Ceftazidime-Avibactam for the Treatment of Infections Due to Ceftazidime Resistant Pathogens

Phase 3

Completed

• Conditions: Complicated Urinary Tract Infection; Complicated Intra-abdominal Infection
• Interventions: Drug: Ceftazidime - Avibactam ( CAZ-AVI); Drug: Best Available Therapy; Drug: Metronidazole

• Registration Number: NCT01644643
• Lead Sponsor: Pfizer

Brief Summary

To Evaluate the Effects of Ceftazidime-Avibactam and Best Available Therapy in patients with complicated urinary tract infections and complicated intra-abdominal infections.

Detailed Description

An Open-Label, Randomized, Multicenter, Phase III Study of Ceftazidime Avibactam (CAZ-AVI, formerly CAZ104) and Best Available Therapy for the Treatment of Infections Due to Ceftazidime Resistant Gram Negative Pathogens

Study Timeline

• Study First Submitted: 2012-06-28
• Study First Submitted QC: 2012-07-18
• Study First Posted: 2012-07-19
• Study Start: 2013-01
• Primary Completion: 2014-09
• Study Completion: 2014-09
• Results First Submitted: 2015-09-28
• Results First Submitted QC: 2015-11-10
• Results First Posted: 2015-12-14
• Status Verified: 2017-08
• Last Update Submitted: 2017-08-31
• Last Update Posted: 2017-09-29

Recruitment & Eligibility

• Status: COMPLETED
• Sex: All
• Target Recruitment: 345

Inclusion Criteria

• Patient must be ≥18 and ≤90 years of age
• Female patients can participate if they are surgically sterile or completed menopause or females capable of having children and agree not to attempt pregnancy while receiving IV study therapy and for a period of 7 days after
• Patient has a ceftazidime-resistant Gram negative pathogen that was isolated from an appropriate culture within 5 days prior to study entry (ie, within 5 days prior to Screening; the study-qualifying culture), which was determined to be the causative agent of the entry infection

Exclusion Criteria

• Patient has an APACHE II score >30 (cIAI patients only)
• Patient has an infection due to Gram negative pathogen that is unlikely to respond to CAZ-AVI treatment (eg, Acinetobacter spp., Stenotrophomonas spp.)
• Patient is receiving hemodialysis or peritoneal dialysis or had a renal transplant Patient is immunocompromised
• Patient has a rapidly progressive or terminal illness with a high risk of mortality due to any cause, including acute hepatic failure, respiratory failure or severe septic shock such that they are unlikely to survive the 4- to 5-week study period.

Study & Design

• Study Type: INTERVENTIONAL
• Study Design: PARALLEL

Arm && Interventions

Group	Intervention	Description
Ceftazidime - Avibactam ( CAZ-AVI)	Ceftazidime - Avibactam ( CAZ-AVI)	IV treatment
Best Available Therapy	Best Available Therapy	IV treatment
Ceftazidime - Avibactam ( CAZ-AVI)	Metronidazole	IV treatment

Primary Outcome Measures

Name	Time	Method
Clinical Response at Test of Cure (TOC) in Microbiological Modified Intent-to-treat (mMITT) Analysis Set	6-12 days after last infusion of study therapy. Duration of study therapy was 5 to 21 days.	Proportion of patients with clinical cure at the TOC visit in the mMITT analysis set. Clinical cure: Complete resolution or significant improvement of signs and symptoms of the index infection such that no further antibacterial therapy (other than those allowed per protocol) is necessary; for cIAI patients no drainage or surgical intervention after 96 hours from randomization is necessary (ie. drainage or surgical intervention up to 96 hours from randomization is permissible).

Secondary Outcome Measures

Name	Time	Method
Clinical Response at End of Treatment (EOT) in mMITT Analysis Set.	28 hours after completion of last infusion of study therapy. Duration of study therapy was 5 to 21 days.	Proportion of patients with clinical cure at the EOT visit in the mMITT analysis set. Clinical cure: Complete resolution or significant improvement of signs and symptoms of the index infection such that no further antibacterial therapy (other than those allowed per protocol) is necessary; for cIAI patients no drainage or surgical intervention after 96 hours from randomization is necessary (ie. drainage or surgical intervention up to 96 hours from randomization is permissible).
Clinical Response at Follow-up 1 (FU1) in mMITT Analysis Set	cIAI: 27-37 calendar days from randomization/cUTI: 20-27 calendar days from randomization	Proportion of patients with clinical cure at the FU1 visit in the mMITT analysis set. Clinical cure: Complete resolution or significant improvement of signs and symptoms of the index infection such that no further antibacterial therapy (other than those allowed per protocol) is necessary; for cIAI patients no drainage or surgical intervention after 96 hours from randomization is necessary (ie. drainage or surgical intervention up to 96 hours from randomization is permissible).
Clinical Response at Follow-up 2 (FU2) in mMITT Analysis Set	At FU2, data was only collected for the cUTI Arms: 28-34 calendar days from randomization	Proportion of patients with clinical cure at the FU2 visit in the mMITT analysis set. Clinical cure: Complete resolution or significant improvement of signs and symptoms of the index infection such that no further antibacterial therapy (other than those allowed per protocol) is necessary; for cIAI patients no drainage or surgical intervention after 96 hours from randomization is necessary (ie. drainage or surgical intervention up to 96 hours from randomization is permissible).
Clinical Response at EOT in Extended Microbiologically Evaluable (EME) at EOT Analysis Set.	28 hours after completion of last infusion of study therapy. Duration of study therapy was 5 to 21 days.	Proportion of patients with clinical cure at the EOT visit in the EME at EOT analysis set. Clinical cure: Complete resolution or significant improvement of signs and symptoms of the index infection such that no further antibacterial therapy (other than those allowed per protocol) is necessary; for cIAI patients no drainage or surgical intervention after 96 hours from randomization is necessary (ie. drainage or surgical intervention up to 96 hours from randomization is permissible).
Clinical Response at TOC in EME at TOC Analysis Set.	6-12 days after last infusion of study therapy.Duration of study therapy was 5 to 21 days.	Proportion of patients with clinical cure at the TOC visit in the EME at TOC analysis set. Clinical cure: Complete resolution or significant improvement of signs and symptoms of the index infection such that no further antibacterial therapy (other than those allowed per protocol) is necessary; for cIAI patients no drainage or surgical intervention after 96 hours from randomization is necessary (ie. drainage or surgical intervention up to 96 hours from randomization is permissible).
Clinical Response at FU1 in EME at FU1 Analysis Set.	cIAI: 27-37 calendar days from randomization/cUTI: 20-27 calendar days from randomization	Proportion of patients with clinical cure at the FU1 visit in EME at FU1 analysis set. Clinical cure: Complete resolution or significant improvement of signs and symptoms of the index infection such that no further antibacterial therapy (other than those allowed per protocol) is necessary; for cIAI patients no drainage or surgical intervention after 96 hours from randomization is necessary (ie. drainage or surgical intervention up to 96 hours from randomization is permissible).
Clinical Cure at TOC by Previously Failed Treatment Class in mMITT Analysis Set	6-12 days after last infusion of study therapy. Duration of study therapy was 5 to 21 days.	Proportion of patients with clinical cure at TOC visit by previously failed treatment class in the mMITT analysis set. Clinical cure: Complete resolution or significant improvement of signs and symptoms of the index infection such that no further antibacterial therapy (other than those allowed per protocol) is necessary; for cIAI patients no drainage or surgical intervention after 96 hours from randomization is necessary (ie. drainage or surgical intervention up to 96 hours from randomization is permissible).
Clinical Response at FU2 in EME at FU2 Analysis Set	At FU2, data was only collected for the cUTI Arms: 28-34 calendar days from randomization	Proportion of patients with clinical cure at the FU2 visit in EME at FU2 analysis set. Clinical cure: Complete resolution or significant improvement of signs and symptoms of the index infection such that no further antibacterial therapy (other than those allowed per protocol) is necessary.
Per-patient Microbiological Response at EOT in mMITT Analysis Set	28 hours after completion of last infusion of study therapy. Duration of study therapy was 5 to 21 days.	Microbiological responses as per the protocoled criteria: responses other than "indeterminate" were classified as "favorable" or "unfavorable." Favorable microbiological response assessments included "eradication" and "presumed eradication." Unfavorable microbiological response assessments included "persistence," "persistence with increasing minimum inhibitory concentration (MIC)," and "presumed persistence." Indeterminate microbiologic response assessments included cIAI patients where the clinical response was changed to indeterminate due to a Surgical Review Panel assessment of inadequate source control (ie, circumstances that preclude classification as eradication, presumed eradication, persistence, persistence with increasing MIC, and presumed persistence).
Per-patient Microbiological Response at TOC in mMITT Analysis Set	6-12 days after last infusion of study therapy. Duration of study therapy was 5 to 21 days.	Microbiological responses as per the protocoled criteria: responses other than "indeterminate" were classified as "favorable" or "unfavorable." Favorable microbiological response assessments included "eradication" and "presumed eradication." Unfavorable microbiological response assessments included "persistence," "persistence with increasing minimum inhibitory concentration (MIC)," and "presumed persistence." Indeterminate microbiologic response assessments included cIAI patients where the clinical response was changed to indeterminate due to a Surgical Review Panel assessment of inadequate source control (ie, circumstances that preclude classification as eradication, presumed eradication, persistence, persistence with increasing MIC, and presumed persistence).
Per-patient Microbiological Response at FU1 in mMITT Analysis Set	cUTI: 20-27 calendar days from randomization/cIAI: 27-37 calendar days from randomization	Microbiological responses as per the protocoled criteria: responses other than "indeterminate" were classified as "favorable" or "unfavorable." Favorable microbiological response assessments included "eradication" and "presumed eradication." Unfavorable microbiological response assessments included "persistence," "persistence with increasing minimum inhibitory concentration (MIC)," and "presumed persistence." Indeterminate microbiologic response assessments included cIAI patients where the clinical response was changed to indeterminate due to a Surgical Review Panel assessment of inadequate source control (ie, circumstances that preclude classification as eradication, presumed eradication, persistence, persistence with increasing MIC, and presumed persistence).
Per-patient Microbiological Response at FU2 in mMITT Analysis Set	At FU2, data was only collected for the cUTI Arms: 28-34 calendar days from randomization	Microbiological responses as per the protocoled criteria: responses other than "indeterminate" were classified as "favorable" or "unfavorable." Favorable microbiological response assessments included "eradication" and "presumed eradication." Unfavorable microbiological response assessments included "persistence," "persistence with increasing minimum inhibitory concentration (MIC)," and "presumed persistence." Indeterminate microbiologic response assessments included cIAI patients where the clinical response was changed to indeterminate due to a Surgical Review Panel assessment of inadequate source control (ie, circumstances that preclude classification as eradication, presumed eradication, persistence, persistence with increasing MIC, and presumed persistence).
Per-patient Microbiological Response at EOT in EME at EOT Analysis Set	28 hours after completion of last infusion of study therapy. Duration of study therapy was 5 to 21 days.	Microbiological responses as per the protocoled criteria: responses other than "indeterminate" were classified as "favorable" or "unfavorable." Favorable microbiological response assessments included "eradication" and "presumed eradication." Unfavorable microbiological response assessments included "persistence," "persistence with increasing minimum inhibitory concentration (MIC)," and "presumed persistence." Indeterminate microbiologic response assessments included cIAI patients where the clinical response was changed to indeterminate due to a Surgical Review Panel assessment of inadequate source control (ie, circumstances that preclude classification as eradication, presumed eradication, persistence, persistence with increasing MIC, and presumed persistence).
Clinical Cure at TOC by Baseline Gram-negative Pathogen in mMITT Analysis Set	6-12 days after last infusion of study therapy.Duration of study therapy was 5 to 21 days.	Proportion of patients with clinical cure at TOC visit by baseline pathogen (\>=10% of frequency in the combined cIAI and cUTI patients) in the mMITT analysis set. Clinical cure: Complete resolution or significant improvement of signs and symptoms of the index infection such that no further antibacterial therapy (other than those allowed per protocol) is necessary; for cIAI patients no drainage or surgical intervention after 96 hours from randomization is necessary (ie. drainage or surgical intervention up to 96 hours from randomization is permissible).
Clinical Cure at TOC by Baseline Gram-negative Pathogen in EME at TOC Analysis Set	6-12 days after last infusion of study therapy.Duration of study therapy was 5 to 21 days.	Proportion of patients with clinical cure at TOC visit by baseline Gram-negative pathogen (\>=10% of frequency in the combined cIAI and cUTI patients) in EME at TOC analysis set. Clinical cure: Complete resolution or significant improvement of signs and symptoms of the index infection such that no further antibacterial therapy (other than those allowed per protocol) is necessary; for cIAI patients no drainage or surgical intervention after 96 hours from randomization is necessary (ie. drainage or surgical intervention up to 96 hours from randomization is permissible).
Clinical Cure at FU1 by Previously Failed Treatment Class in EME at FU1 Analysis Set	cIAI: 27-37 calendar days from randomization/cUTI: 20-27 calendar days from randomization	Proportion of patients with clinical cure at FU1 visit by previously failed treatment class in EME at FU1 analysis set. Clinical cure: Complete resolution or significant improvement of signs and symptoms of the index infection such that no further antibacterial therapy (other than those allowed per protocol) is necessary; for cIAI patients no drainage or surgical intervention after 96 hours from randomization is necessary (ie. drainage or surgical intervention up to 96 hours from randomization is permissible).
Clinical Cure at EOT by Previously Failed Treatment Class in EME at EOT Analysis Set	28 hours after completion of last infusion of study therapy.Duration of study therapy was 5 to 21 days.	Proportion of patients with clinical cure at EOT visit by previously failed treatment class in EME at EOT analysis set. Clinical cure: Complete resolution or significant improvement of signs and symptoms of the index infection such that no further antibacterial therapy (other than those allowed per protocol) is necessary; for cIAI patients no drainage or surgical intervention after 96 hours from randomization is necessary (ie. drainage or surgical intervention up to 96 hours from randomization is permissible).
Clinical Cure at TOC by Previously Failed Treatment Class in EME at TOC Analysis Set	6-12 days after last infusion of study therapy. Duration of study therapy was 5 to 21 days.	Proportion of patients with clinical cure at TOC visit by previously failed treatment class in EME at TOC analysis set. Clinical cure: Complete resolution or significant improvement of signs and symptoms of the index infection such that no further antibacterial therapy (other than those allowed per protocol) is necessary; for cIAI patients no drainage or surgical intervention after 96 hours from randomization is necessary (ie. drainage or surgical intervention up to 96 hours from randomization is permissible).
Clinical Cure at FU2 by Previously Failed Treatment Class in EME at FU2 Analysis Set	At FU2, data was only collected for the cUTI Arms: 28-34 calendar days from randomization	Proportion of patients with clinical cure at FU2 visit by previously failed treatment class in EME at FU2 analysis set. Clinical cure: Complete resolution or significant improvement of signs and symptoms of the index infection such that no further antibacterial therapy (other than those allowed per protocol) is necessary.
Per-patient Microbiological Response at TOC in EME at TOC Analysis Set	6-12 days after last infusion of study therapy.Duration of study therapy was 5 to 21 days.	Microbiological responses as per the protocoled criteria: responses other than "indeterminate" were classified as "favorable" or "unfavorable." Favorable microbiological response assessments included "eradication" and "presumed eradication." Unfavorable microbiological response assessments included "persistence," "persistence with increasing minimum inhibitory concentration (MIC)," and "presumed persistence." Indeterminate microbiologic response assessments included cIAI patients where the clinical response was changed to indeterminate due to a Surgical Review Panel assessment of inadequate source control (ie, circumstances that preclude classification as eradication, presumed eradication, persistence, persistence with increasing MIC, and presumed persistence).
Per-patient Microbiological Response at FU1 in EME at FU1 Analysis Set	cUTI: 20-27 calendar days from randomization/cIAI: 27-37 calendar days from randomization	Microbiological responses as per the protocoled criteria: responses other than "indeterminate" were classified as "favorable" or "unfavorable." Favorable microbiological response assessments included "eradication" and "presumed eradication." Unfavorable microbiological response assessments included "persistence," "persistence with increasing minimum inhibitory concentration (MIC)," and "presumed persistence." Indeterminate microbiologic response assessments included cIAI patients where the clinical response was changed to indeterminate due to a Surgical Review Panel assessment of inadequate source control (ie, circumstances that preclude classification as eradication, presumed eradication, persistence, persistence with increasing MIC, and presumed persistence).
Per-patient Microbiological Response at FU2 in EME at FU2 Analysis Set	At FU2, data was only collected for the cUTI Arms: 28-34 calendar days from randomization	Microbiological responses as per the protocoled criteria: responses other than "indeterminate" were classified as "favorable" or "unfavorable." Favorable microbiological response assessments included "eradication" and "presumed eradication." Unfavorable microbiological response assessments included "persistence," "persistence with increasing minimum inhibitory concentration (MIC)," and "presumed persistence." Indeterminate microbiologic response assessments included cIAI patients where the clinical response was changed to indeterminate due to a Surgical Review Panel assessment of inadequate source control (ie, circumstances that preclude classification as eradication, presumed eradication, persistence, persistence with increasing MIC, and presumed persistence).
Per-pathogen Microbiological Response of Gram-negative Pathogen at EOT in mMITT Analysis Set	28 hours after completion of last infusion of study therapy. Duration of study therapy was 5 to 21 days.	Proportion of patients with a favorable per-pathogen microbiological response for pathogens (\>=10% of frequency in the combined cIAI and cUTI patients): favourable microbiological response includes: Eradication Absence (or urine quantification less than 10\^4 CFU/ml for cUTI patients) of causative pathogen from an appropriately obtained specimen at the site of infection. If the patient was bacteremic at Screening, the bacteremia has also resolved. Presumed eradication where, repeat cultures were not performed/clinically indicated in a patient who had a clinical response of cure (specific to cIAI population).
Per-pathogen Microbiological Response of Gram-negative Pathogen at TOC in mMITT Analysis Set	6-12 days after last infusion of study therapy. Duration of study therapy was 5 to 21 days.	Proportion of patients with a favorable per-pathogen microbiological response for pathogens (\>=10% of frequency in the combined cIAI and cUTI patients): favourable microbiological response includes: Eradication Absence (or urine quantification less than 10\^4 CFU/ml for cUTI patients) of causative pathogen from an appropriately obtained specimen at the site of infection. If the patient was bacteremic at Screening, the bacteremia has also resolved. Presumed eradication where, repeat cultures were not performed/clinically indicated in a patient who had a clinical response of cure (specific to cIAI population).
Per-pathogen Microbiological Response of Gram-negative Pathogen at FU1 in mMITT Analysis Set	cIAI: 27-37 calendar days from randomization/cUTI: 20-27 calendar days from randomization	Proportion of patients with a favorable per-pathogen microbiological response for pathogens (\>=10% of frequency in the combined cIAI and cUTI patients): favourable microbiological response includes: Eradication Absence (or urine quantification less than 10\^4 CFU/ml for cUTI patients) of causative pathogen from an appropriately obtained specimen at the site of infection. If the patient was bacteremic at Screening, the bacteremia has also resolved. Presumed eradication where, repeat cultures were not performed/clinically indicated in a patient who had a clinical response of cure (specific to cIAI population).
Per-pathogen Microbiological Response of Gram-negative Pathogen at FU2 in mMITT Analysis Set	At FU2, data was only collected for the cUTI Arms: 28-34 calendar days from randomization	Proportion of patients with a favorable per-pathogen microbiological response for pathogens (\>=10% of frequncy in the combined cIAI and cUTI patients): favourable microbiological response includes: Eradication Absence (or urine quantification less than 10\^4 CFU/ml for cUTI patients) of causative pathogen from an appropriately obtained specimen at the site of infection. If the patient was bacteremic at Screening, the bacteremia has also resolved. Presumed eradication where, repeat cultures were not performed/clinically indicated in a patient who had a clinical response of cure (specific to cIAI population).
Per-pathogen Microbiological Response of Gram-negative Pathogen at EOT in EME at EOT Analysis Set	28 hours after completion of last infusion of study therapy. Duration of study therapy was 5 to 21 days.	Proportion of patients with a favorable per-pathogen microbiological response for pathogens (\>=10% of frequncy in the combined cIAI and cUTI patients): favourable microbiological response includes: Eradication Absence (or urine quantification less than 10\^4 CFU/ml for cUTI patients) of causative pathogen from an appropriately obtained specimen at the site of infection. If the patient was bacteremic at Screening, the bacteremia has also resolved. Presumed eradication where, repeat cultures were not performed/clinically indicated in a patient who had a clinical response of cure (specific to cIAI population).
Per-pathogen Microbiological Response of Gram-negative Pathogen at TOC in EME at TOC Analysis Set	6-12 days after last infusion of study therapy. Duration of study therapy was 5 to 21 days.	Proportion of patients with a favorable per-pathogen microbiological response for pathogens (\>=10% of frequncy in the combined cIAI and cUTI patients): favourable microbiological response includes: Eradication Absence (or urine quantification less than 10\^4 CFU/ml for cUTI patients) of causative pathogen from an appropriately obtained specimen at the site of infection. If the patient was bacteremic at Screening, the bacteremia has also resolved. Presumed eradication where, repeat cultures were not performed/clinically indicated in a patient who had a clinical response of cure (specific to cIAI population).
Per-pathogen Microbiological Response of Gram-negative Pathogen at FU1 in EME at FU1 Analysis Set	cIAI: 27-37 calendar days from randomization/cUTI: 20-27 calendar days from randomization	Proportion of patients with a favorable per-pathogen microbiological response for pathogens (\>=10% of frequncy in the combined cIAI and cUTI patients): favourable microbiological response includes: Eradication Absence (or urine quantification less than 10\^4 CFU/ml for cUTI patients) of causative pathogen from an appropriately obtained specimen at the site of infection. If the patient was bacteremic at Screening, the bacteremia has also resolved. Presumed eradication where, repeat cultures were not performed/clinically indicated in a patient who had a clinical response of cure (specific to cIAI population).
Per-pathogen Microbiological Response of Gram-negative Pathogen at FU2 in EME at FU2 Analysis Set	At FU2, data was only collected for the cUTI Arms: 28-34 calendar days from randomization	Proportion of patients with a favorable per-pathogen microbiological response for pathogens (\>=10% of frequncy in the combined cIAI and cUTI patients): favourable microbiological response includes: Eradication Absence (or urine quantification less than 10\^4 CFU/ml for cUTI patients) of causative pathogen from an appropriately obtained specimen at the site of infection. If the patient was bacteremic at Screening, the bacteremia has also resolved. Presumed eradication where, repeat cultures were not performed/clinically indicated in a patient who had a clinical response of cure (specific to cIAI population).
Per-pathogen Microbiological Response of Gram-negative Pathogen at TOC by CAZ-AVI MIC in mMITT Analysis Set	6-12 days after last infusion of study therapy. Duration of study therapy was 5 to 21 days.	Proportion of patients with a favorable per-pathogen microbiological response for pathogens (\>=10% of frequncy in the combined cIAI and cUTI patients): favourable microbiological response includes: Eradication Absence (or urine quantification less than 10\^4 CFU/ml for cUTI patients) of causative pathogen from an appropriately obtained specimen at the site of infection. If the patient was bacteremic at Screening, the bacteremia has also resolved. Presumed eradication where, repeat cultures were not performed/clinically indicated in a patient who had a clinical response of cure (specific to cIAI population). For E.coli, MIC available values are: \<=0.008, 0.03, 0.06, 0.12, 0.25, 0.5, 1, 2, 8. For K. pneumoniae, MIC available values are: 0.06, 0.12, 0.25, 0.5, 1, 2, 4, 32, \>32. For P. aeruginosa, MIC available values are: 2, 4, 8, 16, 32, \>32.
Per-pathogen Microbiological Response of Gram-negative Pathogen at TOC by CAZ-AVI MIC in EME at TOC Analysis Set	6-12 days after last infusion of study therapy. Duration of study therapy was 5 to 21 days.	Proportion of patients with a favorable per-pathogen microbiological response for pathogens (\>=10% of frequncy in the combined cIAI and cUTI patients): favourable microbiological response includes: Eradication Absence (or urine quantification less than 10\^4 CFU/ml for cUTI patients) of causative pathogen from an appropriately obtained specimen at the site of infection. If the patient was bacteremic at Screening, the bacteremia has also resolved. Presumed eradication where, repeat cultures were not performed/clinically indicated in a patient who had a clinical response of cure (specific to cIAI population). For E.coli, MIC available values are: \<=0.008, 0.03, 0.06, 0.12, 0.25, 0.5, 1, 2, 8. For K. pneumoniae, MIC available values are: 0.06, 0.12, 0.25, 0.5, 1, 2, 4, \>32. For P. aeruginosa, MIC available values are: 2, 4, 8, 16, 32, \>32.
The Reason for Treatment Change/Discontinuation in mMITT Analysis Set	From first infusion to last infusion of study therapy. Duration of study therapy was 5 to 21 days.	Proportion of patients in the mMITT analysis set for whom the assigned study treatment was changed, discontinued, or interrupted. Creatinine clearance (CrCl)
The 28 Days All Cause Mortality Rate in mMITT Analysis Set	From first infusion to Day 28	Proportion of patients with Day 28 all-cause mortality in mMITT analysis set. The death in the cIAI patient were reviewed independently by the SRP Chair.
The 28 Days All Cause Mortality Rate in EME at TOC Analysis Set	From first infusion to Day 28	Proportion of patients with Day 28 all-cause mortality in EME at TOC analysis set. The death in the cIAI patient were reviewed independently by the SRP Chair.
Plasma Concentrations for Ceftazidime and Avibactam - cIAI in PK Analysis Set	Anytime within 15 minutes prior to or after stopping study drug, anytime between 30 to 90 minutes after stopping study drug, anytime between 300 to 360 minutes after stopping study drug	Blood samples were taken on Day 3 for ceftazidime and avibactam plasma concentration.
Plasma Concentrations for Ceftazidime and Avibactam - cUTI in PK Analysis Set	Anytime within 15 minutes prior to or after stopping study drug, anytime between 30 to 90 minutes after stopping study drug, anytime between 300 to 360 minutes after stopping study drug	Blood samples were taken on Day 3 for ceftazidime and avibactam plasma concentration.

Trial Locations

Locations (1)

Research Site; 🇺🇦 Zaporizhzhya, Ukraine