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Differential interferon- $\alpha$ subtype induced immune signatures are associated with suppression of SARS-CoV-2 infection

Author: Billaud Jean-Noel (Dr.)
Bracht Thilo
Brunotte Linda
Chen Jieliang
Di Yunyun
Dittmer Ulf (Prof. Dr. rer. nat.)
Eisenacher Martin (PD Dr. rer. medic.)
Elsner Carina (Dr. rer. nat.)
Falzarano Darryl (PhD)
Haid Sibylle (Dr. rer. nat.)
Heinen Natalie (M.Sc.)
Karakoese Zehra (M. Sc.)
Krawczyk Adalbert (PD Dr. rer. nat.)
Kumar Sriram
Lavender Kerry J.
Le-Trilling Vu Thuy Khanh (Dr. rer. nat.)
Lew Jocelyne
Ludwig Stephan (Prof. Dr.)
Meister Toni Luise (M.Sc.)
Pfänder Stephanie (Dr. rer. nat.)
Pietschmann Thomas (Prof. Dr. rer. nat.)
Schork Karin
Schuhenn Jonas (M. Sc.)
Sitek Barbara (Dr.)
Steinmann Eike (Prof. Dr. rer. nat.)
Sutter Kathrin (Dr. rer. nat.)
Taube Christian (Dr. med.)
Todt Daniel Matthias (Dr. rer. nat.)
Trilling Mirko (Prof. Dr. rer. nat.)
Wiegmann Bettina Pamela (Dr. med.)
Yuan Zhenghong
Übner Hendrik
Publication venue
Publication date: 07/02/2022
Field of study

Type I interferons (IFN-I) exert pleiotropic biological effects during viral infections, balancing virus control versus immune-mediated pathologies, and have been successfully employed for the treatment of viral diseases. Humans express 12 IFN-alpha (

\alpha

) subtypes, which activate downstream signaling cascades and result in distinct patterns of immune responses and differential antiviral responses. Inborn errors in IFN-I immunity and the presence of anti-IFN autoantibodies account for very severe courses of COVID-19; therefore, early administration of IFN-I may be protective against life-threatening disease. Here we comprehensively analyzed the antiviral activity of all IFN

\alpha

subtypes against severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) to identify the underlying immune signatures and explore their therapeutic potential. Prophylaxis of primary human airway epithelial cells (hAEC) with different IFN

\alpha

subtypes during SARS-CoV-2 infection uncovered distinct functional classes with high, intermediate, and low antiviral IFNs. In particular, IFN

\alpha

5 showed superior antiviral activity against SARS-CoV-2 infection in vitro and in SARS-CoV-2–infected mice in vivo. Dose dependency studies further displayed additive effects upon coadministration with the broad antiviral drug remdesivir in cell culture. Transcriptomic analysis of IFN-treated hAEC revealed different transcriptional signatures, uncovering distinct, intersecting, and prototypical genes of individual IFN

\alpha

subtypes. Global proteomic analyses systematically assessed the abundance of specific antiviral key effector molecules which are involved in IFN-I signaling pathways, negative regulation of viral processes, and immune effector processes for the potent antiviral IFN

\alpha

5. Taken together, our data provide a systemic, multimodular definition of antiviral host responses mediated by defined IFN-I. This knowledge will support the development of novel therapeutic approaches against SARS-CoV-2

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