AI Article Synopsis

  • The study investigates DNA methylation as a potential biomarker for distinguishing between SARS-CoV-2 infected patients and uninfected controls, with implications for predicting disease severity.
  • Using a customized Illumina methylation array, researchers analyzed blood samples from 164 COVID-19 patients and 296 controls, identifying over 13,000 significant methylation sites linked to immune response pathways.
  • Machine learning models demonstrated high predictive accuracy for determining case status and likelihood of severe outcomes, highlighting the relevance of epigenetic signatures in diagnosing and forecasting COVID-19 progression.

Article Abstract

Background: Since the onset of the SARS-CoV-2 pandemic, most clinical testing has focused on RT-PCR. Host epigenome manipulation post coronavirus infection suggests that DNA methylation signatures may differentiate patients with SARS-CoV-2 infection from uninfected individuals, and help predict COVID-19 disease severity, even at initial presentation.

Methods: We customized Illumina's Infinium MethylationEPIC array to enhance immune response detection and profiled peripheral blood samples from 164 COVID-19 patients with longitudinal measurements of disease severity and 296 patient controls.

Results: Epigenome-wide association analysis revealed 13,033 genome-wide significant methylation sites for case-vs-control status. Genes and pathways involved in interferon signaling and viral response were significantly enriched among differentially methylated sites. We observe highly significant associations at genes previously reported in genetic association studies (e.g. IRF7, OAS1). Using machine learning techniques, models built using sparse regression yielded highly predictive findings: cross-validated best fit AUC was 93.6% for case-vs-control status, and 79.1%, 80.8%, and 84.4% for hospitalization, ICU admission, and progression to death, respectively.

Conclusions: In summary, the strong COVID-19-specific epigenetic signature in peripheral blood driven by key immune-related pathways related to infection status, disease severity, and clinical deterioration provides insights useful for diagnosis and prognosis of patients with viral infections.

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Source
http://dx.doi.org/10.1038/s43856-021-00042-yDOI Listing

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