Your search keyword '"Elisa T Helbig"' showing total 19 results

1. Safety, reactogenicity, and immunogenicity of homologous and heterologous prime-boost immunisation with ChAdOx1 nCoV-19 and BNT162b2: a prospective cohort study

Author

David Hillus, Tatjana Schwarz, Pinkus Tober-Lau, Kanika Vanshylla, Hana Hastor, Charlotte Thibeault, Stefanie Jentzsch, Elisa T Helbig, Lena J Lippert, Patricia Tscheak, Marie Luisa Schmidt, Johanna Riege, André Solarek, Christof von Kalle, Chantip Dang-Heine, Henning Gruell, Piotr Kopankiewicz, Norbert Suttorp, Christian Drosten, Harald Bias, Joachim Seybold, Florian Klein, Florian Kurth, Victor Max Corman, Leif Erik Sander, Ben Al-Rim, Lara Bardtke, Jörn Ilmo Beheim-Schwarzbach, Kerstin Behn, Leon Bergfeld, Norma Bethke, Tobias Bleicker, Dana Briesemeister, Sophia Brumhard, Claudia Conrad, Sebastian Dieckmann, Doris Frey, Julie-Anne Gabelich, Philipp Georg, Ute Gläser, Lisbeth Hasler, Andreas Hetey, Anna Luisa Hiller, Alexandra Horn, Claudia Hülso, Luisa Kegel, Willi Koch, Alexander Krannich, Paolo Kroneberg, Michelle Lisy, Petra Mackeldanz, Birgit Maeß, Friederike Münn, Nadine Olk, Christian Peiser, Kai Pohl, Annelie Hermel, Maria Rönnefarth, Carolin Rubisch, Angela Sanchez Rezza, Isabelle Schellenberger, Viktoria Schenkel, Jenny Schlesinger, Sein Schmidt, Georg Schwanitz, Anne-Sophie Sinnigen, Paula Stubbemann, Julia Tesch, Denise Treue, Daniel Wendisch, and Saskia Zvorc

Subjects

Pulmonary and Respiratory Medicine, Health Personnel, Heterologous, Antibodies, Viral, Immunogenicity, Vaccine, Neutralization Tests, ChAdOx1 nCoV-19, Germany, Humans, Medicine, Avidity, Prospective Studies, Prospective cohort study, BNT162 Vaccine, Reactogenicity, Heterologous vaccine, biology, SARS-CoV-2, business.industry, Immunogenicity, Vaccination, COVID-19, Articles, Immunoglobulin G, Immunology, biology.protein, Antibody, business

Abstract

Background Heterologous vaccine regimens have been widely discussed as a way to mitigate intermittent supply shortages and to improve immunogenicity and safety of COVID-19 vaccines. We aimed to assess the reactogenicity and immunogenicity of heterologous immunisations with ChAdOx1 nCov-19 (AstraZeneca, Cambridge, UK) and BNT162b2 (Pfizer-BioNtech, Mainz, Germany) compared with homologous BNT162b2 and ChAdOx1 nCov-19 immunisation. Methods This is an interim analysis of a prospective observational cohort study enrolling health-care workers in Berlin (Germany) who received either homologous ChAdOx1 nCov-19 or heterologous ChAdOx1 nCov-19–BNT162b2 vaccination with a 10–12-week vaccine interval or homologous BNT162b2 vaccination with a 3-week vaccine interval. We assessed reactogenicity after the first and second vaccination by use of electronic questionnaires on days 1, 3, 5, and 7. Immunogenicity was measured by the presence of SARS-CoV-2-specific antibodies (full spike-IgG, S1-IgG, and RBD-IgG), by an RBD–ACE2 binding inhibition assay (surrogate SARS-CoV-2 virus neutralisation test), a pseudovirus neutralisation assay against two variants of concerns (alpha [B.1.1.7] and beta [B.1.351]), and anti-S1-IgG avidity. T-cell reactivity was measured by IFN-γ release assay. Findings Between Dec 27, 2020, and June 14, 2021, 380 participants were enrolled in the study, with 174 receiving homologous BNT162b2 vaccination, 38 receiving homologous ChAdOx1 nCov-19 vaccination, and 104 receiving ChAdOx1 nCov-19–BNT162b2 vaccination. Systemic symptoms were reported by 103 (65%, 95% CI 57·1–71·8) of 159 recipients of homologous BNT162b2, 14 (39%, 24·8–55·1) of 36 recipients of homologous ChAdOx1 nCov-19, and 51 (49%, 39·6–58·5) of 104 recipients of ChAdOx1 nCov-19–BNT162b2 after the booster immunisation. Median anti-RBD IgG levels 3 weeks after boost immunisation were 5·4 signal to cutoff ratio (S/co; IQR 4·8–5·9) in recipients of homologous BNT162b2, 4·9 S/co (4·3–5·6) in recipients of homologous ChAdOx1 nCov-19, and 5·6 S/co (5·1–6·1) in recipients of ChAdOx1 nCov-19– BNT162b2. Geometric mean of 50% inhibitory dose against alpha and beta variants were highest in recipients of ChAdOx1 nCov-19–BNT162b2 (956·6, 95% CI 835·6–1095, against alpha and 417·1, 349·3–498·2, against beta) compared with those in recipients of homologous ChAdOx1 nCov-19 (212·5, 131·2–344·4, against alpha and 48·5, 28·4–82·8, against beta; both p

Published

2021

2. Outbreak of SARS-CoV-2 B.1.1.7 Lineage after Vaccination in Long-Term Care Facility, Germany, February–March 2021

Author

Florian Kurth, Pinkus Tober-Lau, Leon Bergfeld, David Hillus, Daniela Niemeyer, Barbara Mühlemann, Tatjana Schwarz, Stefanie Kasper, Lena J Lippert, Friederike Münn, Claudia Conrad, Elisa T Helbig, Victor M. Corman, Christian Drosten, Norbert Suttorp, Leif E. Sander, Terry Jones, Charlotte Thibeault, Frank Kunitz, Willi Koch, and Jana Spieckermann

Subjects

Microbiology (medical), Pediatrics, medicine.medical_specialty, Lineage (genetic), Epidemiology, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Outbreak of SARS-CoV-2 B.1.1.7 Lineage after Vaccination in Long-Term Care Facility, Germany, February–March 2021, mRNA, Infectious and parasitic diseases, RC109-216, phylogeny, Disease Outbreaks, respiratory infections, vaccine, antibody, Germany, Medicine, Humans, viruses, B cell, outbreak, business.industry, SARS-CoV-2, Vaccination, Dispatch, Outbreak, T cell, COVID-19, immunity, Long-Term Care, Care facility, zoonoses, Berlin, Long-term care, Infectious Diseases, Mild symptoms, coronavirus disease, business, Viral load, severe acute respiratory syndrome coronavirus 2

Abstract

One week after second vaccinations were administered, an outbreak of B.1.1.7 lineage severe acute respiratory syndrome coronavirus 2 infections occurred in a long-term care facility in Berlin, Germany, affecting 16/20 vaccinated and 4/4 unvaccinated residents. Despite considerable viral loads, vaccinated residents experienced mild symptoms and faster time to negative test results.

Published

2021

3. Severity of respiratory failure and computed chest tomography in acute COVID-19 correlates with pulmonary function and respiratory symptoms after infection with SARS-CoV-2: An observational longitudinal study over 12 months

Author

Florian Kurth, Florian Alius, Martin Witzenrath, Christoph Ruwwe-Gloesenkamp, Elisa T Helbig, Norbert Suttorp, Felix Doellinger, Thomas Zoller, Hans-Jakob Meyer, Daniel Grund, Charlotte Thibeault, Lena J Lippert, Raphaela Maria Ring, Philipp Knape, Fridolin Steinbeis, Mirja Mittermaier, Leif E. Sander, Bettina Temmesfeld-Wollbrueck, and Tobias Penzkofer

Subjects

Male, Longitudinal study, medicine.medical_treatment, Vital Capacity, Disease, Severity of Illness Index, Pulmonary function testing, Quality of life, Forced Expiratory Volume, Surveys and Questionnaires, Longitudinal Studies, Respiratory system, Lung, Original Research, Long-COVID, Middle Aged, Respiratory Function Tests, Hospitalization, Post-COVID, Pulmonary outcome, Female, Respiratory Insufficiency, Pulmonary and Respiratory Medicine, Adult, medicine.medical_specialty, Pulmonary function, Post-acute COVID, Extracorporeal Membrane Oxygenation, Post-Acute COVID-19 Syndrome, Internal medicine, medicine, Humans, Aged, Mechanical ventilation, business.industry, SARS-CoV-2, Total Lung Capacity, Oxygen Inhalation Therapy, COVID-19, Recovery of Function, Pneumonia, Respiration, Artificial, Clinical trial, Respiratory failure, Pulmonary Diffusing Capacity, Pulmonary sequelae, business, Tomography, X-Ray Computed, Pulmonary restriction

Abstract

Introduction Prospective and longitudinal data on pulmonary injury over one year after acute coronavirus disease 2019 (COVID-19) are sparse. We aim to determine reductions in pulmonary function and respiratory related quality of life up to 12 months after acute COVID-19. Methods Patients with acute COVID-19 were enrolled into an ongoing single-centre, prospective observational study and prospectively examined 6 weeks, 3, 6 and 12 months after onset of COVID-19 symptoms. Chest CT-scans, pulmonary function and symptoms assessed by St. Georges Respiratory Questionnaire were used to evaluate respiratory limitations. Patients were stratified according to severity of acute COVID-19. Results Median age of all patients was 57 years, 37.8% were female. Higher age, male sex and higher BMI were associated with acute-COVID-19 severity (p, Graphical abstract Image 1

Published

2021

4. Severity of respiratory failure and computed chest tomography in acute COVID-19 correlates with pulmonary function and respiratory symptoms after infection with SARS-CoV-2: an observational longitudinal study over 12 months

Author

Christoph Ruwwe-Gloesenkamp, Felix Doellinger, Lena J Lippert, Raphaela Maria Ring, Thomas Zoller, Daniel Grund, Hans-Jakob Meyer, Florian Alius, Fridolin Steinbeis, Elisa T Helbig, Florian Kurth, Leif E. Sander, Mirja Mittermaier, Norbert Suttorp, Bettina Temmesfeld-Wollbrueck, Tobias Penzkofer, Charlotte Thibeault, Philipp Knape, and Martin Witzenrath

Subjects

Mechanical ventilation, medicine.medical_specialty, Longitudinal study, business.industry, medicine.medical_treatment, Disease, Pulmonary function testing, Clinical trial, Quality of life, Respiratory failure, Internal medicine, medicine, Respiratory system, business

Abstract

BackgroundProspective and longitudinal data on pulmonary injury over one year after acute coronavirus disease 2019 (COVID-19) are sparse.Research questionWith this study, we aim to investigate pulmonary outcome following SARS-CoV-2 infection including pulmonary function, computed chest tomography, respiratory symptoms and quality of life over 12 months.Study design and Methods180 patients after acute COVID-19 were enrolled into a single-centre, prospective observational study and examined 6 weeks, 3, 6 and 12 months after onset of COVID-19 symptoms. Chest CT-scans, pulmonary function and symptoms assessed by St. Georges Respiratory Questionnaire were used to evaluate objective and subjective respiratory limitations. Patients were stratified according to acute COVID-19 disease severity.ResultsOf 180 patients enrolled, 42/180 were not hospitalized during acute SARS-CoV-2 infection, 29/180 were hospitalized without need for oxygen, 43/180 with need for low-flow and 24/180 with high-flow oxygen, 26/180 required invasive mechanical ventilation and 16/180 were treated with ECMO. After acute COVID-19, pulmonary restriction and reduced carbon monoxide diffusion capacity was associated with disease severity after the acute phase and improved over 12 months except for those requiring ECMO treatment. Patients with milder disease showed a predominant reduction of ventilated area instead of simple restriction. The CT score of lung involvement in the acute phase increased significantly with COVID-19 severity and was associated with restriction and reduction in diffusion capacity in follow-up. Respiratory symptoms improved for patients in higher severity groups during follow-up, but not for patients with mild initially disease.InterpretationSeverity of respiratory failure during COVID-19 correlates with the degree of pulmonary function impairment and respiratory quality of life in the year after acute infection. Patients with mild vs. severe disease show different patterns of lung involvement and symptom resolution.Clinical Trial RegistrationThe study is registered at the German registry for clinical studies (DRKS00021688)

Published

2021

5. Clinical and virological characteristics of hospitalised COVID-19 patients in a German tertiary care centre during the first wave of the SARS-CoV-2 pandemic: a prospective observational study

Author

Miriam Stegemann, Alexander Uhrig, Sascha S. Haenel, Pinkus Tober-Lau, Leonie Meiners, Florian Kurth, Janine Wiebach, Martin Witzenrath, Stefan Hippenstiel, Moritz Pfeiffer, Lena J Lippert, Robert Roehle, Tilman Lingscheid, Charlotte Thibeault, Norbert Suttorp, Leif E. Sander, Holger Müller-Redetzky, Christian Drosten, Felix Balzer, Terry Jones, Paula Stubbemann, Laure Bosquillon de Jarcy, Lil Meyer-Arndt, Thomas Zoller, Victor M. Corman, Christof von Kalle, Barbara Mühlemann, Mirja Mittermaier, and Elisa T Helbig

Subjects

Microbiology (medical), medicine.medical_specialty, Time Factors, COVID-19 nucleic acid testing, Respiratory distress syndrome, medicine.medical_treatment, Symptom assessment, Disease, 030204 cardiovascular system & hematology, Artificial respiration, Cohort Studies, Tertiary Care Centers, 03 medical and health sciences, 0302 clinical medicine, Mechanical ventilation, Risk Factors, Internal medicine, Germany, medicine, Humans, 030212 general & internal medicine, Prospective Studies, Risk factor, Prospective study, Prospective cohort study, Original Paper, Viral concentration, business.industry, SARS-CoV-2, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), COVID-19, General Medicine, Viral Load, Respiration, Artificial, Virus Shedding, Coronavirus disease 2019 (COVID-19), Hospitalization, Kinetics, Infectious Diseases, Cohort, Hypertension, Observational study, business, Function and Dysfunction of the Nervous System, Viral load

Abstract

Purpose Adequate patient allocation is pivotal for optimal resource management in strained healthcare systems, and requires detailed knowledge of clinical and virological disease trajectories. The purpose of this work was to identify risk factors associated with need for invasive mechanical ventilation (IMV), to analyse viral kinetics in patients with and without IMV and to provide a comprehensive description of clinical course. Methods A cohort of 168 hospitalised adult COVID-19 patients enrolled in a prospective observational study at a large European tertiary care centre was analysed. Results Forty-four per cent (71/161) of patients required invasive mechanical ventilation (IMV). Shorter duration of symptoms before admission (aOR 1.22 per day less, 95% CI 1.10–1.37, p p p Conclusions Our results indicate a short duration of symptoms before admission as a risk factor for severe disease that merits further investigation and different viral load kinetics in severely affected patients. Median duration of hospitalisation of IMV patients was longer than described for acute respiratory distress syndrome unrelated to COVID-19.

Published

2021

6. A time-resolved proteomic and prognostic map of COVID-19

Author

Vadim Demichev, Pinkus Tober-Lau, Oliver Lemke, Tatiana Nazarenko, Charlotte Thibeault, Harry Whitwell, Annika Röhl, Anja Freiwald, Lukasz Szyrwiel, Daniela Ludwig, Clara Correia-Melo, Simran Kaur Aulakh, Elisa T. Helbig, Paula Stubbemann, Lena J. Lippert, Nana-Maria Grüning, Oleg Blyuss, Spyros Vernardis, Matthew White, Christoph B. Messner, Michael Joannidis, Thomas Sonnweber, Sebastian J. Klein, Alex Pizzini, Yvonne Wohlfarter, Sabina Sahanic, Richard Hilbe, Benedikt Schaefer, Sonja Wagner, Mirja Mittermaier, Felix Machleidt, Carmen Garcia, Christoph Ruwwe-Glösenkamp, Tilman Lingscheid, Laure Bosquillon de Jarcy, Miriam S. Stegemann, Moritz Pfeiffer, Linda Jürgens, Sophy Denker, Daniel Zickler, Philipp Enghard, Aleksej Zelezniak, Archie Campbell, Caroline Hayward, David J. Porteous, Riccardo E. Marioni, Alexander Uhrig, Holger Müller-Redetzky, Heinz Zoller, Judith Löffler-Ragg, Markus A. Keller, Ivan Tancevski, John F. Timms, Alexey Zaikin, Stefan Hippenstiel, Michael Ramharter, Martin Witzenrath, Norbert Suttorp, Kathryn Lilley, Michael Mülleder, Leif Erik Sander, Markus Ralser, Florian Kurth, Malte Kleinschmidt, Katrin M. Heim, Belén Millet, Lil Meyer-Arndt, Ralf H. Hübner, Tim Andermann, Jan M. Doehn, Bastian Opitz, Birgit Sawitzki, Daniel Grund, Peter Radünzel, Mariana Schürmann, Thomas Zoller, Florian Alius, Philipp Knape, Astrid Breitbart, Yaosi Li, Felix Bremer, Panagiotis Pergantis, Dirk Schürmann, Bettina Temmesfeld-Wollbrück, Daniel Wendisch, Sophia Brumhard, Sascha S. Haenel, Claudia Conrad, Philipp Georg, Kai-Uwe Eckardt, Lukas Lehner, Jan M. Kruse, Carolin Ferse, Roland Körner, Claudia Spies, Andreas Edel, Steffen Weber-Carstens, Alexander Krannich, Saskia Zvorc, Linna Li, Uwe Behrens, Sein Schmidt, Maria Rönnefarth, Chantip Dang-Heine, Robert Röhle, Emma Lieker, Lucie Kretzler, Isabelle Wirsching, Christian Wollboldt, Yinan Wu, Georg Schwanitz, David Hillus, Stefanie Kasper, Nadine Olk, Alexandra Horn, Dana Briesemeister, Denise Treue, Michael Hummel, Victor M. Corman, Christian Drosten, Christof von Kalle, Ralser, Markus [0000-0001-9535-7413], and Apollo - University of Cambridge Repository

Subjects

Proteomics, Patient Trajectories, Histology, Proteome, Disease Prognosis, Clinical Disease Progression, Inflammation, Disease, 0601 Biochemistry and Cell Biology, Bioinformatics, Asymptomatic, Article, Pathology and Forensic Medicine, Blood cell, Machine Learning, 03 medical and health sciences, 0302 clinical medicine, Humans, Medicine, 030304 developmental biology, 0303 health sciences, SARS-CoV-2, business.industry, Age Factors, Cell Biology, Prognosis, Blood Cell Count, Enzyme Activation, Longitudinal Profiling, medicine.anatomical_structure, Infectious disease (medical specialty), Cohort, Disease Progression, Blood Gas Analysis, medicine.symptom, business, Covid-19, Physiological parameters, 030217 neurology & neurosurgery, Biomarkers

Abstract

COVID-19 is highly variable in its clinical presentation, ranging from asymptomatic infection to severe organ damage and death. We characterized the time-dependent progression of the disease in 139 COVID-19 inpatients by measuring 86 accredited diagnostic parameters, such as blood cell counts and enzyme activities, as well as untargeted plasma proteomes at 687 sampling points. We report an initial spike in a systemic inflammatory response, which is gradually alleviated and followed by a protein signature indicative of tissue repair, metabolic reconstitution, and immunomodulation. We identify prognostic marker signatures for devising risk-adapted treatment strategies and use machine learning to classify therapeutic needs. We show that the machine learning models based on the proteome are transferable to an independent cohort. Our study presents a map linking routinely used clinical diagnostic parameters to plasma proteomes and their dynamics in an infectious disease., Graphical abstract, Demichev, Tober-Lau et al., present a time-resolved molecular map of the COVID-19, measuring plasma proteomes of patients with COVID-19 along with an extensive panel of clinical diagnostic parameters at 687-time points. They describe the specificity and dynamics, as well as the predictive and prognostic power of the molecular signatures in COVID-19.

Published

2021

7. A proteomic survival predictor for COVID-19 patients in intensive care

Author

Alexander Uhrig, Richard Hilbe, Michael Muelleder, Michael Ramharter, Oleg Blyuss, Sophy Denker, Daniel Zickler, Miriam Stegemann, Christoph B. Messner, Caroline Hayward, Riccardo E. Marioni, Clara Correia-Melo, Rosa Bellmann-Weiler, Mirja Mittermaier, Nils B. Mueller, Elisa T Helbig, Carmen Garcia, Alexey Zaikin, Moritz Pfeiffer, Ivan Tancevski, David J. Porteous, Holger Mueller-Redetzky, Daniela Ludwig, Aleksej Zelezniak, Philipp Enghard, Matthew White, Vadim Demichev, Sonja Wagner, Heinz Zoller, Sebastian J. Klein, Spyros I. Vernardis, Markus A. Keller, Harry J. Whitwell, Leif E. Sander, Annika Roehl, Felix Machleidt, Christoph Ruwwe-Gloesenkamp, Michael Joannidis, Linda Juergens, Yvonne Wohlfarter, Nana-Maria Gruening, Stefan Hippenstiel, Judith Loeffler-Ragg, Kathryn S. Lilley, Simran Kaur Aulakh, Martin Witzenrath, Guenter Weiss, Florian Kurth, Sabina Sahanic, Tilman Lingscheid, Benedikt Schaefer, Thomas Sonnweber, Laure Bosquillon de Jarcy, Anja Freiwald, Norbert Suttorp, Lena J Lippert, Markus Ralser, Charlotte Thibeault, Pinkus Tober-Lau, John F. Timms, Nadine Olk, Lukasz Szyrwiel, Alex Pizzini, Paula Stubbemann, Tatiana Nazarenko, Archie Campbell, Andreas Edel, Claudia Spies, and Oliver Lemke

Subjects

Mechanical ventilation, medicine.medical_specialty, APACHE II, Coronavirus disease 2019 (COVID-19), business.industry, medicine.medical_treatment, Clinical trial, Intensive care, Charlson comorbidity index, Emergency medicine, medicine, SOFA score, Risk assessment, business

Abstract

Global healthcare systems are challenged by the COVID-19 pandemic. There is a need to optimize allocation of treatment and resources in intensive care, as clinically established risk assessments such as SOFA and APACHE II scores show only limited performance for predicting the survival of severely ill COVID-19 patients. Comprehensively capturing the host physiology, we speculated that proteomics in combination with new data-driven analysis strategies could produce a new generation of prognostic discriminators. We studied two independent cohorts of patients with severe COVID-19 who required intensive care and invasive mechanical ventilation. SOFA score, Charlson comorbidity index and APACHE II score were poor predictors of survival. Plasma proteomics instead identified 14 proteins that showed concentration trajectories different between survivors and non-survivors. A proteomic predictor trained on single samples obtained at the first time point at maximum treatment level (i.e. WHO grade 7) and weeks before the outcome, achieved accurate classification of survivors in an exploratory (AUROC 0.81) as well as in the independent validation cohort (AUROC of 1.0). The majority of proteins with high relevance in the prediction model belong to the coagulation system and complement cascade. Our study demonstrates that predictors derived from plasma protein levels have the potential to substantially outperform current prognostic markers in intensive care.Trial registrationGerman Clinical Trials Register DRKS00021688

Published

2021

8. Delayed Antibody and T-Cell Response to BNT162b2 Vaccination in the Elderly, Germany

Author

Victor M. Corman, Florian Kurth, Willi Koch, Leif E. Sander, Christian Drosten, Stefanie Kasper, Tatjana Schwarz, Claudia Conrad, Terry Jones, Daniela Niemeyer, David Hillus, Norbert Suttorp, Pinkus Tober-Lau, Janine Michel, Kai Kappert, Barbara Mühlemann, Rudolf Tauber, Christof von Kalle, Friederike Münn, Irmgard Landgraf, Andreas Nitsche, Harald Bias, Elisa T Helbig, Leon Bergfeld, Lena J Lippert, Piotr Kopankiewicz, Joachim Seybold, Chantip Dang-Heine, Sein Schmidt, and Charlotte Thibeault

Subjects

Pediatrics, Epidemiology, T-Lymphocytes, Psychological intervention, Infectious and parasitic diseases, RC109-216, Disease, medicine.disease_cause, 0302 clinical medicine, Germany, vaccine, antibody, 030212 general & internal medicine, Coronavirus, Aged, 80 and over, B cell, biology, Vaccination, Dispatch, Berlin, Infectious Diseases, coronavirus disease, Medicine, Antibody, severe acute respiratory syndrome coronavirus 2, Adult, Microbiology (medical), medicine.medical_specialty, COVID-19 Vaccines, mRNA, 030231 tropical medicine, T cell response, respiratory infections, 03 medical and health sciences, Elderly persons, Immunity, medicine, Humans, viruses, ddc:610, BNT162 Vaccine, Aged, SARS-CoV-2, business.industry, COVID-19, T cell, immunity, zoonoses, Delayed Antibody and T-Cell Response to BNT162b2 Vaccination in the Elderly, Germany, biology.protein, business, 610 Medizin und Gesundheit

Abstract

We detected delayed and reduced antibody and T-cell responses after BNT162b2 vaccination in 71 elderly persons (median age 81 years) compared with 123 healthcare workers (median age 34 years) in Germany. These data emphasize that nonpharmaceutical interventions for coronavirus disease remain crucial and that additional immunizations for the elderly might become necessary.

Published

2021

9. Safety, reactogenicity, and immunogenicity of homologous and heterologous prime-boost immunisation with ChAdOx1-nCoV19 and BNT162b2: a prospective cohort study

Author

Tatjana Schwarz, David Hillus, Patricia Tscheak, Christian Drosten, Elisa T Helbig, Harald Bias, Stefanie Kasper, Florian Kurth, Norbert Suttorp, Piotr Kopankiewicz, Joachim Seybold, Andr Solarek, Leif E. Sander, Chantip Dang-Heine, Christof von Kalle, Covim, Marie Luisa Schmidt, Johanna Riege, Hana Hastor, Lena J Lippert, Pinkus Tober-Lau, Victor M. Corman, and Charlotte Thibeault

Subjects

Vaccination, Regimen, Reactogenicity, business.industry, Immunogenicity, Cohort, Immunology, Heterologous, Medicine, Avidity, Prospective cohort study, business

Abstract

Objectiveto assess reactogenicity and immunogenicity of heterologous prime-boost immunisations of ChAdOx1-nCoV19 (Vaxzevria, ChAdOx) followed by BNT162b2 (Comirnaty, BNT) compared to homologous BNT/BNT immunisation.Designprospective, observational cohort study.Settingunicenter study in a cohort of health care workers at a tertiary care center in Berlin, Germany.Participants340 health care workers immunised between 27 December 2020 and 21 May 2021 at Charité - Universitätsmedizin Berlin, GermanyMain outcome measuresthe main outcomes were reactogenicity assessed on days one, three, five and seven post prime and boost vaccination, and immunogenicity measured by serum SARS-CoV-2 full spike-, spike S1-, and spike RBD-IgG, virus neutralisation capacity, anti-S1-IgG avidity, and T cell reactivity measured by Interferon gamma release assay at 3-4 weeks post prime and boost immunisation.ResultsHeterologous ChAdOx/BNT booster vaccination was overall well-tolerated and reactogenicity was largely comparable to homologous BNT/BNT vaccination. Systemic reactions were most frequent after prime immunisation with ChAdOx (86%, 95CI: 79-91), and less frequent after homologous BNT/BNT (65%, 95CI: 56-72), or heterologous ChAdOx/BNT booster vaccination (48%, 95CI: 36-59). Serum antibody responses and T cell reactivity were strongly increased after both homologous and heterologous boost, and immunogenicity was overall robust, and comparable between both regimens in this cohort, with slightly increased S1-IgG avidity and T cell responses following heterologous booster immunisation.ConclusionsEvidence of rare thrombotic events associated with ChAdOx has led to recommendation of a heterologous booster with mRNA vaccines for certain age groups in several European countries, despite a lack of robust safety and immunogenicity data for this vaccine regimen. This interim analysis provides evidence that the currently recommended heterologous ChAdOx/BNT immunisation regimen with 10-12 week vaccine intervals is well tolerated and slightly more immunogenic compared to homologous BNT/BNT vaccination with three week vaccine intervals. Heterologous prime-boost immunisation for COVID-19 may be generally applicable to optimise logistics and improve immunogenicity and to mitigate potential intermittent supply shortages for individual vaccines.

Published

2021

10. Complement Activation Induces Excessive T Cell Cytotoxicity in Severe COVID-19

Author

Simran Kaur Aulakh, Maria Schneider, Nils Blüthgen, Axel Schulz, Markus Landthaler, Matthias Barone, Laura Michalick, Tomislav Kostevc, Lorenzo Bonaguro, Peter Boor, Julia Stein, Lena J Lippert, Holger Müller-Redetzky, Rosario Astaburuaga-García, Jacob Nattermann, Münevve Demir, Florian Kurth, Wolfgang M. Kuebler, Vadim Demichev, Michael Mülleder, Alexander Uhrig, Hannah-Philine Dey, Mathias Streitz, Joachim L. Schultze, Victor M. Corman, Pinkus Tober-Lau, Henrik E. Mei, Emanuel Wyler, Benedikt Obermayer-Wasserscheid, Leif-Erik Sander, Sophia Brumhard, Charlotte Thibeault, Hans Wesselmann, Dieter Beule, Markus Ralser, Elisa T Helbig, Ioanna Gemünd, Stefan Hippenstiel, Christian Meisel, Philipp Georg, Norbert Suttorp, Birgit Sawitzki, Christiane Gäbel, Anna C. Aschenbrenner, and Daniela Paclik

Subjects

Oncology, medicine.medical_specialty, Coronavirus disease 2019 (COVID-19), biology, business.industry, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), T cell, Institutional review board, Complement system, medicine.anatomical_structure, Immune system, Internal medicine, medicine, biology.protein, Cytotoxic T cell, Antibody, business

Abstract

Severe COVID-19 is linked to both dysfunctional immune response and unrestrained immunopathogenesis, and it remains unclear if T cells contribute to disease pathology. Here, we combined single-cell transcriptomics and proteomics with mechanistic studies assessing pathogenic T cell functions and inducing signals. We identified activated, CD16+ T cells with increased cytotoxic functions in severe COVID-19. CD16 expression enabled immune complex-mediated, T cell receptor-independent degranulation and cytotoxicity not found in other diseases. CD16+ T cells from COVID-19 patients promoted microvascular endothelial cell injury and release of neutrophil and monocyte chemoattractants. CD16+ T cell clones persisted beyond acute disease maintaining their cytotoxic phenotype. Age-dependent generation of C3a in severe COVID-19 induced activated CD16 + cytotoxic T cells. The proportion of activated CD16+ T cells and plasma levels of complement proteins upstream of C3a correlated with clinical outcome, supporting a pathological role of exacerbated cytotoxicity and complement activation in COVID-19. Funding: This work was supported by the German Research Foundation (DFG): SA1383/3-1 to B.S.; SFB-TR84 114933180 to L.E.S., S.B., P.G., S.H. and W.M.K. INST 37/1049-1, INST 216/981- 1, INST 257/605-1, INST 269/768-1, INST 217/988-1, INST 217/577-1, and EXC2151- 390873048 to J.L.S.; GRK 2168 – 272482170, ERA CVD (00160389 to J.L.S.; SFB 1454 – 432325352 to A.C.A. and J.L.S.; SFB TR57 and SPP1937 to J.N.; GRK2157 to A.-E.S.; and ME 3644/5-1 to H.E.M.; RTG2424 to N.B.; SFB-TRR219 322900939, BO3755/13-1 Project- ID 454024652 to P.B.; the Berlin University Alliance (BUA) (PreEP-Corona grant to L.E.S. and V.M.C.); the Berlin Institute of Health (BIH) (to L.E.S., V.M.C.,B.S. and W.M.K.); Helmholtz- Gemeinschaft Deutscher Forschungszentren, Germany (sparse2big to J.L.S.), EU projects SYSCID (733100 to J.L.S.); European Research Council Horizon 2020 (grant agreement No 101001791 to P.B.); the DZIF, Germany (TTU 04.816 and 04.817 to J.N.); the Hector Foundation (M89 to J.N.); the EU projects ONE STUDY (260687), BIO-DrIM (305147) and INsTRuCT (860003) to B.S.); German Registry of COVID-19 Autopsies through Federal Ministry of Health (ZMVI1-2520COR201 to P.B.); Federal Ministry of Education and Research (DEFEAT PANDEMICs, 01KX2021 and STOP-FSGS-01GM1901A to P.B.); the Berlin Senate to German Rheumatism Research Centre (DRFZ); the Berlin Brandenburg School for regenerative Therapies (BSRT) to C.B.; the German Federal Ministry of Education and Research (BMBF) projects RECAST (01KI20337) to B.S., V.M.C., L.E.S and M.R.; VARIPath (01KI2021) to V.M.C.; NUM COVIM (01KX2021) to L.E.S., V.M.C., F.K., J.L.S., J.N. and B.S.; RAPID to and S.H.,; SYMPATH to N.S. and W.M.K.; PROVID to S.H. and W.M.K.; ZissTrans (02NUK047E) to N.B; National Research Node ‘Mass spectrometry in Systems Medicine (MSCoresys) (031L0220A) to M.R. and N.B.; Diet–Body–Brain (DietBB) (01EA1809A) to J.L.S.; the UKRI/NIHR through the UK Coronavirus Immunology Consortium (UK-CIC), the Francis Crick Institute through the Cancer Research UK (FC001134), the UK Medical Research Council (FC001134), the Wellcome Trust (FC001134 and IA 200829/Z/16/Z) to M.R.; a Charite 3R project (to B.S., S.H., W.M.K.); and an intramural grant from the Department of Genomics & Immunoregulation at the LIMES Institute to A.C.A. We are grateful to the patients and donors volunteering to participate in this study making this research possible in the first place and wish for a speedy and full recovery. Conflict of Interest: V.M.C. is named together with Euroimmun GmbH on a patent application filed recently regarding SARS-CoV-2 diagnostics via antibody testing. A.R.S. and H.E.M. are listed as inventors on a patent application by the DRFZ Berlin in the field of mass cytometry. Ethical Approval: The study was approved by the Institutional Review board of Charite (EA2/066/20).

Published

2021

11. HLA-C*04:01 is a Genetic Risk Allele for Severe Course of COVID-19

Author

Claudia Quedenau, Melina Mueller, Mauricio Salvo, Alice Braun, Martin Witzenrath, Toumy Guettouche, Juan Macias Sanchez, Charlotte Thibeault, Dimitri Patriki, Manuel Holtgrewe, Bettina Heidecker, Hans Rudolf Schmid, January Weiner, JM Doehn, Florian Kurth, Jacopo Saccomanno, Benedikt Wiggli, Norbert Suttorp, Victor M. Corman, Wolfgang Poller, Phillip Suwalski, Tatiana Borodina, Terry Jones, Sandra Siemann, Barbara Muehlemann, Ronald K. Binder, Jonas Rutishauser, Elisa T Helbig, Xiaomin Wang, Ralf-Harto Hübner, B. Hinzmann, Anja Blueher, Stefan Hippenstiel, Ulf Landmesser, Dieter Beule, Lena J Lippert, Kathrin Danninger, Hansjuerg Beer, Paula Stubbemann, Zehra Karadeniz, Stjepan Jurisic, Carsten Skurk, Leif E. Sander, Juan A. Pineda, Marta Fernandez-Fuertes, Tomasz Zemojtel, Ulrike Krueger, Luis Miguel Real, and Stephan Ripke

Subjects

HLA-C, medicine.medical_specialty, Carriage, business.industry, Internal medicine, Pandemic, Hazard ratio, medicine, Disease, Human leukocyte antigen, Allele, business, Exome sequencing

Abstract

BackgroundSince the beginning of the coronavirus disease 2019 (COVID-19) pandemic, there has been increasing demand to identify predictors of severe clinical course in patients infected with severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2). Human leukocyte antigen alleles (HLA) have been suggested as potential genetic host factors. We sought to evaluate this hypothesis by conducting an international multicenter study using HLA sequencing with subsequent independent validation.MethodsWe analyzed a total of 332 samples. First, we enrolled 233 patients in Germany, Spain, and Switzerland for HLA and whole exome sequencing. Furthermore, we validated our results in a public data set (United States, n=99). Patients older than 18 years presenting with COVID-19 were included, representing the full spectrum of the disease. HLA candidate alleles were identified in the derivation cohort (n=92) and tested in two independent validation cohorts (n=240).ResultsWe identified HLA-C* 04:01 as a novel genetic predictor for severe clinical course in COVID-19. Carriers of HLA-C* 04:01 had twice the risk of intubation when infected with SARS-CoV-2 (hazard ratio 2.1, adjusted p-value=0.0036). Importantly, these findings were successfully replicated in an independent data set. Furthermore, our findings are biologically plausible, as HLA-C* 04:01 has fewer predicted bindings sites with relevant SARS-CoV-2 peptides as compared to other HLA alleles. Exome sequencing confirmed findings from HLA analysis.ConclusionsHLA-C* 04:01 carriage is associated with a twofold increased risk of intubation in patients infected with SARS-CoV-2. Testing for HLA-C* 04:01 could have clinical implications to identify high-risk patients and individualize management.

Published

2020

12. Clinical and Virological Characteristics of Hospitalized COVID-19 Patients in a German Tertiary Care Center during the First Wave of the SARS-CoV-2 Pandemic

Author

Florian Kurth, Robert Roehle, Elisa T Helbig, Janine Wiebach, Tilman Lingscheid, Mirja Mittermaier, Paula Stubbemann, Stefan Hippenstiel, Sascha S. Haenel, Charlotte Thibeault, Leonie Meiners, Lil Meyer-Arndt, Felix Balzer, Moritz Pfeiffer, Pinkus Tober-Lau, Laure Bosquillon de Jarcy, Victor M. Corman, Christoph von Kalle, Alexander Uhrig, Miriam Stegemann, Leif E. Sander, Lena J Lippert, Holger Mueller-Redetzky, Barbara Muehlemann, Martin Witzenrath, Thomas Zoller, Norbert Suttorp, Christian Drosten, and Terry Jones

Subjects

Mechanical ventilation, medicine.medical_specialty, Coronavirus disease 2019 (COVID-19), business.industry, medicine.medical_treatment, Disease, Cohort, Emergency medicine, Pandemic, medicine, Observational study, Risk factor, business, Viral load

Abstract

BackgroundAdequate patient allocation is pivotal for optimal resource management in strained healthcare systems, and requires detailed knowledge of clinical and virological disease trajectories.MethodsA cohort of 168 hospitalized adult COVID-19 patients enrolled in a prospective observational study at a large European tertiary care center was analyzed.ResultsForty-four percent (71/161) of patients required invasive mechanical ventilation (IMV). Shorter duration of symptoms before admission (aOR 1.22 per day less, 95%CI 1.10-1.37, pConclusionOur results indicate a short duration of symptoms before admission as a risk factor for severe disease and different viral load kinetics in severely affected patients.

Published

2020

13. A time-resolved proteomic and diagnostic map characterizes COVID-19 disease progression and predicts outcome

Author

Anja Freiwald, Norbert Suttorp, Christoph Ruwwe-Glösenkamp, Michael Joannidis, Daniel Zickler, Vadim Demichev, Charlotte Thibeault, Florian Kurth, Ivan Tancevski, Caroline Hayward, David J. Porteous, Sonja Wagner, Pinkus Tober-Lau, Clara Correia-Melo, Moritz Pfeiffer, Tilman Lingscheid, Markus Ralser, Markus A. Keller, Judith Löffler-Ragg, Archie Campbell, Heinz Zoller, John F. Timms, Daniela Ludwig, Yvonne Wohlfarter, Thomas Sonnweber, Paula Stubbemann, Carmen Garcia, Benedikt Schaefer, Philipp Enghard, Miriam Stegemann, Christoph B. Messner, Riccardo E. Marioni, Alexander Uhrig, Michael Ramharter, Annika Röhl, Sebastian J. Klein, Oleg Blyuss, Alexey Zaikin, Sophy Denker, Matthew White, Leif E. Sander, Harry J. Whitwell, Laure Bosquillon de Jarcy, Felix Machleidt, Stefan Hippenstiel, Sabina Sahanic, Tatiana Nazarenko, Holger Müller-Redetzky, Linda Jürgens, Richard Hilbe, Spyros I. Vernardis, Oliver Lemke, Elisa T Helbig, Aleksej Zelezniak, Michael Mülleder, Kathryn S. Lilley, Martin Witzenrath, Mirja Mittermaier, Nana-Maria Grüning, Lukasz Szyrwiel, and Alex Pizzini

Subjects

Mechanical ventilation, Oncology, medicine.medical_specialty, business.industry, medicine.medical_treatment, Inflammation, Disease, Phenotype, Asymptomatic, Internal medicine, Molecular Response, Proteome, Cohort, medicine, medicine.symptom, business

Abstract

COVID-19 is highly variable in its clinical presentation, ranging from asymptomatic infection to severe organ damage and death. There is an urgent need for predictive markers that can guide clinical decision-making, inform about the effect of experimental therapies, and point to novel therapeutic targets. Here, we characterize the time-dependent progression of COVID-19 through different stages of the disease, by measuring 86 accredited diagnostic parameters and plasma proteomes at 687 sampling points, in a cohort of 139 patients during hospitalization. We report that the time-resolved patient molecular phenotypes reflect an initial spike in the systemic inflammatory response, which is gradually alleviated and followed by a protein signature indicative of tissue repair, metabolic reconstitution and immunomodulation. Further, we show that the early host response is predictive for the disease trajectory and gives rise to proteomic and diagnostic marker signatures that classify the need for supplemental oxygen therapy and mechanical ventilation, and that predict the time to recovery of mildly ill patients. In severely ill patients, the molecular phenotype of the early host response predicts survival, in two independent cohorts and weeks before outcome. We also identify age-specific molecular response to COVID-19, which involves increased inflammation and lipoprotein dysregulation in older patients. Our study provides a deep and time resolved molecular characterization of COVID-19 disease progression, and reports biomarkers for risk-adapted treatment strategies and molecular disease monitoring. Our study demonstrates accurate prognosis of COVID-19 outcome from proteomic signatures recorded weeks earlier.

Published

2020

14. Impact of dexamethasone on SARS-CoV-2 concentration kinetics and antibody response in hospitalized COVID-19 patients: results from a prospective observational study

Author

Barbara Mühlemann, Charlotte Thibeault, David Hillus, Elisa T. Helbig, Lena J. Lippert, Pinkus Tober-Lau, Tatjana Schwarz, Marcel A. Müller, Martin Witzenrath, Norbert Suttorp, Leif E. Sander, Christian Drosten, Terry C. Jones, Victor M. Corman, Florian Kurth, Stefan Hippenstiel, Sascha S. Haenel, Mirja Mittermaier, Fridolin Steinbeis, Tilman Lingscheid, Bettina Temmesfeld-Wollbrück, Thomas Zoller, Holger Müller-Redetzky, Alexander Uhrig, Daniel Grund, Christoph Ruwwe-Glösenkamp, Miriam S. Stegemann, Katrin M. Heim, Ralf H. Hübner, Bastian Opitz, Kai-Uwe Eckardt, Martin Möckel, Felix Balzer, Claudia Spies, Steffen Weber-Carstens, Frank Tacke, Chantip Dang-Heine, Michael Hummel, Georg Schwanitz, Uwe D. Behrens, Maria Rönnefarth, Sein Schmidt, Alexander Krannich, Christof von Kalle, Linda Jürgens, Malte Kleinschmidt, Sophy Denker, Moritz Pfeiffer, Belén Millet Pascual-Leone, Luisa Mrziglod, Felix Machleidt, Sebastian Albus, Felix Bremer, Jan-Moritz Doehn, Tim Andermann, Carmen Garcia, Philipp Knape, Philipp M. Krause, Liron Lechtenberg, Yaosi Li, Panagiotis Pergantis, Till Jacobi, Teresa Ritter, Berna Yedikat, Lennart Pfannkuch, Christian Zobel, Ute Kellermann, Susanne Fieberg, Laure Bosquillon de Jarcy, Anne Wetzel, Christoph Tabeling, Markus C. Brack, Moritz Müller-Plathe, Jan M. Kruse, Daniel Zickler, Andreas Edel, Britta Stier, Roland Körner, Nils B. Müller, Philipp Enghard, Paula Stubbemann, Nadine Olk, Willi M. Koch, Alexandra Horn, Katrin K. Stoyanova, Saskia Zvorc, Lucie Kretzler, Lil A. Meyer-Arndt, Linna Li, Isabelle Wirsching, Denise Treue, Dana Briesemeister, Jenny Schlesinger, Birgit Sawitzki, Lara Bardtke, Kai Pohl, Philipp Georg, Daniel Wendisch, Anna L. Hiller, Sophie Brumhard, Marie Luisa Schmidt, Leonie Meiners, and Patricia Tscheak

Subjects

0301 basic medicine, Microbiology (medical), medicine.medical_specialty, Coronavirus disease 2019 (COVID-19), Respiratory System, 030106 microbiology, Anti-Inflammatory Agents, Antibodies, Viral, Gastroenterology, Dexamethasone, Virus, 03 medical and health sciences, COVID-19 Nucleic Acid testing, 0302 clinical medicine, Internal medicine, medicine, Humans, Prospective Studies, 030212 general & internal medicine, Seroconversion, Antibody, Viral concentration, biology, SARS-CoV-2, business.industry, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), COVID-19, General Medicine, Viral Load, Immunoglobulin A, COVID-19 Drug Treatment, Hospitalization, Research Note, Kinetics, Infectious Diseases, medicine.anatomical_structure, Immunoglobulin G, biology.protein, RNA, Viral, Observational study, business, Viral load, medicine.drug, Respiratory tract

Abstract

Objectives Dexamethasone has become the standard of care for severe coronavirus disease 2019 (COVID-19), but its virological impact is poorly understood. The objectives of this work were to characterize the kinetics of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) concentration in the upper respiratory tract (URT) and the antibody response in patients with (D+) and without (D–) dexamethasone treatment. Methods Data and biosamples from hospitalized patients with severe COVID-19, enrolled between 4th March and 11th December 2020 in a prospective observational study, were analysed. SARS-CoV-2 virus concentration in serial URT samples was measured using RT-PCR. SARS-CoV-2-specific immunoglobulins A and G (IgA and IgG) were measured in serum samples using S1-ELISA. Results We compared 101 immunocompetent patients who received dexamethasone (according to the inclusion criteria and dosage determined in the RECOVERY trial) to 93 immunocompetent patients with comparable disease severity from the first months of the pandemic, who had not been treated with dexamethasone or other glucocorticoids. We found no inter-group differences in virus concentration kinetics, duration of presence of viral loads >106 viral copies/mL (D+ median 17 days (IQR 13–24), D– 19 days (IQR 13–29)), or time from symptom onset until seroconversion (IgA: D+ median 11.5 days (IQR 11–12), D– 14 days (IQR 11.5–15.75); IgG: D+ 13 days (IQR 12–14.5), D– 12 days (IQR 11–15)). Conclusion Dexamethasone does not appear to lead to a change in virus clearance or a delay in antibody response in immunocompetent patients hospitalized with severe COVID-19.

Published

2021

15. Recognition of microbial viability via TLR8 drives TFH cell differentiation and vaccine responses

Author

Sumanlatha Gaddam, Andreas Hutloff, Susanne Hartmann, Melanie L. Conrad, Kristina Dietert, Philipp Georg, Jenny Gerhard, Florian Kurth, Mark V. Boekschoten, Matteo Ugolini, Norbert Suttorp, Bastian Opitz, Christine Stabell Benn, Alexander Schäfer, Shruthi Thada, Ralf R. Schumann, Ulrike Blohm, Laura Bauer, Nickel Dittrich, Leif E. Sander, Elisa T Helbig, Michael Müller, Achim D. Gruber, Saubashya Sur, Gregers Jungersen, Kristoffer Jarlov Jensen, Sarah M. Volkers, Friederike Ebner, and Sanne Burkert

Subjects

Adult, Male, 0301 basic medicine, Vaccines, Attenuated/immunology, Antibody Formation/immunology, Swine, T cell, Cellular differentiation, Immunology, Cell, Lymphocyte Activation/immunology, Biology, Cell Differentiation/immunology, Toll-Like Receptor 8/immunology, Voeding, Metabolisme en Genomica, 03 medical and health sciences, SDG 3 - Good Health and Well-being, T-Lymphocytes, Helper-Inducer/immunology, Voeding, medicine, Animals, Humans, Life Science, Immunology and Allergy, VLAG, Nutrition, Attenuated vaccine, Microbial Viability, TLR8, Metabolism and Genomics, Bacterial vaccine, Vaccination, 030104 developmental biology, medicine.anatomical_structure, Metabolisme en Genomica, Female, Microbial Viability/immunology, Nutrition, Metabolism and Genomics

Abstract

Live attenuated vaccines are generally highly efficacious and often superior to inactivated vaccines, yet the underlying mechanisms of this remain largely unclear. Here we identify recognition of microbial viability as a potent stimulus for follicular helper T cell (TFH cell) differentiation and vaccine responses. Antigen-presenting cells (APCs) distinguished viable bacteria from dead bacteria through Toll-like receptor 8 (TLR8)-dependent detection of bacterial RNA. In contrast to dead bacteria and other TLR ligands, live bacteria, bacterial RNA and synthetic TLR8 agonists induced a specific cytokine profile in human and porcine APCs, thereby promoting TFH cell differentiation. In domestic pigs, immunization with a live bacterial vaccine induced robust TFH cell and antibody responses, but immunization with its heat-killed counterpart did not. Finally, a hypermorphic TLR8 polymorphism was associated with protective immunity elicited by vaccination with bacillus Calmette-Guérin (BCG) in a human cohort. We have thus identified TLR8 as an important driver of TFH cell differentiation and a promising target for TFH cell-skewing vaccine adjuvants.

Published

2018

16. Adjuvant immunotherapies as a novel approach to bacterial infections

Author

Elisa T Helbig, Bastian Opitz, and Leif E. Sander

Subjects

Innate immune system, medicine.drug_class, medicine.medical_treatment, Immunology, Antibiotics, Treatment options, Immunotherapy, Bacterial Infections, Biology, Immune system, Oncology, Adjuvants, Immunologic, Immune System, Tissue damage, medicine, Immunology and Allergy, Humans, Adjuvant

Abstract

The rapid emergence of multidrug-resistant pathogens, especially Gram-negative bacteria and mycobacteria, represents one of the major medical challenges of the 21st century. The gradual loss of effective classical antibiotics for many bacterial pathogens, combined with an increasing population density and mobility, urgently calls for the development of novel treatments. Here, we discuss the potential of adjuvant immunotherapies to selectively stimulate protective immune responses as a treatment option for bacterial infections. In order to elicit appropriate immune responses and to avoid unwanted inflammatory tissue damage, it is essential to identify ligands and receptor pathways that specifically control protective responses at the site of infection. We summarize existing data and discuss suitable candidate targets for future immunotherapies of infectious diseases.

Published

2013

17. Short- and long-term T cell and antibody responses following dexamethasone treatment in COVID-19

Author

Charlotte Thibeault, Lara Bardtke, Kanika Vanshylla, Veronica di Cristanziano, Kirsten A. Eberhardt, Paula Stubbemann, David Hillus, Pinkus Tober-Lau, Parnika Mukherjee, Friederike Münn, Lena J. Lippert, Elisa T. Helbig, Tilman Lingscheid, Fridolin Steinbeis, Mirja Mittermaier, Martin Witzenrath, Thomas Zoller, Pa-COVID study group, Florian Klein, Leif E. Sander, and Florian Kurth

Subjects

Immunology, Infectious disease, Medicine

Abstract

BACKGROUND After its introduction as standard-of-care for severe COVID-19, dexamethasone has been administered to a large number of patients globally. Detailed knowledge of its impact on the cellular and humoral immune response to SARS-CoV-2 remains scarce.METHODS We included immunocompetent individuals with (a) mild COVID-19, (b) severe COVID-19 before introduction of dexamethasone treatment, and (c) severe COVID-19 infection treated with dexamethasone from prospective observational cohort studies at Charité-Universitätsmedizin Berlin, Germany. We analyzed SARS-CoV-2 spike–reactive T cells, spike-specific IgG titers, and serum neutralizing activity against B.1.1.7 and B.1.617.2 in samples ranging from 2 weeks to 6 months after infection. We also analyzed BA.2 neutralization in sera after booster immunization.RESULTS Patients with severe COVID-19 and dexamethasone treatment had lower T cell and antibody responses to SARS-CoV-2 compared with patients without dexamethasone treatment in the early phase of disease, which converged in both groups before 6 months after infection and also after immunization. Patients with mild COVID-19 had comparatively lower T cell and antibody responses than patients with severe disease, including a lower response to booster immunization during convalescence.CONCLUSION Dexamethasone treatment was associated with a short-term reduction in T cell and antibody responses in severe COVID-19 when compared with the nontreated group, but this difference evened out 6 months after infection. We confirm higher cellular and humoral immune responses in patients after severe versus mild COVID-19 and the concept of improved hybrid immunity upon immunization.FUNDING Berlin Institute of Health, German Federal Ministry of Education, and German Federal Institute for Drugs and Medical Devices.

Published

2023

18. Delayed Antibody and T-Cell Response to BNT162b2 Vaccination in the Elderly, Germany

Author

Tatjana Schwarz, Pinkus Tober-Lau, David Hillus, Elisa T. Helbig, Lena J. Lippert, Charlotte Thibeault, Willi Koch, Irmgard Landgraf, Janine Michel, Leon Bergfeld, Daniela Niemeyer, Barbara Mühlemann, Claudia Conrad, Chantip Dang-Heine, Stefanie Kasper, Friederike Münn, Kai Kappert, Andreas Nitsche, Rudolf Tauber, Sein Schmidt, Piotr Kopankiewicz, Harald Bias, Joachim Seybold, Christof von Kalle, Terry C. Jones, Norbert Suttorp, Christian Drosten, Leif Erik Sander, Victor M. Corman, and Florian Kurth

Subjects

vaccine, mRNA, immunity, T cell, B cell, antibody, Medicine, Infectious and parasitic diseases, RC109-216

Abstract

We detected delayed and reduced antibody and T-cell responses after BNT162b2 vaccination in 71 elderly persons (median age 81 years) compared with 123 healthcare workers (median age 34 years) in Germany. These data emphasize that nonpharmaceutical interventions for coronavirus disease remain crucial and that additional immunizations for the elderly might become necessary.

Published

2021

19. Outbreak of SARS-CoV-2 B.1.1.7 Lineage after Vaccination in Long-Term Care Facility, Germany, February–March 2021

Author

Pinkus Tober-Lau, Tatjana Schwarz, David Hillus, Jana Spieckermann, Elisa T. Helbig, Lena J. Lippert, Charlotte Thibeault, Willi Koch, Leon Bergfeld, Daniela Niemeyer, Barbara Mühlemann, Claudia Conrad, Stefanie Kasper, Friederike Münn, Frank Kunitz, Terry C. Jones, Norbert Suttorp, Christian Drosten, Leif Erik Sander, Florian Kurth, and Victor M. Corman

Subjects

vaccine, mRNA, outbreak, phylogeny, immunity, T cell, Medicine, Infectious and parasitic diseases, RC109-216

Abstract

One week after second vaccinations were administered, an outbreak of B.1.1.7 lineage severe acute respiratory syndrome coronavirus 2 infections occurred in a long-term care facility in Berlin, Germany, affecting 16/20 vaccinated and 4/4 unvaccinated residents. Despite considerable viral loads, vaccinated residents experienced mild symptoms and faster time to negative test results.

Published

2021