This study aims to compare treatment with a fixed-dose combination (FDC) of imipenem/relebactam/cilastatin (IMI/REL) with a FDC of piperacillin/tazobactam (PIP/TAZ) in participants with hospital-acquired or ventilator-associated bacterial pneumonia (HABP or VAPB, respectively). The primary hypothesis is that IMI/REL is non-inferior to PIP/TAZ in the incidence rate of all-cause mortality.
Study Type
INTERVENTIONAL
Allocation
RANDOMIZED
Purpose
TREATMENT
Masking
DOUBLE
Enrollment
537
Imipenem 500 mg as part of a FDC administered by IV every 6 hours for a minimum of 7 days, up to 14 days
Relebactam 250 mg as part of a FDC administered by IV every 6 hours for a minimum of 7 days, up to 14 days
Cilastatin 500 mg as part of a FDC administered by IV every 6 hours for a minimum of 7 days, up to 14 days
Percentage of Participants With All-cause Mortality (ACM) Through Day 28 in the Modified Intention-to-treat (MITT) Population
The percentage of participants in the MITT population with mortality due to any cause from randomization through Day 28 was determined for each arm.
Time frame: Up to 28 days
Percentage of Participants in the MITT Population With a Favorable Clinical Response (FCR) at Early Follow-up (EFU) Visit
The percentage of participants with a FCR at EFU was determined for each arm. Favorable clinical response at EFU was defined as either "sustained cure" (all pre-therapy signs and symptoms of the index infection have resolved \[or returned to "pre-infection status"\] with no evidence of resurgence and no additional antibiotics are required) or "cure" (all pre-therapy signs and symptoms of the index infection have resolved \[or returned to "pre-infection status"\] and no additional antibiotics are required).
Time frame: Up to 16 days after end of therapy (up to 30 days)
Percentage of Participants With ≥1 Adverse Event (AE)
An AE is defined as any untoward medical occurrence in a participant administered a pharmaceutical product and which does not necessarily have to have a causal relationship with this treatment.
Time frame: Up to 30 days
Percentage of Participants Discontinuing Study Therapy Due to an AE
An AE is defined as any untoward medical occurrence in a participant administered a pharmaceutical product and which does not necessarily have to have a causal relationship with this treatment.
Time frame: Up to 14 days
Percentage of Participants With ACM in the Microbiological Modified Intention-to-treat (mMITT) Population
The percentage of participants in the mMITT population with mortality due to any cause from randomization through Day 28 was determined for each arm.
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Piperacillin 4000 mg as part of a FDC administered by IV every 6 hours for a minimum of 7 days, up to 14 days
Tazobactam 500 mg as part of a FDC administered by IV every 6 hours for a minimum of 7 days, up to 14 days
Linezolid 600 mg administered open-label by IV every 12 hours for up to 14 days
Time frame: Up to 28 days
Percentage of Participants With ACM at EFU in the MITT Population
The percentage of participants in the MITT population with mortality due to any cause from randomization through EFU was determined for each arm.
Time frame: Up to 16 days after end of therapy (up to 30 days)
Percentage of Participants With ACM at EFU in the mMITT Population
The percentage of participants in the mMITT population with mortality due to any cause from randomization through EFU was determined for each arm.
Time frame: Up to 16 days after end of therapy (up to 30 days)
Percentage of Participants in the Clinically Evaluable (CE) Population With a FCR at On-therapy Visit 1 (OTX1) [Day 3]
The percentage of participants with a FCR at OTX1 was determined for each arm. Favorable clinical response at OTX1 was defined as "improved" (majority of pre-therapy signs and symptoms of the index infection have improved or resolved \[or returned to "pre-infection status"\]).
Time frame: Day 3 (OTX1)
Percentage of Participants in the CE Population With a FCR at OTX2 (Day 6)
The percentage of participants with a FCR at OTX2 was determined for each arm. Favorable clinical response at OTX2 was defined as "improved" (majority of pre-therapy signs and symptoms of the index infection have improved or resolved \[or returned to "pre-infection status"\]).
Time frame: Day 6 (OTX2)
Percentage of Participants in the CE Population With a FCR at OTX3 (Day 10)
The percentage of participants with a FCR at OTX3 was determined for each arm. Favorable clinical response at OTX3 was defined as "improved" (majority of pre-therapy signs and symptoms of the index infection have improved or resolved \[or returned to "pre-infection status"\]).
Time frame: Day 10 (OTX3)
Percentage of Participants in the CE Population With a FCR at EOT Visit
The percentage of participants with a FCR at EOT was determined for each arm. Favorable clinical response at EOT was defined as either "cure" (all pre-therapy signs and symptoms of the index infection have resolved \[or returned to "pre-infection status"\] and no additional antibiotics are required) or "improved" (the majority of pre-therapy signs and symptoms of the index infection have improved or resolved \[or returned to "pre-infection status"\] and no additional antibiotics are required).
Time frame: From Day 7 to Day 14
Percentage of Participants in the CE Population With a FCR at Day 28
The percentage of participants with a FCR at Day 28 was determined for each arm. Favorable clinical response at Day 28 was defined as either "sustained cure" (all pre-therapy signs and symptoms of the index infection have resolved \[or returned to "pre-infection status"\] with no evidence of resurgence and no additional antibiotics are required) or "cure" (all pre-therapy signs and symptoms of the index infection have resolved \[or returned to "pre-infection status"\] and no additional antibiotics are required).
Time frame: Day 28
Percentage of Participants in the CE Population With a FCR at EFU Visit
The percentage of participants with a FCR at EFU was determined for each arm. Favorable clinical response at EFU was defined as either "sustained cure" (all pre-therapy signs and symptoms of the index infection have resolved \[or returned to "pre-infection status"\] with no evidence of resurgence and no additional antibiotics are required) or "cure" (all pre-therapy signs and symptoms of the index infection have resolved \[or returned to "pre-infection status"\] and no additional antibiotics are required).
Time frame: Up to 16 days after end of therapy (up to Day 30)
Percentage of Participants in the MITT Population With a FCR at OTX1 (Day 3)
The percentage of participants with a FCR at OTX1 was determined for each arm. Favorable clinical response at OTX1 was defined as "improved" (majority of pre-therapy signs and symptoms of the index infection have improved or resolved \[or returned to "pre-infection status"\]).
Time frame: Day 3 (OTX1)
Percentage of Participants in the MITT Population With a FCR at OTX2 (Day 6)
The percentage of participants with a FCR at OTX2 was determined for each arm. Favorable clinical response at OTX2 was defined as "improved" (majority of pre-therapy signs and symptoms of the index infection have improved or resolved \[or returned to "pre-infection status"\]).
Time frame: Day 6 (OTX2)
Percentage of Participants in the MITT Population With a FCR at OTX3 (Day 10)
The percentage of participants with a FCR at OTX3 was determined for each arm. Favorable clinical response at OTX3 was defined as "improved" (majority of pre-therapy signs and symptoms of the index infection have improved or resolved \[or returned to "pre-infection status"\]).
Time frame: Day 10 (OTX3)
Percentage of Participants in the MITT Population With a FCR at EOT
The percentage of participants with a FCR at EOT was determined for each arm. Favorable clinical response at EOT was defined as either "cure" (all pre-therapy signs and symptoms of the index infection have resolved \[or returned to "pre-infection status"\] and no additional antibiotics are required) or "improved" (the majority of pre-therapy signs and symptoms of the index infection have improved or resolved \[or returned to "pre-infection status"\] and no additional antibiotics are required).
Time frame: From Day 7 to Day 14
Percentage of Participants in the MITT Population With a FCR at Day 28
The percentage of participants with a FCR at Day 28 was determined for each arm. Favorable clinical response at Day 28 was defined as either "sustained cure" (all pre-therapy signs and symptoms of the index infection have resolved \[or returned to "pre-infection status"\] with no evidence of resurgence and no additional antibiotics are required) or "cure" (all pre-therapy signs and symptoms of the index infection have resolved \[or returned to "pre-infection status"\] and no additional antibiotics are required).
Time frame: Day 28
Percentage of Participants in the mMITT Population With a Favorable Microbiological Response (FMR) at End of Treatment (EOT) Visit
The percentage of participants with a FMR at EOT was determined for each arm. Favorable microbiological response at EOT was defined as either "eradication" (a lower respiratory tract culture taken at EOT showing eradication of baseline pathogen) or "presumed eradication" (no specimen collected because the participant deemed clinically cured or improved).
Time frame: From Day 7 to Day 14
Percentage of Participants in the mMITT Population With a FMR at EFU Visit
The percentage of participants with a FMR at EFU was determined for each arm. Favorable microbiological response at EOT was defined as either "eradication" (a lower respiratory tract culture taken at EFU showing eradication of baseline pathogen) or "presumed eradication" (no specimen collected because the participant deemed clinically cured or improved).
Time frame: Up to 16 days after end of therapy (up to Day 30)
Percentage of Participants in the Microbiologically Evaluable (ME) Population With a FMR at EOT Visit
The percentage of participants with a FMR at EOT was determined for each arm. Favorable microbiological response at EOT was defined as either "eradication" (a lower respiratory tract culture taken at EOT showing eradication of baseline pathogen) or "presumed eradication" (no specimen collected because the participant deemed clinically cured or improved).
Time frame: From Day 7 to Day 14
Percentage of Participants in the ME Population With a FMR at EFU Visit
The percentage of participants with a FMR at EOT was determined for each arm. Favorable microbiological response at EOT was defined as either "eradication" (a lower respiratory tract culture taken at EOT showing eradication of baseline pathogen) or "presumed eradication" (no specimen collected because the participant deemed clinically cured or improved).
Time frame: Up to 16 days after end of therapy (up to Day 30)