4.7 Article

COVID-19 induces new-onset insulin resistance and lipid metabolic dysregulation via regulation of secreted metabolic factors

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SPRINGERNATURE
DOI: 10.1038/s41392-021-00822-x

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  1. joint emergency grants for prevention and control of SARS-CoV-2 of Ministry of Science and Technology of China
  2. Guangdong Science and Technology Department and Guangzhou Municipal Science and Technology Bureau [2020B111108001]
  3. Guangdong Science and Technology Department [2020B1212060018, 2020B1212030004]

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Insulin resistance, hyperglycemia, and decreased HDL-C were found in COVID-19 patients without pre-existing metabolic diseases, with increased expression of REST by SARS-CoV-2 infection being the mechanistic link. Specific lipids were identified as potential biomarkers of COVID-19-induced metabolic dysregulation, especially in insulin resistance.
Abnormal glucose and lipid metabolism in COVID-19 patients were recently reported with unclear mechanism. In this study, we retrospectively investigated a cohort of COVID-19 patients without pre-existing metabolic-related diseases, and found new-onset insulin resistance, hyperglycemia, and decreased HDL-C in these patients. Mechanistically, SARS-CoV-2 infection increased the expression of RE1-silencing transcription factor (REST), which modulated the expression of secreted metabolic factors including myeloperoxidase, apelin, and myostatin at the transcriptional level, resulting in the perturbation of glucose and lipid metabolism. Furthermore, several lipids, including (+/-)5-HETE, (+/-)12-HETE, propionic acid, and isobutyric acid were identified as the potential biomarkers of COVID-19-induced metabolic dysregulation, especially in insulin resistance. Taken together, our study revealed insulin resistance as the direct cause of hyperglycemia upon COVID-19, and further illustrated the underlying mechanisms, providing potential therapeutic targets for COVID-19-induced metabolic complications.

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