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Ioanna D. Gemünd

ORCID: 0000-0003-2217-4178
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A5047255670
Research Areas
  • COVID-19 Clinical Research Studies
  • Neutrophil, Myeloperoxidase and Oxidative Mechanisms
  • Blood disorders and treatments
  • SARS-CoV-2 and COVID-19 Research
  • Immune responses and vaccinations
  • Hepatitis B Virus Studies
  • Hepatitis Viruses Studies and Epidemiology
  • SARS-CoV-2 detection and testing
  • Liver Disease Diagnosis and Treatment
  • Inflammasome and immune disorders
  • Long-Term Effects of COVID-19
  • Immune cells in cancer
  • Gene expression and cancer classification
  • Bioinformatics and Genomic Networks
  • Neuroinflammation and Neurodegeneration Mechanisms
  • Single-cell and spatial transcriptomics
  • Complement system in diseases
  • Immune Cell Function and Interaction

University of Bonn
 2020-2023

Peter Doherty Institute
 2021-2023

The University of Melbourne
 2021-2023

German Center for Neurodegenerative Diseases
 2022-2023

Epigenomics (Germany)
 2021

Charité - Universitätsmedizin Berlin
 2021

Life & Brain (Germany)
 2019

 Disease severity-specific neutrophil signatures in blood transcriptomes stratify COVID-19 patients
OPENALEX - Publications 
Anna C. Aschenbrenner Maria Mouktaroudi Benjamin Krämer Marie Oestreich Nikolaos Antonakos and 50 more Melanie Nuesch-Germano Konstantina Gkizeli Lorenzo Bonaguro Nico Reusch Kevin Baßler Maria Saridaki Rainer Knoll Tal Pecht Theodore S. Kapellos Sarandia Doulou Charlotte Kröger Miriam Herbert Lisa Holsten Arik Horne Ioanna D. Gemünd Νikoletta Ρovina Shobhit Agrawal K. Dahm Martina Van Uelft Anna Drews Lena Lenkeit Niklas Bruse Jelle Gerretsen Jannik Gierlich Matthias Becker Kristian Händler Michael Kraut Heidi Theis Simachew Mengiste Elena De Domenico Eva C. Schulte Lea Seep Jan Raabe Christoph Hoffmeister Michael ToVinh Verena Keitel Gereon Rieke Valentina Talevi Dirk Skowasch N. Ahmad Aziz Peter Pickkers Frank L. van de Veerdonk Mihai G. Netea Joachim L. Schultze Matthijs Kox Monique M.B. Breteler Jacob Nattermann Antonia Koutsoukou Evangelos J. Giamarellos-Bourboulis Thomas Ulas

Abstract Background The SARS-CoV-2 pandemic is currently leading to increasing numbers of COVID-19 patients all over the world. Clinical presentations range from asymptomatic, mild respiratory tract infection, severe cases with acute distress syndrome, failure, and death. Reports on a dysregulated immune system in call for better characterization understanding changes system. Methods In order dissect COVID-19-driven host responses, we performed RNA-seq whole blood cell transcriptomes...

10.1186/s13073-020-00823-5 article EN cc-by Genome Medicine 2021-01-13
 Complement activation induces excessive T cell cytotoxicity in severe COVID-19
OPENALEX - Publications 
Philipp Georg Rosario Astaburuaga-García Lorenzo Bonaguro Sophia Brumhard Laura Michalick and 53 more Lena J. Lippert Tomislav Kostevc Christiane Gäbel Maria Schneider Mathias Streitz Vadim Demichev Ioanna D. Gemünd Matthias Barone Pinkus Tober‐Lau Elisa T. Helbig David Hillus L. A. Petrov Julia Stein Hannah-Philine Dey Daniela Paclik Christina Iwert Michael Mülleder Simran Kaur Aulakh Sonja Djudjaj Roman D. Bülow Henrik E. Mei Axel Schulz Andreas Thiel Stefan Hippenstiel Antoine‐Emmanuel Saliba Roland Eils Irina Lehmann Marcus Mall Sebastian Stricker Jobst Röhmel Victor M. Corman Dieter Beule Emanuel Wyler Markus Landthaler Benedikt Obermayer Saskia von Stillfried Peter Boor Münevver Demir Hans Wesselmann Norbert Suttorp Alexander Uhrig Holger Müller-Redetzky Jacob Nattermann Wolfgang M. Kuebler Christian Meisel Markus Ralser Joachim L. Schultze Anna C. Aschenbrenner Charlotte Thibeault Florian Kurth Leif Erik Sander Nils Blüthgen Birgit Sawitzki

Severe COVID-19 is linked to both dysfunctional immune response and unrestrained immunopathology, it remains unclear whether T cells contribute disease pathology. Here, we combined single-cell transcriptomics proteomics with mechanistic studies assess pathogenic cell functions inducing signals. We identified highly activated CD16

10.1016/j.cell.2021.12.040 article EN cc-by Cell 2021-12-28
 Circulating CD8 T cells are sentinels for intrahepatic T cell responses during HBV infection
OPENALEX - Publications 
Hannah Wintersteller Miriam Bosch Sainitin Donakonda Ioanna D. Gemünd Anna Fürst and 10 more Anna D. Kosinska Edanur Ateş Öz Roni Souleiman Christine Wurmser Gustavo Almeida Markus Cornberg Dietmar Zehn Dirk Wohlleber Ulrike Protzer Percy A. Knolle

10.1055/s-0044-1801212 article EN Zeitschrift für Gastroenterologie 2025-01-01
 Disease severity-specific neutrophil signatures in blood transcriptomes stratify COVID-19 patients
OPENALEX - Publications 
Anna C. Aschenbrenner Maria Mouktaroudi Benjamin Krämer Nikolaos Antonakos Marie Oestreich and 49 more Konstantina Gkizeli Melanie Nuesch-Germano Maria Saridaki Lorenzo Bonaguro Nico Reusch Kevin Baßler Sarandia Doulou Rainer Knoll Tal Pecht Theodore S. Kapellos Νikoletta Ρovina Charlotte Kröger Miriam Herbert Lisa Holsten Arik Horne Ioanna D. Gemünd Shobhit Agrawal K. Dahm Martina Van Uelft Anna Drews Lena Lenkeit Niklas Bruse Jelle Gerretsen Jannik Gierlich Matthias Becker Kristian Händler Michael Kraut Heidi Theis Simachew Mengiste Elena De Domenico Jonas Schulte-Schrepping Lea Seep Jan Raabe Christoph Hoffmeister Michael ToVinh Verena Keitel Gereon Rieke Valentina Talevi N. Ahmad Aziz Peter Pickkers Frank L. van de Veerdonk Mihai G. Netea Joachim L. Schultze Matthijs Kox Monique M.B. Breteler Jacob Nattermann Antonia Koutsoukou Evangelos J. Giamarellos‐Bourboulis Thomas Ulas

SUMMARY The SARS-CoV-2 pandemic is currently leading to increasing numbers of COVID-19 patients all over the world. Clinical presentations range from asymptomatic, mild respiratory tract infection, severe cases with acute distress syndrome, failure, and death. Reports on a dysregulated immune system in calls for better characterization understanding changes system. Here, we profiled whole blood transcriptomes 39 10 control donors enabling data-driven stratification based molecular phenotype....

10.1101/2020.07.07.20148395 preprint EN cc-by-nc-nd medRxiv (Cold Spring Harbor Laboratory) 2020-07-08
 Human variation in population-wide gene expression data predicts gene perturbation phenotype
OPENALEX - Publications 
Lorenzo Bonaguro Jonas Schulte-Schrepping Caterina Carraro Laura L. Sun Benedikt Reiz and 14 more Ioanna D. Gemünd Adem Saglam Souad Rahmouni Michel Georges Peer Arts Alexander Hoischen Leo A. B. Joosten Frank L. van de Veerdonk Mihai G. Netea Kristian Händler Sach Mukherjee Thomas Ulas Joachim L. Schultze Anna C. Aschenbrenner

Population-scale datasets of healthy individuals capture genetic and environmental factors influencing gene expression. The expression variance a interest (GOI) can be exploited to set up quasi loss- or gain-of-function "

10.1016/j.isci.2022.105328 article EN cc-by-nc-nd iScience 2022-10-12
 Complement Activation Induces Excessive T Cell Cytotoxicity in Severe COVID-19
OPENALEX - Publications 
Philipp Georg Rosario Astaburuaga-García Lorenzo Bonaguro Sophia Brumhard Laura Michalick and 40 more Lena J. Lippert Tomislav Kostevc Christiane Gäbel Maria Schneider Mathias Streitz Vadim Demichev Ioanna D. Gemünd Matthias Barone Pinkus Tober‐Lau Elisa Theresa Helbig Julia Stein Hannah-Philine Dey Daniela Paclik Michael Mülleder Simran Kaur Aulakh Henrik E. Mei Axel Schulz Stefan Hippenstiel Victor M. Corman Dieter Beule Emanuel Wyler Markus Landthaler Benedikt Obermayer-Wasserscheid Peter Boor Münevver Demir Hans Wesselmann Norbert Suttorp Alexander Uhrig Holger Müller-Redetzky Jacob Nattermann Wolfgang M. Kuebler Christian Meisel Markus Ralser Joachim L. Schultze Anna C. Aschenbrenner Charlotte Thibeault Florian Kurth Leif Erik Sander Nils Blüthgen Birgit Sawitzki

Severe COVID-19 is linked to both dysfunctional immune response and unrestrained immunopathogenesis, it remains unclear if T cells contribute disease pathology. Here, we combined single-cell transcriptomics proteomics with mechanistic studies assessing pathogenic cell functions inducing signals. We identified activated, CD16+ increased cytotoxic in severe COVID-19. CD16 expression enabled complex-mediated, receptor-independent degranulation cytotoxicity not found other diseases. from...

10.2139/ssrn.3866835 article EN SSRN Electronic Journal 2021-01-01
 Complement activation induces excessive T cell cytotoxicity in severe COVID-19
OPENALEX - Publications 
Philipp Georg Rosario Astaburuaga-García Lorenzo Bonaguro Sophia Brumhard Laura Michalick and 40 more Lena J. Lippert Tomislav Kostevc Christiane Gäbel Maria Schneider Mathias Streitz Vadim Demichev Ioanna D. Gemünd Matthias Barone Pinkus Tober‐Lau Elisa T. Helbig Julia Stein Hannah-Philine Dey Daniela Paclik Michael Mülleder Simran Kaur Aulakh Henrik E. Mei Axel Schulz Stefan Hippenstiel Victor M. Corman Dieter Beule Emanuel Wyler Markus Landthaler Benedikt Obermayer-Wasserscheid Peter Boor Münevver Demir Hans Wesselmann Norbert Suttorp Alexander Uhrig Holger Müller-Redetzky Jacob Nattermann Wolfgang M. Kuebler Christian Meisel Markus Ralser Joachim L. Schultze Anna C. Aschenbrenner Charlotte Thibeault Florian Kurth Leif Erik Sander Nils Blüthgen Birgit Sawitzki

Summary Severe COVID-19 is linked to both dysfunctional immune response and unrestrained immunopathogenesis, it remains unclear if T cells also contribute disease pathology. Here, we combined single-cell transcriptomics proteomics with mechanistic studies assess pathogenic cell functions inducing signals. We identified highly activated, CD16 + increased cytotoxic in severe COVID-19. expression enabled complex-mediated, receptor-independent degranulation cytotoxicity not found other diseases....

10.1101/2021.06.08.21258481 preprint EN medRxiv (Cold Spring Harbor Laboratory) 2021-06-11
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