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1. Dual blockade of IL-10 and PD-1 leads to control of SIV viral rebound following analytical treatment interruption

Author

Pereira Ribeiro, Susan, Strongin, Zachary, Soudeyns, Hugo, ten-Caten, Felipe, Ghneim, Khader, Pacheco Sanchez, Gabriela, Xavier de Medeiros, Giuliana, Del Rio Estrada, Perla Mariana, Pelletier, Adam-Nicolas, Hoang, Timothy, Nguyen, Kevin, Harper, Justin, Jean, Sherrie, Wallace, Chelsea, Balderas, Robert, Lifson, Jeffrey D., Raghunathan, Gopalan, Rimmer, Eric, Pastuskova, Cinthia, Wu, Guoxin, Micci, Luca, Ribeiro, Ruy M., Chan, Chi Ngai, Estes, Jacob D., Silvestri, Guido, Gorman, Daniel M., Howell, Bonnie J., Hazuda, Daria J., Paiardini, Mirko, and Sekaly, Rafick P.

Published
2024
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3. IFNα-blockade during ART-treated SIV infection lowers tissue vDNA, rescues immune function, and improves overall health

Author

Swainson, Louise A, Sharma, Ashish Arunkumar, Ghneim, Khader, Ribeiro, Susan Pereira, Wilkinson, Peter, Dunham, Richard M, Albright, Rebecca G, Wong, Samson, Estes, Jacob D, Piatak, Michael, Deeks, Steven G, Hunt, Peter W, Sekaly, Rafick-Pierre, and McCune, Joseph M

Subjects
Genetics, HIV/AIDS, Infectious Diseases, Hematology, Inflammatory and immune system, Infection, Animals, Anti-Retroviral Agents, DNA, Viral, HIV Infections, Immunity, Interferon-alpha, Macaca mulatta, Simian Acquired Immunodeficiency Syndrome, Simian Immunodeficiency Virus, Weight Loss, Simian immunodeficiency virus, AIDS/HIV, Immunology, Immunotherapy
Abstract

Type I IFNs (TI-IFNs) drive immune effector functions during acute viral infections and regulate cell cycling and systemic metabolism. That said, chronic TI-IFN signaling in the context of HIV infection treated with antiretroviral therapy (ART) also facilitates viral persistence, in part by promoting immunosuppressive responses and CD8+ T cell exhaustion. To determine whether inhibition of IFN-α might provide benefit in the setting of chronic, ART-treated SIV infection of rhesus macaques, we administered an anti-IFN-α antibody followed by an analytical treatment interruption (ATI). IFN-α blockade was well-tolerated and associated with lower expression of TI-IFN-inducible genes (including those that are antiviral) and reduced tissue viral DNA (vDNA). The reduction in vDNA was further accompanied by higher innate proinflammatory plasma cytokines, expression of monocyte activation genes, IL-12-induced effector CD8+ T cell genes, increased heme/metabolic activity, and lower plasma TGF-β levels. Upon ATI, SIV-infected, ART-suppressed nonhuman primates treated with anti-IFN-α displayed lower levels of weight loss and improved erythroid function relative to untreated controls. Overall, these data demonstrated that IFN-α blockade during ART-treated SIV infection was safe and associated with the induction of immune/erythroid pathways that reduced viral persistence during ART while mitigating the weight loss and anemia that typically ensue after ART interruption.

Published
2022

4. In-depth virological and immunological characterization of HIV-1 cure after CCR5Δ32/Δ32 allogeneic hematopoietic stem cell transplantation

Author

Jensen, Björn-Erik Ole, Knops, Elena, Cords, Leon, Lübke, Nadine, Salgado, Maria, Busman-Sahay, Kathleen, Estes, Jacob D., Huyveneers, Laura E. P., Perdomo-Celis, Federico, Wittner, Melanie, Gálvez, Cristina, Mummert, Christiane, Passaes, Caroline, Eberhard, Johanna M., Münk, Carsten, Hauber, Ilona, Hauber, Joachim, Heger, Eva, De Clercq, Jozefien, Vandekerckhove, Linos, Bergmann, Silke, Dunay, Gábor A., Klein, Florian, Häussinger, Dieter, Fischer, Johannes C., Nachtkamp, Kathrin, Timm, Joerg, Kaiser, Rolf, Harrer, Thomas, Luedde, Tom, Nijhuis, Monique, Sáez-Cirión, Asier, Schulze zur Wiesch, Julian, Wensing, Annemarie M. J., Martinez-Picado, Javier, and Kobbe, Guido

Published
2023
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5. Evaluating a New Class of AKT/mTOR Activators for HIV Latency-Reversing Activity Ex Vivo and In Vivo

Author

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

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Immunotherapy, HIV/AIDS, Sexually Transmitted Infections, Infectious Diseases, 5.1 Pharmaceuticals, Good Health and Well Being, HIV cure, HIV-1, HIV latency reversion, SIV, in vivo study, Biological Sciences, Agricultural and Veterinary Sciences, Medical and Health Sciences, Virology, Agricultural, veterinary and food sciences, Biological sciences, Biomedical and clinical sciences
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

7. Allogeneic immunity clears latent virus following allogeneic stem cell transplantation in SIV-infected ART-suppressed macaques

Author

Wu, Helen L., Busman-Sahay, Kathleen, Weber, Whitney C., Waytashek, Courtney M., Boyle, Carla D., Bateman, Katherine B., Reed, Jason S., Hwang, Joseph M., Shriver-Munsch, Christine, Swanson, Tonya, Northrup, Mina, Armantrout, Kimberly, Price, Heidi, Robertson-LeVay, Mitch, Uttke, Samantha, Kumar, Mithra R., Fray, Emily J., Taylor-Brill, Sol, Bondoc, Stephen, Agnor, Rebecca, Junell, Stephanie L., Legasse, Alfred W., Moats, Cassandra, Bochart, Rachele M., Sciurba, Joseph, Bimber, Benjamin N., Sullivan, Michelle N., Dozier, Brandy, MacAllister, Rhonda P., Hobbs, Theodore R., Martin, Lauren D., Panoskaltsis-Mortari, Angela, Colgin, Lois M.A., Siliciano, Robert F., Siliciano, Janet D., Estes, Jacob D., Smedley, Jeremy V., Axthelm, Michael K., Meyers, Gabrielle, Maziarz, Richard T., Burwitz, Benjamin J., Stanton, Jeffrey J., and Sacha, Jonah B.

Published
2023
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8. Recommendations for measuring HIV reservoir size in cure-directed clinical trials.

Author

Abdel-Mohsen, Mohamed, Richman, Douglas, Siliciano, Robert F, Nussenzweig, Michel C, Howell, Bonnie J, Martinez-Picado, Javier, Chomont, Nicolas, Bar, Katharine J, Yu, Xu G, Lichterfeld, Mathias, Alcami, Jose, Hazuda, Daria, Bushman, Frederic, Siliciano, Janet D, Betts, Michael R, Spivak, Adam M, Planelles, Vicente, Hahn, Beatrice H, Smith, Davey M, Ho, Ya-Chi, Buzon, Maria J, Gaebler, Christian, Paiardini, Mirko, Li, Qingsheng, Estes, Jacob D, Hope, Thomas J, Kostman, Jay, Mounzer, Karam, Caskey, Marina, Fox, Lawrence, Frank, Ian, Riley, James L, Tebas, Pablo, Montaner, Luis J, and BEAT-HIV Delaney Collaboratory to Cure HIV-1 infection

Subjects
BEAT-HIV Delaney Collaboratory to Cure HIV-1 infection, Medical and Health Sciences, Immunology
Abstract

Therapeutic strategies are being clinically tested either to eradicate latent HIV reservoirs or to achieve virologic control in the absence of antiretroviral therapy. Attaining this goal will require a consensus on how best to measure the numbers of persistently infected cells with the potential to cause viral rebound after antiretroviral-therapy cessation in assessing the results of cure-directed strategies in vivo. Current measurements assess various aspects of the HIV provirus and its functionality and produce divergent results. Here, we provide recommendations from the BEAT-HIV Martin Delaney Collaboratory on which viral measurements should be prioritized in HIV-cure-directed clinical trials.

Published
2020

9. HIV-1-induced cytokines deplete homeostatic innate lymphoid cells and expand TCF7-dependent memory NK cells

Author

Wang, Yetao, Lifshitz, Lawrence, Gellatly, Kyle, Vinton, Carol L, Busman-Sahay, Kathleen, McCauley, Sean, Vangala, Pranitha, Kim, Kyusik, Derr, Alan, Jaiswal, Smita, Kucukural, Alper, McDonel, Patrick, Hunt, Peter W, Greenough, Thomas, Houghton, JeanMarie, Somsouk, Ma, Estes, Jacob D, Brenchley, Jason M, Garber, Manuel, Deeks, Steven G, and Luban, Jeremy

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Sexually Transmitted Infections, Infectious Diseases, Clinical Research, HIV/AIDS, 2.1 Biological and endogenous factors, Aetiology, Inflammatory and immune system, Infection, Good Health and Well Being, Cytokines, Gene Expression Regulation, HIV Infections, HIV-1, Homeostasis, Humans, Immunity, Innate, Immunologic Memory, In Vitro Techniques, Inflammation, Killer Cells, Natural, Lymphocytes, T Cell Transcription Factor 1, Wnt Signaling Pathway, Biochemistry and cell biology
Abstract

Human immunodeficiency virus 1 (HIV-1) infection is associated with heightened inflammation and excess risk of cardiovascular disease, cancer and other complications. These pathologies persist despite antiretroviral therapy. In two independent cohorts, we found that innate lymphoid cells (ILCs) were depleted in the blood and gut of people with HIV-1, even with effective antiretroviral therapy. ILC depletion was associated with neutrophil infiltration of the gut lamina propria, type 1 interferon activation, increased microbial translocation and natural killer (NK) cell skewing towards an inflammatory state, with chromatin structure and phenotype typical of WNT transcription factor TCF7-dependent memory T cells. Cytokines that are elevated during acute HIV-1 infection reproduced the ILC and NK cell abnormalities ex vivo. These results show that inflammatory cytokines associated with HIV-1 infection irreversibly disrupt ILCs. This results in loss of gut epithelial integrity, microbial translocation and memory NK cells with heightened inflammatory potential, and explains the chronic inflammation in people with HIV-1.

Published
2020

10. In vitro and in vivo characterization of a recombinant rhesus cytomegalovirus containing a complete genome

Author

Taher, Husam, Mahyari, Eisa, Kreklywich, Craig, Uebelhoer, Luke S, McArdle, Matthew R, Moström, Matilda J, Bhusari, Amruta, Nekorchuk, Michael, E, Xiaofei, Whitmer, Travis, Scheef, Elizabeth A, Sprehe, Lesli M, Roberts, Dawn L, Hughes, Colette M, Jackson, Kerianne A, Selseth, Andrea N, Ventura, Abigail B, Cleveland-Rubeor, Hillary C, Yue, Yujuan, Schmidt, Kimberli A, Shao, Jason, Edlefsen, Paul T, Smedley, Jeremy, Kowalik, Timothy F, Stanton, Richard J, Axthelm, Michael K, Estes, Jacob D, Hansen, Scott G, Kaur, Amitinder, Barry, Peter A, Bimber, Benjamin N, Picker, Louis J, Streblow, Daniel N, Früh, Klaus, and Malouli, Daniel

Subjects
Infectious Diseases, Biotechnology, Genetics, 2.2 Factors relating to the physical environment, Aetiology, Infection, Animals, Cell Line, Chromosomes, Artificial, Bacterial, Cytomegalovirus, Cytomegalovirus Infections, DNA, Recombinant, Disease Models, Animal, Female, Fibroblasts, Genome, Viral, Humans, Macaca mulatta, Male, Mutation, Open Reading Frames, Phylogeny, Species Specificity, Viremia, Microbiology, Immunology, Medical Microbiology, Virology
Abstract

Cytomegaloviruses (CMVs) are highly adapted to their host species resulting in strict species specificity. Hence, in vivo examination of all aspects of CMV biology employs animal models using host-specific CMVs. Infection of rhesus macaques (RM) with rhesus CMV (RhCMV) has been established as a representative model for infection of humans with HCMV due to the close evolutionary relationships of both host and virus. However, the only available RhCMV clone that permits genetic modifications is based on the 68-1 strain which has been passaged in fibroblasts for decades resulting in multiple genomic changes due to tissue culture adaptations. As a result, 68-1 displays reduced viremia in RhCMV-naïve animals and limited shedding compared to non-clonal, low passage isolates. To overcome this limitation, we used sequence information from primary RhCMV isolates to construct a full-length (FL) RhCMV by repairing all mutations affecting open reading frames (ORFs) in the 68-1 bacterial artificial chromosome (BAC). Inoculation of adult, immunocompetent, RhCMV-naïve RM with the reconstituted virus resulted in significant viremia in the blood similar to primary isolates of RhCMV and furthermore led to high viral genome copy numbers in many tissues at day 14 post infection. In contrast, viral dissemination was greatly reduced upon deletion of genes also lacking in 68-1. Transcriptome analysis of infected tissues further revealed that chemokine-like genes deleted in 68-1 are among the most highly expressed viral transcripts both in vitro and in vivo consistent with an important immunomodulatory function of the respective proteins. We conclude that FL-RhCMV displays in vitro and in vivo characteristics of a wildtype virus while being amenable to genetic modifications through BAC recombineering techniques.

Published
2020

11. Elite control of HIV is associated with distinct functional and transcriptional signatures in lymphoid tissue CD8+ T cells

Author

Nguyen, Son, Deleage, Claire, Darko, Samuel, Ransier, Amy, Truong, Duc P, Agarwal, Divyansh, Japp, Alberto Sada, Wu, Vincent H, Kuri-Cervantes, Leticia, Abdel-Mohsen, Mohamed, Del Rio Estrada, Perla M, Ablanedo-Terrazas, Yuria, Gostick, Emma, Hoxie, James A, Zhang, Nancy R, Naji, Ali, Reyes-Terán, Gustavo, Estes, Jacob D, Price, David A, Douek, Daniel C, Deeks, Steven G, Buggert, Marcus, and Betts, Michael R

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Genetics, Vaccine Related, Immunization, Sexually Transmitted Infections, HIV/AIDS, Prevention, Clinical Research, Infectious Diseases, Vaccine Related (AIDS), 1.1 Normal biological development and functioning, Underpinning research, Inflammatory and immune system, Infection, Good Health and Well Being, CD4-Positive T-Lymphocytes, CD8-Positive T-Lymphocytes, HIV Infections, HIV-1, Humans, Lymphoid Tissue, Viral Load, Biological Sciences, Medical and Health Sciences, Medical biotechnology, Biomedical engineering
Abstract

The functional properties of circulating CD8+ T cells have been associated with immune control of HIV. However, viral replication occurs predominantly in secondary lymphoid tissues, such as lymph nodes (LNs). We used an integrated single-cell approach to characterize effective HIV-specific CD8+ T cell responses in the LNs of elite controllers (ECs), defined as individuals who suppress viral replication in the absence of antiretroviral therapy (ART). Higher frequencies of total memory and follicle-homing HIV-specific CD8+ T cells were detected in the LNs of ECs compared with the LNs of chronic progressors (CPs) who were not receiving ART. Moreover, HIV-specific CD8+ T cells potently suppressed viral replication without demonstrable cytolytic activity in the LNs of ECs, which harbored substantially lower amounts of CD4+ T cell-associated HIV DNA and RNA compared with the LNs of CPs. Single-cell RNA sequencing analyses further revealed a distinct transcriptional signature among HIV-specific CD8+ T cells from the LNs of ECs, typified by the down-regulation of inhibitory receptors and cytolytic molecules and the up-regulation of multiple cytokines, predicted secreted factors, and components of the protein translation machinery. Collectively, these results provide a mechanistic framework to expedite the identification of novel antiviral factors, highlighting a potential role for the localized deployment of noncytolytic functions as a determinant of immune efficacy against HIV.

Published
2019

12. Disruption of latent HIV in vivo during the clearance of actinic keratosis by ingenol mebutate

Author

Jiang, Guochun, Maverakis, Emanual, Cheng, Michelle Y, Elsheikh, Maher M, Deleage, Claire, Méndez-Lagares, Gema, Shimoda, Michiko, Yukl, Steven A, Hartigan-O’Connor, Dennis J, Thompson, George R, Estes, Jacob D, Wong, Joseph K, and Dandekar, Satya

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Genetics, Sexually Transmitted Infections, Infectious Diseases, Clinical Research, HIV/AIDS, 5.1 Pharmaceuticals, Evaluation of treatments and therapeutic interventions, 6.1 Pharmaceuticals, Development of treatments and therapeutic interventions, Infection, Administration, Cutaneous, Anti-HIV Agents, Biopsy, CD4-Positive T-Lymphocytes, Diterpenes, HIV Infections, HIV-1, Humans, Keratosis, Actinic, Male, Middle Aged, Pilot Projects, Skin, Transcriptional Activation, Treatment Outcome, United States, Virus Activation, Virus Latency, AIDS/HIV, Transcription, Biomedical and clinical sciences, Health sciences
Abstract

Actinic keratosis (AK) is a precancerous skin lesion that is common in HIV-positive patients. Without effective treatment, AKs can progress to squamous cell carcinoma. Ingenol mebutate, a PKC agonist, is a US Food and Drug Administration-approved (FDA-approved) topical treatment for AKs. It can induce reactivation of latent HIV transcription in CD4+ T cells both in vitro and ex vivo. Although PKC agonists are known to be potent inducers of HIV expression from latency, their effects in vivo are not known because of the concerns of toxicity. Therefore, we sought to determine the effects of topical ingenol mebutate gel on the HIV transcription profile in HIV-infected individuals with AKs, specifically in the setting of suppressive antiretroviral therapy (ART). We found that AKs cleared following topical application of ingenol mebutate and detected marginal changes in immune activation in the peripheral blood and in skin biopsies. An overall increase in the level of HIV transcription initiation, elongation, and complete transcription was detected only in skin biopsies after the treatment. Our data demonstrate that application of ingenol mebutate to AKs in ART-suppressed HIV-positive patients can effectively cure AKs as well as disrupt HIV latency in the skin tissue microenvironment in vivo without causing massive immune activation.

Published
2019

13. An in situ analysis pipeline for initial host-pathogen interactions reveals signatures of human colorectal HIV transmission

Author

Baharlou, Heeva, Canete, Nicolas, Vine, Erica E., Hu, Kevin, Yuan, Di, Sandgren, Kerrie J., Bertram, Kirstie M., Nasr, Najla, Rhodes, Jake W., Gosselink, Martijn P., Di Re, Angelina, Reza, Faizur, Ctercteko, Grahame, Pathma-Nathan, Nimalan, Collins, Geoff, Toh, James, Patrick, Ellis, Haniffa, Muzlifah A., Estes, Jacob D., Byrne, Scott N., Cunningham, Anthony L., and Harman, Andrew N.

Published
2022
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14. Combination anti–PD-1 and antiretroviral therapy provides therapeutic benefit against SIV

Author

Mylvaganam, Geetha H, Chea, Lynette S, Tharp, Gregory K, Hicks, Sakeenah, Velu, Vijayakumar, Iyer, Smita S, Deleage, Claire, Estes, Jacob D, Bosinger, Steven E, Freeman, Gordon J, Ahmed, Rafi, and Amara, Rama R

Subjects
Infectious Diseases, HIV/AIDS, 5.1 Pharmaceuticals, 5.2 Cellular and gene therapies, Development of treatments and therapeutic interventions, Infection, Good Health and Well Being, Animals, Anti-Retroviral Agents, Antibodies, Monoclonal, B-Lymphocytes, CD4-Positive T-Lymphocytes, CD8-Positive T-Lymphocytes, Cell Proliferation, Combined Modality Therapy, Disease Models, Animal, Granzymes, HIV Infections, HIV-1, Immunotherapy, Ki-67 Antigen, Macaca mulatta, Programmed Cell Death 1 Receptor, Simian Acquired Immunodeficiency Syndrome, Simian Immunodeficiency Virus, Viremia, Simian immunodeficiency virus, AIDS/HIV, Immunology
Abstract

Therapeutic strategies that augment antiviral immunity and reduce the viral reservoir are critical to achieving durable remission of HIV. The coinhibitory receptor programmed death-1 (PD-1) regulates CD8+ T cell dysfunction during chronic HIV and SIV infections. We previously demonstrated that in vivo blockade of PD-1 during chronic SIV infection improves the function of antiviral CD8+ T cells and B cells. Here, we tested the immunological and virological effects of PD-1 blockade combined with antiretroviral therapy (ART) in rhesus macaques. Administration of anti-PD-1 antibody 10 days prior to ART initiation rapidly enhanced antiviral CD8+ T cell function and diminished IFN-stimulated genes. This resulted in faster viral suppression in plasma and better Th17 cell reconstitution in the rectal mucosa following ART initiation. PD-1 blockade during ART resulted in lower levels of cell-associated replication-competent virus. Following ART interruption, PD-1 antibody-treated animals showed markedly higher expansion of proliferating CXCR5+perforin+granzyme B+ effector CD8+ T cells and lower regulatory T cells that resulted in better control of viremia. Our results show that PD-1 blockade can be administered safely with ART to augment antiviral CD8+ T cell function and reduce the viral reservoir, leading to improved control of viral rebound after ART interruption.

Published
2018

15. Transplantation of CCR5∆32 Homozygous Umbilical Cord Blood in a Child With Acute Lymphoblastic Leukemia and Perinatally Acquired HIV Infection.

Author

Rothenberger, Meghan, Wagner, John E, Haase, Ashley, Richman, Douglas, Grzywacz, Bartosz, Strain, Matthew, Lada, Steven, Estes, Jacob, Fletcher, Courtney V, Podany, Anthony T, Anderson, Jodi, Schmidt, Thomas, Wietgrefe, Steve, Schacker, Timothy, and Verneris, Michael R

Subjects
CCR5∆32, HIV cure, HIV reservoirs, allogeneic bone marrow transplantation, CCR5 Delta 32, Transplantation, Pediatric, HIV/AIDS, Hematology, Stem Cell Research, Stem Cell Research - Nonembryonic - Human, Cancer, Regenerative Medicine, Infection
Abstract

BackgroundAllogeneic hematopoietic cell transplantation (allo-HCT) in a CCR5∆32 homozygous donor resulted in HIV cure. Understanding how allo-HCT impacts the HIV reservoir will inform cure strategies.MethodsA 12-year-old with perinatally acquired, CCR5-tropic HIV and acute lymphoblastic leukemia underwent myeloablative conditioning and umbilical cord blood (UCB) transplantation from a CCR5∆32 homozygous donor. Peripheral blood mononuclear cells (PBMCs) and the rectum were sampled pre- and post-transplant. The brain, lung, lymph node (LN), stomach, duodenum, ileum, and colon were sampled 73 days after transplantation (day +73), when the patient died from graft-vs-host disease. Droplet digital polymerase chain reaction (ddPCR) and in situ hybridization (ISH) were used detect the HIV reservoir in tissues. CCR5 and CD3 expression in the LN was assessed using immunohistochemistry (IHC).ResultsHIV DNA (vDNA) was detected in PBMCs by ddPCR pretransplant but not post-transplant. vDNA was detected by ISH in the rectum at days -8 and +22, and in the LN, colon, lung, and brain day +73. vDNA was also detected in the lung by ddPCR. IHC revealed CCR5+CD3+ cells in the LN postmortem.ConclusionsHIV was detected in multiple tissues 73 days after CCR5∆32 homozygous UCB allo-HCT despite myeloablative conditioning and complete donor marrow engraftment. These results highlight the importance of analyzing tissue during HIV cure interventions and inform the choice of assay used to detect HIV in tissue reservoirs.

Published
2018

16. Telmisartan Therapy Does Not Improve Lymph Node or Adipose Tissue Fibrosis More Than Continued Antiretroviral Therapy Alone

Author

Utay, Netanya S, Kitch, Douglas W, Yeh, Eunice, Fichtenbaum, Carl J, Lederman, Michael M, Estes, Jacob D, Deleage, Claire, Magyar, Clara, Nelson, Scott D, Klingman, Karen L, Bastow, Barbara, Luque, Amneris E, McComsey, Grace A, Douek, Daniel C, Currier, Judith S, Lake, Jordan E, Aweeka, Francesca, Baer, Jenifer, Benns, Alex, Dragavon, Joan, Hensel, Christopher, Hsue, Priscilla, Kaytes, Andy, Ribaudo, Heather, Rusin, David, Shin, Katherine, Simmons, Antoine, and Zhan, Xinyan

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Infectious Diseases, Sexually Transmitted Infections, HIV/AIDS, Clinical Research, Clinical Trials and Supportive Activities, 6.1 Pharmaceuticals, Evaluation of treatments and therapeutic interventions, Infection, Adipose Tissue, Adult, Antihypertensive Agents, Antiretroviral Therapy, Highly Active, Female, Fibrosis, HIV Infections, Humans, Inflammation, Lymph Nodes, Male, Middle Aged, PPAR gamma, Telmisartan, HIV, ART, lymph node fibrosis, adipose tissue fibrosis, TGF-beta, A5317 AIDS Clinical Trials Group Team, Biological Sciences, Medical and Health Sciences, Microbiology, Biological sciences, Biomedical and clinical sciences, Health sciences
Abstract

BackgroundFibrosis in lymph nodes may limit CD4+ T-cell recovery, and lymph node and adipose tissue fibrosis may contribute to inflammation and comorbidities despite antiretroviral therapy (ART). We hypothesized that the angiotensin receptor blocker and peroxisome proliferator-activated receptor γ agonist telmisartan would decrease lymph node or adipose tissue fibrosis in treated human immunodeficiency virus type 1 (HIV) infection.MethodsIn this 48-week, randomized, controlled trial, adults continued HIV-suppressive ART and received telmisartan or no drug. Collagen I, fibronectin, and phosphorylated SMAD3 (pSMAD3) deposition in lymph nodes, as well as collagen I, collagen VI, and fibronectin deposition in adipose tissue, were quantified by immunohistochemical analysis at weeks 0 and 48. Two-sided rank sum and signed rank tests compared changes over 48 weeks.ResultsForty-four participants enrolled; 35 had paired adipose tissue specimens, and 29 had paired lymph node specimens. The median change overall in the percentage of the area throughout which collagen I was deposited was -2.6 percentage points (P = 0.08) in lymph node specimens and -1.3 percentage points (P = .001) in adipose tissue specimens, with no between-arm differences. In lymph node specimens, pSMAD3 deposition changed by -0.5 percentage points overall (P = .04), with no between-arm differences. Telmisartan attenuated increases in fibronectin deposition (P = .06). In adipose tissue, changes in collagen VI deposition (-1.0 percentage point; P = .001) and fibronectin deposition (-2.4 percentage points; P < .001) were observed, with no between-arm differences.ConclusionsIn adults with treated HIV infection, lymph node and adipose tissue fibrosis decreased with continued ART alone, with no additional fibrosis reduction with telmisartan therapy.

Published
2018

18. Defining total-body AIDS-virus burden with implications for curative strategies

Author

Estes, Jacob D, Kityo, Cissy, Ssali, Francis, Swainson, Louise, Makamdop, Krystelle Nganou, Del Prete, Gregory Q, Deeks, Steven G, Luciw, Paul A, Chipman, Jeffrey G, Beilman, Gregory J, Hoskuldsson, Torfi, Khoruts, Alexander, Anderson, Jodi, Deleage, Claire, Jasurda, Jacob, Schmidt, Thomas E, Hafertepe, Michael, Callisto, Samuel P, Pearson, Hope, Reimann, Thomas, Schuster, Jared, Schoephoerster, Jordan, Southern, Peter, Perkey, Katherine, Shang, Liang, Wietgrefe, Stephen W, Fletcher, Courtney V, Lifson, Jeffrey D, Douek, Daniel C, McCune, Joseph M, Haase, Ashley T, and Schacker, Timothy W

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Immunology, HIV/AIDS, Infectious Diseases, Sexually Transmitted Infections, 2.2 Factors relating to the physical environment, Aetiology, Infection, Good Health and Well Being, Anti-HIV Agents, DNA, Viral, HIV, HIV Infections, Humans, Lymphoid Tissue, RNA, Viral, Viral Load, Medical and Health Sciences, Biomedical and clinical sciences, Health sciences
Abstract

In the quest for a functional cure or the eradication of HIV infection, it is necessary to know the sizes of the reservoirs from which infection rebounds after treatment interruption. Thus, we quantified SIV and HIV tissue burdens in tissues of infected nonhuman primates and lymphoid tissue (LT) biopsies from infected humans. Before antiretroviral therapy (ART), LTs contained >98% of the SIV RNA+ and DNA+ cells. With ART, the numbers of virus (v) RNA+ cells substantially decreased but remained detectable, and their persistence was associated with relatively lower drug concentrations in LT than in peripheral blood. Prolonged ART also decreased the levels of SIV- and HIV-DNA+ cells, but the estimated size of the residual tissue burden of 108 vDNA+ cells potentially containing replication-competent proviruses, along with evidence of continuing virus production in LT despite ART, indicated two important sources for rebound following treatment interruption. The large sizes of these tissue reservoirs underscore challenges in developing 'HIV cure' strategies targeting multiple sources of virus production.

Published
2017

19. A Randomized Controlled Trial of Lisinopril to Decrease Lymphoid Fibrosis in Antiretroviral-Treated, HIV-infected Individuals

Author

Cockerham, Leslie R, Yukl, Steven A, Harvill, Kara, Somsouk, Ma, Joshi, Sunil K, Sinclair, Elizabeth, Liegler, Teri, Hoh, Rebecca, Lyons, Sophie, Hunt, Peter W, Rupert, Adam, Sereti, Irini, Morcock, David R, Rhodes, Ajantha, Emson, Claire, Hellerstein, Marc K, Estes, Jacob D, Lewin, Sharon, Deeks, Steven G, and Hatano, Hiroyu

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Infectious Diseases, Clinical Research, HIV/AIDS, Clinical Trials and Supportive Activities, Sexually Transmitted Infections, Evaluation of treatments and therapeutic interventions, 6.1 Pharmaceuticals, Infection, Good Health and Well Being, Anti-Inflammatory Agents/*therapeutic use, CD4 Lymphocyte Count, Disease Reservoirs/*virology, HIV, Lymphoid fibrosis, T-cell activation, Clinical sciences, Medical microbiology
Abstract

BackgroundIn HIV infection, lymphoid tissue is disrupted by fibrosis. Angiotensin converting enzyme inhibitors have anti-fibrotic properties. We completed a pilot study to assess whether the addition of lisinopril to antiretroviral therapy (ART) reverses fibrosis of gut tissue, and whether this leads to reduction of HIV RNA and DNA levels.MethodsThirty HIV-infected individuals on ART were randomized to lisinopril at 20mg daily or matching placebo for 24 weeks. All participants underwent rectal biopsies prior to starting the study drug and at 22 weeks, and there were regular blood draws. The primary end point was the change in HIV RNA and DNA levels in rectal tissue. Secondary outcomes included the change in 1) HIV levels in blood; 2) Gag-specific T-cell responses; 3) levels of T-cell activation; and 4) collagen deposition.ResultsThe addition of lisinopril did not have a significant effect on the levels of HIV RNA or DNA in gut tissue or blood, Gag-specific responses, or levels of T-cell activation. Lisinopril also did not have a significant impact on lymphoid fibrosis in the rectum, as assessed by quantitative histology or heavy water labeling.ConclusionsTreatment with lisinopril for 24 weeks in HIV-infected adults did not have an effect on lymphoid fibrosis, immune activation, or gut tissue viral reservoirs. Further study is needed to see if other anti-fibrotic agents may be useful in reversing lymphoid fibrosis and reducing HIV levels.

Published
2017

21. HIV transcription persists in the brain of virally suppressed people with HIV.

Author

Jamal Eddine, Janna, Angelovich, Thomas A., Zhou, Jingling, Byrnes, Sarah J., Tumpach, Carolin, Saraya, Nadia, Chalmers, Emily, Shepherd, Rory A., Tan, Abigail, Marinis, Stephanie, Gorry, Paul R., Estes, Jacob D., Brew, Bruce J., Lewin, Sharon R., Telwatte, Sushama, Roche, Michael, and Churchill, Melissa J.

Subjects
FRONTAL lobe, GENETIC transcription, MYELOID cells, NEUROBEHAVIORAL disorders, POLYMERASE chain reaction
Abstract

HIV persistence in the brain is a barrier to cure, and potentially contributes to HIV-associated neurocognitive disorders. Whether HIV transcription persists in the brain despite viral suppression with antiretroviral therapy (ART) and is subject to the same blocks to transcription seen in other tissues and blood, is unclear. Here, we quantified the level of HIV transcripts in frontal cortex tissue from virally suppressed or non-virally suppressed people with HIV (PWH). HIV transcriptional profiling of frontal cortex brain tissue (and PBMCs where available) from virally suppressed (n = 11) and non-virally suppressed PWH (n = 13) was performed using digital polymerase chain reaction assays (dPCR). CD68+ myeloid cells or CD3+ T cells expressing HIV p24 protein present in frontal cortex tissue was detected using multiplex immunofluorescence imaging. Frontal cortex brain tissue from PWH had HIV TAR (n = 23/24) and Long-LTR (n = 20/24) transcripts. Completion of HIV transcription was evident in brain tissue from 12/13 non-virally suppressed PWH and from 5/11 virally suppressed PWH, with HIV p24+CD68+ cells detected in these individuals. While a block to proximal elongation was present in frontal cortex tissue from both PWH groups, this block was more extensive in virally suppressed PWH. These findings suggest that the brain is a transcriptionally active HIV reservoir in a subset of virally suppressed PWH. Author summary: HIV reservoirs have been shown to persist within the brain of people with HIV (PWH) despite antiretroviral therapy (ART). Whether this reservoir is transcriptionally or translationally active within the brain during ART remains unclear. We demonstrated that transcription persists in brain of virally suppressed PWH, although at a lower level than reservoirs in circulation CD4+ T cells. Furthermore, while HIV transcripts related to initiation of HIV transcription were detected in brain tissue from all virally suppressed PWH assessed, transcripts related to the completion of transcription was only evident in a small subset. Within this subset, we further demonstrated the presence of HIV proteins within resident brain cells. Our study characterises the persistence of ongoing HIV transcription and translation within the brain of PWH despite viral suppression. This may provide a source of neuroinflammation and contribute to the development of HIV associated neurocognitive disorders. [ABSTRACT FROM AUTHOR]

Published
2024
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22. IL-15 promotes activation and expansion of CD8+ T cells in HIV-1 infection

Author

Younes, Souheil-Antoine, Freeman, Michael L, Mudd, Joseph C, Shive, Carey L, Reynaldi, Arnold, Panigrahi, Soumya, Estes, Jacob D, Deleage, Claire, Lucero, Carissa, Anderson, Jodi, Schacker, Timothy W, Davenport, Miles P, McCune, Joseph M, Hunt, Peter W, Lee, Sulggi A, Serrano-Villar, Sergio, Debernardo, Robert L, Jacobson, Jeffrey M, Canaday, David H, Sekaly, Rafick-Pierre, Rodriguez, Benigno, Sieg, Scott F, and Lederman, Michael M

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Sexually Transmitted Infections, HIV/AIDS, Clinical Research, Infectious Diseases, Health Disparities, Minority Health, Women's Health, 2.1 Biological and endogenous factors, Aetiology, Infection, Good Health and Well Being, Adult, Aged, Animals, Anti-Retroviral Agents, Biopsy, CD8-Positive T-Lymphocytes, Case-Control Studies, Cell Proliferation, Female, Granzymes, HIV Infections, HIV-1, Haplotypes, Humans, Interleukin-15, Ki-67 Antigen, Leukocyte Common Antigens, Leukocytes, Mononuclear, Lymph Nodes, Lymphocyte Activation, Male, Mice, Middle Aged, Phenotype, Receptors, CCR7, Medical and Health Sciences, Biological sciences, Biomedical and clinical sciences, Health sciences
Abstract

In HIV-1-infected patients, increased numbers of circulating CD8+ T cells are linked to increased risk of morbidity and mortality. Here, we identified a bystander mechanism that promotes CD8 T cell activation and expansion in untreated HIV-1-infected patients. Compared with healthy controls, untreated HIV-1-infected patients have an increased population of proliferating, granzyme B+, CD8+ T cells in circulation. Vβ expression and deep sequencing of CDR3 revealed that in untreated HIV-1 infection, cycling memory CD8 T cells possess a broad T cell repertoire that reflects the repertoire of the resting population. This suggests that cycling is driven by bystander activation, rather than specific antigen exposure. Treatment of peripheral blood mononuclear cells with IL-15 induced a cycling, granzyme B+ phenotype in CD8+ T cells. Moreover, elevated IL-15 expression in the lymph nodes of untreated HIV-1-infected patients correlated with circulating CD8+ T cell counts and was normalized in these patients following antiretroviral therapy. Together, these results suggest that IL-15 drives bystander activation of CD8+ T cells, which predicts disease progression in untreated HIV-1-infected patients and suggests that elevated IL-15 may also drive CD8+ T cell expansion that is linked to increased morbidity and mortality in treated patients.

Published
2016

23. Ad26 vaccine protects against SARS-CoV-2 severe clinical disease in hamsters

Author

Tostanoski, Lisa H., Wegmann, Frank, Martinot, Amanda J., Loos, Carolin, McMahan, Katherine, Mercado, Noe B., Yu, Jingyou, Chan, Chi N., Bondoc, Stephen, Starke, Carly E., Nekorchuk, Michael, Busman-Sahay, Kathleen, Piedra-Mora, Cesar, Wrijil, Linda M., Ducat, Sarah, Custers, Jerome, Atyeo, Caroline, Fischinger, Stephanie, Burke, John S., Feldman, Jared, Hauser, Blake M., Caradonna, Timothy M., Bondzie, Esther A., Dagotto, Gabriel, Gebre, Makda S., Jacob-Dolan, Catherine, Lin, Zijin, Mahrokhian, Shant H., Nampanya, Felix, Nityanandam, Ramya, Pessaint, Laurent, Porto, Maciel, Ali, Vaneesha, Benetiene, Dalia, Tevi, Komlan, Andersen, Hanne, Lewis, Mark G., Schmidt, Aaron G., Lauffenburger, Douglas A., Alter, Galit, Estes, Jacob D., Schuitemaker, Hanneke, Zahn, Roland, and Barouch, Dan H.

Published
2020
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24. CTLA-4 and PD-1 dual blockade induces SIV reactivation without control of rebound after antiretroviral therapy interruption

Author

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

Published
2020
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25. Robust and persistent reactivation of SIV and HIV by N-803 and depletion of CD8+ cells

Author

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

Published
2020
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26. Gut epithelial barrier and systemic inflammation during chronic HIV infection

Author

Somsouk, Ma, Estes, Jacob D, Deleage, Claire, Dunham, Richard M, Albright, Rebecca, Inadomi, John M, Martin, Jeffrey N, Deeks, Steven G, McCune, Joseph M, and Hunt, Peter W

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Infectious Diseases, Clinical Research, HIV/AIDS, Sexually Transmitted Infections, 2.1 Biological and endogenous factors, Aetiology, Infection, Adult, Antiretroviral Therapy, Highly Active, Apoptosis, CD4-Positive T-Lymphocytes, Cell Proliferation, Chronic Disease, Cross-Sectional Studies, Epithelial Cells, Female, HIV Infections, HIV-1, Humans, Indoleamine-Pyrrole 2, 3, -Dioxygenase, Inflammation, Interleukin-6, Intestinal Mucosa, Lipopolysaccharide Receptors, Male, Middle Aged, Neutrophil Infiltration, epithelial proliferation, HIV, immune activation, inflammation, microbial translocation, Biological Sciences, Medical and Health Sciences, Psychology and Cognitive Sciences, Virology, Biomedical and clinical sciences, Health sciences
Abstract

ObjectiveMicrobial translocation and innate immune action characterize HIV infection. Continued gut mucosal dysfunction during treatment and its relationship to CD4 T-cell recovery has not been well described.DesignA cross-sectional study was performed of antiretroviral therapy (ART)-suppressed (immunologic responders with CD4 > 500 cells/μl and immunologic nonresponders with CD4

Published
2015

28. Rapamycin limits [CD4.sup.+] T cell proliferation in simian immunodeficiency virus-infected rhesus macaques on antiretroviral therapy

Author

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

Subjects
Rhesus monkey -- Drug therapy, Antiviral agents -- Testing, T cell proliferation -- Research, Rapamycin -- Testing, HIV infection -- Drug therapy -- Models, Health care industry
Abstract

Proliferation of latently infected [CD4.sup.+] 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.sup.+] 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.sup.+] TM cells, chronic mTOR inhibition alone or in combination with T cell activation was not sufficient to disrupt the stability of the SIV reservoir., Introduction The advent of antiretroviral therapy (ART) has dramatically improved the life expectancy of people with HIV (PWH) infection. However, current ART regimens act by blocking de novo infection of [...]

Published
2022
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29. Interleukin-10 contributes to reservoir establishment and persistence in SIV-infected macaques treated with antiretroviral therapy

Author

Harper, Justin, Ribeiro, Susan P., Chan, Chi Ngai, Aid, Malika, Deleage, Claire, Micci, Luca, Pino, Maria, Cervasi, Barbara, Raghunathan, Gopalan, Rimmer, Eric, Ayanoglu, Gulesi, Wu, Guoxin, Shenvi, Neeta, Barnard, Richard J.O., Del Prete, Gregory Q., Busman-Sahay, Kathleen, Silvestri, Guido, Kulpa, Deanna A., Bosinger, Steven E., Easley, Kirk A., Howell, Bonnie J., Gorman, Dan, Hazuda, Daria J., Estes, Jacob D., Sekaly, Rafick-Pierre, and Paiardini, Mirko

Subjects
Immunological research, Immune response -- Research, Viremia -- Measurement, Interleukin-10 -- Health aspects, Health care industry
Abstract

Interleukin-10 (IL-10) is an immunosuppressive cytokine that signals through STAT3 to regulate T follicular helper (Tfh) cell differentiation and germinal center formation. In SIV-infected macaques, levels of IL-10 in plasma and lymph nodes (LNs) were induced by infection and not normalized with antiretroviral therapy (ART). During chronic infection, plasma IL-10 and transcriptomic signatures of IL-10 signaling were correlated with the cell-associated SIV-DNA content within LN [CD4.sup.+] memory subsets, including Tfh cells, and predicted the frequency of [CD4.sup.+] Tfh cells and their cell-associated SIV-DNA content during ART, respectively. In ART-treated rhesus macaques, cells harboring SIV-DNA by DNAscope were preferentially found in the LN B cell follicle in proximity to IL-10. Finally, we demonstrated that the in vivo neutralization of soluble IL-10 in ART-treated, SIV-infected macaques reduced B cell follicle maintenance and, by extension, LN memory [CD4.sup.+] T cells, including Tfh cells and those expressing PD-1 and CTLA-4. Thus, these data support a role for IL-10 in maintaining a pool of target cells in lymphoid tissue that serve as a niche for viral persistence. Targeting IL-10 signaling to impair [CD4.sup.+] T cell survival and improve antiviral immune responses may represent a novel approach to limit viral persistence in ART-suppressed people living with HIV., Introduction While the optimization of antiretroviral therapy (ART) has prevented AIDS and reduced HIV-related morbidities and mortality for the majority of people living with HIV (PLWH), a therapeutic regimen capable [...]

Published
2022
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33. Altered distribution of mucosal NK cells during HIV infection

Author

Sips, Magdalena, Sciaranghella, Gaia, Diefenbach, Thomas, Dugast, Anne-Sophie, Berger, Christoph T, Liu, Qingquan, Kwon, Douglas, Ghebremichael, Musie, Estes, Jacob D, Carrington, Mary, Martin, Jeffrey N, Deeks, Steven G, Hunt, Peter W, and Alter, Galit

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Clinical Research, Sexually Transmitted Infections, Infectious Diseases, HIV/AIDS, Aetiology, 2.1 Biological and endogenous factors, Infection, Inflammatory and immune system, Antiretroviral Therapy, Highly Active, Biomarkers, Pharmacological, Biopsy, Cell Movement, DNA Mutational Analysis, Genotype, HIV, HIV Infections, HLA Antigens, Humans, Intestinal Mucosa, Killer Cells, Natural, Lymphocyte Subsets, Polymorphism, Genetic, Receptors, KIR, Biological Sciences, Medical and Health Sciences
Abstract

The human gut mucosa is a major site of human immunodeficiency virus (HIV) infection and infection-associated pathogenesis. Increasing evidence shows that natural killer (NK) cells have an important role in control of HIV infection, but the mechanism(s) by which they mediate antiviral activity in the gut is unclear. Here, we show that two distinct subsets of NK cells exist in the gut, one localized to intraepithelial spaces (intraepithelial lymphocytes, IELs) and the other to the lamina propria (LP). The frequency of both subsets of NK cells was reduced in chronic infection, whereas IEL NK cells remained stable in spontaneous controllers with protective killer immunoglobulin-like receptor/human leukocyte antigen genotypes. Both IEL and LP NK cells were significantly expanded in immunological non-responsive patients, who incompletely recovered CD4+ T cells on highly active antiretroviral therapy (HAART). These data suggest that both IEL and LP NK cells may expand in the gut in an effort to compensate for compromised CD4+ T-cell recovery, but that only IEL NK cells may be involved in providing durable control of HIV in the gut.

Published
2012

34. Damaged intestinal epithelial integrity linked to microbial translocation in pathogenic simian immunodeficiency virus infections.

Author

Estes, Jacob D, Harris, Levelle D, Klatt, Nichole R, Tabb, Brian, Pittaluga, Stefania, Paiardini, Mirko, Barclay, G Robin, Smedley, Jeremy, Pung, Rhonda, Oliveira, Kenneth M, Hirsch, Vanessa M, Silvestri, Guido, Douek, Daniel C, Miller, Christopher J, Haase, Ashley T, Lifson, Jeffrey, and Brenchley, Jason M

Subjects
Intestinal Mucosa, Animals, Cercocebus atys, Macaca mulatta, Simian Acquired Immunodeficiency Syndrome, Virology, Microbiology, Immunology, Medical Microbiology
Abstract

The chronic phase of HIV infection is marked by pathological activation of the immune system, the extent of which better predicts disease progression than either plasma viral load or CD4(+) T cell count. Recently, translocation of microbial products from the gastrointestinal tract has been proposed as an underlying cause of this immune activation, based on indirect evidence including the detection of microbial products and specific immune responses in the plasma of chronically HIV-infected humans or SIV-infected Asian macaques. We analyzed tissues from SIV-infected rhesus macaques (RMs) to provide direct in situ evidence for translocation of microbial constituents from the lumen of the intestine into the lamina propria and to draining and peripheral lymph nodes and liver, accompanied by local immune responses in affected tissues. In chronically SIV-infected RMs this translocation is associated with breakdown of the integrity of the epithelial barrier of the gastrointestinal (GI) tract and apparent inability of lamina propria macrophages to effectively phagocytose translocated microbial constituents. By contrast, in the chronic phase of SIV infection in sooty mangabeys, we found no evidence of epithelial barrier breakdown, no increased microbial translocation and no pathological immune activation. Because immune activation is characteristic of the chronic phase of progressive HIV/SIV infections, these findings suggest that increased microbial translocation from the GI tract, in excess of capacity to clear the translocated microbial constituents, helps drive pathological immune activation. Novel therapeutic approaches to inhibit microbial translocation and/or attenuate chronic immune activation in HIV-infected individuals may complement treatments aimed at direct suppression of viral replication.

Published
2010

35. Dual blockade of IL-10 and PD-1 leads to control of SIV viral rebound following analytical treatment interruption.

Author

Sekaly, Rafick, primary, Ribeiro, Susan Pereira, additional, Strongin, Zachary, additional, Caten, Felipe Ten, additional, Ghneim, Khader, additional, Sanchez, Gabriela Pacheco, additional, de Medeiros, Giuliana Xavier, additional, Pelletier, Adam-Nicolas, additional, Hoang, Timothy, additional, Nguyen, Kevin, additional, Jean, Sherrie, additional, Wallace, Chelsea, additional, Balderas, Robert, additional, Lifson, Jeffrey, additional, Raghunathan, Gopalan, additional, Rimmer, Eric, additional, Pastuskovas, Cinthia, additional, Wu, Guoxin, additional, Micci, Luca, additional, Ribeiro, Ruy, additional, Chan, Chi, additional, Estes, Jacob, additional, Silvestri, Guido, additional, Gorman, Daniel M, additional, Howell, Bonnie, additional, Hazuda, Daria J, additional, and Paiardini, Mirko, additional

Published
2023
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36. REGIONAL ANALYSIS OF INTACT AND DEFECTIVE HIV PROVIRUSES IN THE BRAIN OF VIREMIC AND VIRALLY SUPPRESSED PEOPLE WITH HIV

Author

Angelovich, Thomas A., primary, Cochrane, Catherine R., additional, Zhou, Jingling, additional, Tumpach, Carolin, additional, Byrnes, Sarah J., additional, Jamal Eddine, Janna, additional, Waring, Emily, additional, Busman‐Sahay, Kathleen, additional, Deleage, Claire, additional, Jenkins, Trisha A., additional, Hearps, Anna C., additional, Turville, Stuart, additional, Gorry, Paul R, additional, Lewin, Sharon R., additional, Brew, Bruce J., additional, Estes, Jacob D, additional, Roche, Michael, additional, and Churchill, Melissa J., additional

Published
2023
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37. Correction: Tracking the Luminal Exposure and Lymphatic Drainage Pathways of Intravaginal and Intrarectal Inocula Used in Nonhuman Primate Models of HIV Transmission

Author

Smedley, Jeremy, primary, Turkbey, Baris, additional, Bernardo, Marcelino L., additional, Del Prete, Gregory Q., additional, Estes, Jacob D., additional, Griffiths, Gary L., additional, Kobayashi, Hisataka, additional, Choyke, Peter L., additional, Lifson, Jeffrey D., additional, and Keele, Brandon F., additional

Published
2023
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38. Lymph-Node-Based CD3 + CD20 + Cells Emerge from Membrane Exchange between T Follicular Helper Cells and B Cells and Increase Their Frequency following Simian Immunodeficiency Virus Infection

Author

Samer, Sadia, primary, Chowdhury, Ankita, additional, Wiche Salinas, Tomas Raul, additional, Estrada, Perla M. Del Rio, additional, Reuter, Morgan, additional, Tharp, Gregory, additional, Bosinger, Steven, additional, Cervasi, Barbara, additional, Auger, James, additional, Gill, Kiran, additional, Ablanedo-Terrazas, Yuria, additional, Reyes-Teran, Gustavo, additional, Estes, Jacob D., additional, Betts, Michael R., additional, Silvestri, Guido, additional, and Paiardini, Mirko, additional

Published
2023
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41. LAIR-1 expression on SIV-specific CD8 T cells is associated with T cell impairment and disease progression

Author

Govindaraj, Sakthivel, primary, Sharma, Asish Arunkumar, additional, Ali, Syed, additional, Babu, Hemalatha, additional, Busman-Sahay, Katheleen, additional, Bosinger, Steven, additional, Estes, Jacob, additional, Sekaly, Rafick-Pierre, additional, Villenger, Francois, additional, Amara, Rama Rao, additional, and Velu, Vijayakumar, additional

Published
2023
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42. Correction: Mitigation of endemic GI-tract pathogen-mediated inflammation through development of multimodal treatment regimen and its impact on SIV acquisition in rhesus macaques

Author

Bochart, Rachele M., primary, Busman-Sahay, Kathleen, additional, Bondoc, Stephen, additional, Morrow, David W., additional, Ortiz, Alexandra M., additional, Fennessey, Christine M., additional, Fischer, Miranda B., additional, Shiel, Oriene, additional, Swanson, Tonya, additional, Shriver-Munsch, Christine M., additional, Crank, Hugh B., additional, Armantrout, Kimberly M., additional, Barber-Axthelm, Aaron M., additional, Langner, Charlotte, additional, Moats, Cassandra R., additional, Labriola, Caralyn S., additional, MacAllister, Rhonda, additional, Axthelm, Michael K., additional, Brenchley, Jason M., additional, Keele, Brandon F., additional, Estes, Jacob D., additional, Hansen, Scott G., additional, and Smedley, Jeremy V., additional

Published
2023
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43. Supplementary Figure 5 from Molecular Response to Neoadjuvant Chemotherapy in High-Grade Serous Ovarian Carcinoma

Author

Arend, Rebecca C., primary, Londoño, Angelina I., primary, Montgomery, Allison M., primary, Smith, Haller J., primary, Dobbin, Zachary C., primary, Katre, Ashwini A., primary, Martinez, Alba, primary, Yang, Eddy S., primary, Alvarez, Ronald D., primary, Huh, Warner K., primary, Bevis, Kerri S., primary, Straughn, J. Michael, primary, Estes, Jacob M., primary, Novak, Lea, primary, Crossman, David K., primary, Cooper, Sara J., primary, Landen, Charles N., primary, and Leath, Charles A., primary

Published
2023
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44. Supplementary Tables 1 - 7 from Molecular Response to Neoadjuvant Chemotherapy in High-Grade Serous Ovarian Carcinoma

Author

Arend, Rebecca C., primary, Londoño, Angelina I., primary, Montgomery, Allison M., primary, Smith, Haller J., primary, Dobbin, Zachary C., primary, Katre, Ashwini A., primary, Martinez, Alba, primary, Yang, Eddy S., primary, Alvarez, Ronald D., primary, Huh, Warner K., primary, Bevis, Kerri S., primary, Straughn, J. Michael, primary, Estes, Jacob M., primary, Novak, Lea, primary, Crossman, David K., primary, Cooper, Sara J., primary, Landen, Charles N., primary, and Leath, Charles A., primary

Published
2023
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45. Data from Molecular Response to Neoadjuvant Chemotherapy in High-Grade Serous Ovarian Carcinoma

Author

Arend, Rebecca C., primary, Londoño, Angelina I., primary, Montgomery, Allison M., primary, Smith, Haller J., primary, Dobbin, Zachary C., primary, Katre, Ashwini A., primary, Martinez, Alba, primary, Yang, Eddy S., primary, Alvarez, Ronald D., primary, Huh, Warner K., primary, Bevis, Kerri S., primary, Straughn, J. Michael, primary, Estes, Jacob M., primary, Novak, Lea, primary, Crossman, David K., primary, Cooper, Sara J., primary, Landen, Charles N., primary, and Leath, Charles A., primary

Published
2023
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46. Supplementary Figure 2 from Molecular Response to Neoadjuvant Chemotherapy in High-Grade Serous Ovarian Carcinoma

Author

Arend, Rebecca C., primary, Londoño, Angelina I., primary, Montgomery, Allison M., primary, Smith, Haller J., primary, Dobbin, Zachary C., primary, Katre, Ashwini A., primary, Martinez, Alba, primary, Yang, Eddy S., primary, Alvarez, Ronald D., primary, Huh, Warner K., primary, Bevis, Kerri S., primary, Straughn, J. Michael, primary, Estes, Jacob M., primary, Novak, Lea, primary, Crossman, David K., primary, Cooper, Sara J., primary, Landen, Charles N., primary, and Leath, Charles A., primary

Published
2023
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47. Supplementary Figure 1 from Molecular Response to Neoadjuvant Chemotherapy in High-Grade Serous Ovarian Carcinoma

Author

Arend, Rebecca C., primary, Londoño, Angelina I., primary, Montgomery, Allison M., primary, Smith, Haller J., primary, Dobbin, Zachary C., primary, Katre, Ashwini A., primary, Martinez, Alba, primary, Yang, Eddy S., primary, Alvarez, Ronald D., primary, Huh, Warner K., primary, Bevis, Kerri S., primary, Straughn, J. Michael, primary, Estes, Jacob M., primary, Novak, Lea, primary, Crossman, David K., primary, Cooper, Sara J., primary, Landen, Charles N., primary, and Leath, Charles A., primary

Published
2023
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48. Supplementary Table, Figure Legends from Molecular Response to Neoadjuvant Chemotherapy in High-Grade Serous Ovarian Carcinoma

Author

Arend, Rebecca C., primary, Londoño, Angelina I., primary, Montgomery, Allison M., primary, Smith, Haller J., primary, Dobbin, Zachary C., primary, Katre, Ashwini A., primary, Martinez, Alba, primary, Yang, Eddy S., primary, Alvarez, Ronald D., primary, Huh, Warner K., primary, Bevis, Kerri S., primary, Straughn, J. Michael, primary, Estes, Jacob M., primary, Novak, Lea, primary, Crossman, David K., primary, Cooper, Sara J., primary, Landen, Charles N., primary, and Leath, Charles A., primary

Published
2023
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49. Supplementary Figure 3 from Molecular Response to Neoadjuvant Chemotherapy in High-Grade Serous Ovarian Carcinoma

Author

Arend, Rebecca C., primary, Londoño, Angelina I., primary, Montgomery, Allison M., primary, Smith, Haller J., primary, Dobbin, Zachary C., primary, Katre, Ashwini A., primary, Martinez, Alba, primary, Yang, Eddy S., primary, Alvarez, Ronald D., primary, Huh, Warner K., primary, Bevis, Kerri S., primary, Straughn, J. Michael, primary, Estes, Jacob M., primary, Novak, Lea, primary, Crossman, David K., primary, Cooper, Sara J., primary, Landen, Charles N., primary, and Leath, Charles A., primary

Published
2023
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50. Supplementary Figure 4 from Molecular Response to Neoadjuvant Chemotherapy in High-Grade Serous Ovarian Carcinoma

Author

Arend, Rebecca C., primary, Londoño, Angelina I., primary, Montgomery, Allison M., primary, Smith, Haller J., primary, Dobbin, Zachary C., primary, Katre, Ashwini A., primary, Martinez, Alba, primary, Yang, Eddy S., primary, Alvarez, Ronald D., primary, Huh, Warner K., primary, Bevis, Kerri S., primary, Straughn, J. Michael, primary, Estes, Jacob M., primary, Novak, Lea, primary, Crossman, David K., primary, Cooper, Sara J., primary, Landen, Charles N., primary, and Leath, Charles A., primary

Published
2023
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