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In vivo kinetics of SARS-CoV-2 infection and its relationship with a person's infectiousness.

Ruian KeCarolin ZitzmannDavid D HoRuy M RibeiroAlan S Perelson
Published in: Proceedings of the National Academy of Sciences of the United States of America (2021)
The within-host viral kinetics of SARS-CoV-2 infection and how they relate to a person's infectiousness are not well understood. This limits our ability to quantify the impact of interventions on viral transmission. Here, we develop viral dynamic models of SARS-CoV-2 infection and fit them to data to estimate key within-host parameters such as the infected cell half-life and the within-host reproductive number. We then develop a model linking viral load (VL) to infectiousness and show a person's infectiousness increases sublinearly with VL and that the logarithm of the VL in the upper respiratory tract is a better surrogate of infectiousness than the VL itself. Using data on VL and the predicted infectiousness, we further incorporated data on antigen and RT-PCR tests and compared their usefulness in detecting infection and preventing transmission. We found that RT-PCR tests perform better than antigen tests assuming equal testing frequency; however, more frequent antigen testing may perform equally well with RT-PCR tests at a lower cost but with many more false-negative tests. Overall, our models provide a quantitative framework for inferring the impact of therapeutics and vaccines that lower VL on the infectiousness of individuals and for evaluating rapid testing strategies.
Keyphrases
  • sars cov
  • respiratory tract
  • electronic health record
  • respiratory syndrome coronavirus
  • big data
  • physical activity
  • single cell
  • small molecule
  • stem cells
  • real time pcr
  • mesenchymal stem cells