Urinary Tract Infection Clinical Trial
— PIVOT-POOfficial title:
A Phase 3, Randomized, Double-blind, Double-dummy, Multicenter, Multinational Study to Assess the Efficacy and Safety of Orally Administered Tebipenem Pivoxil Hydrobromide (TBP-PI-HBr) Compared to Intravenously Administered Imipenem-cilastatin in Patients With Complicated Urinary Tract Infection (cUTI) or Acute Pyelonephritis (AP)
The primary purpose of this study is to assess the efficacy of oral TBP-PI-HBr as compared with intravenous (IV) imipenem-cilastatin with respect to the overall response (combined clinical cure plus microbiological eradication) at the Test-of-Cure (TOC) visit in hospitalized adult participants (≥18 years of age) with cUTI or AP.
Status | Recruiting |
Enrollment | 2648 |
Est. completion date | December 2025 |
Est. primary completion date | November 2025 |
Accepts healthy volunteers | No |
Gender | All |
Age group | 18 Years and older |
Eligibility | Inclusion Criteria: 1. Have a diagnosis of cUTI or AP. 2. Have an adequate urine specimen for evaluation and culture obtained within 24 hours prior to randomization with evidence of pyuria that includes at least one of the following: 1. at least 10 white blood cells (WBCs) per high power field (HPF) in urine sediment 2. at least 10 WBCs per millimeters cubed (mm^3) in unspun urine 3. positive leukocyte esterase (LE) on urinalysis Note: Participants may be randomized and administered study drug prior to knowledge of urine culture results, but pyuria must be documented. 3. Expectation, in the judgment of the Investigator, that the participant will survive with effective antimicrobial therapy and appropriate supportive care for the anticipated duration of the study. Exclusion Criteria: 1. Presence of any known or suspected disease or condition that, in the opinion of the Investigator, may confound the assessment of efficacy. 2. Gross hematuria requiring intervention other than administration of study drug or removal/placement of urinary tract instrumentation. 3. Urinary tract surgery within 7 days prior to randomization or urinary tract surgery planned during the study period. 4. Creatinine clearance (CrCl) of =30 milliliters per minute (mL/min), as estimated by the Cockcroft-Gault formula. 5. Anticipated concomitant use of non-study antimicrobial drug therapy between randomization and the LFU visit that would potentially effect outcome evaluations of cUTI/AP. 6. Receipt of more than a single dose of a potentially effective antimicrobial within 72 hours prior to study randomization. 7. Severe hepatic impairment at Screening, as evidenced by alanine aminotransferase (ALT) or aspartate aminotransferase (AST) >5×upper limit of normal (ULN) or total bilirubin >3×ULN, or clinical signs of cirrhosis or end-stage hepatic disease (e.g., ascites, hepatic encephalopathy). 8. Pregnant or lactating women. 9. History of epilepsy or known seizure disorder (excluding a history of childhood febrile seizures). 10. History of proven or suspected Clostridioides difficile associated diarrhea. 11. History of human immunodeficiency virus (HIV) infection. 12. QT interval corrected using Fridericia's formula (QTcF) >480 milliseconds (msec) based on screening ECG. 13. History of known genetic metabolism anomaly associated with carnitine deficiency. 14. Requirement for concomitant use of valproic acid, divalproex sodium, or probenecid between randomization and EOT. Note: Other inclusion and exclusion criteria as per protocol may apply. |
Country | Name | City | State |
---|---|---|---|
Bosnia and Herzegovina | Medical Facility | Banja Luka | |
Bosnia and Herzegovina | Medical Facility | Sarajevo | |
Bulgaria | Medical Facility | Blagoevgrad | |
Bulgaria | Medical Facility | Dobrich | |
Bulgaria | Medical Facility | Gabrovo | |
Bulgaria | Medical facility | Lom | |
Bulgaria | Medical Facility | Pleven | |
Bulgaria | Medical Facility | Plovdiv | |
Bulgaria | Medical facility | Ruse | |
Bulgaria | Medical facility | Shumen | |
Bulgaria | Medical Facility | Sliven | |
Bulgaria | Medical facility | Sofia | |
Bulgaria | Medical Facility | Varna | |
Croatia | Medical Facility | Cakovec | |
Croatia | Medical Facility | Slavonski Brod | |
Croatia | Medical Facility | Split | |
Croatia | Medical Facility | Zagreb | |
Estonia | Medical Facility | Kohtla-Jarve | |
Estonia | Medical Facility | Parnu | |
Estonia | Medical Facility | Tallinn | |
Estonia | Medical Facility | Voru | |
Georgia | Medical facility | Tbilisi | |
Hungary | Medical Facility | Budapest | |
Hungary | Medical Facility | Eger | |
Hungary | Medical Facility | Kistarcsa | |
Hungary | Medical Facility | Nyiregyhaza | |
Moldova, Republic of | Medical Facility | Chisinau | |
Poland | Medical Facility | Krakow | |
Poland | Medical Facility | Leczna | |
Poland | Medical Facility | Lodz | |
Poland | Medical Facility | Warsaw | |
Romania | Medical Facility | Brasov | |
Romania | Medical facility | Bucharest | |
Romania | Medical facility | Craiova | |
Romania | Medical Facility | Iasi | |
Romania | Medical Facility | Oradea | |
Romania | Medical Facility | Timisoara | |
Serbia | Medical facility | Belgrade | |
Serbia | Medical facility | Kragujevac | |
Serbia | Medical facility | Nis | |
Serbia | Medical facility | Novi Sad | |
Slovakia | Medical Facility | Bratislava | |
Slovakia | Medical Facility | Galanta | |
Slovakia | Medical Facility | Lucenec | |
Slovakia | Medical Facility | Malacky | |
Slovakia | Medical Facility | Poprad | |
South Africa | Medical facility | Benoni | |
South Africa | Medical facility | Durban | |
South Africa | Medical Facility | Pretoria | |
United States | Medical facility | Miami | Florida |
Lead Sponsor | Collaborator |
---|---|
Spero Therapeutics | GlaxoSmithKline |
United States, Bosnia and Herzegovina, Bulgaria, Croatia, Estonia, Georgia, Hungary, Moldova, Republic of, Poland, Romania, Serbia, Slovakia, South Africa,
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | Number of Participants With Overall Response at the Test-of-Cure (TOC) Visit | Overall response includes combination of clinical cure and favorable microbiological response. Clinical cure is defined as a complete resolution or significant improvement of signs and symptoms of cUTI or AP that were present at Baseline and no new symptoms, such that no further antibacterial therapy is warranted, and participant is alive. Favorable microbiological response (microbiological eradication) is defined as a reduction of Baseline uropathogens to <10^3 colony forming unit per milliliter (CFU/mL) and negative repeated blood culture if blood culture was positive for uropathogen growth at baseline and participant is alive. | Day 17 | |
Secondary | Number of Participants in the Microbiologically Evaluable Population With Overall Response at the TOC Visit | Overall response includes combination of clinical cure and favorable microbiological response. Clinical cure is defined as a complete resolution or significant improvement of signs and symptoms of cUTI or AP that were present at Baseline and no new symptoms, such that no further antibacterial therapy is warranted, and participant is alive. Favorable microbiological response (microbiological eradication) is defined as a reduction of Baseline uropathogens to <10^3 CFU/mL and negative repeated blood culture if blood culture was positive for uropathogen growth at Baseline and participant is alive. | Day 17 | |
Secondary | Number of Participants With Overall Response at the End-of-Treatment (EOT) and Late Follow-Up (LFU) Visits | Overall response includes combination of clinical cure and favorable microbiological response. Clinical cure is defined as a complete resolution or significant improvement of signs and symptoms of cUTI or AP that were present at Baseline and no new symptoms, such that no further antibacterial therapy is warranted, and participant is alive. Favorable microbiological response (microbiological eradication) is defined as a reduction of Baseline uropathogens to <10^3 CFU/mL and negative repeated blood culture if blood culture was positive for uropathogen growth at Baseline and participant is alive. | Days 10 and 28 | |
Secondary | Number of Participants With Clinical Response at the EOT, TOC and LFU Visits | Participants will be evaluated for clinical response outcome based on assessment of signs and symptoms as: Cure, including sustained clinical cure: Sustained clinical cure is defined as met criteria for clinical cure at TOC, and remained free of new or recurrent signs and symptoms of cUTI or AP at LFU visit such that no further antibacterial therapy is warranted; Failure, including clinical relapse: Clinical relapse is defined as met criteria for clinical cure at TOC, but new signs and symptoms of cUTI or AP are present at LFU visit and participant requires antibacterial therapy for cUTI; Clinical indeterminate: insufficient data are available to determine if participant is a sustained clinical cure or clinical relapse. If a participant is assessed as a clinical failure at EOT, participant is automatically considered a failure at TOC and LFU visits. If a participant is assessed as a clinical failure at TOC, participant is automatically considered a failure at LFU visit. | Days 10, 17, and 28 | |
Secondary | Number of Participants With Microbiological Response at the EOT, TOC and LFU Visits | Participants will be evaluated for microbiological response based on blood and urine cultures as:Eradication, including sustained microbiologic eradication, i.e.,microbiologic eradication at TOC and no subsequent urine culture after TOC demonstrating recurrence of original Baseline uropathogen at =10^3 CFU/mL;Persistence, including microbiologic recurrence, i.e.,isolation from urine culture at =10^3 CFU/mL or blood culture of any of Baseline uropathogen(s) at any time after documented eradication at TOC visit up to and including LFU visit;Microbiologic indeterminate:no follow-up urine culture is available, or urine culture results are missing, or follow-up urine culture cannot be interpreted for any reason. If a participant is assessed as a microbiological persistence at EOT,participant is automatically considered persistent at TOC and LFU. If assessed as persistent at TOC, participant is automatically considered a persistent at LFU. | Days 10, 17, and 28 | |
Secondary | Number of Participants With Overall Response at the EOT, TOC, and LFU Visits in Participants With Drug-resistant Enterobacterales | Overall response includes combination of clinical cure and favorable microbiological response. Clinical cure is defined as a complete resolution or significant improvement of signs and symptoms of cUTI or AP that were present at Baseline and no new symptoms, such that no further antibacterial therapy is warranted, and participant is alive. Favorable microbiological response (microbiological eradication) is defined as a reduction of Baseline uropathogens to <10^3 CFU/mL and negative repeated blood culture if blood culture was positive for uropathogen growth at Baseline and participant is alive. | Days 10, 17, and 28 | |
Secondary | Number of Participants With Clinical Response at the EOT, TOC, and LFU Visits in Participants With Drug-resistant Enterobacterales | Participants will be evaluated for clinical response outcome based on assessment of signs and symptoms as: Cure, including sustained clinical cure: Sustained clinical cure is defined as met criteria for clinical cure at TOC, and remained free of new or recurrent signs and symptoms of cUTI or AP at LFU visit such that no further antibacterial therapy is warranted; Failure, including clinical relapse: Clinical relapse is defined as met criteria for clinical cure at TOC, but new signs and symptoms of cUTI or AP are present at LFU visit and participant requires antibacterial therapy for cUTI; Clinical indeterminate: insufficient data are available to determine if participant is a sustained clinical cure or clinical relapse. If a participant is assessed as a clinical failure at EOT, participant is automatically considered a failure at TOC and LFU visits. If a participant is assessed as a clinical failure at TOC, participant is automatically considered a failure at LFU visit. | Days 10, 17, and 28 | |
Secondary | Number of Participants With Microbiological Response at the EOT, TOC, and LFU Visits in Participants With Drug-resistant Enterobacterales | Participants will be evaluated for microbiological response based on blood and urine cultures as:Eradication, including sustained microbiologic eradication, i.e.,microbiologic eradication at TOC and no subsequent urine culture after TOC demonstrating recurrence of original Baseline uropathogen at =10^3 CFU/mL;Persistence, including microbiologic recurrence, i.e.,isolation from urine culture at =10^3 CFU/mL or blood culture of any of Baseline uropathogen(s) at any time after documented eradication at TOC visit up to and including LFU visit;Microbiologic indeterminate:no follow-up urine culture is available, or urine culture results are missing, or follow-up urine culture cannot be interpreted for any reason. If a participant is assessed as a microbiological persistence at EOT,participant is automatically considered persistent at TOC and LFU. If assessed as persistent at TOC, participant is automatically considered a persistent at LFU. | Days 10, 17, and 28 | |
Secondary | Number of Participants With Treatment-emergent Adverse Events (TEAEs) and Serious Adverse Events (SAEs) | From first dose of study drug (Day 1) up to Day 28 | ||
Secondary | Plasma Concentration of Tebipenem | At multiple time points post dose on Day 2 |
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