ABSTRACT
Oxidative stress is a key concept in basic, translational, and clinical research to understand the pathophysiology of various disorders, including cardiovascular and renal diseases. Although attempts to directly reduce oxidative stress with redox-active substances have until now largely failed to prove clinical benefit, indirect approaches to combat oxidative stress enzymatically have gained further attention as potential therapeutic strategies. The pantetheinase Vanin-1 is expressed on kidney proximal tubular cells, and its reaction product cysteamine is described to negatively affect redox homeostasis by inhibiting the replenishment of cellular antioxidative glutathione stores. Vanin-1-deficient mice were shown to be protected against oxidative stress damage. The aim of this study was to elucidate whether pharmacological inhibition of Vanin-1 protects mice from oxidative stress-related acute or chronic kidney injury as well. By studying renal ischemia-reperfusion injury in Col4α3-/- (Alport syndrome) mice and in vitro hypoxia-reoxygenation in human proximal tubular cells we found that treatment with a selective and potent Vanin-1 inhibitor resulted in ample inhibition of enzymatic activity in vitro and in vivo. However, surrogate parameters of metabolic and redox homeostasis were only partially and insufficiently affected. Consequently, apoptosis and reactive oxygen species level in tubular cells as well as overall kidney function and fibrotic processes were not improved by Vanin-1 inhibition. We thus conclude that Vanin-1 functionality in the context of cardiovascular diseases needs further investigation and the biological relevance of pharmacological Vanin-1 inhibition for the treatment of kidney diseases remains to be proven.
Subject(s)
Acute Kidney Injury/prevention & control , Amidohydrolases/antagonists & inhibitors , Enzyme Inhibitors/pharmacology , Kidney Tubules, Proximal/drug effects , Nephritis, Hereditary/prevention & control , Oxidative Stress/drug effects , Renal Insufficiency, Chronic/prevention & control , Reperfusion Injury/prevention & control , Acute Kidney Injury/enzymology , Acute Kidney Injury/genetics , Acute Kidney Injury/pathology , Amidohydrolases/genetics , Amidohydrolases/metabolism , Animals , Apoptosis/drug effects , Autoantigens/genetics , Autoantigens/metabolism , Cell Line , Collagen Type IV/genetics , Collagen Type IV/metabolism , Disease Models, Animal , Enzyme Inhibitors/pharmacokinetics , Fibrosis , GPI-Linked Proteins/antagonists & inhibitors , GPI-Linked Proteins/genetics , GPI-Linked Proteins/metabolism , Humans , Kidney Tubules, Proximal/enzymology , Kidney Tubules, Proximal/pathology , Male , Mice, Inbred C57BL , Mice, Knockout , Nephritis, Hereditary/enzymology , Nephritis, Hereditary/genetics , Nephritis, Hereditary/pathology , Renal Insufficiency, Chronic/enzymology , Renal Insufficiency, Chronic/genetics , Renal Insufficiency, Chronic/pathology , Reperfusion Injury/enzymology , Reperfusion Injury/genetics , Reperfusion Injury/pathologyABSTRACT
Aberrant activation in fibroblast growth factor signaling has been implicated in the development of various cancers, including squamous cell lung cancer, squamous cell head and neck carcinoma, colorectal and bladder cancer. Thus, fibroblast growth factor receptors (FGFRs) present promising targets for novel cancer therapeutics. Here, we evaluated the activity of a novel pan-FGFR inhibitor, rogaratinib, in biochemical, cellular and in vivo efficacy studies in a variety of preclinical cancer models. In vitro kinase activity assays demonstrate that rogaratinib potently and selectively inhibits the activity of FGFRs 1, 2, 3 and 4. In line with this, rogaratinib reduced proliferation in FGFR-addicted cancer cell lines of various cancer types including lung, breast, colon and bladder cancer. FGFR and ERK phosphorylation interruption by rogaratinib treatment in several FGFR-amplified cell lines suggests that the anti-proliferative effects are mediated by FGFR/ERK pathway inhibition. Furthermore, rogaratinib exhibited strong in vivo efficacy in several cell line- and patient-derived xenograft models characterized by FGFR overexpression. The observed efficacy of rogaratinib strongly correlated with FGFR mRNA expression levels. These promising results warrant further development of rogaratinib and clinical trials are currently ongoing (ClinicalTrials.gov Identifiers: NCT01976741, NCT03410693, NCT03473756).
Subject(s)
Breast Neoplasms/drug therapy , Neoplasms/drug therapy , Piperazines/pharmacology , Pyrroles/pharmacology , Receptors, Fibroblast Growth Factor/antagonists & inhibitors , Thiophenes/pharmacology , Animals , Antineoplastic Agents/pharmacology , Breast Neoplasms/metabolism , Cell Line, Tumor , Colorectal Neoplasms/drug therapy , Colorectal Neoplasms/metabolism , Drug Screening Assays, Antitumor , Female , Human Umbilical Vein Endothelial Cells , Humans , Lung Neoplasms/drug therapy , Lung Neoplasms/metabolism , Mice , Mice, Inbred BALB C , Mice, Nude , Neoplasms/metabolism , Phosphorylation/drug effects , Random Allocation , Rats , Xenograft Model Antitumor AssaysABSTRACT
The A2B adenosine receptor is a G protein-coupled receptor that belongs to the four member family of adenosine receptors: A1, A2A, A2B, A3. While adenosine-mediated A2B receptor signaling attenuates acute inflammation, facilitates tissue adaptation to hypoxia, and induces increased ischemia tolerance under conditions of an acute insult, persistently elevated adenosine levels and A2B receptor signaling are characteristics of a number of chronic disease states. In this report we describe the discovery of certain thienouracils (thieno[2,3-d]pyrimidine-2,4(1H,3H)-diones) as antagonists of the A2B adenosine receptor by high-throughput screening from our corporate substance collection. The structure optimization of the initial screening hits led to BAY-545, an A2B receptor antagonist that was suitable for in vivo testing. The structure optimization work, SAR that was derived from there, as well as the properties of BAY-545 are also described. In vivo efficacy of BAY-545 was demonstrated in two models of lung fibrosis and data is presented.
Subject(s)
Adenosine A2 Receptor Antagonists/chemistry , High-Throughput Screening Assays , Receptor, Adenosine A2B/drug effects , Adenosine/metabolism , Animals , Pulmonary Fibrosis/drug therapy , Signal Transduction , Structure-Activity Relationship , Uracil/analogs & derivativesABSTRACT
Rogaratinib (BAY 1163877) is a highly potent and selective small-molecule pan-fibroblast growth factor receptor (FGFR) inhibitor (FGFR1-4) for oral application currently being investigated in phaseâ 1 clinical trials for the treatment of cancer. In this publication, we report its discovery by deâ novo structure-based design and medicinal chemistry optimization together with its pharmacokinetic profile.
Subject(s)
Drug Discovery , Piperazines/pharmacology , Protein Kinase Inhibitors/pharmacology , Pyrroles/pharmacology , Receptor, Fibroblast Growth Factor, Type 1/antagonists & inhibitors , Small Molecule Libraries/pharmacology , Thiophenes/pharmacology , Humans , Models, Molecular , Molecular Structure , Piperazines/chemistry , Protein Kinase Inhibitors/chemistry , Pyrroles/chemistry , Small Molecule Libraries/chemistry , Thiophenes/chemistryABSTRACT
The first-in-class soluble guanylate cyclase (sGC) stimulator riociguat was recently introduced as a novel treatment option for pulmonary hypertension. Despite its outstanding pharmacological profile, application of riociguat in other cardiovascular indications is limited by its short half-life, necessitating a three times daily dosing regimen. In our efforts to further optimize the compound class, we have uncovered interesting structure-activity relationships and were able to decrease oxidative metabolism significantly. These studies resulting in the discovery of once daily sGC stimulator vericiguat (compound 24, BAY 1021189), currently in phase 3 trials for chronic heart failure, are now reported.
Subject(s)
Heart Failure/drug therapy , Heterocyclic Compounds, 2-Ring/chemistry , Heterocyclic Compounds, 2-Ring/pharmacology , Pyrimidines/chemistry , Pyrimidines/pharmacology , Soluble Guanylyl Cyclase/metabolism , Structure-Activity Relationship , Administration, Intravenous , Administration, Oral , Animals , Blood Pressure/drug effects , Chemistry Techniques, Synthetic , Dogs , Hepatocytes/drug effects , Heterocyclic Compounds, 2-Ring/administration & dosage , Humans , Male , NG-Nitroarginine Methyl Ester/adverse effects , Pyrimidines/administration & dosage , Rats, Transgenic , Rats, Wistar , Soluble Guanylyl Cyclase/geneticsABSTRACT
Human neutrophil elastase (HNE) is a key driver of inflammation in many cardiopulmonary and systemic inflammatory and autoimmune conditions. Overshooting high HNE activity is the consequence of a disrupted protease-antiprotease balance. Accordingly, there has been an intensive search for potent and selective HNE inhibitors with suitable pharmacokinetics that would allowing oral administration in patients. Based on the chemical probe BAY-678 and the clinical candidate BAY 85-8501 we explored further ring topologies along the equator of the parent pyrimidinone lead series. Novel ring systems were annulated in the east, yielding imidazolo-, triazolo-, and tetrazolopyrimidines in order to ensure additional inhibitor-HNE contacts beyond the S1 and the S2 pocket of HNE. The western annulation of pyridazines led to the polar pyrimidopyridazine BAY-8040, which combines excellent potency and selectivity with a promising pharmacokinetic profile. In vivo efficacy with regard to decreasing cardiac remodeling and amelioration of cardiac function was shown in a monocrotaline-induced rat model for pulmonary arterial hypertension. This demonstrated in vivo proof of concept in animals.
Subject(s)
Hypertension, Pulmonary/drug therapy , Leukocyte Elastase/antagonists & inhibitors , Proteinase Inhibitory Proteins, Secretory/chemistry , Proteinase Inhibitory Proteins, Secretory/pharmacology , Pyridazines/chemistry , Pyridazines/pharmacology , Pyrimidines/chemistry , Pyrimidines/pharmacology , Animals , Disease Models, Animal , Dose-Response Relationship, Drug , Humans , Hypertension, Pulmonary/metabolism , Leukocyte Elastase/metabolism , Models, Molecular , Molecular Structure , Proteinase Inhibitory Proteins, Secretory/chemical synthesis , Pyridazines/chemical synthesis , Pyrimidines/chemical synthesis , Rats , Structure-Activity RelationshipABSTRACT
Human neutrophil elastase (HNE) is a key protease for matrix degradation. High HNE activity is observed in inflammatory diseases. Accordingly, HNE is a potential target for the treatment of pulmonary diseases such as chronic obstructive pulmonary disease (COPD), acute lung injury (ALI), acute respiratory distress syndrome (ARDS), bronchiectasis (BE), and pulmonary hypertension (PH). HNE inhibitors should reestablish the protease-anti-protease balance. By means of medicinal chemistry a novel dihydropyrimidinone lead-structure class was identified. Further chemical optimization yielded orally active compounds with favorable pharmacokinetics such as the chemical probe BAY-678. While maintaining outstanding target selectivity, picomolar potency was achieved by locking the bioactive conformation of these inhibitors with a strategically positioned methyl sulfone substituent. An induced-fit binding mode allowed tight interactions with the S2 and S1 pockets of HNE. BAY 85-8501 ((4S)-4-[4-cyano-2-(methylsulfonyl)phenyl]-3,6-dimethyl-2-oxo-1-[3-(trifluoromethyl)phenyl]-1,2,3,4-tetrahydropyrimidine-5-carbonitrile) was shown to be efficacious in a rodent animal model related to ALI. BAY 85-8501 is currently being tested in clinical studies for the treatment of pulmonary diseases.
Subject(s)
Freezing , Leukocyte Elastase/antagonists & inhibitors , Lung Diseases/enzymology , Proteinase Inhibitory Proteins, Secretory/pharmacology , Pyrimidinones/pharmacology , Sulfones/pharmacology , Dose-Response Relationship, Drug , Humans , Leukocyte Elastase/metabolism , Molecular Conformation , Proteinase Inhibitory Proteins, Secretory/chemistry , Pyrimidinones/chemistry , Structure-Activity Relationship , Sulfones/chemistryABSTRACT
AIMS: The purpose of this work was to support the prediction of a potentially effective dose for the CETP-inhibitor, BAY 60-5521, in humans. METHODS: A combination of allometric scaling of the pharmacokinetics of the CETP-inhibitor BAY 60-5521 with pharmacodynamic studies in CETP-transgenic mice and in human plasma with physiologically-based pharmacokinetic (PBPK) modelling was used to support the selection of the first-in-man dose. RESULTS: The PBPK approach predicts a greater extent of distribution for BAY 60-5521 in humans compared with the allometric scaling method as reflected by a larger predicted volume of distribution and longer elimination half-life. The combined approach led to an estimate of a potentially effective dose for BAY 60-5521 of 51 mg in humans. CONCLUSION: The approach described in this paper supported the prediction of a potentially effective dose for the CETP-inhibitor BAY 60-5521 in humans. Confirmation of the dose estimate was obtained in a first-in-man study.
Subject(s)
Cholesterol Ester Transfer Proteins/antagonists & inhibitors , Hydroxyquinolines/administration & dosage , Models, Biological , Animals , Biometry , Dogs , Dose-Response Relationship, Drug , Female , Humans , Hydroxyquinolines/pharmacokinetics , Hydroxyquinolines/pharmacology , Male , Mice , Mice, Transgenic , Rats , Rats, WistarABSTRACT
Low solubility of drug candidates generated in research contributes to their elimination during subsequent development due to insufficient oral bioavailability (BA) of crystalline compound. Therefore, the purpose of the study was to identify critical in vitro solubility and dissolution parameter that would predict critical in vivo dissolution by means of in vitro-in vivo correlation. Thermodynamic solubility and apparent dissolution rate (ADR) were determined using the shake-flask method and mini-flow-through-cell, respectively. Oral BA studies in rats and humans were conducted from drug solution and suspension/tablets. Relative BA was calculated using F(rel) [%]=AUC(suspension)/AUC(solution)*100, representing a measure of in vivo dissolution. Roughly, F(rel) rat >50% translates into F(rel) human of >90%. Both, ADR and log volume to dissolve applied dose (VDAD), when plotted against F(rel) rat, revealed certain threshold levels, (ADR, â¼150-200 µg of compound dissolved under respective assay conditions; VDAD, â¼100-500 ml/kg) which translate into F(rel) in rats of >50%. Thus, assuming that F(rel)>50% in rats is indicative of sufficient in vivo dissolution in humans after oral application, drugs should exhibit a VDAD of â¼100-500 ml/kg or less in aqueous media to avoid insufficient or varying drug absorption.
Subject(s)
Biological Availability , Pharmaceutical Preparations/metabolism , Administration, Oral , Administration, Topical , Adult , Animals , Caco-2 Cells , Chemical Phenomena , Drug Delivery Systems , Humans , Male , Mouth , Particle Size , Permeability , Pharmaceutical Preparations/analysis , Pharmaceutical Preparations/chemistry , Pharmacokinetics , Rats , Rats, Wistar , Solubility , Suspensions , Young AdultABSTRACT
Based on our former development candidate BAY 38-1315, optimization efforts led to the discovery of a novel chemical class of orally active cholesteryl ester transfer protein (CETP) inhibitors. The chromanol derivative 19b is a highly potent CETP inhibitor with favorable pharmacokinetic properties suitable for clinical studies. Chemical process optimization furnished a robust synthesis for a kilogram-scale process.
Subject(s)
Benzopyrans/chemistry , Cholesterol Ester Transfer Proteins/antagonists & inhibitors , Chromans/chemistry , Spiro Compounds/chemistry , Administration, Oral , Animals , Benzopyrans/chemical synthesis , Benzopyrans/pharmacokinetics , Cholesterol Ester Transfer Proteins/metabolism , Cholesterol, HDL/metabolism , Chromans/chemical synthesis , Chromans/pharmacokinetics , Dogs , Humans , Mice , Mice, Transgenic , Rats , Spiro Compounds/chemical synthesis , Spiro Compounds/pharmacokinetics , Structure-Activity RelationshipABSTRACT
Potent and selective adenosine A(1) receptor antagonists were disclosed. SAR and pharmacological profile of selected compounds were discussed.
Subject(s)
Adenosine A1 Receptor Antagonists/chemistry , Pyrazoles/chemistry , Receptor, Adenosine A1/chemistry , Adenosine A1 Receptor Antagonists/chemical synthesis , Adenosine A1 Receptor Antagonists/pharmacokinetics , Animals , Pyrazoles/chemical synthesis , Pyrazoles/pharmacokinetics , Rats , Rats, Wistar , Receptor, Adenosine A1/metabolism , Structure-Activity RelationshipABSTRACT
The design, synthesis and pharmacological properties of a novel class of PPARalpha agonists is described. Compound 2 is a novel, potent and specific glycine amide with oral bioavailability in rodents. The compound is active in vivo and alters plasma lipids in hAPO-A1 transgenic mice after oral administration.
Subject(s)
Glycine/analogs & derivatives , PPAR alpha/agonists , Animals , Biological Availability , Glycine/pharmacokinetics , Glycine/pharmacology , Mice , Mice, Transgenic , Structure-Activity RelationshipABSTRACT
AIMS: Inhibition of phosphodiesterase 5 (PDE5) decreases pulmonary pressure and improves symptoms in patients with pulmonary arterial hypertension. It is unclear however, whether inhibition of PDE5 can prevent myocardial remodelling during right-ventricular pressure overload. METHODS AND RESULTS: Right-ventricular pressure overload was produced in male rats in a pulmonary hypertension model (monocrotaline 60 mg/kg s.c.) or by surgical pulmonary artery banding. PDE5 inhibition using oral sildenafil (50 mg/kg/day in drinking water) or placebo was initiated 14 days after monocrotaline treatment and continued for 14 days until final examination. In the pulmonary artery banding groups, rats were treated with sildenafil (50 mg/kg/day) or placebo for 21 days following surgical pulmonary artery banding. At the final experiments, right-ventricular haemodynamics were measured and remodelling was analysed using histological, biochemical, and gene expression markers. Both monocrotaline and pulmonary artery banding increased right-ventricular systolic pressure to approximately 80 mmHg. In parallel, both interventions induced markers of hypertrophy (upregulation of natriuretic peptides, increase in myocyte diameter) and fibrosis (upregulation of collagen types 1A2 and 3A1) as well as mRNA expression of the tissue inhibitor of matrix metalloproteases 1 and osteopontin in the right ventricle. In monocrotaline model, sildenafil decreased pulmonary pressure, reduced right-ventricular hypertrophy, and prevented fibrosis marker gene upregulation. After pulmonary artery banding, in contrast, sildenafil increased markers of myocardial remodelling and right-ventricular myocyte diameter. CONCLUSION: Sildenafil prevents myocardial remodelling in pulmonary hypertension through an indirect action via right-ventricular unloading.
Subject(s)
Hemodynamics/drug effects , Hypertension, Pulmonary/drug therapy , Hypertrophy, Right Ventricular/prevention & control , Myocardium/enzymology , Phosphodiesterase 5 Inhibitors , Phosphodiesterase Inhibitors/pharmacology , Piperazines/pharmacology , Sulfones/pharmacology , Ventricular Remodeling/drug effects , Administration, Oral , Animals , Blood Pressure/drug effects , Cyclic GMP/blood , Cyclic Nucleotide Phosphodiesterases, Type 5/metabolism , Disease Models, Animal , Fibrillar Collagens/metabolism , Fibrosis , Hypertension, Pulmonary/chemically induced , Hypertension, Pulmonary/enzymology , Hypertension, Pulmonary/physiopathology , Hypertrophy, Right Ventricular/enzymology , Hypertrophy, Right Ventricular/etiology , Hypertrophy, Right Ventricular/physiopathology , Male , Monocrotaline , Myocardium/pathology , Natriuretic Peptides/metabolism , Osteopontin/metabolism , Phosphodiesterase Inhibitors/administration & dosage , Phosphodiesterase Inhibitors/pharmacokinetics , Piperazines/administration & dosage , Piperazines/pharmacokinetics , Pulmonary Artery/surgery , Purines/administration & dosage , Purines/pharmacokinetics , Purines/pharmacology , RNA, Messenger/metabolism , Rats , Rats, Sprague-Dawley , Rats, Wistar , Sildenafil Citrate , Stroke Volume/drug effects , Sulfones/administration & dosage , Sulfones/pharmacokinetics , Time Factors , Tissue Inhibitor of Metalloproteinase-1/metabolism , Ventricular Pressure/drug effectsABSTRACT
Vitronectin receptor (alpha(V)beta(3)) antagonists have been implicated as a possible new treatment of restenosis following balloon angioplasty. In this work we investigate a series of novel arginine mimetic scaffolds leading to new insight of the alpha(V)beta(3)/ligand interaction. Squaric acid amide 10 is a subnanomolar alpha(V)beta(3) antagonist with improved potency on human smooth muscle cell migration.
