Clinical Sensitivity and Interpretation of PCR and Serological COVID-19 Diagnostics for Patients Presenting to the Hospital

  1. Tyler E. Miller
  2. Wilfredo F. Garcia Beltran
  3. Adam Z. Bard
  4. Tasos Gogakos
  5. Melis N. Anahtar
  6. Michael Gerino Astudillo
  7. Diane Yang
  8. Julia Thierauf
  9. Adam S. Fisch
  10. Grace K. Mahowald
  11. Megan J. Fitzpatrick
  12. Valentina Nardi
  13. Jared Feldman
  14. Blake M. Hauser
  15. Timothy M. Caradonna
  16. Hetal D. Marble
  17. Lauren L. Ritterhouse
  18. Sara E. Turbett
  19. Julie Batten
  20. Nicholas Zeke Georgantas
  21. Galit Alter
  22. Aaron G. Schmidt
  23. Jason B. Harris
  24. Jeffrey A. Gelfand
  25. Mark C. Poznansky
  26. Bradley E. Bernstein
  27. David N. Louis
  28. Anand Dighe
  29. Richelle C. Charles
  30. Edward T. Ryan
  31. John A. Branda
  32. Virginia M. Pierce
  33. Mandakolathur R. Murali
  34. A. John Iafrate
  35. Eric S. Rosenberg
  36. Jochen Lennerz
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Abstract

Introduction

The diagnosis of COVID-19 requires integration of clinical and laboratory data. SARS-CoV-2 diagnostic assays play a central role in diagnosis and have fixed technical performance metrics. Interpretation becomes challenging because the clinical sensitivity changes as the virus clears and the immune response emerges. Our goal was to examine the clinical sensitivity of two most common SARS-CoV-2 diagnostic test modalities, polymerase chain reaction (PCR) and serology, over the disease course to provide insight into their clinical interpretation in patients presenting to the hospital.

Methods

A single-center, retrospective study. To derive clinical sensitivity of PCR, we identified 209 PCR-positive SARS-CoV-2 patients with multiple PCR test results (624 total PCR tests) and calculated daily sensitivity from date of symptom onset or first positive test. To calculate daily clinical sensitivity by serology, we utilized 157 PCR- positive patients with a total of 197 specimens tested by enzyme-linked immunosorbent assay for IgM, IgG, and IgA anti-SARS-CoV-2 antibodies.

Results

Clinical sensitivity of PCR decreased with days post symptom onset with >90% clinical sensitivity during the first 5 days after symptom onset, 70-71% from days 9-11, and 30% at day 21. In contrast, serological sensitivity increased with days post symptom onset with >50% of patients seropositive by at least one antibody isotype after day 7, >80% after day 12, and 100% by day 21.

Conclusion

PCR and serology are complimentary modalities that require time- dependent interpretation. Superimposition of sensitivities over time indicate that serology can function as a reliable diagnostic aid indicating recent or prior infection.

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