Clinical classifiers of COVID-19 infection from novel ultra-high-throughput proteomics

  1. Christoph B. Messner
  2. Vadim Demichev
  3. Daniel Wendisch
  4. Laura Michalick
  5. Matthew White
  6. Anja Freiwald
  7. Kathrin Textoris-Taube
  8. Spyros I. Vernardis
  9. Anna-Sophia Egger
  10. Marco Kreidl
  11. Daniela Ludwig
  12. Christiane Kilian
  13. Federica Agostini
  14. Aleksej Zelezniak
  15. Charlotte Thibeault
  16. Moritz Pfeiffer
  17. Stefan Hippenstiel
  18. Andreas Hocke
  19. Christof von Kalle
  20. Archie Campbell
  21. Caroline Hayward
  22. David J. Porteous
  23. Riccardo E. Marioni
  24. Claudia Langenberg
  25. Kathryn S. Lilley
  26. Wolfgang M. Kuebler
  27. Michael Mülleder
  28. Christian Drosten
  29. Martin Witzenrath
  30. Florian Kurth
  31. Leif Erik Sander
  32. Markus Ralser
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Abstract

The COVID-19 pandemic is an unprecedented global challenge. Highly variable in its presentation, spread and clinical outcome, novel point-of-care diagnostic classifiers are urgently required. Here, we describe a set of COVID-19 clinical classifiers discovered using a newly designed low-cost high-throughput mass spectrometry-based platform. Introducing a new sample preparation pipeline coupled with short-gradient high-flow liquid chromatography and mass spectrometry, our methodology facilitates clinical implementation and increases sample throughput and quantification precision. Providing a rapid assessment of serum or plasma samples at scale, we report 27 biomarkers that distinguish mild and severe forms of COVID-19, of which some may have potential as therapeutic targets. These proteins highlight the role of complement factors, the coagulation system, inflammation modulators as well as pro-inflammatory signalling upstream and downstream of Interleukin 6. Application of novel methodologies hence transforms proteomics from a research tool into a rapid-response, clinically actionable technology adaptable to infectious outbreaks.

Highlights

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    A completely redesigned clinical proteomics platform increases throughput and precision while reducing costs.

  • <label>-</label>

    27 biomarkers are differentially expressed between WHO severity grades for COVID-19.

  • <label>-</label>

    The study highlights potential therapeutic targets that include complement factors, the coagulation system, inflammation modulators as well as pro-inflammatory signalling both upstream and downstream of interleukin 6.

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