Your search keyword '"Aarthi Talla"' showing total 34 results

1. Persistent serum protein signatures define an inflammatory subcategory of long COVID

Author

Aarthi Talla, Suhas V. Vasaikar, Gregory Lee Szeto, Maria P. Lemos, Julie L. Czartoski, Hugh MacMillan, Zoe Moodie, Kristen W. Cohen, Lamar B. Fleming, Zachary Thomson, Lauren Okada, Lynne A. Becker, Ernest M. Coffey, Stephen C. De Rosa, Evan W. Newell, Peter J. Skene, Xiaojun Li, Thomas F. Bumol, M. Juliana McElrath, and Troy R. Torgerson

Subjects

Science

Abstract

Abstract Long COVID or post-acute sequelae of SARS-CoV-2 (PASC) is a clinical syndrome featuring diverse symptoms that can persist for months following acute SARS-CoV-2 infection. The aetiologies may include persistent inflammation, unresolved tissue damage or delayed clearance of viral protein or RNA, but the biological differences they represent are not fully understood. Here we evaluate the serum proteome in samples, longitudinally collected from 55 PASC individuals with symptoms lasting ≥60 days after onset of acute infection, in comparison to samples from symptomatically recovered SARS-CoV-2 infected and uninfected individuals. Our analysis indicates heterogeneity in PASC and identified subsets with distinct signatures of persistent inflammation. Type II interferon signaling and canonical NF-κB signaling (particularly associated with TNF), appear to be the most differentially enriched signaling pathways, distinguishing a group of patients characterized also by a persistent neutrophil activation signature. These findings help to clarify biological diversity within PASC, identify participants with molecular evidence of persistent inflammation, and highlight dominant pathways that may have diagnostic or therapeutic relevance, including a protein panel that we propose as having diagnostic utility for differentiating inflammatory and non-inflammatory PASC.

Published

2023

2. A comprehensive platform for analyzing longitudinal multi-omics data

Author

Suhas V. Vasaikar, Adam K. Savage, Qiuyu Gong, Elliott Swanson, Aarthi Talla, Cara Lord, Alexander T. Heubeck, Julian Reading, Lucas T. Graybuck, Paul Meijer, Troy R. Torgerson, Peter J. Skene, Thomas F. Bumol, and Xiao-jun Li

Subjects

Science

Abstract

The analysis of longitudinal bulk and single-cell multi-omics data is a highly complex task. Here, the authors introduce PALMO, a software platform with five modules to analyse longitudinal bulk and single-cell multi-omics data, which is extensively tested in external datasets that include multiple omics modalities.

Published

2023

3. Selective loss of CD107a TIGIT+ memory HIV-1-specific CD8+ T cells in PLWH over a decade of ART

Author

Oscar Blanch-Lombarte, Dan Ouchi, Esther Jimenez-Moyano, Julieta Carabelli, Miguel Angel Marin, Ruth Peña, Adam Pelletier, Aarthi Talla, Ashish Sharma, Judith Dalmau, José Ramón Santos, Rafick-Pierre Sékaly, Bonaventura Clotet, and Julia G Prado

Subjects

inhibitory receptors, HIV-1-specific CD8+ T cells, TIGIT, CD107a, single-cell CD8+ dynamics, people living with HIV-1, Medicine, Science, Biology (General), QH301-705.5

Abstract

The co-expression of inhibitory receptors (IRs) is a hallmark of CD8+ T-cell exhaustion (Tex) in people living with HIV-1 (PLWH). Understanding alterations of IRs expression in PLWH on long-term antiretroviral treatment (ART) remains elusive but is critical to overcoming CD8+ Tex and designing novel HIV-1 cure immunotherapies. To address this, we combine high-dimensional supervised and unsupervised analysis of IRs concomitant with functional markers across the CD8+ T-cell landscape on 24 PLWH over a decade on ART. We define irreversible alterations of IRs co-expression patterns in CD8+ T cells not mitigated by ART and identify negative associations between the frequency of TIGIT+ and TIGIT+ TIM-3+ and CD4+ T-cell levels. Moreover, changes in total, SEB-activated, and HIV-1-specific CD8+ T cells delineate a complex reshaping of memory and effector-like cellular clusters on ART. Indeed, we identify a selective reduction of HIV-1 specific-CD8+ T-cell memory-like clusters sharing TIGIT expression and low CD107a that can be recovered by mAb TIGIT blockade independently of IFNγ and IL-2. Collectively, these data characterize with unprecedented detail the patterns of IRs expression and functions across the CD8+ T-cell landscape and indicate the potential of TIGIT as a target for Tex precision immunotherapies in PLWH at all ART stages.

Published

2023

4. Germinal Center T follicular helper (GC-Tfh) cell impairment in chronic HIV infection involves c-Maf signaling.

Author

Marita Chakhtoura, Mike Fang, Rafael Cubas, Margaret H O'Connor, Carmen N Nichols, Brian Richardson, Aarthi Talla, Susan Moir, Mark J Cameron, Virginie Tardif, and Elias K Haddad

Subjects

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

Abstract

We have recently demonstrated that the function of T follicular helper (Tfh) cells from lymph nodes (LN) of HIV-infected individuals is impaired. We found that these cells were unable to provide proper help to germinal center (GC)-B cells, as observed by altered and inefficient anti-HIV antibody response and premature death of memory B cells. The underlying molecular mechanisms of this dysfunction remain poorly defined. Herein, we have used a unique transcriptional approach to identify these molecular defects. We consequently determined the transcriptional profiles of LN GC-Tfh cells following their interactions with LN GC-B cells from HIV-infected and HIV-uninfected individuals, rather than analyzing resting ex-vivo GC-Tfh cells. We observed that proliferating GC-Tfh cells from HIV-infected subjects were transcriptionally different than their HIV-uninfected counterparts, and displayed a significant downregulation of immune- and GC-Tfh-associated pathways and genes. Our results strongly demonstrated that MAF (coding for the transcription factor c-Maf) and its upstream signaling pathway mediators (IL6R and STAT3) were significantly downregulated in HIV-infected subjects, which could contribute to the impaired GC-Tfh and GC-B cell functions reported during infection. We further showed that c-Maf function was associated with the adenosine pathway and that the signaling upstream c-Maf could be partially restored by adenosine deaminase -1 (ADA-1) supplementation. Overall, we identified a novel mechanism that contributes to GC-Tfh cell impairment during HIV infection. Understanding how GC-Tfh cell function is altered in HIV is crucial and could provide critical information about the mechanisms leading to the development and maintenance of effective anti-HIV antibodies.

Published

2021

5. Integrated systems approach defines the antiviral pathways conferring protection by the RV144 HIV vaccine

Author

Slim Fourati, Susan Pereira Ribeiro, Filipa Blasco Tavares Pereira Lopes, Aarthi Talla, Francois Lefebvre, Mark Cameron, J. Kaewkungwal, P. Pitisuttithum, S. Nitayaphan, S. Rerks-Ngarm, Jerome H. Kim, Rasmi Thomas, Peter B. Gilbert, Georgia D. Tomaras, Richard A. Koup, Nelson L. Michael, M. Juliana McElrath, Raphael Gottardo, and Rafick-Pierre Sékaly

Subjects

Science

Abstract

The RV144 vaccine trial showed reduced risk of HIV-1 acquisition, but mechanisms underlying protection are poorly understood. Here, Fourati et al. assess the transcriptomic profile of blood collected from 223 vaccinees and 40 placebo recipients and identify IRF7 as a mediator of protection.

Published

2019

6. Automated Manufacture of Autologous CD19 CAR-T Cells for Treatment of Non-hodgkin Lymphoma

Author

Zachary Jackson, Anne Roe, Ashish Arunkumar Sharma, Filipa Blasco Tavares Pereira Lopes, Aarthi Talla, Sarah Kleinsorge-Block, Kayla Zamborsky, Jennifer Schiavone, Shivaprasad Manjappa, Robert Schauner, Grace Lee, Ruifu Liu, Paolo F. Caimi, Ying Xiong, Winfried Krueger, Andrew Worden, Mike Kadan, Dina Schneider, Rimas Orentas, Boro Dropulic, Rafick-Pierre Sekaly, Marcos de Lima, David N. Wald, and Jane S. Reese

Subjects

automated, CAR-T, manufacturing, Prodigy, stem cell memory T, Immunologic diseases. Allergy, RC581-607

Abstract

Chimeric antigen receptor T cells (CAR-T cell) targeting CD19 are effective against several subtypes of CD19-expressing hematologic malignancies. Centralized manufacturing has allowed rapid expansion of this cellular therapy, but it may be associated with treatment delays due to the required logistics. We hypothesized that point of care manufacturing of CAR-T cells on the automated CliniMACS Prodigy® device allows reproducible and fast delivery of cells for the treatment of patients with non-Hodgkin lymphoma. Here we describe cell manufacturing results and characterize the phenotype and effector function of CAR-T cells used in a phase I/II study. We utilized a lentiviral vector delivering a second-generation CD19 CAR construct with 4-1BB costimulatory domain and TNFRSF19 transmembrane domain. Our data highlight the successful generation of CAR-T cells at numbers sufficient for all patients treated, a shortened duration of production from 12 to 8 days followed by fresh infusion into patients, and the detection of CAR-T cells in patient circulation up to 1-year post-infusion.

Published

2020

7. A crowdsourced analysis to identify ab initio molecular signatures predictive of susceptibility to viral infection

Author

Slim Fourati, Aarthi Talla, Mehrad Mahmoudian, Joshua G. Burkhart, Riku Klén, Ricardo Henao, Thomas Yu, Zafer Aydın, Ka Yee Yeung, Mehmet Eren Ahsen, Reem Almugbel, Samad Jahandideh, Xiao Liang, Torbjörn E. M. Nordling, Motoki Shiga, Ana Stanescu, Robert Vogel, The Respiratory Viral DREAM Challenge Consortium, Gaurav Pandey, Christopher Chiu, Micah T. McClain, Christopher W. Woods, Geoffrey S. Ginsburg, Laura L. Elo, Ephraim L. Tsalik, Lara M. Mangravite, and Solveig K. Sieberts

Subjects

Science

Abstract

The response to respiratory virus exposure can currently not be predicted by pre- or early post-exposure molecular signatures. Here, the authors conduct a community-based analysis of blood gene expression from healthy individuals exposed to respiratory viruses and provide predictive models and biological insight into the physiological response.

Published

2018

8. Pre-vaccination inflammation and B-cell signalling predict age-related hyporesponse to hepatitis B vaccination

Author

Slim Fourati, Razvan Cristescu, Andrey Loboda, Aarthi Talla, Ali Filali, Radha Railkar, Andrea K. Schaeffer, David Favre, Dominic Gagnon, Yoav Peretz, I-Ming Wang, Chan R. Beals, Danilo R. Casimiro, Leonidas N. Carayannopoulos, and Rafick-Pierre Sékaly

Subjects

Science

Abstract

Ageing is associated with poor responses to vaccines but the underlying mechanism remains unclear. Here the authors use a systems-based approach to define molecular signatures present before vaccination that correlate with non-responsiveness to hepatitis B vaccination in healthy, elderly adults.

Published

2016

9. Novel mechanisms to inhibit HIV reservoir seeding using Jak inhibitors.

Author

Christina Gavegnano, Jessica H Brehm, Franck P Dupuy, Aarthi Talla, Susan Pereira Ribeiro, Deanna A Kulpa, Cheryl Cameron, Stephanie Santos, Selwyn J Hurwitz, Vincent C Marconi, Jean-Pierre Routy, Laurent Sabbagh, Raymond F Schinazi, and Rafick Pierre Sékaly

Subjects

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

Abstract

Despite advances in the treatment of HIV infection with ART, elucidating strategies to overcome HIV persistence, including blockade of viral reservoir establishment, maintenance, and expansion, remains a challenge. T cell homeostasis is a major driver of HIV persistence. Cytokines involved in regulating homeostasis of memory T cells, the major hub of the HIV reservoir, trigger the Jak-STAT pathway. We evaluated the ability of tofacitinib and ruxolitinib, two FDA-approved Jak inhibitors, to block seeding and maintenance of the HIV reservoir in vitro. We provide direct demonstration for involvement of the Jak-STAT pathway in HIV persistence in vivo, ex vivo, and in vitro; pSTAT5 strongly correlates with increased levels of integrated viral DNA in vivo, and in vitro Jak inhibitors reduce the frequency of CD4+ T cells harboring integrated HIV DNA. We show that Jak inhibitors block viral production from infected cells, inhibit γ-C receptor cytokine (IL-15)-induced viral reactivation from latent stores thereby preventing transmission of infectious particles to bystander activated T cells. These results show that dysregulation of the Jak-STAT pathway is associated with viral persistence in vivo, and that Jak inhibitors target key events downstream of γ-C cytokine (IL-2, IL-7 and IL-15) ligation to their receptors, impacting the magnitude of the HIV reservoir in all memory CD4 T cell subsets in vitro and ex vivo. Jak inhibitors represent a therapeutic modality to prevent key events of T cell activation that regulate HIV persistence and together, specific, potent blockade of these events may be integrated to future curative strategies.

Published

2017

10. PALMO: a comprehensive platform for analyzing longitudinal multi-omics data

Author

Suhas V. Vasaikar, Adam K. Savage, Qiuyu Gong, Elliott Swanson, Aarthi Talla, Cara Lord, Alexander T Heubeck, Julian Reading, Lucas T. Graybuck, Paul Meijer, Troy R. Torgerson, Peter J. Skene, Thomas F. Bumol, and Xiao-jun Li

Abstract

Longitudinal bulk and single-cell omics data is increasingly generated for biological and clinical research but is challenging to analyze due to its many intrinsic types of variations. We present PALMO (https://github.com/aifimmunology/PALMO), a platform that contains five analytical modules to examine longitudinal bulk and single-cell multi-omics data from multiple perspectives, including decomposition of sources of variations within the data, collection of stable or variable features across timepoints and participants, identification of up- or down-regulated markers across timepoints of individual participants, and investigation on samples of same participants for possible outlier events. We tested PALMO performance on a complex longitudinal multi-omics dataset of five data modalities on the same samples and six external datasets of diverse background. Both PALMO and our longitudinal multi-omics dataset can be valuable resources to the scientific community.

Published

2022

11. Single-cell CD8+ dynamics in PLWH uncover the depletion of TIGIT+ memory HIV-1-specific cells during long-term ART

Author

Oscar Blanch-Lombarte, Dan Ouchi, Esther Jiménez-Moyano, Julieta Carabelli, Miguel Angel Marin, Ruth Peña, Adam Pelletier, Aarthi Talla, Ashish Sharma, Judith Dalmau, José Ramón Santos, Rafik-Pierre Sékaly, Bonaventura Clotet, and Julia G. Prado

Abstract

The expression of inhibitory receptors (IRs) is a hallmark of CD8+ T-cell exhaustion (Tex) in people living with HIV-1 (PLWH). Understanding the dynamics of IRs expression in PLWH on long-term antiretroviral treatment (ART) is critical to overcoming CD8+ Tex and designing broadly applicable HIV-1 immunotherapies for cure. To address this, we combine high-dimensional immunophenotype and unsupervised single-cell analysis of IRs and functional markers in CD8+ T-cells among 24 PLWH over a decade of ART. We found irreversible alterations of IRs co-expression patterns in CD8+ T cells and identified negative associations between the frequency of TIGIT+ and TIGIT+TIM-3+ and immune status. Moreover, the single-cell dynamics of total, polyclonal, and HIV-1-specific CD8+ T-cells delineate a complex reshaping of memory-like and effector-like cellular clusters during long-term ART. Indeed, HIV-1 specific-CD8+ T-cells dynamics uncover the selective reduction of memory-like cellular clusters sharing TIGIT expression and low CD107a. Ex vivo single TIGIT but not combinatorial TIGIT+TIM3 antibody blockade restored CD107a expression in HIV-1-specific CD8+ T cells, particularly within the memory compartment. Collectively, these results profile single-cell dynamics of IRs expression across the CD8+ T-cell landscape and propose TIGIT as a target for precision immunotherapies in PLWH on long-term ART.

Published

2022

12. Persistent serum protein signatures define an inflammatory subset of long COVID

Author

Aarthi Talla, Suhas V. Vasaikar, Gregory Lee Szeto, Maria P. Lemos, Julie L. Czartoski, Hugh MacMillan, Zoe Moodie, Kristen W. Cohen, Lamar B. Fleming, Zachary Thomson, Lauren Okada, Lynne A. Becker, Ernest M. Coffey, Stephen C. De Rosa, Evan W. Newell, Peter J. Skene, Xiaojun Li, Thomas F. Bumol, M. Juliana McElrath, and Troy R. Torgerson

Abstract

Long COVID or post-acute sequelae of SARS-CoV-2 (PASC) is a clinical syndrome featuring diverse symptoms that can persist for months after acute SARS-CoV-2 infection. The etiologies are unknown but may include persistent inflammation, unresolved tissue damage, or delayed clearance of viral protein or RNA. Attempts to classify subsets of PASC by symptoms alone have been unsuccessful. To molecularly define PASC, we evaluated the serum proteome in longitudinal samples from 55 PASC individuals with symptoms lasting ≥60 days after onset of acute infection and compared this to symptomatically recovered SARS-CoV-2 infected and uninfected individuals. We identified subsets of PASC with distinct signatures of persistent inflammation. Type II interferon signaling and canonical NF-κB signaling (particularly associated with TNF), were the most differentially enriched pathways. These findings help to resolve the heterogeneity of PASC, identify patients with molecular evidence of persistent inflammation, and highlight dominant pathways that may have diagnostic or therapeutic relevance.One Sentence SummarySerum proteome profiling identifies subsets of long COVID patients with evidence of persistent inflammation including key immune signaling pathways that may be amenable to therapeutic intervention.

Published

2022

13. TGF-β Signaling, Senescence and Impaired Metabolism in Central Memory CD4 T Cells Promotes HIV Persistence

Author

Khader Ghneim, Ashish Arunkumar Sharma, Susan Pereira Ribeiro, Slim Fourati, Jeffery Ahlers, Ali Filali-Mouhim, Deanna Kulpa, Xuan Xu, Jessica Brehm, Aarthi Talla, Benigno Rodriguez, Carey Shive, Razvan Cristescu, Andrey Loboda, Robert Balderas, I-ming Wang, Peter Hunt, Daniel Lamarre, Daniel Douek, Daria Hazuda, Michael Lederman, Steven G. Deeks, and Rafick-Pierre Sekaly

Subjects

History, Polymers and Plastics, Business and International Management, Industrial and Manufacturing Engineering

Published

2022

14. TGF-β associated senescence and impaired metabolism in central memory CD4 T cells promotes HIV persistence

Author

Susan Pereira Ribeiro, Daniel Lamarre, Peter W. Hunt, Carey L. Shive, Andrey Loboda, Aarthi Talla, Jeffery Ahlers, Xuan Xu, Benigno Rodriguez, Deanna A. Kulpa, Razvan Cristescu, Khader Ghneim, Slim Fourati, Robert S. Balderas, Steven G. Deeks, Rafick Pierre Sekaly, I-Ming Wang, Ashish Sharma, Michael M. Lederman, Daria J. Hazuda, Jessica H. Brehm, and Daniel C. Douek

Subjects

Senescence, Immunology, Human immunodeficiency virus (HIV), medicine, Metabolism, Biology, medicine.disease_cause, Persistence (computer science), Transforming growth factor

Abstract

Current therapeutic interventions to eradicate latent HIV (“reservoir”) and restore immune function in ART-treated HIV infection have yet to show efficacy. To explore mechanisms of HIV persistence, we apply an integrated systems biology approach and identify a distinct group of individuals with poor CD4 T-cell reconstitution (Immunologic non-responders, “INRs”) and high frequencies of cells with inducible HIV. Contrary to the prevailing notion that immune activation drives HIV persistence and immune dysfunction, peripheral blood leukocytes from these subjects have enhanced expression of a network of genes regulated by cellular senescence. In these subjects, increased frequencies of regulatory T cells and expression of the TGF-β signaling cascade are concomitant with the downregulation of cell cycle and metabolism in CD4 central memory T (TCM) cells. These cascades, downstream of TGF-β, lead to the accumulation of PD-1 expressing CD4 TCM and are associated with an increase in frequencies of cells with inducible HIV ex vivo. In vitro validation confirmed that this cellular profile was driven by a β-hydroxybutyrates/bile acid rich metabolic milieu and resulted in TGF-β associated latency establishment. Our findings identify targets for PD-1 or TGF-β specific interventions that can overcome cellular senescence; these therapeutic approaches have shown safety and efficacy in cancer, and may prove to be crucial for HIV eradication.

Published

2021

15. Oral immune dysfunction is associated with the expansion of FOXP3+PD-1+Amphiregulin+ T cells during HIV infection

Author

Natarajan Bhaskaran, R. Asaad, Fady F. Faddoul, Elizabeth Schneider, Pushpa Pandiyan, Aarthi Talla, Alan D. Levine, A. Paes da Silva, Michael M. Lederman, Donald M. McDonald, N. Greenspan, and Jonathan Karn

Subjects

Multidisciplinary, business.industry, Science, T cell, General Physics and Astronomy, FOXP3, Inflammasome, General Chemistry, Systemic inflammation, General Biochemistry, Genetics and Molecular Biology, TLR2, Immune system, medicine.anatomical_structure, Amphiregulin, medicine, Cancer research, medicine.symptom, business, Protein kinase B, medicine.drug

Abstract

Residual systemic inflammation and mucosal immune dysfunction persist in people living with HIV, despite treatment with combined anti-retroviral therapy, but the underlying immune mechanisms are poorly understood. Here we report that the altered immune landscape of the oral mucosa of HIV-positive patients on therapy involves increased TLR and inflammasome signaling, localized CD4+ T cell hyperactivation, and, counterintuitively, enrichment of FOXP3+ T cells. HIV infection of oral tonsil cultures in vitro causes an increase in FOXP3+ T cells expressing PD-1, IFN-γ, Amphiregulin and IL-10. These cells persist even in the presence of anti-retroviral drugs, and further expand when stimulated by TLR2 ligands and IL-1β. Mechanistically, IL-1β upregulates PD-1 expression via AKT signaling, and PD-1 stabilizes FOXP3 and Amphiregulin through a mechanism involving asparaginyl endopeptidase, resulting in FOXP3+ cells that are incapable of suppressing CD4+ T cells in vitro. The FOXP3+ T cells that are abundant in HIV-positive patients are phenotypically similar to the in vitro cultured, HIV-responsive FOXP3+ T cells, and their presence strongly correlates with CD4+ T cell hyper-activation. This suggests that FOXP3+ T cell dysregulation might play a role in the mucosal immune dysfunction of HIV patients on therapy.

Published

2021

16. Germinal Center T follicular helper (GC-Tfh) cell impairment in chronic HIV infection involves c-Maf signaling

Author

Susan Moir, Rafael Cubas, Aarthi Talla, Margaret H. O’Connor, Carmen N. Nichols, Elias K. Haddad, Virginie Tardif, Brian Richardson, Mark J. Cameron, Mike Fang, Marita Chakhtoura, HAL-SU, Gestionnaire, Drexel University, Case Western Reserve University [Cleveland], Institute of Immunobiology [St. Gallen], Brustzentrum Kantonsspital St. Gallen, National Institute of Allergy and Infectious Diseases [Bethesda] (NIAID-NIH), National Institutes of Health [Bethesda] (NIH), Centre de recherche en Myologie – U974 SU-INSERM, Institut National de la Santé et de la Recherche Médicale (INSERM)-Sorbonne Université (SU), Departement Hospitalo- Universitaire - Inflammation, Immunopathologie, Biothérapie [Paris] (DHU - I2B), Institut National de la Santé et de la Recherche Médicale (INSERM)-CHU Pitié-Salpêtrière [AP-HP], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU)-Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU)-CHU Trousseau [APHP], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU)-Centre National de la Recherche Scientifique (CNRS)-CHU Saint-Antoine [AP-HP], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU), Centre de Recherche en Myologie, CHU Trousseau [APHP], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU)-Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU)-CHU Saint-Antoine [AP-HP], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU)-Centre National de la Recherche Scientifique (CNRS)-Institut National de la Santé et de la Recherche Médicale (INSERM)-CHU Pitié-Salpêtrière [AP-HP], Sorbonne Université (SU)-Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP), Sorbonne Université (SU)-CHU Pitié-Salpêtrière [AP-HP], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU)-Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)-CHU Saint-Antoine [AP-HP], and Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU)-CHU Trousseau [APHP]

Subjects

RNA viruses, Male, 0301 basic medicine, Cell signaling, Physiology, Cellular differentiation, Cell, Signal transduction, Pathology and Laboratory Medicine, Biochemistry, White Blood Cells, 0302 clinical medicine, Immunodeficiency Viruses, Animal Cells, [SDV.MHEP.MI]Life Sciences [q-bio]/Human health and pathology/Infectious diseases, Immune Physiology, Medicine and Health Sciences, Cell differentiation, Biology (General), Innate Immune System, T Cells, 3. Good health, Cell biology, STAT signaling, medicine.anatomical_structure, [SDV.IMM.IA]Life Sciences [q-bio]/Immunology/Adaptive immunology, Medical Microbiology, Viral Pathogens, Proto-Oncogene Proteins c-maf, [SDV.IMM.IA] Life Sciences [q-bio]/Immunology/Adaptive immunology, Viruses, [SDV.MHEP.MI] Life Sciences [q-bio]/Human health and pathology/Infectious diseases, Infectious diseases, Cytokines, Female, Pathogens, Cellular Types, Antibody, Research Article, HIV infections, Medical conditions, Adult, T Follicular Helper Cells, QH301-705.5, Immune Cells, Immunology, Viral diseases, Biology, Microbiology, 03 medical and health sciences, Immune system, Downregulation and upregulation, Virology, Retroviruses, DNA-binding proteins, Genetics, medicine, Humans, Microbial Pathogens, Molecular Biology, Transcription factor, Blood Cells, Lentivirus, Organisms, Biology and Life Sciences, Proteins, HIV, Germinal center, Molecular Development, RC581-607, Germinal Center, Regulatory Proteins, Gene regulation, Cell cycle and cell division, 030104 developmental biology, Immune System, Chronic Disease, biology.protein, Parasitology, Gene expression, Immunologic diseases. Allergy, Developmental Biology, Transcription Factors, 030215 immunology

Abstract

We have recently demonstrated that the function of T follicular helper (Tfh) cells from lymph nodes (LN) of HIV-infected individuals is impaired. We found that these cells were unable to provide proper help to germinal center (GC)-B cells, as observed by altered and inefficient anti-HIV antibody response and premature death of memory B cells. The underlying molecular mechanisms of this dysfunction remain poorly defined. Herein, we have used a unique transcriptional approach to identify these molecular defects. We consequently determined the transcriptional profiles of LN GC-Tfh cells following their interactions with LN GC-B cells from HIV-infected and HIV-uninfected individuals, rather than analyzing resting ex-vivo GC-Tfh cells. We observed that proliferating GC-Tfh cells from HIV-infected subjects were transcriptionally different than their HIV-uninfected counterparts, and displayed a significant downregulation of immune- and GC-Tfh-associated pathways and genes. Our results strongly demonstrated that MAF (coding for the transcription factor c-Maf) and its upstream signaling pathway mediators (IL6R and STAT3) were significantly downregulated in HIV-infected subjects, which could contribute to the impaired GC-Tfh and GC-B cell functions reported during infection. We further showed that c-Maf function was associated with the adenosine pathway and that the signaling upstream c-Maf could be partially restored by adenosine deaminase -1 (ADA-1) supplementation. Overall, we identified a novel mechanism that contributes to GC-Tfh cell impairment during HIV infection. Understanding how GC-Tfh cell function is altered in HIV is crucial and could provide critical information about the mechanisms leading to the development and maintenance of effective anti-HIV antibodies., Author summary Human immunodeficiency virus (HIV) remains a worldwide burden despite available treatments. The virus induces dysregulations in major immune cells and organs including lymph nodes. Germinal center T follicular helper (GC-Tfh) cells are immune cells which induce specific anti-HIV antibodies by helping GC-B cells. In chronic HIV, the interaction between these two cell types is defective, leading to modified and inefficient anti-HIV antibody responses. In this study, we examined the underlying mechanisms of this dysfunction. We observed that proliferating GC-Tfh cells from HIV-infected individuals, displayed distinctive gene expression than those from -uninfected subjects, following GC-B cell interaction. Furthermore, GC-Tfh cells from HIV patients showed a reduction in important immune-related pathway and gene expression. A number of essential GC-Tfh cell genes, such as MAF and its associated genes (IL6R and STAT3), were particularly attenuated in HIV, contributing to the impaired cells function. Moreover, we found an association between MAF function and the key enzyme adenosine deaminase-1 (ADA-1), where supplementation with ADA-1 partially restored the dysfunctional signaling in GC-Tfh cells during chronic infection. Understanding how GC-Tfh cells are altered in HIV is critical to elucidate the mechanisms leading to effective anti-HIV antibodies.

Published

2021

17. Decreased Enteric Bacterial Composition and Diversity in South American Crohn’s Disease Vary With the Choice of Treatment Strategy and Time Since Diagnosis

Author

Rafick-Pierre Sekaly, Leticia D’argenio Garcia, Alan D. Levine, Aarthi Talla, Angélica Cruz-Lebrón, Miguel E. Quiñones-Mateu, Karina I. Carvalho, and Samira Joussef-Piña

Subjects

Male, Population, Lipopolysaccharide Receptors, Gut flora, Systemic inflammation, Severity of Illness Index, Inflammatory bowel disease, Feces, Crohn Disease, RNA, Ribosomal, 16S, Prevalence, medicine, Humans, Microbiome, Intestinal Mucosa, education, Glucocorticoids, Crohn's disease, education.field_of_study, biology, business.industry, Gastroenterology, Original Articles, General Medicine, medicine.disease, biology.organism_classification, Faecal calprotectin, Gastrointestinal Microbiome, Immunology, Dysbiosis, Tumor Necrosis Factor Inhibitors, medicine.symptom, business, Leukocyte L1 Antigen Complex, Brazil

Abstract

Background and Aims The symptomology of Crohn’s disease [CD], a chronic inflammatory disease of the digestive tract, correlates poorly with clinical, endoscopic or immunological assessments of disease severity. The prevalence of CD in South America is rising, reflecting changes in socio-economic stability. Many treatment options are available to CD patients, including biological agents and corticosteroids, each of which offers variable efficacy attributed to host genetics and environmental factors associated with alterations in the gut microbiota. Methods Based on 16S rRNA gene sequencing and taxonomic differences, we compared the faecal microbial population of Brazilian patients with CD treated with corticosteroid or anti-tumour necrosis factor [anti-TNF] immunotherapy. Faecal calprotectin and plasma sCD14 levels were quantified as markers for local and systemic inflammation, respectively. Results Anti-TNF treatment led to an increased relative abundance of Proteobacteria and a decreased level of Bacteroidetes. In contrast, corticoid treatment was associated with an increase in the relative abundance of Actinobacteria, which has been linked to inflammation in CD. Disruption of the faecal microbiota was related to decreased bacterial diversity and composition. Moreover, the choice of clinical regimen and time since diagnosis modulate the character of the resulting dysbiosis. Conclusions Enteric microbial populations in CD patients who have been treated are modulated by disease pathogenesis, local inflammatory microenvironment and treatment strategy. The dysbiosis that remains after anti-TNF treatment due to decreased bacterial diversity and composition abates restoration of the microbiota to a healthy state, suggesting that the identification and development of new clinical treatments for CD must include their capacity to normalize the gut microbiota.

Published

2019

18. Longitudinal immune dynamics of mild COVID-19 define signatures of recovery and persistence

Author

Kathy Henderson, Troy R. Torgerson, Palak C Genge, Gregory L. Szeto, Aarthi Talla, Nina Kondza, Lynne A Becker, Charles M Roll, Zachary Thomson, Ernest M. Coffey, Mehul S. Suthar, Suhas Vasaikar, Xiao-jun Li, Julie Czartoski, Thomas F. Bumol, Julian Reading, Mark-Phillip Lee Pebworth, Lilin Lai, Evan W. Newell, Hugh MacMillan, Stephen C. De Rosa, Zoe Moodie, Paul Meijer, Maria P. Lemos, Lucas T. Graybuck, M. Juliana McElrath, Peter J Skene, Kristen W. Cohen, Olivia Fong, Morgan Da Weiss, and Alexander T. Heubeck

Subjects

Coronavirus disease 2019 (COVID-19), business.industry, Convalescence, media_common.quotation_subject, Cell, Article, Proinflammatory cytokine, Persistence (computer science), Chromatin, medicine.anatomical_structure, Immune system, Immunology, Gene expression, medicine, business, media_common

Abstract

SARS-CoV-2 has infected over 160 million and caused more than 3 million deaths to date. Most individuals (>80%) have mild symptoms and recover in the outpatient setting, but detailed studies of immune responses have focused primarily on moderate to severe COVID-19. We deeply profiled the longitudinal immune response in individuals with mild COVID beginning with early time points post-infection (1-15 days) and proceeding through convalescence to >100 days after symptom onset. We correlated data from single cell analyses of peripheral blood cells, serum proteomics, virus-specific cellular and humoral immune responses, and clinical metadata. Acute infection was characterized by vigorous coordinated innate and adaptive activation, including an early cellular and proteomic signature that correlated with the amplitude of virus-specific humoral responses after day 30. We characterized signals associated with recovery and convalescence to define a new signature of inflammatory cytokines, gene expression, and chromatin accessibility that persists in individuals with post-acute sequelae of SARS-CoV-2 infection (PASC).

Published

2021

19. PD-1 dependent expansion of Amphregulin+FOXP3+ cells is associated with oral immune dysfunction in HIV patients on therapy

Author

Jonathan Karn, R. Asaad, Aarthi Talla, Natarajan Bhaskaran, Paes da Silva A, Elizabeth Schneider, Fady F. Faddoul, Donald M. McDonald, Pushpa Pandiyan, Alan D. Levine, Michael M. Lederman, and N. Greenspan

Subjects

education.field_of_study, business.industry, T cell, Population, FOXP3, Inflammasome, Systemic inflammation, Immune system, medicine.anatomical_structure, Amphiregulin, Cancer research, Medicine, IL-2 receptor, medicine.symptom, business, education, medicine.drug

Abstract

Residual systemic inflammation and mucosal immune dysfunction persist in people living with HIV (PLWH) despite treatment with combined anti-retroviral therapy (cART), but the underlying immune mechanisms are poorly understood. Here we report an altered immune landscape involving upregulation of TLR- and inflammasome signaling, localized CD4+ T cell hyperactivation, and counterintuitively, an enrichment of CD4+CD25+FOXP3+ regulatory T cells (Tregs) in the oral mucosa of HIV+ patients on therapy. Using human oral tonsil cultures, we found that HIV infection causes an increase in a unique population of FOXP3+ cells expressing PD-1, IFN-γ, Amphiregulin (AREG), and IL-10. These cells persisted even in the presence of the anti-retroviral drug and underwent further expansion driven by TLR-2 ligands and IL-1β. IL-1β also promoted PD-1 upregulation in AKT1 dependent manner. PD-1 stabilized FOXP3 and AREG expression in these cells through a mechanism requiring the activation of Asparaginyl Endopeptidase (AEP). Importantly, these FOXP3+ cells were incapable of suppressing CD4+ T cells in vitro. Concurrently, HIV+ patients harbored higher levels of PD-1, IFN-γ, Amphiregulin (AREG), and IL-10 expressing FOXP3+ cells, which strongly correlated with CD4+ T cell hyperactivation, suggesting an absence of CD4+ T cell regulation in the oral mucosa. Taken together, this study provides insights into a novel mechanism of FOXP3+ cell dysregulation and reveals a critical link in the positive feedback loop of oral mucosal immune activation events in HIV+ patients on therapy.One Sentence SummaryHIV-induced immune dysfunction in lymphoid and mucosal tissues

Published

2021

20. Microbiome And Metabolome Driven Differentiation Of TGF-β Producing Tregs Leads to Senescence and HIV Latency

Author

Steven G. Deeks, Razvan Cristescu, Peter W. Hunt, Khader Ghneim, I-Ming Wang, Robert S. Balderas, Susan Pereira Ribeiro, Samuel Darko, Sahaana Arumugam, Ali Filali-Mouhim, Rafick-Pierre Sekaly, Daniel Lamarre, Aarthi Talla, Michael M. Lederman, Ashish Sharma, Xuan Xu, Benigno Rodriguez, Daniel C. Douek, Daria J. Hazuda, Jessica H. Brehm, Deanna A. Kulpa, Jeffery Ahlers, Carey L. Shive, Andrey Loboda, and Slim Fourati

Subjects

Senescence, Cellular differentiation, Immunology, FOXO3, Metabolome, Microbiome, Butyrate, Biology, IRF3, Transforming growth factor

Abstract

Therapeutic interventions to eradicate latent HIV in ART-treated infection have yet to show efficacy. We used a systems biology approach to identify a subset of ART-treated individuals with immune-dysfunction that had the highest frequencies of cells with inducible HIV. Contrary to the prevailing notion that immune activation drives HIV persistence, blood from these individuals was enriched in senescence-inducing genes (high FOXO3, SMAD2 and IRF3), Treg frequencies and TGF-β signaling expression. In these "Senescent-INRs", high Firmicute phylum plasma nucleotides and butyrate/bile acids (like a-ketobutyrate) correlated with Treg frequencies and inducible HIV levels. Stimulation of naive CD4 T-cells with a-ketobutyrate led to TGF-β producing Treg differentiation, and PD-1 up-regulation on less differentiated cells. A dose dependent increase in latent HIV-infected memory CD4 T-cells was observed after TGF-β stimulation. Senescence cascades identified here can be targeted by PD-1/TGF-β specific interventions that have shown safety/efficacy in cancer, and can be crucial for HIV eradication.

Published

2021

21. Microbiome and Metabolome driven differentiation of TGF-β producing Tregs leads to Senescence and HIV latency

Author

Steven G. Deeks, Ashish Sharma, Jeffrey D. Ahlers, Xuan Xu, I-Ming Wang, Susan Pereira Ribeiro, Robert S. Balderas, Daria J. Hazuda, Sahaana Arumugam, Jessica H. Brehm, Slim Fourati, Daniel Lamarre, Peter W. Hunt, Rafick-Pierre Sekaly, Benigno Rodriguez, Carey L. Shive, Deanna A. Kulpa, Andrey Loboda, Samuel Darko, Aarthi Talla, Michael M. Lederman, Razvan Cristescu, Daniel C. Douek, and Khader Ghneim

Subjects

Senescence, Immune system, Downregulation and upregulation, Immunology, Microbiome, Biology, Cell cycle, IRF3, Transcription factor, Ex vivo

Abstract

SummaryCurrent therapeutic interventions to eradicate latent HIV (“reservoir”) and restore immune function in ART-treated HIV infection have yet to show efficacy. To explore mechanisms of HIV persistence, we apply an integrated systems biology approach and identify a distinct group of individuals with poor CD4 T-cell reconstitution (Immunologic non-responders, “INRs”) and high frequencies of cells with inducible HIV. Contrary to the prevailing notion that immune activation drives HIV persistence and immune dysfunction, peripheral blood leukocytes from these subjects have enhanced expression of a network of genes regulated by cellular senescence driving transcription factors (TFs) FOXO3, SMAD2 and IRF3. In these subjects, increased frequencies of regulatory T cells and expression of the TGF-β signaling cascade are complimented by the downregulation of cell cycle, metabolic and pro-inflammatory pathways. Lactobacillaceae family and metabolites (members of the butyrate family – i.e. α-ketobutyrate) were correlated with Treg frequencies in “Senescent-INRs”ex vivo,triggered the differentiation of TGF-β producing Tregs and promoted HIV latency establishmentin vitro.These cascades, downstream of PD-1/TGF-β, prevent memory T cell differentiation and are associated with an increase in frequencies of cells with inducible HIVex vivo.Our findings identify cellular senescence responses that can be targeted by PD-1 or TGF-β specific interventions that have shown safety and efficacy in cancer, and may prove to be crucial for HIV eradication.

Published

2020

22. Cycling CD4+ T cells in HIV-infected immune nonresponders have mitochondrial dysfunction

Author

Michael L. Freeman, Carey L Shive, Soumya Panigrahi, Souheil-Antoine Younes, Konstantin V. Shmagel, Scott F. Sieg, Benigno Rodriguez, Aarthi Talla, Susan Pereira Ribeiro, Larisa B. Korolevskaya, Donald D. Anthony, Leonard H. Calabrese, Robert Balderas, Evgeniya V. Saidakova, Mark J. Cameron, Daniel C. Douek, Michael M. Lederman, Pushpa Pandiyan, Sophia Alison Zweig, and Leonid Margolis

Subjects

Adult, Male, 0301 basic medicine, T cell, HIV Infections, Mitochondrion, Biology, T-Lymphocytes, Regulatory, Flow cytometry, Mitochondrial Proteins, 03 medical and health sciences, 0302 clinical medicine, Immune system, medicine, Humans, Interleukin-15, medicine.diagnostic_test, General Medicine, Middle Aged, Cell cycle, TFAM, Acquired immune system, Peroxisome Proliferator-Activated Receptor Gamma Coactivator 1-alpha, CD4 Lymphocyte Count, Mitochondria, DNA-Binding Proteins, 030104 developmental biology, medicine.anatomical_structure, Anti-Retroviral Agents, Mitochondrial biogenesis, 030220 oncology & carcinogenesis, Immunology, HIV-1, Female, Research Article, Transcription Factors

Abstract

Immune nonresponder (INR) HIV-1-infected subjects are characterized by their inability to reconstitute the CD4+ T cell pool after antiretroviral therapy. This is linked to poor clinical outcome. Mechanisms underlying immune reconstitution failure are poorly understood, although, counterintuitively, INRs often have increased frequencies of circulating CD4+ T cells in the cell cycle. While cycling CD4+ T cells from healthy controls and HIV+ patients with restored CD4+ T cell numbers complete cell division in vitro, cycling CD4+ T cells from INRs do not. Here, we show that cells with the phenotype and transcriptional profile of Tregs were enriched among cycling cells in health and in HIV infection. Yet there were diminished frequencies and numbers of Tregs among cycling CD4+ T cells in INRs, and cycling CD4+ T cells from INR subjects displayed transcriptional profiles associated with the impaired development and maintenance of functional Tregs. Flow cytometric assessment of TGF-β activity confirmed the dysfunction of Tregs in INR subjects. Transcriptional profiling and flow cytometry revealed diminished mitochondrial fitness in Tregs among INRs, and cycling Tregs from INRs had low expression of the mitochondrial biogenesis regulators peroxisome proliferator-activated receptor γ coactivator 1-α (PGC1α) and transcription factor A for mitochondria (TFAM). In vitro exposure to IL-15 allowed cells to complete division, restored the expression of PGC1α and TFAM, and regenerated mitochondrial fitness in the cycling Tregs of INRs. Our data suggest that rescuing mitochondrial function could correct the immune dysfunction characteristic of Tregs in HIV-1-infected subjects who fail to restore CD4+ T cells during antiretroviral therapy.

Published

2018

23. A crowdsourced analysis to identify ab initio molecular signatures predictive of susceptibility to viral infection

Author

Samad Jahandideh, Christopher Chiu, Slim Fourati, Motoki Shiga, Mehmet Eren Ahsen, Riku Klén, Laura L. Elo, Torbjörn E. M. Nordling, Solveig K. Sieberts, Joshua Burkhart, Xiao Liang, Ricardo Henao, Zafer Aydin, Gaurav Pandey, Reem Almugbel, Robert Vogel, Micah T. McClain, Ephraim L. Tsalik, Ana Stanescu, Christopher W. Woods, Thomas Yu, Geoffrey S. Ginsburg, Lara M. Mangravite, Ka Yee Yeung, Mehrad Mahmoudian, Aarthi Talla, Medical Research Council (MRC), AGÜ, Mühendislik Fakültesi, Bilgisayar Mühendisliği Bölümü, Department of Pathology [Cleveland, OH, USA] (School of Medicine), Case Western Reserve University [Cleveland], Turku Centre for Biotechnology [Turku, Finland], University of Turku-Åbo Academy University, Department of Future Technologies [Turku], University of Turku, Department of Medical Informatics and Clinical Epidemiology [Portland, OR, USA] (School of Medicine), Oregon Health & Science University, Duke Center for Applied Genomics and Precision Medicine [Durham, NC, USA], Duke University School of Medicine [Durham, NC, USA], Sage Bionetworks [Seattle, WA, USA], Department of Computer Engineering [Kayseri, Turkey], Abdullah Gul University [Kayseri, Turkey], School of Engineering and Technology [Tacoma, WA, USA], University of Washington (Tacoma), Department of Genetics and Genomic Sciences and Icahn Institute for Genomics and Multiscale Biology [New York, NY, USA], Icahn School of Medicine at Mount Sinai [New York] (MSSM), Origent Data Sciences, Inc. [Vienna, VA, USA], Department of Mechanical Engineering [Tainan, Taiwan], National Cheng Kung University (NCKU), Department of Electrical, Electronic and Computer Engineering [Gifu, Japan] (Faculty of Engineering), Gifu University, Department of Computer Science [Carrolton, GA, USA], State University of West Georgia (SUWG), IBM T.J. Watson Research Center [Yorktown Heights, NY, USA], Medical Service [Durham, NC, USA], Durham VA Health Care System [Durham, NC, USA], This work was supported by Defense Advanced Research Projects Agency and the Army Research Office through Grant W911NF-15-1-0107. The views expressed are those of the authors and do not reflect the official policy or position of the Department of Defense or the U.S. Government. J.G.B. was supported by a training grant from the National Institutes of Health, USA (NIH grant 4T15LM007088-25). G.P. and A.S.’s work was supported by NIH grant # R01GM114434 and an IBM faculty award to G.P. T.E.M.N. was supported by the Ministry of Science and Technology of Taiwan grants MOST 105-2218-E-006-016-MY2 and 107-2634-F-006-009. K.Y.Y. was supported by NIH grants U54 HL127624 and R01GM126019. M.S. was supported by Grants-in-Aid for Scientific Research JP16H02866 from the Japan Society for the Promotion of Science., and Bleakley, Kevin

Subjects

0301 basic medicine, ENSEMBLES, Rhinovirus, viruses, General Physics and Astronomy, Gene Expression, medicine.disease_cause, Viral infection, DISEASE, EXPRESSION PROFILES, [STAT.ML]Statistics [stat]/Machine Learning [stat.ML], HUMAN ERYTHROCYTE-MEMBRANES, Gene expression, Heme metabolism, Influenza A virus, Respiratory system, lcsh:Science, INFLUENZA-VIRUS INFECTION, Multidisciplinary, GLYCOPHORINS, IRON, Healthy Volunteers, 3. Good health, Respiratory Syncytial Viruses, Multidisciplinary Sciences, INFLUENZA, Science & Technology - Other Topics, VIRUSES, Science, Heme, Biology, General Biochemistry, Genetics and Molecular Biology, Article, 03 medical and health sciences, Text mining, Influenza A Virus, H1N2 Subtype, medicine, Humans, HEME OXYGENASE, Gene, Science & Technology, business.industry, Influenza A Virus, H3N2 Subtype, General Chemistry, Respiratory Viral DREAM Challenge Consortium, GENE, [STAT.ML] Statistics [stat]/Machine Learning [stat.ML], 030104 developmental biology, Immunology, lcsh:Q, CHALLENGE, business, RESPONSES

Abstract

The response to respiratory viruses varies substantially between individuals, and there are currently no known molecular predictors from the early stages of infection. Here we conduct a community-based analysis to determine whether pre- or early post-exposure molecular factors could predict physiologic responses to viral exposure. Using peripheral blood gene expression profiles collected from healthy subjects prior to exposure to one of four respiratory viruses (H1N1, H3N2, Rhinovirus, and RSV), as well as up to 24 h following exposure, we find that it is possible to construct models predictive of symptomatic response using profiles even prior to viral exposure. Analysis of predictive gene features reveal little overlap among models; however, in aggregate, these genes are enriched for common pathways. Heme metabolism, the most significantly enriched pathway, is associated with a higher risk of developing symptoms following viral exposure. This study demonstrates that pre-exposure molecular predictors can be identified and improves our understanding of the mechanisms of response to respiratory viruses., The response to respiratory virus exposure can currently not be predicted by pre- or early post-exposure molecular signatures. Here, the authors conduct a community-based analysis of blood gene expression from healthy individuals exposed to respiratory viruses and provide predictive models and biological insight into the physiological response.

Published

2018

24. Translocated microbiome composition determines immunological outcome in treated HIV infection

Author

Peter Mugyenyi, Benigno Rodriguez, Farida Laboune, Timothy W. Schacker, Rafick Pierre Sekaly, Daniel C. Douek, Jeffery Tomalka, Daniel Kaufmann, Nichole R. Klatt, Sam Darko, Jacob K. Flynn, Elsa Brunet-Ratnasingham, Patrick Ssengendo, Jordan Schoephoerster, Jeffrey G. Chipman, Ryan K. Cheu, Antigoni Morou, Ashish Sharma, Aarthi Talla, Krystelle Nganou-Makamdop, Francis Ssali, Proscovia Muloma, Samuel P. Callisto, Amy Ransier, Michael M. Lederman, Slim Fourati, Gregory J. Beilman, Torfi Hoskuldsson, Noemia S. Lima, Ana Rachel Leda, Thomas E. Schmidt, Cissy Kityo, Jason M. Brenchley, Sahaana Arumugam, and Damee Moon

Subjects

CD4-Positive T-Lymphocytes, Serratia, Transcription, Genetic, Systems biology, HIV Infections, Inflammation, CD8-Positive T-Lymphocytes, Systemic inflammation, Article, Monocytes, General Biochemistry, Genetics and Molecular Biology, Microbiology, Cohort Studies, Th2 Cells, Downregulation and upregulation, Antiretroviral Therapy, Highly Active, Nucleic Acids, Gene expression, medicine, Humans, Uganda, Microbiome, Principal Component Analysis, biology, Biodiversity, Th1 Cells, Viral Load, biology.organism_classification, Gastrointestinal Microbiome, Mitochondria, Chemokines, medicine.symptom, Glycolysis, Homeostasis

Abstract

Summary The impact of the microbiome on HIV disease is widely acknowledged although the mechanisms downstream of fluctuations in microbial composition remain speculative. We detected rapid, dynamic changes in translocated microbial constituents during two years after cART initiation. An unbiased systems biology approach revealed two distinct pathways driven by changes in the abundance ratio of Serratia to other bacterial genera. Increased CD4 T cell numbers over the first year were associated with high Serratia abundance, pro-inflammatory innate cytokines, and metabolites that drive Th17 gene expression signatures and restoration of mucosal integrity. Subsequently, decreased Serratia abundance and downregulation of innate cytokines allowed re-establishment of systemic T cell homeostasis promoting restoration of Th1 and Th2 gene expression signatures. Analyses of three other geographically distinct cohorts of treated HIV infection established a more generalized principle that changes in diversity and composition of translocated microbial species influence systemic inflammation and consequently CD4 T cell recovery.

Published

2021

25. Effect of Anti–IL-15 Administration on T Cell and NK Cell Homeostasis in Rhesus Macaques

Author

Aarthi Talla, Rafick Pierre Sekaly, Matthew D. Reyes, Mukta Vaidya, Amit Sabnis, Michael K. Axthelm, Afam A. Okoye, Jacob D. Estes, Keith A. Reiman, Alfred W. Legasse, Joseph A. Clock, Audrie L. Konfe, Maren Q. Degottardi, Louis J. Picker, Derick M. Duell, and Byung Park

Subjects

0301 basic medicine, T-Lymphocytes, medicine.medical_treatment, T cell, Immunology, Enzyme-Linked Immunosorbent Assay, Cell Separation, Biology, Article, 03 medical and health sciences, Interleukin 21, medicine, Animals, Homeostasis, Immunology and Allergy, Cytotoxic T cell, IL-2 receptor, Oligonucleotide Array Sequence Analysis, Interleukin-15, Interleukin-17, Flow Cytometry, Immunohistochemistry, Macaca mulatta, Lymphocyte Subsets, Cell biology, Killer Cells, Natural, 030104 developmental biology, Cytokine, medicine.anatomical_structure, Interleukin 15, Interleukin 12, CD8

Abstract

IL-15 has been implicated as a key regulator of T and NK cell homeostasis in multiple systems; however, its specific role in maintaining peripheral T and NK cell populations relative to other γ-chain (γc) cytokines has not been fully defined in primates. In this article, we address this question by determining the effect of IL-15 inhibition with a rhesusized anti–IL-15 mAb on T and NK cell dynamics in rhesus macaques. Strikingly, anti–IL-15 treatment resulted in rapid depletion of NK cells and both CD4+ and CD8+ effector memory T cells (TEM) in blood and tissues, with little to no effect on naive or central memory T cells. Importantly, whereas depletion of NK cells was nearly complete and maintained as long as anti–IL-15 treatment was given, TEM depletion was countered by the onset of massive TEM proliferation, which almost completely restored circulating TEM numbers. Tissue TEM, however, remained significantly reduced, and most TEM maintained very high turnover throughout anti–IL-15 treatment. In the presence of IL-15 inhibition, TEM became increasingly more sensitive to IL-7 stimulation in vivo, and transcriptional analysis of TEM in IL-15–inhibited monkeys revealed engagement of the JAK/STAT signaling pathway, suggesting alternative γc cytokine signaling may support TEM homeostasis in the absence of IL-15. Thus, IL-15 plays a major role in peripheral maintenance of NK cells and TEM. However, whereas most NK cell populations collapse in the absence of IL-15, TEM can be maintained in the face of IL-15 inhibition by the activity of other homeostatic regulators, most likely IL-7.

Published

2016

26. A crowdsourced analysis to identifyab initiomolecular signatures predictive of susceptibility to viral infection

Author

Ephraim L. Tsalik, Ana Stanescu, Xiao Liang, Micah T. McClain, Aarthi Talla, Lara M. Mangravite, Slim Fourati, Robert Vogel, Samad Jahandideh, Reem Almugbel, Torbjörn E. M. Nordling, Solveig K. Sieberts, Riku Klén, Zafer Aydin, Gaurav Pandey, Laura L. Elo, Joshua Burkhart, Ricardo Henao, Geoffrey S. Ginsburg, Mehmet Eren Ahsen, Ka Yee Yeung, Christopher Chiu, Christopher W. Woods, Motoki Shiga, and Mehrad Mahmoudian

Subjects

0303 health sciences, viruses, Late stage, Healthy subjects, Biology, medicine.disease_cause, Viral infection, Peripheral blood, 3. Good health, 03 medical and health sciences, 0302 clinical medicine, Gene expression, Immunology, medicine, Rhinovirus, Respiratory system, Gene, 030217 neurology & neurosurgery, 030304 developmental biology

Abstract

Respiratory viruses are highly infectious; however, the variation of individuals’ physiologic responses to viral exposure is poorly understood. Most studies examining molecular predictors of response focus on late stage predictors, typically near the time of peak symptoms. To determine whether pre- or early post-exposure factors could predict response, we conducted a community-based analysis to identify predictors of resilience or susceptibility to several respiratory viruses (H1N1, H3N2, Rhinovirus, and RSV) using peripheral blood gene expression profiles collected from healthy subjects prior to viral exposure, as well as up to 24 hours following exposure. This analysis revealed that it is possible to construct models predictive of symptoms using profiles even prior to viral exposure. Analysis of predictive gene features revealed little overlap among models; however, in aggregate, these genes were enriched for common pathways. Heme Metabolism, the most significantly enriched pathway, was associated with higher risk of developing symptoms following viral exposure.

Published

2018

27. The contribution of memory CD4+ T cell subset phenotype to latency reversal efficiency

Author

Aarthi Talla, N. Chomont, R. Pierre Sékaly, Susan Pereira Ribeiro, Deanna A. Kulpa, Richard J. O. Barnard, and Daria J. Hazuda

Subjects

Cd4 t cell, Epidemiology, Immunology, Public Health, Environmental and Occupational Health, Biology, Phenotype, Microbiology, QR1-502, Infectious Diseases, Virology, Latency (engineering), Public aspects of medicine, RA1-1270, Neuroscience

Published

2017

28. Mucosal Regulatory T Cells and T Helper 17 Cells in HIV-Associated Immune Activation

Author

Pushpa Pandiyan, Aaron Weinberg, Susan Pereira Ribeiro, Aarthi Talla, Natarajan Bhaskaran, Alan D. Levine, David McDonald, Rafick Pierre Sekaly, and Souheil Antoine Younes

Subjects

0301 basic medicine, Immunology, Tregs, chemical and pharmacologic phenomena, Inflammation, Biology, medicine.disease_cause, 03 medical and health sciences, 0302 clinical medicine, Immune system, Hypothesis and Theory, Immunopathology, medicine, Immunology and Allergy, Innate lymphoid cell, Lymphokine, HIV, FOXP3, biochemical phenomena, metabolism, and nutrition, Immune dysregulation, Acquired immune system, 030104 developmental biology, Foxp3, mucosal immunity, bacteria, Th17, medicine.symptom, 030215 immunology

Abstract

Residual mucosal inflammation along with chronic systemic immune activation is an important feature in individuals infected with human immunodeficiency virus (HIV), and has been linked to a wide range of co-morbidities, including malignancy, opportunistic infections, immunopathology, and cardiovascular complications. Although combined antiretroviral therapy (cART) can reduce plasma viral loads to undetectable levels, reservoirs of virus persist, and increased mortality is associated with immune dysbiosis in mucosal lymphoid tissues. Immune-based therapies are pursued with the goal of improving CD4(+) T-cell restoration, as well as reducing chronic immune activation in cART-treated patients. However, the majority of research on immune activation has been derived from analysis of circulating T cells. How immune cell alterations in mucosal tissues contribute to HIV immune dysregulation and the associated risk of non-infectious chronic complications is less studied. Given the significant differences between mucosal T cells and circulating T cells, and the immediate interactions of mucosal T cells with the microbiome, more attention should be devoted to mucosal immune cells and their contribution to systemic immune activation in HIV-infected individuals. Here, we will focus on mucosal immune cells with a specific emphasis on CD4(+) T lymphocytes, such as T helper 17 cells and CD4(+)Foxp3(+) regulatory T cells (Tregs), which play crucial roles in maintaining mucosal barrier integrity and preventing inflammation, respectively. We hypothesize that pro-inflammatory milieu in cART-treated patients with immune activation significantly contributes to enhanced loss of Th17 cells and increased frequency of dysregulated Tregs in the mucosa, which in turn may exacerbate immune dysfunction in HIV-infected patients. We also present initial evidence to support this hypothesis. A better comprehension of how pro-inflammatory milieu impacts these two types of cells in the mucosa will shed light on mucosal immune dysfunction and HIV reservoirs, and lead to novel ways to restore immune functions in HIV(+) patients.

Published

2016

29. Pre-vaccination inflammation and B-cell signalling predict age-related hyporesponse to hepatitis B vaccination

Author

Ali Filali, Dominic Gagnon, Aarthi Talla, Rafick-Pierre Sekaly, Danilo R. Casimiro, Andrea K. Schaeffer, Radha Railkar, Slim Fourati, Leonidas N. Carayannopoulos, Andrey Loboda, I-Ming Wang, Razvan Cristescu, David Favre, Chan R. Beals, and Yoav Peretz

Subjects

Adult, Male, 0301 basic medicine, Aging, Science, General Physics and Astronomy, Inflammation, Biology, medicine.disease_cause, Article, General Biochemistry, Genetics and Molecular Biology, Flow cytometry, Cohort Studies, Transcriptome, 03 medical and health sciences, medicine, Humans, Hepatitis B Vaccines, B cell, Aged, Whole blood, Aged, 80 and over, Hepatitis B virus, B-Lymphocytes, Hepatitis B Surface Antigens, Multidisciplinary, medicine.diagnostic_test, Vaccination, General Chemistry, Middle Aged, Flow Cytometry, Virology, 030104 developmental biology, medicine.anatomical_structure, Signalling, Immunology, Erythrocyte Count, Female, medicine.symptom, Biomarkers

Abstract

Aging is associated with hyporesponse to vaccination, whose mechanisms remain unclear. In this study hepatitis B virus (HBV)-naive older adults received three vaccines, including one against HBV. Here we show, using transcriptional and cytometric profiling of whole blood collected before vaccination, that heightened expression of genes that augment B-cell responses and higher memory B-cell frequencies correlate with stronger responses to HBV vaccine. In contrast, higher levels of inflammatory response transcripts and increased frequencies of pro-inflammatory innate cells correlate with weaker responses to this vaccine. Increased numbers of erythrocytes and the haem-induced response also correlate with poor response to the HBV vaccine. A transcriptomics-based pre-vaccination predictor of response to HBV vaccine is built and validated in distinct sets of older adults. This moderately accurate (area under the curve≈65%) but robust signature is supported by flow cytometry and cytokine profiling. This study is the first that identifies baseline predictors and mechanisms of response to the HBV vaccine., Ageing is associated with poor responses to vaccines but the underlying mechanism remains unclear. Here the authors use a systems-based approach to define molecular signatures present before vaccination that correlate with non-responsiveness to hepatitis B vaccination in healthy, elderly adults.

Published

2016

30. Memory CD4+ T cell subsets show differential responses to HIV latency-reversing agents

Author

Rafick Pierre Sekaly, Aarthi Talla, Michael W. Miller, Nicolas Chomont, A.G. Bebein-Blackwell, Jessica H. Brehm, Daria J. Hazuda, Richard J. O. Barnard, Deanna A. Kulpa, and S. Yuan

Subjects

Cd4 t cell, Epidemiology, Immunology, Public Health, Environmental and Occupational Health, Human immunodeficiency virus (HIV), Biology, medicine.disease_cause, Microbiology, QR1-502, Infectious Diseases, Virology, medicine, Reversing, Latency (engineering), Public aspects of medicine, RA1-1270, Neuroscience

Published

2015

31. A-108 The Contribution of memory CD4+ T cell subset phenotype to latency reversal efficiency

Author

Aarthi Talla, Deanna A. Kulpa, Daria J. Hazuda, Rafick Pierre Sekaly, Nicolas Chomont, Susan Pereira Ribeiro, and Richard J. O. Barnard

Subjects

Infectious Diseases, Cd4 t cell, Pharmacology (medical), Latency (engineering), Biology, Phenotype, Neuroscience

Published

2018

32. Novel mechanisms to inhibit HIV reservoir seeding using Jak inhibitors

Author

Laurent Sabbagh, Susan Pereira Ribeiro, Christina Gavegnano, Cheryl M. Cameron, Selwyn J. Hurwitz, Vincent C. Marconi, Stephanie Santos, Franck P. Dupuy, Raymond F. Schinazi, Aarthi Talla, Jessica H. Brehm, Rafick Pierre Sekaly, Deanna A. Kulpa, and Jean-Pierre Routy

Subjects

CD4-Positive T-Lymphocytes, RNA viruses, 0301 basic medicine, Physiology, medicine.medical_treatment, HIV Infections, Virus Replication, Pathology and Laboratory Medicine, Biochemistry, Memory T cells, White Blood Cells, 0302 clinical medicine, Piperidines, Immunodeficiency Viruses, Animal Cells, Immune Physiology, Virus latency, Medicine and Health Sciences, Post-Translational Modification, Phosphorylation, Receptor, lcsh:QH301-705.5, Cells, Cultured, Innate Immune System, T Cells, Virus Latency, 3. Good health, Cytokine, medicine.anatomical_structure, Medical Microbiology, Viral Pathogens, 030220 oncology & carcinogenesis, Viruses, Cytokines, Infectious diseases, Pathogens, Cellular Types, Research Article, lcsh:Immunologic diseases. Allergy, Anti-HIV Agents, Immune Cells, T cell, Immunology, Viral diseases, Biology, Microbiology, 03 medical and health sciences, In vivo, Virology, Nitriles, Retroviruses, Genetics, medicine, Humans, Janus Kinase Inhibitors, Pyrroles, T Helper Cells, Microbial Pathogens, Molecular Biology, Blood Cells, Lentivirus, Organisms, Biology and Life Sciences, HIV, Proteins, Cell Biology, Molecular Development, medicine.disease, Viral Replication, In vitro, Pyrimidines, 030104 developmental biology, lcsh:Biology (General), Viral replication, Immune System, HIV-1, Cancer research, Pyrazoles, Parasitology, lcsh:RC581-607, Ex vivo, Developmental Biology

Abstract

Despite advances in the treatment of HIV infection with ART, elucidating strategies to overcome HIV persistence, including blockade of viral reservoir establishment, maintenance, and expansion, remains a challenge. T cell homeostasis is a major driver of HIV persistence. Cytokines involved in regulating homeostasis of memory T cells, the major hub of the HIV reservoir, trigger the Jak-STAT pathway. We evaluated the ability of tofacitinib and ruxolitinib, two FDA-approved Jak inhibitors, to block seeding and maintenance of the HIV reservoir in vitro. We provide direct demonstration for involvement of the Jak-STAT pathway in HIV persistence in vivo, ex vivo, and in vitro; pSTAT5 strongly correlates with increased levels of integrated viral DNA in vivo, and in vitro Jak inhibitors reduce the frequency of CD4+ T cells harboring integrated HIV DNA. We show that Jak inhibitors block viral production from infected cells, inhibit γ-C receptor cytokine (IL-15)-induced viral reactivation from latent stores thereby preventing transmission of infectious particles to bystander activated T cells. These results show that dysregulation of the Jak-STAT pathway is associated with viral persistence in vivo, and that Jak inhibitors target key events downstream of γ-C cytokine (IL-2, IL-7 and IL-15) ligation to their receptors, impacting the magnitude of the HIV reservoir in all memory CD4 T cell subsets in vitro and ex vivo. Jak inhibitors represent a therapeutic modality to prevent key events of T cell activation that regulate HIV persistence and together, specific, potent blockade of these events may be integrated to future curative strategies., Author summary HIV persists in infected hosts in a small number of CD4 + memory T cells as latently infected proviruses. Homeostatic cytokines, which play a major role in the maintenance of T cell memory, also enable the persistence of latently infected cells. The pathways downstream of these homeostatic cytokines are well known and drugs that target these pathways have been developed and have been safely used in inflammatory diseases and in myelofibrosis. We have used these drugs to inhibit the maintenance and the spread of HIV infected cells carrying latent forms of the virus. We show that ruxolitinib and tofacitinib will inhibit the expansion of these cells and their capacity to infect other cells upon reactivation. This class of drugs is currently being tested in clinical trials.

Published

2017

33. Mechanisms of T follicular helper (Tfh) impairment in chronic HIV infection

Author

Marita Chakhtoura, Rafael Cubas, Aarthi Talla, Virginie TARDIF, and Elias Haddad

Subjects

Immunology, Immunology and Allergy

Abstract

Human immunodeficiency virus (HIV) infects millions of people worldwide. In secondary lymphoid organs, site where the anti-HIV immune response is mounted, the virus has been shown to induce a predominant dysregulation and disturbance of the microvenvironment. Previous work in our laboratory has identified the lack of protective anti-HIV antibodies in patients to be due, at least in part, to an inadequate T follicular helper (Tfh) cell help to germinal center (GC) B cells in draining lymph nodes through impaired PD-1/PD-L1 interactions. Since the mechanism of this impairment is not yet fully elucidated, we have used our co-culture assay followed by a unique gene array analysis to screen for key molecular pathways that could be accountable for the difference between helper programs in Tfh cells of HIV positive and negative individuals. The major driver of gene profile clustering was observed within Tfh proliferation programs as well as infection status. Gene set enrichment analysis included repair mechanisms, cell cycle regulation, metabolism, signal transduction and co-stimulation in the top 10 enriched pathways. Careful examination of gene fold changes in proliferating vs non-proliferating Tfh cells between healthy and HIV individuals showed a decrease with HIV, in immune regulatory gene expression such as the transcription factor c-maf and its mediators, responsible for Tfh differentiation, development, survival and performance. Investigating this pathway would contribute to a better understanding of the HIV-mediated dysregulation.

Published

2017

34. Small RNA profiling of virus-infected grapevines: evidences for virus infection-associated and variety-specific miRNAs

Author

Aarthi Talla, Kashmir Singh, and Wenping Qiu

Subjects

Small RNA, biology, Cell Cycle, RNA, Caulimoviridae, General Medicine, biology.organism_classification, Virology, Virus, MicroRNAs, Viral replication, Gene Expression Regulation, Plant, RNA, Plant, Stress, Physiological, Gene expression, Genetics, Gene silencing, Vitis, RNA, Small Interfering, Transcriptome, Gene, Plant Diseases, Plant Proteins, Transcription Factors

Abstract

Grapevine is one of the economically and culturally important perennial fruit crops. More than 60 viruses infect grapevines and adversely affect their growth and development. Latent infection of most viruses in grapevines leads to chronic modulation of gene expression at transcriptional and post-transcriptional levels. Plant small RNAs (sRNAs) consist of microRNA (miRNA) and small interfering RNA (siRNA). miRNAs are expressed from the plant genome while most siRNAs are derived from double-stranded RNA molecules which are intermediates during virus replication. In a previous study, we constructed four cDNA libraries of sRNAs that were enriched from three virus-infected grapevines and one virus-free grapevine. Majority of siRNAs align most closely with the genomes of DNA viruses in the genus Badnavirus, family Caulimoviridae that led to the discovery of a new Grapevine vein clearing virus in grapevines. In this study, we conducted a comprehensive analysis of miRNAs in the four cDNA libraries and identified novel and stress-related miRNAs. The results indicated that miRNA abundance was influenced by virus infection. A total of 54 new miRNAs were identified and characterized, six of which, VITIS-MIR17, 18, 19, 20, 21, and 22, were detected only in virus-infected samples. One target of VITIS-MIR18 is the gene coding a non-apical meristem protein (GSVIVT00035370001), a transcription factor in the regulation of plant development and stress responses. Among the virus infection-induced known miRNAs, miRNA168 and miRNA3623 likely regulate grapevine's defense response, miRNA319 and miRNA395 modulate the expression of genes that are involved in nutrient metabolisms while miRNA396 plays a role in the regulation of cell division and cell cycle. The abiotic stress-induced miR169 and mi398 were negatively regulated by virus infection in grapevines. In addition, variety-specific miRNAs were discovered and compiled. The newly discovered miRNAs expand the miRNA profiles in the Vitis species. The characteristics of variety-specific and virus infection-associated miRNAs help understand the biology underlying the development and defense response of grapevines.

Published

2012