An Allele of the MTHFR one-carbon metabolism gene predicts severity of COVID-19

  1. Boryana Petrova
  2. Caitlin Syphurs
  3. Andrew J Culhane
  4. Jing Chen
  5. Ernie Chen
  6. Chris Cotsapas
  7. Denise Esserman
  8. Ruth Montgomery
  9. Steven Kleinstein
  10. Kinga Smolen
  11. Kevin Mendez
  12. IMPACC Network
  13. Jessica Lasky-Su
  14. Hanno Steen
  15. Ofer Levy
  16. Joann Diray-Arce
  17. Naama Kanarek
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Abstract

While the public health burden of SARS-CoV-2 infection has lessened due to natural and vaccine-acquired immunity, the emergence of less virulent variants, and antiviral medications, COVID-19 continues to take a significant toll. There are > 10,000 new hospitalizations per week in the U.S., many of whom develop post-acute sequelae of SARS-CoV-2 (PASC), or “long COVID”, with long-term health issues and compromised quality of life. Early identification of individuals at high risk of severe COVID-19 is key for monitoring and supporting respiratory status and improving outcomes. Therefore, precision tools for early detection of patients at high risk of severe disease can reduce morbidity and mortality. Here we report an untargeted and longitudinal metabolomic study of plasma derived from adult patients with COVID-19. One-carbon metabolism, a pathway previously shown as critical for viral propagation and disease progression, and a potential target for COVID-19 treatment, scored strongly as differentially abundant in patients with severe COVID-19. A follow-up targeted metabolite profiling revealed that one arm of the one-carbon metabolism pathway, the methionine cycle, is a major driver of the metabolic profile associated with disease severity. The methionine cycle produces S-adenosylmethionine (SAM), the methyl group donor important for methylation of DNA, RNA, and proteins, and its high abundance was reported to correlate with disease severity. Further, genomic data from the profiled patients revealed a genetic contributor to methionine metabolism and identified the C677T allele of the MTHFR gene as a pre-existing predictor of disease trajectory - patients homozygous for the MTHFR C677T have higher incidence of experiencing severe disease. Our results raise the possibility that screening for the common genetic MTHFR variant may be an actionable approach to stratify risk of COVID severity and may inform novel precision COVID-19 treatment strategies.

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  1. Version published to 10.1101/2025.02.28.25323089v1 on medRxiv