1959. Ceftriaxone-Sulbactam-EDTA (CSE) vs. Meropenem (MR) in PLEA (a Phase 3, Randomized, Double-Blind Trial): Outcomes in Patients Infected With Ceftriaxone Non-Susceptible, Extended-Spectrum β-Lactamase and Multi-Drug-resistant Pathogens at Baseline

BACKGROUND: CSE, a novel combination of Ceftriaxone, Sulbactam and Disodium EDTA (Class 1 Antibiotic Resistance Breaker), is being developed for the treatment of patients with serious Gram-negative infections and has completed a Phase-3 clinical trial (NCT03477422) for treatment of complicated urina...

Descripción completa

Detalles Bibliográficos
Autores principales: Mir, Mohd Amin, Chaudhary, Saransh, Mammen, Kim Jacob, Sood, Rajeev, Dogra, P N, Chadha, Sudhir, Mavuduru, Ravimohan, Sinha, Rahul Janak, Chaudhary, Manu, Shiekh, Gazalla
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2018
Materias:
Abstracts
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6252982/
http://dx.doi.org/10.1093/ofid/ofy210.1615
_version_ 1783373391074426880
author Mir, Mohd Amin
Chaudhary, Saransh
Mammen, Kim Jacob
Sood, Rajeev
Dogra, P N
Chadha, Sudhir
Mavuduru, Ravimohan
Sinha, Rahul Janak
Chaudhary, Manu
Shiekh, Gazalla
author_facet Mir, Mohd Amin
Chaudhary, Saransh
Mammen, Kim Jacob
Sood, Rajeev
Dogra, P N
Chadha, Sudhir
Mavuduru, Ravimohan
Sinha, Rahul Janak
Chaudhary, Manu
Shiekh, Gazalla
author_sort Mir, Mohd Amin
collection PubMed
description BACKGROUND: CSE, a novel combination of Ceftriaxone, Sulbactam and Disodium EDTA (Class 1 Antibiotic Resistance Breaker), is being developed for the treatment of patients with serious Gram-negative infections and has completed a Phase-3 clinical trial (NCT03477422) for treatment of complicated urinary tract infections (cUTI), including acute pyelonephritis (AP). It restores and enhances the in vitro activity of Ceftriaxone against various β-lactamases (BLs), including enzyme families that belong to Ambler class A (TEM, SHV, CTX-M), class B (NDM, VIM, IMP), class C (some variants of AmpC), and class D {OXA extended spectrum BLs (ESBLs)}. This analysis was performed to assess the clinical and microbiological outcomes in patients infected with Ceftriaxone non-susceptible (C-NS), MDR and ESBL-producing Gram-negative pathogens at baseline. METHODS: Patients were randomized 1:1 to receive either CSE (1g Ceftriaxone/500 mg Sulbactam/37 mg EDTA) every 12 hours or Meropenem (MR) 1 g every 8 hours as 30 minutes IV infusion for 5–14 days. Oral step-down therapy was not allowed. Biological specimens were analyzed, and resistant pathogens identified. MDR was defined as resistance to at least three categories of antimicrobials. Identification of pathogens and antibiotic susceptibility testing were performed and interpreted according to Clinical and Laboratory Standards Institute methodologies. Combined Disc Diffusion Test was used to detect ESBL-production in pathogens. RESULTS: Of 230 randomized patients, 143 (62.2%) were included in m-MITT [72/74 (97.3) in CSE and 68/69 (98.6%) in MR groups had C-NS pathogens; 63/74 (85.1%) in CSE and 56/69 (81.2%) in MR groups had ESBL-producing pathogens; 55/74 (74.3%) in CSE and 45/69 (65.2%) in MR group had MDR pathogens]. Mean duration of IV therapy was 7 days. The clinical cure and microbiological eradication rates for CSE and MR at the test of cure (TOC) visit in C-NS, ESBL and MDR pathogens is shown in Figures 1, 2, and 3, respectively. [Image: see text] [Image: see text] [Image: see text] CONCLUSION: At TOC, clinical cure and microbiological eradication rates were higher for CSE as compared with MR across all three analyses sets. Overall, CSE was effective in the treatment of patients with cUTI and AP caused by resistant Gram-negative pathogens. DISCLOSURES: M. A. Mir, Venus Medicine Research Centre: Employee, Salary. S. Chaudhary, Venus Medicine Research Centre: Employee and Shareholder, Salary. M. Chaudhary, Venus Medicine Research Centre: Board Member and Shareholder, Salary. G. Shiekh, Venus Medicine Research Centre: Employee, Salary.
format Online
Article
Text
id pubmed-6252982
institution National Center for Biotechnology Information
language English
publishDate 2018
publisher Oxford University Press
record_format MEDLINE/PubMed
spelling pubmed-62529822018-11-28 1959. Ceftriaxone-Sulbactam-EDTA (CSE) vs. Meropenem (MR) in PLEA (a Phase 3, Randomized, Double-Blind Trial): Outcomes in Patients Infected With Ceftriaxone Non-Susceptible, Extended-Spectrum β-Lactamase and Multi-Drug-resistant Pathogens at Baseline Mir, Mohd Amin Chaudhary, Saransh Mammen, Kim Jacob Sood, Rajeev Dogra, P N Chadha, Sudhir Mavuduru, Ravimohan Sinha, Rahul Janak Chaudhary, Manu Shiekh, Gazalla Open Forum Infect Dis Abstracts BACKGROUND: CSE, a novel combination of Ceftriaxone, Sulbactam and Disodium EDTA (Class 1 Antibiotic Resistance Breaker), is being developed for the treatment of patients with serious Gram-negative infections and has completed a Phase-3 clinical trial (NCT03477422) for treatment of complicated urinary tract infections (cUTI), including acute pyelonephritis (AP). It restores and enhances the in vitro activity of Ceftriaxone against various β-lactamases (BLs), including enzyme families that belong to Ambler class A (TEM, SHV, CTX-M), class B (NDM, VIM, IMP), class C (some variants of AmpC), and class D {OXA extended spectrum BLs (ESBLs)}. This analysis was performed to assess the clinical and microbiological outcomes in patients infected with Ceftriaxone non-susceptible (C-NS), MDR and ESBL-producing Gram-negative pathogens at baseline. METHODS: Patients were randomized 1:1 to receive either CSE (1g Ceftriaxone/500 mg Sulbactam/37 mg EDTA) every 12 hours or Meropenem (MR) 1 g every 8 hours as 30 minutes IV infusion for 5–14 days. Oral step-down therapy was not allowed. Biological specimens were analyzed, and resistant pathogens identified. MDR was defined as resistance to at least three categories of antimicrobials. Identification of pathogens and antibiotic susceptibility testing were performed and interpreted according to Clinical and Laboratory Standards Institute methodologies. Combined Disc Diffusion Test was used to detect ESBL-production in pathogens. RESULTS: Of 230 randomized patients, 143 (62.2%) were included in m-MITT [72/74 (97.3) in CSE and 68/69 (98.6%) in MR groups had C-NS pathogens; 63/74 (85.1%) in CSE and 56/69 (81.2%) in MR groups had ESBL-producing pathogens; 55/74 (74.3%) in CSE and 45/69 (65.2%) in MR group had MDR pathogens]. Mean duration of IV therapy was 7 days. The clinical cure and microbiological eradication rates for CSE and MR at the test of cure (TOC) visit in C-NS, ESBL and MDR pathogens is shown in Figures 1, 2, and 3, respectively. [Image: see text] [Image: see text] [Image: see text] CONCLUSION: At TOC, clinical cure and microbiological eradication rates were higher for CSE as compared with MR across all three analyses sets. Overall, CSE was effective in the treatment of patients with cUTI and AP caused by resistant Gram-negative pathogens. DISCLOSURES: M. A. Mir, Venus Medicine Research Centre: Employee, Salary. S. Chaudhary, Venus Medicine Research Centre: Employee and Shareholder, Salary. M. Chaudhary, Venus Medicine Research Centre: Board Member and Shareholder, Salary. G. Shiekh, Venus Medicine Research Centre: Employee, Salary. Oxford University Press 2018-11-26 /pmc/articles/PMC6252982/ http://dx.doi.org/10.1093/ofid/ofy210.1615 Text en © The Author(s) 2018. Published by Oxford University Press on behalf of Infectious Diseases Society of America. http://creativecommons.org/licenses/by-nc-nd/4.0/ This is an Open Access article distributed under the terms of the Creative Commons Attribution-NonCommercial-NoDerivs licence (http://creativecommons.org/licenses/by-nc-nd/4.0/), which permits non-commercial reproduction and distribution of the work, in any medium, provided the original work is not altered or transformed in any way, and that the work is properly cited. For commercial re-use, please contact journals.permissions@oup.com
spellingShingle Abstracts
Mir, Mohd Amin
Chaudhary, Saransh
Mammen, Kim Jacob
Sood, Rajeev
Dogra, P N
Chadha, Sudhir
Mavuduru, Ravimohan
Sinha, Rahul Janak
Chaudhary, Manu
Shiekh, Gazalla
1959. Ceftriaxone-Sulbactam-EDTA (CSE) vs. Meropenem (MR) in PLEA (a Phase 3, Randomized, Double-Blind Trial): Outcomes in Patients Infected With Ceftriaxone Non-Susceptible, Extended-Spectrum β-Lactamase and Multi-Drug-resistant Pathogens at Baseline
title 1959. Ceftriaxone-Sulbactam-EDTA (CSE) vs. Meropenem (MR) in PLEA (a Phase 3, Randomized, Double-Blind Trial): Outcomes in Patients Infected With Ceftriaxone Non-Susceptible, Extended-Spectrum β-Lactamase and Multi-Drug-resistant Pathogens at Baseline
title_full 1959. Ceftriaxone-Sulbactam-EDTA (CSE) vs. Meropenem (MR) in PLEA (a Phase 3, Randomized, Double-Blind Trial): Outcomes in Patients Infected With Ceftriaxone Non-Susceptible, Extended-Spectrum β-Lactamase and Multi-Drug-resistant Pathogens at Baseline
title_fullStr 1959. Ceftriaxone-Sulbactam-EDTA (CSE) vs. Meropenem (MR) in PLEA (a Phase 3, Randomized, Double-Blind Trial): Outcomes in Patients Infected With Ceftriaxone Non-Susceptible, Extended-Spectrum β-Lactamase and Multi-Drug-resistant Pathogens at Baseline
title_full_unstemmed 1959. Ceftriaxone-Sulbactam-EDTA (CSE) vs. Meropenem (MR) in PLEA (a Phase 3, Randomized, Double-Blind Trial): Outcomes in Patients Infected With Ceftriaxone Non-Susceptible, Extended-Spectrum β-Lactamase and Multi-Drug-resistant Pathogens at Baseline
title_short 1959. Ceftriaxone-Sulbactam-EDTA (CSE) vs. Meropenem (MR) in PLEA (a Phase 3, Randomized, Double-Blind Trial): Outcomes in Patients Infected With Ceftriaxone Non-Susceptible, Extended-Spectrum β-Lactamase and Multi-Drug-resistant Pathogens at Baseline
title_sort 1959. ceftriaxone-sulbactam-edta (cse) vs. meropenem (mr) in plea (a phase 3, randomized, double-blind trial): outcomes in patients infected with ceftriaxone non-susceptible, extended-spectrum β-lactamase and multi-drug-resistant pathogens at baseline
topic Abstracts
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6252982/
http://dx.doi.org/10.1093/ofid/ofy210.1615
work_keys_str_mv AT mirmohdamin 1959ceftriaxonesulbactamedtacsevsmeropenemmrinpleaaphase3randomizeddoubleblindtrialoutcomesinpatientsinfectedwithceftriaxonenonsusceptibleextendedspectrumblactamaseandmultidrugresistantpathogensatbaseline
AT chaudharysaransh 1959ceftriaxonesulbactamedtacsevsmeropenemmrinpleaaphase3randomizeddoubleblindtrialoutcomesinpatientsinfectedwithceftriaxonenonsusceptibleextendedspectrumblactamaseandmultidrugresistantpathogensatbaseline
AT mammenkimjacob 1959ceftriaxonesulbactamedtacsevsmeropenemmrinpleaaphase3randomizeddoubleblindtrialoutcomesinpatientsinfectedwithceftriaxonenonsusceptibleextendedspectrumblactamaseandmultidrugresistantpathogensatbaseline
AT soodrajeev 1959ceftriaxonesulbactamedtacsevsmeropenemmrinpleaaphase3randomizeddoubleblindtrialoutcomesinpatientsinfectedwithceftriaxonenonsusceptibleextendedspectrumblactamaseandmultidrugresistantpathogensatbaseline
AT dograpn 1959ceftriaxonesulbactamedtacsevsmeropenemmrinpleaaphase3randomizeddoubleblindtrialoutcomesinpatientsinfectedwithceftriaxonenonsusceptibleextendedspectrumblactamaseandmultidrugresistantpathogensatbaseline
AT chadhasudhir 1959ceftriaxonesulbactamedtacsevsmeropenemmrinpleaaphase3randomizeddoubleblindtrialoutcomesinpatientsinfectedwithceftriaxonenonsusceptibleextendedspectrumblactamaseandmultidrugresistantpathogensatbaseline
AT mavudururavimohan 1959ceftriaxonesulbactamedtacsevsmeropenemmrinpleaaphase3randomizeddoubleblindtrialoutcomesinpatientsinfectedwithceftriaxonenonsusceptibleextendedspectrumblactamaseandmultidrugresistantpathogensatbaseline
AT sinharahuljanak 1959ceftriaxonesulbactamedtacsevsmeropenemmrinpleaaphase3randomizeddoubleblindtrialoutcomesinpatientsinfectedwithceftriaxonenonsusceptibleextendedspectrumblactamaseandmultidrugresistantpathogensatbaseline
AT chaudharymanu 1959ceftriaxonesulbactamedtacsevsmeropenemmrinpleaaphase3randomizeddoubleblindtrialoutcomesinpatientsinfectedwithceftriaxonenonsusceptibleextendedspectrumblactamaseandmultidrugresistantpathogensatbaseline
AT shiekhgazalla 1959ceftriaxonesulbactamedtacsevsmeropenemmrinpleaaphase3randomizeddoubleblindtrialoutcomesinpatientsinfectedwithceftriaxonenonsusceptibleextendedspectrumblactamaseandmultidrugresistantpathogensatbaseline
AT 1959ceftriaxonesulbactamedtacsevsmeropenemmrinpleaaphase3randomizeddoubleblindtrialoutcomesinpatientsinfectedwithceftriaxonenonsusceptibleextendedspectrumblactamaseandmultidrugresistantpathogensatbaseline

Ejemplares similares