Host–microbiome associations in saliva predict COVID-19 severity

Author:

Alqedari Hend12ORCID,Altabtbaei Khaled3ORCID,Espinoza Josh L4ORCID,Bin-Hasan Saadoun5ORCID,Alghounaim Mohammad6,Alawady Abdullah5,Altabtabae Abdullah5,AlJamaan Sarah5,Devarajan Sriraman2,AlShammari Tahreer2,Ben Eid Mohammed5ORCID,Matsuoka Michele4,Jang Hyesun4,Dupont Christopher L4ORCID,Freire Marcelo47ORCID

Affiliation:

1. Department of Public Health and Community Service, Tufts University School of Dental Medicine , 1 Kneeland Street, Boston, MA 02111 , USA

2. Dasman Diabetes Institute , 1180 Dasman, 9XQV+V9 Kuwait City , Kuwait

3. Faculty of Medicine and Dentistry, School of Dentistry, University of Alberta , Edmonton, AB T6G 2L7 , Canada

4. Department of Genomic Medicine and Infectious Diseases, J. Craig Venter Institute , La Jolla, CA 92037 , USA

5. Department of Pediatrics, Farwaniyah Hospital, Ministry of Health , 7XF4+WPJ Al Farwaniyah , Kuwait

6. Department of Pediatrics, Amiri Hospital, Ministry of Health , 9XQQ+42 Kuwait City , Kuwait

7. Division of Infectious Diseases and Global Public Health Department of Medicine, University of California San Diego , La Jolla, CA 92093 , USA

Abstract

Abstract Established evidence indicates that oral microbiota plays a crucial role in modulating host immune responses to viral infection. Following severe acute respiratory syndrome coronavirus 2, there are coordinated microbiome and inflammatory responses within the mucosal and systemic compartments that are unknown. The specific roles the oral microbiota and inflammatory cytokines play in the pathogenesis of coronavirus disease 2019 (COVID-19) are yet to be explored. Here, we evaluated the relationships between the salivary microbiome and host parameters in different groups of COVID-19 severity based on their oxygen requirement. Saliva and blood samples (n = 80) were collected from COVID-19 and from noninfected individuals. We characterized the oral microbiomes using 16S ribosomal RNA gene sequencing and evaluated saliva and serum cytokines and chemokines using multiplex analysis. Alpha diversity of the salivary microbial community was negatively associated with COVID-19 severity, while diversity increased with health. Integrated cytokine evaluations of saliva and serum showed that the oral host response was distinct from the systemic response. The hierarchical classification of COVID-19 status and respiratory severity using multiple modalities separately (i.e. microbiome, salivary cytokines, and systemic cytokines) and simultaneously (i.e. multimodal perturbation analyses) revealed that the microbiome perturbation analysis was the most informative for predicting COVID-19 status and severity, followed by the multimodal. Our findings suggest that oral microbiome and salivary cytokines may be predictive of COVID-19 status and severity, whereas atypical local mucosal immune suppression and systemic hyperinflammation provide new cues to understand the pathogenesis in immunologically compromised populations.

Funder

J Craig Venter Institute, CA, USA

Kuwait Ministry of Health

Dasman Diabetes Institute, Kuwait

L’Oréal-UNESCO

NIH

Conrad Prebys Foundation

Publisher

Oxford University Press (OUP)

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