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The role of human C5a as a non-genomic target in corticosteroid therapy for management of severe COVID19

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ELSEVIER SCI LTD
DOI: 10.1016/j.compbiolchem.2021.107482

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COVID19; Cytokine storm; C5a; Prednisone; Corticosteroids; Circular dichroism; Fluorescence; Molecular dynamics

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  1. SERB [EMR/2016/000681]

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The complement system plays a crucial role in COVID19, with studies suggesting that neutralizing C5a can help in effectively managing the disease.
Complement system plays a dual role; physiological as well as pathophysiological. While physiological role protects the host, pathophysiological role can substantially harm the host, by triggering several hyperinflammatory pathways, referred as hypercytokinaemia. Emerging clinical evidence suggests that exposure to severe acute respiratory syndrome coronavirus-2 (SARS-CoV2), tricks the complement to aberrantly activate the hypercytokinaemia loop, which significantly contributes to the severity of the COVID19. The pathophysiological response of the complement is usually amplified by the over production of potent chemoattractants and inflammatory modulators, like C3a and C5a. Therefore, it is logical that neutralizing the harmful effects of the inflammatory modulators of the complement system can be beneficial for the management of COVID19. While the hunt for safe and efficacious vaccines were underway, polypharmacology based combination therapies were fairly successful in reducing both the morbidity and mortality of COVID19 across the globe. Repurposing of small molecule drugs as neutraligands of C5a appears to be an alternative for modulating the hyper-inflammatory signals, triggered by the C5a-C5aR signaling axes. Thus, in the current study, few specific and non-specific immunomodulators (azithromycin, colchicine, famotidine, fluvoxamine, dexamethasone and prednisone) generally prescribed for prophylactic usage for management of COVID19 were subjected to computational and biophysical studies to probe whether any of the above drugs can act as neutraligands, by selectively binding to C5a over C3a. The data presented in this study indicates that corticosteroids, like prednisone can have potentially better selectively (K-d similar to 0.38 mu M) toward C5a than C3a, suggesting the positive modulatory role of C5a in the general success of the corticosteroid therapy in moderate to severe COVID19.

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