Author: Isidori, AM.; Giannetta, E.; Pofi, R.; Venneri, M.A.; Gianfrilli, D; Campolo, F.; Mastroianni, CM; Lenzi, A.; d’Ettorre, G.
Title: Targeting the NOâ€cGMPâ€PDE5 pathway in COVIDâ€19 infection Cord-id: znrhobb2 Document date: 2020_6_11
ID: znrhobb2
Snippet: A pandemic outbreak of COVIDâ€19 has been sweeping the world since December. It begins as a respiratory infection that, mainly in men with diabetes or renal impairment, evolves into a systemic disease, with SARDS, progressive endothelial cell damage, abnormal clotting and impaired cardiovascular and liver function. Some clinical trials are testing biological drugs to limit the immune system dysregulation, “cytokines stormâ€, that causes the systemic complications of COVIDâ€19. The contraind
Document: A pandemic outbreak of COVIDâ€19 has been sweeping the world since December. It begins as a respiratory infection that, mainly in men with diabetes or renal impairment, evolves into a systemic disease, with SARDS, progressive endothelial cell damage, abnormal clotting and impaired cardiovascular and liver function. Some clinical trials are testing biological drugs to limit the immune system dysregulation, “cytokines stormâ€, that causes the systemic complications of COVIDâ€19. The contraindications of these drugs and their cost raise concerns over the implications of their widespread availability. Numerous clinical and experimental studies have revealed a role for the nitric oxide (NO)â€cyclic GMPâ€phosphodiesterase type 5 (PDE5) pathway in modulating lowâ€grade inflammation in patients with metabolic diseases, offering cardiovascular protection. PDE5 inhibition favors an antiâ€inflammatory response by modulating activated T cells, reducing cytokine release, lowering fibrosis, increasing oxygen diffusion, stimulating vascular repair. PDE5 is highly expressed in the lungs, where its inhibition improves pulmonary fibrosis, a complication of severe COVIDâ€19 disease. We performed a systematic review of all evidence documenting any involvement of the NOâ€cGMPâ€PDE5 axis in the pathophysiology of COVIDâ€19, presenting the ongoing clinical trials aimed at modulating this axis, including our own “silDEnafil administration in DiAbetic and dysmetaboLic patients with COVIDâ€19 (DEDALO trial)â€. The reviewed evidence suggests that PDE5 inhibitors could offer a new strategy in managing COVIDâ€19 by (i) counteracting the Angâ€IIâ€mediated downregulation of ATâ€1 receptor; (ii) acting on monocyte switching, thus reducing proâ€inflammatory cytokines, interstitial infiltration and the vessel damage responsible for alveolar hemorrhageâ€necrosis; (iii) inhibiting the transition of endothelial and smooth muscle cells to mesenchymal cells in the pulmonary artery, preventing clotting and thrombotic complications. If the ongoing trials presented herein should provide positive findings, the low cost, wide availability and temperature stability of PDE5 inhibitors could make them a major resource to combat COVIDâ€19 in developing countries.
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