ABSTRACT
Elevated levels of receptor tyrosine kinase-like orphan receptor 1 (RORl) expression are observed in multiple hematological and solid tumors, but not in most of the healthy adult tissues, identifying ROR1 as an attractive target for tumor-specific therapy. Herein we will describe the discovery of macrocyclic peptides as binders of the extracellular Cysteine-Rich Domain (CRD) of human ROR1 via mRNA in vitro selection technology using the PDPS platform, followed by exploration of sidechain SAR of parent macrocycle peptides, fluorescently labeled analogs, and a Peptide Drug Conjugate (PDC). The parent macrocyclic peptides represented by Compound 1 and Compound 14 displayed nanomolar cell-based binding to ROR1 and relatively good internalization in 786-O and MDA-MB-231 tumor cell lines. However, these peptides were not observed to induce apoptosis in Mia PaCa-2 cells, a model pancreatic tumor cell line with a relatively low level of cell surface expression of ROR1.
Subject(s)
Peptides, Cyclic , Receptor Tyrosine Kinase-like Orphan Receptors , Adult , Humans , Cell Line, Tumor , Receptor Tyrosine Kinase-like Orphan Receptors/drug effects , Receptor Tyrosine Kinase-like Orphan Receptors/metabolism , Peptides, Cyclic/chemistry , Peptides, Cyclic/pharmacologyABSTRACT
Lead optimization of the diphenylpyridylethanamine (DPPE) and triphenylethanamine (TPE) series of CETP inhibitors to improve their pharmaceutical profile is described. Polar groups at the N-terminus position in the DPPE series resulted in further improvement in potency and pharmaceutical properties concomitant with retaining the safety, efficacy, and pharmacokinetic (PK) profile. A structure-activity relationship observed in the DPPE series was extended to the corresponding analogs in the more potent TPE series, and further optimization resulted in the identification of 2-amino-N-((R)-1-(3-cyclopropoxy-4-fluorophenyl)-1-(3-fluoro-5-(1,1,2,2-tetrafluoroethoxy)phenyl)-2-phenylethyl)-4,4,4-trifluoro-3-hydroxy-3-(trifluoromethyl)butanamide (13). Compound 13 demonstrated no significant changes in either mean arterial blood pressure or heart rate in telemetry rats, had an excellent PK profile, and demonstrated robust efficacy in human CETP/apo-B-100 dual transgenic mice and in hamsters.
ABSTRACT
Endothelial lipase (EL) inhibitors have been shown to elevate HDL-C levels in pre-clinical murine models and have potential benefit in prevention and treatment of cardiovascular diseases. Modification of the 1-ethyl-3-hydroxy-1,5-dihydro-2H-pyrrol-2-one (DHP) lead, 1, led to the discovery of a series of potent tetrahydropyrimidinedione (THP) EL inhibitors. Synthesis and SAR studies including modification of the amide group, together with changes on the pyrimidinone core led to a series of arylcycloalkyl, indanyl, and tetralinyl substituted 5-amino or 5-hydroxypyrimidinedione-4-carboxamides. Several compounds were advanced to PK evaluation. Among them, compound 4a was one of the most potent with measurable ELHDL hSerum potency and compound 3g demonstrated the best overall pharmacokinetic parameters.
Subject(s)
Enzyme Inhibitors/chemistry , Enzyme Inhibitors/pharmacology , Lipase/antagonists & inhibitors , Pyrimidinones/chemistry , Pyrimidinones/pharmacology , Animals , Cholesterol, HDL/blood , Cholesterol, HDL/metabolism , Enzyme Inhibitors/blood , Enzyme Inhibitors/chemical synthesis , Humans , Lipase/blood , Lipase/metabolism , Mice , Models, Molecular , Pyrimidinones/blood , Pyrimidinones/chemical synthesis , Structure-Activity RelationshipABSTRACT
BMS-A is an inhibitor of cholesteryl ester transfer protein and is a highly lipophilic compound (clogP 10.5) with poor aqueous solubility (<0.0001 mg/mL at pH 6.5). The compound exhibits low oral exposure when dosed as cosolvent solution formulations. The purpose of this study was to evaluate lipid-based formulations for enabling high-dose toxicology studies and enhancing toxicology margins of BMS-A in preclinical studies in nonrodent species. The solubility of BMS-A was screened in lipid and cosolvent/surfactant excipients, and prototype formulations were developed. In vitro tests showed that fine/microemulsions were formed after aqueous dilution of lipid formulations, and BMS-A was transferred from oil phase to aqueous phase with enhanced solubility following lipid digestion. When dosed in dogs at 200 mg/kg, a Gelucire-based formulation exhibited more than 10-fold higher exposure compared to the solution formulation and was thus selected for toxicology studies in dogs. For monkeys, an olive oil formulation was developed, and the exposure was about 7-fold higher than that from the solution. In summary, lipid-based drug delivery could be applied in early stages of drug discovery to enhance oral exposure and enable preclinical toxicology studies of highly lipophilic compounds, while facilitating the candidate selection of a molecule which is more specifically designed for bioperformance in a lipid-based drug delivery strategy.
Subject(s)
Benzamides/administration & dosage , Cholesterol Ester Transfer Proteins/antagonists & inhibitors , Emulsions/chemistry , Excipients/chemistry , Fluorobenzenes/administration & dosage , Lipids/chemistry , Administration, Oral , Animals , Benzamides/adverse effects , Benzamides/pharmacokinetics , Biological Availability , Dogs , Drug Compounding , Drug Stability , Fluorobenzenes/adverse effects , Fluorobenzenes/pharmacokinetics , Macaca fascicularis , Male , Mice, Inbred BALB C , Olive Oil/chemistry , Solubility , Triglycerides/chemistry , Water/chemistryABSTRACT
A one-step synthesis of Fmoc-protected aryl/heteroaryl-substituted phenylalanines (Bip derivatives) using the nonaqueous palladium-catalyzed Suzuki-Miyaura cross-coupling (SMC) reaction of Fmoc-protected bromo- or iodophenylalanines is reported. This protocol allows for the direct formation of a variety of unnatural biaryl-containing amino acids in good to excellent yield, which can be readily used in subsequent Fmoc solid-phase peptide synthesis. The synthetic utility of this method is also demonstrated by the SMC reaction of bromophenylalanine-containing tripeptides.
ABSTRACT
Cholesteryl ester transfer protein (CETP) inhibitors raise HDL-C in animals and humans and may be antiatherosclerotic by enhancing reverse cholesterol transport (RCT). In this article, we describe the lead optimization efforts resulting in the discovery of a series of triphenylethanamine (TPE) ureas and amides as potent and orally available CETP inhibitors. Compound 10g is a potent CETP inhibitor that maximally inhibited cholesteryl ester (CE) transfer activity at an oral dose of 1 mg/kg in human CETP/apoB-100 dual transgenic mice and increased HDL cholesterol content and size comparable to torcetrapib (1) in moderately-fat fed hamsters. In contrast to the off-target liabilities with 1, no blood pressure increase was observed with 10g in rat telemetry studies and no increase of aldosterone synthase (CYP11B2) was detected in H295R cells. On the basis of its preclinical profile, compound 10g was advanced into preclinical safety studies.
Subject(s)
Anticholesteremic Agents/chemical synthesis , Anticholesteremic Agents/pharmacology , Benzamides/chemical synthesis , Benzamides/pharmacology , Benzylamines/chemical synthesis , Benzylamines/pharmacology , Cholesterol Ester Transfer Proteins/antagonists & inhibitors , Animals , Anticholesteremic Agents/pharmacokinetics , Atherosclerosis/drug therapy , Benzamides/pharmacokinetics , Benzylamines/pharmacokinetics , Blood Pressure/drug effects , Cell Line , Cholesterol/metabolism , Cholesterol, HDL/blood , Cricetinae , Cytochrome P-450 CYP11B2/antagonists & inhibitors , Dogs , Drug Discovery , Humans , Macaca fascicularis , Male , Mesocricetus , Mice , Mice, Transgenic , Motor Activity/drug effects , Quinolines/pharmacology , Rats , Rats, Sprague-DawleyABSTRACT
Current antithrombotic discovery efforts target compounds that are highly efficacious in thrombus reduction with less bleeding liability than the standard of care. Preclinical data suggest that P2Y1 antagonists may have lower bleeding liabilities than P2Y12 antagonists while providing similar antithrombotic efficacy. This article describes our continuous SAR efforts in a series of 7-hydroxyindolinyl diaryl ureas. When dosed orally, 4-trifluoromethyl-7-hydroxy-3,3-dimethylindolinyl analogue 4 was highly efficacious in a model of arterial thrombosis in rats with limited bleeding. The chemically labile CF3 group in 4 was then transformed to various groups via a novel one-step synthesis, yielding a series of potent P2Y1 antagonists. Among them, the 4-benzothiazole-substituted indolines had desirable PK properties in rats, specifically, low clearance and small volume of distribution. In addition, compound 40 had high i.v. exposure and modest bioavailability, giving it the best overall profile.
Subject(s)
Purinergic P2Y Receptor Antagonists/pharmacology , Urea/analogs & derivatives , Animals , Humans , Magnetic Resonance Spectroscopy , Purinergic P2Y Receptor Antagonists/pharmacokinetics , Spectrometry, Mass, Electrospray Ionization , Urea/pharmacokinetics , Urea/pharmacologyABSTRACT
Adenosine diphosphate (ADP)-mediated platelet aggregation is signaled through two distinct G protein-coupled receptors (GPCR) on the platelet surface: P2Y12 and P2Y1. Blocking P2Y12 receptor is a clinically well-validated strategy for antithrombotic therapy. P2Y1 antagonists have been shown to have the potential to provide equivalent antithrombotic efficacy as P2Y12 inhibitors with reduced bleeding in preclinical animal models. We have previously reported the discovery of a potent and orally bioavailable P2Y1 antagonist, 1. This paper describes further optimization of 1 by introducing 4-aryl groups at the hydroxylindoline in two series. In the neutral series, 10q was identified with excellent potency and desirable pharmacokinetic (PK) profile. It also demonstrated similar antithrombotic efficacy with less bleeding compared with the known P2Y12 antagonist prasugrel in rabbit efficacy/bleeding models. In the basic series, 20c (BMS-884775) was discovered with an improved PK and liability profile over 1. These results support P2Y1 antagonism as a promising new antiplatelet target.
Subject(s)
Drug Discovery , Indoles/pharmacology , Platelet Aggregation Inhibitors/pharmacology , Purinergic P2Y Receptor Antagonists/pharmacology , Receptors, Purinergic P2Y1/metabolism , Animals , Blood Coagulation/drug effects , Dose-Response Relationship, Drug , Humans , Indoles/chemistry , Mice , Microsomes, Liver/chemistry , Microsomes, Liver/drug effects , Microsomes, Liver/metabolism , Molecular Structure , Platelet Aggregation/drug effects , Platelet Aggregation Inhibitors/chemical synthesis , Platelet Aggregation Inhibitors/chemistry , Purinergic P2Y Receptor Antagonists/chemical synthesis , Purinergic P2Y Receptor Antagonists/chemistry , Rabbits , Rats , Structure-Activity Relationship , Thrombosis/drug therapyABSTRACT
Blockade of the P2Y1 receptor is important to the treatment of thrombosis with potentially improved safety margins compared with P2Y12 receptor antagonists. Investigation of a series of urea surrogates of the diaryl urea lead 3 led to the discovery of 2-amino-1,3,4-thiadiazoles in the 7-hydroxy-N-neopentyl spiropiperidine indolinyl series as potent P2Y1 receptor antagonists, among which compound 5a was the most potent and the first non-urea analog with platelet aggregation (PA) IC50 less than 0.5 µM with 10 µM ADP. Several 2-amino-1,3,4-thiadiazole analogs such as 5b and 5f had a more favorable pharmacokinetic profile, such as higher Ctrough, lower Cl, smaller Vdss, and similar bioavailability compared with 3.
Subject(s)
Indoles/chemistry , Piperidines/chemistry , Receptors, Purinergic P2Y1/metabolism , Thiadiazoles/pharmacology , Animals , Dose-Response Relationship, Drug , Humans , Indoles/administration & dosage , Molecular Structure , Piperidines/administration & dosage , Rats , Structure-Activity Relationship , Thiadiazoles/administration & dosage , Thiadiazoles/chemistryABSTRACT
Spiropiperidine indoline-substituted diaryl ureas had been identified as antagonists of the P2Y1 receptor. Enhancements in potency were realized through the introduction of a 7-hydroxyl substitution on the spiropiperidinylindoline chemotype. SAR studies were conducted to improve PK and potency, resulting in the identification of compound 3e, a potent, orally bioavailable P2Y1 antagonist with a suitable PK profile in preclinical species. Compound 3e demonstrated a robust antithrombotic effect in vivo and improved bleeding risk profile compared to the P2Y12 antagonist clopidogrel in rat efficacy/bleeding models.
Subject(s)
Phenylurea Compounds/chemistry , Platelet Aggregation Inhibitors/chemistry , Purinergic P2Y Receptor Antagonists/chemistry , Receptors, Purinergic P2Y1/chemistry , Thiazoles/chemistry , Urea/analogs & derivatives , Administration, Oral , Animals , Dogs , Half-Life , Macaca fascicularis , Phenylurea Compounds/pharmacokinetics , Phenylurea Compounds/pharmacology , Phenylurea Compounds/therapeutic use , Platelet Aggregation/drug effects , Platelet Aggregation Inhibitors/pharmacokinetics , Platelet Aggregation Inhibitors/pharmacology , Platelet Aggregation Inhibitors/therapeutic use , Purinergic P2Y Receptor Antagonists/pharmacokinetics , Purinergic P2Y Receptor Antagonists/pharmacology , Purinergic P2Y Receptor Antagonists/therapeutic use , Rats , Receptors, Purinergic P2Y1/metabolism , Structure-Activity Relationship , Thiazoles/pharmacokinetics , Thiazoles/pharmacology , Thiazoles/therapeutic use , Thrombosis/drug therapy , Urea/pharmacokinetics , Urea/pharmacology , Urea/therapeutic useABSTRACT
Preclinical antithrombotic efficacy and bleeding models have demonstrated that P2Y1 antagonists are efficacious as antiplatelet agents and may offer a safety advantage over P2Y12 antagonists in terms of reduced bleeding liabilities. In this article, we describe the structural modification of the tert-butyl phenoxy portion of lead compound 1 and the subsequent discovery of a novel series of conformationally constrained ortho-anilino diaryl ureas. In particular, spiropiperidine indoline-substituted diaryl ureas are described as potent, orally bioavailable small-molecule P2Y1 antagonists with improved activity in functional assays and improved oral bioavailability in rats. Homology modeling and rat PK/PD studies on benchmark compound 3l will also be presented. Compound 3l was our first P2Y1 antagonist to demonstrate a robust oral antithrombotic effect with mild bleeding liability in the rat thrombosis and hemostasis models.
Subject(s)
Drug Design , Molecular Conformation , Phenylurea Compounds/pharmacology , Phenylurea Compounds/pharmacokinetics , Purinergic P2Y Receptor Antagonists/pharmacology , Purinergic P2Y Receptor Antagonists/pharmacokinetics , Receptors, Purinergic P2Y1/metabolism , Spiro Compounds/pharmacology , Spiro Compounds/pharmacokinetics , Urea/pharmacology , Urea/pharmacokinetics , Animals , Biological Availability , Humans , Indoles/chemistry , Models, Molecular , Phenylurea Compounds/chemistry , Phenylurea Compounds/metabolism , Purinergic P2Y Receptor Antagonists/chemistry , Purinergic P2Y Receptor Antagonists/metabolism , Rats , Rats, Sprague-Dawley , Receptors, Purinergic P2Y1/chemistry , Sequence Homology, Amino Acid , Spiro Compounds/chemistry , Spiro Compounds/metabolism , Urea/chemistry , Urea/metabolismABSTRACT
Preclinical data suggests that P2Y1 antagonists, such as diarylurea compound 1, may provide antithrombotic efficacy similar to P2Y12 antagonists and may have the potential of providing reduced bleeding liabilities. This manuscript describes a series of diarylureas bearing solublizing amine side chains as potent P2Y1 antagonists. Among them, compounds 2l and 3h had improved aqueous solubility and maintained antiplatelet activity compared with compound 1. Compound 2l was moderately efficacious in both rat and rabbit thrombosis models and had a moderate prolongation of bleeding time in rats similar to that of compound 1.
Subject(s)
Fibrinolytic Agents/chemistry , Phenylurea Compounds/chemistry , Purinergic P2Y Receptor Antagonists/chemistry , Pyridines/chemistry , Receptors, Purinergic P2Y1/chemistry , Urea/chemistry , Animals , Caco-2 Cells , Disease Models, Animal , Drug Evaluation, Preclinical , Fibrinolytic Agents/chemical synthesis , Fibrinolytic Agents/pharmacokinetics , Half-Life , Humans , Microsomes, Liver/metabolism , Partial Thromboplastin Time , Phenylurea Compounds/pharmacokinetics , Phenylurea Compounds/therapeutic use , Platelet Aggregation/drug effects , Purinergic P2Y Receptor Antagonists/pharmacokinetics , Purinergic P2Y Receptor Antagonists/therapeutic use , Pyridines/pharmacokinetics , Pyridines/therapeutic use , Rabbits , Rats , Receptors, Purinergic P2Y1/metabolism , Solubility , Structure-Activity Relationship , Thrombosis/drug therapy , Urea/pharmacokinetics , Urea/therapeutic use , Water/chemistryABSTRACT
A series of diphenylpyridylethanamine (DPPE) derivatives was identified exhibiting potent CETP inhibition. Replacing the labile ester functionality in the initial lead 7 generated a series of amides and ureas. Further optimization of the DPPE series for potency resulted in the discovery of cyclopentylurea 15d, which demonstrated a reduction in cholesterol ester transfer activity (48% of predose level) in hCETP/apoB-100 dual transgenic mice. The PK profile of 15d was suboptimal, and further optimization of the N-terminus resulted in the discovery of amide 20 with an improved PK profile and robust efficacy in transgenic hCETP/apoB-100 mice and in hamsters. Compound 20 demonstrated no significant changes in either mean arterial blood pressure or heart rate in telemeterized rats despite sustained high exposures.
Subject(s)
Anticholesteremic Agents/chemistry , Anticholesteremic Agents/pharmacology , Cholesterol Ester Transfer Proteins/antagonists & inhibitors , Pyridines/chemistry , Pyridines/pharmacology , Stilbenes/chemistry , Stilbenes/pharmacology , Animals , Anticholesteremic Agents/chemical synthesis , Apolipoprotein B-100/antagonists & inhibitors , Apolipoprotein B-100/metabolism , Blood Pressure/drug effects , Cholesterol Ester Transfer Proteins/metabolism , Coronary Disease/drug therapy , Cricetinae , Drug Discovery , Heart Rate/drug effects , Humans , Inhibitory Concentration 50 , Male , Mice , Mice, Transgenic , Molecular Structure , Pyridines/chemical synthesis , Rats , Stilbenes/chemical synthesisABSTRACT
The (hetero)aromatic trifluoromethyl group is present in many biologically active molecules and is generally considered to be chemically stable. In this paper, a convenient one-step synthesis of C-C linked aryl-heterocycles or heteroaryl-heterocycles in good to excellent yields via the reaction of anionically activated trifluoromethyl groups with amino nucleophiles containing a second NH, OH, or SH nucleophile in 1 N sodium hydroxide is reported. The method has high functional group tolerability and is potentially useful in parallel synthesis.
Subject(s)
Fluorine Compounds/chemistry , Heterocyclic Compounds/chemistry , Anions/chemistry , Methylation , Molecular Structure , StereoisomerismABSTRACT
2-Arylbenzoxazole 5 was identified as a hit from a fluorescence-based high-throughput screen for CETP inhibitors. The synthesis and SAR investigation employing array synthesis of the A- and B-rings are described.
Subject(s)
Benzoxazoles/chemical synthesis , Benzoxazoles/pharmacology , Cholesterol Ester Transfer Proteins/antagonists & inhibitors , Benzoxazoles/chemistry , Cholesterol Ester Transfer Proteins/metabolism , Humans , Models, Molecular , Molecular Structure , Structure-Activity RelationshipABSTRACT
We previously reported a series of enantiopure cis-(1R,2S)-cyclopentyldiamine derivatives as potent and selective inhibitors of Factor Xa (FXa). Herein, we describe our approach to improve the metabolic stability of this series via core modifications. Multiple resulting series of compounds demonstrated similarly high FXa potency and improved metabolic stability in human liver microsomes compared with the cyclopentyldiamide 1. (3R,4S)-Pyrrolidinyldiamide 31 was the best overall compound with human FXa K(i) of 0.50 nM, PT EC(2x) of 2.1 microM in human plasma, bioavailability of 25% and t(1/2)of 2.7h in dogs. Further biochemical characterization of compound 31 is also presented.
Subject(s)
Factor Xa Inhibitors , Serine Proteinase Inhibitors/pharmacology , Animals , Biological Availability , Dogs , Half-Life , Humans , Models, Molecular , Serine Proteinase Inhibitors/chemistry , Serine Proteinase Inhibitors/pharmacokinetics , Stereoisomerism , Structure-Activity RelationshipABSTRACT
In the search of Factor Xa (FXa) inhibitors structurally different from the pyrazole-based series, we identified a viable series of enantiopure cis-(1R,2S)-cycloalkyldiamine derivatives as potent and selective inhibitors of FXa. Among them, cyclohexyldiamide 7 and cyclopentyldiamide 9 were the most potent neutral compounds, and had good anticoagulant activity comparable to the pyrazole-based analogs. Crystal structures of 7-FXa and 9-FXa illustrate binding similarities and differences between the five- and the six-membered core systems, and provide rationales for the observed SAR of P1 and linker moieties.
Subject(s)
Diamines/chemistry , Diamines/pharmacology , Factor Xa Inhibitors , Anticoagulants/chemistry , Anticoagulants/pharmacology , Binding Sites , Humans , Models, Molecular , Molecular Structure , Prothrombin Time , Structure-Activity Relationship , X-Ray DiffractionABSTRACT
A novel, N-aryl-bicyclohydantoin selective androgen receptor modulator scaffold was discovered through structure-guided modifications of androgen receptor antagonists. A prototype compound (7R,7aS)-10b from this series is a potent and highly tissue-selective agonist of the androgen receptor. After oral dosing in a rat atrophied levator ani muscle model, (7R,7aS)-10b demonstrated efficacy at restoring levator ani muscle mass to that of intact controls and exhibited >50-fold selectivity for muscle over prostate.
Subject(s)
Bridged-Ring Compounds/pharmacology , Hydantoins/pharmacology , Muscle, Skeletal/drug effects , Muscular Atrophy/drug therapy , Receptors, Androgen/metabolism , Administration, Oral , Animals , Breast Neoplasms/drug therapy , Bridged-Ring Compounds/chemical synthesis , Bridged-Ring Compounds/chemistry , Cells, Cultured , Dihydrotestosterone/pharmacology , Humans , Hydantoins/administration & dosage , Hydantoins/chemical synthesis , Hydantoins/chemistry , Luciferases/metabolism , Male , Mice , Muscle, Skeletal/growth & development , Myoblasts/drug effects , Rats , Transcriptional ActivationABSTRACT
A series of retro-binding inhibitors of human alpha-thrombin was prepared to elucidate structure-activity relationships (SAR) and optimize in vivo performance. Compounds 9 and 11, orally active inhibitors of thrombin catalytic activity, were identified to be efficacious in a thrombin-induced lethality model in mice.
Subject(s)
Oligopeptides/chemical synthesis , Oligopeptides/pharmacology , Serine Proteinase Inhibitors/chemical synthesis , Serine Proteinase Inhibitors/pharmacology , Thrombin/antagonists & inhibitors , Animals , Binding Sites/drug effects , Catalysis , Humans , Mice , Structure-Activity Relationship , Thrombin/chemistry , Thrombin/toxicityABSTRACT
A series of structurally novel small molecule inhibitors of human alpha-thrombin was prepared to elucidate their structure- activity relationships (SAR), selectivity and activity in vivo. BMS-189090 (5) is identified as a potent, selective, and reversible inhibitor of human alpha-thrombin that is efficacious in vivo in a mice lethality model, and in inhibiting both arterial and venous thrombosis in a rat model.