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1. ACE2-independent sarbecovirus cell entry can be supported by TMPRSS2-related enzymes and can reduce sensitivity to antibody-mediated neutralization.

2. Pharmacological inhibition of bromodomain and extra-terminal proteins induces an NRF-2-mediated antiviral state that is subverted by SARS-CoV-2 infection.

3. Reduced IFN-ß inhibitory activity of Lagos bat virus phosphoproteins in human compared to Eidolon helvum bat cells.

4. Impact of time pressure on software quality: A laboratory experiment on a game-theoretical model.

5. The papain-like protease determines a virulence trait that varies among members of the SARS-coronavirus species.

6. Transcriptome profile of lung dendritic cells after in vitro porcine reproductive and respiratory syndrome virus (PRRSV) infection.

7. Serological Evidence of Influenza A Viruses in Frugivorous Bats from Africa.

8. CD26/DPP4 Cell-Surface Expression in Bat Cells Correlates with Bat Cell Susceptibility to Middle East Respiratory Syndrome Coronavirus (MERS-CoV) Infection and Evolution of Persistent Infection.

9. Targeting Membrane-Bound Viral RNA Synthesis Reveals Potent Inhibition of Diverse Coronaviruses Including the Middle East Respiratory Syndrome Virus.

10. Bat Airway Epithelial Cells: A Novel Tool for the Study of Zoonotic Viruses.

11. Differential Sensitivity of Bat Cells to Infection by Enveloped RNA Viruses: Coronaviruses, Paramyxoviruses, Filoviruses, and Influenza Viruses.

12. Evidence for Novel Hepaciviruses in Rodents.

13. Two Novel Parvoviruses in Frugivorous New and Old World Bats.

14. Type I Interferon Reaction to Viral Infection in Interferon-Competent, Immortalized Cell Lines from the African Fruit Bat Eidolon helvum.

15. The SARS-Coronavirus-Host Interactome: Identification of Cyclophilins as Target for Pan-Coronavirus Inhibitors.

16. Henipavirus RNA in African Bats.

17. The papain-like protease determines a virulence trait that varies among members of the SARS-coronavirus species

18. SARS-CoV-2 variant Alpha has a spike-dependent replication advantage over the ancestral B.1 strain in human cells with low ACE2 expression.

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