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1. Delayed Expression of PD-1 and TIGIT on HIV-Specific CD8 T Cells in Untreated HLA-B*57:01 Individuals Followed from Early Infection

Author

Scharf, Lydia, Tauriainen, Johanna, Buggert, Marcus, Hartogensis, Wendy, Nolan, David J, Deeks, Steven G, Salemi, Marco, Hecht, Frederick M, and Karlsson, Annika C

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Immunization, Cancer, HIV/AIDS, Clinical Research, Sexually Transmitted Infections, Infectious Diseases, Immunotherapy, Genetics, Vaccine Related, Prevention, 2.1 Biological and endogenous factors, Infection, Good Health and Well Being, Adult, CD8-Positive T-Lymphocytes, Female, Gene Expression Regulation, HIV Infections, HIV-1, HLA-B Antigens, Humans, Male, Middle Aged, Programmed Cell Death 1 Receptor, Receptors, Immunologic, CD8-positive T lymphocytes, HIV Gag, human HLA-B*5701 antigen, disease progression, viral load, CD4, programmed cell death protein 1, PD-1, T-cell immunoreceptor with Ig and ITIM domain, TIGIT, cellular immunity, molecular evolution, evolution, Biological Sciences, Agricultural and Veterinary Sciences, Medical and Health Sciences, Virology, Agricultural, veterinary and food sciences, Biological sciences, Biomedical and clinical sciences
Abstract

While the relationship of protective human leukocyte antigen (HLA) class I alleles and HIV progression is well defined, the interaction of HLA-mediated protection and CD8 T-cell exhaustion is less well characterized. To gain insight into the influence of HLA-B*57:01 on the deterioration of CD8 T-cell responses during HIV infection in the absence of antiretroviral treatment, we compared HLA-B*57:01-restricted HIV-specific CD8 T-cell responses to responses restricted by other HLA class I alleles longitudinally after control of peak viremia. Detailed characterization of polyfunctionality, differentiation phenotypes, transcription factor, and inhibitory receptor expression revealed progression of CD8 T-cell exhaustion over the course of the infection in both patient groups. However, early effects on the phenotype of the total CD8 T-cell population were apparent only in HLA-B*57-negative patients. The HLA-B*57:01-restricted, HIV epitope-specific CD8 T-cell responses showed beneficial functional patterns and significantly lower frequencies of inhibitory receptor expression, i.e., PD-1 and coexpression of PD-1 and TIGIT, within the first year of infection. Coexpression of PD-1 and TIGIT was correlated with clinical markers of disease progression and declining percentages of the T-bethi Eomesdim CD8 T-cell population. In accordance with clinical and immunological deterioration in the HLA-B*57:01 group, the difference in PD-1 and TIGIT receptor expression did not persist to later stages of the disease.IMPORTANCE Given the synergistic nature of TIGIT and PD-1, the coexpression of those inhibitory receptors should be considered when evaluating T-cell pathogenesis, developing immunomodulatory therapies or vaccines for HIV, and when using immunotherapy or vaccination for other causes in HIV-infected patients. HIV-mediated T-cell exhaustion influences the patient´s disease progression, immune system and subsequently non-AIDS complications, and efficacy of vaccinations against other pathogens. Consequently, the possibilities of interfering with exhaustion are numerous. Expanding the use of immunomodulatory therapies to include HIV treatment depends on information about possible targets and their role in the deterioration of the immune system. Furthermore, the rise of immunotherapies against cancer and elevated cancer incidence in HIV-infected patients together increase the need for detailed knowledge of T-cell exhaustion and possible interactions. A broader approach to counteract immune exhaustion to alleviate complications and improve efficacy of other vaccines also promises to increase patients' health and quality of life.

Published
2020

2. Ancestral SARS-CoV-2-specific T cells cross-recognize the Omicron variant

Author

Gao, Yu, Cai, Curtis, Grifoni, Alba, Müller, Thomas R., Niessl, Julia, Olofsson, Anna, Humbert, Marion, Hansson, Lotta, Österborg, Anders, Bergman, Peter, Chen, Puran, Olsson, Annika, Sandberg, Johan K., Weiskopf, Daniela, Price, David A., Ljunggren, Hans-Gustaf, Karlsson, Annika C., Sette, Alessandro, Aleman, Soo, and Buggert, Marcus

Published
2022
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3. Limited immune surveillance in lymphoid tissue by cytolytic CD4+ T cells during health and HIV disease.

Author

Buggert, Marcus, Nguyen, Son, McLane, Laura M, Steblyanko, Maria, Anikeeva, Nadia, Paquin-Proulx, Dominic, Del Rio Estrada, Perla M, Ablanedo-Terrazas, Yuria, Noyan, Kajsa, Reuter, Morgan A, Demers, Korey, Sandberg, Johan K, Eller, Michael A, Streeck, Hendrik, Jansson, Marianne, Nowak, Piotr, Sönnerborg, Anders, Canaday, David H, Naji, Ali, Wherry, E John, Robb, Merlin L, Deeks, Steven G, Reyes-Teran, Gustavo, Sykulev, Yuri, Karlsson, Annika C, and Betts, Michael R

Subjects
Lymphoid Tissue, Lymph Nodes, CD4-Positive T-Lymphocytes, Humans, HIV-1, HIV Infections, Viral Load, Case-Control Studies, Immunologic Surveillance, Virology, Microbiology, Immunology, Medical Microbiology
Abstract

CD4+ T cells subsets have a wide range of important helper and regulatory functions in the immune system. Several studies have specifically suggested that circulating effector CD4+ T cells may play a direct role in control of HIV replication through cytolytic activity or autocrine β-chemokine production. However, it remains unclear whether effector CD4+ T cells expressing cytolytic molecules and β-chemokines are present within lymph nodes (LNs), a major site of HIV replication. Here, we report that expression of β-chemokines and cytolytic molecules are enriched within a CD4+ T cell population with high levels of the T-box transcription factors T-bet and eomesodermin (Eomes). This effector population is predominately found in peripheral blood and is limited in LNs regardless of HIV infection or treatment status. As a result, CD4+ T cells generally lack effector functions in LNs, including cytolytic capacity and IFNγ and β-chemokine expression, even in HIV elite controllers and during acute/early HIV infection. While we do find the presence of degranulating CD4+ T cells in LNs, these cells do not bear functional or transcriptional effector T cell properties and are inherently poor to form stable immunological synapses compared to their peripheral blood counterparts. We demonstrate that CD4+ T cell cytolytic function, phenotype, and programming in the peripheral blood is dissociated from those characteristics found in lymphoid tissues. Together, these data challenge our current models based on blood and suggest spatially and temporally dissociated mechanisms of viral control in lymphoid tissues.

Published
2018

4. Perturbed CD8+ T cell TIGIT/CD226/PVR axis despite early initiation of antiretroviral treatment in HIV infected individuals.

Author

Tauriainen, Johanna, Scharf, Lydia, Frederiksen, Juliet, Naji, Ali, Ljunggren, Hans-Gustaf, Sönnerborg, Anders, Lund, Ole, Reyes-Terán, Gustavo, Hecht, Frederick M, Deeks, Steven G, Betts, Michael R, Buggert, Marcus, and Karlsson, Annika C

Subjects
CD8-Positive T-Lymphocytes, Humans, HIV, HIV Infections, Receptors, Immunologic, Receptors, Virus, Antigens, Differentiation, T-Lymphocyte, Antiretroviral Therapy, Highly Active, Signal Transduction, Gene Expression Regulation, Adult, Middle Aged, Female, Male, Receptors, Immunologic, Virus, Antigens, Differentiation, T-Lymphocyte, Antiretroviral Therapy, Highly Active
Abstract

HIV-specific CD8+ T cells demonstrate an exhausted phenotype associated with increased expression of inhibitory receptors, decreased functional capacity, and a skewed transcriptional profile, which are only partially restored by antiretroviral treatment (ART). Expression levels of the inhibitory receptor, T cell immunoglobulin and ITIM domain (TIGIT), the co-stimulatory receptor CD226 and their ligand PVR are altered in viral infections and cancer. However, the extent to which the TIGIT/CD226/PVR-axis is affected by HIV-infection has not been characterized. Here, we report that TIGIT expression increased over time despite early initiation of ART. HIV-specific CD8+ T cells were almost exclusively TIGIT+, had an inverse expression of the transcription factors T-bet and Eomes and co-expressed PD-1, CD160 and 2B4. HIV-specific TIGIThi cells were negatively correlated with polyfunctionality and displayed a diminished expression of CD226. Furthermore, expression of PVR was increased on CD4+ T cells, especially T follicular helper (Tfh) cells, in HIV-infected lymph nodes. These results depict a skewing of the TIGIT/CD226 axis from CD226 co-stimulation towards TIGIT-mediated inhibition of CD8+ T cells, despite early ART. These findings highlight the importance of the TIGIT/CD226/PVR axis as an immune checkpoint barrier that could hinder future "cure" strategies requiring potent HIV-specific CD8+ T cells.

Published
2017

5. Correction: Rapid Progressing Allele HLA-B35 Px Restricted Anti-HIV-1 CD8+ T Cells Recognize Vestigial CTL Epitopes

Author

Willberg, Christian B, Garrison, Keith E, Jones, R Brad, Meiklejohn, Duncan A, Spotts, Gerald, Liegler, Teri J, Ostrowski, Mario A, Karlsson, Annika C, Hecht, Frederick M, and Nixon, Douglas F

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Immunization, Vaccine Related, HIV/AIDS, Sexually Transmitted Infections, Infectious Diseases, General Science & Technology
Abstract

[This corrects the article DOI: 10.1371/journal.pone.0010249.].

Published
2016

6. Functional Avidity and IL-2/Perforin Production Is Linked to the Emergence of Mutations within HLA-B*5701–Restricted Epitopes and HIV-1 Disease Progression

Author

Buggert, Marcus, Norström, Melissa M, Salemi, Marco, Hecht, Frederick M, and Karlsson, Annika C

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Vaccine Related, HIV/AIDS, Clinical Research, Immunization, Sexually Transmitted Infections, Infectious Diseases, Prevention, Aetiology, 2.1 Biological and endogenous factors, Infection, Good Health and Well Being, Base Sequence, Cell Cycle, Cytokines, Disease Progression, Epitopes, Gene Products, gag, HIV Infections, HIV-1, HLA-B Antigens, Humans, Interleukin-2, Male, Molecular Sequence Data, Mutation, Perforin, Up-Regulation, Biochemistry and cell biology
Abstract

Viral escape from HIV-1-specific CD8(+) T cells has been demonstrated in numerous studies previously. However, the qualitative features driving the emergence of mutations within epitopes are still unclear. In this study, we aimed to distinguish whether specific functional characteristics of HLA-B*5701-restricted CD8(+) T cells influence the emergence of mutations in high-risk progressors (HRPs) versus low-risk progressors (LRPs). Single-genome sequencing was performed to detect viral mutations (variants) within seven HLA-B*5701-restricted epitopes in Gag (n = 4) and Nef (n = 3) in six untreated HLA-B*5701 subjects followed from early infection up to 7 y. Several well-characterized effector markers (IFN-γ, IL-2, MIP-1β, TNF, CD107a, and perforin) were identified by flow cytometry following autologous (initial and emerging variant/s) epitope stimulations. This study demonstrates that specific functional attributes may facilitate the outgrowth of mutations within HLA-B*5701-restricted epitopes. A significantly lower fraction of IL-2-producing cells and a decrease in functional avidity and polyfunctional sensitivity were evident in emerging epitope variants compared with the initial autologous epitopes. Interestingly, the HRPs mainly drove these differences, whereas the LRPs maintained a directed and maintained functional response against emerging epitope variants. In addition, LRPs induced improved cell-cycle progression and perforin upregulation after autologous and emerging epitope variant stimulations in contrast to HRPs. The maintained quantitative and qualitative features of the CD8(+) T cell responses in LRPs toward emerging epitope variants provide insights into why HLA-B*5701 subjects have different risks of HIV-1 disease progression.

Published
2014

7. Targeting of Conserved Gag-Epitopes in Early HIV Infection Is Associated with Lower Plasma Viral Load and Slower CD4+ T Cell Depletion

Author

Perez, Carina L, Milush, Jeffrey M, Buggert, Marcus, Eriksson, Emily M, Larsen, Mette V, Liegler, Teri, Hartogensis, Wendy, Bacchetti, Peter, Lund, Ole, Hecht, Frederick M, Nixon, Douglas F, and Karlsson, Annika C

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Infectious Diseases, Sexually Transmitted Infections, HIV/AIDS, Clinical Research, Aetiology, 2.1 Biological and endogenous factors, Infection, Good Health and Well Being, CD8-Positive T-Lymphocytes, Cohort Studies, Disease Progression, Epitopes, Flow Cytometry, HIV, HIV Infections, Humans, Molecular Sequence Data, Plasma, RNA, Viral, San Francisco, Sequence Analysis, DNA, Viral Load, gag Gene Products, Human Immunodeficiency Virus, Clinical Sciences, Virology, Clinical sciences
Abstract

We aimed to investigate whether the character of the immunodominant HIV-Gag peptide (variable or conserved) targeted by CD8(+) T cells in early HIV infection would influence the quality and quantity of T cell responses, and whether this would affect the rate of disease progression. Treatment-naive HIV-infected study subjects within the OPTIONS cohort at the University of California, San Francisco, were monitored from an estimated 44 days postinfection for up to 6 years. CD8(+) T cells responses targeting HLA-matched HIV-Gag-epitopes were identified and characterized by multicolor flow cytometry. The autologous HIV gag sequences were obtained. We demonstrate that patients targeting a conserved HIV-Gag-epitope in early infection maintained their epitope-specific CD8(+) T cell response throughout the study period. Patients targeting a variable epitope showed decreased immune responses over time, although there was no limitation of the functional profile, and they were likely to target additional variable epitopes. Maintained immune responses to conserved epitopes were associated with no or limited sequence evolution within the targeted epitope. Patients with immune responses targeting conserved epitopes had a significantly lower median viral load over time compared to patients with responses targeting a variable epitope (0.63 log(10) difference). Furthermore, the rate of CD4(+) T cell decline was slower for subjects targeting a conserved epitope (0.85% per month) compared to subjects targeting a variable epitope (1.85% per month). Previous studies have shown that targeting of antigens based on specific HLA types is associated with a better disease course. In this study we show that categorizing epitopes based on their variability is associated with clinical outcome.

Published
2013

8. Combination of Immune and Viral Factors Distinguishes Low-Risk versus High-Risk HIV-1 Disease Progression in HLA-B*5701 Subjects

Author

Norström, Melissa M, Buggert, Marcus, Tauriainen, Johanna, Hartogensis, Wendy, Prosperi, Mattia C, Wallet, Mark A, Hecht, Frederick M, Salemi, Marco, and Karlsson, Annika C

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Immunization, Clinical Research, Vaccine Related, Infectious Diseases, Sexually Transmitted Infections, HIV/AIDS, Aetiology, 2.1 Biological and endogenous factors, Infection, Good Health and Well Being, CD4 Lymphocyte Count, CD8-Positive T-Lymphocytes, Disease Progression, Evolution, Molecular, HIV Core Protein p24, HIV Infections, HIV-1, HLA-B Antigens, Host-Pathogen Interactions, Humans, Likelihood Functions, Longitudinal Studies, Male, Molecular Sequence Data, Phylogeny, Risk Factors, Biological Sciences, Agricultural and Veterinary Sciences, Medical and Health Sciences, Virology, Agricultural, veterinary and food sciences, Biological sciences, Biomedical and clinical sciences
Abstract

HLA-B*5701 is the host factor most strongly associated with slow HIV-1 disease progression, although rates can vary within this group. Underlying mechanisms are not fully understood but likely involve both immunological and virological dynamics. The present study investigated HIV-1 in vivo evolution and epitope-specific CD8(+) T cell responses in six HLA-B*5701 patients who had not received antiretroviral treatment, monitored from early infection for up to 7 years. The subjects were classified as high-risk progressors (HRPs) or low-risk progressors (LRPs) based on baseline CD4(+) T cell counts. Dynamics of HIV-1 Gag p24 evolution and multifunctional CD8(+) T cell responses were evaluated by high-resolution phylogenetic analysis and polychromatic flow cytometry, respectively. In all subjects, substitutions occurred more frequently in flanking regions than in HLA-B*5701-restricted epitopes. In LRPs, p24 sequence diversity was significantly lower; sequences exhibited a higher degree of homoplasy and more constrained mutational patterns than HRPs. The HIV-1 intrahost evolutionary rate was also lower in LRPs and followed a strict molecular clock, suggesting neutral genetic drift rather than positive selection. Additionally, polyfunctional CD8(+) T cell responses, particularly to TW10 and QW9 epitopes, were more robust in LRPs, who also showed significantly higher interleukin-2 (IL-2) production in early infection. Overall, the findings indicate that HLA-B*5701 patients with higher CD4 counts at baseline have a lower risk of HIV-1 disease progression because of the interplay between specific HLA-linked immune responses and the rate and mode of viral evolution. The study highlights the power of a multidisciplinary approach, integrating high-resolution evolutionary and immunological data, to understand mechanisms underlying HIV-1 pathogenesis.

Published
2012

9. Sequential broadening of CTL responses in early HIV-1 infection is associated with viral escape.

Author

Karlsson, Annika C, Iversen, Astrid KN, Chapman, Joan M, de Oliviera, Tulio, Spotts, Gerald, McMichael, Andrew J, Davenport, Miles P, Hecht, Frederick M, and Nixon, Douglas F

Subjects
T-Lymphocytes, Cytotoxic, Humans, HIV-1, HIV Infections, Disease Progression, Tumor Necrosis Factor-alpha, HLA-A2 Antigen, HIV Antigens, Epitopes, Amino Acid Substitution, Sequence Alignment, Evolution, Molecular, Phylogeny, Base Sequence, Consensus Sequence, Sequence Homology, Nucleic Acid, Molecular Sequence Data, Female, Male, gag Gene Products, Human Immunodeficiency Virus, pol Gene Products, Human Immunodeficiency Virus, nef Gene Products, Human Immunodeficiency Virus, Interferon-gamma, Immune Evasion, T-Lymphocytes, Cytotoxic, Evolution, Molecular, Sequence Homology, Nucleic Acid, gag Gene Products, Human Immunodeficiency Virus, pol Gene Products, nef Gene Products, General Science & Technology
Abstract

BackgroundAntigen-specific CTL responses are thought to play a central role in containment of HIV-1 infection, but no consistent correlation has been found between the magnitude and/or breadth of response and viral load changes during disease progression.Methods and findingsWe undertook a detailed investigation of longitudinal CTL responses and HIV-1 evolution beginning with primary infection in 11 untreated HLA-A2 positive individuals. A subset of patients developed broad responses, which selected for consensus B epitope variants in Gag, Pol, and Nef, suggesting CTL-induced adaptation of HIV-1 at the population level. The patients who developed viral escape mutations and broad autologous CTL responses over time had a significantly higher increase in viral load during the first year of infection compared to those who did not develop viral escape mutations.ConclusionsA continuous dynamic development of CTL responses was associated with viral escape from temporarily effective immune responses. Our results suggest that broad CTL responses often represent footprints left by viral CTL escape rather than effective immune control, and help explain earlier findings that fail to show an association between breadth of CTL responses and viral load. Our results also demonstrate that CTL pressures help to maintain certain elements of consensus viral sequence, which likely represent viral escape from common HLA-restricted CTL responses. The ability of HIV to evolve to escape CTL responses restricted by a common HLA type highlights the challenges posed to development of an effective CTL-based vaccine.

Published
2007

10. Functional SARS-CoV-2 cross-reactive CD4 + T cells established in early childhood decline with age

Author

Humbert, Marion, primary, Olofsson, Anna, additional, Wullimann, David, additional, Niessl, Julia, additional, Hodcroft, Emma B., additional, Cai, Curtis, additional, Gao, Yu, additional, Sohlberg, Ebba, additional, Dyrdak, Robert, additional, Mikaeloff, Flora, additional, Neogi, Ujjwal, additional, Albert, Jan, additional, Malmberg, Karl-Johan, additional, Lund-Johansen, Fridtjof, additional, Aleman, Soo, additional, Björkhem-Bergman, Linda, additional, Jenmalm, Maria C., additional, Ljunggren, Hans-Gustaf, additional, Buggert, Marcus, additional, and Karlsson, Annika C., additional

Published
2023
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11. Additive effects of booster mRNA vaccination and SARS-CoV-2 Omicron infection on T cell immunity across immunocompromised states

Author

Müller, Thomas R., Sekine, Takuya, Trubach, Darya, Niessl, Julia, Chen, Puran, Bergman, Peter, Blennow, Ola, Hansson, Lotta, Mielke, Stephan, Nowak, Piotr, Vesterbacka, Jan, Akber, Mira, Olofsson, Anna, Amaya Hernandez, Susana Patricia, Gao, Yu, Cai, Curtis, Söderdahl, Gunnar, Smith, C I Edvard, Österborg, Anders, Loré, Karin, Sällberg Chen, Margaret, Ljungman, Per, Ljunggren, Hans-Gustaf, Karlsson, Annika C., Saini, Sunil Kumar, Aleman, Soo, Buggert, Marcus, Müller, Thomas R., Sekine, Takuya, Trubach, Darya, Niessl, Julia, Chen, Puran, Bergman, Peter, Blennow, Ola, Hansson, Lotta, Mielke, Stephan, Nowak, Piotr, Vesterbacka, Jan, Akber, Mira, Olofsson, Anna, Amaya Hernandez, Susana Patricia, Gao, Yu, Cai, Curtis, Söderdahl, Gunnar, Smith, C I Edvard, Österborg, Anders, Loré, Karin, Sällberg Chen, Margaret, Ljungman, Per, Ljunggren, Hans-Gustaf, Karlsson, Annika C., Saini, Sunil Kumar, Aleman, Soo, and Buggert, Marcus

Abstract

Suboptimal immunity to SARS-CoV-2 mRNA vaccination has frequently been observed in individuals with various immunodeficiencies. Given the increased antibody evasion properties of emerging SARS-CoV-2 subvariants, it is necessary to assess whether other components of adaptive immunity generate resilient and protective responses against infection. We assessed T cell responses in 279 individuals, covering five different immunodeficiencies and healthy controls, before and after booster mRNA vaccination, as well as after Omicron infection in a subset of patients. We observed robust and persistent Omicron-reactive T cell responses that increased markedly upon booster vaccination and correlated directly with antibody titers across all patient groups. Poor vaccination responsiveness in immunocompromised or elderly individuals was effectively counteracted by the administration of additional vaccine doses. Functionally, Omicron-reactive T cell responses exhibited a pronounced cytotoxic profile and signs of longevity, characterized by CD45RA+ effector memory subpopulations with stem cell-like properties and increased proliferative capacity. Regardless of underlying immunodeficiency, booster-vaccinated and Omicron-infected individuals appeared protected against severe disease and exhibited enhanced and diversified T cell responses against conserved and Omicron-specific epitopes. Our findings indicate that T cells retain the ability to generate highly functional responses against newly emerging variants, even after repeated antigen exposure and a robust immunological imprint from ancestral SARS-CoV-2 mRNA vaccination.

Published
2023
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12. Hierarchical Clustering and Trajectory Analyses Reveal Viremia-Independent B-Cell Perturbations in HIV-2 Infection

Author

Johansson, Emil, Kerkman, Priscilla, Scharf, Lydia, Lindman, Jacob, Szojka, Zsófia I., Månsson, Fredrik, Biague, Antonio, Medstrand, Patrik, Norrgren, Hans, Buggert, Marcus, Karlsson, Annika C., Forsell, Mattias N. E., Esbjörnsson, Joakim, Jansson, Marianne, Johansson, Emil, Kerkman, Priscilla, Scharf, Lydia, Lindman, Jacob, Szojka, Zsófia I., Månsson, Fredrik, Biague, Antonio, Medstrand, Patrik, Norrgren, Hans, Buggert, Marcus, Karlsson, Annika C., Forsell, Mattias N. E., Esbjörnsson, Joakim, and Jansson, Marianne

Abstract

Time to AIDS in HIV-2 infection is approximately twice as long compared to in HIV-1 infection. Despite reduced viremia, HIV-2-infected individuals display signs of chronic immune activation. In HIV-1-infected individuals, B-cell hyperactivation is driven by continuous antigen exposure. However, the contribution of viremia to B-cell perturbations in HIV-2-infected individuals remains largely unexplored. Here, we used polychromatic flow cytometry, consensus hierarchical clustering and pseudotime trajectory inference to characterize B-cells in HIV-1- or HIV-2-infected and in HIV seronegative individuals. We observed increased frequencies of clusters containing hyperactivated T-bethighCD95highCD27int and proliferating T-bet+CD95highCD27+CD71+ memory B-cells in viremic HIV-1 (p < 0.001 and p < 0.001, respectively), viremic HIV-2 (p < 0.001 and p = 0.014, respectively) and in treatment-naïve aviremic HIV-2 (p = 0.004 and p = 0.020, respectively)-infected individuals, compared to seronegative individuals. In contrast, these expansions were not observed in successfully treated HIV-1-infected individuals. Finally, pseudotime trajectory inference showed that T-bet-expressing hyperactivated and proliferating memory B-cell populations were located at the terminal end of two trajectories, in both HIV-1 and HIV-2 infections. As the treatment-naïve aviremic HIV-2-infected individuals, but not the successfully ART-treated HIV-1-infected individuals, showed B-cell perturbations, our data suggest that aviremic HIV-2-infected individuals would also benefit from antiretroviral treatment.

Published
2022
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13. Ancestral SARS-CoV-2-specific T cells cross-recognize Omicron

Author

Gao, Yu, primary, Cai, Curtis, additional, Grifoni, Alba, additional, Müller, Thomas R., additional, Niessl, Julia, additional, Olofsson, Anna, additional, Humbert, Marion, additional, Hansson, Lotta, additional, Österborg, Anders, additional, Bergman, Peter, additional, Chen, Puran, additional, Olsson, Annika, additional, Sandberg, Johan K., additional, Weiskopf, Daniela, additional, Price, David A., additional, Ljunggren, Hans-Gustaf, additional, Karlsson, Annika C., additional, Sette, Alessandro, additional, Aleman, Soo, additional, and Buggert, Marcus, additional

Published
2022
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17. Identification of resident memory CD8+ T cells with functional specificity for SARS-CoV-2 in unexposed oropharyngeal lymphoid tissue

Author

Niessl, Julia, Sekine, Takuya, Lange, Joshua, Konya, Viktoria, Forkel, Marianne, Maric, Jovana, Rao, Anna, Mazzurana, Luca, Kokkinou, Efthymia, Weigel, Whitney, Llewellyn-Lacey, Sian, Hodcroft, Emma B., Karlsson, Annika C., Fehrm, Johan, Sundman, Joar, Price, David A., Mjösberg, Jenny, Friberg, Danielle, Buggert, Marcus, Niessl, Julia, Sekine, Takuya, Lange, Joshua, Konya, Viktoria, Forkel, Marianne, Maric, Jovana, Rao, Anna, Mazzurana, Luca, Kokkinou, Efthymia, Weigel, Whitney, Llewellyn-Lacey, Sian, Hodcroft, Emma B., Karlsson, Annika C., Fehrm, Johan, Sundman, Joar, Price, David A., Mjösberg, Jenny, Friberg, Danielle, and Buggert, Marcus

Abstract

Cross-reactive CD4+ T cells that recognize severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) are more commonly detected in the peripheral blood of unexposed individuals compared with SARS-CoV-2–reactive CD8+ T cells. However, large numbers of memory CD8+ T cells reside in tissues, feasibly harboring localized SARS-CoV-2–specific immune responses. To test this idea, we performed a comprehensive functional and phenotypic analysis of virus-specific T cells in tonsils, a major lymphoid tissue site in the upper respiratory tract, and matched peripheral blood samples obtained from children and adults before the emergence of COVID-19 (coronavirus disease 2019). We found that SARS-CoV-2–specific memory CD4+ T cells could be found at similar frequencies in the tonsils and peripheral blood in unexposed individuals, whereas functional SARS-CoV-2–specific memory CD8+ T cells were almost only detectable in the tonsils. Tonsillar SARS-CoV-2–specific memory CD8+ T cells displayed a follicular homing and tissue-resident memory phenotype, similar to tonsillar Epstein-Barr virus–specific memory CD8+ T cells, but were functionally less potent than other virus-specific memory CD8+ T cell responses. The presence of preexisting tissue-resident memory CD8+ T cells in unexposed individuals could potentially enable rapid sentinel immune responses against SARS-CoV-2., Title in Web of Science: Identification of resident memory CD8(+) T cells with functional specificity for SARS-CoV-2 in unexposed oropharyngeal lymphoid tissue

Published
2021
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18. Inverted CD8 T-Cell Exhaustion and Co-Stimulation Marker Balance Differentiate Aviremic HIV-2-Infected From Seronegative Individuals

Author

Scharf, Lydia, Pedersen, Christina B., Johansson, Emil, Lindman, Jacob, Olsen, Lars R, Buggert, Marcus, Wilhelmson, Sten, Månsson, Fredrik, Esbjörnsson, Joakim, Biague, Antonio, Medstrand, Patrik, Norrgren, Hans, Karlsson, Annika C., Jansson, Marianne, Scharf, Lydia, Pedersen, Christina B., Johansson, Emil, Lindman, Jacob, Olsen, Lars R, Buggert, Marcus, Wilhelmson, Sten, Månsson, Fredrik, Esbjörnsson, Joakim, Biague, Antonio, Medstrand, Patrik, Norrgren, Hans, Karlsson, Annika C., and Jansson, Marianne

Abstract

HIV-2 is less pathogenic compared to HIV-1. Still, disease progression may develop in aviremic HIV-2 infection, but the driving forces and mechanisms behind such development are unclear. Here, we aimed to reveal the immunophenotypic pattern associated with CD8 T-cell pathology in HIV-2 infection, in relation to viremia and markers of disease progression. The relationships between pathological differences of the CD8 T-cell memory population and viremia were analyzed in blood samples obtained from an occupational cohort in Guinea-Bissau, including HIV-2 viremic and aviremic individuals. For comparison, samples from HIV-1- or dually HIV-1/2-infected and seronegative individuals were obtained from the same cohort. CD8 T-cell exhaustion was evaluated by the combined expression patterns of activation, stimulatory and inhibitory immune checkpoint markers analyzed using multicolor flow cytometry and advanced bioinformatics. Unsupervised multidimensional clustering analysis identified a cluster of late differentiated CD8 T-cells expressing activation (CD38+, HLA-DRint/high), co-stimulatory (CD226+/-), and immune inhibitory (2B4+, PD-1high, TIGIThigh) markers that distinguished aviremic from viremic HIV-2, and treated from untreated HIV-1-infected individuals. This CD8 T-cell population displayed close correlations to CD4%, viremia, and plasma levels of IP-10, sCD14 and beta-2 microglobulin in HIV-2 infection. Detailed analysis revealed that aviremic HIV-2-infected individuals had higher frequencies of exhausted TIGIT+ CD8 T-cell populations lacking CD226, while reduced percentage of stimulation-receptive TIGIT-CD226+ CD8 T-cells, compared to seronegative individuals. Our results suggest that HIV-2 infection, independent of viremia, skews CD8 T-cells towards exhaustion and reduced co-stimulation readiness. Further knowledge on CD8 T-cell phenotypes might provide help in therapy monitoring and identification of immunotherapy targets.

Published
2021

19. The known unknowns of T cell immunity to COVID-19

Author

Karlsson, Annika C., Humbert, Marion, and Buggert, Marcus

Subjects
0301 basic medicine, 2019-20 coronavirus outbreak, Coronavirus disease 2019 (COVID-19), T-Lymphocytes, T cell, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Immunology, Cellular Immunology, Antibodies, Viral, 03 medical and health sciences, 0302 clinical medicine, Immunity, medicine, T cell immunity, Humans, Pandemics, Immunity, Cellular, biology, SARS-CoV-2, COVID-19, General Medicine, biochemical phenomena, metabolism, and nutrition, Immunity, Humoral, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Host-Pathogen Interactions, biology.protein, Antibody, Immunologic Memory
Abstract

Tremendous progress has been made in understanding the role of T cell immunity in acute and convalescent COVID-19 infection. Here we shed light on the "known unknowns" of pre-existing and acquired T cell responses in relation to acute and convalescent SARS-CoV-2 infection.

Published
2020

20. Seroreversion in subjects receiving antiretroviral therapy during acute/early HIV infection

Author

Hare, C. Bradley, Pappalardo, Brandee L., Busch, Michael P., Karlsson, Annika C., Phelps, Bruce H., Alexander, Steven S., Bentsen, Christopher, Ramstead, Clarissa A., Nixon, Douglas F., Levy, Jay A., and Hecht, Frederick M.

Subjects
Antiviral agents -- Usage, HIV infection -- Care and treatment, Health, Health care industry, University of California -- Services
Published
2006

24. Viral dynamics in primary HIV-1 infection

Author

Lindbäck, Stefan, Karlsson, Annika C., Mittler, John, Blaxhult, Anders, Carlsson, Mikael, Briheim, Gunnar, Sönnerborg, Anders, and Gaines, Hans

Published
2000

26. Reduction of the HIV-1 reservoir in resting CD4+ T-lymphocytes by high dosage intravenous immunoglobulin treatment: a proof-of-concept study

Author

Karlsson Annika C, Svennerholm Bo, Nilsson Staffan, Gonzalez Veronica D, Norström Melissa M, Edén Arvid, Lindkvist Annica, Sandberg Johan K, Sönnerborg Anders, and Gisslén Magnus

Subjects
Immunologic diseases. Allergy, RC581-607
Abstract

Abstract Background The latency of HIV-1 in resting CD4+ T-lymphocytes constitutes a major obstacle for the eradication of virus in patients on antiretroviral therapy (ART). As yet, no approach to reduce this viral reservoir has proven effective. Methods Nine subjects on effective ART were included in the study and treated with high dosage intravenous immunoglobulin (IVIG) for five consecutive days. Seven of those had detectable levels of replication-competent virus in the latent reservoir and were thus possible to evaluate. Highly purified resting memory CD4+ T-cells were activated and cells containing replication-competent HIV-1 were quantified. HIV-1 from plasma and activated memory CD4+ T-cells were compared with single genome sequencing (SGS) of the gag region. T-lymphocyte activation markers and serum interleukins were measured. Results The latent HIV-1 pool decreased with in median 68% after IVIG was added to effective ART. The reservoir decreased in five, whereas no decrease was found in two subjects with detectable virus. Plasma HIV-1 RNA ≥ 2 copies/mL was detected in five of seven subjects at baseline, but in only one at follow-up after 8–12 weeks. The decrease of the latent HIV-1 pool and the residual plasma viremia was preceded by a transitory low-level increase in plasma HIV-1 RNA and serum interleukin 7 (IL-7) levels, and followed by an expansion of T regulatory cells. The magnitude of the viral increase in plasma correlated to the size of the latent HIV-1 pool and SGS of the gag region showed that viral clones from plasma clustered together with virus from activated memory T-cells, pointing to the latent reservoir as the source of HIV-1 RNA in plasma. Conclusion The findings from this uncontrolled proof-of-concept study suggest that the reservoir became accessible by IVIG treatment through activation of HIV-1 gene expression in latently-infected resting CD4+ T-cells. We propose that IVIG should be further evaluated as an adjuvant to effective ART.

Published
2009
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27. Human Immunodeficiency Virus-Infected Women Have High Numbers of CD103-CD8+ T Cells Residing Close to the Basal Membrane of the Ectocervical Epithelium

Author

Gibbs, Anna, Buggert, Marcus, Edfeldt, Gabriella, Ranefall, Petter, Introini, Andrea, Cheuk, Stanley, Martini, Elisa, Eidsmo, Liv, Ball, Terry B., Kimani, Joshua, Kaul, Rupert, Karlsson, Annika C., Wählby, Carolina, Broliden, Kristina, Tjernlund, Annelie, Gibbs, Anna, Buggert, Marcus, Edfeldt, Gabriella, Ranefall, Petter, Introini, Andrea, Cheuk, Stanley, Martini, Elisa, Eidsmo, Liv, Ball, Terry B., Kimani, Joshua, Kaul, Rupert, Karlsson, Annika C., Wählby, Carolina, Broliden, Kristina, and Tjernlund, Annelie

Published
2018
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28. Increased numbers of CD103-CD8+ TRM cells in the cervical mucosa of HIV-infected women

Author

Gibbs, Anna, Buggert, Marcus, Edfeldt, Gabriella, Ranefall, Petter, Introini, Andrea, Cheuk, Stanley, Martini, Elisa, Eidsmo, Liv, Hirbod, Taha, Ball, Terry B., Kimani, Joshua, Kaul, Rupert, Karlsson, Annika C., Wählby, Carolina, Broliden, Kristina, Tjernlund, Annelie, Gibbs, Anna, Buggert, Marcus, Edfeldt, Gabriella, Ranefall, Petter, Introini, Andrea, Cheuk, Stanley, Martini, Elisa, Eidsmo, Liv, Hirbod, Taha, Ball, Terry B., Kimani, Joshua, Kaul, Rupert, Karlsson, Annika C., Wählby, Carolina, Broliden, Kristina, and Tjernlund, Annelie

Published
2017
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29. Combined immunodeficiency and Epstein-Barr virus-induced B cell malignancy in humans with inherited CD70 deficiency

Author

Abolhassani, Hassan, Edwards, Emily S. J., Ikinciogullari, Aydan, Jing, Huie, Borte, Stephan, Buggert, Marcus, Du, Likun, Matsuda-Lennikov, Mami, Romano, Rosa, Caridha, Rozina, Bade, Sangeeta, Zhang, Yu, Frederiksen, Juliet Wairimu, Fang, Mingyan, Bal, Sevgi Kostel, Haskologlu, Sule, Dogu, Figen, Tacyildiz, Nurdan, Matthews, Helen F., McElwee, Joshua J, Gostick, Emma, Price, David A., Palendira, Umaimainthan, Aghamohammadi, Asghar, Boisson, Bertrand, Rezaei, Nima, Karlsson, Annika C, Lenardo, Michael J., Casanova, Jean-Laurent, Hammarström, Lennart, Tangye, Stuart G., Su, Helen C, Pan-Hammarström, Qiang, Abolhassani, Hassan, Edwards, Emily S. J., Ikinciogullari, Aydan, Jing, Huie, Borte, Stephan, Buggert, Marcus, Du, Likun, Matsuda-Lennikov, Mami, Romano, Rosa, Caridha, Rozina, Bade, Sangeeta, Zhang, Yu, Frederiksen, Juliet Wairimu, Fang, Mingyan, Bal, Sevgi Kostel, Haskologlu, Sule, Dogu, Figen, Tacyildiz, Nurdan, Matthews, Helen F., McElwee, Joshua J, Gostick, Emma, Price, David A., Palendira, Umaimainthan, Aghamohammadi, Asghar, Boisson, Bertrand, Rezaei, Nima, Karlsson, Annika C, Lenardo, Michael J., Casanova, Jean-Laurent, Hammarström, Lennart, Tangye, Stuart G., Su, Helen C, and Pan-Hammarström, Qiang

Abstract

In this study, we describe four patients from two unrelated families of different ethnicities with a primary immunodeficiency, predominantly manifesting as susceptibility to Epstein-Barr virus (EBV)-related diseases. Three patients presented with EBV-associated Hodgkin's lymphoma and hypogammaglobulinemia; one also had severe varicella infection. The fourth had viral encephalitis during infancy. Homozygous frameshift or in-frame deletions in CD70 in these patients abolished either CD70 surface expression or binding to its cognate receptor CD27. Blood lymphocyte numbers were normal, but the proportions of memory B cells and EBV-specific effector memory CD8+ T cells were reduced. Furthermore, although T cell proliferation was normal, in vitro-generated EBV-specific cytotoxic T cell activity was reduced because of CD70 deficiency. This reflected impaired activation by, rather than effects during killing of, EBV-transformed B cells. Notably, expression of 2B4 and NKG2D, receptors implicated in controlling EBV infection, on memory CD8+ T cells from CD70-deficient individuals was reduced, consistent with their impaired killing of EBV-infected cells. Thus, autosomal recessive CD70 deficiency is a novel cause of combined immunodeficiency and EBV-associated diseases, reminiscent of inherited CD27 deficiency. Overall, human CD70-CD27 interactions therefore play a nonredundant role in T and B cell-mediated immunity, especially for protection against EBV and humoral immunity.

Published
2017

31. Combined immunodeficiency and Epstein-Barr virus–induced B cell malignancy in humans with inherited CD70 deficiency

Author

Abolhassani, Hassan, primary, Edwards, Emily S.J., additional, Ikinciogullari, Aydan, additional, Jing, Huie, additional, Borte, Stephan, additional, Buggert, Marcus, additional, Du, Likun, additional, Matsuda-Lennikov, Mami, additional, Romano, Rosa, additional, Caridha, Rozina, additional, Bade, Sangeeta, additional, Zhang, Yu, additional, Frederiksen, Juliet, additional, Fang, Mingyan, additional, Bal, Sevgi Kostel, additional, Haskologlu, Sule, additional, Dogu, Figen, additional, Tacyildiz, Nurdan, additional, Matthews, Helen F., additional, McElwee, Joshua J., additional, Gostick, Emma, additional, Price, David A., additional, Palendira, Umaimainthan, additional, Aghamohammadi, Asghar, additional, Boisson, Bertrand, additional, Rezaei, Nima, additional, Karlsson, Annika C., additional, Lenardo, Michael J., additional, Casanova, Jean-Laurent, additional, Hammarström, Lennart, additional, Tangye, Stuart G., additional, Su, Helen C., additional, and Pan-Hammarström, Qiang, additional

Published
2016
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32. Analysis of the distribution of CD103 on CD8 T cells in blood and genital mucosa of HIV-infected female sex workers

Author

Gibbs, Anna, Buggert, Marcus, Ranefall, Petter, Introini, Andrea, Cheuk, Stanley, Eidsmo, Liv, Hirbod, Taha, Ball, Terry B., Kimani, Joshua, Kaul, Rupert, Karlsson, Annika C., Wählby, Carolina, Broliden, Kristina, Tjernlund, Annelie, Gibbs, Anna, Buggert, Marcus, Ranefall, Petter, Introini, Andrea, Cheuk, Stanley, Eidsmo, Liv, Hirbod, Taha, Ball, Terry B., Kimani, Joshua, Kaul, Rupert, Karlsson, Annika C., Wählby, Carolina, Broliden, Kristina, and Tjernlund, Annelie

Published
2016

33. Single-cell characterization of in vitro migration and interaction dynamics of T cells expanded with IL-2 and IL-7

Author

Tauriainen, Johanna, Gustafsson, Karin, Göthlin, Mårten, Gertow, Jens, Buggert, Marcus, Frisk, Thomas W., Karlsson, Annika C., Uhlin, Michael, Önfelt, Björn, Tauriainen, Johanna, Gustafsson, Karin, Göthlin, Mårten, Gertow, Jens, Buggert, Marcus, Frisk, Thomas W., Karlsson, Annika C., Uhlin, Michael, and Önfelt, Björn

Abstract

T cells are pivotal in the immune defense against cancers and infectious agents. To mount an effector response against cancer cells, T cells need to migrate to the cancer-site, engage in contacts with cancer cells, and perform their effector functions. Adoptive T cell therapy is an effective strategy as treatment of complications such as relapse or opportunistic infections after hematopoietic stem cell transplantations. This requires a sufficient amount of cells that are able to expand and respond to tumor or viral antigens. The cytokines interleukin (IL)-2 and IL-7 drive T cell differentiation, proliferation, and survival and are commonly used to expand T cells ex vivo. Here, we have used microchip-based live-cell imaging to follow the migration of individual T cells, their interactions with allogeneic monocytes, cell division, and apoptosis for extended periods of time; something that cannot be achieved by commonly used methods. Our data indicate that cells grown in IL-7 + IL-2 had similar migration and contact dynamics as cells grown in IL-2 alone. However, the addition of IL-7 decreased cell death creating a more viable cell population, which should be beneficial when preparing cells for immunotherapy., QC 20150617

Published
2015
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34. Multidimensional Clusters of CD4+T Cell Dysfunction Are Primarily Associated with the CD4/CD8 Ratio in Chronic HIV Infection

Author

Frederiksen, Juliet Wairimu, Buggert, Marcus, Noyan, Kajsa, Nowak, Piotr, Sönnerborg, Anders, Lund, Ole, Karlsson, Annika C., Frederiksen, Juliet Wairimu, Buggert, Marcus, Noyan, Kajsa, Nowak, Piotr, Sönnerborg, Anders, Lund, Ole, and Karlsson, Annika C.

Abstract

HIV infection provokes a myriad of pathological effects on the immune system where many markers of CD4+ T cell dysfunction have been identified. However, most studies to date have focused on single/double measurements of immune dysfunction, while the identification of pathological CD4+ T cell clusters that is highly associated to a specific biomarker for HIV disease remain less studied. Here, multi-parametric flow cytometry was used to investigate immune activation, exhaustion, and senescence of diverse maturation phenotypes of CD4+ T cells. The traditional method of manual data analysis was compared to a multidimensional clustering tool, FLOw Clustering with K (FLOCK) in two cohorts of 47 untreated HIV-infected individuals and 21 age and sex matched healthy controls. In order to reduce the subjectivity of FLOCK, we developed an "artificial reference", using 2% of all CD4+ gated T cells from each of the HIV-infected individuals. Principle component analyses demonstrated that using an artificial reference lead to a better separation of the HIV-infected individuals from the healthy controls as compared to using a single HIV-infected subject as a reference or analyzing data manually. Multiple correlation analyses between laboratory parameters and pathological CD4+ clusters revealed that the CD4/CD8 ratio was the preeminent surrogate marker of CD4+ T cells dysfunction using all three methods. Increased frequencies of an early-differentiated CD4+ T cell cluster with high CD38, HLA-DR and PD-1 expression were best correlated (Rho = -0.80, P value = 1.96x10-11) with HIV disease progression as measured by the CD4/CD8 ratio. The novel approach described here can be used to identify cell clusters that distinguish healthy from HIV infected subjects and is biologically relevant for HIV disease progression. These results further emphasize that a simple measurement of the CD4/CD8 ratio is a useful biomarker for assessment of combined CD4+ T cell dysfunction in chronic

Published
2015

38. T-bet and Eomes Are Differentially Linked to the Exhausted Phenotype of CD8+ T Cells in HIV Infection.

Author

Buggert, Marcus, Tauriainen, Johanna, Yamamoto, Takuya, Frederiksen, Juliet, Ivarsson, Martin A, Michaëlsson, Jakob, Lund, Ole, Hejdeman, Bo, Jansson, Marianne, Sönnerborg, Anders, Koup, Richard A, Betts, Michael R, Karlsson, Annika C, Buggert, Marcus, Tauriainen, Johanna, Yamamoto, Takuya, Frederiksen, Juliet, Ivarsson, Martin A, Michaëlsson, Jakob, Lund, Ole, Hejdeman, Bo, Jansson, Marianne, Sönnerborg, Anders, Koup, Richard A, Betts, Michael R, and Karlsson, Annika C

Abstract

CD8+ T cell exhaustion represents a major hallmark of chronic HIV infection. Two key transcription factors governing CD8+ T cell differentiation, T-bet and Eomesodermin (Eomes), have previously been shown in mice to differentially regulate T cell exhaustion in part through direct modulation of PD-1. Here, we examined the relationship between these transcription factors and the expression of several inhibitory receptors (PD-1, CD160, and 2B4), functional characteristics and memory differentiation of CD8+ T cells in chronic and treated HIV infection. The expression of PD-1, CD160, and 2B4 on total CD8+ T cells was elevated in chronically infected individuals and highly associated with a T-betdimEomeshi expressional profile. Interestingly, both resting and activated HIV-specific CD8+ T cells in chronic infection were almost exclusively T-betdimEomeshi cells, while CMV-specific CD8+ T cells displayed a balanced expression pattern of T-bet and Eomes. The T-betdimEomeshi virus-specific CD8+ T cells did not show features of terminal differentiation, but rather a transitional memory phenotype with poor polyfunctional (effector) characteristics. The transitional and exhausted phenotype of HIV-specific CD8+ T cells was longitudinally related to persistent Eomes expression after antiretroviral therapy (ART) initiation. Strikingly, these characteristics remained stable up to 10 years after ART initiation. This study supports the concept that poor human viral-specific CD8+ T cell functionality is due to an inverse expression balance between T-bet and Eomes, which is not reversed despite long-term viral control through ART. These results aid to explain the inability of HIV-specific CD8+ T cells to control the viral replication post-ART cessation.

Published
2014

39. T-bet and Eomes Are Differentially Linked to the Exhausted Phenotype of CD8+T Cells in HIV Infection

Author

Buggert, Marcus, Tauriainen, Johanna, Yamamoto, Takuya, Frederiksen, Juliet Wairimu, Ivarsson, Martin A., Michaelsson, Jakob, Lund, Ole, Hejdeman, Bo, Jansson, Marianne, Sonnerborg, Anders, Koup, Richard A., Betts, Michael R., Karlsson, Annika C., Buggert, Marcus, Tauriainen, Johanna, Yamamoto, Takuya, Frederiksen, Juliet Wairimu, Ivarsson, Martin A., Michaelsson, Jakob, Lund, Ole, Hejdeman, Bo, Jansson, Marianne, Sonnerborg, Anders, Koup, Richard A., Betts, Michael R., and Karlsson, Annika C.

Abstract

CD8+ T cell exhaustion represents a major hallmark of chronic HIV infection. Two key transcription factors governing CD8+ T cell differentiation, T-bet and Eomesodermin (Eomes), have previously been shown in mice to differentially regulate T cell exhaustion in part through direct modulation of PD-1. Here, we examined the relationship between these transcription factors and the expression of several inhibitory receptors (PD-1, CD160, and 2B4), functional characteristics and memory differentiation of CD8+ T cells in chronic and treated HIV infection. The expression of PD-1, CD160, and 2B4 on total CD8+ T cells was elevated in chronically infected individuals and highly associated with a T-betdimEomeshi expressional profile. Interestingly, both resting and activated HIV-specific CD8+ T cells in chronic infection were almost exclusively T-betdimEomeshi cells, while CMV-specific CD8+ T cells displayed a balanced expression pattern of T-bet and Eomes. The T-betdimEomeshi virus-specific CD8+ T cells did not show features of terminal differentiation, but rather a transitional memory phenotype with poor polyfunctional (effector) characteristics. The transitional and exhausted phenotype of HIV-specific CD8+ T cells was longitudinally related to persistent Eomes expression after antiretroviral therapy (ART) initiation. Strikingly, these characteristics remained stable up to 10 years after ART initiation. This study supports the concept that poor human viral-specific CD8+ T cell functionality is due to an inverse expression balance between T-bet and Eomes, which is not reversed despite long-term viral control through ART. These results aid to explain the inability of HIV-specific CD8+ T cells to control the viral replication post-ART cessation.

Published
2014

42. T-bet and Eomes Are Differentially Linked to the Exhausted Phenotype of CD8+ T Cells in HIV Infection

Author

Buggert, Marcus, primary, Tauriainen, Johanna, additional, Yamamoto, Takuya, additional, Frederiksen, Juliet, additional, Ivarsson, Martin A., additional, Michaëlsson, Jakob, additional, Lund, Ole, additional, Hejdeman, Bo, additional, Jansson, Marianne, additional, Sönnerborg, Anders, additional, Koup, Richard A., additional, Betts, Michael R., additional, and Karlsson, Annika C., additional

Published
2014
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43. Targeting of conserved gag-epitopes in early HIV infection is associated with lower plasma viral load and slower CD4+ T cell depletion.

Author

Perez, Carina L., Milush, Jeffrey M., Buggert, Marcus, Eriksson, Emily M., Larsen, Mette Voldby, Liegler, Teri, Hartogensis, Wendy, Bacchetti, Peter, Lund, Ole, Hecht, Frederick M., Nixon, Douglas F., Karlsson, Annika C., Perez, Carina L., Milush, Jeffrey M., Buggert, Marcus, Eriksson, Emily M., Larsen, Mette Voldby, Liegler, Teri, Hartogensis, Wendy, Bacchetti, Peter, Lund, Ole, Hecht, Frederick M., Nixon, Douglas F., and Karlsson, Annika C.

Abstract

We aimed to investigate whether the character of the immunodominant HIV-Gag peptide (variable or conserved) targeted by CD8+ T cells in early HIV infection would influence the quality and quantity of T cell responses, and whether this would affect the rate of disease progression. Treatment-naive HIV-infected study subjects within the OPTIONS cohort at the University of California, San Francisco, were monitored from an estimated 44 days postinfection for up to 6 years. CD8+ T cells responses targeting HLA-matched HIV-Gag-epitopes were identified and characterized by multicolor flow cytometry. The autologous HIV gag sequences were obtained. We demonstrate that patients targeting a conserved HIV-Gag-epitope in early infection maintained their epitope-specific CD8+ T cell response throughout the study period. Patients targeting a variable epitope showed decreased immune responses over time, although there was no limitation of the functional profile, and they were likely to target additional variable epitopes. Maintained immune responses to conserved epitopes were associated with no or limited sequence evolution within the targeted epitope. Patients with immune responses targeting conserved epitopes had a significantly lower median viral load over time compared to patients with responses targeting a variable epitope (0.63 log10 difference). Furthermore, the rate of CD4+ T cell decline was slower for subjects targeting a conserved epitope (0.85% per month) compared to subjects targeting a variable epitope (1.85% per month). Previous studies have shown that targeting of antigens based on specific HLA types is associated with a better disease course. In this study we show that categorizing epitopes based on their variability is associated with clinical outcome.

Published
2013

44. Characterization of HIV-Specific CD4+T Cell Responses against Peptides Selected with Broad Population and Pathogen Coverage

Author

Buggert, Marcus, Norstrom, Melissa M., Czarnecki, Chris, Tupin, Emmanuel, Luo, Ma, Gyllensten, Katarina, Sonnerborg, Anders, Lundegaard, Claus, Lund, Ole, Nielsen, Morten, Karlsson, Annika C., Buggert, Marcus, Norstrom, Melissa M., Czarnecki, Chris, Tupin, Emmanuel, Luo, Ma, Gyllensten, Katarina, Sonnerborg, Anders, Lundegaard, Claus, Lund, Ole, Nielsen, Morten, and Karlsson, Annika C.

Abstract

CD4+ T cells orchestrate immunity against viral infections, but their importance in HIV infection remains controversial. Nevertheless, comprehensive studies have associated increase in breadth and functional characteristics of HIV-specific CD4+ T cells with decreased viral load. A major challenge for the identification of HIV-specific CD4+ T cells targeting broadly reactive epitopes in populations with diverse ethnic background stems from the vast genomic variation of HIV and the diversity of the host cellular immune system. Here, we describe a novel epitope selection strategy, PopCover, that aims to resolve this challenge, and identify a set of potential HLA class II-restricted HIV epitopes that in concert will provide optimal viral and host coverage. Using this selection strategy, we identified 64 putative epitopes (peptides) located in the Gag, Nef, Env, Pol and Tat protein regions of HIV. In total, 73% of the predicted peptides were found to induce HIV-specific CD4+ T cell responses. The Gag and Nef peptides induced most responses. The vast majority of the peptides (93%) had predicted restriction to the patient's HLA alleles. Interestingly, the viral load in viremic patients was inversely correlated to the number of targeted Gag peptides. In addition, the predicted Gag peptides were found to induce broader polyfunctional CD4+ T cell responses compared to the commonly used Gag-p55 peptide pool. These results demonstrate the power of the PopCover method for the identification of broadly recognized HLA class II-restricted epitopes. All together, selection strategies, such as PopCover, might with success be used for the evaluation of antigen-specific CD4+ T cell responses and design of future vaccines.

Published
2012

45. Characterization of HIV-Specific CD4+ T Cell Responses against Peptides Selected with Broad Population and Pathogen Coverage

Author

Buggert, Marcus, primary, Norström, Melissa M., additional, Czarnecki, Chris, additional, Tupin, Emmanuel, additional, Luo, Ma, additional, Gyllensten, Katarina, additional, Sönnerborg, Anders, additional, Lundegaard, Claus, additional, Lund, Ole, additional, Nielsen, Morten, additional, and Karlsson, Annika C., additional

Published
2012
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48. Reduction of the HIV-1 reservoir in resting CD4+ T-lymphocytes by high dosage intravenous immunoglobulin treatment: a proof-of-concept study

Author

Lindkvist, Annica, primary, Edén, Arvid, additional, Norström, Melissa M, additional, Gonzalez, Veronica D, additional, Nilsson, Staffan, additional, Svennerholm, Bo, additional, Karlsson, Annika C, additional, Sandberg, Johan K, additional, Sönnerborg, Anders, additional, and Gisslén, Magnus, additional

Published
2009
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49. Viral dynamics and evolution following primary HIV-1 infection

Author

Karlsson, Annika C and Karlsson, Annika C

Abstract

The knowledge of the early events during primary HIV-1 infection (PER) is of great importance for the understanding of the pathogenesis of HIV-1. A major problem in studies on PHI is the limited amount of data accessible from the early time-points. In our study, frequent blood sampling was done during the first weeks at PHI and thereafter in the chronic phase of infection, from both untreated (n = 8) and treated (n = 15) patients. The overall aim of this thesis was to obtain insights in the dynamics of viral load, diversity and divergence during PHI and the subsequent events in the chronic phase of infection, including the conceivable persistence of earlier viral quasispecies in resting CD4+ T-lymphocytes, a proposed reservoir for HIV-1. In untreated patients, a novel four phase model of the HIV-1 RNA dynamics during PHI was described. The initial rapid increase reached a peak one week after onset of symptoms, thereafter a rapid decay was followed at the third week by a reduced viral clearance before a seemingly steady state was reached after about two months. The rapid decay most probably reflects the onset of HIV-1 specific immune activity. The phase of reduced viral clearance may be due to the appearance of escape mutants and/or outgrow of minor transmitted variants. Nevertheless, the decay continued although at a much lower rate suggesting that the immune system continues to respond to the new viral variants resulting in a steady state between replication and clearance. The virus population was characterized mainly by direct sequencing, but also by cloning, of the partial gag, pol, and env genes. Although a completely homogeneous viral population was uncommon the viral diversity was restricted in most patients. However, in some patients a more heterogeneous pattern was identified, which could reflect that several HIV-1 strains were transmitted and/or that an antiretroviral immune response caused a rapid selection of a fit master sequence. In the chronic phase, t

Published
2000

50. CD8 T cell effector maturation in HIV-1-infected children

Author

Jordan, Kimberly A., primary, Furlan, Scott N., additional, Gonzalez, Veronica D., additional, Karlsson, Annika C., additional, Quigley, Máire F., additional, Deeks, Steven G., additional, Rosenberg, Michael G., additional, Nixon, Douglas F., additional, and Sandberg, Johan K., additional

Published
2006
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