Author: Carvacho, Ingrid; Piesche, Matthias
Title: RGDâ€binding integrins and TGFâ€Î² in SARSâ€CoVâ€2 infections – novel targets to treat COVIDâ€19 patients? Cord-id: lk8m50w7 Document date: 2021_3_18
ID: lk8m50w7
Snippet: The new coronavirus SARSâ€CoVâ€2 is a global pandemic and a severe public health crisis. SARSâ€CoVâ€2 is highly contagious and shows high mortality rates, especially in elderly and patients with preâ€existing medical conditions. At the current stage, no effective drugs are available to treat these patients. In this review, we analyse the rationale of targeting RGDâ€binding integrins to potentially inhibit viral cell infection and to block TGFâ€Î² activation, which is involved in the sever
Document: The new coronavirus SARSâ€CoVâ€2 is a global pandemic and a severe public health crisis. SARSâ€CoVâ€2 is highly contagious and shows high mortality rates, especially in elderly and patients with preâ€existing medical conditions. At the current stage, no effective drugs are available to treat these patients. In this review, we analyse the rationale of targeting RGDâ€binding integrins to potentially inhibit viral cell infection and to block TGFâ€Î² activation, which is involved in the severity of several human pathologies, including the complications of severe COVIDâ€19 cases. Furthermore, we demonstrate the correlation between ACE2 and TGFâ€Î² expression and the possible consequences for severe COVIDâ€19 infections. Finally, we list approved drugs or drugs in clinical trials for other diseases that also target the RGDâ€binding integrins or TGFâ€Î². These drugs have already shown a good safety profile and, therefore, can be faster brought into a trial to treat COVIDâ€19 patients.
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