Meropenem-Vaborbactam vs. Best Available Therapy for Carbapenem-Resistant Enterobacteriaceae Infections in TANGO II: Outcomes in Immunocompromised Patients
Abstract Background Immunocompromised patients are at high risk for mortality due to carbapenem-resistant Enterobacteriaceae (CRE). Meropenem-vaborbactam (M-V) is a novel cyclic boronic acid β-lactamase inhibitor combination being developed for treatment of serious gram-negative infections, includin...
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| Published in | Open forum infectious diseases Vol. 4; no. suppl_1; p. S537 |
|---|---|
| Main Authors | , , , , , , , |
| Format | Journal Article |
| Language | English |
| Published |
US
Oxford University Press
01.10.2017
|
| Online Access | Get full text |
| ISSN | 2328-8957 2328-8957 |
| DOI | 10.1093/ofid/ofx163.1398 |
Cover
| Abstract | Abstract
Background
Immunocompromised patients are at high risk for mortality due to carbapenem-resistant Enterobacteriaceae (CRE). Meropenem-vaborbactam (M-V) is a novel cyclic boronic acid β-lactamase inhibitor combination being developed for treatment of serious gram-negative infections, including CRE. This analysis reports outcomes among immunocompromised subjects in TANGO II, a randomized, open-label comparative trial with best available therapy (BAT) in subjects with complicated urinary tract infection (cUTI), acute pyelonephritis (AP), HABP/VABP, bacteremia, and cIAI, due to known or suspected CRE.
Methods
Eligible subjects were randomized 2:1 to M-V (2g/2g every 8h) or BAT for 7 to 14 days. BAT included any of the following, alone or in combination: carbapenems, aminoglycosides, polymyxin B, colistin, tigecycline, or ceftazidime-avibactam (monotherapy only). Clinical cure was defined as complete resolution of signs or symptoms such that no further antimicrobial therapy was required.
Results
Of the 50 subjects who had a baseline pathogen (m-MITT population), 19 (38.0%) were immunocompromised (4 leukemia/lymphoma, 5 medication, 10 transplant). Among the 43 subjects with a baseline CRE pathogen (mCRE-MITT), 18 (41.9%) were immunocompromised. The most common infection types among immunocompromised subjects (mCRE-MITT) were bacteremia (61.1%), cUTI/AP (16.7%), HABP/VABP (11.1%), and cIAI (11.1%). Clinical efficacy and mortality among immunocompromised in the mCRE-MITT population are shown. M-V was associated with fewer drug-related adverse events (30.8% vs. 40.0%), serious adverse events (38.5% vs. 50.0%), and renal-related adverse events (7.7% vs. 40.0%) than BAT.
Conclusion
In immunocompromised subjects, receipt of M-V was associated with higher clinical cure rates and a lower mortality rate than BAT (m-MITT, mCRE-MITT populations). M-V is a promising treatment option for CRE in this population.
Disclosures
D. L. Paterson, Achaogen: Consultant, Consulting fee; Merck: Consultant and Investigator, Consulting fee and Research grant; Shionogi: Consultant, Consulting fee; GlaxoSmithKline: Consultant, Consulting fee; E. Alexander, The Medicines Company: Shareholder, Salary; J. S. Loutit, The Medicine’s Company: Employee and Shareholder, Salary; S. Zhang, The Medicines Company: Shareholder, Salary; M. N. Dudley, The Medicine’s Company: Employee and Shareholder, Salary; T. J. Walsh, The Medicines Company: Consultant and Investigator, Consulting fee and Research grant; Astellas: Consultant and Investigator, Consulting fee and Research grant; Allergan: Consultant and Investigator, Consulting fee and Research grant; Merck: Consultant and Investigator, Consulting fee and Research grant
Outcomes in mCRE-MITT
M-V (n = 10)
BAT (n = 8)
ALL (n = 18)
Difference (95% CI)
Clinical Cure at End of Therapy (EOT)
6 (60%)
2 (25%)
8 (44.4%)
+35% (-13.5% to 72.8%)
Clinical Cure at Test of Cure (EOT+7 days)
7 (70%)
0 (0%)
7 (38.9%)
+70% (26.9% to 93.3%)
All-Cause Mortality Day 28
2 (20%)
3 (37.5%)
5 (27.8%)
-17.5% (-59.2% to 29.3%) |
|---|---|
| AbstractList | Abstract
Background
Immunocompromised patients are at high risk for mortality due to carbapenem-resistant Enterobacteriaceae (CRE). Meropenem-vaborbactam (M-V) is a novel cyclic boronic acid β-lactamase inhibitor combination being developed for treatment of serious gram-negative infections, including CRE. This analysis reports outcomes among immunocompromised subjects in TANGO II, a randomized, open-label comparative trial with best available therapy (BAT) in subjects with complicated urinary tract infection (cUTI), acute pyelonephritis (AP), HABP/VABP, bacteremia, and cIAI, due to known or suspected CRE.
Methods
Eligible subjects were randomized 2:1 to M-V (2g/2g every 8h) or BAT for 7 to 14 days. BAT included any of the following, alone or in combination: carbapenems, aminoglycosides, polymyxin B, colistin, tigecycline, or ceftazidime-avibactam (monotherapy only). Clinical cure was defined as complete resolution of signs or symptoms such that no further antimicrobial therapy was required.
Results
Of the 50 subjects who had a baseline pathogen (m-MITT population), 19 (38.0%) were immunocompromised (4 leukemia/lymphoma, 5 medication, 10 transplant). Among the 43 subjects with a baseline CRE pathogen (mCRE-MITT), 18 (41.9%) were immunocompromised. The most common infection types among immunocompromised subjects (mCRE-MITT) were bacteremia (61.1%), cUTI/AP (16.7%), HABP/VABP (11.1%), and cIAI (11.1%). Clinical efficacy and mortality among immunocompromised in the mCRE-MITT population are shown. M-V was associated with fewer drug-related adverse events (30.8% vs. 40.0%), serious adverse events (38.5% vs. 50.0%), and renal-related adverse events (7.7% vs. 40.0%) than BAT.
Conclusion
In immunocompromised subjects, receipt of M-V was associated with higher clinical cure rates and a lower mortality rate than BAT (m-MITT, mCRE-MITT populations). M-V is a promising treatment option for CRE in this population.
Disclosures
D. L. Paterson, Achaogen: Consultant, Consulting fee; Merck: Consultant and Investigator, Consulting fee and Research grant; Shionogi: Consultant, Consulting fee; GlaxoSmithKline: Consultant, Consulting fee; E. Alexander, The Medicines Company: Shareholder, Salary; J. S. Loutit, The Medicine’s Company: Employee and Shareholder, Salary; S. Zhang, The Medicines Company: Shareholder, Salary; M. N. Dudley, The Medicine’s Company: Employee and Shareholder, Salary; T. J. Walsh, The Medicines Company: Consultant and Investigator, Consulting fee and Research grant; Astellas: Consultant and Investigator, Consulting fee and Research grant; Allergan: Consultant and Investigator, Consulting fee and Research grant; Merck: Consultant and Investigator, Consulting fee and Research grant
Outcomes in mCRE-MITT
M-V (n = 10)
BAT (n = 8)
ALL (n = 18)
Difference (95% CI)
Clinical Cure at End of Therapy (EOT)
6 (60%)
2 (25%)
8 (44.4%)
+35% (-13.5% to 72.8%)
Clinical Cure at Test of Cure (EOT+7 days)
7 (70%)
0 (0%)
7 (38.9%)
+70% (26.9% to 93.3%)
All-Cause Mortality Day 28
2 (20%)
3 (37.5%)
5 (27.8%)
-17.5% (-59.2% to 29.3%) |
| Author | Paterson, David L Bhowmick, Tanaya Loutit, Jeffrey S Alexander, Elizabeth Dudley, Michael N Zhang, Shu Kwak, Eun J Walsh, Thomas J |
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Background
Immunocompromised patients are at high risk for mortality due to carbapenem-resistant Enterobacteriaceae (CRE). Meropenem-vaborbactam (M-V)... |
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