COVID-19 in non-hospitalised adults caused by either SARS-CoV-2 sub-variants Omicron BA.1, BA.2, BA.4/5 or Delta associates with similar illness duration, symptom severity and viral kinetics, irrespective of vaccination history

Hermaleigh Townsley; Joshua Gahir; Timothy W Russell; David Greenwood; Edward J Carr; Matala Dyke; Lorin Adams; Murad Miah; Bobbi Clayton; Callie Smith; Mauro Miranda; Harriet V Mears; Chris Bailey; James R M Black; Ashley S Fowler; Margaret Crawford; Katalin Wilkinson; Matthew Hutchinson; Ruth Harvey; Nicola O'Reilly; Gavin Kelly; Robert Goldstone; Rupert Beale; Padmasayee Papineni; Tumena Corrah; Richard Gilson; Simon Caidan; Jerome Nicod; Steve Gamblin; George Kassiotis; Vincenzo Libri; Bryan Williams; Sonia Gandhi; Adam J Kucharski; Charles Swanton; David L V Bauer; Emma C Wall

doi:10.1371/journal.pone.0294897

COVID-19 in non-hospitalised adults caused by either SARS-CoV-2 sub-variants Omicron BA.1, BA.2, BA.4/5 or Delta associates with similar illness duration, symptom severity and viral kinetics, irrespective of vaccination history

PLoS One. 2024 Mar 21;19(3):e0294897. doi: 10.1371/journal.pone.0294897. eCollection 2024.

Authors

Hermaleigh Townsley^{1

2}, Joshua Gahir^{1

2}, Timothy W Russell³, David Greenwood¹, Edward J Carr¹, Matala Dyke^{1

2}, Lorin Adams⁴, Murad Miah¹, Bobbi Clayton¹, Callie Smith¹, Mauro Miranda¹, Harriet V Mears¹, Chris Bailey¹, James R M Black^{1

5}, Ashley S Fowler¹, Margaret Crawford¹, Katalin Wilkinson¹, Matthew Hutchinson¹, Ruth Harvey^{1

4}, Nicola O'Reilly¹, Gavin Kelly¹, Robert Goldstone¹, Rupert Beale^{1

5

6}, Padmasayee Papineni⁷, Tumena Corrah⁷, Richard Gilson⁸, Simon Caidan¹, Jerome Nicod¹, Steve Gamblin¹, George Kassiotis^{1

9}, Vincenzo Libri^{2

4}, Bryan Williams^{2

4}, Sonia Gandhi^{1

5}, Adam J Kucharski³, Charles Swanton^{1

5}, David L V Bauer^{1

6}, Emma C Wall^{1

2}

Affiliations

¹ The Francis Crick Institute, London, United Kingdom.
² National Institute for Health Research (NIHR) University College London Hospitals (UCLH) Biomedical Research Centre and NIHR UCLH Clinical Research Facility, London, United Kingdom.
³ Centre for Mathematical Modelling of Infectious Diseases, London School of Hygiene & Tropical Medicine, London, United Kingdom.
⁴ Worldwide Influenza Centre, The Francis Crick Institute, London, United Kingdom.
⁵ University College London, London, United Kingdom.
⁶ Genotype-to-Phenotype UK National Virology Consortium (G2P-UK).
⁷ London Northwest University Healthcare NHS Trust, London, United Kingdom.
⁸ Camden and North West London NHS Community Trust, London, United Kingdom.
⁹ Department of Infectious Disease, St Mary's Hospital, Imperial College London, London, United Kingdom.

Abstract

Background: SARS-CoV-2 variant Omicron rapidly evolved over 2022, causing three waves of infection due to sub-variants BA.1, BA.2 and BA.4/5. We sought to characterise symptoms and viral loads over the course of COVID-19 infection with these sub-variants in otherwise-healthy, vaccinated, non-hospitalised adults, and compared data to infections with the preceding Delta variant of concern (VOC).

Methods: In a prospective, observational cohort study, healthy vaccinated UK adults who reported a positive polymerase chain reaction (PCR) or lateral flow test, self-swabbed on alternate weekdays until day 10. We compared participant-reported symptoms and viral load trajectories between infections caused by VOCs Delta and Omicron (sub-variants BA.1, BA.2 or BA.4/5), and tested for relationships between vaccine dose, symptoms and PCR cycle threshold (Ct) as a proxy for viral load using Chi-squared (χ2) and Wilcoxon tests.

Results: 563 infection episodes were reported among 491 participants. Across infection episodes, there was little variation in symptom burden (4 [IQR 3-5] symptoms) and duration (8 [IQR 6-11] days). Whilst symptom profiles differed among infections caused by Delta compared to Omicron sub-variants, symptom profiles were similar between Omicron sub-variants. Anosmia was reported more frequently in Delta infections after 2 doses compared with Omicron sub-variant infections after 3 doses, for example: 42% (25/60) of participants with Delta infection compared to 9% (6/67) with Omicron BA.4/5 (χ2 P < 0.001; OR 7.3 [95% CI 2.7-19.4]). Fever was less common with Delta (20/60 participants; 33%) than Omicron BA.4/5 (39/67; 58%; χ2 P = 0.008; OR 0.4 [CI 0.2-0.7]). Amongst infections with an Omicron sub-variants, symptoms of coryza, fatigue, cough and myalgia predominated. Viral load trajectories and peaks did not differ between Delta, and Omicron, irrespective of symptom severity (including asymptomatic participants), VOC or vaccination status. PCR Ct values were negatively associated with time since vaccination in participants infected with BA.1 (β = -0.05 (CI -0.10-0.01); P = 0.031); however, this trend was not observed in BA.2 or BA.4/5 infections.

Conclusion: Our study emphasises both the changing symptom profile of COVID-19 infections in the Omicron era, and ongoing transmission risk of Omicron sub-variants in vaccinated adults.

Trial registration: NCT04750356.

Copyright: © 2024 Townsley et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.

Publication types

Observational Study

MeSH terms

Adult
COVID-19* / prevention & control
Humans
Prospective Studies
SARS-CoV-2
Vaccination

Supplementary concepts

SARS-CoV-2 variants

Associated data

ClinicalTrials.gov/NCT04750356

Grants and funding

This work was supported by UCLH/UCL who received a proportion of funding from the National Institute for Health Research (NIHR) University College London Hospitals Department of Health’s NIHR Biomedical Research Centre (BRC). EW, VL and BW are supported by the Centre’s funding scheme. This work was supported jointly by the BRC and core funding from the Francis Crick Institute, which receives its funding from Cancer Research UK, the UK Medical Research Council, and the Wellcome Trust. This research was funded in whole, or in part, by the Wellcome Trust [FC011104, FC011233, FC001030, FC001159, FC001827, FC001078, FC001099, FC001169, 206250/Z/17/Z]. For the purpose of Open Access, the author has applied a CC BY public copyright licence to any Author Accepted Manuscript version arising from this submission. DLVB is additionally supported by the Genotype-to-Phenotype National Virology Consortium (G2P-UK) via UK Research and Innovation and the UK Medical Research Council, and TWR and AJK are additionally supported by the Wellcome Trust.