EBioMedicine (Apr 2021)

Association of SARS-CoV-2 clades with clinical, inflammatory and virologic outcomes: An observational study

  • Barnaby E Young,
  • Wycliffe E Wei,
  • Siew-Wai Fong,
  • Tze-Minn Mak,
  • Danielle E Anderson,
  • Yi-Hao Chan,
  • Rachael Pung,
  • Cheryl SY Heng,
  • Li Wei Ang,
  • Adrian Kang Eng Zheng,
  • Bernett Lee,
  • Shirin Kalimuddin,
  • Surinder Pada,
  • Paul A Tambyah,
  • Purnima Parthasarathy,
  • Seow Yen Tan,
  • Louisa Sun,
  • Gavin JD Smith,
  • Raymond Tzer Pin Lin,
  • Yee-Sin Leo,
  • Laurent Renia,
  • Lin-Fa Wang,
  • Lisa FP Ng,
  • Sebastian Maurer-Stroh,
  • David Chien Lye,
  • Vernon J Lee

Journal volume & issue
Vol. 66
p. 103319

Abstract

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Background: Host determinants of severe coronavirus disease 2019 include advanced age, comorbidities and male sex. Virologic factors may also be important in determining clinical outcome and transmission rates, but limited patient-level data is available. Methods: We conducted an observational cohort study at seven public hospitals in Singapore. Clinical and laboratory data were collected and compared between individuals infected with different SARS-CoV-2 clades. Firth's logistic regression was used to examine the association between SARS-CoV-2 clade and development of hypoxia, and quasi-Poisson regression to compare transmission rates. Plasma samples were tested for immune mediator levels and the kinetics of viral replication in cell culture were compared. Findings: 319 patients with PCR-confirmed SARS-CoV-2 infection had clinical and virologic data available for analysis. 29 (9%) were infected with clade S, 90 (28%) with clade L/V, 96 (30%) with clade G (containing D614G variant), and 104 (33%) with other clades ‘O’ were assigned to lineage B.6. After adjusting for age and other covariates, infections with clade S (adjusted odds ratio (aOR) 0·030 (95% confidence intervals (CI): 0·0002–0·29)) or clade O (B·6) (aOR 0·26 (95% CI 0·064–0·93)) were associated with lower odds of developing hypoxia requiring supplemental oxygen compared with clade L/V. Patients infected with clade L/V had more pronounced systemic inflammation with higher concentrations of pro-inflammatory cytokines, chemokines and growth factors. No significant difference in the severity of clade G infections was observed (aOR 0·95 (95% CI: 0·35–2·52). Though viral loads were significantly higher, there was no evidence of increased transmissibility of clade G, and replicative fitness in cell culture was similar for all clades. Interpretation: Infection with clades L/V was associated with increased severity and more systemic release of pro-inflammatory cytokines. Infection with clade G was not associated with changes in severity, and despite higher viral loads there was no evidence of increased transmissibility.

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