Author: Garg, Ankita; Seeliger, Benjamin; Derda, Anselm A.; Xiao, Ke; Gietz, Anika; Scherf, Kristian; Sonnenschein, Kristina; Pink, Isabell; Hoeper, Marius M.; Welte, Tobias; Bauersachs, Johann; David, Sascha; Bär, Christian; Thum, Thomas
Title: Circulating cardiovascular microRNAs in critically ill COVIDâ€19 patients Cord-id: 5e2gfg7z Document date: 2021_3_5
ID: 5e2gfg7z
Snippet: AIMS: Coronavirus disease 2019 (COVIDâ€19) is a still growing pandemic, causing many deaths and socioâ€economic damage. Elevated expression of the severe acute respiratory syndrome coronavirus 2 (SARSâ€CoVâ€2) entry receptor angiotensinâ€converting enzyme 2 on cardiac cells of patients with heart diseases may be related to cardiovascular burden. We have thus analysed cardiovascular and inflammatory microRNAs (miRs), sensitive markers of cardiovascular damage, in critically ill, ventilated p
Document: AIMS: Coronavirus disease 2019 (COVIDâ€19) is a still growing pandemic, causing many deaths and socioâ€economic damage. Elevated expression of the severe acute respiratory syndrome coronavirus 2 (SARSâ€CoVâ€2) entry receptor angiotensinâ€converting enzyme 2 on cardiac cells of patients with heart diseases may be related to cardiovascular burden. We have thus analysed cardiovascular and inflammatory microRNAs (miRs), sensitive markers of cardiovascular damage, in critically ill, ventilated patients with COVIDâ€19 or influenzaâ€associated acute respiratory distress syndrome (Influenzaâ€ARDS) admitted to the intensive care unit and healthy controls. METHODS AND RESULTS: Circulating miRs (miRâ€21, miRâ€126, miRâ€155, miRâ€208a, and miRâ€499) were analysed in a discovery cohort consisting of patients with mechanicallyâ€ventilated COVIDâ€19 (n = 18) and healthy controls (n = 15). A validation study was performed in an independent cohort of mechanicallyâ€ventilated COVIDâ€19 patients (n = 20), Influenzaâ€ARDS patients (n = 13) and healthy controls (n = 32). In both cohorts, RNA was isolated from serum and cardiovascular disease/inflammatoryâ€relevant miR concentrations were measured by miRâ€specific TaqMan PCR analyses. In both the discovery and the validation cohort, serum concentration of miRâ€21, miRâ€155, miRâ€208a and miRâ€499 were significantly increased in COVIDâ€19 patients compared to healthy controls. Calculating the area under the curve using receiver operating characteristic analysis miRâ€155, miRâ€208a and miRâ€499 showed a clear distinction between COVIDâ€19 and Influenzaâ€ARDS patients. CONCLUSION: In this exploratory study, inflammation and cardiac myocyteâ€specific miRs were upregulated in critically ill COVIDâ€19 patients. Importantly, miR profiles were able to differentiate between severely ill, mechanicallyâ€ventilated Influenzaâ€ARDS and COVIDâ€19 patients, indicating a rather specific response and cardiac involvement of COVIDâ€19.
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