately 2% of the circulating IgG in this monkey is this one monoclonal antibody. This monkey generated little or no anti-drug antibodies (ADA) to the AAV-delivered antibody for the duration of the study. Due to the nature of the high-dose challenge used and in order to rule out a potential low-level infection not detected by regular viral loads, we have used ultrasensitive techniques to detect cell-associated viral DNA and RNA in PBMCs from this animal. In addition, we have tested serum from 84-05 by ELISA against overlapping peptides spanning the whole envelope sequence for SIVmac239 (PepScan) and against recombinant p27 and gp41 proteins. No reactivity has been detected in the ELISAs indicating the absence of naturally arising anti-SIV antibodies; moreover, the ultrasensitive cell-associated viral tests yielded no positive reaction. We conclude that macaque 84-05 was effectively protected and remained uninfected. Our data show that durable, continuous antibody expression can be achieved after one single administration of AAV and support the potential for lifelong protection against HIV from a single vector administration.

Published

2020

15. Griffithsin carrageenan fast dissolving inserts prevent SHIV HSV-2 and HPV infections in vivo

Author

Nina Derby, Manjari Lal, Meropi Aravantinou, Larisa Kizima, Patrick Barnable, Aixa Rodriguez, Manshun Lai, Asa Wesenberg, Shweta Ugaonkar, Keith Levendosky, Olga Mizenina, Kyle Kleinbeck, Jeffrey D. Lifson, M. Melissa Peet, Zachary Lloyd, Michael Benson, Walid Heneine, Barry R O’Keefe, Melissa Robbiani, Elena Martinelli, Brooke Grasperge, James Blanchard, Agegnehu Gettie, Natalia Teleshova, José A. Fernández-Romero, and Thomas M. Zydowsky

Subjects

Science

Abstract

Safety and efficacy remain important challenges for non-antiretroviral-based microbicides. Here, Derby et al. show that a Griffithsin-Carrageenan fast dissolving vaginal insert provides on-demand protection against SHIV infections in macaques, paving the way for the development of pre-exposure prophylaxis on-demand products.

Published

2018

16. Defining HIV and SIV Reservoirs in Lymphoid Tissues

Author

Claire Deleage, Stephen W. Wietgrefe, Gregory Del Prete, David R. Morcock, Xing-Pei Hao, Michael Piatak, Jr., Julian Bess, Jodi L. Anderson, Katherine Perkey, Cavan Reilly, Joseph M. McCune, Ashley T. Haase, Jeffrey D. Lifson, Timothy W. Schacker, and Jacob D. Estes

Subjects

HIV, SIV, Reservoir, Follicular Dendritic Cells, B cell follicles, In situ hybridization, RNAscope, DNAscope, Pathology, RB1-214, Immunologic diseases. Allergy, RC581-607

Abstract

A primary obstacle to an HIV-1 cure is long-lived viral reservoirs, which must be eliminated or greatly reduced. Cure strategies have largely focused on monitoring changes in T cell reservoirs in peripheral blood (PB), even though the lymphoid tissues (LT) are primary sites for viral persistence. To track and discriminate viral reservoirs within tissue compartments we developed a specific and sensitive next-generation in situ hybridization approach to detect vRNA, including vRNA+ cells and viral particles (“RNAscope”), vDNA+ cells (“DNAscope”) and combined vRNA and vDNA with immunohistochemistry to detect and phenotype active and latently infected cells in the same tissue section. RNAscope is highly sensitive with greater speed of analysis compared to traditional in situ hybridization. Highly sensitive and specific DNAscope detected SIV/HIV vDNA+ cells, including duplexed detection of vDNA and vRNA or immunophenotypic markers in the same section. Analysis of LT samples from macaques prior to and during combination antiretroviral therapy demonstrated that B cell follicles are an important anatomical compartment for both latent and active viral persistence during treatment. These new tools should allow new insights into viral reservoir biology and evaluation of cure strategies.

Published

2016

17. Experimental Oral Herpes Simplex Virus-1 (HSV-1) Co-infection in Simian Immunodeficiency Virus (SIV)-Infected Rhesus Macaques

Author

Meropi Aravantinou, Olga Mizenina, Giulia Calenda, Jessica Kenney, Ines Frank, Jeffrey D. Lifson, Moriah Szpara, Lichen Jing, David M. Koelle, Natalia Teleshova, Brooke Grasperge, James Blanchard, Agegnehu Gettie, Elena Martinelli, and Nina Derby

Subjects

HSV-1, SIV, non-human primate model, oral infection, immune response, Microbiology, QR1-502

Abstract

Herpes simplex virus 1 and 2 (HSV-1/2) similarly initiate infection in mucosal epithelia and establish lifelong neuronal latency. Anogenital HSV-2 infection augments the risk for sexual human immunodeficiency virus (HIV) transmission and is associated with higher HIV viral loads. However, whether oral HSV-1 infection contributes to oral HIV susceptibility, viremia, or oral complications of HIV infection is unknown. Appropriate non-human primate (NHP) models would facilitate this investigation, yet there are no published studies of HSV-1/SIV co-infection in NHPs. Thus, we performed a pilot study for an oral HSV-1 infection model in SIV-infected rhesus macaques to describe the feasibility of the modeling and resultant immunological changes. Three SIV-infected, clinically healthy macaques became HSV-1-infected by inoculation with 4 × 108 pfu HSV-1 McKrae on buccal, tongue, gingiva, and tonsils after gentle abrasion. HSV-1 DNA was shed in oral swabs for up to 21 days, and shedding recurred in association with intra-oral lesions after periods of no shedding during 56 days of follow up. HSV-1 DNA was detected in explant cultures of trigeminal ganglia collected at euthanasia on day 56. In the macaque with lowest baseline SIV viremia, SIV plasma RNA increased following HSV-1 infection. One macaque exhibited an acute pro-inflammatory response, and all three animals experienced T cell activation and mobilization in blood. However, T cell and antibody responses to HSV-1 were low and atypical. Through rigorous assessesments, this study finds that the virulent HSV-1 strain McKrae resulted in a low level HSV-1 infection that elicited modest immune responses and transiently modulated SIV infection.

Published

2017

18. Programming cytomegalovirus as an HIV vaccine

Author

Louis J. Picker, Jeffrey D. Lifson, Michael Gale, Scott G. Hansen, and Klaus Früh

Subjects

Immunology, Immunology and Allergy

Published

2023

19. Lymphoid tissues contribute to viral clonotypes present in plasma at early post-ATI in SIV-infected rhesus macaques

Author

Antonio Solis-Leal, Nongthombam Boby, Suvadip Mallick, Yilun Cheng, Fei Wu, Grey De La Torre, Jason Dufour, Xavier Alvarez, Vinay Shivanna, Yaozhong Liu, Christine M Fennessey, Jeffrey D Lifson, Qingsheng Li, Brandon F Keele, and Binhua Ling

Subjects

Article

Abstract

The rebound-competent viral reservoir (RCVR), comprised of virus that is able to persist during antiretroviral therapy (ART) and mediate reactivation of systemic viral replication and rebound viremia after antiretroviral therapy interruption (ATI), remains the biggest obstacle to the eradication of HIV infection. A better understanding of the cellular and tissue origins and the dynamics of viral populations that initiate rebound upon ATI could help develop targeted therapeutic strategies for reducing the RCVR. In this study, barcoded SIVmac239M was used to infect rhesus macaques to enable monitoring of viral barcode clonotypes contributing to virus detectable in plasma after ATI. Blood, lymphoid tissues (LTs, spleen, mesenteric and inguinal lymph nodes), and non-lymphoid tissues (NLTs, colon, ileum, lung, liver, and brain) were analyzed using viral barcode sequencing, intact proviral DNA assay, single-cell RNA sequencing, and combined CODEX/RNAscope/ in situ hybridization. Four of seven animals had viral barcodes detectable by deep sequencing of plasma at necropsy although plasma viral RNA remained < 22 copies/mL. Among the tissues studied, mesenteric and inguinal lymph nodes, and spleen contained viral barcodes detected in plasma, and trended to have higher cell-associated viral loads, higher intact provirus levels, and greater diversity of viral barcodes. CD4+ T cells were the main cell type harboring viral RNA (vRNA) after ATI. Further, T cell zones in LTs showed higher vRNA levels than B cell zones for most animals. These findings are consistent with LTs contributing to virus present in plasma early after ATI. ONE SENTENCE SUMMARY: The reemerging of SIV clonotypes at early post-ATI are likely from the secondary lymphoid tissues.

Published

2023

20. SIV clearance from neonatal macaques following transient CCR5 depletion

Author

Jesse D. Deere, David Merriam, Kawthar Machmach Leggat, Wen-Lan William Chang, Gema Méndez-Lagares, Hung Kieu, Joseph Dutra, Justin Fontaine, Wenze Lu, Ning Chin, Connie Chen, Bryant Chi-Thien Tran, Jessica Salinas, Corey N. Miller, Steven G. Deeks, Jeffrey D. Lifson, Kathleen Engelman, Diogo Magnani, Keith Reimann, Mario Stevenson, and Dennis J. Hartigan-O’Connor

Subjects

Article

Abstract

SUMMARY PARAGRAPHTreatment of people with HIV (PWH) with antiretroviral therapy (ART) results in sustained suppression of viremia, but HIV persists indefinitely as integrated provirus in CD4-expressing cells. Intact persistent provirus, the “rebound competent viral reservoir” (RCVR), is the primary obstacle to achieving a cure. Most variants of HIV enter CD4+T cells by binding to the chemokine receptor, CCR5. The RCVR has been successfully depleted only in a handful of PWH following cytotoxic chemotherapy and bone marrow transplantation from donors with a mutation inCCR5. Here we show that long-term SIV remission and apparent cure can be achieved for infant macaques via targeted depletion of potential reservoir cells that express CCR5. Neonatal rhesus macaques were infected with virulent SIVmac251, then treated with ART beginning one week after infection, followed by treatment with either a CCR5/CD3-bispecific or a CD4-specific antibody, both of which depleted target cells and increased the rate of plasma viremia decrease. Upon subsequent cessation of ART, three of seven animals treated with CCR5/CD3-bispecific antibody rebounded quickly and two rebounded 3 or 6 months later. Remarkably, the other two animals remained aviremic and efforts to detect replication-competent virus were unsuccessful. Our results show that bispecific antibody treatment can achieve meaningful SIV reservoir depletion and suggest that functional HIV cure might be achievable for recently infected individuals having a restricted reservoir.

Published

2023

21. Myeloid cell tropism enables MHC-E-restricted CD8(+) T cell priming and vaccine efficacy by the RhCMV/SIV vaccine

Author

Scott G. Hansen, Meaghan H. Hancock, Daniel Malouli, Emily E. Marshall, Colette M. Hughes, Kurt T. Randall, David Morrow, Julia C. Ford, Roxanne M. Gilbride, Andrea N. Selseth, Renee Espinosa Trethewy, Lindsey M. Bishop, Kelli Oswald, Rebecca Shoemaker, Brian Berkemeier, William J. Bosche, Michael Hull, Lorna Silipino, Michael Nekorchuk, Kathleen Busman-Sahay, Jacob D. Estes, Michael K. Axthelm, Jeremy Smedley, Danica Shao, Paul T. Edlefsen, Jeffrey D. Lifson, Klaus Früh, Jay A. Nelson, and Louis J. Picker

Subjects

Immunology, SAIDS Vaccines, Simian Acquired Immunodeficiency Syndrome, Cytomegalovirus, Vaccine Efficacy, General Medicine, CD8-Positive T-Lymphocytes, Macaca mulatta, Tropism, Article, Major Histocompatibility Complex, Cytomegalovirus Vaccines, Epitopes, MicroRNAs, Animals, Myeloid Cells, Simian Immunodeficiency Virus

Abstract

The strain 68-1 rhesus cytomegalovirus (RhCMV)–based vaccine for simian immunodeficiency virus (SIV) can stringently protect rhesus macaques (RMs) from SIV challenge by arresting viral replication early in primary infection. This vaccine elicits unconventional SIV-specific CD8 + T cells that recognize epitopes presented by major histocompatibility complex (MHC)–II and MHC-E instead of MHC-Ia. Although RhCMV/SIV vaccines based on strains that only elicit MHC-II– and/or MHC-Ia–restricted CD8 + T cells do not protect against SIV, it remains unclear whether MHC-E–restricted T cells are directly responsible for protection and whether these responses can be separated from the MHC-II–restricted component. Using host microRNA (miR)–mediated vector tropism restriction, we show that the priming of MHC-II and MHC-E epitope–targeted responses depended on vector infection of different nonoverlapping cell types in RMs. Selective inhibition of RhCMV infection in myeloid cells with miR-142–mediated tropism restriction eliminated MHC-E epitope–targeted CD8 + T cell priming, yielding an exclusively MHC-II epitope–targeted response. Inhibition with the endothelial cell–selective miR-126 eliminated MHC-II epitope–targeted CD8 + T cell priming, yielding an exclusively MHC-E epitope–targeted response. Dual miR-142 + miR-126–mediated tropism restriction reverted CD8 + T cell responses back to conventional MHC-Ia epitope targeting. Although the magnitude and differentiation state of these CD8 + T cell responses were generally similar, only the vectors programmed to elicit MHC-E–restricted CD8 + T cell responses provided protection against SIV challenge, directly demonstrating the essential role of these responses in RhCMV/SIV vaccine efficacy.

Published

2022

22. CTLA-4 and PD-1 dual blockade induces SIV reactivation without control of rebound after antiretroviral therapy interruption

Author

Jenna Read, Colin T. King, Maria Pino, Mirko Paiardini, Heather Amrine-Madsen, Michael Nekorchuk, Chi Ngai Chan, Cristin M. Galardi, Hong Wang, James Schawalder, Katharine J. Bar, A. Alicia Koblansky, Colleen S. McGary, Kevin Nguyen, Jacob D. Estes, Sherrie Jean, Samuel L. M. Raines, Shane D. Falcinelli, Jeffrey D. Lifson, Shari Gordon, Luca Micci, Guido Silvestri, Andrew Sanderson, Justin L. Harper, Brian Johns, David Favre, Emily Lindemuth, Kathleen Busman-Sahay, Barbara Cervasi, and David M. Margolis

Subjects

0301 basic medicine, biology, business.industry, T cell, General Medicine, General Biochemistry, Genetics and Molecular Biology, Immune checkpoint, Blockade, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, CTLA-4, 030220 oncology & carcinogenesis, Immunology, medicine, biology.protein, Cytotoxic T cell, Antibody, business, CD8, B cell

Abstract

The primary human immunodeficiency virus (HIV) reservoir is composed of resting memory CD4+ T cells, which often express the immune checkpoint receptors programmed cell death protein 1 (PD-1) and cytotoxic T lymphocyte-associated protein 4 (CTLA-4), which limit T cell activation via synergistic mechanisms. Using simian immunodeficiency virus (SIV)-infected, long-term antiretroviral therapy (ART)-treated rhesus macaques, we demonstrate that PD-1, CTLA-4 and dual CTLA-4/PD-1 immune checkpoint blockade using monoclonal antibodies is well tolerated, with evidence of bioactivity in blood and lymph nodes. Dual blockade was remarkably more effective than PD-1 blockade alone in enhancing T cell cycling and differentiation, expanding effector-memory T cells and inducing robust viral reactivation in plasma and peripheral blood mononuclear cells. In lymph nodes, dual CTLA-4/PD-1 blockade, but not PD-1 alone, decreased the total and intact SIV-DNA in CD4+ T cells, and SIV-DNA and SIV-RNA in B cell follicles, a major site of viral persistence during ART. None of the tested interventions enhanced SIV-specific CD8+ T cell responses during ART or viral control after ART interruption. Thus, despite CTLA-4/PD-1 blockade inducing robust latency reversal and reducing total levels of integrated virus, the degree of reservoir clearance was still insufficient to achieve viral control. These results suggest that immune checkpoint blockade regimens targeting PD-1 and/or CTLA-4, if performed in people living with HIV with sustained aviremia, are unlikely to induce HIV remission in the absence of additional interventions.

Published

2020

23. Induction of Transient Virus Replication Facilitates Antigen-Independent Isolation of SIV-Specific Monoclonal Antibodies

Author

Jeffrey D. Lifson, Eva G. Rakasz, Brandon C. Rosen, Khoa Le, Mauricio A. Martins, Lucas Gonzalez-Nieto, Raiees Andrabi, Michael J. Ricciardi, Nicholas Pomplun, Martin J. Gutman, José M. Martinez-Navio, Sebastian P. Fuchs, Varian K. Bailey, Christine M. Dang, David I. Watkins, Kim L. Weisgrau, Ge Song, Diogo M. Magnani, Matthias Pauthner, Jens Wrammert, Dennis R. Burton, and Nuria Pedreño-Lopez

Subjects

0301 basic medicine, lcsh:QH426-470, medicine.drug_class, viruses, Viremia, Biology, medicine.disease_cause, Monoclonal antibody, Article, CD8b depletion, rhesus macaques, 03 medical and health sciences, 0302 clinical medicine, Antigen, Genetics, medicine, lcsh:QH573-671, Molecular Biology, chemistry.chemical_classification, lcsh:Cytology, virus diseases, Simian immunodeficiency virus, medicine.disease, Virology, Antiretroviral therapy, 3. Good health, lcsh:Genetics, 030104 developmental biology, SIV, Viral replication, chemistry, 030220 oncology & carcinogenesis, Molecular Medicine, monoclonal antibodies, antiretroviral therapy interruption, Clone (B-cell biology), Glycoprotein

Abstract

Structural characterization of the HIV-1 Envelope (Env) glycoprotein has facilitated the development of Env probes to isolate HIV-specific monoclonal antibodies (mAbs). However, preclinical studies have largely evaluated these virus-specific mAbs against chimeric viruses, which do not naturally infect non-human primates, in contrast to the unconstrained simian immunodeficiency virus (SIV)mac239 clone. Given the paucity of native-like reagents for the isolation of SIV-specific B cells, we examined a method to isolate SIVmac239-specific mAbs without using Env probes. We first activated virus-specific B cells by inducing viral replication after the infusion of a CD8β-depleting mAb or withdrawal of antiretroviral therapy in SIVmac239-infected rhesus macaques. Following the rise in viremia, we observed 2- to 4-fold increases in the number of SIVmac239 Env-reactive plasmablasts in circulation. We then sorted these activated B cells and obtained 206 paired Ab sequences. After expressing 122 mAbs, we identified 14 Env-specific mAbs. While these Env-specific mAbs bound to both the SIVmac239 SOSIP.664 trimer and to infected primary rhesus CD4+ T cells, five also neutralized SIVmac316. Unfortunately, none of these mAbs neutralized SIVmac239. Our data show that this method can be used to isolate virus-specific mAbs without antigenic probes by inducing bursts of contemporary replicating viruses in vivo. Keywords: SIV, monoclonal antibodies, rhesus macaques, CD8b depletion, antiretroviral therapy interruption

Published

2020

24. Pembrolizumab induces HIV latency reversal in people living with HIV and cancer on antiretroviral therapy

Author

Thomas S. Uldrick, Scott V. Adams, Remi Fromentin, Michael Roche, Steven P. Fling, Priscila H. Gonçalves, Kathryn Lurain, Ramya Ramaswami, Chia-ching Jackie Wang, Robert J. Gorelick, Jorden L. Welker, Liz O’Donoghue, Harleen Choudhary, Jeffrey D. Lifson, Thomas A. Rasmussen, Ajantha Rhodes, Carolin Tumpach, Robert Yarchoan, Frank Maldarelli, Martin A. Cheever, Rafick Sékaly, Nicolas Chomont, Steven G. Deeks, and Sharon R. Lewin

Subjects

CD4-Positive T-Lymphocytes, Programmed Cell Death 1 Receptor, virus diseases, HIV Infections, General Medicine, Biological Sciences, Antibodies, Monoclonal, Humanized, Medical and Health Sciences, Antibodies, Article, Virus Latency, Infectious Diseases, Neoplasms, Monoclonal, Genetics, HIV-1, HIV/AIDS, 2.2 Factors relating to the physical environment, Humans, RNA, Aetiology, Infection, Humanized, Phylogeny, Cancer

Abstract

In people living with HIV (PLWH) on antiretroviral therapy (ART), virus persists in a latent form where there is minimal transcription or protein expression. Latently infected cells are a major barrier to curing HIV. Increasing HIV transcription and viral production in latently infected cells could facilitate immune recognition and reduce the pool of infected cells that persist on ART. Given that programmed cell death protein 1 (PD-1) expressing CD4 + T cells are preferentially infected with HIV in PLWH on ART, we aimed to determine whether administration of antibodies targeting PD-1 would reverse HIV latency in vivo. We therefore evaluated the impact of intravenous administration of pembrolizumab every 3 weeks on HIV latency in 32 PLWH and cancer on ART. After the first infusion of anti–PD-1, we observed a median 1.32-fold increase in unspliced HIV RNA and 1.61-fold increase in unspliced RNA:DNA ratio in sorted blood CD4 + T cells compared to baseline. We also observed a 1.65-fold increase in plasma HIV RNA. The frequency of CD4 + T cells with inducible virus evaluated using the tat/rev limiting dilution assay was higher after 6 cycles compared to baseline. Phylogenetic analyses of HIV env sequences in a participant who developed low concentrations of HIV viremia after 6 cycles of pembrolizumab did not demonstrate clonal expansion of HIV-infected cells. These data are consistent with anti–PD-1 being able to reverse HIV latency in vivo and support the rationale for combining anti–PD-1 with other interventions to reduce the HIV reservoir.

Published

2022

25. The ingenol-based protein kinase C agonist GSK445A is a potent inducer of HIV and SIV RNA transcription

Author

Afam A. Okoye, Rémi Fromentin, Hiroshi Takata, Jessica H. Brehm, Yoshinori Fukazawa, Bryan Randall, Marion Pardons, Vincent Tai, Jun Tang, Jeremy Smedley, Michael Axthelm, Jeffrey D. Lifson, Louis J. Picker, David Favre, Lydie Trautmann, and Nicolas Chomont

Subjects

CD4(+) T-CELLS, RNA viruses, Transcription, Genetic, REVERSAL, Physiology, viruses, Pathology and Laboratory Medicine, Memory T cells, White Blood Cells, ANTIRETROVIRAL THERAPY, Immunodeficiency Viruses, Animal Cells, ANIMAL-MODEL, IN-VIVOACTIVATION, Medicine and Health Sciences, Biology (General), RHESUS MACAQUE RHADINOVIRUS, Protein Kinase C, LATENT-VIRUS REACTIVATION, T Cells, virus diseases, Virus Latency, Body Fluids, Viral Persistence and Latency, PROSTRATIN, Blood, SIV, Medical Microbiology, Viral Pathogens, Viruses, RNA, Viral, Simian Immunodeficiency Virus, Diterpenes, Cellular Types, Pathogens, Anatomy, Research Article, QH301-705.5, Immune Cells, Immunology, Cytotoxic T cells, Microbiology, Blood Plasma, Virology, Retroviruses, Genetics, Animals, Humans, Microbial Pathogens, Molecular Biology, Blood Cells, Lentivirus, Organisms, HIV, Biology and Life Sciences, Cell Biology, RC581-607, Macaca mulatta, Viral Replication, INFECTED INDIVIDUALS, Virus Activation, Parasitology, Immunologic diseases. Allergy

Abstract

Activation of the NF-κB signaling pathway by Protein Kinase C (PKC) agonists is a potent mechanism for human immunodeficiency virus (HIV) latency disruption in vitro. However, significant toxicity risks and the lack of evidence supporting their activity in vivo have limited further evaluation of PKC agonists as HIV latency-reversing agents (LRA) in cure strategies. Here we evaluated whether GSK445A, a stabilized ingenol-B derivative, can induce HIV/simian immunodeficiency virus (SIV) transcription and virus production in vitro and demonstrate pharmacological activity in nonhuman primates (NHP). CD4+ T cells from people living with HIV and from SIV+ rhesus macaques (RM) on antiretroviral therapy (ART) exposed in vitro to 25 nM of GSK445A produced cell-associated viral transcripts as well as viral particles at levels similar to those induced by PMA/Ionomycin, indicating that GSK445A can potently reverse HIV/SIV latency. Importantly, these concentrations of GSK445A did not impair the proliferation or survival of HIV-specific CD8+ T cells, but instead, increased their numbers and enhanced IFN-γ production in response to HIV peptides. In vivo, GSK445A tolerability was established in SIV-naïve RM at 15 μg/kg although tolerability was reduced in SIV-infected RM on ART. Increases in plasma viremia following GSK445A administration were suggestive of increased SIV transcription in vivo. Collectively, these results indicate that GSK445A is a potent HIV/SIV LRA in vitro and has a tolerable safety profile amenable for further evaluation in vivo in NHP models of HIV cure/remission., Author summary Antiretroviral therapy (ART) is not a definitive cure for HIV infection, in part, because the virus is able to integrate its genetic material in the host cell and remain in a dormant but fully replication-competent form during ART. These latently-infected cells can persist for long periods of time and remain hidden from the host’s immune system. If ART is stopped, the virus can reactivate from this pool of infected cells and resume HIV replication and disease progression. As such, finding and eliminating cells with latent HIV infection is priority for HIV cure research. One approach is to use compounds referred to as latency-reversing agents, that can induce HIV reactivation during ART. The goal of this approach is to facilitate elimination of infected cells by the virus itself once it reactivates or by the host’s immune system, once virus induction renders the cells detectable by the immune system, while also preventing the virus from infecting new cells due to the continued presence of ART. In this study we report on the activity of a novel latency-reversing agent called GSK445A, a potent activator of the enzyme protein kinase C (PKC). We show that GSK445A can induce HIV and simian immunodeficiency virus (SIV) latency reversal in vitro and has a tolerable saftey profile in nonhuman primates that should permit further testing of this PKC-agonist in strategies to cure HIV.

Published

2022

26. Role of IL-15 Signaling in the Pathogenesis of Simian Immunodeficiency Virus Infection in Rhesus Macaques

Author

Rebecca L. Skalsky, Scott W. Wong, Derick M. Duell, Lina Gao, Richard Lum, Michael K. Axthelm, Audrie L. Konfe, Maren Q. DeGottardi, Afam A. Okoye, Devin N. Fachko, Mukta Vaidya, He Li, Byung Park, Louis J. Picker, Yoshinori Fukazawa, Chike O. Abana, Jeffrey D. Lifson, and Anne D. Lewis

Subjects

Male, T cell, Immunology, Cell, Simian Acquired Immunodeficiency Syndrome, Biology, Article, Pathogenesis, 03 medical and health sciences, 0302 clinical medicine, medicine, Animals, Immunology and Allergy, Rhadinovirus, Interleukin-15, Effector, virus diseases, biology.organism_classification, Macaca mulatta, Chronic infection, medicine.anatomical_structure, Interleukin 15, Female, Simian Immunodeficiency Virus, CD8, Signal Transduction, 030215 immunology

Abstract

Although IL-15 has been implicated in the pathogenic hyperimmune activation that drives progressive HIV and SIV infection, as well as in the generation of HIV/SIV target cells, it also supports NK and T cell homeostasis and effector activity, potentially benefiting the host. To understand the role of IL-15 in SIV infection and pathogenesis, we treated two cohorts of SIVmac239-infected rhesus macaques (RM; Macaca mulatta), one with chronic infection, the other with primary infection, with a rhesusized, IL-15–neutralizing mAb (versus an IgG isotype control) for up to 10 wk (n = 7–9 RM per group). In both cohorts, anti–IL-15 was highly efficient at blocking IL-15 signaling in vivo, causing 1) profound depletion of NK cells in blood and tissues throughout the treatment period; 2) substantial, albeit transient, depletion of CD8+ effector memory T cells (TEM) (but not the naive and central memory subsets); and 3) CD4+ and CD8+ TEM hyperproliferation. In primary infection, reduced frequencies of SIV-specific effector T cells in an extralymphoid tissue site were also observed. Despite these effects, the kinetics and extent of SIV replication, CD4+ T cell depletion, and the onset of AIDS were comparable between anti–IL-15– and control-treated groups in both cohorts. However, RM treated with anti–IL-15 during primary infection manifested accelerated reactivation of RM rhadinovirus. Thus, IL-15 support of NK cell and TEM homeostasis does not play a demonstrable, nonredundant role in SIV replication or CD4+ T cell deletion dynamics but may contribute to immune control of oncogenic γ-herpesviruses.

Published

2019

27. Molecular insights into antibody-mediated protection against the prototypic simian immunodeficiency virus

Author

Fangzhu Zhao, Zachary T. Berndsen, Nuria Pedreño-Lopez, Alison Burns, Joel D. Allen, Shawn Barman, Wen-Hsin Lee, Srirupa Chakraborty, Sandrasegaram Gnanakaran, Leigh M. Sewall, Gabriel Ozorowski, Oliver Limbo, Ge Song, Peter Yong, Sean Callaghan, Kim L. Weisgrau, Jeffrey D. Lifson, Rebecca Nedellec, Thomas B Voigt, Fernanda Laurino, Johan Louw, Brandon C. Rosen, Michael Ricciardi, Max Crispin, Ronald C. Desrosiers, Eva G. Rakasz, David I. Watkins, Raiees Andrabi, Andrew B. Ward, Dennis R. Burton, and Devin Sok

Subjects

stomatognathic system, animal diseases, viruses, virus diseases, biochemical phenomena, metabolism, and nutrition

Abstract

SUMMARYSIVmac239 infection of macaques is a favored model of human HIV infection. However, the SIVmac239 envelope (Env) trimer structure, glycan occupancy, and the targets and ability of neutralizing antibodies (nAbs) to protect against SIVmac239 remain unknown. Here, we report the isolation of SIVmac239 nAbs that recognize a glycan hole and the V1/V4 loop. A high-resolution structure of a SIVmac239 Env trimer-nAb complex shows many similarities to HIV and SIVcpz Envs, but with distinct V4 features and an extended V1 loop. Moreover, SIVmac239 Env has a higher glycan shield density than HIV Env that may contribute to poor or delayed nAb responses in SIVmac239-infected macaques. Passive transfer of a nAb protects macaques from repeated low dose intraveneous SIVmac239 challenge at serum titers comparable to those described for protection of humans against HIV infection. Our results provide structural insights for vaccine design and shed light on antibody-mediated protection in the SIV model.

Published

2021

28. Cryo-EM structures of prefusion SIV envelope trimer

Author

Jason Gorman, Chunyan Wang, Rosemarie D. Mason, Alexandra F. Nazzari, Hugh C. Welles, Tongqing Zhou, Julian W. Bess, Tatsiana Bylund, Myungjin Lee, Yaroslav Tsybovsky, Raffaello Verardi, Shuishu Wang, Yongping Yang, Baoshan Zhang, Reda Rawi, Brandon F. Keele, Jeffrey D. Lifson, Jun Liu, Mario Roederer, and Peter D. Kwong

Subjects

Electron Microscope Tomography, Structural Biology, Cryoelectron Microscopy, HIV-1, env Gene Products, Human Immunodeficiency Virus, Animals, HIV Antibodies, Molecular Biology, Macaca mulatta, Antibodies, Neutralizing

Abstract

Simian immunodeficiency viruses (SIVs) are lentiviruses that naturally infect non-human primates of African origin and seeded cross-species transmissions of HIV-1 and HIV-2. Here we report prefusion stabilization and cryo-EM structures of soluble envelope (Env) trimers from rhesus macaque SIV (SIV

Published

2021

29. Concordance of immunological events between intrarectal and intravenous SHIVAD8-EO infection when assessed by Fiebig-equivalent staging

Author

Amarendra Pegu, Giulia Fabozzi, Joana Dias, John R. Mascola, Wanwisa Promsote, Cassandra G. Almasri, Richard A. Koup, Lucio Gama, Constantinos Petrovas, John Paul Todd, Jonathan Fintzi, Yoshiaki Nishimura, Mangaiarkarasi Asokan, Kylie March, Malcolm A. Martin, and Jeffrey D. Lifson

Subjects

Male, Time Factors, T cell, Simian Acquired Immunodeficiency Syndrome, HIV Infections, Viremia, CD8-Positive T-Lymphocytes, Serology, Translational Research, Biomedical, Administration, Rectal, Follicular phase, medicine, Animals, Humans, CXCL13, Lymph node, business.industry, General Medicine, Viral Load, medicine.disease, Acquired immune system, Macaca mulatta, medicine.anatomical_structure, Immunology, Disease Progression, HIV-1, Administration, Intravenous, Female, Simian Immunodeficiency Virus, business, CD8, Research Article

Abstract

Primary HIV-1 infection can be classified into six Fiebig stages based on virological and serological laboratory testing, whereas simian-HIV (SHIV) infection in nonhuman primates (NHPs) is defined in time post-infection, making it difficult to extrapolate NHP experiments to the clinics. We identified and extensively characterized the Fiebig-equivalent stages in NHPs challenged intrarectally or intravenously with SHIV(AD8-EO). During the first month post-challenge, intrarectally challenged monkeys were up to 1 week delayed in progression through stages. However, regardless of the challenge route, stages I–II predominated before, and stages V–VI predominated after, peak viremia. Decrease in lymph node (LN) CD4(+) T cell frequency and rise in CD8(+) T cells occurred at stage V. LN virus-specific CD8(+) T cell responses, dominated by degranulation and TNF, were first detected at stage V and increased at stage VI. A similar late elevation in follicular CXCR5(+) CD8(+) T cells occurred, consistent with higher plasma CXCL13 levels at these stages. LN SHIV(AD8-EO) RNA(+) cells were present at stage II, but appeared to decline at stage VI when virions accumulated in follicles. Fiebig-equivalent staging of SHIV(AD8-EO) infection revealed concordance of immunological events between intrarectal and intravenous infection despite different infection progressions, and can inform comparisons of NHP studies with clinical data.

Published

2021

30. Cytomegalovirus-vaccine-induced unconventional T cell priming and control of SIV replication is conserved between primate species

Author

Daniel Malouli, Roxanne M. Gilbride, Helen L. Wu, Joseph M. Hwang, Nicholas Maier, Colette M. Hughes, Daniel Newhouse, David Morrow, Abigail B. Ventura, Lynn Law, Jennifer Tisoncik-Go, Leanne Whitmore, Elise Smith, Inah Golez, Jean Chang, Jason S. Reed, Courtney Waytashek, Whitney Weber, Husam Taher, Luke S. Uebelhoer, Jennie L. Womack, Matthew R. McArdle, Junwei Gao, Courtney R. Papen, Jeffrey D. Lifson, Benjamin J. Burwitz, Michael K. Axthelm, Jeremy Smedley, Klaus Früh, Michael Gale, Louis J. Picker, Scott G. Hansen, and Jonah B. Sacha

Subjects

AIDS Vaccines, Interleukin-15, SAIDS Vaccines, Simian Acquired Immunodeficiency Syndrome, Cytomegalovirus, CD8-Positive T-Lymphocytes, Macaca mulatta, Microbiology, Cytomegalovirus Vaccines, Macaca fascicularis, Virology, Cytomegalovirus Infections, Animals, Simian Immunodeficiency Virus, Parasitology

Abstract

Strain 68-1 rhesus cytomegalovirus expressing simian immunodeficiency virus (SIV) antigens (RhCMV/SIV) primes MHC-E-restricted CD8+ T cells that control SIV replication in 50%-60% of the vaccinated rhesus macaques. Whether this unconventional SIV-specific immunity and protection is unique to rhesus macaques or RhCMV or is intrinsic to CMV remains unknown. Here, using cynomolgus CMV vectors expressing SIV antigens (CyCMV/SIV) and Mauritian cynomolgus macaques, we demonstrate that the induction of MHC-E-restricted CD8+ T cells requires matching CMV to its host species. RhCMV does not elicit MHC-E-restricted CD8+ T cells in cynomolgus macaques. However, cynomolgus macaques vaccinated with species-matched 68-1-like CyCMV/SIV mounted MHC-E-restricted CD8+ T cells, and half of the vaccinees stringently controlled SIV post-challenge. Protected animals manifested a vaccine-induced IL-15 transcriptomic signature that is associated with efficacy in rhesus macaques. These findings demonstrate that the ability of species-matched CMV vectors to elicit MHC-E-restricted CD8+ T cells that are required for anti-SIV efficacy is conserved in nonhuman primates, and these data support the development of HCMV/HIV for a prophylactic HIV vaccine.

Published

2022

31. Interleukin-15 response signature predicts RhCMV/SIV vaccine efficacy

Author

Taryn Urion, Connor B. Driscoll, Rebecca Shoemaker, Emily Ainslie, Rafick Pierre Sekaly, Slim Fourati, Yoshinori Fukazawa, Lynn Law, Richard Green, Fredrik Barrenäs, Ewelina Kosmider, Randy Fast, David Morrow, Paul T. Edlefsen, Kurt T. Randall, Michael K. Axthelm, Andrea N. Selseth, William J. Bosche, Julia C. Ford, Jeffrey D. Lifson, Jan Komorowski, Barbara K. Felber, Jean Chang, Elise Smith, Leanne S. Whitmore, Bryan E. Randall, Danica Shao, Kelli Oswald, Michael Gale, Colette M. Hughes, Inah Golez, George N. Pavlakis, Scott G. Hansen, Daniel J. Newhouse, Xinxia Peng, Louis J. Picker, Wenjun Song, and Roxanne M. Gilbride

Subjects

0301 basic medicine, Male, RNA viruses, Simian Acquired Immunodeficiency Syndrome, Cytomegalovirus, Gene Expression, CD8-Positive T-Lymphocytes, medicine.disease_cause, Pathology and Laboratory Medicine, White Blood Cells, 0302 clinical medicine, Medical Conditions, Immunodeficiency Viruses, Animal Cells, Medicine and Health Sciences, Cytotoxic T cell, Public and Occupational Health, Biology (General), Interleukin-15, Vaccines, T Cells, Viral Vaccine, SAIDS Vaccines, Vaccination and Immunization, Vaccination, medicine.anatomical_structure, Infectious Diseases, SIV, Interleukin 15, Medical Microbiology, Viral Pathogens, Immunologi, Viruses, Female, Simian Immunodeficiency Virus, Pathogens, Cellular Types, Research Article, Infectious Disease Control, QH301-705.5, T cell, Immune Cells, Genetic Vectors, Immunology, Cytotoxic T cells, Biology, Microbiology, 03 medical and health sciences, Immune system, Virology, Retroviruses, medicine, Genetics, Animals, Molecular Biology, Microbial Pathogens, Blood Cells, Viral vaccines, Lentivirus, Organisms, HIV vaccines, Biology and Life Sciences, Cell Biology, Simian immunodeficiency virus, RC581-607, Vaccine efficacy, Macaca mulatta, 030104 developmental biology, Parasitology, Preventive Medicine, Immunologic diseases. Allergy, 030215 immunology

Abstract

Simian immunodeficiency virus (SIV) challenge of rhesus macaques (RMs) vaccinated with strain 68–1 Rhesus Cytomegalovirus (RhCMV) vectors expressing SIV proteins (RhCMV/SIV) results in a binary outcome: stringent control and subsequent clearance of highly pathogenic SIV in ~55% of vaccinated RMs with no protection in the remaining 45%. Although previous work indicates that unconventionally restricted, SIV-specific, effector-memory (EM)-biased CD8+ T cell responses are necessary for efficacy, the magnitude of these responses does not predict efficacy, and the basis of protection vs. non-protection in 68–1 RhCMV/SIV vector-vaccinated RMs has not been elucidated. Here, we report that 68–1 RhCMV/SIV vector administration strikingly alters the whole blood transcriptome of vaccinated RMs, with the sustained induction of specific immune-related pathways, including immune cell, toll-like receptor (TLR), inflammasome/cell death, and interleukin-15 (IL-15) signaling, significantly correlating with subsequent vaccine efficacy. Treatment of a separate RM cohort with IL-15 confirmed the central involvement of this cytokine in the protection signature, linking the major innate and adaptive immune gene expression networks that correlate with RhCMV/SIV vaccine efficacy. This change-from-baseline IL-15 response signature was also demonstrated to significantly correlate with vaccine efficacy in an independent validation cohort of vaccinated and challenged RMs. The differential IL-15 gene set response to vaccination strongly correlated with the pre-vaccination activity of this pathway, with reduced baseline expression of IL-15 response genes significantly correlating with higher vaccine-induced induction of IL-15 signaling and subsequent vaccine protection, suggesting that a robust de novo vaccine-induced IL-15 signaling response is needed to program vaccine efficacy. Thus, the RhCMV/SIV vaccine imparts a coordinated and persistent induction of innate and adaptive immune pathways featuring IL-15, a known regulator of CD8+ T cell function, that support the ability of vaccine-elicited unconventionally restricted CD8+ T cells to mediate protection against SIV challenge., Author summary SIV insert-expressing vaccine vectors based on strain 68–1 RhCMV elicit robust, highly effector-memory-biased, unconventionally restricted T cell responses that are associated with an unprecedented level of SIV control after challenge (replication arrest leading to clearance) in slightly over half of vaccinated monkeys. Since efficacy among monkeys vaccinated with the effective 68–1 vaccine is not predicted by standard measures of immunogenicity, we used functional genomics analysis of RhCMV/SIV vaccinated monkeys with known challenge outcomes to identify immune correlates of protection. We found that vaccine efficacy significantly correlates with a vaccine-induced response to IL-15 that includes modulation of immune cell, inflammation, TLR signaling, and cell death programming response pathways. These data suggest that RhCMV/SIV efficacy results from a coordinated and sustained vaccine-mediated induction of innate and adaptive immune pathways featuring IL-15, a known regulator of CD8+ effector-memory T cell function, that cooperates with vaccine-elicited CD8+ T cells to mediate efficacy.

Published

2021

32. Recombinant Herpesvirus Vectors: Durable Immune Responses and Durable Protection against Simian Immunodeficiency Virus SIVmac239 Acquisition

Author

Jeffrey D. Lifson, Lucas Gonzalez-Nieto, Ronald C. Desrosiers, Isabelle M. Castro, Mauricio A. Martins, Eva G. Rakasz, Michael J. Ricciardi, and David I. Watkins

Subjects

Male, Rhadinovirus, Time Factors, T-Lymphocytes, viruses, Genetic Vectors, Immunology, Biology, Antibodies, Viral, medicine.disease_cause, Microbiology, Virus, 03 medical and health sciences, Immunogenicity, Vaccine, Immunity, Virology, Vaccines and Antiviral Agents, medicine, Animals, HIV vaccine, 030304 developmental biology, 0303 health sciences, 030306 microbiology, SAIDS Vaccines, virus diseases, Simian immunodeficiency virus, biology.organism_classification, Macaca mulatta, Vaccination, HIV Antigens, Insect Science, Female, Simian Immunodeficiency Virus, Immunologic Memory, Viral load, Follow-Up Studies

Abstract

A prophylactic vaccine that confers durable protection against human immunodeficiency virus (HIV) would provide a valuable tool to prevent new HIV/AIDS cases. As herpesviruses establish lifelong infections that remain largely subclinical, the use of persistent herpesvirus vectors to deliver HIV antigens may facilitate the induction of long-term anti-HIV immunity. We previously developed recombinant (r) forms of the gamma-herpesvirus rhesus monkey rhadinovirus (rRRV) expressing a replication-incompetent, near-full-length simian immunodeficiency virus (SIVnfl) genome. We recently showed that 8/16 rhesus macaques (RMs) vaccinated with a rDNA/rRRV-SIVnfl regimen were significantly protected against intrarectal (i.r.) challenge with SIVmac239. Here we investigated the longevity of this vaccine-mediated protection. Despite receiving no additional booster immunizations, the protected rDNA/rRRV-SIVnfl vaccinees maintained detectable cellular and humoral anti-SIV immune responses for more than 1.5 years after the rRRV boost. To assess if these responses were still protective, the rDNA/rRRV-SIVnfl vaccinees were subjected to a second round of marginal-dose i.r. SIVmac239 challenges, with eight SIV-naive RMs serving as concurrent controls. After three SIV exposures, 8/8 control animals became infected, compared to 3/8 vaccinees. This difference in SIV acquisition was statistically significant (P = 0.0035). The three vaccinated monkeys that became infected exhibited significantly lower viral loads than those in unvaccinated controls. Collectively, these data illustrate the ability of rDNA/rRRV-SIVnfl vaccination to provide long-term immunity against stringent mucosal challenges with SIVmac239. Future work is needed to identify the critical components of this vaccine-mediated protection and the extent to which it can tolerate sequence mismatches in the challenge virus. IMPORTANCE We report on the long-term follow-up of a group of rhesus macaques (RMs) that received an AIDS vaccine regimen and were subsequently protected against rectal acquisition of simian immunodeficiency virus (SIV) infection. The vaccination regimen employed included a live recombinant herpesvirus vector that establishes persistent infection in RMs. Consistent with the recurrent SIV antigen expression afforded by this herpesvirus vector, vaccinees maintained detectable SIV-specific immune responses for more than 1.5 years after the last vaccination. Importantly, these vaccinated RMs were significantly protected against a second round of rectal SIV exposures performed 1 year after the first SIV challenge phase. These results are relevant for HIV vaccine development because they show the potential of herpesvirus-based vectors to maintain functional antiretroviral immunity without the need for repeated boosting.

Published

2021

33. Recombinant Human Interleukin-15 and Anti-PD-L1 Combination Therapy Expands a CXCR3+PD1−/low CD8 T-Cell Subset in Simian Immunodeficiency Virus-Infected Rhesus Macaques

Author

Tong Li, Ping Chen, Steven Godin, Jie Cheng, Jing Qin, Ludmila Krymskaya, Marta Catalfamo, Maha Moussa, Michael C. Sneller, Jeffrey D. Lifson, H. Clifford Lane, and Hui Chen

Subjects

Male, 0301 basic medicine, Receptors, CXCR3, Programmed Cell Death 1 Receptor, Simian Acquired Immunodeficiency Syndrome, Viremia, CD8-Positive T-Lymphocytes, Antibodies, Monoclonal, Humanized, medicine.disease_cause, B7-H1 Antigen, Recombinant Human Interleukin-15, Major Articles and Brief Reports, 03 medical and health sciences, 0302 clinical medicine, Immune system, Animals, Humans, Immunology and Allergy, Cytotoxic T cell, Medicine, Interleukin-15, business.industry, virus diseases, Viral Load, Simian immunodeficiency virus, medicine.disease, Macaca mulatta, Virology, Recombinant Proteins, Treatment Outcome, 030104 developmental biology, Infectious Diseases, Interleukin 15, 030220 oncology & carcinogenesis, Drug Therapy, Combination, Female, Simian Immunodeficiency Virus, business, Viral load, CD8

Abstract

Background The PD1/PD-L1 pathway contributes to the pathogenesis of human immunodeficiency virus (HIV)/simian immunodeficiency virus (SIV) infection, and blockade of this pathway may have potential to restore immune function and promote viral control or elimination. In this study, we combined a checkpoint inhibitor anti-PD-L1 (Avelumab) and recombinant human interleukin-15 (rhIL-15) in SIV-infected rhesus macaques (RM). Methods The rhIL-15 was administered as continuous infusion in 2 cycles of 10 days in the context of weekly administration of anti-PD-L1 (Avelumab) in SIV-infected RM receiving combination antiretroviral therapy (cART). Safety, immunological parameters, and viral loads were monitored during the study. Results Administration of rhIL-15/anti-PD-L1 was safe and well tolerated. Treatment resulted in transient increases in proliferating (Ki67+) natural killer and CD8 T cells. In addition, treatment expanded a CXCR3+PD1−/low CD8 T-cell subset with the ability to secrete cytokines. Despite these effects, no changes in plasma viremia were observed after cART interruption. Conclusions Expansion of the CXCR3+PD1−/low CD8 T-cell subset with functional capacity and potential to traffic to sites of viral reservoirs in SIV-infected rhesus macaques had no demonstrable effect on plasma viremia after cART interruption.

Published

2019

34. Blocking α 4 β 7 integrin binding to SIV does not improve virologic control

Author

Brandon F. Keele, Nami Iwamoto, Peter D. Kwong, Jeffrey D. Lifson, Mario Roederer, Susie Min, Jason Gorman, Kaimei Song, Rosemarie D. Mason, Kathryn E. Foulds, Hugh C. Welles, Hannah A. D. King, Aaron J. Belli, James Arthos, Claudia Cicala, and Keith A. Reimann

Subjects

0301 basic medicine, Integrin beta Chains, medicine.drug_class, Integrin alpha4, T-Lymphocytes, Simian Acquired Immunodeficiency Syndrome, HIV Infections, Biology, Antibodies, Viral, Virus Replication, medicine.disease_cause, Monoclonal antibody, Article, 03 medical and health sciences, 0302 clinical medicine, In vivo, medicine, Animals, Viral Regulatory and Accessory Proteins, chemistry.chemical_classification, Multidisciplinary, Antibodies, Monoclonal, Gene Products, env, Viral Load, Simian immunodeficiency virus, Macaca mulatta, Virology, Stop codon, 030104 developmental biology, Viral replication, chemistry, DNA, Viral, biology.protein, RNA, Viral, Simian Immunodeficiency Virus, Antibody, Glycoprotein, Viral load, 030215 immunology

Abstract

An antibody is not the antidote An HIV therapeutic that would give long-term remission without sustained antiretroviral therapy (ART) is a long-term goal. Byrareddy et al. [ Science 354 , 197 (2016)] reported that treating simian immunodeficiency virus (SIV)–positive macaques with an antibody against integrin α 4 β 7 during and after ART results in sustained virologic control after stopping all treatment. Three studies in this issue question the reproducibility of that result. Di Mascio et al. sequenced the virus used in the 2016 study and found that it was a variant with a stop codon in the nef gene rather than a wild-type virus. Abbink et al. used the same antibody for α 4 β 7 as before but tested control of a more commonly used pathogenic virus. Iwamato et al. used the same nef -stop virus as in the earlier paper but combined the antibody against the integrin with an antibody against the SIV envelope glycoprotein, which also blocks viral binding of the integrin. None of these three new studies found that treating with the antibody had any effect on virologic control after stopping ART treatment. Science , this issue p. 1025 , p. 1029 , p. 1033

Published

2019

35. Vaccine protection against SIVmac239 acquisition

Author

Eva G. Rakasz, Mauricio A. Martins, Georg F. Bischof, Lucas Gonzalez-Nieto, Young C. Shin, Ronald C. Desrosiers, Jeffrey D. Lifson, David I. Watkins, and William A. Lauer

Subjects

Protective immunity, viruses, animal diseases, Simian Acquired Immunodeficiency Syndrome, Human immunodeficiency virus (HIV), Biology, Antibodies, Viral, Virus Replication, medicine.disease_cause, Immune system, Human use, medicine, Animals, Cells, Cultured, Herpesviridae, Multidisciplinary, Vaccination, SAIDS Vaccines, Virion, virus diseases, Biological Sciences, Antibodies, Neutralizing, Macaca mulatta, Virology, biology.protein, Simian Immunodeficiency Virus, Antibody

Abstract

The biological characteristics of HIV pose serious difficulties for the success of a preventive vaccine. Molecularly cloned SIVmac239 is difficult for antibodies to neutralize, and a variety of vaccine approaches have had great difficulty achieving protective immunity against it in rhesus monkey models. Here we report significant protection against i.v. acquisition of SIVmac239 using a long-lasting approach to vaccination. The vaccine regimen includes a replication-competent herpesvirus engineered to contain a near-full-length SIV genome that expresses all nine SIV gene products, assembles noninfectious SIV virion particles, and is capable of eliciting long-lasting effector-memory cellular immune responses to all nine SIV gene products. Vaccinated monkeys were significantly protected against acquisition of SIVmac239 following repeated marginal dose i.v. challenges over a 4-month period. Further work is needed to define the critical components necessary for eliciting this protective immunity, evaluate the breadth of the protection against a variety of strains, and explore how this approach may be extended to human use.

Published

2019

36. A cellular trafficking signal in the SIV envelope protein cytoplasmic domain is strongly selected for in pathogenic infection

Author

Scott P. Lawrence, Samra E. Elser, Workineh Torben, Robert V. Blair, Bapi Pahar, Pyone P. Aye, Faith Schiro, Dawn Szeltner, Lara A. Doyle-Meyers, Beth S. Haggarty, Andrea P. O. Jordan, Josephine Romano, George J. Leslie, Xavier Alvarez, David H. O’Connor, Roger W. Wiseman, Christine M. Fennessey, Yuan Li, Michael Piatak, Jeffrey D. Lifson, Celia C. LaBranche, Andrew A. Lackner, Brandon F. Keele, Nicholas J. Maness, Mark Marsh, and James A. Hoxie

Subjects

Virology, Immunology, Simian Acquired Immunodeficiency Syndrome, Genetics, Animals, Gene Products, env, Simian Immunodeficiency Virus, Parasitology, Macaca nemestrina, Macaca mulatta, Molecular Biology, Microbiology, Endocytosis

Abstract

The HIV/SIV envelope glycoprotein (Env) cytoplasmic domain contains a highly conserved Tyr-based trafficking signal that mediates both clathrin-dependent endocytosis and polarized sorting. Despite extensive analysis, the role of these functions in viral infection and pathogenesis is unclear. An SIV molecular clone (SIVmac239) in which this signal is inactivated by deletion of Gly-720 and Tyr-721 (SIVmac239ΔGY), replicates acutely to high levels in pigtail macaques (PTM) but is rapidly controlled. However, we previously reported that rhesus macaques and PTM can progress to AIDS following SIVmac239ΔGY infection in association with novel amino acid changes in the Env cytoplasmic domain. These included an R722G flanking the ΔGY deletion and a nine nucleotide deletion encoding amino acids 734–736 (ΔQTH) that overlaps therevandtatopen reading frames. We show that molecular clones containing these mutations reconstitute signals for both endocytosis and polarized sorting. In one PTM, a novel genotype was selected that generated a new signal for polarized sorting but not endocytosis. This genotype, together with the ΔGY mutation, was conserved in association with high viral loads for several months when introduced into naïve PTMs. For the first time, our findings reveal strong selection pressure for Env endocytosis and particularly for polarized sorting during pathogenic SIV infectionin vivo.

Published

2022

37. A tyrosine-based trafficking signal in the simian immunodeficiency virus envelope cytoplasmic domain is strongly selected for in pathogenic SIV infection

Author

Faith Schiro, Robert V Blair, Mark Marsh, Bapi Pahar, Celia C. LaBranche, David H. O’Connor, Beth S. Haggarty, Christine M. Fennessey, Dawn M. Szeltner, Yuxing Li, Nicholas J. Maness, James A. Hoxie, Workineh Torben, Xavier Alvarez, Brandon F. Keele, Josephine Romano, Jeffrey D. Lifson, Scott P. Lawrence, Lara A. Doyle-Meyers, Samra E. Elser, Michael Piatak, Roger W. Wiseman, Andrea P. O. Jordan, Pyone P. Aye, and Andrew A. Lackner

Subjects

chemistry.chemical_classification, Mutation, Clone (cell biology), Pigtail macaque, Simian immunodeficiency virus, Biology, Endocytosis, medicine.disease_cause, biology.organism_classification, Virology, Open reading frame, chemistry, medicine, Tyrosine, Glycoprotein

Abstract

SUMMARYThe HIV/SIV envelope glycoprotein (Env) cytoplasmic domain contains a highly conserved Tyr-dependent trafficking signal that mediates both clathrin-dependent endocytosis and polarized sorting of Env. Despite extensive characterization, the role of these functions in viral infection and pathogenesis is unclear. An SIV molecular clone (SIVmac239) in which the Tyr-based signal is inactivated by deletion of Gly-720 and Tyr-721 (SIVmac239ΔGY) replicates to high levels acutely in pigtail macaques (PTM) but is rapidly controlled. We previously reported that rhesus macaques and PTM can progress to AIDS following SIVmac239ΔGY infection in association with novel amino acid changes in the Env cytoplasmic domain. These included an R722G flanking the ΔGY deletion and a nine nucleotide deletion that encodes amino acids 734-736 (ΔQTH) and overlaps with the rev and tat open reading frames. We show that molecular clones containing these mutations reconstitute signals for both endocytosis and polarized sorting. In one PTM, a novel genotype was selected, which generated a new signal for polarized sorting but not endocytosis. This mutation by itself was sufficient to maintain high viral loads for several months when introduced into naïve PTMs. These findings reveal, for the first time, strong selection pressure for Env endocytosis and, in particular, for polarized sorting during pathogenic SIV infection in vivo.

Published

2021

38. Evaluating a New Class of AKT/mTOR Activators for HIV Latency-Reversing Activity Ex Vivo and In Vivo

Author

Emilie Besnard, Timothy J. Henrich, Warner C. Greene, Melanie Ott, Jacob D. Estes, William Brantley, Danielle M. Rosenthal, Nevan J. Krogan, Benjamin Varco-Merth, Michael Snape, Satish K. Pillai, Zachary W. Grimmett, Jeffrey D. Lifson, Hannah S. Sperber, Steven G. Deeks, Louise E. Hogan, Louis J. Picker, Michael Nekorchuk, Mark Connors, Stephen A. Migueles, Roland Schwarzer, Bernard Kiernan, Feng Hsiao, Thomas A. Packard, Jeffrey R. Johnson, Philip A. Hull, Nadia R. Roan, Mauricio Montano, Afam A. Okoye, Andrea Gramatica, Eytan Herzig, and Eric Verdin

Subjects

0303 health sciences, T cell, Immunology, Medizin, Pharmacology, Biology, Microbiology, 03 medical and health sciences, 0302 clinical medicine, Immune system, medicine.anatomical_structure, In vivo, Virology, Insect Science, medicine, Cytotoxic T cell, Protein kinase B, 030217 neurology & neurosurgery, PI3K/AKT/mTOR pathway, CD8, Ex vivo, 030304 developmental biology

Abstract

An ability to activate latent HIV-1 expression could benefit many HIV cure strategies, but the first generation of latency reversing agents (LRAs) has proven disappointing. We evaluated AKT/mTOR activators as a potential new class of LRAs. Two glycogen synthase kinase-3 inhibitors (GSK-3i's), SB-216763 and tideglusib (the latter already in phase II clinical trials) that activate AKT/mTOR signaling were tested. These GSK-3i's reactivated latent HIV-1 present in blood samples from aviremic individuals on antiretroviral therapy (ART) in the absence of T cell activation, release of inflammatory cytokines, cell toxicity, or impaired effector function of cytotoxic T lymphocytes or NK cells. However, when administered in vivo to SIV-infected rhesus macaques on suppressive ART, tideglusib exhibited poor pharmacodynamic properties and resulted in no clear evidence of significant SIV latency reversal. Whether alternative pharmacological formulations or combinations of this drug with other classes of LRAs will lead to an effective in vivo latency-reversing strategy remains to be determined.IMPORTANCE If combined with immune therapeutics, latency reversing agents (LRAs) have the potential to reduce the size of the reservoir sufficiently that an engineered immune response can control the virus in the absence of antiretroviral therapy. We have identified a new class of LRAs that do not induce T-cell activation and that are able to potentiate, rather than inhibit, CD8+ T and NK cell cytotoxic effector functions. This new class of LRAs corresponds to inhibitors of glycogen synthase kinase-3. In this work, we have also studied the effects of one member of this drug class, tideglusib, in SIV-infected rhesus monkeys. When tested in vivo, however, tideglusib showed unfavorable pharmacokinetic properties, which resulted in lack of SIV latency reversal. The disconnect between our ex vivo and in vivo results highlights the importance of developing next generation LRAs with pharmacological properties that allow systemic drug delivery in relevant anatomical compartments harboring latent reservoirs.

Published

2021

39. CD8 Lymphocyte Depletion Enhances the Latency Reversal Activity of the SMAC Mimetic AZD5582 in ART-Suppressed Simian Immunodeficiency Virus-Infected Rhesus Macaques

Author

Jeffrey D. Lifson, Nils Schoof, Guido Silvestri, Kirk Easley, Ann Chahroudi, Julia Bergild McBrien, Thomas H. Vanderford, Laura E. Liao, Diane G. Carnathan, Deanna A. Kulpa, Mirko Paiardini, Cameron Mattingly, Richard M. Dunham, Alan S. Perelson, Alyssa D. Brooks, David M. Margolis, Ruian Ke, Shan Liang, and Maud Mavigner

Subjects

biology, Immunology, Cell, Viremia, medicine.disease, Microbiology, Virus, medicine.anatomical_structure, Immune system, In vivo, Virology, Insect Science, biology.protein, medicine, Antibody, Latency (engineering), CD8

Abstract

Inducing latency reversal to reveal infected cells to the host immune system represents a potential strategy to cure HIV infection. In separate studies, we have previously shown that CD8+ T cells may contribute to the maintenance of viral latency and identified a novel SMAC mimetic/IAP inhibitor (AZD5582) capable of reversing HIV/SIV latency in vivo by activating the non-canonical (nc) NF-κB pathway. Here, we use AZD5582 in combination with antibody-mediated depletion of CD8α+ cells to further evaluate the role of CD8+ T cells in viral latency maintenance. Six rhesus macaques (RM) were infected with SIVmac239 and treated with ART starting at week 8 post-infection. After 84-85 weeks of ART, all animals received a single dose of the anti-CD8α depleting antibody (Ab), MT807R1 (50mg/kg, s.c.), followed by 5 weekly doses of AZD5582 (0.1 mg/kg, i.v.). Following CD8α depletion + AZD5582 combined treatment, 100% of RMs experienced on-ART viremia above 60 copies per ml of plasma. In comparator groups of ART-suppressed SIV-infected RMs treated with AZD5582 only or CD8α depletion only, on-ART viremia was experienced by 56% and 57% of the animals respectively. Furthermore, the frequency of increased viremic episodes during the treatment period was greater in the CD8α depletion + AZD5582 group as compared to other groups. Mathematical modeling of virus reactivation suggested that, in addition to viral dynamics during acute infection, CD8α depletion influenced the response to AZD5582. This work suggests that the latency reversal induced by activation of the ncNF-κB signaling pathway with AZD5582 can be enhanced by CD8α+ cell depletion.

Published

2021

40. New SHIVs and Improved Design Strategy for Modeling HIV-1 Transmission, Immunopathogenesis, Prevention and Cure

Author

Beatrice H. Hahn, Jessica G. Smith, Yu Ding, Neha Chohan, Brandon F. Keele, Mark G. Lewis, Katharine J. Bar, Alex I. Murphy, Cristian Apetrei, Jeffrey D. Lifson, Hui Li, Fang-Hua Lee, Ivona Pandrea, Thomas N. Denny, Barton F. Haynes, Emily Lindemuth, Juliette Rando, Shuyi Wang, Chengyan Zhao, George M. Shaw, Ryan S. Roark, and Eunlim Kim

Subjects

Antigenicity, simian immunodeficiency virus, viruses, animal diseases, Immunology, Biology, Gp41, Microbiology, Virus, Neutralization, 03 medical and health sciences, 0302 clinical medicine, In vivo, Viral entry, Virology, Gene, Tropism, 030304 developmental biology, 0303 health sciences, human immunodeficiency virus, Wild type, virus diseases, Vaccine efficacy, In vitro, AIDS, Immunization, SHIV, Insect Science, biology.protein, Pathogenesis and Immunity, Antibody, 030217 neurology & neurosurgery

Abstract

SHIV infection of Indian rhesus macaques is an important animal model for studying HIV-1 transmission, prevention, immunopathogenesis, and cure. Such research is timely, given recent progress with active and passive immunization and novel approaches to HIV-1 cure., Previously, we showed that substitution of HIV-1 envelope (Env) residue 375-Ser by bulky aromatic residues enhances binding to rhesus CD4 and enables primary HIV-1 Envs to support efficient replication as simian-human immunodeficiency virus (SHIV) chimeras in rhesus macaques (RMs). Here, we test this design strategy more broadly by constructing SHIVs containing 10 primary Envs corresponding to HIV-1 subtypes A, B, C, AE, and AG. All 10 SHIVs bearing wild-type Env375 residues replicated efficiently in human CD4+ T cells, but only one replicated efficiently in primary rhesus cells. This was a subtype AE SHIV that naturally contained His at Env375. Replacement of wild-type Env375 residues by Trp, Tyr, Phe, or His in the other nine SHIVs led to efficient replication in rhesus CD4+ T cells in vitro and in vivo. Nine SHIVs containing optimized Env375 alleles were grown large-scale in primary rhesus CD4+ T cells to serve as challenge stocks in preclinical prevention trials. These virus stocks were genetically homogeneous, native-like in Env antigenicity and tier 2 neutralization sensitivity, and transmissible by rectal, vaginal, penile, oral, or intravenous routes. To facilitate future SHIV constructions, we engineered a simplified second-generation design scheme and validated it in RMs. Overall, our findings demonstrate that SHIVs bearing primary Envs with bulky aromatic substitutions at Env375 consistently replicate in RMs, recapitulating many features of HIV-1 infection in humans. Such SHIVs are efficiently transmitted by mucosal routes common to HIV-1 infection and can be used to test vaccine efficacy in preclinical monkey trials. IMPORTANCE SHIV infection of Indian rhesus macaques is an important animal model for studying HIV-1 transmission, prevention, immunopathogenesis, and cure. Such research is timely, given recent progress with active and passive immunization and novel approaches to HIV-1 cure. Given the multifaceted roles of HIV-1 Env in cell tropism and virus entry, and as a target for neutralizing and nonneutralizing antibodies, Envs selected for SHIV construction are of paramount importance. Until recently, it has been impossible to strategically design SHIVs bearing clinically relevant Envs that replicate consistently in monkeys. This changed with the discovery that bulky aromatic substitutions at residue Env375 confer enhanced affinity to rhesus CD4. Here, we show that 10 new SHIVs bearing primary HIV-1 Envs with residue 375 substitutions replicated efficiently in RMs and could be transmitted efficiently across rectal, vaginal, penile, and oral mucosa. These findings suggest an expanded role for SHIVs as a model of HIV-1 infection.

Published

2021

41. CD8 lymphocyte depletion enhances the latency reversal activity of the SMAC mimetic AZD5582 in ART-suppressed SIV-infected rhesus macaques

Author

Maud, Mavigner, Laura E, Liao, Alyssa D, Brooks, Ruian, Ke, Cameron, Mattingly, Nils, Schoof, Julia, McBrien, Diane, Carnathan, Shan, Liang, Thomas H, Vanderford, Mirko, Paiardini, Deanna, Kulpa, Jeffrey D, Lifson, Richard M, Dunham, Kirk A, Easley, David M, Margolis, Alan S, Perelson, Guido, Silvestri, and Ann, Chahroudi

Subjects

rhesus macaques, SMAC mimetic, SIV/HIV, Pathogenesis and Immunity, ART, CD8 lymphocyte depletion, latency-reversing agents

Abstract

A favored approach to curing HIV infection aims at inducing viral expression using latency-reversing agents (LRAs) to allow the elimination of infected cells. Here, we tested a combination of two recently identified LRAs, the SMAC mimetic/IAP inhibitor AZD5582, which activates the noncanonical NF-κB pathway, and the antibody (Ab) MT807R1, which depletes CD8α+ cells, in SIV-infected rhesus macaques (RMs) on ART., Inducing latency reversal to reveal infected cells to the host immune system represents a potential strategy to cure human immunodeficiency virus (HIV) infection. In separate studies, we have shown previously that CD8+ T cells may contribute to the maintenance of viral latency and have identified a novel SMAC (second mitochondrial activator of caspases) mimetic/IAP (inhibitor of apoptosis protein) inhibitor (AZD5582) capable of reversing HIV/simian immunodeficiency virus (SIV) latency in vivo by activating the noncanonical (nc) NF-κB pathway. Here, we use AZD5582 in combination with antibody (Ab)-mediated depletion of CD8α+ cells to further evaluate the role of CD8+ T cells in the maintenance of viral latency. Six rhesus macaques (RMs) were infected with SIVmac239 and treated with antiretroviral therapy (ART) starting at week 8 postinfection. After 84 to 85 weeks of ART, all animals received a single dose of the anti-CD8α depleting Ab MT807R1 (50 mg/kg of body weight, administered subcutaneously [s.c.]), followed by five weekly doses of AZD5582 (0.1 mg/kg, administered intravenously [i.v.]). Following combined treatment with CD8α depletion and AZD5582, 100% of RMs experienced on-ART viremia levels above 60 copies per ml of plasma. In comparator groups of SIV-infected, ART-suppressed RMs treated with AZD5582 only or CD8α depletion only, on-ART viremia was experienced by 56% and 57% of the animals, respectively. Furthermore, the increased frequency of viremic episodes during the treatment period was greater in the group treated with CD8α depletion plus AZD5582 than in the other groups. Mathematical modeling of virus reactivation suggested that in addition to viral dynamics during acute infection, CD8α depletion influenced the response to AZD5582. This work suggests that the latency reversal induced by activation of the ncNF-κB signaling pathway with AZD5582 can be enhanced by CD8α+ cell depletion. IMPORTANCE A favored approach to curing HIV infection aims at inducing viral expression using latency-reversing agents (LRAs) to allow the elimination of infected cells. Here, we tested a combination of two recently identified LRAs, the SMAC mimetic/IAP inhibitor AZD5582, which activates the noncanonical NF-κB pathway, and the antibody (Ab) MT807R1, which depletes CD8α+ cells, in SIV-infected rhesus macaques (RMs) on ART. Latency reversal, as defined by increased on-ART viremia, was observed in all six SIV-infected, ART-treated RMs that received this combined treatment. Furthermore, comparison of viral reactivation between these animals and groups of SIV-infected, ART-treated RMs treated with AZD5582 only or CD8α+ cell depletion only showed more frequent increases in viremic episodes when the two treatments were combined. This study provides additional evidence that CD8+ T cells may contribute to the maintenance of HIV/SIV latency on ART and potentially inhibit latency reversal during HIV cure approaches.

Published

2021

42. Evaluating a New Class of AKT/mTOR Activators for HIV Latency Reversing Activity

Author

Andrea, Gramatica, Roland, Schwarzer, William, Brantley, Benjamin, Varco-Merth, Hannah S, Sperber, Philip A, Hull, Mauricio, Montano, Stephen A, Migueles, Danielle, Rosenthal, Louise E, Hogan, Jeffrey R, Johnson, Thomas A, Packard, Zachary W, Grimmett, Eytan, Herzig, Emilie, Besnard, Michael, Nekorchuk, Feng, Hsiao, Steven G, Deeks, Michael, Snape, Bernard, Kiernan, Nadia R, Roan, Jeffrey D, Lifson, Jacob D, Estes, Louis J, Picker, Eric, Verdin, Nevan J, Krogan, Timothy J, Henrich, Mark, Connors, Melanie, Ott, Satish K, Pillai, Afam A, Okoye, and Warner C, Greene

Subjects

Vaccines and Antiviral Agents

Abstract

An ability to activate latent human immunodeficiency virus type 1 (HIV-1) expression could benefit many HIV cure strategies; however, most latency-reversing agents (LRAs) have proven disappointing. We evaluated AKT/mTOR activators as a potential new class of LRAs. Two glycogen synthase kinase-3 inhibitors (GSK-3i’s), SB-216763 and tideglusib (the latter already in phase II clinical trials), that activate AKT/mTOR signaling were tested. These GSK-3i’s reactivated latent HIV-1 present in blood samples from aviremic individuals on antiretroviral therapy (ART) in the absence of T cell activation, release of inflammatory cytokines, cell toxicity, or impaired effector function of cytotoxic T lymphocytes or NK cells. However, when administered in vivo to simian immunodeficiency virus (SIV)-infected rhesus macaques on suppressive ART, tideglusib exhibited poor pharmacodynamic properties and resulted in no clear evidence of significant SIV latency reversal. Whether alternative pharmacological formulations or combinations of this drug with other classes of LRAs will lead to an effective in vivo latency-reversing strategy remains to be determined. IMPORTANCE If combined with immune therapeutics, latency-reversing agents (LRAs) have the potential to reduce the size of the reservoir sufficiently that an engineered immune response can control the virus in the absence of antiretroviral therapy. We have identified a new class of LRAs that do not induce T-cell activation and that are able to potentiate, rather than inhibit, CD8(+) T and NK cell cytotoxic effector functions. This new class of LRAs corresponds to inhibitors of glycogen synthase kinase-3. In this work, we have also studied the effects of one member of this drug class, tideglusib, in SIV-infected rhesus monkeys. When tested in vivo, however, tideglusib showed unfavorable pharmacokinetic properties, which resulted in lack of SIV latency reversal. The disconnect between our ex vivo and in vivo results highlights the importance of developing novel LRAs with pharmacological properties that allow systemic drug delivery in relevant anatomical compartments harboring latent reservoirs.

Published

2021

43. Sustained IL-15 response signature predicts RhCMV/SIV vaccine efficacy

Author

Richard Green, Julia C. Ford, Jeffrey D. Lifson, David Morrow, Emily Ainslie, Rafick-Pierre Sekaly, Kurt T. Randall, William J. Bosche, Barbara K. Felber, Michael K. Axthelm, Colette M. Hughes, Louis J. Picker, Daniel J. Newhouse, Paul T. Edlefsen, Jason Shao, Scott G. Hansen, Yoshinori Fukazawa, Wenjun Song, Roxanne M. Gilbride, Andrea N. Selseth, Kelli Oswald, Jan Komorowski, Fredrik Barrenäs, Xinxia Peng, Connor B. Driscoll, George N. Pavlakis, Leanne S. Whitmore, Rebecca Shoemaker, Inah Golez, Taryn Urion, Slim Fourati, Bryan E. Randall, Lynn Law, Elise Smith, Michael Gale, Ewelina Kosmider, Randy Fast, and Jean Chang

Subjects

Immunogenicity, T cell, Inflammation, Simian immunodeficiency virus, Biology, medicine.disease_cause, Virology, Vaccination, medicine.anatomical_structure, Immune system, Interleukin 15, medicine, medicine.symptom, CD8

Abstract

Simian immunodeficiency virus (SIV) challenge of rhesus macaques (RMs) vaccinated with Rhesus Cytomegalovirus (RhCMV) vectors expressing SIV proteins (RhCMV/SIV) results in a binary outcome: stringent control and subsequent clearance of highly pathogenic SIV in ~55% of vaccinated RMs with no protection in the remaining 45%. Although previous work suggests that unconventionally restricted, SIV-specific, effector-memory (EM)-biased CD8+ T cell responses are necessary for efficacy, the magnitude of these responses does not predict efficacy, and the basis of protection vs. non-protection in RhCMV/SIV vector-vaccinated RMs has not been elucidated. Here, we report that RhCMV/SIV vector administration strikingly alters the whole blood transcriptome of vaccinated RMs, with the sustained induction of specific immune-related pathways, including non-canonical T cell receptor (TCR), toll-lie receptor (TLR), inflammasome/cell death, and interleukin-15 (IL-15) signaling, significantly predicting protection. The IL-15 gene expression signature was further evaluated in an independent RM IL-15 treatment cohort, revealing that in whole blood the response to IL-15 is inclusive of innate and adaptive immune gene expression networks that link with RhCMV/SIV vaccine efficacy. We also show that this IL-15 response signature similarly tracks with vaccine protection in an independent RhCMV/SIV vaccination/SIV challenge RM validation cohort. Thus, the RhCMV/SIV vaccine imparts a coordinated and persistent induction of innate and adaptive immune pathways featuring IL-15, a known regulator of CD8+ T cell function, that enable vaccine-elicited CD8+ T cells to mediate protection against highly pathogenic SIV challenge.Author SummarySIV insert-expressing vaccine vectors based on strain 68-1 RhCMV elicit robust, highly effector-memory-biased T cell responses that are associated with an unprecedented level of SIV control after challenge (replication arrest leading to clearance) in slightly over half of vaccinated monkeys. Since efficacy is not predicted by standard measures of immunogenicity, we used functional genomics analysis of RhCMV/SIV vaccinated monkeys with known challenge outcomes to identify immune correlates of protection. We found that arrest of viral replication after challenge significantly correlates with a vaccine-induced response to IL-15 that includes modulation of T cell, inflammation, TLR signaling, and cell death programming. These data suggest that RhCMV/SIV efficacy is not based on chance, but rather, results from a coordinated and sustained vaccine-mediated induction of innate and adaptive immune pathways featuring IL-15, a known regulator of CD8+ effector-memory T cell function, that enable vaccine-elicited CD8+ T cells to mediate efficacy.

Published

2021

44. Potent Anti-Viral Activity of a Trispecific HIV Antibody in SHIV-Infected Monkeys

Author

Jason Hataye, Zhi Yong Yang, Nicole A. Doria-Rose, John R. Mascola, Giulia Fabozzi, Hui Li, Tongqing Zhou, Wei Shi, Kylie March, Brandon F. Keele, George M. Shaw, Joseph P. Casazza, Kathryn E. Foulds, Joana Dias, Wanwisa Promsote, Gary J. Nabel, Michelle D. Cully, Richard A. Koup, Xuejun Chen, Amarendra Pegu, Ling Xu, Ronnie Wei, Hui Geng, Cuiping Liu, Amy Noe, Jeffrey D. Lifson, Cassandra G. Almasri, Ercole Rao, Constantinos Petrovas, Mangaiarkarasi Asokan, John-Paul Todd, Krisha McKee, Christine M. Fennessey, Stephen D. Schmidt, Eun Sung Yang, Megan E. DeMouth, Keyun Wang, and Shing-Fen Kao

Subjects

biology, medicine.medical_treatment, Human immunodeficiency virus (HIV), virus diseases, Viremia, Immunotherapy, Immune control, medicine.disease_cause, medicine.disease, Virology, Pharmacotherapy, In vivo, Viral Activity, medicine, biology.protein, Antibody

Abstract

Broadly neutralizing antibodies (bNAbs) represent an alternative to drug therapy for the treatment of HIV-1 infection. Immunotherapy with single bNAbs often leads to emergence of escape variants, suggesting a potential benefit of combination bNAb therapy. Here a trispecific bNAb is shown to reduce viremia 100- to 1000-fold in viremic SHIV-infected macaques. After treatment discontinuation, viremia rebounded transiently and returned to low levels, through CD8-mediated immune control. These viruses remained sensitive to the trispecific despite loss of sensitivity to one of the parental bNAbs. Similarly, the trispecific bNAb suppressed the emergence of resistance in viruses derived from HIV-1 infected subjects, in contrast to parental bNAbs. Trispecific HIV-1 antibodies therefore mediates potent antiviral activity in vivo that minimizes the potential for immune escape.

Published

2021

45. Rectal Acquisition of Simian Immunodeficiency Virus (SIV) SIVmac239 Infection despite Vaccine-Induced Immune Responses against the Entire SIV Proteome

Author

Jeffrey D. Lifson, Patricia L. Earl, Bernard Moss, Dennis R. Burton, Eva G. Rakasz, Lucas Gonzalez-Nieto, Georg F. Bischof, Mauricio A. Martins, Matthias Pauthner, Nuria Pedreño-Lopez, Michael J. Ricciardi, Christine M. Dang, David I. Watkins, Christopher L. Parks, Ronald C. Desrosiers, and Varian K. Bailey

Subjects

Modified vaccinia Ankara, Proteome, animal diseases, viruses, Immunology, Immunization, Secondary, Simian Acquired Immunodeficiency Syndrome, Viremia, CD8-Positive T-Lymphocytes, medicine.disease_cause, Antibodies, Viral, Microbiology, Virus, 03 medical and health sciences, 0302 clinical medicine, Virology, Vaccines and Antiviral Agents, medicine, Animals, Humans, HIV vaccine, Antigens, Viral, 030304 developmental biology, 0303 health sciences, biology, Vaccination, Immunity, SAIDS Vaccines, virus diseases, Simian immunodeficiency virus, Viral Load, Vaccine efficacy, biology.organism_classification, medicine.disease, Antibodies, Neutralizing, Macaca mulatta, Vesicular stomatitis virus, Insect Science, Simian Immunodeficiency Virus, 030215 immunology

Abstract

Given the complex biology of human immunodeficiency virus (HIV) and its remarkable capacity to evade host immune responses, HIV vaccine efficacy may benefit from the induction of both humoral and cellular immune responses of maximal breadth, potency, and longevity. Guided by this rationale, we set out to develop an immunization protocol aimed at maximizing the induction of anti-Envelope (anti-Env) antibodies and CD8(+) T cells targeting non-Env epitopes in rhesus macaques (RMs). Our approach was to deliver the entire simian immunodeficiency virus (SIV) proteome by serial vaccinations. To that end, 12 RMs were vaccinated over 81 weeks with DNA, modified vaccinia Ankara (MVA), vesicular stomatitis virus (VSV), adenovirus type 5 (Ad5), rhesus monkey rhadinovirus (RRV), and DNA again. Both the RRV and the final DNA boosters delivered a near-full-length SIVmac239 genome capable of assembling noninfectious SIV particles and inducing T-cell responses against all nine SIV proteins. Compared to previous SIV vaccine trials, the present DNA-MVA-VSV-Ad5-RRV-DNA regimen resulted in comparable levels of Env-binding antibodies and SIV-specific CD8(+) T-cells. Interestingly, one vaccinee developed low titers of neutralizing antibodies (NAbs) against SIVmac239, a tier 3 virus. Following repeated intrarectal marginal-dose challenges with SIVmac239, vaccinees were not protected from SIV acquisition but manifested partial control of viremia. Strikingly, the animal with the low-titer vaccine-induced anti-SIVmac239 NAb response acquired infection after the first SIVmac239 exposure. Collectively, these results highlight the difficulties in eliciting protective immunity against immunodeficiency virus infection. IMPORTANCE Our results are relevant to HIV vaccine development efforts because they suggest that increasing the number of booster immunizations or delivering additional viral antigens may not necessarily improve vaccine efficacy against immunodeficiency virus infection.

Published

2020

46. Modulation of MHC-E transport by viral decoy ligands is required for RhCMV/SIV vaccine efficacy

Author

Michael K. Axthelm, Klaus Früh, Julia C. Ford, Jeffrey D. Lifson, Ravi Iyer, Louis J. Picker, William J. Bosche, Nessy John, Roxanne M. Gilbride, Daniel Malouli, Shaheed Abdulhaqq, Brian Berkemeier, Abigail B. Ventura, Jennie Womack, David Morrow, Kelli Oswald, Isabel Scholz, Jonah B. Sacha, Jason Shao, Scott G. Hansen, Michael Hull, Andrea N. Selseth, Paul T. Edlefsen, Colette M. Hughes, Rebecca Shoemaker, and Marieke C. Verweij

Subjects

0301 basic medicine, T cell, Genetic Vectors, Cytomegalovirus, Epitopes, T-Lymphocyte, Priming (immunology), chemical and pharmacologic phenomena, CD8-Positive T-Lymphocytes, Ligands, Major histocompatibility complex, medicine.disease_cause, Article, Epitope, Cell Line, 03 medical and health sciences, 0302 clinical medicine, Immune system, Antigen, medicine, Animals, Multidisciplinary, biology, Histocompatibility Antigens Class I, SAIDS Vaccines, Fibroblasts, Simian immunodeficiency virus, Macaca mulatta, Virology, Peptide Fragments, Protein Transport, 030104 developmental biology, medicine.anatomical_structure, biology.protein, Simian Immunodeficiency Virus, Intracellular, CD8, 030215 immunology

Abstract

Strain 68-1 rhesus cytomegalovirus (RhCMV) vectors expressing simian immunodeficiency virus (SIV) antigens elicit CD8+ T cells that recognize peptide epitopes presented by major histocompatibility complex (MHC)-II and MHC-E molecules, instead of MHC-Ia, and are uniquely able to mediate stringent control and subsequent clearance of highly pathogenic SIV in ∼50% of vaccinated rhesus macaques (RMs). We show that the MHC-E ligand VMAPRTLLL (VL9), encoded by the Rh67 gene (or its HCMV UL40 counterpart) is required for recognition of RhCMV-infected fibroblasts by MHC-E-restricted CD8+ T cells via its ability to promote intracellular MHC-E transport. Moreover, deletion of Rh67 from 68-1 RhCMV/SIV vectors, or mutation of its embedded VL9 ligand, abrogated induction of MHC-E-restricted CD8+ T cell responses, leaving responses that exclusively target MHC-II-restricted epitopes. These MHC-II-presented CD8+ T cell responses, though comparable in response magnitude and functional differentiation to responses arising from the efficacious 68-1 vector, did not protect RMs against SIV challenge, indicating that Rh67/UL40-enabled direct priming of MHC-E-targeted CD8+ T cells is a crucial element of RhCMV/SIV vaccine efficacy.One Sentence SummaryA cytomegalovirus protein (Rh67/UL40) that upregulates MHC-E expression on RhCMV/SIV-vector infected cells is required for induction of MHC-E-restricted CD8+ T cells and for protection against SIV.

Published

2020

47. Cytomegaloviral determinants of CD8+ T cell programming and RhCMV/SIV vaccine efficacy

Author

Justin M. Greene, Renee G. Espinosa Trethewy, Abigail B. Ventura, Husam Taher, Brian Berkemeier, Luke S. Uebelhoer, Jay A. Nelson, Finn Grey, Colette M. Hughes, Rebecca Shoemaker, Daniel Malouli, Courtney R. Papen, William J. Bosche, Louis J. Picker, David Morrow, Meaghan H. Hancock, Roxanne M. Gilbride, Michael Hull, Michael K. Axthelm, Julia C. Ford, Paul T. Edlefsen, Jonah B. Sacha, Daniel N. Streblow, Kurt T. Randall, Jason Shao, Scott G. Hansen, Jeffrey D. Lifson, Kelli Oswald, Matthew R. McArdle, and Klaus Früh

Subjects

viruses, T cell, Immunology, virus diseases, General Medicine, Simian immunodeficiency virus, Biology, Vaccine efficacy, medicine.disease_cause, Major histocompatibility complex, Virology, medicine.anatomical_structure, medicine, biology.protein, Cytotoxic T cell, Vector (molecular biology), Gene, CD8

Abstract

Simian immunodeficiency virus (SIV) insert-expressing, 68-1 Rhesus Cytomegalovirus (RhCMV/SIV) vectors elicit major histocompatibility complex (MHC)-E- and -II-restricted, SIV-specific CD8+ T cell responses, but the basis of these unconventional responses and their contribution to demonstrated vaccine efficacy against SIV challenge in the rhesus monkeys (RMs) has not been characterized. We demonstrate that these unconventional responses resulted from a chance genetic rearrangement in 68-1 RhCMV that abrogated the function of eight distinct immunomodulatory gene products encoded in two RhCMV genomic regions (Rh157.5/.4 and Rh158-161). Differential repair of these genes with either RhCMV-derived or orthologous human CMV (HCMV)-derived sequences (UL128/130; UL146/147) leads to either of two distinct CD8+ T cell response types – MHC-Ia-restricted-only, or a mix of MHC-II- and MHC-Ia-restricted CD8+ T cells. Despite response magnitude and functional differentiation being similar to RhCMV 68-1, neither alternative response type mediated protection against SIV challenge. These findings implicate MHC-E-restricted CD8+ T cell responses as mediators of anti-SIV efficacy and indicate that translation of RhCMV/SIV vector efficacy to humans will likely require deletion of all the genes that inhibit these responses from the HCMV/HIV vector.One-sentence summaryEight genes in two spatially distinct RhCMV gene regions control induction of unconventionally restricted CD8+ T cell responses and the efficacy of RhCMV/SIV vaccine vectors against SIV challenge.

Published

2020

48. IL-21 and IFNα therapy rescues terminally differentiated NK cells and limits SIV reservoir in ART-treated macaques

Author

Steven E. Bosinger, Jeffrey D. Lifson, Kirk Easley, Francois Villinger, Hong Wang, Philippe Rascle, Luca Micci, Guido Silvestri, Neeta Shenvi, Gregory K. Tharp, Nicolas Huot, Cristin M. Galardi, Colin T. King, Michaela Müller-Trutwin, Justin L. Harper, Amit A. Upadhyay, Beatrice Jacquelin, Mirko Paiardini, Emory University [Atlanta, GA], HIV, Inflammation et persistance, Institut Pasteur [Paris], Université Paris Diderot, Sorbonne Paris Cité, Paris, France, Université Paris Diderot - Paris 7 (UPD7), University of North Carolina [Chapel Hill] (UNC), University of North Carolina System (UNC), ViiV Healthcare US, ViiV Healthcare [Brentford, UK], University of Louisiana, Frederick National Laboratory for Cancer Research (FNLCR), Emory University School of Medicine, This work was supported by the NIAID, NIH under award number R01AI116379 to M. P. and R01AI143457 to M. M.-T. Support for this work was also provided by ANRS and the Fondation J. Beytout to M. M.-T., NCRR, NIH award 5R24RR016988 to F. V. and the Resource for Nonhuman Primate Immune Reagents, ORIP/OD award P51OD011132 to YNPRC, and NCI, NIH award HHSN261200800001E and 75N91019D00024 to Leidos Biomedical Research. P.R. was recipient of a PhD fellowship from the University Paris Diderot, Sorbonne Paris Cité., HIV, Inflammation et persistance - HIV, Inflammation and Persistence, and Institut Pasteur [Paris] (IP)

Subjects

0301 basic medicine, CD4-Positive T-Lymphocytes, animal diseases, Science, [SDV]Life Sciences [q-bio], Immunology, Simian Acquired Immunodeficiency Syndrome, General Physics and Astronomy, Alpha interferon, Inflammation, Lymphocyte Activation, Antiviral Agents, General Biochemistry, Genetics and Molecular Biology, Article, Natural killer cell, Natural killer cell differentiation, 03 medical and health sciences, Interferon-gamma, 0302 clinical medicine, Interferon, medicine, Animals, Viremia, Lymph node, Multidisciplinary, biology, Interleukins, virus diseases, General Chemistry, Viral host response, Viral Load, biology.organism_classification, Virology, Macaca mulatta, 3. Good health, Killer Cells, Natural, Rhesus macaque, 030104 developmental biology, medicine.anatomical_structure, Anti-Retroviral Agents, 030220 oncology & carcinogenesis, Female, Simian Immunodeficiency Virus, African Green Monkey, Immunotherapy, medicine.symptom, medicine.drug, HIV infections

Abstract

Unlike HIV infection, which progresses to AIDS absent suppressive anti-retroviral therapy, nonpathogenic infections in natural hosts, such African green monkeys, are characterized by a lack of gut microbial translocation and robust secondary lymphoid natural killer cell responses resulting in an absence of chronic inflammation and limited SIV dissemination in lymph node B-cell follicles. Here we report, using the pathogenic model of antiretroviral therapy-treated, SIV-infected rhesus macaques that sequential interleukin-21 and interferon alpha therapy generate terminally differentiated blood natural killer cells (NKG2a/clowCD16+) with potent human leukocyte antigen-E-restricted activity in response to SIV envelope peptides. This is in contrast to control macaques, where less differentiated, interferon gamma-producing natural killer cells predominate. The frequency and activity of terminally differentiated NKG2a/clowCD16+ natural killer cells correlates with a reduction of replication-competent SIV in lymph node during antiretroviral therapy and time to viral rebound following analytical treatment interruption. These data demonstrate that African green monkey-like natural killer cell differentiation profiles can be rescued in rhesus macaques to promote viral clearance in tissues., Infection of African green monkeys with SIV is associated with reduced pathogenicity. Here the authors explore the requirement of differentiated NK cell populations in a pathogenic Rhesus macaque model of SIV infection and show administration of IL-21 and IFNα rescues terminally differentiated NK cells, similarly to what found in African green monkeys, and limits the SIV reservoir in antiretroviral therapy treated macaques.

Published

2020

49. Fc-mediated effector function contributes to the in vivo antiviral effect of an HIV neutralizing antibody

Author

Sung Hee Ko, Wei Shi, Anna Maximova, Wanwisa Promsote, Laura E. Liao, Richard A. Koup, Eli Boritz, John R. Mascola, Katharine Best, Jeffrey D. Lifson, Keenan Ernste, Mangaiarkarasi Asokan, Daniel C. Douek, Alan S. Perelson, Andrew R. Crowley, Joana Dias, Krisha McKee, Amarendra Pegu, Jianfei Hu, Xuejun Chen, Rafick Pierre Sekaly, Cuiping Liu, Slim Fourati, John-Paul Todd, David R. Ambrozak, Cassandra G Almasri, Lucio Gama, Margaret E. Ackerman, and Divya Kilam

Subjects

medicine.drug_class, Simian Acquired Immunodeficiency Syndrome, HIV Infections, HIV Antibodies, Monoclonal antibody, Virus, Viral entry, In vivo, Medicine, Animals, Humans, Neutralizing antibody, Cells, Cultured, Antibody-dependent cell-mediated cytotoxicity, Multidisciplinary, biology, business.industry, Effector, Receptors, IgG, Antibody-Dependent Cell Cytotoxicity, virus diseases, Biological Sciences, Virology, Antibodies, Neutralizing, Macaca mulatta, Disease Models, Animal, biology.protein, HIV-1, Leukocytes, Mononuclear, Fc-Gamma Receptor, Simian Immunodeficiency Virus, business

Abstract

Treatment of HIV infection with either antiretroviral (ARV) therapy or neutralizing monoclonal antibodies (NAbs) leads to a reduction in HIV plasma virus. Both ARVs and NAbs prevent new rounds of viral infection, but NAbs may have the additional capacity to accelerate the loss of virus-infected cells through Fc gamma receptor (FcγR)-mediated effector functions, which should affect the kinetics of plasma-virus decline. Here, we formally test the role of effector function in vivo by comparing the rate and timing of plasma-virus clearance in response to a single-dose treatment with either unmodified NAb or those with either reduced or augmented Fc function. When infused into viremic simian HIV (SHIV)-infected rhesus macaques, there was a 21% difference in slope of plasma-virus decline between NAb and NAb with reduced Fc function. NAb engineered to increase FcγRIII binding and improve antibody-dependent cellular cytotoxicity (ADCC) in vitro resulted in arming of effector cells in vivo, yet led to viral-decay kinetics similar to NAbs with reduced Fc function. These studies show that the predominant mechanism of antiviral activity of HIV NAbs is through inhibition of viral entry, but that Fc function can contribute to the overall antiviral activity, making them distinct from standard ARVs.

Published

2020

50. Antibody-mediated depletion of viral reservoirs is limited in SIV-infected macaques treated early with antiretroviral therapy

Author

Michael Hull, Jacob D. Estes, Randy Fast, Joshua A. Kramer, Laura Newman, Rodney Wiles, Rebecca Shoemaker, William J. Bosche, Claire Deleage, Christine M. Fennessey, Tyler Malys, James A. Thomas, Charles M. Trubey, Lorna Silipino, Vicky Coalter, Gregory Q. Del Prete, Jeffrey D. Lifson, Cathi Pyle, Duncan Donohue, Adam Wiles, Jacob Kiser, Brandon F. Keele, David R. Morcock, Adrienne E. Swanstrom, Taina T. Immonen, Kelli Oswald, and Matthew W. Breed

Subjects

0301 basic medicine, Viral rebound, Cart, CD4-Positive T-Lymphocytes, Male, Viral protein, medicine.drug_class, Anti-HIV Agents, Lymphoid Tissue, T cell, Simian Acquired Immunodeficiency Syndrome, HIV Infections, Biology, medicine.disease_cause, Monoclonal antibody, Antibodies, Viral, Virus Replication, Lymphocyte Depletion, 03 medical and health sciences, 0302 clinical medicine, medicine, Animals, Humans, Antibodies, Monoclonal, General Medicine, Viral Load, Virology, Antiretroviral therapy, Macaca mulatta, 030104 developmental biology, medicine.anatomical_structure, Anti-Retroviral Agents, 030220 oncology & carcinogenesis, CD4 Antigens, biology.protein, HIV-1, Female, Simian Immunodeficiency Virus, Virus Activation, Lymph, Antibody, Research Article

Abstract

The effectiveness of virus-specific strategies, including administered HIV-specific mAbs, to target cells that persistently harbor latent, rebound-competent HIV genomes during combination antiretroviral therapy (cART) has been limited by inefficient induction of viral protein expression. To examine antibody-mediated viral reservoir targeting without a need for viral induction, we used an anti-CD4 mAb to deplete both infected and uninfected CD4(+) T cells. Ten rhesus macaques infected with barcoded SIVmac239M received cART for 93 weeks starting 4 days after infection. During cART, 5 animals received 5 to 6 anti-CD4 antibody administrations and CD4(+) T cell populations were then allowed 1 year on cART to recover. Despite profound CD4(+) T cell depletion in blood and lymph nodes, time to viral rebound following cART cessation was not significantly delayed in anti-CD4–treated animals compared with controls. Viral reactivation rates, determined based on rebounding SIVmac239M clonotype proportions, also were not significantly different in CD4-depleted animals. Notably, antibody-mediated depletion was limited in rectal tissue and negligible in lymphoid follicles. These results suggest that, even if robust viral reactivation can be achieved, antibody-mediated viral reservoir depletion may be limited in key tissue sites.

Published

2020