Your search keyword '"SIV"' showing total 2,499 results

1. CSF1R inhibition depletes brain macrophages and reduces brain virus burden in SIV-infected macaques.

Author

Bohannon, Diana, Zablocki-Thomas, Laurent, Leung, Evan, Dupont, Jinbum, Hattler, Julian, Kowalewska, Jolanta, Zhao, Miaoyun, Luo, Jiangtao, Salemi, Marco, Amedee, Angela, Li, Qingsheng, Kuroda, Marcelo, and Kim, Woong-Ki

Subjects

BLZ945, CSF1R, HIV, SIV, perivascular macrophage, Animals, Simian Acquired Immunodeficiency Syndrome, Macaca mulatta, Simian Immunodeficiency Virus, Macrophages, Brain, Receptors, Granulocyte-Macrophage Colony-Stimulating Factor, Viral Load, Pyrimidines, Antigens, CD, Male, Microglia, Antigens, Differentiation, Myelomonocytic, Receptors, Cell Surface, Anisoles

Abstract

Perivascular macrophages (PVMs) and, to a lesser degree, microglia are targets and reservoirs of HIV and simian immunodeficiency virus (SIV) in the brain. Previously, we demonstrated that colony-stimulating factor 1 receptor (CSF1R) in PVMs was upregulated and activated in chronically SIV-infected rhesus macaques with encephalitis, correlating with SIV infection of PVMs. Herein, we investigated the role of CSF1R in the brain during acute SIV infection using BLZ945, a brain-penetrant CSF1R kinase inhibitor. Apart from three uninfected historic controls, nine Indian rhesus macaques were infected acutely with SIVmac251 and divided into three groups (n = 3 each): an untreated control and two groups treated for 20-30 days with low- (10 mg/kg/day) or high- (30 mg/kg/day) dose BLZ945. With the high-dose BLZ945 treatment, there was a significant reduction in cells expressing CD163 and CD206 across all four brain areas examined, compared with the low-dose treatment and control groups. In 9 of 11 tested regions, tissue viral DNA (vDNA) loads were reduced by 95%-99% following at least one of the two doses, and even to undetectable levels in some instances. Decreased numbers of CD163+ and CD206+ cells correlated significantly with lower levels of vDNA in all four corresponding brain areas. In contrast, BLZ945 treatment did not significantly affect the number of microglia. Our results indicate that doses as low as 10 mg/kg/day of BLZ945 are sufficient to reduce the tissue vDNA loads in the brain with no apparent adverse effect. This study provides evidence that infected PVMs are highly sensitive to CSF1R inhibition, opening new possibilities to achieve viral clearance.

Published

2024

2. Minimally Modified HIV-1 Infection of Macaques: Development, Utility, and Limitations of Current Models.

Author

Sharma, Manish, Nag, Mukta, and Del Prete, Gregory Q.

Abstract

Nonhuman primate (NHP) studies that utilize simian immunodeficiency virus (SIV) to model human immunodeficiency virus (HIV-1) infection have proven to be powerful, highly informative research tools. However, there are substantial differences between SIV and HIV-1. Accordingly, there are numerous research questions for which SIV-based models are not well suited, including studies of certain aspects of basic HIV-1 biology, and pre-clinical evaluations of many proposed HIV-1 treatment, prevention, and vaccination strategies. To overcome these limitations of NHP models of HIV-1 infection, several groups have pursued the derivation of a minimally modified HIV-1 (mmHIV-1) capable of establishing pathogenic infection in macaques that authentically recapitulates key features of HIV-1 in humans. These efforts have focused on three complementary objectives: (1) engineering HIV-1 to circumvent species-specific cellular restriction factors that otherwise potently inhibit HIV-1 in macaques, (2) introduction of a C chemokine receptor type 5 (CCR5)-tropic envelope, ideally that can efficiently engage macaque CD4, and (3) correction of gene expression defects inadvertently introduced during viral genome manipulations. While some progress has been made toward development of mmHIV-1 variants for use in each of the three macaque species (pigtail, cynomolgus, and rhesus), model development progress has been most promising in pigtail macaques (PTMs), which do not express an HIV-1-restricting tripartite motif-containing protein 5 α (TRIM5α). In our work, we have derived a CCR5-tropic mmHIV-1 clone designated stHIV-A19 that comprises 94% HIV-1 genome sequence and replicates to high acute-phase titers in PTMs. In animals treated with a cell-depleting CD8α antibody at the time of infection, stHIV-A19 maintains chronically elevated plasma viral loads with progressive CD4+ T-cell loss and the development of acquired immune-deficiency syndrome (AIDS)-defining clinical endpoints. However, in the absence of CD8α+ cell depletion, no mmHIV-1 model has yet displayed high levels of chronic viremia or AIDS-like pathogenesis. Here, we review mmHIV-1 development approaches, the phenotypes, features, limitations, and potential utility of currently available mmHIV-1s, and propose future directions to further advance these models. [ABSTRACT FROM AUTHOR]

Published

2024

3. Refinements in Clinical and Behavioral Management for Macaques on Infectious Disease Protocols.

Author

Martin, Lauren Drew, Shelton, Jaclyn, Houser, Lisa A., MacAllister, Rhonda, and Coleman, Kristine

Abstract

Simple Summary: Nonhuman primates (NHPs) on infectious disease studies can be challenging to manage both clinically and behaviorally. These animals may develop significant clinical signs as well as stress-related problems. Not only does this negatively affect the welfare of the animals, but it can also impact the validity of scientific outcomes. Thus, while collaboration between the veterinary and behavioral teams is critical to maximize animal welfare and research outcomes in any study, it is especially true in infectious disease work. In this review, we discuss some refinements to promote the psychological well-being and resiliency and to enhance the overall health of NHPs on infectious disease studies, which can help improve welfare and, in turn, scientific outcomes. Providing optimal clinical and behavioral care is a key component of promoting animal welfare for macaques and other nonhuman primates (NHPs) in research. This overlap between critical areas of management is particularly important for NHPs on infectious disease protocols, which often have unique challenges. For example, traditionally these NHPs were often housed alone, which can have behavioral and clinical consequences. However, in the past decade or so, considerable effort has been directed at modifying procedures in an effort to improve animal welfare for this group of NHPs. In this review, we examine some refinements that can positively impact the clinical and behavioral management of macaques on infectious disease studies, including increased social housing and the use of positive reinforcement techniques to train animals to cooperate with procedures such as daily injections or awake blood draws. We also discuss ways to facilitate the implementation of these refinements, as well as to identify logistical considerations for their implementation. Finally, we look to the future and consider what more we can do to improve the welfare of these animals. [ABSTRACT FROM AUTHOR]

Published

2024

4. Nonnegligible Contribution of Nonlymphoid Tissue to Viral Reservoir During the Short-Term Early cART in SIVmac239-Infected Chinese Rhesus Macaques.

Author

Tian, Ren-Rong, Li, Ting, Zhang, Ming-Xu, Song, Tian-Zhang, Zheng, Hong-Yi, and Zheng, Yong-Tang

Abstract

HIV/AIDS cannot be cured because of the persistence of the viral reservoir. Because of the complexity of the cellular composition and structure of the human organs, HIV reservoirs of anatomical site are also complex. Recently, although a variety of molecules have been reported to be involved in the establishment and maintenance of the viral reservoirs, or as marker of latent cells, the research mainly focuses on blood and lymph nodes. Now, the characteristics of the viral reservoir in tissue are not yet fully understood. In this study, various tissues were collected from SIVmac239-infected monkeys, and the level of total SIV DNA, SIV 2-LTR DNA, and cell-associated virus RNA in them were compared with character of the anatomical viral reservoir under early treatment. The results showed that short-term combination antiretroviral therapy (cART) starting from 3 days after infection could significantly inhibit viremia and reduce the size of the anatomical viral reservoir, but it could not eradicate de novo infections and ongoing replication of virus. Moreover, the effects of early cART on the level of total SIV DNA, SIV 2-LTR DNA, and cell-associated virus RNA in different tissues were different, which changed the size distribution of viral reservoir in anatomical site. Finally, the contribution of nonlymphoid tissues, especially liver and lung, to the viral reservoir increased after treatment, while the contribution of intestinal lymphoid to the viral reservoir significantly reduced. These results suggested that early treatment effectively decreased the size of viral reservoir, and that the effects of cART on the tissue viral reservoir varied greatly by tissue type. The results implied that persistent existence of virus in nonlymphoid tissues after short-term treatment suggested that the role of nonlymphoid tissues cannot be ignored in development strategies for AIDS therapy. [ABSTRACT FROM AUTHOR]

Published

2024

5. Schlieren Image Velocimetry and colorimetry for a burning candle and its thermal plume

Author

Raluca Andreea ROSU

Subjects

siv, particle image velocimetry (piv), calibrated color filter schlieren, image post-processing, high temperature flame, Motor vehicles. Aeronautics. Astronautics, TL1-4050

Abstract

This article explores the feasibility of generating velocity maps for a flame and its plume from a burning candle using Schlieren Image Velocimetry (SIV). Currently, SIV is predominantly employed in the literature to track highly turbulent flows by using the developing eddies as flow markers. The novelty of this study lies in evaluating the quality of a nearly laminar flame, which exhibits significant background density variation due to its own plume. In addition to the SIV technique, a brief assessment is conducted using a segmented color filter, specially designed and manufactured to evaluate the potential for measuring the temperature range of the flame.

Published

2024

6. Dual role for microbial short-chain fatty acids in modifying SIV disease trajectory following anti-α4β7 antibody administration.

Author

Johnson, Samuel D., Pilli, Nageswara, Yu, Jianshi, Knight, Lindsey A., Kane, Maureen A., and Byrareddy, Siddappa N.

Subjects

SHORT-chain fatty acids, CROHN'S disease, INFLAMMATORY bowel diseases, HIV, ULCERATIVE colitis

Abstract

Background: Human Immunodeficiency Virus (HIV)/Simian Immunodeficiency Virus (SIV) infection is associated with significant gut damage, similar to that observed in patients with inflammatory bowel disease (IBD). This pathology includes loss of epithelial integrity, microbial translocation, dysbiosis, and resultant chronic immune activation. Additionally, the levels of all-trans-retinoic acid (atRA) are dramatically attenuated. Data on the therapeutic use of anti-α4β7 antibodies has shown promise in patients with ulcerative colitis and Crohn's disease. Recent evidence has suggested that the microbiome and short-chain fatty acid (SCFA) metabolites it generates may be critical for anti-α4β7 efficacy and maintaining intestinal homeostasis. Materials and Methods: To determine whether the microbiome contributes to gut homeostasis after anti-α4β7 antibody administered to SIV-infected rhesus macaques, faecal SCFA concentrations were determined, 16S rRNA sequencing was performed, plasma viral loads were determined, plasma retinoids were measured longitudinally, and gut retinoid synthesis/response gene expression was quantified. Results: Our results suggest that anti-α4β7 antibody facilitates the return of retinoid metabolism to baseline levels after SIV infection. Furthermore, faecal SCFAs were shown to be associated with retinoid synthesis gene expression and rebound viral loads after therapy interruption. Conclusions: Taken together, these data demonstrate the therapeutic advantages of anti-α4β7 antibody administration during HIV/SIV infection and that the efficacy of anti-α4β7 antibody may depend on microbiome composition and SCFA generation. [ABSTRACT FROM AUTHOR]

Published

2024

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

Author

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

Subjects

VIRAL mutation, SIMIAN immunodeficiency virus, RHESUS monkeys, VACCINATION status, T cells

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. [ABSTRACT FROM AUTHOR]

Published

2024

8. The Association between IL-1β and IL-18 Levels, Gut Barrier Disruption, and Monocyte Activation during Chronic Simian Immunodeficiency Virus Infection and Long-Term Suppressive Antiretroviral Therapy.

Author

Thirugnanam, Siva, Wang, Chenxiao, Zheng, Chen, Grasperge, Brooke F., Datta, Prasun K., Rappaport, Jay, Qin, Xuebin, and Rout, Namita

Subjects

*MONONUCLEAR leukocytes, *FATTY acid-binding proteins, *INFLAMMATORY mediators, *RHESUS monkeys, *NEUROBEHAVIORAL disorders, *SIMIAN immunodeficiency virus, *HIV

Abstract

HIV-induced persistent immune activation is a key mediator of inflammatory comorbidities such as cardiovascular disease (CVD) and neurocognitive disorders. While a preponderance of data indicate that gut barrier disruption and microbial translocation are drivers of chronic immune activation, the molecular mechanisms of this persistent inflammatory state remain poorly understood. Here, utilizing the nonhuman primate model of Human Immunodeficiency Virus (HIV) infection with suppressive antiretroviral therapy (ART), we investigated activation of inflammasome pathways and their association with intestinal epithelial barrier disruption (IEBD). Longitudinal blood samples obtained from rhesus macaques with chronic SIV infection and long-term suppressive ART were evaluated for IEBD biomarkers, inflammasome activation (IL-1β and IL-18), inflammatory cytokines, and triglyceride (TG) levels. Activated monocyte subpopulations and glycolytic potential were investigated in peripheral blood mononuclear cells (PBMCs). During the chronic phase of treated SIV infection, elevated levels of plasma IL-1β and IL-18 were observed following the hallmark increase in IEBD biomarkers, intestinal fatty acid-binding protein (IFABP) and LPS-binding protein (LBP). Further, significant correlations of plasma IFABP levels with IL-1β and IL-18 were observed between 10 and 12 months of ART. Higher levels of sCD14, IL-6, and GM-CSF, among other inflammatory mediators, were also observed only during the long-term SIV + ART phase along with a trend of increase in the frequencies of activated CD14+CD16+ intermediate monocyte subpopulations. Lastly, we found elevated levels of blood TG and higher glycolytic capacity in PBMCs of chronic SIV-infected macaques with long-term ART. The increase in circulating IL-18 and IL-1β following IEBD and their significant positive correlation with IFABP suggest a connection between gut barrier disruption and inflammasome activation during chronic SIV infection, despite viral suppression with ART. Additionally, the increase in markers of monocyte activation, along with elevated TG and enhanced glycolytic pathway activity, indicates metabolic remodeling that could fuel metabolic syndrome. Further research is needed to understand the mechanisms by which gut dysfunction and inflammasome activation contribute to HIV-associated metabolic complications, enabling targeted interventions in people with HIV. [ABSTRACT FROM AUTHOR]

Published

2024

9. Schlieren Image Velocimetry and colorimetry for a burning candle and its thermal plume.

Author

ROSU, Raluca Andreea

Subjects

*FLAME temperature, *PARTICLE image velocimetry, *LIGHT filters, *TURBULENCE, *TURBULENT flow

Abstract

This article explores the feasibility of generating velocity maps for a flame and its plume from a burning candle using Schlieren Image Velocimetry (SIV). Currently, SIV is predominantly employed in the literature to track highly turbulent flows by using the developing eddies as flow markers. The novelty of this study lies in evaluating the quality of a nearly laminar flame, which exhibits significant background density variation due to its own plume. In addition to the SIV technique, a brief assessment is conducted using a segmented color filter, specially designed and manufactured to evaluate the potential for measuring the temperature range of the flame. [ABSTRACT FROM AUTHOR]

Published

2024

10. Immune restoration by TIGIT blockade is insufficient to control chronic SIV infection.

Author

Webb, Gabriela M., Pessoa, Cleiton T., McCullen, Allyson J., Hwang, Joseph M., Humkey, Matthew C., ThorminOdum, Raymond, Kukula, Kaitlyn A., Smedley, Jeremy, Fischer, Miranda, Sciurba, Joseph, Bochart, Rachele M., Shriver-Munsch, Christine, Ndhlovu, Lishomwa C., and Sacha, Jonah B.

Subjects

*T cells, *CYTOTOXIC T cells, *T-cell exhaustion, *KILLER cells, *T cell receptors, *IMMUNE checkpoint proteins

Abstract

TIGIT is a negative immune checkpoint receptor associated with T cell exhaustion in cancer and HIV. TIGIT upregulation in virus-specific CD8+ T cells and NK cells during HIV/SIV infection results in dysfunctional effector capabilities. In vitro studies targeting TIGIT on CD8+ T cells suggest TIGIT blockade as a viable strategy to restore SIV-specific T cell responses. Here, we extend these studies in vivo using TIGIT blockage in nonhuman primates in an effort to reverse T cell and NK cell exhaustion in the setting of SIV infection. We demonstrate that in vivo administration of a humanized anti-TIGIT monoclonal antibody (mAb) is well tolerated in both cynomolgus macaques and rhesus macaques. Despite sustained plasma concentrations of anti-TIGIT mAb, we observed no consistent improvement in NK or T cell cytolytic capacity. TIGIT blockade minimally enhanced T cell proliferation and virus-specific T cell responses in both magnitude and breadth though plasma viral loads in treated animals remained stable indicating that anti-TIGIT mAb treatment alone was insufficient to increase anti-SIV CD8+ T cell function. The enhancement of virus-specific T cell proliferative responses observed in vitro with single or dual blockade of TIGIT and/or PD-1 highlights TIGIT as a potential target to reverse T cell dysfunction. Our studies, however, reveal that targeting the TIGIT pathway alone may be insufficient in the setting of viremia and that combining immune checkpoint blockade with other immunotherapeutics may be a future path forward for improved viral control or elimination of HIV. IMPORTANCE Upregulation of the immune checkpoint receptor TIGIT is associated with HIV-mediated T cell dysfunction and correlates with HIV disease progression. Compelling evidence exists for targeting immune checkpoint receptor pathways that would potentially enhance immunity and refocus effector cell efforts toward viral clearance. In this report, we investigate TIGIT blockade as an immunotherapeutic approach to reverse immune exhaustion during chronic SIV/SHIV infection in a nonhuman primate model of HIV infection. We show that interfering with the TIGIT signaling axis alone is insufficient to improve viral control despite modest improvement in T cell immunity. Our data substantiate the use of targeting multiple immune checkpoint receptors to promote synergy and ultimately eliminate HIV-infected cells. [ABSTRACT FROM AUTHOR]

Published

2024

11. SIV infection and ARV treatment reshape the transcriptional and epigenetic profile of naïve and memory T cells in vivo.

Author

Rahmberg, Andrew R., Markowitz, Tovah E., Mudd, Joseph C., Ortiz, Alexandra M., and Brenchley, Jason M.

Subjects

*T cells, *IMMUNOLOGIC memory, *SIMIAN immunodeficiency virus, *HIV, *EPIGENETICS, *EPIGENOMICS, *GENE expression, *IMMUNOSENESCENCE

Abstract

Human and simian immunodeficiency viruses (HIV and SIV) are lentiviruses that reverse transcribe their RNA genome with subsequent integration into the genome of the target cell. How progressive infection and administration of antiretrovirals (ARVs) longitudinally influence the transcriptomic and epigenetic landscape of particular T cell subsets, and how these may influence the genetic location of integration are unclear. Here, we use RNAseq and ATACseq to study the transcriptomics and epigenetic landscape of longitudinally sampled naïve and memory CD4+ and CD8+ T cells in two species of non-human primates prior to SIV infection, during chronic SIV infection, and after administration of ARVs. We find that SIV infection leads to significant alteration to the transcriptomic profile of all T cell subsets that are only partially reversed by administration of ARVs. Epigenetic changes were more apparent in animals with longer periods of untreated SIV infection and correlated well with changes in corresponding gene expression. Known SIV integration sites did not vary due to SIV status but did contain more open chromatin in rhesus macaque memory T cells, and the expression of proteasome-related genes at the pre-SIV timepoint correlated with subsequent viremia. IMPORTANCE Chronic inflammation during progressive human and simian immunodeficiency virus (HIV and SIV) infections leads to significant co-morbidities in infected individuals with significant consequences. Antiretroviral (ARV)-treated individuals also manifest increased levels of inflammation which are associated with increased mortalities. These data will help guide rational development of modalities to reduce inflammation observed in people living with HIV and suggest mechanisms underlying lentiviral integration site preferences. [ABSTRACT FROM AUTHOR]

Published

2024

12. Interaction Between Vpx and SAMHD1, Vital for SAMHD1 Inhibition.

Author

Hasanshahi, Zahra, Dehghani, Behzad, and Hashempour, Ava

Abstract

It was confirmed that the sterile alpha motif and HD domain 1 (SAMHD1) limits human immunodeficiency virus type 1 (HIV-1) replication. In contrast, viral protein x (Vpx) in HIV-2 and some simian immunodeficiency viruses can counteract this effect. The possible interaction between SAMHD1 and Vpx was suggested by previous studies; however, there are no data to confirm this interaction. Therefore, this study aimed to study the interaction between two proteins and the properties of Vpx protein for the first time using bioinformatic tools. Vpx and SAMHD1 sequences were obtained from the National Center for Biotechnology Information GenBank. Several software were used to define Vpx properties and the interaction between Vpx and different SAMHD1 isoforms. Our findings indicated the difference in interaction sites among different Vpx. However, in all Vpx proteins, this region is from amino acids 4 to 90. In addition, two regions (26–31 and 134–139) and two amino acids 425 and 429 in SAMHD1 are vital in the possible interaction. In addition, our analysis determined the physicochemical and immunological properties of the Vpx. Considering all factors, this study could confirm that Vpx interacts with SAMHD1, which could inhibit SAMHD1. Moreover, our findings can pave the way for future studies to express and purify Vpx in the laboratory and study this protein in vitro. [ABSTRACT FROM AUTHOR]

Published

2024

13. SIV infection in sooty mangabeys does not impact survival but changes the relative frequency of the main cause of death

Author

Cristina Ceriani, Brianne Beisner, Maria Crane, Joyce Cohen, Ian N. Moore, Deanna A. Kulpa, Beatrice H. Hahn, and Guido Silvestri

Subjects

SIV, sooty mangabeys, SIV infection, cause of death, Microbiology, QR1-502

Abstract

ABSTRACT Sooty mangabeys (SMs) are natural hosts of simian immunodeficiency virus (SIV) and do not progress to AIDS despite high viral replication. The main factors involved in the benign nature of this infection are (i) low level of immune activation, (ii) relative preservation of specific CD4+ T-cell subsets from direct virus infection, and (iii) absence of microbial translocation from the gut to the systemic circulation. To determine the impact of SIV infection on underlying cause of death, we retrospectively analyzed data from 307 SMs (219 SIV infected and 88 uninfected) housed at the Emory Primate Center that have died between 1986 and 2022. Interestingly, we found that SIV-infected SMs live ~4 years longer than SIV-uninfected SMs, although this result is hard to interpret due to differences in how animals were housed and assigned to specific experimental studies. While the causes of death were not different between SIV-infected and uninfected SMs that died before age 15 (i.e., adult), we found significant differences in the relative frequency of specific causes of death in the elderly population (≥15 years old). Specifically, we observed that SIV-infected SMs were more likely to die from infections but less likely to die from cardiovascular disease (and diabetes in female animals) as compared to uninfected SMs. While confirming the non-pathogenic nature of SIV infection in SMs, these data reveal, for the first time, a qualitative impact of SIV infection on the host physiology that induces a significant change in the mortality pattern in these natural SIV hosts.IMPORTANCEIn this study, we demonstrate, for the first time, that the natural, non-pathogenic SIV infection of the African monkey SM has a clinical impact which is revealed in terms of main causes of mortality, which are significantly different in the infected animals as compared to the uninfected ones. Indeed, SIV-infected SMs are at higher risk of dying of infectious diseases but appear to be somewhat protected from cardiovascular causes of death. The identification of a specific pattern of mortality associated with the infection suggests that the host-pathogen interaction between SIV and the SM immune system, while non-pathogenic in nature, has a detectable impact on the overall health status of the animals.

Published

2024

14. HIHISIV: a database of gene expression in HIV and SIV host immune response

Author

Raquel L. Costa, Luiz Gadelha, Mirela D’arc, Marcelo Ribeiro-Alves, David L. Robertson, Jean-Marc Schwartz, Marcelo A. Soares, and Fábio Porto

Subjects

HIV-1, SIV, Immune response, High-throughput gene expression data, Computer applications to medicine. Medical informatics, R858-859.7, Biology (General), QH301-705.5

Abstract

Abstract In the battle of the host against lentiviral pathogenesis, the immune response is crucial. However, several questions remain unanswered about the interaction with different viruses and their influence on disease progression. The simian immunodeficiency virus (SIV) infecting nonhuman primates (NHP) is widely used as a model for the study of the human immunodeficiency virus (HIV) both because they are evolutionarily linked and because they share physiological and anatomical similarities that are largely explored to understand the disease progression. The HIHISIV database was developed to support researchers to integrate and evaluate the large number of transcriptional data associated with the presence/absence of the pathogen (SIV or HIV) and the host response (NHP and human). The datasets are composed of microarray and RNA-Seq gene expression data that were selected, curated, analyzed, enriched, and stored in a relational database. Six query templates comprise the main data analysis functions and the resulting information can be downloaded. The HIHISIV database, available at https://hihisiv.github.io , provides accurate resources for browsing and visualizing results and for more robust analyses of pre-existing data in transcriptome repositories.

Published

2024

15. Dual role for microbial short-chain fatty acids in modifying SIV disease trajectory following anti-α4β7 antibody administration

Author

Samuel D. Johnson, Nageswara Pilli, Jianshi Yu, Lindsey A. Knight, Maureen A. Kane, and Siddappa N. Byrareddy

Subjects

Anti-α4β7 antibodies, SIV, short-chain fatty acid (SCFA), 16S rRNA, retinoic acid, gut, Medicine

Abstract

AbstractBackground Human Immunodeficiency Virus (HIV)/Simian Immunodeficiency Virus (SIV) infection is associated with significant gut damage, similar to that observed in patients with inflammatory bowel disease (IBD). This pathology includes loss of epithelial integrity, microbial translocation, dysbiosis, and resultant chronic immune activation. Additionally, the levels of all-trans-retinoic acid (atRA) are dramatically attenuated. Data on the therapeutic use of anti-α4β7 antibodies has shown promise in patients with ulcerative colitis and Crohn’s disease. Recent evidence has suggested that the microbiome and short-chain fatty acid (SCFA) metabolites it generates may be critical for anti-α4β7 efficacy and maintaining intestinal homeostasis.Materials and Methods To determine whether the microbiome contributes to gut homeostasis after anti-α4β7 antibody administered to SIV-infected rhesus macaques, faecal SCFA concentrations were determined, 16S rRNA sequencing was performed, plasma viral loads were determined, plasma retinoids were measured longitudinally, and gut retinoid synthesis/response gene expression was quantified.Results Our results suggest that anti-α4β7 antibody facilitates the return of retinoid metabolism to baseline levels after SIV infection. Furthermore, faecal SCFAs were shown to be associated with retinoid synthesis gene expression and rebound viral loads after therapy interruption.Conclusions Taken together, these data demonstrate the therapeutic advantages of anti-α4β7 antibody administration during HIV/SIV infection and that the efficacy of anti-α4β7 antibody may depend on microbiome composition and SCFA generation.

Published

2024

16. Antiviral Activity of Lenacapavir Against Human Immunodeficiency Virus Type 2 (HIV-2) Isolates and Drug-Resistant HIV-2 Mutants.

Author

Smith, Robert A, Raugi, Dana N, Nixon, Robert S, Seydi, Moussa, Margot, Nicolas A, Callebaut, Christian, Gottlieb, Geoffrey S, and Group, for the University of Washington–Senegal HIV-2 Study

Subjects

*HIV, *VIRAL load

Abstract

The activity of lenacapavir against human immunodeficiency virus type 1 (HIV-1) has been extensively evaluated in vitro, but comparable data for human immunodeficiency virus type 2 (HIV-2) are scarce. We determined the anti–HIV-2 activity of lenacapavir using single-cycle infections of MAGIC-5A cells and multicycle infections of a T-cell line. Lenacapavir exhibited low-nanomolar activity against HIV-2, but was 11- to 14-fold less potent against HIV-2 in comparison to HIV-1. Mutations in HIV-2 that confer resistance to other antiretrovirals did not confer cross-resistance to lenacapavir. Although lenacapavir-containing regimens might be considered for appropriate patients with HIV-2, more frequent viral load and/or CD4 testing may be needed to assess clinical response. [ABSTRACT FROM AUTHOR]

Published

2024

17. RNA Landscapes of Brain and Brain-Derived Extracellular Vesicles in Simian Immunodeficiency Virus Infection and Central Nervous System Pathology.

Author

Huang, Yiyao, Abdelgawad, Ahmed, Turchinovich, Andrey, Queen, Suzanne, Abreu, Celina Monteiro, Zhu, Xianming, Batish, Mona, Zheng, Lei, and Witwer, Kenneth W

Subjects

*SIMIAN immunodeficiency virus, *EXTRACELLULAR vesicles, *VIRUS diseases, *CIRCULAR RNA, CENTRAL nervous system infections

Abstract

Background Brain tissue-derived extracellular vesicles (bdEVs) act locally in the central nervous system (CNS) and may indicate molecular mechanisms in human immunodeficiency virus (HIV) CNS pathology. Using brain homogenate (BH) and bdEVs from a simian immunodeficiency virus (SIV) model of HIV disease, we identified RNA networks in SIV infection and neuroinflammation. Methods Postmortem occipital cortex samples were obtained from uninfected controls and SIV-infected subjects (acute and chronic phases with or without CNS pathology [SIV encephalitis]). bdEVs were separated and characterized per international consensus guidelines. RNAs from bdEVs and BH were sequenced and quantitative polymerase chain reaction (qPCR)-amplified to detect levels of small RNAs (sRNAs, including microRNAs [miRNAs]) and longer RNAs including messenger RNAs (mRNAs) and circular RNAs (circRNAs). Results Dysregulated RNAs in BH and bdEVs were identified in acute and chronic infection with pathology groups, including mRNAs, miRNAs, and circRNAs. Most dysregulated mRNAs in bdEVs reflected dysregulation in source BH. These mRNAs are disproportionately involved in inflammation and immune responses. Based on target prediction, several circRNAs that were differentially abundant in source tissue might be responsible for specific differences in sRNA levels in bdEVs during SIV infection. Conclusions RNA profiling of bdEVs and source tissues reveals potential regulatory networks in SIV infection and SIV-related CNS pathology. [ABSTRACT FROM AUTHOR]

Published

2024

18. HIHISIV: a database of gene expression in HIV and SIV host immune response.

Author

Costa, Raquel L., Gadelha, Luiz, D'arc, Mirela, Ribeiro-Alves, Marcelo, Robertson, David L., Schwartz, Jean-Marc, Soares, Marcelo A., and Porto, Fábio

Abstract

In the battle of the host against lentiviral pathogenesis, the immune response is crucial. However, several questions remain unanswered about the interaction with different viruses and their influence on disease progression. The simian immunodeficiency virus (SIV) infecting nonhuman primates (NHP) is widely used as a model for the study of the human immunodeficiency virus (HIV) both because they are evolutionarily linked and because they share physiological and anatomical similarities that are largely explored to understand the disease progression. The HIHISIV database was developed to support researchers to integrate and evaluate the large number of transcriptional data associated with the presence/absence of the pathogen (SIV or HIV) and the host response (NHP and human). The datasets are composed of microarray and RNA-Seq gene expression data that were selected, curated, analyzed, enriched, and stored in a relational database. Six query templates comprise the main data analysis functions and the resulting information can be downloaded. The HIHISIV database, available at https://hihisiv.github.io, provides accurate resources for browsing and visualizing results and for more robust analyses of pre-existing data in transcriptome repositories. [ABSTRACT FROM AUTHOR]

Published

2024

19. Neutralizing antibody response to SARS‐CoV‐2 bivalent mRNA vaccine in SIV‐infected rhesus macaques: Enhanced immunity to XBB subvariants by two‐dose vaccination.

Author

Faraone, Julia N., Wang, Xiaolwei, Qu, Panke, Zheng, Yi‐Min, Vincent, Eunice, Xu, Huanbin, and Liu, Shan‐Lu

Subjects

RHESUS monkeys, SARS-CoV-2 Omicron variant, ANTIBODY formation, SARS-CoV-2, VACCINE effectiveness

Abstract

The evolution of SARS‐CoV‐2 paired with immune imprinting by prototype messenger RNA (mRNA) vaccine has challenged the current vaccination efficacy against newly emerged Omicron subvariants. In our study, we investigated a cohort of macaques infected by SIV and vaccinated with two doses of bivalent Pfizer mRNA vaccine containing wildtype and BA.5 spikes. Using a pseudotyped lentivirus neutralization assay, we determined neutralizing antibody (nAb) titers against new XBB variants, i.e., XBB.1.5, XBB.1.16, and XBB.2.3, alongside D614G and BA.4/5. We found that compared to humans vaccinated with three doses of monovalent mRNA vaccine plus a bivalent booster, the monkeys vaccinated with two doses of bivalent mRNA vaccines exhibited relatively increased titers against XBB subvariants. Of note, SIV‐positive dam macaques had reduced nAb titers relative to SIV‐negative dams. Additionally, SIV positive dams that received antiretroviral therapy had lower nAb titers than untreated dams. Our study underscores the importance of reformulating the COVID‐19 vaccine to better protect against newly emerged XBB subvariants as well as the need for further investigation of vaccine efficacy in individuals living with HIV‐1. [ABSTRACT FROM AUTHOR]

Published

2024

20. 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

21. Refinements in Clinical and Behavioral Management for Macaques on Infectious Disease Protocols

Author

Lauren Drew Martin, Jaclyn Shelton, Lisa A. Houser, Rhonda MacAllister, and Kristine Coleman

Subjects

social housing, positive reinforcement training, SIV, procedure cage, Veterinary medicine, SF600-1100

Abstract

Providing optimal clinical and behavioral care is a key component of promoting animal welfare for macaques and other nonhuman primates (NHPs) in research. This overlap between critical areas of management is particularly important for NHPs on infectious disease protocols, which often have unique challenges. For example, traditionally these NHPs were often housed alone, which can have behavioral and clinical consequences. However, in the past decade or so, considerable effort has been directed at modifying procedures in an effort to improve animal welfare for this group of NHPs. In this review, we examine some refinements that can positively impact the clinical and behavioral management of macaques on infectious disease studies, including increased social housing and the use of positive reinforcement techniques to train animals to cooperate with procedures such as daily injections or awake blood draws. We also discuss ways to facilitate the implementation of these refinements, as well as to identify logistical considerations for their implementation. Finally, we look to the future and consider what more we can do to improve the welfare of these animals.

Published

2024

22. Minimally Modified HIV-1 Infection of Macaques: Development, Utility, and Limitations of Current Models

Author

Manish Sharma, Mukta Nag, and Gregory Q. Del Prete

Subjects

HIV-1, AIDS, SIV, animal model, nonhuman primate, macaque, Microbiology, QR1-502

Abstract

Nonhuman primate (NHP) studies that utilize simian immunodeficiency virus (SIV) to model human immunodeficiency virus (HIV-1) infection have proven to be powerful, highly informative research tools. However, there are substantial differences between SIV and HIV-1. Accordingly, there are numerous research questions for which SIV-based models are not well suited, including studies of certain aspects of basic HIV-1 biology, and pre-clinical evaluations of many proposed HIV-1 treatment, prevention, and vaccination strategies. To overcome these limitations of NHP models of HIV-1 infection, several groups have pursued the derivation of a minimally modified HIV-1 (mmHIV-1) capable of establishing pathogenic infection in macaques that authentically recapitulates key features of HIV-1 in humans. These efforts have focused on three complementary objectives: (1) engineering HIV-1 to circumvent species-specific cellular restriction factors that otherwise potently inhibit HIV-1 in macaques, (2) introduction of a C chemokine receptor type 5 (CCR5)-tropic envelope, ideally that can efficiently engage macaque CD4, and (3) correction of gene expression defects inadvertently introduced during viral genome manipulations. While some progress has been made toward development of mmHIV-1 variants for use in each of the three macaque species (pigtail, cynomolgus, and rhesus), model development progress has been most promising in pigtail macaques (PTMs), which do not express an HIV-1-restricting tripartite motif-containing protein 5 α (TRIM5α). In our work, we have derived a CCR5-tropic mmHIV-1 clone designated stHIV-A19 that comprises 94% HIV-1 genome sequence and replicates to high acute-phase titers in PTMs. In animals treated with a cell-depleting CD8α antibody at the time of infection, stHIV-A19 maintains chronically elevated plasma viral loads with progressive CD4+ T-cell loss and the development of acquired immune-deficiency syndrome (AIDS)-defining clinical endpoints. However, in the absence of CD8α+ cell depletion, no mmHIV-1 model has yet displayed high levels of chronic viremia or AIDS-like pathogenesis. Here, we review mmHIV-1 development approaches, the phenotypes, features, limitations, and potential utility of currently available mmHIV-1s, and propose future directions to further advance these models.

Published

2024

23. SIV Infection Is Associated with Transient Acute-Phase Steatosis in Hepatocytes In Vivo.

Author

Derby, Nina, Biswas, Sreya, Yusova, Sofiya, Luevano-Santos, Cristina, Pacheco, Maria Cristina, Meyer, Kimberly A., Johnson, Brooke I., Fischer, Miranda, Fancher, Katherine A., Fisher, Cole, Abraham, Yohannes M., McMahon, Conor J., Lutz, Savannah S., Smedley, Jeremy V., Burwitz, Benjamin J., and Sodora, Donald L.

Subjects

*CHOLESTEROL metabolism, *FATTY liver, *LIVER cells, *FATTY degeneration, *RHESUS monkeys, *AUTOPSY

Abstract

Metabolic-dysfunction-associated fatty liver disease (MAFLD) is a major cause of morbidity and mortality in HIV-infected individuals, even those receiving optimal antiretroviral therapy. Here, we utilized the SIV rhesus macaque model and advanced laparoscopic techniques for longitudinal collection of liver tissue to elucidate the timing of pathologic changes. The livers of both SIV-infected (N = 9) and SIV-naïve uninfected (N = 8) macaques were biopsied and evaluated at four time points (weeks −4, 2, 6, and 16–20 post-infection) and at necropsy (week 32). SIV DNA within the macaques' livers varied by over 4 logs at necropsy, and liver SIV DNA significantly correlated with SIV RNA in the plasma throughout the study. Acute phase liver pathology (2 weeks post-infection) was characterized by evidence for fat accumulation (microvesicular steatosis), a transient elevation in both AST and cholesterol levels within the serum, and increased hepatic expression of the PPARA gene associated with cholesterol metabolism and beta oxidation. By contrast, the chronic phase of the SIV infection (32 weeks post-infection) was associated with sinusoidal dilatation, while steatosis resolved and concentrations of AST and cholesterol remained similar to those in uninfected macaques. These findings suggest differential liver pathologies associated with the acute and chronic phases of infection and the possibility that therapeutic interventions targeting metabolic function may benefit liver health in people newly diagnosed with HIV. [ABSTRACT FROM AUTHOR]

Published

2024

24. Current HIV/SIV Reservoir Assays for Preclinical and Clinical Applications: Recommendations from the Experts 2022 NIAID Workshop Summary.

Author

Sanders-Beer, Brigitte E., Archin, Nancie M., Brumme, Zabrina L., Busch, Michael P., Deleage, Claire, O'Doherty, Una, Hughes, Stephen H., Jerome, Keith R., Jones, R. Brad, Karn, Jonathan, Kearney, Mary F., Keele, Brandon F., Kulpa, Deanna A., Laird, Gregory M., Li, Jonathan Z., Lichterfeld, Mathias D., Nussenzweig, Michel C., Persaud, Deborah, Yukl, Steven A., and Siliciano, Robert F.

Abstract

Since the first HIV-cured person was reported in 2009, a strong interest in developing highly sensitive HIV and SIV reservoir assays has emerged. In particular, the question arose about the comparative value of state-of-the-art assays to measure and characterize the HIV reservoir, and how these assays can be applied to accurately detect changes in the reservoir during efforts to develop a cure for HIV infection. Second, it is important to consider the impact on the outcome of clinical trials if these relatively new HIV reservoir assays are incorporated into clinical trial endpoints and/or used for clinical decision-making. To understand the advantages and limitations and the regulatory implications of HIV reservoir assays, the National Institute of Allergy and Infectious Diseases (NIAID) sponsored and convened a meeting on September 16, 2022, to discuss the state of knowledge concerning these questions and best practices for selecting HIV reservoir assays for a particular research question or clinical trial protocol. [ABSTRACT FROM AUTHOR]

Published

2024

25. Toll-like Receptor 2 Mediated Immune Regulation in Simian Immunodeficiency Virus-Infected Rhesus Macaques.

Author

Boby, Nongthombam, Williams, Kelsey M., Das, Arpita, and Pahar, Bapi

Subjects

RHESUS monkeys, TOLL-like receptors, CYTOTOXIC T cells, KILLER cells, HIV infections

Abstract

Toll-like receptors (TLRs) are crucial to the innate immune response. They regulate inflammatory reactions by initiating the production of pro-inflammatory cytokines and chemokines. TLRs also play a role in shaping the adaptive immune responses. While this protective response is important for eliminating infectious pathogens, persistent activation of TLRs may result in chronic immune activation, leading to detrimental effects. The role of TLR2 in regulating HIV-1 infection in vivo has yet to be well described. In this study, we used an SIV-infected rhesus macaque model to simulate HIV infection in humans. We evaluated the plasma of the macaques longitudinally and found a significant increase in the soluble TLR2 (sTLR2) level after SIV infection. We also observed an increase in membrane-bound TLR2 (mb-TLR2) in cytotoxic T cells, B cells, and NK cells in PBMC and NK cells in the gut after infection. Our results suggest that sTLR2 regulates the production of various cytokines and chemokines, including IL-18, IL-1RA, IL-15, IL-13, IL-9, TPO, FLT3L, and IL-17F, as well as chemokines, including IP-10, MCP-1, MCP-2, ENA-78, GRO-α, I-TAC, Fractalkine, SDF-1α, and MIP-3α. Interestingly, these cytokines and chemokines were also upregulated after the infection. The positive correlation between SIV copy number and sTLR2 in the plasma indicated the involvement of TLR2 in the regulation of viral replication. These cytokines and chemokines could directly or indirectly regulate viral replication through the TLR2 signaling pathways. When we stimulated PBMC with the TLR2 agonist in vitro, we observed a direct induction of various cytokines and chemokines. Some of these cytokines and chemokines, such as IL-1RA, IL-9, IL-15, GRO-α, and ENA-78, were positively correlated with sTLR2 in vivo, highlighting the direct involvement of TLR2 in the regulation of the production of these factors. Our findings suggest that TLR2 expression may be a target for developing new therapeutic strategies to combat HIV infection. [ABSTRACT FROM AUTHOR]

Published

2023

26. Erratum to: Progress Note 2024: Curing HIV; Not in My Lifetime or Just Around the Corner?

Author

Justiin Harper, Michael Betts, Mathias Lichterfeld, Michaela Müller-Trutwin, David Margolis, Katharine Bar, Jonathan Li, Joseph McCune, Sharon Lewin, Deanna Kulpa, Santiago Ávila-Ríos, Dázon Diallo, Michael Lederman, and Mirko Paiardini

Subjects

HIV, SIV, reservoir, persistence, ART, HIV cure, Pathology, RB1-214, Immunologic diseases. Allergy, RC581-607

Abstract

Erratum to: Progress Note 2024: Curing HIV; Not in My Lifetime or Just Around the Corner? doi: 10.20411/pai.v8i2.665 In the original publication, the comments provided by Santiago Ávila-Ríos were mistakenly omitted. In this version, his comments are included in the “Comments by Leaders” section, and his name has been included in the list of authors. --- Once a death sentence, HIV is now considered a manageable chronic disease due to the development of antiretroviral therapy (ART) regimens with minimal toxicity and a high barrier for genetic resistance. While highly effective in arresting AIDS progression and rendering the virus untransmissible in people living with HIV (PLWH) with undetectable viremia (U=U) [1, 2]), ART alone is incapable of eradicating the “reservoir” of resting, latently infected CD4+ T cells from which virus recrudesces upon treatment cessation. As of 2022 estimates, there are 39 million PLWH, of whom 86% are aware of their status and 76% are receiving ART [3]. As of 2017, ART-treated PLWH exhibit near normalized life expectancies without adjustment for socioeconomic differences [4]. Furthermore, there is a global deceleration in the rate of new infections [3] driven by expanded access to pre-exposure prophylaxis (PrEP), HIV testing in vulnerable populations, and by ART treatment [5]. Therefore, despite outstanding issues pertaining to cost and access in developing countries, there is strong enthusiasm that aggressive testing, treatment, and effective viral suppression may be able to halt the ongoing HIV epidemic (ie, UNAIDS’ 95-95-95 targets) [6–8]; especially as evidenced by recent encouraging observations in Sydney [9]. Despite these promising efforts to limit further viral transmission, for PLWH, a “cure” remains elusive; whether it be to completely eradicate the viral reservoir (ie, cure) or to induce long-term viral remission in the absence of ART (ie, control; Figure 1). In a previous salon hosted by Pathogens and Immunity in 2016 [10], some researchers were optimistic that a cure was a feasible, scalable goal, albeit with no clear consensus on the best route. So, how are these cure strategies panning out? In this commentary, 8 years later, we will provide a brief overview on recent advances and failures towards identifying determinants of viral persistence and developing a scalable cure for HIV. Based on these observations, and as in the earlier salon, we have asked several prominent HIV cure researchers for their perspectives.

Published

2024

27. Progress Note 2024: Curing HIV; Not in My Lifetime or Just Around the Corner?

Author

Justin Harper, Michael Betts, Mathias Lichterfeld, Michaela Müller-Trutwin, David Margolis, Katharine Bar, Jonathan Li, Joseph McCune, Sharon Lewin, Deanna Kulpa, Dázon Diallo, Michael M. Lederman, and Mirko Paiardini

Subjects

HIV, SIV, reservoir, persistence, ART, HIV cure, Pathology, RB1-214, Immunologic diseases. Allergy, RC581-607

Abstract

Once a death sentence, HIV is now considered a manageable chronic disease due to the development of antiretroviral therapy (ART) regimens with minimal toxicity and a high barrier for genetic resistance. While highly effective in arresting AIDS progression and rendering the virus untransmissible in people living with HIV (PLWH) with undetectable viremia (U=U) [1, 2]), ART alone is incapable of eradicating the “reservoir” of resting, latently infected CD4+ T cells from which virus recrudesces upon treatment cessation. As of 2022 estimates, there are 39 million PLWH, of whom 86% are aware of their status and 76% are receiving ART [3]. As of 2017, ART-treated PLWH exhibit near normalized life expectancies without adjustment for socioeconomic differences [4]. Furthermore, there is a global deceleration in the rate of new infections [3] driven by expanded access to pre-exposure prophylaxis (PrEP), HIV testing in vulnerable populations, and by ART treatment [5]. Therefore, despite outstanding issues pertaining to cost and access in developing countries, there is strong enthusiasm that aggressive testing, treatment, and effective viral suppression may be able to halt the ongoing HIV epidemic (ie, UNAIDS’ 95-95-95 targets) [6–8]; especially as evidenced by recent encouraging observations in Sydney [9]. Despite these promising efforts to limit further viral transmission, for PLWH, a “cure” remains elusive; whether it be to completely eradicate the viral reservoir (ie, cure) or to induce long-term viral remission in the absence of ART (ie, control; Figure 1). In a previous salon hosted by Pathogens and Immunity in 2016 [10], some researchers were optimistic that a cure was a feasible, scalable goal, albeit with no clear consensus on the best route. So, how are these cure strategies panning out? In this commentary, 8 years later, we will provide a brief overview on recent advances and failures towards identifying determinants of viral persistence and developing a scalable cure for HIV. Based on these observations, and as in the earlier salon, we have asked several prominent HIV cure researchers for their perspectives.

Published

2024

28. A Summary of the Sixth International Workshop on Microbiome in HIV Pathogenesis, Prevention, and Treatment.

Author

Sherrill-Mix, Scott, Yang, Michelle, Aldrovandi, Grace M, Brenchley, Jason M, Bushman, Frederic D, Collman, Ronald G, Dandekar, Satya, Klatt, Nichole R, Lagenaur, Laurel A, Landay, Alan L, Paredes, Roger, Tachedjian, Gilda, Turpin, Jim A, Serrano-Villar, Sergio, Lozupone, Catherine A, and Ghosh, Mimi

Subjects

Humans, HIV Infections, Comorbidity, Microbiota, HIV/SIV, comorbidities, microbiome, pathogenesis, prevention, therapeutics, transmission, Genetics, HIV/AIDS, Prevention, Human Genome, Infection, Good Health and Well Being, HIV, SIV, Clinical Sciences, Virology

Abstract

In October of 2020, researchers from around the world met online for the sixth annual International Workshop on Microbiome in HIV Pathogenesis, Prevention, and Treatment. New research was presented on the roles of the microbiome on immune response and HIV transmission and pathogenesis and the potential for alterations in the microbiome to decrease transmission and affect comorbidities. This article presents a summary of the findings reported.

Published

2022

29. Schlieren image velocimetry methods for a round, hot, turbulent air-jet

Author

Emilia Georgiana PRISACARIU and Tudor PRISECARU

Subjects

bos, siv, cross-correlation, pivlab, kymography, Motor vehicles. Aeronautics. Astronautics, TL1-4050

Abstract

The present article investigates the accuracy of measurements regarding the velocity profile of a turbulent jet. The measurements are obtained by applying image processing techniques to schlieren methods. The schlieren methods described here are relatively new, having been patented and used for the first time in the last few years. Generally, SIV methods applied to turbulent flows result in unrelatable/ unrelated data, given the path-integrated nature of the flow. The global measurement errors and ways to reduce them are also discussed.

Published

2023

30. Altered Expression of ACE2 and Co-receptors of SARS-CoV-2 in the Gut Mucosa of the SIV Model of HIV/AIDS

Author

Hu, Shuang, Buser, Elise, Arredondo, Juan, Relyea, Dylan, Rocha, Clarissa Santos, and Dandekar, Satya

Subjects

Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Digestive Diseases, Vaccine Related, Infectious Diseases, HIV/AIDS, Sexually Transmitted Infections, Immunization, Emerging Infectious Diseases, Coronaviruses, Prevention, 2.1 Biological and endogenous factors, 2.2 Factors relating to the physical environment, Inflammatory and immune system, Infection, Good Health and Well Being, HIV, SIV, ACE2, SARS-CoV-2, gut mucosa, co-receptors, inflammation, metabolism, Environmental Science and Management, Soil Sciences, Microbiology, Medical microbiology

Abstract

The severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection, the cause of the COVID-19 pandemic, is initiated by its binding to the ACE2 receptor and other co-receptors on mucosal epithelial cells. Variable outcomes of the infection and disease severity can be influenced by pre-existing risk factors. Human immunodeficiency virus (HIV), the cause of AIDS, targets the gut mucosal immune system and impairs epithelial barriers and mucosal immunity. We sought to determine the impact and mechanisms of pre-existing HIV infection increasing mucosal vulnerability to SARS-CoV-2 infection and disease. We investigated changes in the expression of ACE2 and other SARS-CoV-2 receptors and related pathways in virally inflamed gut by using the SIV infected rhesus macaque model of HIV/AIDS. Immunohistochemical analysis showed sustained/enhanced ACE2 expression in the gut epithelium of SIV infected animals compared to uninfected controls. Gut mucosal transcriptomic analysis demonstrated enhanced expression of host factors that support SARS-CoV-2 entry, replication, and infection. Metabolomic analysis of gut luminal contents revealed the impact of SIV infection as demonstrated by impaired mitochondrial function and decreased immune response, which render the host more vulnerable to other pathogens. In summary, SIV infection resulted in sustained or increased ACE2 expression in an inflamed and immune-impaired gut mucosal microenvironment. Collectively, these mucosal changes increase the susceptibility to SARS-CoV-2 infection and disease severity and result in ineffective viral clearance. Our study highlights the use of the SIV model of AIDS to fill the knowledge gap of the enteric mechanisms of co-infections as risk factors for poor disease outcomes, generation of new viral variants and immune escape in COVID-19.

Published

2022

31. The Association between IL-1β and IL-18 Levels, Gut Barrier Disruption, and Monocyte Activation during Chronic Simian Immunodeficiency Virus Infection and Long-Term Suppressive Antiretroviral Therapy

Author

Siva Thirugnanam, Chenxiao Wang, Chen Zheng, Brooke F. Grasperge, Prasun K. Datta, Jay Rappaport, Xuebin Qin, and Namita Rout

Subjects

IL-18, IL-1β, IFABP, SIV, immune activation, monocyte, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

HIV-induced persistent immune activation is a key mediator of inflammatory comorbidities such as cardiovascular disease (CVD) and neurocognitive disorders. While a preponderance of data indicate that gut barrier disruption and microbial translocation are drivers of chronic immune activation, the molecular mechanisms of this persistent inflammatory state remain poorly understood. Here, utilizing the nonhuman primate model of Human Immunodeficiency Virus (HIV) infection with suppressive antiretroviral therapy (ART), we investigated activation of inflammasome pathways and their association with intestinal epithelial barrier disruption (IEBD). Longitudinal blood samples obtained from rhesus macaques with chronic SIV infection and long-term suppressive ART were evaluated for IEBD biomarkers, inflammasome activation (IL-1β and IL-18), inflammatory cytokines, and triglyceride (TG) levels. Activated monocyte subpopulations and glycolytic potential were investigated in peripheral blood mononuclear cells (PBMCs). During the chronic phase of treated SIV infection, elevated levels of plasma IL-1β and IL-18 were observed following the hallmark increase in IEBD biomarkers, intestinal fatty acid-binding protein (IFABP) and LPS-binding protein (LBP). Further, significant correlations of plasma IFABP levels with IL-1β and IL-18 were observed between 10 and 12 months of ART. Higher levels of sCD14, IL-6, and GM-CSF, among other inflammatory mediators, were also observed only during the long-term SIV + ART phase along with a trend of increase in the frequencies of activated CD14+CD16+ intermediate monocyte subpopulations. Lastly, we found elevated levels of blood TG and higher glycolytic capacity in PBMCs of chronic SIV-infected macaques with long-term ART. The increase in circulating IL-18 and IL-1β following IEBD and their significant positive correlation with IFABP suggest a connection between gut barrier disruption and inflammasome activation during chronic SIV infection, despite viral suppression with ART. Additionally, the increase in markers of monocyte activation, along with elevated TG and enhanced glycolytic pathway activity, indicates metabolic remodeling that could fuel metabolic syndrome. Further research is needed to understand the mechanisms by which gut dysfunction and inflammasome activation contribute to HIV-associated metabolic complications, enabling targeted interventions in people with HIV.

Published

2024

32. Permutation-Based Deterministic Authenticated Encryption with Minimum Memory Size

Author

Hiraga, Yukihito, Naito, Yusuke, Sasaki, Yu, Sugawara, Takeshi, Goos, Gerhard, Founding Editor, Hartmanis, Juris, Founding Editor, Bertino, Elisa, Editorial Board Member, Gao, Wen, Editorial Board Member, Steffen, Bernhard, Editorial Board Member, Yung, Moti, Editorial Board Member, Athanasopoulos, Elias, editor, and Mennink, Bart, editor

Published

2023

33. HIV/AIDS, the Pandemic that Went from Initial Despair to a Contained Threat

Author

Ferreira, Claudia, Doursout, Marie-Françoise J., Balingit, Joselito S., Ferreira, Claudia, Doursout, Marie-Françoise J., and Balingit, Joselito S.

Published

2023

34. Antibody glycosylation correlates with disease progression in SIV‐Mycobacterium tuberculosis coinfected cynomolgus macaques.

Author

Haycroft, Ebene R, Damelang, Timon, Lopez, Ester, Rodgers, Mark A, Wines, Bruce D, Hogarth, Mark, Ameel, Cassaundra L, Kent, Stephen J, Scanga, Charles A, O'Connor, Shelby L, and Chung, Amy W

Subjects

*MACAQUES, *DISEASE progression, *SIMIAN immunodeficiency virus, *GLYCOSYLATION, *TUBERCULOSIS, *TUBERCULOUS meningitis

Abstract

Objectives: Tuberculosis (TB) remains a substantial cause of morbidity and mortality among people living with human immunodeficiency virus (HIV) worldwide. However, the immunological mechanisms associated with the enhanced susceptibility among HIV‐positive individuals remain largely unknown. Methods: Here, we used a simian immunodeficiency virus (SIV)/TB‐coinfection Mauritian cynomolgus macaque (MCM) model to examine humoral responses from the plasma of SIV‐negative (n = 8) and SIV‐positive (n = 7) MCM 8‐week postinfection with Mycobacterium tuberculosis (Mtb). Results: Antibody responses to Mtb were impaired during SIV coinfection. Elevated inflammatory bulk IgG antibody glycosylation patterns were observed in coinfected macaques early at 8‐week post‐Mtb infection, including increased agalactosylation (G0) and reduced di‐galactosylation (G2), which correlated with endpoint Mtb bacterial burden and gross pathology scores, as well as the time‐to‐necropsy. Conclusion: These studies suggest that humoral immunity may contribute to control of TB disease and support growing literature that highlights antibody Fc glycosylation as a biomarker of TB disease progression. [ABSTRACT FROM AUTHOR]

Published

2023

35. In Vivo Treatment with Insulin-like Growth Factor 1 Reduces CCR5 Expression on Vaccine-Induced Activated CD4 + T-Cells.

Author

Bissa, Massimiliano, Galli, Veronica, Schifanella, Luca, Vaccari, Monica, Rahman, Mohammad Arif, Gorini, Giacomo, Binello, Nicolò, Sarkis, Sarkis, Gutowska, Anna, Silva de Castro, Isabela, Doster, Melvin N., Moles, Ramona, Ferrari, Guido, Shen, Xiaoying, Tomaras, Georgia D., Montefiori, David C., N'guessan, Kombo F., Paquin-Proulx, Dominic, Kozlowski, Pamela A., and Venzon, David J.

Subjects

SOMATOMEDIN C, CHEMOKINE receptors, T cells, VACCINE effectiveness, CD4 antigen

Abstract

At the heart of the DNA/ALVAC/gp120/alum vaccine's efficacy in the absence of neutralizing antibodies is a delicate balance of pro- and anti-inflammatory immune responses that effectively decreases the risk of SIVmac251 acquisition in macaques. Vaccine efficacy is linked to antibodies recognizing the V2 helical conformation, DC-10 tolerogenic dendritic cells eliciting the clearance of apoptotic cells via efferocytosis, and CCR5 downregulation on vaccine-induced gut homing CD4+ cells. RAS activation is also linked to vaccine efficacy, which prompted the testing of IGF-1, a potent inducer of RAS activation with vaccination. We found that IGF-1 changed the hierarchy of V1/V2 epitope recognition and decreased both ADCC specific for helical V2 and efferocytosis. Remarkably, IGF-1 also reduced the expression of CCR5 on vaccine-induced CD4+ gut-homing T-cells, compensating for its negative effect on ADCC and efferocytosis and resulting in equivalent vaccine efficacy (71% with IGF-1 and 69% without). [ABSTRACT FROM AUTHOR]

Published

2023

36. Innate adaptive immune cell dynamics in tonsillar tissues during chronic SIV infection.

Author

Shukla, Rajni Kant, Gunasena, Manuja, Reinhold-Larsson, Nicole, Duncan, Michael, Hatharasinghe, Amila, Cray, Samuel, Weragalaarachchi, Krishanthi, Kasturiratna, Dhanuja, Demberg, Thorsten, and Liyanage, Namal P. M.

Subjects

B cell lymphoma, LYMPHOID tissue, CELL transformation, EPSTEIN-Barr virus diseases, MUCOUS membranes

Abstract

HIV-infected patients are at higher risk of developing oral mucosal infection and Epstein-Barr virus (EBV)-associated B cell malignancies. However, the potential role of oral immunity in the pathogenesis of oral lesions is unknown. Tonsils are oral-pharyngeal mucosal-associated lymphoid tissues that play an important role in oral mucosal immunity. In this study, we investigated the changes of innate and adaptive immune cells in macaque tonsils during chronic SIV infection. We found significantly higher frequencies of classical monocytes, CD3+CD56+ (NKT-like) cells, CD3+CD4+CD8+ (DP), and CD161+ CD4 T cells in tonsils from chronic infected compared to naïve animals. On the contrary, intermediate monocytes and CD3+CD4-CD8-(DN) cells were lower in chronic SIV-infected macaques. We further confirmed a recently described small B-cell subset, NKB cells, were higher during chronic infection. Furthermore, both adaptive and innate cells showed significantly higher TNF-a and cytotoxic marker CD107a, while IL-22 production was significantly reduced in innate and adaptive immune cells in chronic SIV-infected animals. A dramatic reduction of IFN-g production by innate immune cells might indicate enhanced susceptibility to EBV infection and potential transformation of B cells in the tonsils. In summary, our observation shows that the SIV-associated immune responses are distinct in the tonsils compared to other mucosal tissues. Our data extends our understanding of the oral innate immune system during SIV infection and could aid future studies in evaluating the role of tonsillar immune cells during HIV-associated oral mucosal infections. [ABSTRACT FROM AUTHOR]

Published

2023

37. Enhanced IL-17 Producing and Maintained Cytolytic Effector Functions of Gut Mucosal CD161 + CD8 + T Cells in SIV-Infected Rhesus Macaques.

Author

Thirugnanam, Siva, Walker, Edith M., Schiro, Faith, Aye, Pyone P., Rappaport, Jay, and Rout, Namita

Subjects

*RHESUS monkeys, *IMMUNE response, *T helper cells, *INTERLEUKIN-17, *T cells, *CD8 antigen

Abstract

Previous studies have indicated that the loss of CD161-expressing CD4+ Th17 cells is linked to the progression of chronic HIV. These cells are significantly depleted in peripheral blood and gut mucosa of HIV-infected individuals, contributing to inflammation and disruption of the gut barrier. However, the impact of HIV infection on CD161-expressing CD8+ T cells remain unclear. Here, we examined the functions of peripheral blood and mucosal CD161+CD8+ T cells in the macaque model of HIV infection. In contrast to the significant loss of CD161+CD4+ T cells, CD161+CD8+ T cell frequencies were maintained in blood and gut during chronic SIV infection. Furthermore, gut CD161+CD8+ T cells displayed greater IL-17 production and maintained Th1-type and cytolytic functions, contrary to impaired IL-17 and granzyme-B production in CD161+CD4+ T cells of SIV-infected macaques. These results suggest that augmented Th17-type effector functions of CD161+CD8+ T cells during SIV infection is a likely mechanism to compensate for the sustained loss of gut mucosal Th17 cells. Targeting the cytokine and cytolytic effector functions of CD161+CD8+ T cells in the preclinical setting of chronic SIV infection with antiretroviral therapy has implications in the restoration of gut barrier disruption in persons with HIV infection. [ABSTRACT FROM AUTHOR]

Published

2023

38. The role of CD4 T cells in the rhesus central nervous system during homeostasis and viral-induced neuroinflammation

Author

Elizaldi, Sonny Ramirez

Subjects

Immunology, Brain, Central Nervous System, HIV, Neuroinflammation, SIV, T cells

Abstract

Despite the advent and implementation of Anti-retroviral therapy (ART) in 1987, people living with HIV (PLWH) continue to experience a high incidence of age-associated comorbidities, particularly HIV associated neurocognitive disorders (HAND) which affect 40-70% of PLWH. Research over the past four decades has predominantly focused on the role of myeloid cells in the development of HAND due, in part, to the initial discovery of HIV-infected myeloid cells in the post-mortem brain tissue of AIDS patients. My dissertation examines the understudied role of T lymphocytes in HAND, in light of three significant advancements in the fields of HIV and neuroimmunology. Firstly, ART treatment has not only stabilized disease progression but has also led to the reconstitution and stabilization of CD4 T cells, highlighting a newfound potential role for CD4 T cells in the neurological disease process. Secondly, we now recognize that T cells are an important immune population within the central nervous system (CNS) both during homeostasis and disease. Thirdly, data from neurodegenerative diseases such as Alzheimer’s, Parkinson’s, and Multiple Sclerosis highlight a critical role for T cells in contributing to neuroinflammation and disease progression.Together, these advancements collectively provide a strong rationale for developing a more comprehensive understanding of the role of T cells in HAND. Given the early establishment of transmitted/founder (T/F) HIV in the CNS, the surveillance of the CNS by CCR5 (R5) + T helper 1 cells, which serve as primary HIV targets, and the influence of T-cell derived cytokines on microglial activation, we hypothesized that T cells are pivotal in acute CNS viral seeding and neuroinflammation. We tested this hypothesis in rhesus macaques (Macaca mulatta) - among the most robust models for studying the CNS and HIV pathogenesis. We employed models of both acute and chronic simian HIV (SHIV) infection using distinct strains: the R5/CD4 tropic T/F SHIV C.CH505, the virulent R5-T cell-tropic SIVmac251, and the macrophage-tropic SIVCL757, used in studies of neuro-HIV. Together, our studies with these distinct viruses offer the following insights into the role of CD4 T cells in the brain during HIV infection.In Chapter II, we presented RNA sequencing and viral load data across four synapse-dense regions of the brain susceptible to HIV infection (Prefrontal Cortex (PFC), Superior Temporal Sulcus, Caudate Nucleus, Hippocampus). First, our data demonstrated that these synapse-dense cognitive regions are rich in immune gene signatures at homeostasis. Following infection with T/F SHIV.C.CH505, our analysis showed activation of biological pathways consistent with T cell recruitment and microglial activation. Despite relatively low plasma and cerebrospinal fluid (CSF) viral loads, we observed viral (v)RNA and vDNA within these regions - an observation aligning with infiltration of SIV infected Th1 CD4 T cells into the PFC. In Chapter III, we delved deeply into the phenotype of CD4 T cells within the CNS, including the brain and its associated border tissues. Our rationale for this comprehensive analysis was to delineate target cells in these regions to better understand susceptibility to viral establishment. We conducted single-cell analysis of CD45+ immune cells in brain parenchyma, comparing them to counterparts in the spleen of both uninfected macaques and those acutely infected with SIVmac251. The data demonstrated colocalization of viral transcripts within CD4 clusters and furthermore showed induction of antiviral responses during acute SIV infection. This supports the observations made in Chapter II that target cells for HIV populate the CNS, including the dura, choroid plexus stroma, and the skull bone marrow. Correspondingly, during the acute phase of SIVmac251 infection, we observed significant levels of viral RNA and DNA in these regions. In animals chronically infected with SIVmac251 (40 weeks) and treated with suboptimal ART, our data demonstrated that despite CSF viral suppression, there is incomplete reconstitution of CD4 T cells in the brain and surrounding CNS tissues underscoring their active engagement during acute and chronic phases of SIVmac251 infection. In Chapter IV, we comprehensively assessed phenotypic and functional features of CCR7+ cells identified in Chapter III. Leveraging single-transcriptomic analysis, ATAC-seq, spatial transcriptomics and flow cytometry we show that CCR7+ CD4 T cells in the brain have T lymphocyte central memory-like features. Moreover, the skull bone marrow emerged as a potential niche for CCR7+ CD4 T cells. In a cohort of macaques chronically infected (112 weeks) with SIVCL757 and treated with suboptimal ART, we noted a decrease in CCR7+ CD4 T cells within the brain in parallel with evidence for microglial activation and induction of neurodegenerative pathways. These findings suggested that changes in CD4 T cell subsets within the CNS may drive neuroinflammation during chronic HIV infection. In summary, the findings across my three chapters lead to three major conclusions. First, the presence of both CCR5 and CCR7 CD4 T cells in the parenchymal and border regions of the CNS, renders this organ susceptible to initial HIV infection and establishment of latent reservoirs. Second, our studies of acute infection with two viruses - SHIVC.CH505 and SIVmac251- suggests that CD4 T cells within the brain parenchyma are actively engaged during acute HIV infection serving as both viral targets and mediators of neuroinflammation. Third, our models of chronic infection under suboptimal ART with two viruses - SIVmac251 and SIVCL757 - demonstrate that inadequate CD4 T cell reconstitution together with reduction of CCR7+ CD4 T cells may underlie neuroimmune dysregulation in HIV-infected patients on ART.

Published

2024

39. 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

40. Cannabinoids modulate the microbiota–gut–brain axis in HIV/SIV infection by reducing neuroinflammation and dysbiosis while concurrently elevating endocannabinoid and indole-3-propionate levels

Author

Marina McDew-White, Eunhee Lee, Lakmini S. Premadasa, Xavier Alvarez, Chioma M. Okeoma, and Mahesh Mohan

Subjects

THC, SIV, Rhesus macaque, Neuroinflammation, Type-I interferon, Microbiota–gut–brain axis, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Background Although the advent of combination anti-retroviral therapy (cART) has transformed HIV into a manageable chronic disease, an estimated 30–50% of people living with HIV (PLWH) exhibit cognitive and motor deficits collectively known as HIV-associated neurocognitive disorders (HAND). A key driver of HAND neuropathology is chronic neuroinflammation, where proinflammatory mediators produced by activated microglia and macrophages are thought to inflict neuronal injury and loss. Moreover, the dysregulation of the microbiota–gut–brain axis (MGBA) in PLWH, consequent to gastrointestinal dysfunction and dysbiosis, can lead to neuroinflammation and persistent cognitive impairment, which underscores the need for new interventions. Methods We performed RNA-seq and microRNA profiling in basal ganglia (BG), metabolomics (plasma) and shotgun metagenomic sequencing (colon contents) in uninfected and SIV-infected rhesus macaques (RMs) administered vehicle (VEH/SIV) or delta-9-tetrahydrocannabinol (THC) (THC/SIV). Results Long-term, low-dose THC reduced neuroinflammation and dysbiosis and significantly increased plasma endocannabinoid, endocannabinoid-like, glycerophospholipid and indole-3-propionate levels in chronically SIV-infected RMs. Chronic THC potently blocked the upregulation of genes associated with type-I interferon responses (NLRC5, CCL2, CXCL10, IRF1, IRF7, STAT2, BST2), excitotoxicity (SLC7A11), and enhanced protein expression of WFS1 (endoplasmic reticulum stress) and CRYM (oxidative stress) in BG. Additionally, THC successfully countered miR-142-3p-mediated suppression of WFS1 protein expression via a cannabinoid receptor-1-mediated mechanism in HCN2 neuronal cells. Most importantly, THC significantly increased the relative abundance of Firmicutes and Clostridia including indole-3-propionate (C. botulinum, C. paraputrificum, and C. cadaveris) and butyrate (C. butyricum, Faecalibacterium prausnitzii and Butyricicoccus pullicaecorum) producers in colonic contents. Conclusion This study demonstrates the potential of long-term, low-dose THC to positively modulate the MGBA by reducing neuroinflammation, enhancing endocannabinoid levels and promoting the growth of gut bacterial species that produce neuroprotective metabolites, like indole-3-propionate. The findings from this study may benefit not only PLWH on cART, but also those with no access to cART and more importantly, those who fail to suppress the virus under cART.

Published

2023

41. Novel engineered chimeric engulfment receptors trigger T cell effector functions against SIV-infected CD4+ T cells

Author

Daniel Corey, Francoise Haeseleer, Joe Hou, and Lawrence Corey

Subjects

SIV, HIV, chimeric engulfment receptor (CER), TIM-4, phosphatidylserine, Genetics, QH426-470, Cytology, QH573-671

Abstract

Adoptive therapy with genetically engineered T cells offers potential for infectious disease treatment in immunocompromised persons. HIV/simian immunodeficiency virus (SIV)-infected cells express phosphatidylserine (PS) early post infection. We tested whether chimeric engulfment receptor (CER) T cells designed to recognize PS-expressing cells could eliminate SIV-infected cells. Lentiviral CER constructs composed of the extracellular domain of T cell immunoglobulin and mucin domain containing 4 (TIM-4), the PS receptor, and engulfment signaling domains were transduced into primary rhesus macaque (RM) T cells. We measured PS binding and T cell engulfment of RM CD4+ T cells infected with SIV expressing GFP and in vitro, TIM-4 CER CD4+ T cells effectively killed SIV-infected cells, which was dependent on TIM-4 binding to PS. Enhanced killing of SIV-infected CD4+ T cells by CER and chimeric antigen receptor T cell combinations was also observed. This installation of innate immune functions into T cells presents an opportunity to enhance elimination of SIV-infected cells, and studies to evaluate their effect in vivo are warranted.

Published

2023

42. Shifts in microbial diversity, composition, and functionality in the gut and genital microbiome during a natural SIV infection in vervet monkeys

Author

Jasinska, Anna J, Dong, Tien S, Lagishetty, Venu, Katzka, William, Jacobs, Jonathan P, Schmitt, Christopher A, Cramer, Jennifer Danzy, Ma, Dongzhu, Coetzer, Willem G, Grobler, J Paul, Turner, Trudy R, Freimer, Nelson, Pandrea, Ivona, and Apetrei, Cristian

Subjects

Microbiology, Biological Sciences, Genetics, HIV/AIDS, Infectious Diseases, Prevention, 2.1 Biological and endogenous factors, Aetiology, 2.2 Factors relating to the physical environment, Infection, Good Health and Well Being, Animals, Bacteria, Chlorocebus aethiops, Feces, Female, Gastrointestinal Microbiome, Male, Microbiota, Monkey Diseases, Rectum, Simian Acquired Immunodeficiency Syndrome, Simian Immunodeficiency Virus, Vagina, SIV, Microbiome, Proteobacteria, Succinivibrio, Acute infection, Primate, Simian immunodeficiency virus, Ecology, Medical Microbiology, Evolutionary biology

Abstract

BackgroundThe microbiota plays an important role in HIV pathogenesis in humans. Microbiota can impact health through several pathways such as increasing inflammation in the gut, metabolites of bacterial origin, and microbial translocation from the gut to the periphery which contributes to systemic chronic inflammation and immune activation and the development of AIDS. Unlike HIV-infected humans, SIV-infected vervet monkeys do not experience gut dysfunction, microbial translocation, and chronic immune activation and do not progress to immunodeficiency. Here, we provide the first reported characterization of the microbial ecosystems of the gut and genital tract in a natural nonprogressing host of SIV, wild vervet monkeys from South Africa.ResultsWe characterized fecal, rectal, vaginal, and penile microbiomes in vervets from populations heavily infected with SIV from diverse locations across South Africa. Geographic site, age, and sex affected the vervet microbiome across different body sites. Fecal and vaginal microbiome showed marked stratification with three enterotypes in fecal samples and two vagitypes, which were predicted functionally distinct within each body site. External bioclimatic factors, biome type, and environmental temperature influenced microbiomes locally associated with vaginal and rectal mucosa. Several fecal microbial taxa were linked to plasma levels of immune molecules, for example, MIG was positively correlated with Lactobacillus and Escherichia/Shigella and Helicobacter, and IL-10 was negatively associated with Erysipelotrichaceae, Anaerostipes, Prevotella, and Anaerovibrio, and positively correlated with Bacteroidetes and Succinivibrio. During the chronic phase of infection, we observed a significant increase in gut microbial diversity, alterations in community composition (including a decrease in Proteobacteria/Succinivibrio in the gut) and functionality (including a decrease in genes involved in bacterial invasion of epithelial cells in the gut), and partial reversibility of acute infection-related shifts in microbial abundance observed in the fecal microbiome. As part of our study, we also developed an accurate predictor of SIV infection using fecal samples.ConclusionsThe vervets infected with SIV and humans infected with HIV differ in microbial responses to infection. These responses to SIV infection may aid in preventing microbial translocation and subsequent disease progression in vervets, and may represent host microbiome adaptations to the virus. Video Abstract.

Published

2020

43. Editorial: Preclinical macaque models of viral diseases

Author

Jeremy Smedley

Subjects

macaque, model, HIV, SIV, transplantation, Zika (ZIKV), Immunologic diseases. Allergy, RC581-607

Published

2023

44. Lipid metabolic reprogramming of hepatic CD4+ T cells during SIV infection

Author

Julien A. Clain, Steven Boutrais, Juliette Dewatines, Gina Racine, Henintsoa Rabezanahary, Arnaud Droit, Ouafa Zghidi-Abouzid, and Jérôme Estaquier

Subjects

AIDS, SIV, liver, CD4, metabolism, lipid, Microbiology, QR1-502

Abstract

ABSTRACT While liver inflammation is associated with AIDS, little is known so far about hepatic CD4+ T cells. By using the simian immunodeficiency virus (SIV)-infected rhesus macaque (RM) model, we aimed to characterize CD4+ T cells. The phenotype of CD4+ T cells was assessed by flow cytometry from uninfected (n = 3) and infected RMs, with either SIVmac251 (n = 6) or SHIVSF162p3 (n = 6). After cell sorting of hepatic CD4+ T cells, viral DNA quantification and RNA sequencing were performed.Thus, we demonstrated that liver CD4+ T cells strongly expressed the SIV coreceptor, CCR5. We showed that viremia was negatively correlated with the percentage of hepatic effector memory CD4+ T cells. Consistent with viral sensing, inflammatory and interferon gene transcripts were increased. We also highlighted the presence of harmful CD4+ T cells expressing GZMA and members of TGFB that could contribute to fuel inflammation and fibrosis. Whereas RNA sequencing demonstrated activated CD4+ T cells displaying higher levels of mitoribosome and membrane lipid synthesis transcripts, few genes were related to glycolysis and oxidative phosphorylation, which are essential to sustain activated T cells. Furthermore, we observed lower levels of mitochondrial DNA and higher levels of genes associated with damaged organelles (reticulophagy and mitophagy). Altogether, our data revealed that activated hepatic CD4+ T cells are reprogrammed to lipid metabolism. Thus, strategies aiming to reprogram T cell metabolism with effector function could be of interest for controlling viral infection and preventing liver disorders. IMPORTANCE Human immunodeficiency virus (HIV) infection may cause liver diseases, associated with inflammation and tissue injury, contributing to comorbidity in people living with HIV. Paradoxically, the contribution of hepatic CD4+ T cells remains largely underestimated. Herein, we used the model of simian immunodeficiency virus (SIV)-infected rhesus macaques to access liver tissue. Our work demonstrates that hepatic CD4+ T cells express CCR5, the main viral coreceptor, and are infected. Viral infection is associated with the presence of inflamed and activated hepatic CD4+ T cells expressing cytotoxic molecules. Furthermore, hepatic CD4+ T cells are reprogrammed toward lipid metabolism after SIV infection. Altogether, our findings shed new light on hepatic CD4+ T cell profile that could contribute to liver injury following viral infection.

Published

2023

45. Opioid abuse and SIV infection in non-human primates.

Author

Deshetty, Uma Maheswari, Ray, Sudipta, Singh, Seema, Buch, Shilpa, and Periyasamy, Palsamy

Subjects

*OPIOID abuse, *SIMIAN immunodeficiency virus, *HIV, *HIV infections, *PRIMATES

Abstract

Human immunodeficiency virus (HIV) and drug abuse are intertwined epidemics, leading to compromised adherence to combined antiretroviral therapy (cART) and exacerbation of NeuroHIV. As opioid abuse causes increased viral replication and load, leading to a further compromised immune system in people living with HIV (PLWH), it is paramount to address this comorbidity to reduce the NeuroHIV pathogenesis. Non-human primates are well-suited models to study mechanisms involved in HIV neuropathogenesis and provide a better understanding of the underlying mechanisms involved in the comorbidity of HIV and drug abuse, leading to the development of more effective treatments for PLWH. Additionally, using broader behavioral tests in these models can mimic mild NeuroHIV and aid in studying other neurocognitive diseases without encephalitis. The simian immunodeficiency virus (SIV)–infected rhesus macaque model is instrumental in studying the effects of opioid abuse on PLWH due to its similarity to HIV infection. The review highlights the importance of using non-human primate models to study the comorbidity of opioid abuse and HIV infection. It also emphasizes the need to consider modifiable risk factors such as gut homeostasis and pulmonary pathogenesis associated with SIV infection and opioid abuse in this model. Moreover, the review suggests that these non-human primate models can also be used in developing effective treatment strategies for NeuroHIV and opioid addiction. Therefore, non-human primate models can significantly contribute to understanding the complex interplay between HIV infection, opioid abuse, and associated comorbidities. [ABSTRACT FROM AUTHOR]

Published

2023

46. Antiretroviral Therapy Ameliorates Simian Immunodeficiency Virus–Associated Myocardial Inflammation by Dampening Interferon Signaling and Pathogen Response in the Heart.

Author

Robinson, Jake A, Niu, Meng, Fox, Howard S, and Burdo, Tricia H

Subjects

*ANTIRETROVIRAL agents, *INTERFERONS, *SIMIAN immunodeficiency virus, *HIV, *RHESUS monkeys

Abstract

People with human immunodeficiency virus have an increased risk of developing cardiovascular disease. RNA-Seq was performed on hearts from simian immunodeficiency virus (SIV)–infected rhesus macaques with or without antiretroviral therapy (ART). SIV infection led to high plasma viral load with very little myocardial viral RNA. SIV infection promoted an inflammatory environment in the heart through interferon and pathogen signaling, in the absence of myocardial viral RNA. While ART dampened interferon and cytokine response in the heart, SIV-infected animals receiving ART had deficits in the expression of genes directly involved in fatty acid metabolism relative to SIV-uninfected animals. [ABSTRACT FROM AUTHOR]

Published

2023

47. Downregulation of CCR5 on brain perivascular macrophages in simian immunodeficiency virus‐infected rhesus macaques.

Author

Hattler, Julian B., Irons, Derek L., Luo, Jiangtao, and Kim, Woong‐Ki

Subjects

*ENDOCYTOSIS, *CHEMOKINE receptors, *RHESUS monkeys, *GAG proteins, *SIMIAN immunodeficiency virus, *HIV

Abstract

Background: C‐C chemokine receptor 5 (CCR5) is a major coreceptor for Human immunodeficiency virus (HIV) and simian immunodeficiency virus (SIV) cell entry; however, its role in brain pathogenesis is largely understudied. Thus, we sought to examine cell type‐specific protein expression of CCR5 during SIV infection of the brain. Methods: We examined occipital cortical tissue from uninfected rhesus macaques and SIV‐infected animals with or without encephalitis using immunohistochemistry and immunofluorescence microscopy to determine the number and distribution of CCR5‐positive cells. Results: An increase in the number of CCR5+ cells in the brain of SIV‐infected animals with encephalitis was accounted for by increased CD3+CD8+ cells expressing CCR5, but not by increased CCR5+ microglia or perivascular macrophages (PVMs), and a concurrent decrease in the percentage of CCR5+ PVMs was observed. Levels of CCR5 and SIV Gag p28 protein expression were examined on a per‐cell basis, and a significant, negative relationship was established indicating decreased CCR5 expression in productively infected cells. While investigating the endocytosis‐mediated CCR5 internalization as a mechanism for CCR5 downregulation, we found that phospho‐ERK1/2, an indicator of clathrin‐mediated endocytosis, was colocalized with infected PVMs and that macrophages from infected animals showed significantly increased expression of clathrin heavy chain 1. Conclusions: These findings show a shift in CCR5‐positive cell types in the brain during SIV pathogenesis with an increase in the number of CCR5+ CD8 T cells, and downregulated CCR5 expression on infected PVMs, likely through ERK1/2‐driven, clathrin‐mediated endocytosis. [ABSTRACT FROM AUTHOR]

Published

2023

48. Osteopontin Is an Integral Mediator of Cardiac Interstitial Fibrosis in Models of Human Immunodeficiency Virus Infection.

Author

Robinson, Jake A, Mahmud, Farina J, Greif, Elizabeth, Toribio, Mabel, Zanni, Markella V, Brown, Amanda M, and Burdo, Tricia H

Subjects

*HIV infections, *HEART fibrosis, *GROWTH differentiation factors, *OSTEOPONTIN, *SIMIAN immunodeficiency virus

Abstract

Background People with human immunodeficiency virus (HIV) have heightened incidence/risk of diastolic dysfunction and heart failure. Women with HIV have elevated cardiac fibrosis, and plasma osteopontin (Opn) is correlated to cardiac pathology. Therefore, this study provides mechanistic insight into the relationship between osteopontin and cardiac fibrosis during HIV infection. Methods Mouse embryonic fibroblasts (MEFs) modeled cardiac fibroblasts in vitro. Simian immunodeficiency virus (SIV)-infected macaques with or without antiretroviral therapy and HIV-infected humanized mice modeled HIV-associated cardiac fibrosis. Results Lipopolysaccharide-stimulated MEFs were myofibroblast-like, secreted cytokines, and produced Opn transcripts. SIV-infected animals had elevated plasma Opn at necropsy, full-length Opn in the ventricle, and ventricular interstitial fibrosis. Regression modeling identified growth differentiation factor 15, CD14+CD16+ monocytes, and CD163 expression on CD14+CD16+ monocytes as independent predictors of plasma Opn during SIV infection. HIV-infected humanized mice showed increased interstitial fibrosis compared to uninfected/untreated animals, and systemic inhibition of osteopontin by RNA aptamer reduced left ventricle fibrosis in HIV-infected humanized mice. Conclusions Since Opn is elevated in the plasma and left ventricle during SIV infection and systemic inhibition of Opn reduced cardiac fibrosis in HIV-infected mice, Opn may be a potential target for adjunctive therapies to reduce cardiac fibrosis in people with HIV. [ABSTRACT FROM AUTHOR]

Published

2023

49. Schlieren image velocimetry methods for a round, hot, turbulent air-jet.

Author

PRISACARIU, Emilia Georgiana and PRISECARU, Tudor

Subjects

*VELOCIMETRY, *MEASUREMENT errors, *TURBULENT flow, *TURBULENCE, *IMAGE processing, *TURBULENT jets (Fluid dynamics)

Abstract

The present article investigates the accuracy of measurements regarding the velocity profile of a turbulent jet. The measurements are obtained by applying image processing techniques to schlieren methods. The schlieren methods described here are relatively new, having been patented and used for the first time in the last few years. Generally, SIV methods applied to turbulent flows result in unrelatable/unrelated data, given the path-integrated nature of the flow. The global measurement errors and ways to reduce them are also discussed. [ABSTRACT FROM AUTHOR]

Published

2023

50. 2-Hydroxypropyl-b-Cyclodextrin Treatment Induces Modest Immune Activation in Healthy Rhesus Macaques.

Author

Ortiz, Alexandra M., Casta, Fabiola Castello, Rahmberg, Andrew, Markowitz, Tovah E., Brooks, Kelsie, Simpson, Jennifer, and Brenchley, Jason M.

Subjects

*MACAQUES, *RHESUS monkeys, *MONONUCLEAR leukocytes, *MYELOID cells, *SIMIAN immunodeficiency virus

Abstract

Experimental simian immunodeficiency virus (SIV) infection of Asian macaques is an excellent model for HIV disease progression and therapeutic development. Recent coformulations of nucleoside analogs and an integrase inhibitor have been used for parenteral antiretroviral (ARV) administration in SIV-infected macaques, successfully resulting in undetectable plasma SIV RNA. In a cohort of SIVmac239-infected macaques, we recently observed that administration of coformulated ARVs resulted in an unexpected increase in plasma levels of soluble CD14 (sCD14), associated with stimulation of myeloid cells. We hypothesized that the coformulation solubilizing agent Kleptose (2-hydroxypropyl-β-cyclodextrin [HP βCD]) may induce inflammation with myeloid cell activation and the release of sCD14. Herein, we stimulated peripheral blood mononuclear cells (PBMCs) from healthy macaques with HP βCD from different commercial sources and evaluated inflammatory cytokine production in vitro. Treatment of PBMCs resulted in increased sCD14 release and myeloid cell interleukin-1β (IL-1β) production--with stimulation varying significantly by HP βCD source--and destabilized lymphocyte CCR5 surface expression. We further treated healthy macaques with Kleptose alone. In vivo, we observed modestly increased myeloid cell activation in response to Kleptose treatment without significant perturbation of the immunological transcriptome or epigenome. Our results demonstrate a need for vehicle-only controls and highlight immunological perturbations that can occur when using HP βCD in pharmaceutical coformulations. [ABSTRACT FROM AUTHOR]

Published

2023