Your search keyword '"Thanh, Cassandra"' showing total 34 results

1. A cohort-based study of host gene expression: tumor suppressor and innate immune/inflammatory pathways associated with the HIV reservoir size.

Author

Dwivedi, Ashok, Gornalusse, Germán, Siegel, David, Barbehenn, Alton, Thanh, Cassandra, Hoh, Rebecca, Hobbs, Kristen, Pan, Tony, Gibson, Erica, Martin, Jeffrey, Hecht, Frederick, Pilcher, Christopher, Milush, Jeffrey, Busch, Michael, Stone, Mars, Huang, Meei-Li, Reppetti, Julieta, Vo, Phuong, Levy, Claire, Roychoudhury, Pavitra, Jerome, Keith, Hladik, Florian, Henrich, Timothy, Deeks, Steven, and Lee, Sulggi

Abstract

The major barrier to an HIV cure is the HIV reservoir: latently-infected cells that persist despite effective antiretroviral therapy (ART). There have been few cohort-based studies evaluating host genomic or transcriptomic predictors of the HIV reservoir. We performed host RNA sequencing and HIV reservoir quantification (total DNA [tDNA], unspliced RNA [usRNA], intact DNA) from peripheral CD4+ T cells from 191 ART-suppressed people with HIV (PWH). After adjusting for nadir CD4+ count, timing of ART initiation, and genetic ancestry, we identified two host genes for which higher expression was significantly associated with smaller total DNA viral reservoir size, P3H3 and NBL1, both known tumor suppressor genes. We then identified 17 host genes for which lower expression was associated with higher residual transcription (HIV usRNA). These included novel associations with membrane channel (KCNJ2, GJB2), inflammasome (IL1A, CSF3, TNFAIP5, TNFAIP6, TNFAIP9, CXCL3, CXCL10), and innate immunity (TLR7) genes (FDR-adjusted q

Published

2023

2. Host variation in type I interferon signaling genes (MX1), C-C chemokine receptor type 5 gene, and major histocompatibility complex class I alleles in treated HIV+ noncontrollers predict viral reservoir size.

Author

Siegel, David A, Thanh, Cassandra, Wan, Eunice, Hoh, Rebecca, Hobbs, Kristen, Pan, Tony, Gibson, Erica A, Kroetz, Deanna L, Martin, Jeffrey, Hecht, Frederick, Pilcher, Christopher, Martin, Maureen, Carrington, Mary, Pillai, Satish, Busch, Michael P, Stone, Mars, Levy, Claire N, Huang, Meei-Li, Roychoudhury, Pavitra, Hladik, Florian, Jerome, Keith R, Kiem, Hans-Peter, Henrich, Timothy J, Deeks, Steven G, and Lee, Sulggi A

Subjects

CD8-Positive T-Lymphocytes, Humans, HIV-1, HIV Infections, Interferon Type I, Histocompatibility Antigens Class I, HLA Antigens, Cross-Sectional Studies, Alleles, Myxovirus Resistance Proteins, Major Histocompatibility Complex, Receptors, Chemokine, RNA, Viral Load, Genetics, Infectious Diseases, Human Genome, HIV/AIDS, Aetiology, 2.1 Biological and endogenous factors, Infection, C-C chemokine receptor type 5 gene, HIV reservoir, host genetics, major histocompatibility complex class I, type I interferon, Biological Sciences, Medical and Health Sciences, Psychology and Cognitive Sciences, Virology

Abstract

ObjectivePrior genomewide association studies have identified variation in major histocompatibility complex (MHC) class I alleles and C-C chemokine receptor type 5 gene (CCR5Δ32) as genetic predictors of viral control, especially in 'elite' controllers, individuals who remain virally suppressed in the absence of therapy.DesignCross-sectional genomewide association study.MethodsWe analyzed custom whole exome sequencing and direct human leukocyte antigen (HLA) typing from 202 antiretroviral therapy (ART)-suppressed HIV+ noncontrollers in relation to four measures of the peripheral CD4+ T-cell reservoir: HIV intact DNA, total (t)DNA, unspliced (us)RNA, and RNA/DNA. Linear mixed models were adjusted for potential covariates including age, sex, nadir CD4+ T-cell count, pre-ART HIV RNA, timing of ART initiation, and duration of ART suppression.ResultsPreviously reported 'protective' host genetic mutations related to viral setpoint (e.g. among elite controllers) were found to predict smaller HIV reservoir size. The HLA 'protective' B∗57:01 was associated with significantly lower HIV usRNA (q = 3.3 × 10-3), and among the largest subgroup, European ancestry individuals, the CCR5Δ32 deletion was associated with smaller HIV tDNA (P = 4.3 × 10-3) and usRNA (P = 8.7 × 10-3). In addition, genomewide analysis identified several single nucleotide polymorphisms in MX1 (an interferon stimulated gene) that were significantly associated with HIV tDNA (q = 0.02), and the direction of these associations paralleled MX1 gene eQTL expression.ConclusionsWe observed a significant association between previously reported 'protective' MHC class I alleles and CCR5Δ32 with the HIV reservoir size in noncontrollers. We also found a novel association between MX1 and HIV total DNA (in addition to other interferon signaling relevant genes, PPP1CB, DDX3X). These findings warrant further investigation in future validation studies.

Published

2023

3. Pre-clerkship Teaching and Learning in the Virtual Learning Environment: Lessons Learned and Future Directions.

Author

Sewell, Justin L, Joshi, Mihir, Thanh, Cassandra, Apollon, Chantilly, Austin, Elizabeth, Burke, Christian, Cornes, Susannah, Davis, John A, and Hermiston, Michelle

Subjects

Cognitive load theory, Curriculum development, Sociocultural learning theory, Undergraduate medical education, Virtual learning, Brain Disorders, Behavioral and Social Science

Abstract

In response to the COVID-19 pandemic, we developed and implemented a theory-informed process to adapt a comprehensive pre-clerkship medical school curriculum to run in the virtual learning environment utilizing sociocultural learning theory and cognitive load theory. Of 124 student respondents, 45% rated virtual learning as very or extremely effective, and 49% as moderately effective. Positive aspects of virtual learning included effectiveness of chat moderators, displaying pronouns on Zoom, active learning technology, and captioning and transcription. Negative aspects included access to technology and feeling isolated from community. Overall course ratings, examination performance, and work hours did not differ pre- and post-implementation.

Published

2022

4. First-in-human immunoPET imaging of HIV-1 infection using 89Zr-labeled VRC01 broadly neutralizing antibody

Author

Beckford-Vera, Denis R, Flavell, Robert R, Seo, Youngho, Martinez-Ortiz, Enrique, Aslam, Maya, Thanh, Cassandra, Fehrman, Emily, Pardons, Marion, Kumar, Shreya, Deitchman, Amelia N, Ravanfar, Vahid, Schulte, Brailee, Wu, I-Wei Katherine, Pan, Tony, Reeves, Jacqueline D, Nixon, Christopher C, Iyer, Nikita S, Torres, Leonel, Munter, Sadie E, Hyunh, Tony, Petropoulos, Christos J, Hoh, Rebecca, Franc, Benjamin L, Gama, Lucio, Koup, Richard A, Mascola, John R, Chomont, Nicolas, Deeks, Steven G, VanBrocklin, Henry F, and Henrich, Timothy J

Subjects

Medical Microbiology, Biomedical and Clinical Sciences, Immunology, HIV/AIDS, Infectious Diseases, Biomedical Imaging, Clinical Research, 2.1 Biological and endogenous factors, Aetiology, Infection, Good Health and Well Being, Antibodies, Neutralizing, Broadly Neutralizing Antibodies, CD4-Positive T-Lymphocytes, HIV Infections, HIV-1, Humans, Positron-Emission Tomography, Viral Load, Viremia

Abstract

A major obstacle to achieving long-term antiretroviral (ART) free remission or functional cure of HIV infection is the presence of persistently infected cells that establish a long-lived viral reservoir. HIV largely resides in anatomical regions that are inaccessible to routine sampling, however, and non-invasive methods to understand the longitudinal tissue-wide burden of HIV persistence are urgently needed. Positron emission tomography (PET) imaging is a promising strategy to identify and characterize the tissue-wide burden of HIV. Here, we assess the efficacy of using immunoPET imaging to characterize HIV reservoirs and identify anatomical foci of persistent viral transcriptional activity using a radiolabeled HIV Env-specific broadly neutralizing antibody, 89Zr-VRC01, in HIV-infected individuals with detectable viremia and on suppressive ART compared to uninfected controls (NCT03729752). We also assess the relationship between PET tracer uptake in tissues and timing of ART initiation and direct HIV protein expression in CD4 T cells obtained from lymph node biopsies. We observe significant increases in 89Zr-VRC01 uptake in various tissues (including lymph nodes and gut) in HIV-infected individuals with detectable viremia (N = 5) and on suppressive ART (N = 5) compared to uninfected controls (N = 5). Importantly, PET tracer uptake in inguinal lymph nodes in viremic and ART-suppressed participants significantly and positively correlates with HIV protein expression measured directly in tissue. Our strategy may allow non-invasive longitudinal characterization of residual HIV infection and lays the framework for the development of immunoPET imaging in a variety of other infectious diseases.

Published

2022

5. Long-term SARS-CoV-2-specific immune and inflammatory responses in individuals recovering from COVID-19 with and without post-acute symptoms.

Author

Peluso, Michael J, Deitchman, Amelia N, Torres, Leonel, Iyer, Nikita S, Munter, Sadie E, Nixon, Christopher C, Donatelli, Joanna, Thanh, Cassandra, Takahashi, Saki, Hakim, Jill, Turcios, Keirstinne, Janson, Owen, Hoh, Rebecca, Tai, Viva, Hernandez, Yanel, Fehrman, Emily A, Spinelli, Matthew A, Gandhi, Monica, Trinh, Lan, Wrin, Terri, Petropoulos, Christos J, Aweeka, Francesca T, Rodriguez-Barraquer, Isabel, Kelly, J Daniel, Martin, Jeffrey N, Deeks, Steven G, Greenhouse, Bryan, Rutishauser, Rachel L, and Henrich, Timothy J

Subjects

COVID-19, PASC, SARS-CoV-2, T cell, immunity, long COVID, post-acute sequelae of SARS-CoV-2 infection, Biochemistry and Cell Biology, Medical Physiology

Abstract

We describe severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2)-specific T cell responses, soluble markers of inflammation, and antibody levels and neutralization capacity longitudinally in 70 individuals with PCR-confirmed SARS-CoV-2 infection. Participants represent a spectrum of illness and recovery, including some with persistent viral shedding in saliva and many experiencing post-acute sequelae of SARS-CoV-2 infection (PASC). T cell responses remain stable for up to 9 months. Whereas the magnitude of early CD4+ T cell immune responses correlates with severity of initial infection, pre-existing lung disease is independently associated with higher long-term SARS-CoV-2-specific CD8+ T cell responses. Among participants with PASC 4 months following coronavirus disease 2019 (COVID-19) symptom onset, we observe a lower frequency of CD8+ T cells expressing CD107a, a marker of degranulation, in response to Nucleocapsid (N) peptide pool stimulation, and a more rapid decline in the frequency of N-specific interferon-γ-producing CD8+ T cells. Neutralizing antibody levels strongly correlate with SARS-CoV-2-specific CD4+ T cell responses.

Published

2021

6. SARS-CoV-2 antibody magnitude and detectability are driven by disease severity, timing, and assay

Author

Peluso, Michael J, Takahashi, Saki, Hakim, Jill, Kelly, J Daniel, Torres, Leonel, Iyer, Nikita S, Turcios, Keirstinne, Janson, Owen, Munter, Sadie E, Thanh, Cassandra, Donatelli, Joanna, Nixon, Christopher C, Hoh, Rebecca, Tai, Viva, Fehrman, Emily A, Hernandez, Yanel, Spinelli, Matthew A, Gandhi, Monica, Palafox, Mary-Ann, Vallari, Ana, Rodgers, Mary A, Prostko, John, Hackett, John, Trinh, Lan, Wrin, Terri, Petropoulos, Christos J, Chiu, Charles Y, Norris, Philip J, DiGermanio, Clara, Stone, Mars, Busch, Michael P, Elledge, Susanna K, Zhou, Xin X, Wells, James A, Shu, Albert, Kurtz, Theodore W, Pak, John E, Wu, Wesley, Burbelo, Peter D, Cohen, Jeffrey I, Rutishauser, Rachel L, Martin, Jeffrey N, Deeks, Steven G, Henrich, Timothy J, Rodriguez-Barraquer, Isabel, and Greenhouse, Bryan

Subjects

Medical Microbiology, Biomedical and Clinical Sciences, Coronaviruses, Emerging Infectious Diseases, Infectious Diseases, Infection, Good Health and Well Being

Abstract

Interpretation of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) serosurveillance studies is limited by poorly defined performance of antibody assays over time in individuals with different clinical presentations. We measured antibody responses in plasma samples from 128 individuals over 160 days using 14 assays. We found a consistent and strong effect of disease severity on antibody magnitude, driven by fever, cough, hospitalization, and oxygen requirement. Responses to spike protein versus nucleocapsid had consistently higher correlation with neutralization. Assays varied substantially in sensitivity during early convalescence and time to seroreversion. Variability was dramatic for individuals with mild infection, who had consistently lower antibody titers, with sensitivities at 6 months ranging from 33 to 98% for commercial assays. Thus, the ability to detect previous infection by SARS-CoV-2 is highly dependent on infection severity, timing, and the assay used. These findings have important implications for the design and interpretation of SARS-CoV-2 serosurveillance studies.

Published

2021

7. Everolimus, an mTORC1/2 inhibitor, in ART‐suppressed individuals who received solid organ transplantation: A prospective study

Author

Henrich, Timothy J, Schreiner, Corinna, Cameron, Cheryl, Hogan, Louise E, Richardson, Brian, Rutishauser, Rachel L, Deitchman, Amelia N, Chu, Simon, Rogers, Rodney, Thanh, Cassandra, Gibson, Erica A, Zarinsefat, Arya, Bakkour, Sonia, Aweeka, Francesca, Busch, Michael P, Liegler, Teri, Baker, Christopher, Milush, Jeffrey, Deeks, Steven G, and Stock, Peter G

Subjects

Medical Microbiology, Biomedical and Clinical Sciences, Clinical Sciences, Immunology, Clinical Trials and Supportive Activities, Sexually Transmitted Infections, Genetics, Infectious Diseases, Transplantation, Organ Transplantation, HIV/AIDS, Clinical Research, 6.1 Pharmaceuticals, Adult, Everolimus, Humans, Immunosuppressive Agents, Mechanistic Target of Rapamycin Complex 1, Pharmaceutical Preparations, Prospective Studies, clinical research/practice, immunosuppressant - mechanistic target of rapamycin: everolimus, immunosuppression/immune modulation, infection and infectious agents - viral: human immunodeficiency virus (HIV)/acquired immunodeficiency syndrome, infectious disease, organ transplantation in general, translational research/science, Medical and Health Sciences, Surgery, Clinical sciences

Abstract

Pharmacologic inhibition of the mammalian target of rapamycin (mTOR) in the setting of renal transplantation has previously been associated with lower human immunodeficiency virus 1 (HIV-1) DNA burden, and in vitro studies suggest that mTOR inhibition may lead to HIV transcriptional silencing. Because prospective clinical trials are lacking, we conducted an open-label, single-arm study to determine the impact of the broad mTOR inhibitor, everolimus, on residual HIV burden, transcriptional gene expression profiles, and immune responses in HIV-infected adult solid organ transplant (SOT) recipients on antiretroviral therapy. Whereas everolimus therapy did not have an overall effect on cell-associated HIV-1 DNA and RNA levels in the entire cohort, participants who maintained everolimus time-averaged trough levels >5 ng/mL during the first 2 months of therapy had significantly lower RNA levels up to 6 months after the cessation of study drug. Time-averaged everolimus trough levels significantly correlated with greater inhibition of mTOR gene pathway transcriptional activity. Everolimus treatment also led to decreased PD-1 expression on certain T cell subsets. These data support the rationale for further study of the effects of mTOR inhibition on HIV transcriptional silencing in non-SOT populations, either alone or in combination with other strategies. Trial Registration: ClinicalTrials.gov NCT02429869.

Published

2021

8. Circulating CD30+CD4+ T Cells Increase Before Human Immunodeficiency Virus Rebound After Analytical Antiretroviral Treatment Interruption

Author

Prator, Cecilia A, Thanh, Cassandra, Kumar, Shreya, Pan, Tony, Peluso, Michael J, Bosch, Ronald, Jones, Norman, Milush, Jeffrey M, Bakkour, Sonia, Stone, Mars, Busch, Michael P, Deeks, Steven G, Hunt, Peter W, and Henrich, Timothy J

Subjects

Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Genetics, Sexually Transmitted Infections, Clinical Research, Infectious Diseases, HIV/AIDS, Infection, Anti-Retroviral Agents, Biomarkers, CD4 Lymphocyte Count, CD4-Positive T-Lymphocytes, Cells, Cultured, HIV Infections, Humans, Ki-1 Antigen, Leukocytes, Mononuclear, Longitudinal Studies, RNA, Viral, Viral Load, Viremia, Withholding Treatment, analytical treatment interruption, CD30, HIV biomarkers, HIV-1 persistence, monitored antiretroviral pause, Biological Sciences, Medical and Health Sciences, Microbiology, Biological sciences, Biomedical and clinical sciences, Health sciences

Abstract

BackgroundIdentification of nonviral markers of human immunodeficiency virus (HIV) infection that increase before viral rebound during analytical treatment interruption (ATI) may affect HIV persistence research. We previously showed that HIV ribonucleic acid (RNA) is enriched in CD30+CD4+ T cells in many individuals. Here, we studied CD30+CD4+ T-cell dynamics before ATI, during ATI (before detectable plasma RNA), and after HIV rebound.MethodsPeripheral blood mononuclear cells from 23 participants collected longitudinally from 5 Adult AIDS Clinical Trials Group studies incorporating ATI were included in this study. Flow cytometric characterization of expression of CD30 and markers of T-cell activation and exhaustion were performed along with HIV-1 RNA and deoxyribonucleic acid quantification and measurement of soluble plasma CD30 and CD30 ligand.ResultsThe percentage of CD4+ T cells expressing CD30 significantly increased from pre-ATI to postinterruption time points before detectible viremia (1.65 mean relative increase, P = .005). Seventy-seven percent of participants experienced an increase in CD30+ cells before viral rebound. In contrast, there were no significant differences between pre-ATI and postinterruption pre-rebound time points in percentages of lymphocytes expressing CD69, CD38/HLA-DR, or PD-1 until after HIV recrudescence.ConclusionsCD30 may be a surrogate marker of early replication or viral transcriptional activity before detection by routine peripheral blood sampling.

Published

2020

9. Cerebrospinal fluid soluble CD30 elevation despite suppressive antiretroviral therapy in individuals living with HIV-1.

Author

Peluso, Michael J, Thanh, Cassandra, Prator, Cecilia A, Hogan, Louise E, Arechiga, Victor M, Stephenson, Sophie, Norris, Philip J, Di Germanio, Clara, Fuchs, Dietmar, Zetterberg, Henrik, Deeks, Steven G, Gisslén, Magnus, Price, Richard W, and Henrich, Timothy J

Subjects

CD30, HIV-1, central nervous system, cerebrospinal fluid, reservoir

Abstract

ObjectivesThe aim of this study was to assess soluble CD30 (sCD30), a protein that colocalises with HIV-1 RNA and DNA in lymphoid cells and tissues, in cerebrospinal fluid (CSF) as a marker of HIV-1 infection in the central nervous system (CNS).MethodsThis was a cross-sectional study using archived samples from two clinical cohorts. Soluble CD30 concentrations were measured in paired CSF and plasma from untreated viraemic individuals (n=52), individuals on suppressive antiretroviral therapy (ART) (n=33), HIV-1 controllers (n=10), participants with CSF HIV-1 'escape' (n=11) and controls without HIV-1 infection (n=16). Nonparametric tests were used to compare levels across groups and evaluate correlations with HIV-1 RNA, CSF neurofilament light chain protein (NFL) and neopterin.ResultsCompared with controls (median 30 ng/mL, interquartile range [IRQ] 23-50), plasma sCD30 levels were elevated in viraemic participants (75 ng/mL, 52-116; P

Published

2020

10. Correction to: Rapid development of HIV elite control in a patient with acute infection

Author

Morley, Deirdre, Lambert, John S, Hogan, Louise E, De Gascun, Cillian, Redmond, Niamh, Rutishauser, Rachel L, Thanh, Cassandra, Gibson, Erica A, Hobbs, Kristen, Bakkour, Sonia, Busch, Michael P, Farrell, Jeremy, McGetrick, Padraig, and Henrich, Timothy J

Subjects

Medical Microbiology, Biomedical and Clinical Sciences, Infectious Diseases, Sexually Transmitted Infections, HIV/AIDS, Microbiology, Clinical Sciences, Clinical sciences, Medical microbiology, Public health

Abstract

After publication of the original article [1], we were notified in Table 1 a column should be removed.

Published

2019

11. Rapid development of HIV elite control in a patient with acute infection

Author

Morley, Deirdre, Lambert, John S, Hogan, Louise E, De Gascun, Cillian, Redmond, Niamh, Rutishauser, Rachel L, Thanh, Cassandra, Gibson, Erica A, Hobbs, Kristen, Bakkour, Sonia, Busch, Michael P, Farrell, Jeremy, McGetrick, Padraig, and Henrich, Timothy J

Subjects

Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Sexually Transmitted Infections, Clinical Research, Infectious Diseases, HIV/AIDS, Detection, screening and diagnosis, 4.1 Discovery and preclinical testing of markers and technologies, Infection, Adult, Anti-Retroviral Agents, CD4 Lymphocyte Count, CD8-Positive T-Lymphocytes, Female, HIV Antibodies, HIV Infections, HIV-1, Humans, RNA, Viral, Viral Load, Elite control, Acute HIV infection, Antiretroviral therapy, HIV immune responses, HIV reservoirs, Microbiology, Clinical Sciences, Clinical sciences, Medical microbiology, Public health

Abstract

BackgroundElite controllers (EC), a small subset of the HIV-positive population (

Published

2019

12. Transient loss of detectable HIV-1 RNA following brentuximab vedotin anti-CD30 therapy for Hodgkin lymphoma

Author

Wang, Chia-Ching, Thanh, Cassandra, Gibson, Erica A, Ball-Burack, Maya, Hogan, Louise E, Descours, Benjamin, Jones, Norman, Carvidi, Alexander B, Munter, Sadie, Bakkour, Sonia, Busch, Michael P, Milush, Jeffrey M, Deeks, Steven G, and Henrich, Timothy J

Subjects

Biomedical and Clinical Sciences, Cardiovascular Medicine and Haematology, Immunology, Medical Microbiology, Oncology and Carcinogenesis, Hodgkin's Disease, HIV/AIDS, Lymphatic Research, Hematology, Sexually Transmitted Infections, Lymphoma, Infectious Diseases, Cancer, Rare Diseases, Infection, Adult, Anti-Retroviral Agents, Brentuximab Vedotin, CD4-Positive T-Lymphocytes, CD8-Positive T-Lymphocytes, HIV Infections, HIV-1, Hodgkin Disease, Humans, Immunoconjugates, Immunophenotyping, Ki-1 Antigen, Male, RNA, Viral, Cardiovascular medicine and haematology

Abstract

Anti-CD30 therapy for Hodgkin lymphoma led to transient loss of detectable CD4+ T-cell HIV RNA and a decrease in residual plasma viremia. Targeting nonviral markers expressed on HIV-1 transcriptionally active cells may lead to reduced measures of HIV-1 persistence.

Published

2018

13. Elucidating the Burden of HIV in Tissues Using Multiplexed Immunofluorescence and In Situ Hybridization: Methods for the Single-Cell Phenotypic Characterization of Cells Harboring HIV In Situ

Author

Vasquez, Joshua J, Hussien, Rajaa, Aguilar-Rodriguez, Brandon, Junger, Henrik, Dobi, Dejan, Henrich, Timothy J, Thanh, Cassandra, Gibson, Erica, Hogan, Louise E, McCune, Joseph, Hunt, Peter W, Stoddart, Cheryl A, and Laszik, Zoltan G

Subjects

Biochemistry and Cell Biology, Medicinal and Biomolecular Chemistry, Chemical Sciences, Biological Sciences, Biotechnology, Infectious Diseases, Sexually Transmitted Infections, HIV/AIDS, Genetics, Infection, DNA, Viral, Fluorescent Antibody Technique, HIV, HIV Infections, Humans, In Situ Hybridization, Paraffin Embedding, RNA, Viral, Single-Cell Analysis, Tissue Fixation, Viral Load, HIV reservoir, quantitative image analysis, tissue fixation, Medical and Health Sciences, Biochemistry & Molecular Biology, Biochemistry and cell biology, Medicinal and biomolecular chemistry

Abstract

Persistent tissue reservoirs of HIV present a major barrier to cure. Defining subsets of infected cells in tissues is a major focus of HIV cure research. Herein, we describe a novel multiplexed in situ hybridization (ISH) (RNAscope) protocol to detect HIV-DNA (vDNA) and HIV-RNA (vRNA) in formalin-fixed paraffin-embedded (FFPE) human tissues in combination with immunofluorescence (IF) phenotyping of the infected cells. We show that multiplexed IF and ISH (mIFISH) is suitable for quantitative assessment of HIV vRNA and vDNA and that multiparameter IF phenotyping allows precise identification of the cellular source of the ISH signal. We also provide semi-quantitative data on the impact of various tissue fixatives on the detectability of vDNA and vRNA with RNAscope technology. Finally, we describe methods to quantitate the ISH signal on whole-slide digital images and validation of the quantitative ISH data with quantitative real-time PCR for vRNA. It is our hope that this approach will provide insight into the biology of HIV tissue reservoirs and to inform strategies aimed at curing HIV.

Published

2018

14. Increased HIV-1 transcriptional activity and infectious burden in peripheral blood and gut-associated CD4+ T cells expressing CD30.

Author

Hogan, Louise E, Vasquez, Joshua, Hobbs, Kristen S, Hanhauser, Emily, Aguilar-Rodriguez, Brandon, Hussien, Rajaa, Thanh, Cassandra, Gibson, Erica A, Carvidi, Alexander B, Smith, Louis CB, Khan, Shahzada, Trapecar, Martin, Sanjabi, Shomyseh, Somsouk, Ma, Stoddart, Cheryl A, Kuritzkes, Daniel R, Deeks, Steven G, and Henrich, Timothy J

Subjects

Rectum, Lymphoid Tissue, CD4-Positive T-Lymphocytes, Cells, Cultured, Humans, HIV-1, HIV Infections, DNA, Viral, RNA, Viral, Immunoconjugates, Anti-HIV Agents, CD4 Lymphocyte Count, Antiretroviral Therapy, Highly Active, In Situ Hybridization, Viral Load, Cohort Studies, Solubility, Transcriptional Activation, Biomarkers, Ki-1 Antigen, Brentuximab Vedotin, Microbiology, Immunology, Medical Microbiology, Virology

Abstract

HIV-1-infected cells persist indefinitely despite the use of combination antiretroviral therapy (ART), and novel therapeutic strategies to target and purge residual infected cells in individuals on ART are urgently needed. Here, we demonstrate that CD4+ T cell-associated HIV-1 RNA is often highly enriched in cells expressing CD30, and that cells expressing this marker considerably contribute to the total pool of transcriptionally active CD4+ lymphocytes in individuals on suppressive ART. Using in situ RNA hybridization studies, we show co-localization of CD30 with HIV-1 transcriptional activity in gut-associated lymphoid tissues. We also demonstrate that ex vivo treatment with brentuximab vedotin, an antibody-drug conjugate (ADC) that targets CD30, significantly reduces the total amount of HIV-1 DNA in peripheral blood mononuclear cells obtained from infected, ART-suppressed individuals. Finally, we observed that an HIV-1-infected individual, who received repeated brentuximab vedotin infusions for lymphoma, had no detectable virus in peripheral blood mononuclear cells. Overall, CD30 may be a marker of residual, transcriptionally active HIV-1 infected cells in the setting of suppressive ART. Given that CD30 is only expressed on a small number of total mononuclear cells, it is a potential therapeutic target of persistent HIV-1 infection.

Published

2018

15. HIV-1 persistence following extremely early initiation of antiretroviral therapy (ART) during acute HIV-1 infection: An observational study.

Author

Henrich, Timothy J, Hatano, Hiroyu, Bacon, Oliver, Hogan, Louise E, Rutishauser, Rachel, Hill, Alison, Kearney, Mary F, Anderson, Elizabeth M, Buchbinder, Susan P, Cohen, Stephanie E, Abdel-Mohsen, Mohamed, Pohlmeyer, Christopher W, Fromentin, Remi, Hoh, Rebecca, Liu, Albert Y, McCune, Joseph M, Spindler, Jonathan, Metcalf-Pate, Kelly, Hobbs, Kristen S, Thanh, Cassandra, Gibson, Erica A, Kuritzkes, Daniel R, Siliciano, Robert F, Price, Richard W, Richman, Douglas D, Chomont, Nicolas, Siliciano, Janet D, Mellors, John W, Yukl, Steven A, Blankson, Joel N, Liegler, Teri, and Deeks, Steven G

Subjects

Humans, HIV-1, HIV Infections, Recurrence, Anti-Retroviral Agents, Treatment Outcome, Flow Cytometry, Prospective Studies, Phenotype, Adult, Middle Aged, Male, Secondary Prevention, Biomarkers, HIV/AIDS, Genetics, Infectious Diseases, Clinical Research, 2.1 Biological and endogenous factors, Infection, General & Internal Medicine, Medical and Health Sciences

Abstract

BackgroundIt is unknown if extremely early initiation of antiretroviral therapy (ART) may lead to long-term ART-free HIV remission or cure. As a result, we studied 2 individuals recruited from a pre-exposure prophylaxis (PrEP) program who started prophylactic ART an estimated 10 days (Participant A; 54-year-old male) and 12 days (Participant B; 31-year-old male) after infection with peak plasma HIV RNA of 220 copies/mL and 3,343 copies/mL, respectively. Extensive testing of blood and tissue for HIV persistence was performed, and PrEP Participant A underwent analytical treatment interruption (ATI) following 32 weeks of continuous ART.Methods and findingsColorectal and lymph node tissues, bone marrow, cerebral spinal fluid (CSF), plasma, and very large numbers of peripheral blood mononuclear cells (PBMCs) were obtained longitudinally from both participants and were studied for HIV persistence in several laboratories using molecular and culture-based detection methods, including a murine viral outgrowth assay (mVOA). Both participants initiated PrEP with tenofovir/emtricitabine during very early Fiebig stage I (detectable plasma HIV-1 RNA, antibody negative) followed by 4-drug ART intensification. Following peak viral loads, both participants experienced full suppression of HIV-1 plasma viremia. Over the following 2 years, no further HIV could be detected in blood or tissue from PrEP Participant A despite extensive sampling from ileum, rectum, lymph nodes, bone marrow, CSF, circulating CD4+ T cell subsets, and plasma. No HIV was detected from tissues obtained from PrEP Participant B, but low-level HIV RNA or DNA was intermittently detected from various CD4+ T cell subsets. Over 500 million CD4+ T cells were assayed from both participants in a humanized mouse outgrowth assay. Three of 8 mice infused with CD4+ T cells from PrEP Participant B developed viremia (50 million input cells/surviving mouse), but only 1 of 10 mice infused with CD4+ T cells from PrEP Participant A (53 million input cells/mouse) experienced very low level viremia (201 copies/mL); sequence confirmation was unsuccessful. PrEP Participant A stopped ART and remained aviremic for 7.4 months, rebounding with HIV RNA of 36 copies/mL that rose to 59,805 copies/mL 6 days later. ART was restarted promptly. Rebound plasma HIV sequences were identical to those obtained during acute infection by single-genome sequencing. Mathematical modeling predicted that the latent reservoir size was approximately 200 cells prior to ATI and that only around 1% of individuals with a similar HIV burden may achieve lifelong ART-free remission. Furthermore, we observed that lymphocytes expressing the tumor marker CD30 increased in frequency weeks to months prior to detectable HIV-1 RNA in plasma. This study was limited by the small sample size, which was a result of the rarity of individuals presenting during hyperacute infection.ConclusionsWe report HIV relapse despite initiation of ART at one of the earliest stages of acute HIV infection possible. Near complete or complete loss of detectable HIV in blood and tissues did not lead to indefinite ART-free HIV remission. However, the small numbers of latently infected cells in individuals treated during hyperacute infection may be associated with prolonged ART-free remission.

Published

2017

16. High-throughput Characterization of HIV-1 Reservoir Reactivation Using a Single-Cell-in-Droplet PCR Assay

Author

Yucha, Robert W, Hobbs, Kristen S, Hanhauser, Emily, Hogan, Louise E, Nieves, Wildaliz, Ozen, Mehmet O, Inci, Fatih, York, Vanessa, Gibson, Erica A, Thanh, Cassandra, Shafiee, Hadi, Assal, Rami El, Kiselinova, Maja, Robles, Yvonne P, Bae, Helen, Leadabrand, Kaitlyn S, Wang, ShuQi, Deeks, Steven G, Kuritzkes, Daniel R, Demirci, Utkan, and Henrich, Timothy J

Subjects

Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Infectious Diseases, Clinical Research, HIV/AIDS, Genetics, Biotechnology, Sexually Transmitted Infections, Infection, Adult, CD4-Positive T-Lymphocytes, Cells, Cultured, HIV Infections, HIV-1, High-Throughput Screening Assays, Humans, Middle Aged, Polymerase Chain Reaction, RNA, Viral, Sequence Analysis, DNA, Single-Cell Analysis, Viral Load, Virus Activation, Virus Latency, Human Immunodeficiency Virus, Single cell quantification, Digital PCR, HIV reservoirs, HIV reactivation, Histone deacetylase inhibitors, Clinical Sciences, Public Health and Health Services, Clinical sciences, Epidemiology

Abstract

Reactivation of latent viral reservoirs is on the forefront of HIV-1 eradication research. However, it is unknown if latency reversing agents (LRAs) increase the level of viral transcription from cells producing HIV RNA or harboring transcriptionally-inactive (latent) infection. We therefore developed a microfluidic single-cell-in-droplet (scd)PCR assay to directly measure the number of CD4+ T cells that produce unspliced (us)RNA and multiply spliced (ms)RNA following ex vivo latency reversal with either an histone deacetylase inhibitor (romidepsin) or T cell receptor (TCR) stimulation. Detection of HIV-1 transcriptional activity can also be performed on hundreds of thousands of CD4+ T-cells in a single experiment. The scdPCR method was then applied to CD4+ T cells obtained from HIV-1-infected individuals on antiretroviral therapy. Overall, our results suggest that effects of LRAs on HIV-1 reactivation may be heterogeneous-increasing transcription from active cells in some cases and increasing the number of transcriptionally active cells in others. Genomic DNA and human mRNA isolated from HIV-1 reactivated cells could also be detected and quantified from individual cells. As a result, our assay has the potential to provide needed insight into various reservoir eradication strategies.

Published

2017

17. Differences in expression of tumor suppressor, innate immune, inflammasome, and potassium/gap junction channel host genes significantly predict viral reservoir size during treated HIV infection

Author

Dwivedi, Ashok K., primary, Siegel, David A., additional, Thanh, Cassandra, additional, Hoh, Rebecca, additional, Hobbs, Kristen S., additional, Pan, Tony, additional, Gibson, Erica A., additional, Martin, Jeffrey, additional, Hecht, Frederick, additional, Pilcher, Christopher, additional, Milush, Jeffrey, additional, Busch, Michael P., additional, Stone, Mars, additional, Huang, Meei-Li, additional, Levy, Claire N., additional, Roychoudhury, Pavitra, additional, Hladik, Florian, additional, Jerome, Keith R., additional, Henrich, Timothy J., additional, Deeks, Steven G., additional, and Lee, Sulggi A., additional

Published

2023

18. Host variation in type I interferon signaling genes (MX1), C–C chemokine receptor type 5 gene, and major histocompatibility complex class I alleles in treated HIV+ noncontrollers predict viral reservoir size

Author

Siegel, David A., primary, Thanh, Cassandra, additional, Wan, Eunice, additional, Hoh, Rebecca, additional, Hobbs, Kristen, additional, Pan, Tony, additional, Gibson, Erica A., additional, Kroetz, Deanna L., additional, Martin, Jeffrey, additional, Hecht, Frederick, additional, Pilcher, Christopher, additional, Martin, Maureen, additional, Carrington, Mary, additional, Pillai, Satish, additional, Busch, Michael P., additional, Stone, Mars, additional, Levy, Claire N., additional, Huang, Meei-Li, additional, Roychoudhury, Pavitra, additional, Hladik, Florian, additional, Jerome, Keith R., additional, Kiem, Hans-Peter, additional, Henrich, Timothy J., additional, Deeks, Steven G., additional, and Lee, Sulggi A., additional

Published

2022

19. Host variation in type I interferon signaling genes (MX1),CCR5Δ32, and MHC class I alleles in treated HIV+ non-controllers predict viral reservoir size

Author

Siegel, David A., primary, Thanh, Cassandra, additional, Wan, Eunice, additional, Hoh, Rebecca, additional, Hobbs, Kristen, additional, Pan, Tony, additional, Gibson, Erica A., additional, Kroetz, Deanna L., additional, Hunt, Peter W., additional, Martin, Jeffrey, additional, Hecht, Frederick, additional, Pilcher, Christopher, additional, Milush, Jeffrey, additional, Martin, Maureen, additional, Carrington, Mary, additional, Pillai, Satish, additional, Busch, Michael P., additional, Stone, Mars, additional, Levy, Claire N., additional, Huang, Meei-Li, additional, Roychoudhury, Pavitra, additional, Hladik, Florian, additional, Jerome, Keith R., additional, Kiem, Hans-Peter, additional, Henrich, Timothy J., additional, Deeks, Steven G., additional, and Lee, Sulggi, additional

Published

2021

20. First-in-human immunoPET imaging of HIV-1 infection using 89Zr-labeled VRC01 broadly neutralizing antibody.

Author

Beckford-Vera, Denis R., Flavell, Robert R., Seo, Youngho, Martinez-Ortiz, Enrique, Aslam, Maya, Thanh, Cassandra, Fehrman, Emily, Pardons, Marion, Kumar, Shreya, Deitchman, Amelia N., Ravanfar, Vahid, Schulte, Brailee, Wu, I-Wei Katherine, Pan, Tony, Reeves, Jacqueline D., Nixon, Christopher C., Iyer, Nikita S., Torres, Leonel, Munter, Sadie E., and Hyunh, Tony

Subjects

MONOCLONAL antibodies, HIV infections, POSITRON emission tomography, HIV, CD4 antigen, LYMPH nodes

Abstract

A major obstacle to achieving long-term antiretroviral (ART) free remission or functional cure of HIV infection is the presence of persistently infected cells that establish a long-lived viral reservoir. HIV largely resides in anatomical regions that are inaccessible to routine sampling, however, and non-invasive methods to understand the longitudinal tissue-wide burden of HIV persistence are urgently needed. Positron emission tomography (PET) imaging is a promising strategy to identify and characterize the tissue-wide burden of HIV. Here, we assess the efficacy of using immunoPET imaging to characterize HIV reservoirs and identify anatomical foci of persistent viral transcriptional activity using a radiolabeled HIV Env-specific broadly neutralizing antibody, 89Zr-VRC01, in HIV-infected individuals with detectable viremia and on suppressive ART compared to uninfected controls (NCT03729752). We also assess the relationship between PET tracer uptake in tissues and timing of ART initiation and direct HIV protein expression in CD4 T cells obtained from lymph node biopsies. We observe significant increases in 89Zr-VRC01 uptake in various tissues (including lymph nodes and gut) in HIV-infected individuals with detectable viremia (N = 5) and on suppressive ART (N = 5) compared to uninfected controls (N = 5). Importantly, PET tracer uptake in inguinal lymph nodes in viremic and ART-suppressed participants significantly and positively correlates with HIV protein expression measured directly in tissue. Our strategy may allow non-invasive longitudinal characterization of residual HIV infection and lays the framework for the development of immunoPET imaging in a variety of other infectious diseases. Here, the authors apply positron emission tomography (PET) imaging to visualize HIV tissue-wide burden in infected individuals using a radiolabeled broadly neutralizing antibody, 89Zr-VRC01, and show that PET tracer lymph node uptake positively correlates with HIV protein levels measured directly from cells obtained from these tissues. This strategy may allow non-invasive characterization of residual HIV infection in the setting of therapeutic interventions. [ABSTRACT FROM AUTHOR]

Published

2022

21. SARS-CoV-2 antibody magnitude and detectability are driven by disease severity, timing, and assay

Author

Peluso, Michael J., primary, Takahashi, Saki, additional, Hakim, Jill, additional, Kelly, J. Daniel, additional, Torres, Leonel, additional, Iyer, Nikita S., additional, Turcios, Keirstinne, additional, Janson, Owen, additional, Munter, Sadie E., additional, Thanh, Cassandra, additional, Nixon, Christopher C., additional, Hoh, Rebecca, additional, Tai, Viva, additional, Fehrman, Emily A., additional, Hernandez, Yanel, additional, Spinelli, Matthew A., additional, Gandhi, Monica, additional, Palafox, Mary-Ann, additional, Vallari, Ana, additional, Rodgers, Mary A., additional, Prostko, John, additional, Hackett, John, additional, Trinh, Lan, additional, Wrin, Terri, additional, Petroplolous, Christos J., additional, Chiu, Charles Y., additional, Norris, Philip J., additional, DiGermanio, Clara, additional, Stone, Mars, additional, Busch, Michael P., additional, Elledge, Susanna K., additional, Zhou, Xin X., additional, Wells, James A., additional, Shu, Albert, additional, Kurtz, Theodore W., additional, Pak, John E., additional, Wu, Wesley, additional, Burbelo, Peter D., additional, Cohen, Jeffrey I., additional, Rutishauser, Rachel L., additional, Martin, Jeffrey N., additional, Deeks, Steven G., additional, Henrich, Timothy J., additional, Rodriguez-Barraquer, Isabel, additional, and Greenhouse, Bryan, additional

Published

2021

22. Long-Term SARS-CoV-2-Specific Immune and Inflammatory Responses Across a Clinically Diverse Cohort of Individuals Recovering from COVID-19

Author

Peluso, Michael J., primary, Deitchman, Amelia N., additional, Torres, Leonel, additional, Iyer, Nikita S., additional, Nixon, Christopher C., additional, Munter, Sadie E., additional, Donatelli, Joanna, additional, Thanh, Cassandra, additional, Takahashi, Saki, additional, Hakim, Jill, additional, Turcios, Keirstinne, additional, Janson, Owen, additional, Hoh, Rebecca, additional, Tai, Viva, additional, Hernandez, Yanel, additional, Fehrman, Emily, additional, Spinelli, Matthew A., additional, Gandhi, Monica, additional, Trinh, Lan, additional, Wrin, Terri, additional, Petropoulos, Christos J., additional, Aweeka, Francesca T., additional, Rodriguez-Barraquer, Isabel, additional, Kelly, J. Daniel, additional, Martin, Jeffrey N., additional, Deeks, Steven G., additional, Greenhouse, Bryan, additional, Rutishauser, Rachel L., additional, and Henrich, Timothy J., additional

Published

2021

23. Biosensing: Tunable Fano‐Resonant Metasurfaces on a Disposable Plastic‐Template for Multimodal and Multiplex Biosensing (Adv. Mater. 19/2020)

Author

Ahmed, Rajib, primary, Ozen, Mehmet Ozgun, additional, Karaaslan, Merve Goksin, additional, Prator, Cecilia A., additional, Thanh, Cassandra, additional, Kumar, Shreya, additional, Torres, Leonel, additional, Iyer, Nikita, additional, Munter, Sadie, additional, Southern, Sarka, additional, Henrich, Timothy J., additional, Inci, Fatih, additional, and Demirci, Utkan, additional

Published

2020

24. Tunable Fano‐Resonant Metasurfaces on a Disposable Plastic‐Template for Multimodal and Multiplex Biosensing

Author

Ahmed, Rajib, primary, Ozen, Mehmet Ozgun, additional, Karaaslan, Merve Goksin, additional, Prator, Cecilia A., additional, Thanh, Cassandra, additional, Kumar, Shreya, additional, Torres, Leonel, additional, Iyer, Nikita, additional, Munter, Sadie, additional, Southern, Sarka, additional, Henrich, Timothy J., additional, Inci, Fatih, additional, and Demirci, Utkan, additional

Published

2020

25. Circulating CD30+CD4+ T Cells Increase Before Human Immunodeficiency Virus Rebound After Analytical Antiretroviral Treatment Interruption

Author

Prator, Cecilia A, primary, Thanh, Cassandra, primary, Kumar, Shreya, primary, Pan, Tony, primary, Peluso, Michael J, primary, Bosch, Ronald, primary, Jones, Norman, primary, Milush, Jeffrey M, primary, Bakkour, Sonia, primary, Stone, Mars, primary, Busch, Michael P, primary, Deeks, Steven G, primary, Hunt, Peter W, primary, and Henrich, Timothy J, primary

Published

2019

26. Circulating CD30+CD4+ T Cells Increase Before Human Immunodeficiency Virus Rebound After Analytical Antiretroviral Treatment Interruption.

Author

Prator, Cecilia A, Thanh, Cassandra, Kumar, Shreya, Pan, Tony, Peluso, Michael J, Bosch, Ronald, Jones, Norman, Milush, Jeffrey M, Bakkour, Sonia, Stone, Mars, Busch, Michael P, Deeks, Steven G, Hunt, Peter W, and Henrich, Timothy J

Subjects

*HIV, *T cells, *DNA, *RNA, *BIOMARKERS

Abstract

Background Identification of nonviral markers of human immunodeficiency virus (HIV) infection that increase before viral rebound during analytical treatment interruption (ATI) may affect HIV persistence research. We previously showed that HIV ribonucleic acid (RNA) is enriched in CD30+CD4+ T cells in many individuals. Here, we studied CD30+CD4+ T-cell dynamics before ATI, during ATI (before detectable plasma RNA), and after HIV rebound. Methods Peripheral blood mononuclear cells from 23 participants collected longitudinally from 5 Adult AIDS Clinical Trials Group studies incorporating ATI were included in this study. Flow cytometric characterization of expression of CD30 and markers of T-cell activation and exhaustion were performed along with HIV-1 RNA and deoxyribonucleic acid quantification and measurement of soluble plasma CD30 and CD30 ligand. Results The percentage of CD4+ T cells expressing CD30 significantly increased from pre-ATI to postinterruption time points before detectible viremia (1.65 mean relative increase, P =.005). Seventy-seven percent of participants experienced an increase in CD30+ cells before viral rebound. In contrast, there were no significant differences between pre-ATI and postinterruption pre-rebound time points in percentages of lymphocytes expressing CD69, CD38/HLA-DR, or PD-1 until after HIV recrudescence. Conclusions CD30 may be a surrogate marker of early replication or viral transcriptional activity before detection by routine peripheral blood sampling. [ABSTRACT FROM AUTHOR]

Published

2020

27. NK-cell activation is associated with increased HIV transcriptional activity following allogeneic hematopoietic cell transplantation

Author

Hogan, Louise E., primary, Körner, Christian, additional, Hobbs, Kristen, additional, Simoneau, Camille R., additional, Thanh, Cassandra, additional, Gibson, Erica A., additional, Palmer, Christine D., additional, Pandit, Alisha, additional, Marty, Francisco M., additional, Kuritzkes, Daniel R., additional, Jost, Stephanie, additional, Ritz, Jerome, additional, and Henrich, Timothy J., additional

Published

2018

28. High-throughput Characterization of HIV-1 Reservoir Reactivation Using a Single-Cell-in-Droplet PCR Assay

Author

Yucha, Robert W., primary, Hobbs, Kristen S., additional, Hanhauser, Emily, additional, Hogan, Louise E., additional, Nieves, Wildaliz, additional, Ozen, Mehmet O., additional, Inci, Fatih, additional, York, Vanessa, additional, Gibson, Erica A., additional, Thanh, Cassandra, additional, Shafiee, Hadi, additional, El Assal, Rami, additional, Kiselinova, Maja, additional, Robles, Yvonne P., additional, Bae, Helen, additional, Leadabrand, Kaitlyn S., additional, Wang, ShuQi, additional, Deeks, Steven G., additional, Kuritzkes, Daniel R., additional, Demirci, Utkan, additional, and Henrich, Timothy J., additional

Published

2017

29. Increased HIV-1 transcriptional activity and infectious burden in peripheral blood and gut-associated CD4+ T cells expressing CD30.

Author

Hogan, Louise E., Vasquez, Joshua, Hobbs, Kristen S., Hanhauser, Emily, Aguilar-Rodriguez, Brandon, Hussien, Rajaa, Thanh, Cassandra, Gibson, Erica A., Carvidi, Alexander B., Smith, Louis C. B., Khan, Shahzada, Trapecar, Martin, Sanjabi, Shomyseh, Somsouk, Ma, Stoddart, Cheryl A., Kuritzkes, Daniel R., Deeks, Steven G., and Henrich, Timothy J.

Subjects

HIV, HIGHLY active antiretroviral therapy, T cells, CD4 antigen, LYMPHOID tissue

Abstract

HIV-1-infected cells persist indefinitely despite the use of combination antiretroviral therapy (ART), and novel therapeutic strategies to target and purge residual infected cells in individuals on ART are urgently needed. Here, we demonstrate that CD4+ T cell-associated HIV-1 RNA is often highly enriched in cells expressing CD30, and that cells expressing this marker considerably contribute to the total pool of transcriptionally active CD4+ lymphocytes in individuals on suppressive ART. Using in situ RNA hybridization studies, we show co-localization of CD30 with HIV-1 transcriptional activity in gut-associated lymphoid tissues. We also demonstrate that ex vivo treatment with brentuximab vedotin, an antibody-drug conjugate (ADC) that targets CD30, significantly reduces the total amount of HIV-1 DNA in peripheral blood mononuclear cells obtained from infected, ART-suppressed individuals. Finally, we observed that an HIV-1-infected individual, who received repeated brentuximab vedotin infusions for lymphoma, had no detectable virus in peripheral blood mononuclear cells. Overall, CD30 may be a marker of residual, transcriptionally active HIV-1 infected cells in the setting of suppressive ART. Given that CD30 is only expressed on a small number of total mononuclear cells, it is a potential therapeutic target of persistent HIV-1 infection. [ABSTRACT FROM AUTHOR]

Published

2018

30. High-throughput Characterization of HIV-1 Reservoir Reactivation Using a Single-Cell-in-Droplet PCR Assay

Author

Yucha, Robert W., Hobbs, Kristen S., Hanhauser, Emily, Hogan, Louise E., Nieves, Wildaliz, Ozen, Mehmet O., Inci, Fatih, York, Vanessa, Gibson, Erica A., Thanh, Cassandra, Shafiee, Hadi, El Assal, Rami, Kiselinova, Maja, Robles, Yvonne P., Bae, Helen, Leadabrand, Kaitlyn S., Wang, ShuQi, Deeks, Steven G., Kuritzkes, Daniel R., Demirci, Utkan, and Henrich, Timothy J.

Subjects

Human Immunodeficiency Virus (HIV), Single cell quantification, Digital PCR, HIV reservoirs, HIV reactivation, Histone deacetylase inhibitors

Abstract

Reactivation of latent viral reservoirs is on the forefront of HIV-1 eradication research. However, it is unknown if latency reversing agents (LRAs) increase the level of viral transcription from cells producing HIV RNA or harboring transcriptionally-inactive (latent) infection. We therefore developed a microfluidic single-cell-in-droplet (scd)PCR assay to directly measure the number of CD4+ T cells that produce unspliced (us)RNA and multiply spliced (ms)RNA following ex vivo latency reversal with either an histone deacetylase inhibitor (romidepsin) or T cell receptor (TCR) stimulation. Detection of HIV-1 transcriptional activity can also be performed on hundreds of thousands of CD4 + T-cells in a single experiment. The scdPCR method was then applied to CD4+ T cells obtained from HIV-1-infected individuals on antiretroviral therapy. Overall, our results suggest that effects of LRAs on HIV-1 reactivation may be heterogeneous—increasing transcription from active cells in some cases and increasing the number of transcriptionally active cells in others. Genomic DNA and human mRNA isolated from HIV-1 reactivated cells could also be detected and quantified from individual cells. As a result, our assay has the potential to provide needed insight into various reservoir eradication strategies.

Published

2017

31. Differences in expression of tumor suppressor, innate immune, inflammasome, and potassium/gap junction channel host genes significantly predict viral reservoir size during treated HIV infection.

Author

Dwivedi AK, Siegel DA, Thanh C, Hoh R, Hobbs KS, Pan T, Gibson EA, Martin J, Hecht F, Pilcher C, Milush J, Busch MP, Stone M, Huang ML, Levy CN, Roychoudhury P, Hladik F, Jerome KR, Henrich TJ, Deeks SG, and Lee SA

Abstract

The major barrier to an HIV cure is the persistence of infected cells that evade host immune surveillance despite effective antiretroviral therapy (ART). Most prior host genetic HIV studies have focused on identifying DNA polymorphisms (e.g., CCR5Δ32 , MHC class I alleles) associated with viral load among untreated "elite controllers" (~1% of HIV+ individuals who are able to control virus without ART). However, there have been few studies evaluating host genetic predictors of viral control for the majority of people living with HIV (PLWH) on ART. We performed host RNA sequencing and HIV reservoir quantification (total DNA, unspliced RNA, intact DNA) from peripheral CD4+ T cells from 191 HIV+ ART-suppressed non-controllers. Multivariate models included covariates for timing of ART initiation, nadir CD4+ count, age, sex, and ancestry. Lower HIV total DNA (an estimate of the total reservoir) was associated with upregulation of tumor suppressor genes NBL1 (q=0.012) and P3H3 (q=0.012). Higher HIV unspliced RNA (an estimate of residual HIV transcription) was associated with downregulation of several host genes involving inflammasome ( IL1A, CSF3, TNFAIP5, TNFAIP6, TNFAIP9 , CXCL3, CXCL10 ) and innate immune ( TLR7 ) signaling, as well as novel associations with potassium ( KCNJ2 ) and gap junction ( GJB2 ) channels, all q<0.05. Gene set enrichment analyses identified significant associations with TLR4/microbial translocation (q=0.006), IL-1β/NRLP3 inflammasome (q=0.008), and IL-10 (q=0.037) signaling. HIV intact DNA (an estimate of the "replication-competent" reservoir) demonstrated trends with thrombin degradation ( PLGLB1 ) and glucose metabolism ( AGL ) genes, but data were (HIV intact DNA detected in only 42% of participants). Our findings demonstrate that among treated PLWH, that inflammation, innate immune responses, bacterial translocation, and tumor suppression/cell proliferation host signaling play a key role in the maintenance of the HIV reservoir during ART. Further data are needed to validate these findings, including functional genomic studies, and expanded epidemiologic studies in female, non-European cohorts., Author Summary: Although lifelong HIV antiretroviral therapy (ART) suppresses virus, the major barrier to an HIV cure is the persistence of infected cells that evade host immune surveillance despite effective ART, "the HIV reservoir." HIV eradication strategies have focused on eliminating residual virus to allow for HIV remission, but HIV cure trials to date have thus far failed to show a clinically meaningful reduction in the HIV reservoir. There is an urgent need for a better understanding of the host-viral dynamics during ART suppression to identify potential novel therapeutic targets for HIV cure. This is the first epidemiologic host gene expression study to demonstrate a significant link between HIV reservoir size and several well-known immunologic pathways (e.g., IL-1β, TLR7, TNF-α signaling pathways), as well as novel associations with potassium and gap junction channels (Kir2.1, connexin 26). Further data are needed to validate these findings, including functional genomic studies and expanded epidemiologic studies in female, non-European cohorts.

Published

2023

32. First-in-human immunoPET imaging of HIV-1 infection using 89 Zr-labeled VRC01 broadly neutralizing antibody.

Author

Beckford-Vera DR, Flavell RR, Seo Y, Martinez-Ortiz E, Aslam M, Thanh C, Fehrman E, Pardons M, Kumar S, Deitchman AN, Ravanfar V, Schulte B, Wu IK, Pan T, Reeves JD, Nixon CC, Iyer NS, Torres L, Munter SE, Hyunh T, Petropoulos CJ, Hoh R, Franc BL, Gama L, Koup RA, Mascola JR, Chomont N, Deeks SG, VanBrocklin HF, and Henrich TJ

Subjects

Antibodies, Neutralizing, Broadly Neutralizing Antibodies, CD4-Positive T-Lymphocytes, Humans, Positron-Emission Tomography, Viral Load, Viremia diagnostic imaging, HIV Infections diagnostic imaging, HIV-1

Abstract

A major obstacle to achieving long-term antiretroviral (ART) free remission or functional cure of HIV infection is the presence of persistently infected cells that establish a long-lived viral reservoir. HIV largely resides in anatomical regions that are inaccessible to routine sampling, however, and non-invasive methods to understand the longitudinal tissue-wide burden of HIV persistence are urgently needed. Positron emission tomography (PET) imaging is a promising strategy to identify and characterize the tissue-wide burden of HIV. Here, we assess the efficacy of using immunoPET imaging to characterize HIV reservoirs and identify anatomical foci of persistent viral transcriptional activity using a radiolabeled HIV Env-specific broadly neutralizing antibody, 89 Zr-VRC01, in HIV-infected individuals with detectable viremia and on suppressive ART compared to uninfected controls (NCT03729752). We also assess the relationship between PET tracer uptake in tissues and timing of ART initiation and direct HIV protein expression in CD4 T cells obtained from lymph node biopsies. We observe significant increases in 89 Zr-VRC01 uptake in various tissues (including lymph nodes and gut) in HIV-infected individuals with detectable viremia (N = 5) and on suppressive ART (N = 5) compared to uninfected controls (N = 5). Importantly, PET tracer uptake in inguinal lymph nodes in viremic and ART-suppressed participants significantly and positively correlates with HIV protein expression measured directly in tissue. Our strategy may allow non-invasive longitudinal characterization of residual HIV infection and lays the framework for the development of immunoPET imaging in a variety of other infectious diseases., (© 2022. The Author(s).)

Published

2022

33. SARS-CoV-2 antibody magnitude and detectability are driven by disease severity, timing, and assay.

Author

Peluso MJ, Takahashi S, Hakim J, Kelly JD, Torres L, Iyer NS, Turcios K, Janson O, Munter SE, Thanh C, Nixon CC, Hoh R, Tai V, Fehrman EA, Hernandez Y, Spinelli MA, Gandhi M, Palafox MA, Vallari A, Rodgers MA, Prostko J, Hackett J Jr, Trinh L, Wrin T, Petroplolous CJ, Chiu CY, Norris PJ, DiGermanio C, Stone M, Busch MP, Elledge SK, Zhou XX, Wells JA, Shu A, Kurtz TW, Pak JE, Wu W, Burbelo PD, Cohen JI, Rutishauser RL, Martin JN, Deeks SG, Henrich TJ, Rodriguez-Barraquer I, and Greenhouse B

Abstract

Serosurveillance studies are critical for estimating SARS-CoV-2 transmission and immunity, but interpretation of results is currently limited by poorly defined variability in the performance of antibody assays to detect seroreactivity over time in individuals with different clinical presentations. We measured longitudinal antibody responses to SARS-CoV-2 in plasma samples from a diverse cohort of 128 individuals over 160 days using 14 binding and neutralization assays. For all assays, we found a consistent and strong effect of disease severity on antibody magnitude, with fever, cough, hospitalization, and oxygen requirement explaining much of this variation. We found that binding assays measuring responses to spike protein had consistently higher correlation with neutralization than those measuring responses to nucleocapsid, regardless of assay format and sample timing. However, assays varied substantially with respect to sensitivity during early convalescence and in time to seroreversion. Variations in sensitivity and durability were particularly dramatic for individuals with mild infection, who had consistently lower antibody titers and represent the majority of the infected population, with sensitivities often differing substantially from reported test characteristics (e.g., amongst commercial assays, sensitivity at 6 months ranged from 33% for ARCHITECT IgG to 98% for VITROS Total Ig). Thus, the ability to detect previous infection by SARS-CoV-2 is highly dependent on the severity of the initial infection, timing relative to infection, and the assay used. These findings have important implications for the design and interpretation of SARS-CoV-2 serosurveillance studies.

Published

2021

34. Long-Term SARS-CoV-2-Specific Immune and Inflammatory Responses Across a Clinically Diverse Cohort of Individuals Recovering from COVID-19.

Author

Peluso MJ, Deitchman AN, Torres L, Iyer NS, Nixon CC, Munter SE, Donatelli J, Thanh C, Takahashi S, Hakim J, Turcios K, Janson O, Hoh R, Tai V, Hernandez Y, Fehrman E, Spinelli MA, Gandhi M, Trinh L, Wrin T, Petropoulos CJ, Aweeka FT, Rodriguez-Barraquer I, Kelly JD, Martin JN, Deeks SG, Greenhouse B, Rutishauser RL, and Henrich TJ

Abstract

A detailed understanding of long-term SARS-CoV-2-specific T cell responses and their relationship to humoral immunity and markers of inflammation in diverse groups of individuals representing the spectrum of COVID-19 illness and recovery is urgently needed. Data are also lacking as to whether and how adaptive immune and inflammatory responses differ in individuals that experience persistent symptomatic sequelae months following acute infection compared to those with complete, rapid recovery. We measured SARS-CoV-2-specific T cell responses, soluble markers of inflammation, and antibody levels and neutralization capacity longitudinally up to 9 months following infection in a diverse group of 70 individuals with PCR-confirmed SARS-CoV-2 infection. The participants had varying degrees of initial disease severity and were enrolled in the northern California Long-term Impact of Infection with Novel Coronavirus (LIINC) cohort. Adaptive T cell responses remained remarkably stable in all participants across disease severity during the entire study interval. Whereas the magnitude of the early CD4+ T cell immune response is determined by the severity of initial infection (participants requiring hospitalization or intensive care), pre-existing lung disease was significantly associated with higher long-term SARS-CoV2-specific CD8+ T cell responses, independent of initial disease severity or age. Neutralizing antibody levels were strongly correlated with SARS-CoV-2-specific CD4+ T but not CD8+ T cell responses. Importantly, we did not identify substantial differences in long-term virus-specific T cell or antibody responses between participants with and without COVID-19-related symptoms that persist months after initial infection.

Published

2021