Analysis Of Salivary Herpesviruses Reveals Associations Between HHV-6 And Long COVID Severity

  1. Claire S. Laxton
  2. Alexandra Tabachnikova
  3. Lily Cooke
  4. Kexin Wang
  5. Simone Blaser
  6. Julio Silva
  7. Jamie Wood
  8. Henna S. Nam
  9. Zhenni Lu
  10. Christine Miller
  11. Gisele Rodrigues
  12. Victoria Fisher
  13. Christian Guirgis
  14. William B. Hooper
  15. Alexandra Lee
  16. Mackenzie Doerstling
  17. Bornali Bhattacharjee
  18. Leying Guan
  19. David Putrino
  20. Akiko Iwasaki
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Abstract

Background

Reactivation of human herpesviruses (HHVs), particularly EBV, is associated with more severe acute SARS-CoV-2 infections and the development of Long COVID (LC). Observations of higher anti-EBV antibody levels in individuals with LC support the idea that chronic reactivation of HHVs could contribute to LC pathology. HHV shedding in saliva has also been previously associated with saliva hormone levels. This study aims to examine the relationship between salivary shedding of HHV DNA and LC symptoms, as well as cortisol, testosterone, and estradiol levels.

Methods

We enrolled 45 participants with LC, and 45 age-sex-matched controls. Surveys and validated health questionnaires were used to collect demographics, medical history, and symptom profiles. Saliva was self-collected at waking, 15, 30, and 45 minutes, and 8 and 16 hours after waking, across two consecutive days. Salivary cortisol, testosterone and estradiol were measured, and extracted nucleic acid was tested for EBV, HSV 1/2, HCMV and HHV-6 A/B using multiplex qPCR, plus SARS-CoV-2 and RNaseP using RT-qPCR.

Findings

Detection of salivary EBV and HHV-6 DNA was highest early in the morning. There were no significant differences in salivary cortisol, testosterone, or estradiol, or in EBV or HHV-6 shedding between the LC and control groups. However, salivary HHV-6 DNA levels were positively associated with a greater aggregated LC propensity score, as well as anxiety and depression scores.

Interpretation

The observed correlation between salivary HHV-6 shedding and symptom severity suggests HHV-6 may contribute to post-acute disease, though mechanisms remain unclear. While our study did not identify a relationship between salivary EBV shedding and LC, EBV may still play a role at earlier time points in the disease course, or in compartments not sampled here. These findings highlight the potential importance of HHV-6 in LC pathophysiology and underscore the need for longitudinal, multi-compartment studies of herpesvirus reactivation in LC.

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  1. Version published to 10.64898/2026.05.19.26353495 on medRxiv