Effect of physicochemical properties on the pharmacokinetic parameters of the new representative of benzothiazinones antituberculosis drug macozinonе

Abstract: Introduction.Tuberculosis (TB) is one of the top ten causes of death worldwide. Improvement of the treatment options via development of new drugs and treatment regimens that would be more convenient for patients is one of key options of improving the effecacy of the TB prevention and careis. Since the creation of new treatment regimens by minimizing the number of the drugs used and reducing the duration of treatment is the most promising and correct direction, macozinone, a new candidate of the benzothiazinone… Show more

“…The pharmacokinetics (PK) of macozinone immediate-release dispersible tablet for oral suspension in Beagle dogs after a single oral administration of 160 mg supported the primary in vitro findings on the narrow absorption window of the drug, the maximum drug concentration in plasma ( C max ) and the total drug exposure (AUC inf ) in the fed state are 1.8 and 1.3 times, respectively, higher than in the fasted states: absorption is confined to the upper gastrointestinal tract ( 9 ). In addition, macozinone is rapidly eliminated, the mean residence time (MRT last ) was low (3.6 h) and the half-life ( t 1/2 ) was short (3.2 h) ( 9 ). Guo and colleagues ( 10 ) reported low absolute bioavailability of macozinone ( F abs ~10%) in mice after a single oral administration of 12.5 or 25.0 mg/kg.…”

“…The antibacterial potency of benzothiazinone-based molecule derivatives is directly proportional to their lipophilicity ( 4 ), but the high lipophilicity of a drug contributes to its poor water solubility and variable oral bioavailability ( 8 ). Moreover, the water solubility of macozinone strongly depends on the pH level: it highly dissolves in strongly acidic solutions (pH ~1 to 2) and poorly dissolves in moderately acidic solutions (pH ~5 to 6) ( 9 ). In biorelevant media, macozinone is more soluble in fed-state simulated intestinal fluid (FeSSIF) than in fasted-state simulated intestinal fluid (FaSSIF).…”

“…Further, MCZ shows low permeability in the Caco-2 assay (an early drug discovery assay that uses a human colon epithelial cancer cell line as a model for human intestinal absorption of an experimental compound) with an efflux ratio of 0.6 ( 9 ). The pharmacokinetics (PK) of macozinone immediate-release dispersible tablet for oral suspension in Beagle dogs after a single oral administration of 160 mg supported the primary in vitro findings on the narrow absorption window of the drug, the maximum drug concentration in plasma ( C max ) and the total drug exposure (AUC inf ) in the fed state are 1.8 and 1.3 times, respectively, higher than in the fasted states: absorption is confined to the upper gastrointestinal tract ( 9 ). In addition, macozinone is rapidly eliminated, the mean residence time (MRT last ) was low (3.6 h) and the half-life ( t 1/2 ) was short (3.2 h) ( 9 ).…”

“…1 ). According to the Biopharmaceutical Classification System, macozinone is considered a class IV drug owing to its low water solubility and permeability ( 9 ). Hence, MCZ has been proposed as a suitable candidate for a mucoadhesive gastroretentive (or extended-release [ER]) drug delivery system.…”

Antituberculosis Macozinone Extended-Release Tablets To Enhance Bioavailability: a Pilot Pharmacokinetic Study in Beagle Dogs

“…The pharmacokinetics (PK) of macozinone immediate-release dispersible tablet for oral suspension in Beagle dogs after a single oral administration of 160 mg supported the primary in vitro findings on the narrow absorption window of the drug, the maximum drug concentration in plasma ( C max ) and the total drug exposure (AUC inf ) in the fed state are 1.8 and 1.3 times, respectively, higher than in the fasted states: absorption is confined to the upper gastrointestinal tract ( 9 ). In addition, macozinone is rapidly eliminated, the mean residence time (MRT last ) was low (3.6 h) and the half-life ( t 1/2 ) was short (3.2 h) ( 9 ). Guo and colleagues ( 10 ) reported low absolute bioavailability of macozinone ( F abs ~10%) in mice after a single oral administration of 12.5 or 25.0 mg/kg.…”

“…The antibacterial potency of benzothiazinone-based molecule derivatives is directly proportional to their lipophilicity ( 4 ), but the high lipophilicity of a drug contributes to its poor water solubility and variable oral bioavailability ( 8 ). Moreover, the water solubility of macozinone strongly depends on the pH level: it highly dissolves in strongly acidic solutions (pH ~1 to 2) and poorly dissolves in moderately acidic solutions (pH ~5 to 6) ( 9 ). In biorelevant media, macozinone is more soluble in fed-state simulated intestinal fluid (FeSSIF) than in fasted-state simulated intestinal fluid (FaSSIF).…”

“…Further, MCZ shows low permeability in the Caco-2 assay (an early drug discovery assay that uses a human colon epithelial cancer cell line as a model for human intestinal absorption of an experimental compound) with an efflux ratio of 0.6 ( 9 ). The pharmacokinetics (PK) of macozinone immediate-release dispersible tablet for oral suspension in Beagle dogs after a single oral administration of 160 mg supported the primary in vitro findings on the narrow absorption window of the drug, the maximum drug concentration in plasma ( C max ) and the total drug exposure (AUC inf ) in the fed state are 1.8 and 1.3 times, respectively, higher than in the fasted states: absorption is confined to the upper gastrointestinal tract ( 9 ). In addition, macozinone is rapidly eliminated, the mean residence time (MRT last ) was low (3.6 h) and the half-life ( t 1/2 ) was short (3.2 h) ( 9 ).…”

“…1 ). According to the Biopharmaceutical Classification System, macozinone is considered a class IV drug owing to its low water solubility and permeability ( 9 ). Hence, MCZ has been proposed as a suitable candidate for a mucoadhesive gastroretentive (or extended-release [ER]) drug delivery system.…”

Antituberculosis Macozinone Extended-Release Tablets To Enhance Bioavailability: a Pilot Pharmacokinetic Study in Beagle Dogs

“…PBTZ169 has successfully passed preclinical safety, toxicology and pharmacokinetic [26] assessments, and ascending dose Phase I and Phase II trials taking place both in Russia [27] , and in Switzerland (study name: IM-006–11 and IM-006–13, ClinicalTrials.gov identifier: NCT03776500 and NCT03423030). An analytical method by tandem mass spectrometry was developed by our group for the quantification of macozinone and five active metabolites in plasma samples collected during the first pharmacokinetic studies performed at the Lausanne Hospital Center [28] .…”

Optimized LC-MS/MS quantification of tuberculosis drug candidate macozinone (PBTZ169), its dearomatized Meisenheimer Complex and other metabolites, in human plasma and urine

Synthesis, structures, reactivity and medicinal chemistry of antitubercular benzothiazinones