Abstract

Background and objectives: Critically and non-critically ill patients with SARS-CoV-2 infection (Covid-19) may present with higher-than-expected glycemia, even in the absence of diabetes. With this study we aimed to assess glucose, glycemic gap (GlyG) and insulin secretion/sensitivity measures in patients with Covid-19. Materials and Methods: We studied, upon admission, 157 patients with Covid-19 (84: in wards and 73: in intensive care units; ICU); 135 had no history of diabetes. We measured blood glucose upon admission as well as glycated hemoglobin (A1c), plasma insulin and C-peptide. We calculated the GlyG and the Homeostasis Model Assessment 2 (HOMA2) estimates of steady state beta cell function (HOMA2%B) and insulin sensitivity (HOMA2%S). Statistical assessment was done with analysis or the Kruskal-Wallis test. Results: Compared to patients in the wards without diabetes, patients with diabetes in the wards, as well as patients in the ICU (without or with diabetes) had higher admission glycemia. The GlyG was significantly higher in patients without diabetes in the ICU compared to patients without diabetes in the wards, while HOMA2%B based on glucose and insulin was significantly higher in the ICU patients compared to patients in the wards. Of all the parameters, HOMA2%S based on C-peptide/glucose was higher in survivors (n = 133). Conclusions: In our series of patients with Covid-19, a substantial number of patients with and without diabetes had admission hyperglycemia and those who were critically ill may have had compromised insulin secretion and lowered sensitivity to insulin. These findings lend credence to reports of association between Covid-19 and hyperglycemia/secondary diabetes.

Highlights

  • Infection with coronaviridae may have repercussions in insulin secretion and glycemia [1]

  • Patients with diabetes were treated with metformin (MTF) and/or inhibitors of dipeptidyl peptidase 4 (DPP4i) and/or sodium-glucose cotransporter-2 inhibitors (SGLT2i); no treatment had been given on the day of admission

  • Hx: positive medical history, A1c: glycated hemoglobin A1c, GlyG: glycemic gap, Homeostasis Model Assessment 2 (HOMA2)%Bins: Homeostasis Model Assessment HOMA2 estimate of steady state beta cell function based on glucose and insulin measurements as a % of normal, HOMA2%Bc-pept: HOMA2 estimate of steady state beta cell function based on glucose and C-peptide measurements as a % of normal, HOMA2%Sins: HOMA2 estimate of insulin sensitivity based on glucose and insulin measurements as a % of normal, HOMA2%Sc-pept: HOMA2 estimate of insulin sensitivity based on glucose and C-peptide measurements as a % of normal; * p = 0.001 (2,3,4) vs (1), ** p = 0.031 (3) vs (1), +p = 0.016 (3&4)

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Summary

Introduction

Infection with coronaviridae may have repercussions in insulin secretion and glycemia [1]. Criticallyill and non-critically ill patients with SARS-CoV-2 infection (Covid-19). May present with higher-than-expected glycemia, even in the absence of diabetes [1,2,3,4,5,6,7]. Ill patients may show stress hyperglycemia [8]. In patients with diabetes and serious respiratory diseases, the glycemic gap (GlyG; defined by the admission blood glucose measurement minus the average glycemia as calculated from levels of glycated 4.0/). Hemoglobin [A1c]) has been associated with prognosis [9,10,11,12]. With this study we aimed to assess glucose, GlyG and insulin secretion/sensitivity measures in patients with Covid-19

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