Pharmacokinetic and Pharmacodynamic Profiling of Minocycline for Injection following a Single Infusion in Critically Ill Adults in a Phase IV Open-Label Multicenter Study (ACUMIN)

Lodise, Thomas P.; Wart, Scott Van; Sund, Zoë; Bressler, Adam; Khan, Akram; Makley, Amy T.; Hamad, Yasir; Salata, Robert A.; Silveira, Fernanda P.; Sims, Matthew; Kabchi, Badih A.; Saad, Mohamed; Brown, Carrie; Oler, Randolph E.; Fowler, Vance G.; Wunderink, Richard G.

doi:10.1128/aac.01809-20

Cited by 24 publications

(26 citation statements)

References 30 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Unfortunately, the accurate determination of minocycline MICs against A. baumannii is challenging; disk-diffusion and E-test methods may overcall resistance [ 44 ]. The ACUMIN study, a 2021 PK/PD investigation evaluating minocycline in critically ill patients, described the lack of target attainment with minocycline dosed 200 mg IV q12 h against CRAB isolates with MICs > 1 mg/L [ 45 ]. These data emphasize the need for clinicians to consider requesting broth microdilution to confirm minocycline susceptibility if alternative agents are unavailable, and prioritize use only in cases where MICs are less than 1 mg/L.…”

Section: Linking Mechanisms Of Resistance To Treatment Optionsmentioning

confidence: 99%

Contemporary Perspective on the Treatment of Acinetobacter baumannii Infections: Insights from the Society of Infectious Diseases Pharmacists

et al. 2021

View full text Add to dashboard Cite

The purpose of this narrative review is to bring together the most recent epidemiologic, preclinical, and clinical findings to offer our perspective on best practices for managing patients with A. baumannii infections with an emphasis on carbapenem-resistant A. baumannii (CRAB). To date, the preferred treatment for CRAB infections has not been defined. Traditional agents with retained in vitro activity (aminoglycosides, polymyxins, and tetracyclines) are limited by suboptimal pharmacokinetic characteristics, emergence of resistance, and/or toxicity. Recently developed and US Food and Drug Administration (FDA)-approved β-lactam/β-lactamase inhibitor agents do not provide enhanced activity against CRAB. On balance, cefiderocol and eravacycline demonstrate potent in vitro activity and are well tolerated, but clinical data for patients with CRAB infections do not yet support widespread use. Given that CRAB has the capacity to infect vulnerable patients and preferred regimens have not been identified, we advocate for combination therapy. Our preferred regimen for critically ill patients infected, or considered to be at high risk for CRAB, includes meropenem, polymyxin B, and ampicillin/sulbactam. Importantly, site of infection, severity of illness, and local epidemiology are essential factors to be considered in selecting combination therapies. Molecular mechanisms of resistance may unveil preferred combinations at individual centers; however, such data are often unavailable to treating clinicians and have not been linked to improved clinical outcomes. Combination strategies may also pose an increased risk for antibiotic toxicity and Clostridioides difficile infection, and should therefore be balanced by understanding patient goals of care and underlying health conditions. Promising therapies that are in clinical development and/or under investigation include durlobactam–sulbactam, cefiderocol combination regimens, and bacteriophage therapy, which may over time eliminate the need for the continued use of polymyxins. Future goals for CRAB management include pathogen-focused treatment paradigms that are based on molecular mechanisms of resistance, local susceptibility rates, and the availability of well-tolerated, effective treatment options.

show abstract

Section: Linking Mechanisms Of Resistance To Treatment Optionsmentioning

confidence: 99%

Contemporary Perspective on the Treatment of Acinetobacter baumannii Infections: Insights from the Society of Infectious Diseases Pharmacists

et al. 2021

View full text Add to dashboard Cite

show abstract

“…In a PK study of critically ill patients receiving minocycline 200 mg IV q12 h, critical ƒ AUC:MIC targets in plasma associated with stasis ( f AUC/MIC of 12) was achieved for isolates with MICs ≤1 mg/L and 1‐log killing ( f AUC/MIC of 18) was only achieved at MICs ≤0.5 mg/L. Like tigecycline, PTA varied as a function of the patients’ baseline albumin 85 …”

Section: Pharmacodynamic Probability Of Target Attainment Studiesmentioning

confidence: 99%

Treatment of patients with serious infections due to carbapenem‐resistant Acinetobacter baumannii: How viable are the current options?

2021

Self Cite

View full text Add to dashboard Cite

This review critically appraises the published microbiologic and clinical data on the treatment of patients with carbapenem‐resistant Acinetobacter baumannii infections. Despite being recognized as an urgent threat pathogen by the CDC and WHO, optimal treatment of patients with serious CRAB infections remains ill‐defined. Few commercially available agents exhibit reliable in vitro activity against CRAB. Historically, polymyxins have been the most active agents in vitro, though interpretations of susceptibility data are difficult given issues surrounding MIC testing methodologies and lack of correlation between MICs and clinical outcomes. Most available preclinical and clinical data involve use of polymyxins, tetracyclines, and sulbactam, alone and in combination. As the number of viable treatment options is limited, combination therapy with a polymyxin is often used for patients with CRAB infections, despite the significant risk of nephrotoxicity. However, no treatment regimen has been found to reduce mortality, which exceeds 40% across most studies, or substantially improve clinical response. While some newer agents, such as eravacycline and cefiderocol, have demonstrated in vitro activity, clinical efficacy has not been fully established. New agents with clinically relevant activity against CRAB isolates and favorable toxicity profiles are sorely needed.

show abstract

“…However, increased risk of hypoglycemia in non-diabetic patients can induce cerebral damage. 36 , 49 The intravenous formulation of glibenclamide (BIIB093) facilitates rapid supra-therapeutic levels and stable maintenance of desired plasma levels of the drug. 42 …”

Section: Acute Intervention Targets For Attenuating Secondary Injury After Ichmentioning

confidence: 99%

“…The overall conclusions from both PK models suggest that current intravenous dosing of minocycline used in the intensive care unit might provide only suboptimal dosing and microbiological efficacy, and the higher intravenous minocycline doses used in critically ill patients with infections will require a detailed risk versus benefit assessment for toxicities related to potential kidney damage. 49 …”

Section: Acute Intervention Targets For Attenuating Secondary Injury After Ichmentioning

confidence: 99%

Secondary mechanisms of injury and viable pathophysiological targets in intracerebral hemorrhage

Bautista

Adelson

Bicher

et al. 2021

Ther Adv Neurol Disord

View full text Add to dashboard Cite

Intracerebral hemorrhage (ICH) can be divided into a primary and secondary phase. In the primary phase, hematoma volume is evaluated and therapies are focused on reducing hematoma expansion. In the secondary, neuroprotective phase, complex systemic inflammatory cascades, direct cellular toxicity, and blood-brain barrier disruption can result in worsening perihematomal edema that can adversely affect functional outcome. To date, all major randomized phase 3 trials for ICH have targeted primary phase hematoma volume and incorporated clot evacuation, intensive blood pressure control, and hemostasis. Reasons for this lack of clinical efficacy in the major ICH trials may be due to the lack of therapeutics involving mitigation of secondary injury and inflexible trial design that favors unilateral mechanisms in a complex pathophysiology. Potential pathophysiological targets for attenuating secondary injury are highlighted in this review and include therapies increasing calcium, antagonizing microglial activation, maintaining macrophage M1 versus M2 balance by decreasing M1 signaling, aquaporin inhibition, NKCCl inhibition, endothelin receptor inhibition, Sur1-TRPM4 inhibition, matrix metalloproteinase inhibition, and sphingosine-1-phosphate receptor modulation. Future clinical trials in ICH focusing on secondary phase injury and, potentially implementing adaptive trial design approaches with multifocal targets, may improve insight into these mechanisms and provide potential therapies that may improve survival and functional outcome.

show abstract

Pharmacokinetic and Pharmacodynamic Profiling of Minocycline for Injection following a Single Infusion in Critically Ill Adults in a Phase IV Open-Label Multicenter Study (ACUMIN)

Cited by 24 publications

References 30 publications

Contemporary Perspective on the Treatment of Acinetobacter baumannii Infections: Insights from the Society of Infectious Diseases Pharmacists

Contemporary Perspective on the Treatment of Acinetobacter baumannii Infections: Insights from the Society of Infectious Diseases Pharmacists

Treatment of patients with serious infections due to carbapenem‐resistant Acinetobacter baumannii: How viable are the current options?

Secondary mechanisms of injury and viable pathophysiological targets in intracerebral hemorrhage

Contact Info

Product

Resources

About