The SARS-CoV-2 Receptor Angiotensin-converting Enzyme 2 (ACE2) in Myalgic Encephalomyelitis/chronic Fatigue Syndrome: A Meta-analysis of Public DNA Methylation and Gene Expression Data

Overview

Journal Heliyon

Specialty Social Sciences

Date 2021 Aug 3

PMID 34341773

Citations 6

Authors

Joao Malato

Franziska Sotzny

Sandra Bauer

Helma Freitag

Andre Fonseca

Anna D Grabowska

Luis Graca

Clara Cordeiro

Luis Nacul

Eliana M Lacerda

Jesus Castro-Marrero

Carmen Scheibenbogen

Francisco Westermeier

Nuno Sepulveda

Affiliations

Soon will be listed here.

Abstract

People with myalgic encephalomyelitis/chronic fatigue syndrome (ME/CFS) often report a high frequency of viral infections and flu-like symptoms during their disease course. Given that this reporting agrees with different immunological abnormalities and altered gene expression profiles observed in the disease, we aimed at answering whether the expression of the human angiotensin-converting enzyme 2 (ACE2), the major cell entry receptor for SARS-CoV-2, is also altered in these patients. In particular, a low expression of could be indicative of a high risk of developing COVID-19. We then performed a meta-analysis of public data on CpG DNA methylation and gene expression of this enzyme and its homologous ACE protein in peripheral blood mononuclear cells and related subsets. We found that patients with ME/CFS have decreased methylation levels of four CpG probes in the locus (cg09920557, cg19802564, cg21094739, and cg10468385) and of another probe in the promoter region of the gene (cg08559914). We also found a decreased expression of but not of in patients when compared to healthy controls. Accordingly, in newly collected data, there was evidence for a significant higher proportion of samples with an expression below the limit of detection in patients than healthy controls. Altogether, patients with ME/CFS can be at a higher COVID-19 risk and, if so, they should be considered a priority group for vaccination by public health authorities. To further support this conclusion, similar research is recommended for other human cell entry receptors and cell types, namely, those cells targeted by the virus.

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