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1. Generating and measuring effective vaccine-elicited HIV-specific CD8+ T cell responses

Author

Borgo, Gina M and Rutishauser, Rachel L

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Women's Health, Vaccine Related (AIDS), Sexually Transmitted Infections, Immunization, Vaccine Related, Infectious Diseases, Biotechnology, HIV/AIDS, Prevention, 3.4 Vaccines, Infection, Good Health and Well Being, Humans, AIDS Vaccines, HIV Infections, CD8-Positive T-Lymphocytes, Genetic Vectors, Epitopes, CD8(+) T cell, HIV vaccine, nucleic acid vaccine platforms, T cell quality, viral vectors, Public Health and Health Services, Virology, Clinical sciences, Medical microbiology, Epidemiology
Abstract

Purpose of reviewThere is growing consensus that eliciting CD8 + T cells in addition to antibodies may be required for an effective HIV vaccine for both prevention and cure. Here, we review key qualities of vaccine-elicited CD8 + T cells as well as major CD8 + T cell-based delivery platforms used in recent HIV vaccine clinical trials.Recent findingsMuch progress has been made in improving HIV immunogen design and delivery platforms to optimize CD8 + T cell responses. With regards to viral vectors, recent trials have tested newer chimp and human adenovirus vectors as well as a CMV vector. DNA vaccine immunogenicity has been increased by delivering the vaccines by electroporation and together with adjuvants as well as administering them as part of a heterologous regimen. In preclinical models, self-amplifying RNA vaccines can generate durable tissue-based CD8 + T cells. While it may be beneficial for HIV vaccines to recapitulate the functional and phenotypic features of HIV-specific CD8 + T cells isolated from elite controllers, most of these features are not routinely measured in HIV vaccine clinical trials.SummaryIdentifying a vaccine capable of generating durable T cell responses that target mutationally vulnerable epitopes and that can rapidly intercept infecting or rebounding virus remains a challenge for HIV. Comprehensive assessment of HIV vaccine-elicited CD8 + T cells, as well as comparisons between different vaccine platforms, will be critical to advance our understanding of how to design better CD8 + T cell-based vaccines for HIV.

Published
2023

3. In vivo killing of primary HIV-infected cells by peripheral-injected early memory–enriched anti-HIV duoCAR T cells

Author

Anthony-Gonda, Kim, Ray, Alex, Su, Hang, Wang, Yuge, Xiong, Ying, Lee, Danica, Block, Ariele, Chilunda, Vanessa, Weiselberg, Jessica, Zemelko, Lily, Wang, Yen Y, Kleinsorge-Block, Sarah, Reese, Jane S, de Lima, Marcos, Ochsenbauer, Christina, Kappes, John C, Dimitrov, Dimiter S, Orentas, Rimas, Deeks, Steven G, Rutishauser, Rachel L, Berman, Joan W, Goldstein, Harris, and Dropulić, Boro

Subjects
Clinical Research, HIV/AIDS, Stem Cell Research - Nonembryonic - Human, Infectious Diseases, Genetics, Human Fetal Tissue, Immunization, Stem Cell Research, Development of treatments and therapeutic interventions, 5.2 Cellular and gene therapies, Infection, Animals, Mice, CD4-Positive T-Lymphocytes, HIV Infections, HIV-1, Leukocytes, Mononuclear, Receptors, Chimeric Antigen, Clinical Trials, Phase I as Topic, Clinical Trials, Phase II as Topic, AIDS/HIV, Immunotherapy, Therapeutics
Abstract

HIV-specific chimeric antigen receptor-T cell (CAR T cell) therapies are candidates to functionally cure HIV infection in people with HIV (PWH) by eliminating reactivated HIV-infected cells derived from latently infected cells within the HIV reservoir. Paramount to translating such therapeutic candidates successfully into the clinic will require anti-HIV CAR T cells to localize to lymphoid tissues in the body and eliminate reactivated HIV-infected cells such as CD4+ T cells and monocytes/macrophages. Here we show that i.v. injected anti-HIV duoCAR T cells, generated using a clinical-grade anti-HIV duoCAR lentiviral vector, localized to the site of active HIV infection in the spleen of humanized mice and eliminated HIV-infected PBMCs. CyTOF analysis of preinfusion duoCAR T cells revealed an early memory phenotype composed predominantly of CCR7+ stem cell-like/central memory T cells (TSCM/TCM) with expression of some effector-like molecules. In addition, we show that anti-HIV duoCAR T cells effectively sense and kill HIV-infected CD4+ T cells and monocytes/macrophages. Furthermore, we demonstrate efficient genetic modification of T cells from PWH on suppressive ART into anti-HIV duoCAR T cells that subsequently kill autologous PBMCs superinfected with HIV. These studies support the safety and efficacy of anti-HIV duoCAR T cell therapy in our presently open phase I/IIa clinical trial (NCT04648046).

Published
2022

4. Postacute sequelae and adaptive immune responses in people with HIV recovering from SARS-COV-2 infection

Author

Peluso, Michael J, Spinelli, Matthew A, Deveau, Tyler-Marie, Forman, Carrie A, Munter, Sadie E, Mathur, Sujata, Tang, Alex F, Lu, Scott, Goldberg, Sarah A, Arreguin, Mireya I, Hoh, Rebecca, Tai, Viva, Chen, Jessica Y, Martinez, Enrique O, Yee, Brandon C, Chenna, Ahmed, Winslow, John W, Petropoulos, Christos J, Sette, Alessandro, Weiskopf, Daniella, Kumar, Nitasha, Lynch, Kara L, Hunt, Peter W, Durstenfeld, Matthew S, Hsue, Priscilla Y, Kelly, J Daniel, Martin, Jeffrey N, Glidden, David V, Gandhi, Monica, Deeks, Steven G, Rutishauser, Rachel L, and Henrich, Timothy J

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Emerging Infectious Diseases, Clinical Research, Coronaviruses, Infectious Diseases, Sexually Transmitted Infections, HIV/AIDS, Infection, Inflammatory and immune system, Good Health and Well Being, Humans, Antibodies, Viral, CD4-Positive T-Lymphocytes, COVID-19, HIV Infections, Immunologic Memory, Programmed Cell Death 1 Receptor, SARS-CoV-2, Post-Acute COVID-19 Syndrome, coronavirus disease 2019, HIV, immune response, long coronavirus disease, postacute sequelae of SARS-CoV-2, Biological Sciences, Medical and Health Sciences, Psychology and Cognitive Sciences, Virology, Biomedical and clinical sciences, Health sciences
Abstract

BackgroundLimited data are available on the long-term clinical and immunologic consequences of SARS-CoV-2 infection in people with HIV (PWH).MethodsWe measured SARS-CoV-2-specific humoral and cellular responses in people with and without HIV recovering from COVID-19 ( n  = 39 and n  = 43, respectively) using binding antibody, surrogate virus neutralization, intracellular cytokine staining, and inflammatory marker assays. We identified individuals experiencing postacute sequelae of SARS-CoV-2 infection (PASC) and evaluated immunologic parameters. We used linear regression and generalized linear models to examine differences by HIV status in the magnitude of inflammatory and virus-specific antibody and T-cell responses, as well as differences in the prevalence of PASC.ResultsAmong PWH, we found broadly similar SARS-CoV-2-specific antibody and T-cell responses as compared with a well matched group of HIV-negative individuals. PWH had 70% lower relative levels of SARS-CoV-2-specific memory CD8 + T cells ( P  = 0.007) and 53% higher relative levels of PD-1+ SARS-CoV-2-specific CD4 + T cells ( P  = 0.007). Higher CD4 + /CD8 + ratio was associated with lower PD-1 expression on SARS-CoV-2-specific CD8 + T cells (0.34-fold effect, P  = 0.02). HIV status was strongly associated with PASC (odds ratio 4.01, P  = 0.008), and levels of certain inflammatory markers (IL-6, TNF-alpha, and IP-10) were associated with persistent symptoms.ConclusionWe identified potentially important differences in SARS-CoV-2-specific CD4 + and CD8 + T cells in PWH and HIV-negative participants that might have implications for long-term immunity conferred by natural infection. HIV status strongly predicted the presence of PASC. Larger and more detailed studies of PASC in PWH are urgently needed.

Published
2022

5. CD8+ T-cell responses in HIV controllers: potential implications for novel HIV remission strategies

Author

Rutishauser, Rachel L and Trautmann, Lydie

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Vaccine Related (AIDS), Prevention, Immunization, Vaccine Related, HIV/AIDS, Infectious Diseases, Inflammatory and immune system, Infection, Good Health and Well Being, Animals, CD8-Positive T-Lymphocytes, HIV Infections, HIV Non-Progressors, Humans, Macaca mulatta, Simian Acquired Immunodeficiency Syndrome, Simian Immunodeficiency Virus, Viral Load, CD8(+) T cells, HIV controllers, HIV remission strategies, Simian immunodeficiency virus, Public Health and Health Services, Virology, Clinical sciences, Medical microbiology, Epidemiology
Abstract

Purpose of reviewImmunological studies of spontaneous HIV and simian virus (SIV) controllers have identified virus-specific CD8 +  T cells as a key immune mechanism of viral control. The purpose of this review is to consider how knowledge about the mechanisms that are associated with CD8 +  T cell control of HIV/SIV in natural infection can be harnessed in HIV remission strategies.Recent findingsWe discuss characteristics of CD8 +  T-cell responses that may be critical for suppressing HIV replication in spontaneous controllers comprising HIV antigen recognition including specific human leukocyte antigen types, broadly cross-reactive T cell receptors and epitope targeting, enhanced expansion and antiviral functions, and localization of virus-specific T cells near sites of reservoir persistence. We also discuss the need to better understand the timing of CD8 +  T-cell responses associated with viral control of HIV/SIV during acute infection and after treatment interruption as well as the mechanisms by which HIV/SIV-specific CD8 +  T cells coordinate with other immune responses to achieve control.SummaryWe propose implications as to how this knowledge from natural infection can be applied in the design and evaluation of CD8 +  T-cell-based remission strategies and offer questions to consider as these strategies target distinct CD8 +  T-cell-dependent mechanisms of viral control.

Published
2022

6. A cytotoxic-skewed immune set point predicts low neutralizing antibody levels after Zika virus infection

Author

McCarthy, Elizabeth E, Odorizzi, Pamela M, Lutz, Emma, Smullin, Carolyn P, Tenvooren, Iliana, Stone, Mars, Simmons, Graham, Hunt, Peter W, Feeney, Margaret E, Norris, Philip J, Busch, Michael P, Spitzer, Matthew H, and Rutishauser, Rachel L

Subjects
Biological Sciences, Biotechnology, Prevention, Infectious Diseases, Immunization, HIV/AIDS, Rare Diseases, Vaccine Related, Infection, Inflammatory and immune system, Good Health and Well Being, Antibodies, Neutralizing, Antibodies, Viral, Humans, Vaccination, Zika Virus, Zika Virus Infection, CP: Immunology, CyTOF, Zika virus, immune signatures, neutralizing antibodies, systems immunology, Biochemistry and Cell Biology, Medical Physiology, Biological sciences
Abstract

Although generating high neutralizing antibody levels is a key component of protective immunity after acute viral infection or vaccination, little is known about why some individuals generate high versus low neutralizing antibody titers. Here, we leverage the high-dimensional single-cell profiling capacity of mass cytometry to characterize the longitudinal cellular immune response to Zika virus (ZIKV) infection in viremic blood donors in Puerto Rico. During acute ZIKV infection, we identify widely coordinated responses across innate and adaptive immune cell lineages. High frequencies of multiple activated cell types during acute infection are associated with high titers of ZIKV neutralizing antibodies 6 months post-infection, while stable immune features suggesting a cytotoxic-skewed immune set point are associated with low titers. Our study offers insight into the coordination of immune responses and identifies candidate cellular biomarkers that may offer predictive value in vaccine efficacy trials aimed at inducing high levels of antiviral neutralizing antibodies.

Published
2022

7. Persistence, Magnitude, and Patterns of Postacute Symptoms and Quality of Life Following Onset of SARS-CoV-2 Infection: Cohort Description and Approaches for Measurement

Author

Peluso, Michael J, Kelly, J Daniel, Lu, Scott, Goldberg, Sarah A, Davidson, Michelle C, Mathur, Sujata, Durstenfeld, Matthew S, Spinelli, Matthew A, Hoh, Rebecca, Tai, Viva, Fehrman, Emily A, Torres, Leonel, Hernandez, Yanel, Williams, Meghann C, Arreguin, Mireya I, Ngo, Lynn H, Deswal, Monika, Munter, Sadie E, Martinez, Enrique O, Anglin, Khamal A, Romero, Mariela D, Tavs, Jacqueline, Rugart, Paulina R, Chen, Jessica Y, Sans, Hannah M, Murray, Victoria W, Ellis, Payton K, Donohue, Kevin C, Massachi, Jonathan A, Weiss, Jacob O, Mehdi, Irum, Pineda-Ramirez, Jesus, Tang, Alex F, Wenger, Megan A, Assenzio, Melissa T, Yuan, Yan, Krone, Melissa R, Rutishauser, Rachel L, Rodriguez-Barraquer, Isabel, Greenhouse, Bryan, Sauceda, John A, Gandhi, Monica, Scheffler, Aaron Wolfe, Hsue, Priscilla Y, Henrich, Timothy J, Deeks, Steven G, and Martin, Jeffrey N

Subjects
Lung, Prevention, Clinical Research, Pneumonia, Infectious Diseases, Good Health and Well Being, COVID-19, long COVID, post-acute sequelae of SARS-CoV-2, quality of life, SARS-CoV-2
Abstract

BackgroundThere is mounting evidence for the presence of postacute sequelae of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection (PASC), but there is limited information on the spectrum, magnitude, duration, and patterns of these sequelae as well as their influence on quality of life.MethodsWe assembled a cohort of adults with a documented history of SARS-CoV-2 RNA positivity at ≥2 weeks past onset of coronavirus disease 2019 (COVID-19) symptoms or, if asymptomatic, first positive test. At 4-month intervals, we queried physical and mental health symptoms and quality of life.ResultsOf the first 179 participants enrolled, 10 were asymptomatic during the acute phase of SARS-CoV-2 infection, 125 were symptomatic but not hospitalized, and 44 were symptomatic and hospitalized. During the postacute phase, fatigue, shortness of breath, concentration problems, headaches, trouble sleeping, and anosmia/dysgeusia were most common through 8 months of observation. Symptoms were typically at least somewhat bothersome and sometimes exhibited a waxing-and-waning course. Some participants experienced symptoms of depression, anxiety, and post-traumatic stress, as well as difficulties with performance of usual activities. The median visual analogue scale rating of general health was lower at 4 and 8 months compared with pre-COVID-19. Two clusters of symptom domains were identified.ConclusionsMany participants report bothersome symptoms following onset of COVID-19 with variable patterns of persistence and impact on quality of life. The substantial variability suggests the existence of multiple subphenotypes of PASC. A rigorous approach to the prospective measurement of symptoms and functional manifestations sets the stage for the next phase of research focusing on the pathophysiologic causes of the various subgroups of PASC.

Published
2022

8. 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

9. Discordant Virus-Specific Antibody Levels, Antibody Neutralization Capacity, and T-cell Responses Following 3 Doses of SARS-CoV-2 Vaccination in a Patient With Connective Tissue Disease

Author

Peluso, Michael J, Munter, Sadie E, Lynch, Kara L, Yun, Cassandra, Torres, Leonel, Iyer, Nikita S, Donatelli, Joanna, Ryan, Lindsay, Deitchman, Amelia N, Deeks, Steven G, Rutishauser, Rachel L, and Henrich, Timothy J

Subjects
Biomedical and Clinical Sciences, Immunology, Pneumonia & Influenza, Biotechnology, Lung, Infectious Diseases, Prevention, Rare Diseases, Immunization, Clinical Research, Pneumonia, Emerging Infectious Diseases, Vaccine Related, Biodefense, Inflammatory and immune system, Infection, Good Health and Well Being, COVID-19 vaccine, neutralizing antibodies, rheumatological disease, SARS-CoV-2, T-cell immunity, Clinical sciences, Medical microbiology
Abstract

We report a patient with connective tissue disease who developed modest severe acute respiratory syndrome coronavirus 2 receptor binding domain-specific antibody levels and a lack of neutralization capacity, despite having received 3 mRNA coronavirus disease 2019 vaccines and holding anti-B-cell therapy for >7 months before vaccination. The patient developed virus-specific T-cell responses.

Published
2021

10. 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

11. 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

12. Characterization and Biomarker Analyses of Post-COVID-19 Complications and Neurological Manifestations.

Author

Sun, Bing, Tang, Norina, Peluso, Michael J, Iyer, Nikita S, Torres, Leonel, Donatelli, Joanna L, Munter, Sadie E, Nixon, Christopher C, Rutishauser, Rachel L, Rodriguez-Barraquer, Isabel, Greenhouse, Bryan, Kelly, John D, Martin, Jeffrey N, Deeks, Steven G, Henrich, Timothy J, and Pulliam, Lynn

Subjects
SARS-CoV-2, comorbidities, cytokines, exosome, neurodegeneration
Abstract

As the SARS-CoV-2 pandemic continues, reports have demonstrated neurologic sequelae following COVID-19 recovery. Mechanisms to explain long-term neurological sequelae are unknown and need to be identified. Plasma from 24 individuals recovering from COVID-19 at 1 to 3 months after initial infection were collected for cytokine and antibody levels and neuronal-enriched extracellular vesicle (nEV) protein cargo analyses. Plasma cytokine IL-4 was increased in all COVID-19 participants. Volunteers with self-reported neurological problems (nCoV, n = 8) had a positive correlation of IL6 with age or severity of the sequalae, at least one co-morbidity and increased SARS-CoV-2 antibody compared to those COVID-19 individuals without neurological issues (CoV, n = 16). Protein markers of neuronal dysfunction including amyloid beta, neurofilament light, neurogranin, total tau, and p-T181-tau were all significantly increased in the nEVs of all participants recovering from COVID-19 compared to historic controls. This study suggests ongoing peripheral and neuroinflammation after COVID-19 infection that may influence neurological sequelae by altering nEV proteins. Individuals recovering from COVID-19 may have occult neural damage while those with demonstrative neurological symptoms additionally had more severe infection. Longitudinal studies to monitor plasma biomarkers and nEV cargo are warranted to assess persistent neurodegeneration and systemic effects.

Published
2021

13. TCF-1 regulates HIV-specific CD8+ T cell expansion capacity

Author

Rutishauser, Rachel L, Deguit, Christian Deo T, Hiatt, Joseph, Blaeschke, Franziska, Roth, Theodore L, Wang, Lynn, Raymond, Kyle A, Starke, Carly E, Mudd, Joseph C, Chen, Wenxuan, Smullin, Carolyn P, Matus-Nicodemos, Rodrigo, Hoh, Rebecca, Krone, Melissa R, Hecht, Frederick M, Pilcher, Christopher D, Martin, Jeffrey N, Koup, Richard A, Douek, Daniel C, Brenchley, Jason M, Sékaly, Rafick-Pierre, Pillai, Satish K, Marson, Alexander, Deeks, Steven G, McCune, Joseph M, and Hunt, Peter W

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Sexually Transmitted Infections, HIV/AIDS, Infectious Diseases, Underpinning research, 1.1 Normal biological development and functioning, Infection, Good Health and Well Being, Adult, Aged, Animals, CD8-Positive T-Lymphocytes, Female, Gene Knockout Techniques, HIV Antigens, HIV Infections, HIV-1, Humans, Immunologic Memory, Macaca mulatta, Male, Middle Aged, Simian Acquired Immunodeficiency Syndrome, Simian Immunodeficiency Virus, T Cell Transcription Factor 1, Viral Load, Simian immunodeficiency virus, AIDS/HIV, Adaptive immunity, T cells, Biomedical and clinical sciences, Health sciences
Abstract

Although many HIV cure strategies seek to expand HIV-specific CD8+ T cells to control the virus, all are likely to fail if cellular exhaustion is not prevented. A loss in stem-like memory properties (i.e., the ability to proliferate and generate secondary effector cells) is a key feature of exhaustion; little is known, however, about how these properties are regulated in human virus-specific CD8+ T cells. We found that virus-specific CD8+ T cells from humans and nonhuman primates naturally controlling HIV/SIV infection express more of the transcription factor TCF-1 than noncontrollers. HIV-specific CD8+ T cell TCF-1 expression correlated with memory marker expression and expansion capacity and declined with antigenic stimulation. CRISPR-Cas9 editing of TCF-1 in human primary T cells demonstrated a direct role in regulating expansion capacity. Collectively, these data suggest that TCF-1 contributes to the regulation of the stem-like memory property of secondary expansion capacity of HIV-specific CD8+ T cells, and they provide a rationale for exploring the enhancement of this pathway in T cell-based therapeutic strategies for HIV.

Published
2021

14. Clinical Utility of Universal Broad-Range Polymerase Chain Reaction Amplicon Sequencing for Pathogen Identification: A Retrospective Cohort Study

Author

Kerkhoff, Andrew D, Rutishauser, Rachel L, Miller, Steve, and Babik, Jennifer M

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Good Health and Well Being, Humans, Polymerase Chain Reaction, Retrospective Studies, Sensitivity and Specificity, broad-range universal PCR, DNA sequencing, molecular diagnostics, pathogen identification, Biological Sciences, Medical and Health Sciences, Microbiology, Clinical sciences
Abstract

We assessed the real-world utility of universal broad-range polymerase chain reaction sequencing for pathogen detection. Among 1062 clinical samples, 107/1062 (10.1%) had a clinically significant, positive result, with substantial variation by specimen type. Clinical management was changed in 44/1062 (4.1%). These data can help maximize utility of this emerging diagnostic.

Published
2020

15. Beta cell-specific CD8+ T cells maintain stem cell memory-associated epigenetic programs during type 1 diabetes

Author

Abdelsamed, Hossam A, Zebley, Caitlin C, Nguyen, Hai, Rutishauser, Rachel L, Fan, Yiping, Ghoneim, Hazem E, Crawford, Jeremy Chase, Alfei, Francesca, Alli, Shanta, Ribeiro, Susan Pereira, Castellaw, Ashley H, McGargill, Maureen A, Jin, Hongjian, Boi, Shannon K, Speake, Cate, Serti, Elisavet, Turka, Laurence A, Busch, Michael E, Stone, Mars, Deeks, Steven G, Sekaly, Rafick-Pierre, Zehn, Dietmar, James, Eddie A, Nepom, Gerald T, and Youngblood, Ben

Subjects
Biomedical and Clinical Sciences, Immunology, Genetics, Diabetes, Autoimmune Disease, Stem Cell Research, Aetiology, 2.1 Biological and endogenous factors, Metabolic and endocrine, Adolescent, Adult, Animals, Autoantigens, CD8-Positive T-Lymphocytes, Cell Plasticity, Cells, Cultured, DNA Methylation, Diabetes Mellitus, Type 1, Epigenesis, Genetic, Female, Flow Cytometry, Humans, Immunologic Memory, Insulin-Secreting Cells, Male, Mice, Pluripotent Stem Cells, Single-Cell Analysis, Young Adult, Biochemistry and cell biology
Abstract

The pool of beta cell-specific CD8+ T cells in type 1 diabetes (T1D) sustains an autoreactive potential despite having access to a constant source of antigen. To investigate the long-lived nature of these cells, we established a DNA methylation-based T cell 'multipotency index' and found that beta cell-specific CD8+ T cells retained a stem-like epigenetic multipotency score. Single-cell assay for transposase-accessible chromatin using sequencing confirmed the coexistence of naive and effector-associated epigenetic programs in individual beta cell-specific CD8+ T cells. Assessment of beta cell-specific CD8+ T cell anatomical distribution and the establishment of stem-associated epigenetic programs revealed that self-reactive CD8+ T cells isolated from murine lymphoid tissue retained developmentally plastic phenotypic and epigenetic profiles relative to the same cells isolated from the pancreas. Collectively, these data provide new insight into the longevity of beta cell-specific CD8+ T cell responses and document the use of this methylation-based multipotency index for investigating human and mouse CD8+ T cell differentiation.

Published
2020

16. A collaborative, multidisciplinary approach to HIV transmission risk mitigation during analytic treatment interruption

Author

Peluso, Michael J, Dee, Lynda, Campbell, Danielle, Taylor, Jeff, Hoh, Rebecca, Rutishauser, Rachel L, Sauceda, John, Deeks, Steven G, and Dubé, Karine

Subjects
Biomedical and Clinical Sciences, Immunology, Women's Health, HIV/AIDS, Sexually Transmitted Infections, Clinical Research, Infectious Diseases, Clinical Trials and Supportive Activities, 6.1 Pharmaceuticals, Evaluation of treatments and therapeutic interventions, Infection, HIV, HIV cure research, HIV remission research, analytical treatment interruption
Abstract

Analytic treatment interruptions (ATIs) are currently the standard for assessing the impact of experimental interventions aimed at inducing sustained antiretroviral therapy (ART)-free remission in trials related to HIV cure. ATIs are associated with substantial risk to both study participants and their sexual partner(s). Two documented HIV transmissions occurring in the context of ATIs have been recently reported, but recommendations for mitigating the risk of such events during ATIs are limited. We outline a practical approach to risk mitigation during ATI studies and describe strategies we are utilising in an upcoming clinical trial that may be applicable to other centres.

Published
2020

17. 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

18. 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

19. Some Aspects of CD8+ T-Cell Exhaustion Are Associated With Altered T-Cell Mitochondrial Features and ROS Content in HIV Infection.

Author

Deguit, Christian Deo T, Hough, Michelle, Hoh, Rebecca, Krone, Melissa, Pilcher, Christopher D, Martin, Jeffrey N, Deeks, Steven G, McCune, Joseph M, Hunt, Peter W, and Rutishauser, Rachel L

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Immunotherapy, Sexually Transmitted Infections, Clinical Research, HIV/AIDS, Infectious Diseases, 2.1 Biological and endogenous factors, Aetiology, Infection, Good Health and Well Being, CD8-Positive T-Lymphocytes, HIV Infections, Humans, Interleukin-7 Receptor alpha Subunit, Lymphocyte Activation, Membrane Potential, Mitochondrial, Mitochondria, Programmed Cell Death 1 Receptor, Reactive Oxygen Species, Viremia, CD8(+) T-cell, exhaustion, mitochondrial features, ROS content, HIV, Clinical Sciences, Public Health and Health Services, Virology, Clinical sciences, Epidemiology, Public health
Abstract

BackgroundReversing or preventing T-cell exhaustion is an important treatment goal in the context of HIV disease; however, the mechanisms that regulate HIV-specific CD8 T-cell exhaustion are incompletely understood. Since mitochondrial mass (MM), mitochondrial membrane potential (MMP), and cellular reactive oxygen species (ROS) content are altered in exhausted CD8 T cells in other settings, we hypothesized that similar lesions may arise in HIV infection.MethodsWe sampled cryopreserved peripheral blood mononuclear cells from HIV-uninfected (n = 10) and HIV-infected participants with varying levels and mechanisms of viral control: viremic (VL > 2000 copies/mL; n = 8) or aviremic (VL < 40 copies/mL) due to antiretroviral therapy (n = 11) or natural control (n = 9). We characterized the MM, MMP, and ROS content of bulk CD8 T cells and MHC class I tetramer+ HIV-specific CD8 T cells by flow cytometry.ResultsWe observed higher MM, MMP, and ROS content across bulk effector-memory CD8 T-cell subsets in HIV-infected compared with HIV-uninfected participants. Among HIV-specific CD8 T cells, these features did not vary by the extent or mechanism of viral control but were significantly altered in cells displaying characteristics associated with exhaustion (eg, high PD-1 expression, low CD127 expression, and impaired proliferative capacity).ConclusionsWhile we did not find that control of HIV replication in vivo correlates with the CD8 T-cell MM, MMP, or ROS content, we did find that some features of CD8 T-cell exhaustion are associated with alterations in mitochondrial state. Our findings support further studies to probe the relationship between mitochondrial dynamics and CD8 T-cell functionality in HIV infection.

Published
2019

20. Limited engraftment of donor microbiome via one-time fecal microbial transplantation in treated HIV-infected individuals

Author

Vujkovic-Cvijin, Ivan, Rutishauser, Rachel L, Pao, Montha, Hunt, Peter W, Lynch, Susan V, McCune, Joseph M, and Somsouk, Ma

Subjects
Microbiology, Biological Sciences, Sexually Transmitted Infections, Digestive Diseases, HIV/AIDS, Transplantation, Clinical Research, Minority Health, Health Disparities, Microbiome, Infectious Diseases, 2.1 Biological and endogenous factors, Evaluation of treatments and therapeutic interventions, 6.1 Pharmaceuticals, Aetiology, Infection, Good Health and Well Being, Adult, Aged, Dysbiosis, Fecal Microbiota Transplantation, Gastrointestinal Microbiome, HIV Infections, Humans, Male, Middle Aged, Treatment Outcome, Microbiota, fecal transplant, engraftment, HIV, inflammation, fecal microbiome transplant, microbiome engraftment
Abstract

Many HIV-infected individuals on antiretroviral therapy (ART) exhibit persistent systemic inflammation, which predicts morbidity and mortality. ART-treated subjects concurrently exhibit marked compositional alterations in the gut bacterial microbiota and the degree of dysbiosis correlates with systemic inflammation. Whether interventions to modulate the microbiome can affect systemic inflammation is unknown. An open-label fecal microbial transplantation (FMT) was delivered by colonoscopy to asymptomatic HIV-infected ART-suppressed individuals without antibiotic pre-treatment. Stool was assessed before and after FMT for engraftment of donor microbes, and peripheral blood was assayed for immune activation biomarkers. Six participants received FMT and 2 participants served as controls. No serious adverse effects occurred during 24 weeks of follow-up. At baseline, HIV-infected individuals exhibited microbiota profiles distinct from uninfected donors. During the 8 weeks post-FMT, recipients demonstrated partial engraftment of the donor microbiome (P < 0.05). Recipient microbiota remained significantly distant from donors, unlike that observed following FMT for treatment of C. difficile infection. Systemic inflammatory markers showed no significant change post-FMT. FMT was well-tolerated in ART-treated, HIV-infected individuals. Engraftment was detectable but modest, and appeared to be limited to specific bacterial taxa. Whether antibiotic conditioning can enhance engraftment and the capacity of microbiota to modulate inflammation remains to be investigated.

Published
2017

21. Disseminated Acanthamoeba infection in a heart transplant recipient treated successfully with a miltefosine‐containing regimen: Case report and review of the literature

Author

Brondfield, Max N, Reid, Michael JA, Rutishauser, Rachel L, Cope, Jennifer R, Tang, Jevon, Ritter, Jana M, Matanock, Almea, Ali, Ibne, Doernberg, Sarah B, Hilts‐Horeczko, Alexandra, DeMarco, Teresa, Klein, Liviu, and Babik, Jennifer M

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Emerging Infectious Diseases, Organ Transplantation, Transplantation, Infectious Diseases, 6.4 Surgery, Evaluation of treatments and therapeutic interventions, Infection, Acanthamoeba, Amebiasis, Amebicides, Amphotericin B, Anti-Bacterial Agents, Antilymphocyte Serum, Biopsy, Cardiomyopathies, Drugs, Investigational, Endoscopy, Female, Fluconazole, Flucytosine, Heart Transplantation, Humans, Immunocompromised Host, Immunosuppressive Agents, Magnetic Resonance Imaging, Metacarpal Bones, Metronidazole, Middle Aged, Phosphorylcholine, Polymerase Chain Reaction, Radiography, Sinusitis, Skin, heart transplant, miltefosine, Acanthamoeba, Surgery, Clinical sciences
Abstract

Disseminated acanthamoebiasis is a rare, often fatal, infection most commonly affecting immunocompromised patients. We report a case involving sinuses, skin, and bone in a 60-year-old woman 5 months after heart transplantation. She improved with a combination of flucytosine, fluconazole, miltefosine, and decreased immunosuppression. To our knowledge, this is the first case of successfully treated disseminated acanthamoebiasis in a heart transplant recipient and only the second successful use of miltefosine for this infection among solid organ transplant recipients. Acanthamoeba infection should be considered in transplant recipients with evidence of skin, central nervous system, and sinus infections that are unresponsive to antibiotics. Miltefosine may represent an effective component of a multidrug therapeutic regimen for the treatment of this amoebic infection.

Published
2017

22. Safety and Broad Immunogenicity of HIVconsvX Conserved Mosaic Candidate T-Cell Vaccines Vectored by ChAdOx1 and MVA in HIV-CORE 006: A Double-Blind, Randomized, Placebo-Controlled Phase 1 Trial in Healthy Adults Living Without HIV-1 in Eastern and Southern Africa

Author

Chanda, Chama, primary, Kibengo, Freddie, additional, Mutua, Michael, additional, Ogada, Fred, additional, Muturi-Kioi, Vincent, additional, Yildirim, Belkis M. Akis, additional, Amondi, Mary, additional, Baines, Andrea, additional, Basajja, Vincent, additional, Borthwick, Nicola, additional, Bosire, Kefa, additional, Chambula, Elias, additional, Chetty, Paramesh, additional, Chinyenze, Kundai, additional, Chirro, Oscar, additional, Crook, Alison, additional, De Bont, Jan, additional, Fernandez, Natalia, additional, Ejou, Peter, additional, Farah, Bashir, additional, Glaze, Molly, additional, Gombe, Ben, additional, Gumbe, Anne, additional, Hayes, Peter, additional, Itwi, Sally, additional, Juma, Sheba, additional, Karambi, Anita, additional, Kabengele, Chishiba, additional, Kafeero, Paddy, additional, Kakande, Ayoub, additional, Kanungi, Jennifer, additional, Kidega, William, additional, King, Deborah, additional, Phiri, Hilda, additional, Mahira, Rose, additional, Malogo, Roselyn, additional, Matsoso, Mabela, additional, Michelo, Clive, additional, Moyo, Annie, additional, Mugaba, Susan, additional, Mugenya, Irene, additional, Muhumuza, Patrick, additional, Mujadidi, Yama, additional, Muriuki, Moses, additional, Musale, Vernon, additional, Mutua, Gaudensia, additional, Muwowo, Meya, additional, Mwale, Fatima, additional, Mwangi, Irene, additional, Nakimbugwe, Maria, additional, Namuyanja, Angella, additional, Nduati, Eunice, additional, Nielsen, Leslie, additional, Nyange, Jaquelyn, additional, Oino, Geofrey, additional, Okech, Brenda, additional, Omosa, Gloria, additional, Otieno, Dan, additional, Palmer, Shaun, additional, Ramko, Kelly, additional, Rutishauser, Rachel L., additional, Sayeed, Eddy, additional, Sajabi, Rose, additional, Serwanga, Jennifer, additional, Wee, Edmund, additional, Wenden, Claire, additional, Cicconi, Paola, additional, Fast, Patricia, additional, Gilmour, Jill, additional, Jaoko, Walter, additional, Kaleebu, Pontiano, additional, Kilembe, William, additional, Kuipers, Hester, additional, Sanders, Eduard, additional, and Hanke, Tomas, additional

Published
2024
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25. CD8 + T-cell responses in HIV controllers: potential implications for novel HIV remission strategies.

Author

Rutishauser, Rachel L, Rutishauser, Rachel L, Trautmann, Lydie, Rutishauser, Rachel L, Rutishauser, Rachel L, and Trautmann, Lydie

Abstract

Purpose of reviewImmunological studies of spontaneous HIV and simian virus (SIV) controllers have identified virus-specific CD8 + T cells as a key immune mechanism of viral control. The purpose of this review is to consider how knowledge about the mechanisms that are associated with CD8 + T cell control of HIV/SIV in natural infection can be harnessed in HIV remission strategies.Recent findingsWe discuss characteristics of CD8 + T-cell responses that may be critical for suppressing HIV replication in spontaneous controllers comprising HIV antigen recognition including specific human leukocyte antigen types, broadly cross-reactive T cell receptors and epitope targeting, enhanced expansion and antiviral functions, and localization of virus-specific T cells near sites of reservoir persistence. We also discuss the need to better understand the timing of CD8 + T-cell responses associated with viral control of HIV/SIV during acute infection and after treatment interruption as well as the mechanisms by which HIV/SIV-specific CD8 + T cells coordinate with other immune responses to achieve control.SummaryWe propose implications as to how this knowledge from natural infection can be applied in the design and evaluation of CD8 + T-cell-based remission strategies and offer questions to consider as these strategies target distinct CD8 + T-cell-dependent mechanisms of viral control.

Published
2022

27. Pneumonia surveillance with culture-independent metatranscriptomics in HIV-positive adults in Uganda: a cross-sectional study

Author

Spottiswoode, Natasha, primary, Bloomstein, Joshua D, additional, Caldera, Saharai, additional, Sessolo, Abdul, additional, McCauley, Kathryn, additional, Byanyima, Patrick, additional, Zawedde, Josephine, additional, Kalantar, Katrina, additional, Kaswabuli, Sylvia, additional, Rutishauser, Rachel L, additional, Lieng, Monica K, additional, Davis, J Lucian, additional, Moore, Julia, additional, Jan, Amanda, additional, Iwai, Shoko, additional, Shenoy, Meera, additional, Sanyu, Ingvar, additional, DeRisi, Joseph L, additional, Lynch, Susan V, additional, Worodria, William, additional, Huang, Laurence, additional, and Langelier, Charles R, additional

Published
2022
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28. HIV-specific CD8 T cells from elite controllers have an epigenetic imprint that preserves effector functions

Author

Frias, Adolfo B, primary, Rutishauser, Rachel L, additional, Sharma, Ashish Arunkumar, additional, Mi, Tian, additional, Abdelsamed, Hossam Aly, additional, Zebley, Caitlin, additional, Constantz, Christian M, additional, Stone, Mars, additional, Busch, Michael, additional, Deeks, Steven, additional, Sekaly, Rafick, additional, and Youngblood, Ben A, additional

Published
2022
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29. POST-ACUTE SEQUELAE AND ADAPTIVE IMMUNE RESPONSES IN PEOPLE LIVING WITH HIV RECOVERING FROM SARS-COV-2 INFECTION

Author

Peluso, Michael J., primary, Spinelli, Matthew A., additional, Deveau, Tyler-Marie, additional, Forman, Carrie A., additional, Munter, Sadie E., additional, Mathur, Sujata, additional, Tang, Alex F., additional, Lu, Scott, additional, Goldberg, Sarah A., additional, Arreguin, Mireya I., additional, Hoh, Rebecca, additional, Tai, Viva, additional, Chen, Jessica Y., additional, Martinez, Enrique O., additional, Chenna, Ahmed, additional, Winslow, John W., additional, Petropoulos, Christos J., additional, Sette, Alessandro, additional, Weiskopf, Daniella, additional, Kumar, Nitasha, additional, Lynch, Kara L., additional, Hunt, Peter W., additional, Durstenfeld, Matthew S., additional, Hsue, Priscilla Y., additional, Kelly, J. Daniel, additional, Martin, Jeffrey N., additional, Glidden, David V., additional, Gandhi, Monica, additional, Deeks, Steven G., additional, Rutishauser, Rachel L., additional, and Henrich, Timothy J., additional

Published
2022
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30. A Cytotoxic-Skewed Immune Set Point Predicts Low Neutralizing Antibody Levels After Zika Virus Infection

Author

McCarthy, Elizabeth E., primary, Odorizzi, Pamela, additional, Lutz, Emma, additional, Smullin, Carolyn, additional, Tenvooren, Iliana, additional, Stone, Mars, additional, Simmons, Graham, additional, Hunt, Peter, additional, Feeney, Margo, additional, Norris, Philip, additional, Busch, Michael, additional, Spitzer, Matthew, additional, and Rutishauser, Rachel L., additional

Published
2022
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31. Persistence, Magnitude, and Patterns of Postacute Symptoms and Quality of Life Following Onset of SARS-CoV-2 Infection: Cohort Description and Approaches for Measurement

Author

Peluso, Michael J, primary, Kelly, J Daniel, additional, Lu, Scott, additional, Goldberg, Sarah A, additional, Davidson, Michelle C, additional, Mathur, Sujata, additional, Durstenfeld, Matthew S, additional, Spinelli, Matthew A, additional, Hoh, Rebecca, additional, Tai, Viva, additional, Fehrman, Emily A, additional, Torres, Leonel, additional, Hernandez, Yanel, additional, Williams, Meghann C, additional, Arreguin, Mireya I, additional, Ngo, Lynn H, additional, Deswal, Monika, additional, Munter, Sadie E, additional, Martinez, Enrique O, additional, Anglin, Khamal A, additional, Romero, Mariela D, additional, Tavs, Jacqueline, additional, Rugart, Paulina R, additional, Chen, Jessica Y, additional, Sans, Hannah M, additional, Murray, Victoria W, additional, Ellis, Payton K, additional, Donohue, Kevin C, additional, Massachi, Jonathan A, additional, Weiss, Jacob O, additional, Mehdi, Irum, additional, Pineda-Ramirez, Jesus, additional, Tang, Alex F, additional, Wenger, Megan A, additional, Assenzio, Melissa T, additional, Yuan, Yan, additional, Krone, Melissa R, additional, Rutishauser, Rachel L, additional, Rodriguez-Barraquer, Isabel, additional, Greenhouse, Bryan, additional, Sauceda, John A, additional, Gandhi, Monica, additional, Scheffler, Aaron Wolfe, additional, Hsue, Priscilla Y, additional, Henrich, Timothy J, additional, Deeks, Steven G, additional, and Martin, Jeffrey N, additional

Published
2021
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32. HIV-specific CD8 T cells from elite controllers have an epigenetic imprint that preserves effector functions

Author

Frias, Adolfo B., primary, Rutishauser, Rachel L., additional, Sharma, Ashish A., additional, Mi, Tian, additional, Abdelsamed, Hossam, additional, Zebley, Caitlin, additional, Constantz, Christian M., additional, Stone, Mars, additional, Busch, Michael P., additional, Deeks, Steven G., additional, Sékaly, Rafick-Pierre, additional, and Youngblood, Ben, additional

Published
2021
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34. SARS-CoV-2 Vaccination in the Context of Ongoing HIV Cure-Related Research Studies

Author

Peluso, Michael J., primary, Dee, Lynda, additional, Taylor, Jeff, additional, Campbell, Danielle M., additional, Ehm, Adam, additional, Agosto-Rosario, Moisés, additional, Shao, Shirley, additional, Williams, Meghann C., additional, Hoh, Rebecca, additional, Rutishauser, Rachel L., additional, Deeks, Steven G., additional, Sauceda, John A., additional, and Dubé, Karine, additional

Published
2021
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35. Distinct cellular immune signatures in acute Zika virus infection are associated with high or low persisting neutralizing antibody titers

Author

McCarthy, Elizabeth E., primary, Odorizzi, Pamela M., additional, Lutz, Emma, additional, Smullin, Carolyn P., additional, Tenvooren, Iliana, additional, Stone, Mars, additional, Simmons, Graham, additional, Hunt, Peter W., additional, Feeney, Margaret E., additional, Norris, Philip J., additional, Busch, Michael P., additional, Spitzer, Matthew H., additional, and Rutishauser, Rachel L., additional

Published
2021
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36. Rapid implementation of a cohort for the study of post-acute sequelae of SARS-CoV-2 infection/COVID-19

Author

Peluso, Michael J., primary, Kelly, J. Daniel, additional, Lu, Scott, additional, Goldberg, Sarah A., additional, Davidson, Michelle C., additional, Mathur, Sujata, additional, Durstenfeld, Matthew S., additional, Spinelli, Matthew A., additional, Hoh, Rebecca, additional, Tai, Viva, additional, Fehrman, Emily A., additional, Torres, Leonel, additional, Hernandez, Yanel, additional, Williams, Meghann C., additional, Arreguin, Mireya I., additional, Bautista, Jennifer A., additional, Ngo, Lynn H., additional, Deswal, Monika, additional, Munter, Sadie E., additional, Martinez, Enrique O., additional, Anglin, Khamal A., additional, Romero, Mariela D., additional, Tavs, Jacqueline, additional, Rugart, Paulina R., additional, Chen, Jessica Y., additional, Sans, Hannah M., additional, Murray, Victoria W., additional, Ellis, Payton K., additional, Donohue, Kevin C., additional, Massachi, Jonathan A., additional, Weiss, Jacob O., additional, Mehdi, Irum, additional, Pineda-Ramirez, Jesus, additional, Tang, Alex F., additional, Wenger, Megan, additional, Assenzio, Melissa, additional, Yuan, Yan, additional, Krone, Melissa, additional, Rutishauser, Rachel L., additional, Rodriguez-Barraquer, Isabel, additional, Greenhouse, Bryan, additional, Sauceda, John A., additional, Gandhi, Monica, additional, Hsue, Priscilla Y., additional, Henrich, Timothy J., additional, Deeks, Steven G., additional, and Martin, Jeffrey N., additional

Published
2021
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37. 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
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38. 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
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39. Pneumonia Surveillance in Ugandans with HIV Through the Lens of Culture-Independent Metatranscriptomics: A Cross Sectional Study

Author

Spottiswoode, Natasha, primary, Bloomstein, Joshua, additional, Caldera, Saharai, additional, Sessolo, Abdul, additional, Byanyima, Patrick, additional, Zawedde, Josephine, additional, Kalantar, Katrina, additional, Kaswabuli, Sylvia, additional, Rutishauser, Rachel L., additional, Davis, J. Lucian, additional, Jan, Amanda, additional, Moore, Julia, additional, Iwai, Shoko, additional, Shenoy, Meera, additional, Sanyu, Ingvar, additional, DeRisi, Joseph L., additional, Lynch, Susan V., additional, Worodria, William, additional, Huang, Laurence, additional, and Langelier, Charles, additional

Published
2021
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40. Single-Cell Mapping of Progressive Fetal-to-Adult Transition in Human Naive T Cells

Author

Bunis, Daniel G., primary, Bronevetsky, Yelena, additional, Krow-Lucal, Elisabeth, additional, Bhakta, Nirav R., additional, Kim, Charles C., additional, Nerella, Srilaxmi, additional, Jones, Norman, additional, Mendoza, Ventura F., additional, Bryson, Yvonne J., additional, Gern, James E., additional, Rutishauser, Rachel L., additional, Ye, Chun Jimmie, additional, Sirota, Marina, additional, McCune, Joseph M., additional, and Burt, Trevor D., additional

Published
2021
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42. TCF-1 regulates the stem-like memory potential of HIV-specific CD8+ T cells in elite controllers

Author

Rutishauser, Rachel L., primary, Deguit, Christian Deo T., additional, Hiatt, Joseph, additional, Blaeschke, Franziska, additional, Roth, Theodore L., additional, Wang, Lynn, additional, Raymond, Kyle, additional, Starke, Carly E., additional, Mudd, Joseph C., additional, Chen, Wenxuan, additional, Smullin, Carolyn, additional, Matus-Nicodemos, Rodrigo, additional, Hoh, Rebecca, additional, Krone, Melissa, additional, Hecht, Frederick M., additional, Pilcher, Christopher D., additional, Martin, Jeffrey N., additional, Koup, Richard A., additional, Douek, Daniel C., additional, Brenchley, Jason M., additional, Sékaly, Rafick-Pierre, additional, Pillai, Satish K., additional, Marson, Alexander, additional, Deeks, Steven G., additional, McCune, Joseph M., additional, and Hunt, Peter W., additional

Published
2020
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43. Single-Cell Mapping of Progressive Fetal-to-Adult Transition in Human Hematopoiesis

Author

Bunis, Daniel, primary, Bronevetsky, Yelena, additional, Krow-Lucal, Elisabeth, additional, Bhakta, Nirav R., additional, Kim, Charles C., additional, Nerella, Srilaxmi, additional, Jones, Norman, additional, Mendoza, Ventura F., additional, Bryson, Yvonne J., additional, Gern, James E., additional, Rutishauser, Rachel L., additional, Ye, Chun Jimmie, additional, Sirota, Marina, additional, McCune, Joseph M., additional, and Burt, Trevor D., additional

Published
2020
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44. Single-Cell Mapping of Progressive Fetal-to-Adult Transition in Human Naïve T Cells

Author

Bunis, Daniel, primary, Bronevetsky, Yelena, additional, Krow-Lucal, Elisabeth, additional, Bhakta, Nirav R., additional, Kim, Charles C., additional, Nerella, Srilaxmi, additional, Jones, Norman, additional, Mendoza, Ventura F., additional, Bryson, Yvonne J., additional, Gern, James E., additional, Rutishauser, Rachel L., additional, Ye, Chun Jimmie, additional, Sirota, Marina, additional, McCune, Joseph M., additional, and Burt, Trevor D., additional

Published
2020
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47. Beta cell-specific CD8+T cells maintain stem cell memory-associated epigenetic programs during type 1 diabetes

Author

Abdelsamed, Hossam A., Zebley, Caitlin C., Nguyen, Hai, Rutishauser, Rachel L., Fan, Yiping, Ghoneim, Hazem E., Crawford, Jeremy Chase, Alfei, Francesca, Alli, Shanta, Ribeiro, Susan Pereira, Castellaw, Ashley H., McGargill, Maureen A., Jin, Hongjian, Boi, Shannon K., Speake, Cate, Serti, Elisavet, Turka, Laurence A., Busch, Michael E., Stone, Mars, Deeks, Steven G., Sekaly, Rafick-Pierre, Zehn, Dietmar, James, Eddie A., Nepom, Gerald T., and Youngblood, Ben

Abstract

The pool of beta cell-specific CD8+T cells in type 1 diabetes (T1D) sustains an autoreactive potential despite having access to a constant source of antigen. To investigate the long-lived nature of these cells, we established a DNA methylation-based T cell ‘multipotency index’ and found that beta cell-specific CD8+T cells retained a stem-like epigenetic multipotency score. Single-cell assay for transposase-accessible chromatin using sequencing confirmed the coexistence of naive and effector-associated epigenetic programs in individual beta cell-specific CD8+T cells. Assessment of beta cell-specific CD8+T cell anatomical distribution and the establishment of stem-associated epigenetic programs revealed that self-reactive CD8+T cells isolated from murine lymphoid tissue retained developmentally plastic phenotypic and epigenetic profiles relative to the same cells isolated from the pancreas. Collectively, these data provide new insight into the longevity of beta cell-specific CD8+T cell responses and document the use of this methylation-based multipotency index for investigating human and mouse CD8+T cell differentiation.

Published
2020
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