ABSTRACT
The metabolism of lufotrelvir, a novel phosphate prodrug of PF-00835231 for the treatment of COVID-19, was evaluated in healthy human volunteers and clinical trial participants with COVID-19 following intravenous infusion. The prodrug was completely converted to PF-00835231 that was subsequently cleared by hydrolysis, hydroxylation, ketoreduction, epimerization, renal clearance, and secretion into the feces. The main circulating metabolite was a hydrolysis product (M7) that was present at concentrations greater than PF-00835231, and this was consistent between healthy volunteers and participants with COVID-19. On administration of [14C]lufotrelvir, only 63% of the dose was obtained in excreta over 10 days and total drug-related material demonstrated a prolonged terminal phase half-life in plasma. A considerable portion of the labeled material was unextractable from fecal homogenate and plasma. The position of the carbon-14 atom in the labeled material was at a leucine carbonyl, and pronase digestion of the pellet derived from extraction of the fecal homogenate showed that [14C]leucine was released. SIGNIFICANCE STATEMENT: Lufotrelvir is an experimental phosphate prodrug intravenous therapy investigated for the potential treatment of COVID-19 in a hospital setting. The overall metabolism of lufotrelvir was determined in human healthy volunteers and clinical trial participants with COVID-19. Conversion of the phosphate prodrug to the active drug PF-00835231 was complete and the subsequent metabolic clearance of the active drug was largely via amide bond hydrolysis. Substantial drug-related material was not recovered due to loss of the carbon-14 label to endogenous metabolism.
Subject(s)
COVID-19 , Prodrugs , Humans , Carbon Radioisotopes/analysis , Infusions, Intravenous , RNA, Viral/analysis , Leucine , SARS-CoV-2 , Administration, Intravenous , Phosphates , Feces/chemistryABSTRACT
COVID-19 caused by the SARS-CoV-2 virus has become a global pandemic. 3CL protease is a virally encoded protein that is essential across a broad spectrum of coronaviruses with no close human analogs. PF-00835231, a 3CL protease inhibitor, has exhibited potent in vitro antiviral activity against SARS-CoV-2 as a single agent. Here we report, the design and characterization of a phosphate prodrug PF-07304814 to enable the delivery and projected sustained systemic exposure in human of PF-00835231 to inhibit coronavirus family 3CL protease activity with selectivity over human host protease targets. Furthermore, we show that PF-00835231 has additive/synergistic activity in combination with remdesivir. We present the ADME, safety, in vitro, and in vivo antiviral activity data that supports the clinical evaluation of PF-07304814 as a potential COVID-19 treatment.
Subject(s)
COVID-19 Drug Treatment , Coronavirus 3C Proteases/antagonists & inhibitors , Coronavirus Protease Inhibitors/administration & dosage , Indoles/administration & dosage , Leucine/administration & dosage , Pyrrolidinones/administration & dosage , Adenosine Monophosphate/administration & dosage , Adenosine Monophosphate/adverse effects , Adenosine Monophosphate/analogs & derivatives , Adenosine Monophosphate/pharmacokinetics , Alanine/administration & dosage , Alanine/adverse effects , Alanine/analogs & derivatives , Alanine/pharmacokinetics , Animals , COVID-19/virology , Chlorocebus aethiops , Coronavirus 229E, Human/drug effects , Coronavirus 229E, Human/enzymology , Coronavirus Protease Inhibitors/adverse effects , Coronavirus Protease Inhibitors/pharmacokinetics , Disease Models, Animal , Drug Design , Drug Synergism , Drug Therapy, Combination , HeLa Cells , Humans , Indoles/adverse effects , Indoles/pharmacokinetics , Infusions, Intravenous , Leucine/adverse effects , Leucine/pharmacokinetics , Mice , Pyrrolidinones/adverse effects , Pyrrolidinones/pharmacokinetics , Severe acute respiratory syndrome-related coronavirus/drug effects , Severe acute respiratory syndrome-related coronavirus/enzymology , SARS-CoV-2/drug effects , SARS-CoV-2/enzymology , Vero CellsABSTRACT
The atypical chemokine receptor C-X-C chemokine receptor type 7 (CXCR7) is an attractive therapeutic target for a variety of cardiac and immunological diseases. As a strategy to mitigate known risks associated with the development of higher molecular weight, basic compounds, a series of pyrrolidinyl-azolopyrazines were identified as promising small-molecule CXCR7 modulators. Using a highly enabled parallel medicinal chemistry strategy, structure-activity relationship studies geared towards a reduction in lipophilicity and incorporation of saturated heterocycles led to the identification of representative tool compound 20. Notably, compound 20 maintained good potency against CXCR7 with a suitable balance of physicochemical properties to support in vivo pharmacokinetic studies.
Subject(s)
Drug Discovery , Immunologic Factors/chemical synthesis , Immunologic Factors/pharmacology , Receptors, CXCR/antagonists & inhibitors , Animals , Drug Delivery Systems , Drug Design , Immunologic Factors/pharmacokinetics , Male , Mice , Mice, Inbred C57BL , Models, Molecular , Molecular Structure , Signal Transduction , Structure-Activity RelationshipABSTRACT
COVID-19 caused by the SARS-CoV-2 virus has become a global pandemic. 3CL protease is a virally encoded protein that is essential across a broad spectrum of coronaviruses with no close human analogs. The designed phosphate prodrug PF-07304814 is metabolized to PF-00835321 which is a potent inhibitor in vitro of the coronavirus family 3CL pro, with selectivity over human host protease targets. Furthermore, PF-00835231 exhibits potent in vitro antiviral activity against SARS-CoV-2 as a single agent and it is additive/synergistic in combination with remdesivir. We present the ADME, safety, in vitro , and in vivo antiviral activity data that supports the clinical evaluation of this compound as a potential COVID-19 treatment.
ABSTRACT
C-X-C chemokine receptor type 7 (CXCR7) is involved in cardiac and immune pathophysiology. We report the discovery of a novel 1,4-diazepine CXCR7 modulator, demonstrating for the first time the role of pharmacological CXCR7 intervention in cardiac repair. Structure-activity-relationship (SAR) studies demonstrated that a net reduction in lipophilicity (log D) and an incorporation of saturated ring systems yielded compounds with good CXCR7 potencies and improvements in oxidative metabolic stability in human-liver microsomes (HLM). Tethering an ethylene amide further improved the selectivity profile (e.g., for compound 18, CXCR7 Ki = 13 nM, adrenergic α 1a Kb > 10â¯000 nM, and adrenergic ß 2 Kb > 10â¯000 nM). The subcutaneous administration of 18 in mice led to a statistically significant increase in circulating concentrations of plasma stromal-cell-derived factor 1α (SDF-1α) of approximately 2-fold. Chronic dosing of compound 18 in a mouse model of isoproterenol-induced cardiac injury further resulted in a statistically significant reduction of cardiac fibrosis.
Subject(s)
Acetamides/therapeutic use , Azepines/therapeutic use , Cardiotonic Agents/therapeutic use , Fibrosis/drug therapy , Heart Diseases/drug therapy , Receptors, CXCR/metabolism , Acetamides/chemical synthesis , Acetamides/chemistry , Acetamides/pharmacology , Animals , Azepines/chemical synthesis , Azepines/chemistry , Azepines/pharmacology , Cardiotonic Agents/chemical synthesis , Cardiotonic Agents/chemistry , Cardiotonic Agents/pharmacology , Dogs , Fibrosis/chemically induced , Heart Diseases/chemically induced , Humans , Hydrophobic and Hydrophilic Interactions , Isoproterenol , Madin Darby Canine Kidney Cells , Male , Mice, Inbred BALB C , Mice, Inbred C57BL , Microsomes, Liver/metabolism , Molecular Structure , Structure-Activity RelationshipABSTRACT
By use of a structure-based computational method for identification of structurally novel Janus kinase (JAK) inhibitors predicted to bind beyond the ATP binding site, a potent series of indazoles was identified as selective pan-JAK inhibitors with a type 1.5 binding mode. Optimization of the series for potency and increased duration of action commensurate with inhaled or topical delivery resulted in potent pan-JAK inhibitor 2 (PF-06263276), which was advanced into clinical studies.
Subject(s)
Anti-Inflammatory Agents/pharmacology , Heterocyclic Compounds, 2-Ring/pharmacology , Indazoles/pharmacology , Janus Kinases/antagonists & inhibitors , Lung Diseases/drug therapy , Protein Kinase Inhibitors/pharmacology , Skin Diseases/drug therapy , Administration, Cutaneous , Administration, Inhalation , Animals , Anti-Inflammatory Agents/administration & dosage , Anti-Inflammatory Agents/chemical synthesis , Anti-Inflammatory Agents/toxicity , Binding Sites , Crystallography, X-Ray , Dogs , Drug Design , Hepatocytes/metabolism , Heterocyclic Compounds, 2-Ring/administration & dosage , Heterocyclic Compounds, 2-Ring/chemical synthesis , Heterocyclic Compounds, 2-Ring/toxicity , Humans , Indazoles/administration & dosage , Indazoles/chemical synthesis , Indazoles/toxicity , Janus Kinase 1/antagonists & inhibitors , Janus Kinase 2/antagonists & inhibitors , Janus Kinase 3/antagonists & inhibitors , Mice, Inbred BALB C , Microsomes, Liver/metabolism , Phosphorylation , Protein Kinase Inhibitors/administration & dosage , Protein Kinase Inhibitors/chemical synthesis , Protein Kinase Inhibitors/toxicity , Rats , SolubilityABSTRACT
A 1,2,4-triazole motif was employed as a bioisostere for the ester commonly used in muscarinic antagonists, and subsequent integrative conjugation to a ß2 agonist quinolinone furnished a new class of bifunctional MABAs for the treatment of COPD. Medicinal chemistry optimization using the principles of 'inhalation by design' furnished a clinical candidate with desirable pharmacological, pharmacokinetic and biopharmaceutical properties.
Subject(s)
Adrenergic beta-2 Receptor Agonists/chemical synthesis , Bronchodilator Agents/chemical synthesis , Muscarinic Antagonists/chemical synthesis , Pulmonary Disease, Chronic Obstructive/drug therapy , Triazoles/chemical synthesis , Adrenergic beta-2 Receptor Agonists/pharmacokinetics , Adrenergic beta-2 Receptor Agonists/pharmacology , Animals , Biological Availability , Bronchoconstriction/drug effects , Bronchodilator Agents/pharmacokinetics , Bronchodilator Agents/pharmacology , CHO Cells , Cricetulus , Dogs , Humans , Ipratropium/pharmacology , Muscarinic Antagonists/pharmacokinetics , Muscarinic Antagonists/pharmacology , Rats , Receptor, Muscarinic M3/antagonists & inhibitors , Salmeterol Xinafoate/pharmacology , Tiotropium Bromide/pharmacology , Triazoles/pharmacokinetics , Triazoles/pharmacologyABSTRACT
PURPOSE: There is demand in applied sport settings to measure recovery briefly and accurately. Research indicates mood disturbance as the strongest psychological predictor of mental and physical recovery. The Brief Assessment of Mood (BAM) is a shortened version of the Profile of Mood States that can be completed in less than 30 s. The purpose of this study was to examine the BAM as a quick measure of mood in relation to recovery status in elite rugby players alongside established physiological markers of recovery. METHOD: Using elite rugby union players (N = 12), this study examined the utility of BAM as an indicator of mental and physical recovery in elite athletes by exploring pattern change in mood disturbance, energy index, power output, cortisol, and testosterone 36 hr before and 12 hr, 36 hr, and 60 hr after a competitive rugby match. RESULTS: Repeated-measures multivariate analysis of variance indicated significant changes in all variables across the 4 time points (p < .05, η(2) range = .20-.48), concurrent with previous study findings. Although visual inspection of the graphs indicated that the pattern of change for mood disturbance and energy index mapped changes in all physiological variables, only a low correlation was observed for power output (r = - .34). CONCLUSIONS: Although BAM scores changed significantly over time in accordance with the hypotheses, further testing is required to confirm the utility of the BAM as a measure of recovery. The results indicate that the BAM could be used as 1 indicator of recovery status alongside other measures.
Subject(s)
Affect/physiology , Athletic Performance/physiology , Athletic Performance/psychology , Hydrocortisone/metabolism , Soccer/physiology , Soccer/psychology , Testosterone/metabolism , Exercise Test , Humans , Male , Saliva/metabolism , Time Factors , Young AdultABSTRACT
No published research has assessed sleep patterns of elite rugby union players following match-play. The present study examined sleep patterns of professional rugby union players, prior and post-match-play, to assess the influence of competition. Twenty-eight male rugby union players (24.4 ± 2.9 years, 103.9 ± 12.2â kg) competed in one of four competitive home matches. Player's sleep behaviours were monitored continuously using an Actiwatch® from two days before the match, until three days post-match. Repeated measures of analysis of variance (ANOVA) showed significant differences across the time points measured for time to bed (F = 26.425, η(2) = 0.495, p < .001), get up time (F = 21.175, η(2) = 0.440, p < .001), time spent in bed (F = 10.669, η(2) = 0.283, p < .001), time asleep (F = 8.752, η(2) = 0.245, p < .001) and percentage of time moving (F = 4.602, η(2) = 0.146 p < .05). Most notable, post hocs revealed a significant increase for time in bed the night before the match (p < .01; 95% CI = 0 : 10-1 : 28â h; 9.7 ± 13.5%) compared with the reference night sleep. Furthermore, time asleep significantly decreased post-match (p < .05; 95% CI = -0:03 to -1:59â h; -19.5 ± 19.8%) compared to two nights pre-match. Across all time points, sleep latency and efficiency for most players were considered abnormal compared to that expected in normal populations. The results demonstrate that sleep that is deprived post-match may have detrimental effects on the recovery process.
Subject(s)
Football/physiology , Sleep/physiology , Actigraphy , Adult , Analysis of Variance , Humans , Male , Recovery of Function/physiology , Time FactorsABSTRACT
AIM: The aim of the present study was to investigate the relationship between maximal aerobic capacity (VO(2max)) and repeated sprint ability (RSA) in a group of professional soccer players. METHODS: Forty-one professional soccer players (age 23 ± 4 yrs, height 180.0 ± 5.3 cm, weight 79.6 ± 5.3 kg) were required to perform tests to assess RSA and VO(2max) on two separate days with at least 48 hr rest between testing sessions. Each player performed a treadmill test to determine their VO(2max) and a test for RSA involving the players completing 6 × 40 m sprints (turn after 20 m) with 20 s active recovery between each sprint. RESULTS: There was a significant negative correlation between body mass normalised VO(2max) and mean sprint time (RSAmean) (r = -0.655; P < 0.01) and total sprint time (RSAtotal) (r = -0.591, P < 0.01). CONCLUSION: Results of the current study indicate that VO(2max) is one important factor aiding soccer players in the recovery from repeated sprint type activities.
Subject(s)
Athletic Performance/physiology , Soccer , Adult , Exercise Test , Humans , Oxygen Consumption , Time Factors , Young AdultABSTRACT
Prediction of pharmacokinetic (PK) profile for inhaled drugs in humans provides valuable information to aid toxicology safety assessment, evaluate the potential for systemic accumulation on multiple dosing and enable an estimate for the clinical plasma assay requirements. The accuracy in prediction of inhaled human PK profiles for seven inhaled drugs or drug candidates (salmeterol, salbutamol, formoterol, fluticasone propionate, budesonide, CP-325366 and UK-432097) was assessed using rat oratracheal solution and dry powder PK data. The prediction methodology incorporates allometric scaling and mean residence time (MRT) principles with a two compartmental PK approach. Across the range of compounds tested, the prediction of human inhaled maximum concentration (C(max)) and MRT was within 2-fold for 5 of the 7 compounds, providing an accuracy of prediction similar to the current methodologies used to predict human oral C(max) from preclinical data ( De Buck et al. 2007 ). Administering as a dry powder formulation slowed the rat lung absorption rate of the least soluble compound (fluticasone propionate), impacting the prediction of C(max) and MRT. This flags the potential for preclinical studies with dry powder formulations to positively influence predictive accuracy, although further studies with low solubility inhaled drugs are required to confirm this. This study illustrates the value of preclinical assessment of PKs following administration to the lung, and provides a viable means of predicting the human PK profile for inhaled drugs.
Subject(s)
Bronchodilator Agents/pharmacokinetics , Adenosine/administration & dosage , Adenosine/analogs & derivatives , Adenosine/blood , Adenosine/pharmacokinetics , Administration, Inhalation , Albuterol/administration & dosage , Albuterol/analogs & derivatives , Albuterol/blood , Albuterol/pharmacokinetics , Androstadienes/administration & dosage , Androstadienes/blood , Androstadienes/pharmacokinetics , Animals , Biostatistics , Bronchodilator Agents/administration & dosage , Bronchodilator Agents/blood , Budesonide/administration & dosage , Budesonide/blood , Budesonide/pharmacokinetics , Ethanolamines/administration & dosage , Ethanolamines/blood , Ethanolamines/pharmacokinetics , Fluticasone , Formoterol Fumarate , Humans , Male , Pharmacokinetics , Rats , Salmeterol XinafoateABSTRACT
The increasing use of poorly-soluble inhaled dry powder pharmaceuticals means that animal toxicology studies of these drugs frequently produce lung changes related to the physical presence of undissolved particulate material within the alveolar spaces. These changes are independent of any chemically- or pharmacologically-mediated toxicity and present a challenge to drug developers and regulators in that risk depends on the retained lung burden of undissolved drug material, rather than the delivered dose, systemic exposure or duration of dosing as traditionally used in risk assessment for inhaled compounds. The methodology presented uses basic pharmacokinetic principles to estimate lung particulate burdens achieved in rat inhalation toxicity studies for four inhaled compounds which have reached clinical evaluation. The estimated lung particulate burdens and associated histopathological findings were compared with published thresholds for similar effects caused by inert particulates such as titanium dioxide. Results of the analysis illustrate that regardless of the duration of the study, estimated lung burdens in excess of â¼1 mg drug per g lung were associated with adverse changes consistent with those described in the literature for inert insoluble particles. For all low solubility inhaled pharmaceuticals so far examined, the calculated steady-state retained lung burden of drug in humans is several orders of magnitude lower than that associated with adverse effects in human or animals.
Subject(s)
Lung/metabolism , Particulate Matter/pharmacokinetics , Pharmaceutical Preparations/metabolism , Administration, Inhalation , Animals , Biostatistics , Clinical Trials as Topic , Drug-Related Side Effects and Adverse Reactions/metabolism , Humans , Lung/drug effects , Models, Biological , Models, Chemical , Particle Size , Particulate Matter/toxicity , Pharmaceutical Preparations/administration & dosage , Rats , Risk Assessment , Titanium/adverse effects , Titanium/pharmacokinetics , Titanium/toxicityABSTRACT
We describe the development of novel benzimidazoles as small molecule histamine H4 receptor (H4R) antagonists and their profiling in rat early toxicity studies. The discovery and optimisation of a second series of pyrimidine based antagonists is then described culminating in the identification of the clinical development candidate 13 (PF-3893787). The pre-clinical profile of 13 (PF-3893787) is presented including the development of a translatable biomarker. Our pragmatic approach to target selection, safety assessment, and testing for efficacy faced numerous challenges and we share a number of lessons which the team learned and which will assist us and others in future drug discovery projects.
Subject(s)
Drug Discovery , Histamine Antagonists/chemistry , Histamine Antagonists/pharmacology , Pyrimidines/chemistry , Pyrimidines/pharmacology , Pyrrolidines/chemistry , Pyrrolidines/pharmacology , Receptors, G-Protein-Coupled/drug effects , Receptors, Histamine/drug effects , Animals , Drug Evaluation, Preclinical , Humans , Rats , Receptors, Histamine H4ABSTRACT
We describe the identification of a potent, selective lead series that shows antagonism against the human histamine H4 receptor from thirteen actives identified in an HTS as part of a hit to lead program. By focusing on ligand efficiency and concurrently using a diversity based approach, compounds based around 2,4-diaminopyrimidine were identified with compound 25 being quickly shown to be a good lead. It also had the highest ligand efficiency in the series.
Subject(s)
Histamine Antagonists/chemistry , Histamine Antagonists/pharmacology , Receptors, G-Protein-Coupled/antagonists & inhibitors , Small Molecule Libraries , Humans , Ligands , Receptors, Histamine , Receptors, Histamine H4 , Stereoisomerism , Structure-Activity RelationshipABSTRACT
In this Letter we present data for a novel series of ICS for the treatment of asthma. 'Inhalation by design' principles have been applied to a series of highly potent steroidal GR agonists, with a focus on optimising the potential therapeutic index in human. Pharmacokinetic properties were tuned with high intrinsic clearance and low oral bioavailability in mind, to minimise systemic exposure and reduce systemically driven adverse events. High CYP mediated clearance as well as glucuronidation were targeted to achieve high intrinsic clearance coupled with multiple routes of clearance to minimise drug-drug interactions. Furthermore, pharmaceutical properties such as stability, crystallinity and solubility were considered to ensure compatibility with a dry powder inhaler. This work culminated in the identification of the clinical candidate 15, which demonstrates preclinically the desired efficacy and safety profiles confirming its potential as an inhaled agent for the treatment of asthma.
Subject(s)
Adrenal Cortex Hormones/chemical synthesis , Adrenal Cortex Hormones/pharmacokinetics , Anti-Asthmatic Agents/chemical synthesis , Anti-Asthmatic Agents/pharmacokinetics , Asthma/drug therapy , Drug Design , Administration, Inhalation , Adrenal Cortex Hormones/administration & dosage , Adrenal Cortex Hormones/pharmacology , Adrenergic beta-Agonists/administration & dosage , Adrenergic beta-Agonists/therapeutic use , Androstadienes/chemistry , Androstadienes/pharmacology , Animals , Anti-Asthmatic Agents/administration & dosage , Anti-Asthmatic Agents/pharmacology , Asthma/epidemiology , Asthma/physiopathology , Delayed-Action Preparations , Dose-Response Relationship, Drug , Drug Evaluation, Preclinical , Drug Therapy, Combination , Dry Powder Inhalers , Fluticasone , Hepatocytes , Humans , Liver , Lung , Microsomes, Liver , Neutrophils/metabolism , Randomized Controlled Trials as Topic , Rats , Tumor Necrosis Factor-alpha/biosynthesis , Tumor Necrosis Factor-alpha/bloodABSTRACT
Preventing entry of HIV into human host cells has emerged as an attractive approach to controlling viral replication. Maraviroc 1 is an approved antagonist of the human CCR5 receptor which prevents the entry of HIV. Herein, we report the design and discovery of a series of imidazopiperidine CCR5 antagonists which retain the attractive antiviral profile and window over hERG activity of maraviroc 1, combined with improved absorption profiles in rat and dog. Furthermore, this series of compounds has been shown to retain activity against a laboratory generated maraviroc-resistant HIV-1 strain, which indicates an alternative resistance profile to that of maraviroc 1. Compound 41f (PF-232798) was selected as a clinical candidate from the imidazopiperidine series and is currently in phase II clinical trials.
Subject(s)
Anti-HIV Agents/chemical synthesis , Azabicyclo Compounds/chemical synthesis , CCR5 Receptor Antagonists , HIV-1/drug effects , Imidazoles/chemical synthesis , Animals , Anti-HIV Agents/chemistry , Anti-HIV Agents/pharmacology , Azabicyclo Compounds/chemistry , Azabicyclo Compounds/pharmacology , Cell Line , Cricetinae , Cyclohexanes/pharmacology , Dogs , Drug Resistance, Viral , ERG1 Potassium Channel , Ether-A-Go-Go Potassium Channels/metabolism , HIV-1/isolation & purification , Humans , Imidazoles/chemistry , Imidazoles/pharmacology , Leukocytes, Mononuclear/drug effects , Leukocytes, Mononuclear/virology , Maraviroc , Models, Molecular , Protein Binding , Rats , Stereoisomerism , Structure-Activity Relationship , Triazoles/pharmacology , TropanesABSTRACT
This paper describes the successful design and development of dual pharmacology ß-2 agonists-M3 antagonists, for the treatment of chronic obstructive pulmonary disorder using the principles of 'inhalation by design'. A key feature of this work is the combination of balanced potency and pharmacodynamic duration with desirable pharmacokinetic and material properties, whilst keeping synthetic complexity to a minimum.
Subject(s)
Adrenergic beta-2 Receptor Agonists , Drug Design , Muscarinic Antagonists , Pulmonary Disease, Chronic Obstructive/drug therapy , Administration, Inhalation , Adrenergic beta-2 Receptor Agonists/administration & dosage , Animals , Benzhydryl Compounds/administration & dosage , Cresols/administration & dosage , Drug Therapy, Combination , Guinea Pigs , Molecular Structure , Muscarinic Antagonists/administration & dosage , Phenylpropanolamine/administration & dosage , Tolterodine TartrateABSTRACT
A novel series of potent and selective sulfonamide derived ß(2)-adrenoreceptor agonists are described that exhibit potential as inhaled ultra-long-acting bronchodilators for the treatment of asthma and chronic obstructive pulmonary disease. Analogues from this series mediate very long-lasting smooth muscle relaxation in guinea pig tracheal strips. The sulfonamide agonist headgroup confers high levels of intrinsic crystallinity that could relate to the acidic sulfonamide motif supporting a zwitterionic form in the solid state. Optimization of pharmacokinetic properties was achieved through targeted introduction of a phenolic moiety to support rapid phase II clearance, thereby minimizing systemic exposure following inhalation and reducing systemically mediated adverse events. Compound 38 (PF-610355) is identified as a clinical candidate from this series, with in vivo duration of action studies confirming its potential for once-daily use in humans. Compound 38 is currently in advanced phase II clinical studies.
Subject(s)
Adrenergic beta-2 Receptor Agonists , Adrenergic beta-Agonists/chemical synthesis , Asthma/drug therapy , Benzeneacetamides/chemical synthesis , Pulmonary Disease, Chronic Obstructive/drug therapy , Sulfonamides/chemical synthesis , Administration, Inhalation , Adrenergic beta-Agonists/pharmacokinetics , Adrenergic beta-Agonists/pharmacology , Animals , Benzeneacetamides/pharmacokinetics , Benzeneacetamides/pharmacology , Bronchoconstriction/drug effects , CHO Cells , Cricetinae , Cricetulus , Crystallography, X-Ray , Dogs , Female , Guinea Pigs , Hepatocytes/metabolism , Humans , In Vitro Techniques , Liver/metabolism , Male , Microsomes, Liver/drug effects , Microsomes, Liver/metabolism , Models, Molecular , Molecular Structure , Muscle, Smooth/drug effects , Muscle, Smooth/physiopathology , Rats , Stereoisomerism , Sulfonamides/pharmacokinetics , Sulfonamides/pharmacology , Trachea/drug effects , Trachea/metabolism , Trachea/physiopathologyABSTRACT
COPD is a major cause of mortality in the western world. A(2A) agonists are postulated to reduce the lung inflammation that causes COPD. The cardiovascular effects of A(2A) agonists dictate that a compound needs to be delivered by inhalation to be therapeutically useful. A strategy of minimizing side-effect liability by maximizing systemic clearance was followed and pharmacological and pharmacokinetic SAR of a series of inhaled A(2A) agonists described. A sevenfold improvement in potency and 150-fold reduction in side-effect liability over the lead compound CGS-21680, were obtained.
Subject(s)
Adenosine A2 Receptor Agonists , Adenosine/analogs & derivatives , Pulmonary Disease, Chronic Obstructive/drug therapy , Adenosine/pharmacokinetics , Adenosine/pharmacology , Administration, Inhalation , Administration, Oral , Amines/pharmacokinetics , Amines/pharmacology , Animals , Guinea Pigs , Humans , Lung/metabolism , Phenethylamines/pharmacokinetics , Phenethylamines/pharmacology , Pulmonary Disease, Chronic Obstructive/metabolism , Rats , Structure-Activity RelationshipABSTRACT
The sulfonamide group is widely used in medicinal chemistry and appears in many marketed drugs in a variety of forms. One class of drugs that contain this group has been termed the 'sulfonamide antibacterials'. These compounds are inhibitors of tetrahydropteroic acid synthetase. Sulfonamide antibacterials are derivatives of 4-aminobenzenesulfonamide, in which the sulfonamide moiety acts as an isostere of the carboxylic acid group of the natural substrate 4-aminobenzoic acid. The 4-amino group is essential for activity in this class of compounds. These drugs, however, can cause hypersensitivity and severe skin rash, toxicities which are now associated with the presence of the aniline structure (4-amino), although, historically, the class affect was referred to as 'sulfa allergy'. This class effect has also been wrongly associated with other sulfonamide-containing drugs in a number of cases, and has led to warnings and labels that are not scientifically correct. This review explains how this confusion arose and illustrates the scientific evidence indicating that the sulfonamide group is an essential and safe part of the medicinal chemist's arsenal.
