Use my Search Websuite to scan PubMed, PMCentral, Journal Hosts and Journal Archives, FullText. Kick-your-searchterm to multiple Engines kick-your-query now !>

A dictionary by aggregated review articles of nephrology, medicine and the life sciences Your one-stop-run pathway from word to the immediate pdf of peer-reviewed on-topic knowledge.

10.1016/j.clim.2020.108598 http://scihub22266oqcxt.onion/10.1016/j.clim.2020.108598 32961333!7501834!32961333     free     free     free Warning: file_get_contents(https://eutils.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&id=32961333&cmd=llinks): Failed to open stream: HTTP request failed! HTTP/1.1 429 Too Many Requests in C:\Inetpub\vhosts\kidney.de\httpdocs\pget.php on line 215       Clin+Immunol 2020 ; 220 (?): 108598 Nephropedia Template TP {{tp|p=32961333|t=2020. Complement C3 vs C5 inhibition in severe COVID-19: Early clinical findings reveal differential biological efficacy |pdf=|usr=}}{{32961333}} gab.com Text Complement C3 vs C5 inhibition in severe COVID-19: Early clinical findings reveal differential biological efficacy JO: Clin Immunol http://www.kidney.de/pget.php?&tw=1&pmid=32961333 #FOAvip Growing clinical evidence has implicated complement as a pivotal driver of COVID-19 immunopathology. Deregulated complement activation may fuel cytokine-driven hyper-inflammation, thrombotic microangiopathy and NET-driven immunothrombosis, thereby leading to multi-organ failure. Complement therapeutics have gained traction as candidate drugs for countering the detrimental consequences of SARS-CoV-2 infection. Whether blockade of terminal complement effectors (C5, C5a, or C5aR1) may elicit similar outcomes to upstream intervention at the level of C3 remains debated. Here we compare the efficacy of the C5-targeting monoclonal antibody eculizumab with that of the compstatin-based C3-targeted drug candidate AMY-101 in small independent cohorts of severe COVID-19 patients. Our exploratory study indicates that therapeutic complement inhibition abrogates COVID-19 hyper-inflammation. Both C3 and C5 inhibitors elicit a robust anti-inflammatory response, reflected by a steep decline in C-reactive protein and IL-6 levels, marked lung function improvement, and resolution of SARS-CoV-2-associated acute respiratory distress syndrome (ARDS). C3 inhibition afforded broader therapeutic control in COVID-19 patients by attenuating both C3a and sC5b-9 generation and preventing FB consumption. This broader inhibitory profile was associated with a more robust decline of neutrophil counts, attenuated neutrophil extracellular trap (NET) release, faster serum LDH decline, and more prominent lymphocyte recovery. These early clinical results offer important insights into the differential mechanistic basis and underlying biology of C3 and C5 inhibition in COVID-19 and point to a broader pathogenic involvement of C3-mediated pathways in thromboinflammation. They also support the evaluation of these complement-targeting agents as COVID-19 therapeutics in large prospective trials. Twit Text FOAVip Complement C3 vs C5 inhibition in severe COVID-19: Early clinical findings reveal differential biological efficacy ????Clin Immunol http://www.kidney.de/pget.php?&tw=1&pmid=32961333 #FOAvip Twit Text # Free Paper on # # # # # LINK http://www.kidney.de/pget.php?&tw=1&pmid=32961333 #FOAvip English Wikipedia <ref>{{Cite pmid|32961333}}</ref> Complement C3 vs C5 inhibition in severe COVID-19: Early clinical findings reveal differential biological efficacy #MMPMID32961333 Mastellos DC; Pires da Silva BGP; Fonseca BAL; Fonseca NP; Auxiliadora-Martins M; Mastaglio S; Ruggeri A; Sironi M; Radermacher P; Chrysanthopoulou A; Skendros P; Ritis K; Manfra I; Iacobelli S; Huber-Lang M; Nilsson B; Yancopoulou D; Connolly ES; Garlanda C; Ciceri F; Risitano AM; Calado RT; Lambris JD Clin Immunol 2020[Nov]; 220 (?): 108598 PMID32961333show ga Growing clinical evidence has implicated complement as a pivotal driver of COVID-19 immunopathology. Deregulated complement activation may fuel cytokine-driven hyper-inflammation, thrombotic microangiopathy and NET-driven immunothrombosis, thereby leading to multi-organ failure. Complement therapeutics have gained traction as candidate drugs for countering the detrimental consequences of SARS-CoV-2 infection. Whether blockade of terminal complement effectors (C5, C5a, or C5aR1) may elicit similar outcomes to upstream intervention at the level of C3 remains debated. Here we compare the efficacy of the C5-targeting monoclonal antibody eculizumab with that of the compstatin-based C3-targeted drug candidate AMY-101 in small independent cohorts of severe COVID-19 patients. Our exploratory study indicates that therapeutic complement inhibition abrogates COVID-19 hyper-inflammation. Both C3 and C5 inhibitors elicit a robust anti-inflammatory response, reflected by a steep decline in C-reactive protein and IL-6 levels, marked lung function improvement, and resolution of SARS-CoV-2-associated acute respiratory distress syndrome (ARDS). C3 inhibition afforded broader therapeutic control in COVID-19 patients by attenuating both C3a and sC5b-9 generation and preventing FB consumption. This broader inhibitory profile was associated with a more robust decline of neutrophil counts, attenuated neutrophil extracellular trap (NET) release, faster serum LDH decline, and more prominent lymphocyte recovery. These early clinical results offer important insights into the differential mechanistic basis and underlying biology of C3 and C5 inhibition in COVID-19 and point to a broader pathogenic involvement of C3-mediated pathways in thromboinflammation. They also support the evaluation of these complement-targeting agents as COVID-19 therapeutics in large prospective trials. |Antibodies, Monoclonal, Humanized/therapeutic use[MESH] |Betacoronavirus/*pathogenicity[MESH] |Biomarkers/blood[MESH] |C-Reactive Protein/metabolism[MESH] |COVID-19[MESH] |Cohort Studies[MESH] |Complement Activation/drug effects[MESH] |Complement C3/*antagonists & inhibitors/genetics/immunology[MESH] |Complement C5/*antagonists & inhibitors/genetics/immunology[MESH] |Complement Inactivating Agents/*therapeutic use[MESH] |Coronavirus Infections/complications/*drug therapy/immunology/virology[MESH] |Extracellular Traps/drug effects[MESH] |Female[MESH] |Gene Expression[MESH] |Humans[MESH] |Immunologic Factors/*therapeutic use[MESH] |Interleukin-6/metabolism[MESH] |Male[MESH] |Middle Aged[MESH] |Neutrophils/drug effects/immunology/virology[MESH] |Pandemics[MESH] |Peptides, Cyclic/therapeutic use[MESH] |Pneumonia, Viral/complications/*drug therapy/immunology/virology[MESH] |Respiratory Distress Syndrome/complications/*drug therapy/immunology/virology[MESH] |SARS-CoV-2[MESH]Complement C3 vs C5 inhibition in severe COVID-19: Early clinical find(epmc).pdf DeepDyve Pubget Overpricing