Randomised controlled trial of intravenous nafamostat mesylate in COVID pneumonitis: Phase 1b/2a experimental study to investigate safety, Pharmacokinetics and Pharmacodynamics

BACKGROUND: Many repurposed drugs have progressed rapidly to Phase 2 and 3 trials in COVID19 without characterisation of Pharmacokinetics /Pharmacodynamics including safety data. One such drug is nafamostat mesylate. METHODS: We present the findings of a phase Ib/IIa open label, platform randomised...

Descripción completa

Detalles Bibliográficos
Autores principales: Quinn, Tom M., Gaughan, Erin E., Bruce, Annya, Antonelli, Jean, O'Connor, Richard, Li, Feng, McNamara, Sarah, Koch, Oliver, MacKintosh, Claire, Dockrell, David, Walsh, Timothy, Blyth, Kevin G., Church, Colin, Schwarze, Jürgen, Boz, Cecilia, Valanciute, Asta, Burgess, Matthew, Emanuel, Philip, Mills, Bethany, Rinaldi, Giulia, Hardisty, Gareth, Mills, Ross, Findlay, Emily Gwyer, Jabbal, Sunny, Duncan, Andrew, Plant, Sinéad, Marshall, Adam D.L., Young, Irene, Russell, Kay, Scholefield, Emma, Nimmo, Alastair F., Nazarov, Islom B., Churchill, Grant C., McCullagh, James S.O., Ebrahimi, Kourosh H., Ferrett, Colin, Templeton, Kate, Rannard, Steve, Owen, Andrew, Moore, Anne, Finlayson, Keith, Shankar-Hari, Manu, Norrie, John, Parker, Richard A., Akram, Ahsan R., Anthony, Daniel C., Dear, James W., Hirani, Nik, Dhaliwal, Kevin
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2022
Materias:
Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8831100/
https://www.ncbi.nlm.nih.gov/pubmed/35152152
http://dx.doi.org/10.1016/j.ebiom.2022.103856
_version_ 1784648427404001280
author Quinn, Tom M.
Gaughan, Erin E.
Bruce, Annya
Antonelli, Jean
O'Connor, Richard
Li, Feng
McNamara, Sarah
Koch, Oliver
MacKintosh, Claire
Dockrell, David
Walsh, Timothy
Blyth, Kevin G.
Church, Colin
Schwarze, Jürgen
Boz, Cecilia
Valanciute, Asta
Burgess, Matthew
Emanuel, Philip
Mills, Bethany
Rinaldi, Giulia
Hardisty, Gareth
Mills, Ross
Findlay, Emily Gwyer
Jabbal, Sunny
Duncan, Andrew
Plant, Sinéad
Marshall, Adam D.L.
Young, Irene
Russell, Kay
Scholefield, Emma
Nimmo, Alastair F.
Nazarov, Islom B.
Churchill, Grant C.
McCullagh, James S.O.
Ebrahimi, Kourosh H.
Ferrett, Colin
Templeton, Kate
Rannard, Steve
Owen, Andrew
Moore, Anne
Finlayson, Keith
Shankar-Hari, Manu
Norrie, John
Parker, Richard A.
Akram, Ahsan R.
Anthony, Daniel C.
Dear, James W.
Hirani, Nik
Dhaliwal, Kevin
author_facet Quinn, Tom M.
Gaughan, Erin E.
Bruce, Annya
Antonelli, Jean
O'Connor, Richard
Li, Feng
McNamara, Sarah
Koch, Oliver
MacKintosh, Claire
Dockrell, David
Walsh, Timothy
Blyth, Kevin G.
Church, Colin
Schwarze, Jürgen
Boz, Cecilia
Valanciute, Asta
Burgess, Matthew
Emanuel, Philip
Mills, Bethany
Rinaldi, Giulia
Hardisty, Gareth
Mills, Ross
Findlay, Emily Gwyer
Jabbal, Sunny
Duncan, Andrew
Plant, Sinéad
Marshall, Adam D.L.
Young, Irene
Russell, Kay
Scholefield, Emma
Nimmo, Alastair F.
Nazarov, Islom B.
Churchill, Grant C.
McCullagh, James S.O.
Ebrahimi, Kourosh H.
Ferrett, Colin
Templeton, Kate
Rannard, Steve
Owen, Andrew
Moore, Anne
Finlayson, Keith
Shankar-Hari, Manu
Norrie, John
Parker, Richard A.
Akram, Ahsan R.
Anthony, Daniel C.
Dear, James W.
Hirani, Nik
Dhaliwal, Kevin
author_sort Quinn, Tom M.
collection PubMed
description BACKGROUND: Many repurposed drugs have progressed rapidly to Phase 2 and 3 trials in COVID19 without characterisation of Pharmacokinetics /Pharmacodynamics including safety data. One such drug is nafamostat mesylate. METHODS: We present the findings of a phase Ib/IIa open label, platform randomised controlled trial of intravenous nafamostat in hospitalised patients with confirmed COVID-19 pneumonitis. Patients were assigned randomly to standard of care (SoC), nafamostat or an alternative therapy. Nafamostat was administered as an intravenous infusion at a dose of 0.2 mg/kg/h for a maximum of seven days. The analysis population included those who received any dose of the trial drug and all patients randomised to SoC. The primary outcomes of our trial were the safety and tolerability of intravenous nafamostat as an add on therapy for patients hospitalised with COVID-19 pneumonitis. FINDINGS: Data is reported from 42 patients, 21 of which were randomly assigned to receive intravenous nafamostat. 86% of nafamostat-treated patients experienced at least one AE compared to 57% of the SoC group. The nafamostat group were significantly more likely to experience at least one AE (posterior mean odds ratio 5.17, 95% credible interval (CI) 1.10 – 26.05) and developed significantly higher plasma creatinine levels (posterior mean difference 10.57 micromol/L, 95% CI 2.43–18.92). An average longer hospital stay was observed in nafamostat patients, alongside a lower rate of oxygen free days (rate ratio 0.55–95% CI 0.31–0.99, respectively). There were no other statistically significant differences in endpoints between nafamostat and SoC. PK data demonstrated that intravenous nafamostat was rapidly broken down to inactive metabolites. We observed no significant anticoagulant effects in thromboelastometry. INTERPRETATION: In hospitalised patients with COVID-19, we did not observe evidence of anti-inflammatory, anticoagulant or antiviral activity with intravenous nafamostat, and there were additional adverse events. FUNDING: DEFINE was funded by LifeArc (an independent medical research charity) under the STOPCOVID award to the University of Edinburgh. We also thank the Oxford University COVID-19 Research Response Fund (BRD00230).
format Online
Article
Text
id pubmed-8831100
institution National Center for Biotechnology Information
language English
publishDate 2022
publisher Elsevier
record_format MEDLINE/PubMed
spelling pubmed-88311002022-02-11 Randomised controlled trial of intravenous nafamostat mesylate in COVID pneumonitis: Phase 1b/2a experimental study to investigate safety, Pharmacokinetics and Pharmacodynamics Quinn, Tom M. Gaughan, Erin E. Bruce, Annya Antonelli, Jean O'Connor, Richard Li, Feng McNamara, Sarah Koch, Oliver MacKintosh, Claire Dockrell, David Walsh, Timothy Blyth, Kevin G. Church, Colin Schwarze, Jürgen Boz, Cecilia Valanciute, Asta Burgess, Matthew Emanuel, Philip Mills, Bethany Rinaldi, Giulia Hardisty, Gareth Mills, Ross Findlay, Emily Gwyer Jabbal, Sunny Duncan, Andrew Plant, Sinéad Marshall, Adam D.L. Young, Irene Russell, Kay Scholefield, Emma Nimmo, Alastair F. Nazarov, Islom B. Churchill, Grant C. McCullagh, James S.O. Ebrahimi, Kourosh H. Ferrett, Colin Templeton, Kate Rannard, Steve Owen, Andrew Moore, Anne Finlayson, Keith Shankar-Hari, Manu Norrie, John Parker, Richard A. Akram, Ahsan R. Anthony, Daniel C. Dear, James W. Hirani, Nik Dhaliwal, Kevin EBioMedicine Articles BACKGROUND: Many repurposed drugs have progressed rapidly to Phase 2 and 3 trials in COVID19 without characterisation of Pharmacokinetics /Pharmacodynamics including safety data. One such drug is nafamostat mesylate. METHODS: We present the findings of a phase Ib/IIa open label, platform randomised controlled trial of intravenous nafamostat in hospitalised patients with confirmed COVID-19 pneumonitis. Patients were assigned randomly to standard of care (SoC), nafamostat or an alternative therapy. Nafamostat was administered as an intravenous infusion at a dose of 0.2 mg/kg/h for a maximum of seven days. The analysis population included those who received any dose of the trial drug and all patients randomised to SoC. The primary outcomes of our trial were the safety and tolerability of intravenous nafamostat as an add on therapy for patients hospitalised with COVID-19 pneumonitis. FINDINGS: Data is reported from 42 patients, 21 of which were randomly assigned to receive intravenous nafamostat. 86% of nafamostat-treated patients experienced at least one AE compared to 57% of the SoC group. The nafamostat group were significantly more likely to experience at least one AE (posterior mean odds ratio 5.17, 95% credible interval (CI) 1.10 – 26.05) and developed significantly higher plasma creatinine levels (posterior mean difference 10.57 micromol/L, 95% CI 2.43–18.92). An average longer hospital stay was observed in nafamostat patients, alongside a lower rate of oxygen free days (rate ratio 0.55–95% CI 0.31–0.99, respectively). There were no other statistically significant differences in endpoints between nafamostat and SoC. PK data demonstrated that intravenous nafamostat was rapidly broken down to inactive metabolites. We observed no significant anticoagulant effects in thromboelastometry. INTERPRETATION: In hospitalised patients with COVID-19, we did not observe evidence of anti-inflammatory, anticoagulant or antiviral activity with intravenous nafamostat, and there were additional adverse events. FUNDING: DEFINE was funded by LifeArc (an independent medical research charity) under the STOPCOVID award to the University of Edinburgh. We also thank the Oxford University COVID-19 Research Response Fund (BRD00230). Elsevier 2022-02-11 /pmc/articles/PMC8831100/ /pubmed/35152152 http://dx.doi.org/10.1016/j.ebiom.2022.103856 Text en © 2022 The Authors https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Articles
Quinn, Tom M.
Gaughan, Erin E.
Bruce, Annya
Antonelli, Jean
O'Connor, Richard
Li, Feng
McNamara, Sarah
Koch, Oliver
MacKintosh, Claire
Dockrell, David
Walsh, Timothy
Blyth, Kevin G.
Church, Colin
Schwarze, Jürgen
Boz, Cecilia
Valanciute, Asta
Burgess, Matthew
Emanuel, Philip
Mills, Bethany
Rinaldi, Giulia
Hardisty, Gareth
Mills, Ross
Findlay, Emily Gwyer
Jabbal, Sunny
Duncan, Andrew
Plant, Sinéad
Marshall, Adam D.L.
Young, Irene
Russell, Kay
Scholefield, Emma
Nimmo, Alastair F.
Nazarov, Islom B.
Churchill, Grant C.
McCullagh, James S.O.
Ebrahimi, Kourosh H.
Ferrett, Colin
Templeton, Kate
Rannard, Steve
Owen, Andrew
Moore, Anne
Finlayson, Keith
Shankar-Hari, Manu
Norrie, John
Parker, Richard A.
Akram, Ahsan R.
Anthony, Daniel C.
Dear, James W.
Hirani, Nik
Dhaliwal, Kevin
Randomised controlled trial of intravenous nafamostat mesylate in COVID pneumonitis: Phase 1b/2a experimental study to investigate safety, Pharmacokinetics and Pharmacodynamics
title Randomised controlled trial of intravenous nafamostat mesylate in COVID pneumonitis: Phase 1b/2a experimental study to investigate safety, Pharmacokinetics and Pharmacodynamics
title_full Randomised controlled trial of intravenous nafamostat mesylate in COVID pneumonitis: Phase 1b/2a experimental study to investigate safety, Pharmacokinetics and Pharmacodynamics
title_fullStr Randomised controlled trial of intravenous nafamostat mesylate in COVID pneumonitis: Phase 1b/2a experimental study to investigate safety, Pharmacokinetics and Pharmacodynamics
title_full_unstemmed Randomised controlled trial of intravenous nafamostat mesylate in COVID pneumonitis: Phase 1b/2a experimental study to investigate safety, Pharmacokinetics and Pharmacodynamics
title_short Randomised controlled trial of intravenous nafamostat mesylate in COVID pneumonitis: Phase 1b/2a experimental study to investigate safety, Pharmacokinetics and Pharmacodynamics
title_sort randomised controlled trial of intravenous nafamostat mesylate in covid pneumonitis: phase 1b/2a experimental study to investigate safety, pharmacokinetics and pharmacodynamics
topic Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8831100/
https://www.ncbi.nlm.nih.gov/pubmed/35152152
http://dx.doi.org/10.1016/j.ebiom.2022.103856
work_keys_str_mv AT quinntomm randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT gaughanerine randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT bruceannya randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT antonellijean randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT oconnorrichard randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT lifeng randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT mcnamarasarah randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT kocholiver randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT mackintoshclaire randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT dockrelldavid randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT walshtimothy randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT blythkeving randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT churchcolin randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT schwarzejurgen randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT bozcecilia randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT valanciuteasta randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT burgessmatthew randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT emanuelphilip randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT millsbethany randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT rinaldigiulia randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT hardistygareth randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT millsross randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT findlayemilygwyer randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT jabbalsunny randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT duncanandrew randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT plantsinead randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT marshalladamdl randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT youngirene randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT russellkay randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT scholefieldemma randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT nimmoalastairf randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT nazarovislomb randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT churchillgrantc randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT mccullaghjamesso randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT ebrahimikouroshh randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT ferrettcolin randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT templetonkate randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT rannardsteve randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT owenandrew randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT mooreanne randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT finlaysonkeith randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT shankarharimanu randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT norriejohn randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT parkerricharda randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT akramahsanr randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT anthonydanielc randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT dearjamesw randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT hiraninik randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics
AT dhaliwalkevin randomisedcontrolledtrialofintravenousnafamostatmesylateincovidpneumonitisphase1b2aexperimentalstudytoinvestigatesafetypharmacokineticsandpharmacodynamics

Ejemplares similares