Literature DB >> 31970713

Omadacycline: A Novel Oral and Intravenous Aminomethylcycline Antibiotic Agent.

George G Zhanel1,2, Jenine Esquivel3, Sheryl Zelenitsky3, Courtney K Lawrence3, Heather J Adam4,5, Alyssa Golden4, Rachel Hink4, Liam Berry6, Frank Schweizer4,6, Michael A Zhanel4, Denice Bay4, Philippe R S Lagacé-Wiens4,5, Andrew J Walkty4,5, Joseph P Lynch7, James A Karlowsky4,5.   

Abstract

Omadacycline is a novel aminomethylcycline antibiotic developed as a once-daily, intravenous and oral treatment for acute bacterial skin and skin structure infection (ABSSSI) and community-acquired bacterial pneumonia (CABP). Omadacycline, a derivative of minocycline, has a chemical structure similar to tigecycline with an alkylaminomethyl group replacing the glycylamido group at the C-9 position of the D-ring of the tetracycline core. Similar to other tetracyclines, omadacycline inhibits bacterial protein synthesis by binding to the 30S ribosomal subunit. Omadacycline possesses broad-spectrum antibacterial activity against Gram-positive and Gram-negative aerobic, anaerobic, and atypical bacteria. Omadacycline remains active against bacterial isolates possessing common tetracycline resistance mechanisms such as efflux pumps (e.g., TetK) and ribosomal protection proteins (e.g., TetM) as well as in the presence of resistance mechanisms to other antibiotic classes. The pharmacokinetics of omadacycline are best described by a linear, three-compartment model following a zero-order intravenous infusion or first-order oral administration with transit compartments to account for delayed absorption. Omadacycline has a volume of distribution (Vd) ranging from 190 to 204 L, a terminal elimination half-life (t½) of 13.5-17.1 h, total clearance (CLT) of 8.8-10.6 L/h, and protein binding of 21.3% in healthy subjects. Oral bioavailability of omadacycline is estimated to be 34.5%. A single oral dose of 300 mg (bioequivalent to 100 mg IV) of omadacycline administered to fasted subjects achieved a maximum plasma concentration (Cmax) of 0.5-0.6 mg/L and an area under the plasma concentration-time curve from 0 to infinity (AUC0-∞) of 9.6-11.9 mg h/L. The free plasma area under concentration-time curve divided by the minimum inhibitory concentration (i.e., fAUC24h/MIC), has been established as the pharmacodynamic parameter predictive of omadacycline antibacterial efficacy. Several animal models including neutropenic murine lung infection, thigh infection, and intraperitoneal challenge model have documented the in vivo antibacterial efficacy of omadacycline. A phase II clinical trial on complicated skin and skin structure infection (cSSSI) and three phase III clinical trials on ABSSSI and CABP demonstrated the safety and efficacy of omadacycline. The phase III trials, OASIS-1 (ABSSSI), OASIS-2 (ABSSSI), and OPTIC (CABP), established non-inferiority of omadacycline to linezolid (OASIS-1, OASIS-2) and moxifloxacin (OPTIC), respectively. Omadacycline is currently approved by the FDA for use in treatment of ABSSSI and CABP. Phase II clinical trials involving patients with acute cystitis and acute pyelonephritis are in progress. Mild, transient gastrointestinal events are the predominant adverse effects associated with use of omadacycline. Based on clinical trial data to date, the adverse effect profile of omadacycline is similar to studied comparators, linezolid and moxifloxacin. Unlike tigecycline and eravacycline, omadacycline has an oral formulation that allows for step-down therapy from the intravenous formulation, potentially facilitating earlier hospital discharge, outpatient therapy, and cost savings. Omadacycline has a potential role as part of an antimicrobial stewardship program in the treatment of patients with infections caused by antibiotic-resistant and multidrug-resistant Gram-positive [including methicillin-resistant Staphylococcus aureus (MRSA)] and Gram-negative pathogens.

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Year:  2020        PMID: 31970713     DOI: 10.1007/s40265-020-01257-4

Source DB:  PubMed          Journal:  Drugs        ISSN: 0012-6667            Impact factor:   9.546


  52 in total

Review 1.  The history of the tetracyclines.

Authors:  Mark L Nelson; Stuart B Levy
Journal:  Ann N Y Acad Sci       Date:  2011-12       Impact factor: 5.691

2.  In Vivo Pharmacodynamic Evaluation of Omadacycline (PTK 0796) against Streptococcus pneumoniae in the Murine Pneumonia Model.

Authors:  Alexander J Lepak; Miao Zhao; Karen Marchillo; Jamie VanHecker; David R Andes
Journal:  Antimicrob Agents Chemother       Date:  2017-04-24       Impact factor: 5.191

3.  Clinical disposition, metabolism and in vitro drug-drug interaction properties of omadacycline.

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Journal:  Xenobiotica       Date:  2016-08-08       Impact factor: 1.908

4.  The in vitro evaluation of tigecycline tested against pathogens isolated in eight countries in the Asia-Western Pacific region (2008).

Authors:  David J Farrell; John D Turnidge; Jan Bell; Helio S Sader; Ronald N Jones
Journal:  J Infect       Date:  2010-03-31       Impact factor: 6.072

5.  In vitro activity of tigecycline alone and antimicrobial combinations against clinical Neisseria gonorrhoeae isolates.

Authors:  Hyukmin Lee; Hyunsoo Kim; Young Hee Seo; Dongeun Yong; Seok Hoon Jeong; Kyungwon Lee; Younsop Chong
Journal:  Diagn Microbiol Infect Dis       Date:  2016-10-25       Impact factor: 2.803

6.  A randomized, evaluator-blind, phase 2 study comparing the safety and efficacy of omadacycline to those of linezolid for treatment of complicated skin and skin structure infections.

Authors:  Gary J Noel; Michael P Draper; Howard Hait; S Ken Tanaka; Robert D Arbeit
Journal:  Antimicrob Agents Chemother       Date:  2012-08-20       Impact factor: 5.191

Review 7.  The glycylcyclines: a comparative review with the tetracyclines.

Authors:  George G Zhanel; Kristen Homenuik; Kim Nichol; Ayman Noreddin; Lavern Vercaigne; John Embil; Alfred Gin; James A Karlowsky; Daryl J Hoban
Journal:  Drugs       Date:  2004       Impact factor: 9.546

8.  Safety and Pharmacokinetics of the Aminomethylcycline Antibiotic Omadacycline Administered to Healthy Subjects in Oral Multiple-Dose Regimens.

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Journal:  Antimicrob Agents Chemother       Date:  2018-01-25       Impact factor: 5.191

9.  Structure-activity relationship of the aminomethylcyclines and the discovery of omadacycline.

Authors:  Laura Honeyman; Mohamed Ismail; Mark L Nelson; Beena Bhatia; Todd E Bowser; Jackson Chen; Rachid Mechiche; Kwasi Ohemeng; Atul K Verma; E Pat Cannon; Ann Macone; S Ken Tanaka; Stuart Levy
Journal:  Antimicrob Agents Chemother       Date:  2015-09-08       Impact factor: 5.191

10.  The Novel Aminomethylcycline Omadacycline Has High Specificity for the Primary Tetracycline-Binding Site on the Bacterial Ribosome.

Authors:  Corina G Heidrich; Sanya Mitova; Andreas Schedlbauer; Sean R Connell; Paola Fucini; Judith N Steenbergen; Christian Berens
Journal:  Antibiotics (Basel)       Date:  2016-09-22
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  17 in total

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4.  Potency of Omadacycline against Mycobacteroides abscessus Clinical Isolates In Vitro and in a Mouse Model of Pulmonary Infection.

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5.  In Vitro Activity of Omadacycline and Five Comparators against Contemporary Ribotypes of Clostridioides difficile in Stockholm, Sweden.

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6.  Efficacy of Omadacycline against Multidrug-Resistant Enterococcus faecium Strains in a Mouse Peritonitis Model.

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Review 7.  Treatment for carbapenem-resistant Enterobacterales infections: recent advances and future directions.

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Review 8.  Multidrug Resistance (MDR) and Collateral Sensitivity in Bacteria, with Special Attention to Genetic and Evolutionary Aspects and to the Perspectives of Antimicrobial Peptides-A Review.

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Review 9.  Present and Future Perspectives on Therapeutic Options for Carbapenemase-Producing Enterobacterales Infections.

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Review 10.  The Development of Third-Generation Tetracycline Antibiotics and New Perspectives.

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