Insights of How Lung Microbiome can Contribute to COVID-19 Severity in Intensive Care Unit Patients

Fab�ola Marques de Carvalho; Le; ro Nascimento Lemos; Luciane Prioli Ciapina; Rennan Garcias Moreira; Alex; ra Gerber; Ana Paula C. Guimar�es; Tatiani Fereguetti; Virg�nia Antunes de Andrade Zambelli; Renata Avila; Tailah Bernardo de Almeida; Jheimson da Silva Lima; Shana Priscila C. Barroso; Mauro Martins Teixeira; Renan Pedra Souza; Cynthia Chester Cardoso; Renato Santana Aguiar; Ana Tereza R. de Vasconcelos

doi:10.35248/2157-7560.21.12.450

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Abstract

Insights of How Lung Microbiome can Contribute to COVID-19 Severity in Intensive Care Unit Patients

Fabíola Marques de Carvalho, Leandro Nascimento Lemos, Luciane Prioli Ciapina, Rennan Garcias Moreira, Alexandra Gerber, Ana Paula C. Guimarães, Tatiani Fereguetti, Virgínia Antunes de Andrade Zambelli, Renata Avila, Tailah Bernardo de Almeida, Jheimson da Silva Lima, Shana Priscila C. Barroso, Mauro Martins Teixeira, Renan Pedra Souza, Cynthia Chester Cardoso, Renato Santana Aguiar and Ana Tereza R. de Vasconcelos*

Objectives: Secondary bacterial and fungal infections are associated with respiratory viral infections and invasive mechanical ventilation. Microbiome influence on COVID-19 severity in patients admitted to intensive care units (ICU) remains poorly understood. This work described the lung microbiota of Brazilian COVID-19 patients and explored how microbial pathogens can contribute to Coronavirus disease 2019 clinical outcome.

Methods: Total DNA of bronchoalveolar lavage fluids from 21 Brazilian COVID-19 patients was extracted. All patients were positive RT-PCR and admitted to intensive care units in two Brazilian centers. For metagenomic analyses, sequenced reads were submitted to bioinformatic tools for taxonomic and functional inferences.

Results: We identified respiratory, nosocomial, and opportunistic pathogens as prevalent bacteria in the lung, suggesting a dysbiosis process (microbial imbalance) in ICU COVID-19 patients. Microbial functional analyses showed metabolic pathways associated with virulence repertoire, such as biofilm production, secreted toxins, capsular polysaccharides, and iron acquisition. Microbial pathogens and their virulence mechanisms were associated with host immunological responses, and a cellular model suggesting how bacterial species could participate in COVID-19 worsening was presented.

Conclusion: We explore how microbial species present in the lung could potentially modulate and aggravate the immunological processes of patients admitted to intensive care units, contributing to COVID-19 severity.

Published Date: 2021-05-20; Received Date: 2021-04-28