RÉSUMÉ
Efforts directed at improving potency and preparing structurally different TYK2 JH2 inhibitors from the first generation of compounds such as 1a led to the SAR study of new central pyridyl based analogs 2-4. The current SAR study resulted in the identification of 4h as a potent and selective TYK2 JH2 inhibitor with distinct structural differences from 1a. In this manuscript, the in vitro and in vivo profiles of 4h are described. The hWB IC50 of 4h was shown as 41 nM with 94% bioavailability in the mouse PK study.
Sujet(s)
Pyridines , TYK2 Kinase , Souris , Animaux , Relation structure-activité , Pyridines/pharmacologieRÉSUMÉ
The toll-like receptors (TLRs) play key roles in activation of the innate immune system. Aberrant activation of TLR7 and TLR8 pathways can occur in the context of autoimmune disorders due to the elevated presence and recognition of self-RNA as activating ligands. Control of this unintended activation via inhibition of TLR7/8 signaling holds promise for the treatment of diseases such as psoriasis, arthritis, and lupus. Optimization of a 2-pyridinylindole series of compounds led to the identification of potent dual inhibitors of TLR7 and TLR8, which demonstrated good selectivity against TLR9 and other family members. The in vitro characterization and in vivo evaluation in rodent pharmacokinetic/pharmacodynamic and efficacy studies of BMS-905 is detailed, along with structural information obtained through X-ray cocrystallographic studies.
RÉSUMÉ
Sphingosine-1-phosphate (S1P) binds to a family of sphingosine-1-phosphate G-protein-coupled receptors (S1P1-5). The interaction of S1P with these S1P receptors has a fundamental role in many physiological processes in the vascular and immune systems. Agonist-induced functional antagonism of S1P1 has been shown to result in lymphopenia. As a result, agonists of this type hold promise as therapeutics for autoimmune disorders. The previously disclosed differentiated S1P1 modulator BMS-986104 (1) exhibited improved preclinical cardiovascular and pulmonary safety profiles as compared to earlier full agonists of S1P1; however, it demonstrated a long pharmacokinetic half-life (T1/2 18 days) in the clinic and limited formation of the desired active phosphate metabolite. Optimization of this series through incorporation of olefins, ethers, thioethers, and glycols into the alkyl side chain afforded an opportunity to reduce the projected human T1/2 and improve the formation of the active phosphate metabolite while maintaining efficacy as well as the improved safety profile. These efforts led to the discovery of 12 and 24, each of which are highly potent, biased agonists of S1P1. These compounds not only exhibited shorter in vivo T1/2 in multiple species but are also projected to have significantly shorter T1/2 values in humans when compared to our first clinical candidate. In models of arthritis, treatment with 12 and 24 demonstrated robust efficacy.
Sujet(s)
Composés bicycliques pontés/synthèse chimique , Composés bicycliques pontés/pharmacologie , Proprotein convertases/effets des médicaments et des substances chimiques , Serine endopeptidases/effets des médicaments et des substances chimiques , Animaux , Arthrite expérimentale/traitement médicamenteux , Maladies auto-immunes/traitement médicamenteux , Biotransformation , Composés bicycliques pontés/effets indésirables , Liquide de lavage bronchoalvéolaire , Chimiotaxie des leucocytes/effets des médicaments et des substances chimiques , Évaluation préclinique de médicament , Période , Humains , Maladies pulmonaires/induit chimiquement , Maladies pulmonaires/anatomopathologie , Mâle , Myocytes cardiaques/effets des médicaments et des substances chimiques , Phosphorylation , Rats , Rats de lignée LEW , Relation structure-activitéRÉSUMÉ
The toll-like receptor (TLR) family is an evolutionarily conserved component of the innate immune system, responsible for the early detection of foreign or endogenous threat signals. In the context of autoimmunity, the unintended recognition of self-motifs as foreign promotes initiation or propagation of disease. Overactivation of TLR7 and TLR9 have been implicated as factors contributing to autoimmune disorders such as psoriasis, arthritis, and lupus. In our search for small molecule antagonists of TLR7/9, 7f was identified as possessing excellent on-target potency for human TLR7/9 as well as for TLR8, with selectivity against other representative TLR family members. Good pharmacokinetic properties and a relatively balanced potency against TLR7 and TLR9 in mouse systems (systems which lack functional TLR8) made this an excellent in vivo tool compound, and efficacy from oral dosing in preclinical models of autoimmune disease was demonstrated.
RÉSUMÉ
Efforts aimed at increasing the in vivo potency and reducing the elimination half-life of 1 and 2 led to the identification of aryl ether and thioether-derived bicyclic S1P1 differentiated modulators 3-6. The effects of analogs 3-6 on lymphocyte reduction in the rat (desired pharmacology) along with pulmonary- and cardiovascular-related effects (undesired pharmacology) are described. Optimization of the overall properties in the aryl ether series yielded 3d, and the predicted margin of safety against the cardiovascular effects of 3d would be large enough for human studies. Importantly, compared to 1 and 2, compound 3d had a better profile in both potency (ED50 < 0.05 mg/kg) and predicted human half-life (t 1/2 â¼ 5 days).
RÉSUMÉ
Recently, our research group reported the identification of BMS-986104 (2) as a differentiated S1P1 receptor modulator. In comparison to fingolimod (1), a full agonist of S1P1 currently marketed for the treatment of relapse remitting multiple sclerosis (RRMS), 2 offers several potential advantages having demonstrated improved safety multiples in preclinical evaluations against undesired pulmonary and cardiovascular effects. In clinical trials, 2 was found to exhibit a pharmacokinetic half-life ( T1/2) longer than that of 1, as well as a reduced formation of the phosphate metabolite that is required for activity against S1P1. Herein, we describe our efforts to discover highly potent, partial agonists of S1P1 with a shorter T1/2 and increased in vivo phosphate metabolite formation. These efforts culminated in the discovery of BMS-986166 (14a), which was advanced to human clinical evaluation. The pharmacokinetic/pharmacodynamic (PK/PD) relationship as well as pulmonary and cardiovascular safety assessments are discussed. Furthermore, efficacy of 14a in multiple preclinical models of autoimmune diseases are presented.
Sujet(s)
Essais cliniques comme sujet , Naphtalènes/pharmacologie , Récepteurs de la sphingosine-1-phosphate/agonistes , 1,2,3,4-Tétrahydro-naphtalènes/pharmacologie , Animaux , Liquide de lavage bronchoalvéolaire , Relation dose-effet des médicaments , Période , Humains , Naphtalènes/composition chimique , Naphtalènes/pharmacocinétique , Rats , Rats de lignée LEW , 1,2,3,4-Tétrahydro-naphtalènes/composition chimique , 1,2,3,4-Tétrahydro-naphtalènes/pharmacocinétiqueRÉSUMÉ
The sphingoid base derived class of lipids (sphingolipids) is a family of interconverting molecules that play key roles in numerous structural and signaling processes. The biosynthetic pathway of the sphingolipids affords many opportunities for therapeutic intervention: targeting the ligands directly, targeting the various proteins involved in the interconversion of the ligands, or targeting the receptors that respond to the ligands. The focus of this article is on the most advanced of the sphingosine-related therapeutics, agonists of sphingosine-1-phosphate receptor 1 (S1P1). The diverse structural classes of S1P1 agonists will be discussed and the status of compounds of clinical relevance will be detailed. An examination of how potential safety concerns are being navigated with compounds currently under clinical evaluation is followed by a discussion of the novel methods being explored to identify next-generation S1P1 agonists with improved safety profiles. Finally, therapeutic opportunities for sphingosine-related targets outside of S1P1 are touched upon.
Sujet(s)
Chlorhydrate de fingolimod/pharmacologie , Lysophospholipides/métabolisme , Récepteurs aux lysosphingolipides/agonistes , Sphingosine/analogues et dérivés , Relation dose-effet des médicaments , Chlorhydrate de fingolimod/composition chimique , Humains , Ligands , Structure moléculaire , Récepteurs aux lysosphingolipides/métabolisme , Sphingosine/métabolisme , Relation structure-activitéRÉSUMÉ
Recently, our research group reported the identification of prodrug amino-alcohol 2 as a potent and efficacious S1P1 receptor modulator. This molecule is differentiated preclinically over the marketed drug fingolimod (Gilenya 1), whose active phosphate metabolite is an S1P1 full agonist, in terms of pulmonary and cardiovascular safety. S1P1 partial agonist 2, however, has a long half-life in rodents and was projected to have a long half-life in humans. The purpose of this communication is to disclose highly potent partial agonists of S1P1 with shorter half-lives relative to the clinical compound 2. PK/PD relationships as well as their preclinical pulmonary and cardiovascular safety assessment are discussed.
RÉSUMÉ
We describe a highly efficient route for the synthesis of 4a (BMS-986104). A key step in the synthesis is the asymmetric hydroboration of trisubstituted alkene 6. Particularly given the known difficulties involved in this type of transformation (6 â 7), the current methodology provides an efficient approach to prepare this class of compounds. In addition, we disclose the efficacy of 4a in a mouse EAE model, which is comparable to 4c (FTY720). Mechanistically, 4a exhibited excellent remyelinating effects on lysophosphatidylcholine (LPC) induced demyelination in a three-dimensional brain cell culture assay.
Sujet(s)
Encéphalomyélite auto-immune expérimentale/traitement médicamenteux , Naphtalènes/pharmacologie , Récepteurs aux lysosphingolipides/agonistes , Animaux , Cellules cultivées , Modèles animaux de maladie humaine , Relation dose-effet des médicaments , Femelle , Cellules HEK293 , Humains , Lymphocytes/effets des médicaments et des substances chimiques , Souris , Souris de lignée BALB C , Souris de lignée C57BL , Structure moléculaire , Naphtalènes/synthèse chimique , Naphtalènes/composition chimique , Relation structure-activitéRÉSUMÉ
Fingolimod (1) is the first approved oral therapy for the treatment of relapsing remitting multiple sclerosis. While the phosphorylated metabolite of fingolimod was found to be a nonselective S1P receptor agonist, agonism specifically of S1P1 is responsible for the peripheral blood lymphopenia believed to be key to its efficacy. Identification of modulators that maintain activity on S1P1 while sparing activity on other S1P receptors could offer equivalent efficacy with reduced liabilities. We disclose in this paper a ligand-based drug design approach that led to the discovery of a series of potent tricyclic agonists of S1P1 with selectivity over S1P3 and were efficacious in a pharmacodynamic model of suppression of circulating lymphocytes. Compound 10 had the desired pharmacokinetic (PK) and pharmacodynamic (PD) profile and demonstrated maximal efficacy when administered orally in a rat adjuvant arthritis model.
Sujet(s)
Conception de médicament , Chlorhydrate de fingolimod/pharmacologie , Composés hétérocycliques 3 noyaux/pharmacologie , Récepteurs aux lysosphingolipides/agonistes , Animaux , Arthrite expérimentale/traitement médicamenteux , Arthrite expérimentale/immunologie , Chiens , Relation dose-effet des médicaments , Chlorhydrate de fingolimod/administration et posologie , Chlorhydrate de fingolimod/composition chimique , Adjuvant Freund/administration et posologie , Composés hétérocycliques 3 noyaux/administration et posologie , Composés hétérocycliques 3 noyaux/composition chimique , Ligands , Lymphocytes/effets des médicaments et des substances chimiques , Macaca fascicularis , Mâle , Souris , Structure moléculaire , Mycobacterium/effets des médicaments et des substances chimiques , Rats , Rats de lignée LEW , Relation structure-activité , Distribution tissulaireRÉSUMÉ
Sphingosine-1-phosphate (S1P) is a bioactive sphingolipid metabolite that regulates a multitude of physiological processes such as lymphocyte trafficking, cardiac function, vascular development, and inflammation. Because of the ability of S1P1 receptor agonists to suppress lymphocyte egress, they have great potential as therapeutic agents in a variety of autoimmune diseases. In this article, the discovery of selective, direct acting S1P1 agonists utilizing an ethanolamine scaffold containing a terminal carboxylic acid is described. Potent S1P1 agonists such as compounds 18a and 19a which have greater than 1000-fold selectivity over S1P3 are described. These compounds efficiently reduce blood lymphocyte counts in rats through 24 h after single doses of 1 and 0.3 mpk, respectively. Pharmacodynamic properties of both compounds are discussed. Compound 19a was further studied in two preclinical models of disease, exhibiting good efficacy in both the rat adjuvant arthritis model (AA) and the mouse experimental autoimmune encephalomyelitis model (EAE).
Sujet(s)
Éthanolamine/composition chimique , Éthanolamine/pharmacologie , Lymphocytes/effets des médicaments et des substances chimiques , Récepteurs aux lysosphingolipides/agonistes , Animaux , Arthrite/traitement médicamenteux , Chiens , Encéphalomyélite auto-immune expérimentale/traitement médicamenteux , Éthanolamine/pharmacocinétique , Éthanolamine/usage thérapeutique , Femelle , Haplorhini , Humains , Numération des lymphocytes , Lymphocytes/cytologie , Mâle , Souris , Souris de lignée C57BL , Rats , Rats de lignée LEW , Récepteurs aux lysosphingolipides/métabolisme , Relation structure-activitéRÉSUMÉ
The synthesis and structure-activity relationship (SAR) of a series of pyridyl-isoxazole based agonists of S1P1 are discussed. Compound 5b provided potent in vitro activity with selectivity, had an acceptable pharmacokinetic profile, and demonstrated efficacy in a dose dependent manner when administered orally in a rodent model of arthritis.
Sujet(s)
Arthrite expérimentale/traitement médicamenteux , Lysophospholipides/agonistes , Sphingosine/analogues et dérivés , Relation structure-activité , Administration par voie orale , Animaux , Techniques de chimie synthétique , Relation dose-effet des médicaments , Évaluation préclinique de médicament/méthodes , Humains , Isoxazoles/composition chimique , Isoxazoles/pharmacologie , Numération des lymphocytes , Mâle , Rats de lignée LEW , Récepteurs aux lysosphingolipides/agonistes , Sphingosine/agonistesRÉSUMÉ
Clinical validation of S1P receptor modulation therapy was achieved with the approval of fingolimod (Gilenya, 1) as the first oral therapy for relapsing remitting multiple sclerosis. However, 1 causes a dose-dependent reduction in the heart rate (bradycardia), which occurs within hours after first dose. We disclose the identification of clinical compound BMS-986104 (3d), a novel S1P1 receptor modulator, which demonstrates ligand-biased signaling and differentiates from 1 in terms of cardiovascular and pulmonary safety based on preclinical pharmacology while showing equivalent efficacy in a T-cell transfer colitis model.
RÉSUMÉ
Sphingosine 1-phosphate (S1P) is the endogenous ligand for the sphingosine 1-phosphate receptors (S1P1-5) and evokes a variety of cellular responses through their stimulation. The interaction of S1P with the S1P receptors plays a fundamental physiological role in a number of processes including vascular development and stabilization, lymphocyte migration, and proliferation. Agonism of S1P1, in particular, has been shown to play a significant role in lymphocyte trafficking from the thymus and secondary lymphoid organs, resulting in immunosuppression. This article will detail the discovery and SAR of a potent and selective series of isoxazole based full agonists of S1P1. Isoxazole 6d demonstrated impressive efficacy when administered orally in a rat model of arthritis and in a mouse experimental autoimmune encephalomyelitis (EAE) model of multiple sclerosis.
Sujet(s)
Isoxazoles/synthèse chimique , Isoxazoles/pharmacologie , Lysophospholipides/agonistes , Sphingosine/analogues et dérivés , Animaux , Arthrite expérimentale/traitement médicamenteux , Cellules CHO , Mouvement cellulaire/effets des médicaments et des substances chimiques , Prolifération cellulaire/effets des médicaments et des substances chimiques , Cricetinae , Cricetulus , Découverte de médicament , Encéphalomyélite auto-immune expérimentale/traitement médicamenteux , Humains , Immunosuppresseurs/synthèse chimique , Immunosuppresseurs/pharmacologie , Système lymphatique/cytologie , Système lymphatique/effets des médicaments et des substances chimiques , Lymphocytes/effets des médicaments et des substances chimiques , Souris , Souris de lignée C57BL , Rats , Rats de lignée LEW , Sphingosine/agonistes , Relation structure-activité , Thymus (glande)/cytologie , Thymus (glande)/effets des médicaments et des substances chimiquesRÉSUMÉ
Investigation of various heterocyclic core isosteres of imidazopyrazines 1 & 2 yielded purine derivatives 3 & 8 as potent and selective BTK inhibitors. Subsequent SAR studies of the purine series led to the discovery of 20 as a leading compound. Compound 20 is very selective when screened against a panel of 400 kinases and is a potent inhibitor in cellular assays of human B cell function including B-Cell proliferation and CD86 cell surface expression and exhibited in vivo efficacy in a mouse PCA model. Its X-ray co-crystal structure with BTK shows that the high selectivity is gained from filling a BTK specific lipophilic pocket. However, physical and ADME properties leading to low oral exposure hindered further development.
Sujet(s)
Inhibiteurs de protéines kinases/composition chimique , Inhibiteurs de protéines kinases/pharmacologie , Protein-tyrosine kinases/antagonistes et inhibiteurs , Purines/composition chimique , Purines/pharmacologie , Agammaglobulinaemia tyrosine kinase , Animaux , Maladies auto-immunes/traitement médicamenteux , Maladies auto-immunes/enzymologie , Lymphocytes B/effets des médicaments et des substances chimiques , Cristallographie aux rayons X , Humains , Souris , Modèles moléculaires , Anaphylaxie cutanée passive/effets des médicaments et des substances chimiques , Protein-tyrosine kinases/métabolisme , RatsRÉSUMÉ
A novel series of p38 MAP kinase inhibitors with high selectivity for the p38α isoform over the other family members including the highly homologous p38ß isoform has been identified. X-ray co-crystallographic studies have revealed an unprecedented kinase binding mode in p38α for representative analogs, 5c and 9d, in which a Leu108/Met109 peptide flip occurs within the p38α hinge region. Based on these findings, a general strategy for the rational design of additional promising p38α isoform selective inhibitors by targeting this novel binding mode is proposed.
Sujet(s)
Mitogen-Activated Protein Kinase 14/antagonistes et inhibiteurs , Inhibiteurs de protéines kinases/composition chimique , Sites de fixation , Cristallographie aux rayons X , Humains , Liaison hydrogène , Mitogen-Activated Protein Kinase 14/métabolisme , Simulation de dynamique moléculaire , Liaison aux protéines , Isoformes de protéines/antagonistes et inhibiteurs , Isoformes de protéines/métabolisme , Inhibiteurs de protéines kinases/synthèse chimique , Inhibiteurs de protéines kinases/métabolisme , Structure tertiaire des protéines , Relation structure-activitéRÉSUMÉ
The synthesis, structure-activity relationships (SAR), and biological results of pyridyl-substituted azaindole based tricyclic inhibitors of IKK2 are described. Compound 4m demonstrated potent in vitro potency, acceptable pharmacokinetic and physicochemical properties, and efficacy when dosed orally in a mouse model of inflammatory bowel disease.
Sujet(s)
Acétamides/composition chimique , Découverte de médicament , Antienzymes/composition chimique , Composés hétérocycliques 3 noyaux/composition chimique , I-kappa B Kinase/antagonistes et inhibiteurs , Acétamides/synthèse chimique , Acétamides/pharmacologie , Administration par voie orale , Animaux , Activation enzymatique/effets des médicaments et des substances chimiques , Antienzymes/synthèse chimique , Antienzymes/pharmacologie , Composés hétérocycliques 3 noyaux/synthèse chimique , Composés hétérocycliques 3 noyaux/pharmacologie , Humains , Maladies inflammatoires intestinales/traitement médicamenteux , Concentration inhibitrice 50 , Souris , Structure moléculaire , Rats , Relation structure-activitéRÉSUMÉ
Pyrrolo[2,1-f][1,2,4]triazine based inhibitors of p38α have been prepared exploring functional group modifications at the C6 position. Incorporation of aryl and heteroaryl ketones at this position led to potent inhibitors with efficacy in in vivo models of acute and chronic inflammation.
Sujet(s)
Anti-inflammatoires/composition chimique , Mitogen-Activated Protein Kinase 14/antagonistes et inhibiteurs , Inhibiteurs de protéines kinases/composition chimique , Pyrroles/composition chimique , Triazines/composition chimique , Administration par voie orale , Animaux , Anti-inflammatoires/pharmacologie , Anti-inflammatoires/usage thérapeutique , Arthrite/traitement médicamenteux , Sites de fixation , Cristallographie aux rayons X , Modèles animaux de maladie humaine , Évaluation préclinique de médicament , Femelle , Souris , Mitogen-Activated Protein Kinase 14/métabolisme , Inhibiteurs de protéines kinases/pharmacologie , Inhibiteurs de protéines kinases/usage thérapeutique , Structure tertiaire des protéines , Rats , Relation structure-activité , Triazines/pharmacologie , Triazines/usage thérapeutiqueRÉSUMÉ
The synthesis, structure-activity relationships (SAR) and biological evaluation of thiazole based tricyclic inhibitors of IKK2 are described. Compound 9 was determined to be orally efficacious in a murine model of rheumatoid arthritis.
Sujet(s)
Polyarthrite rhumatoïde/traitement médicamenteux , I-kappa B Kinase/antagonistes et inhibiteurs , Imidazoles/composition chimique , Inhibiteurs de protéines kinases/composition chimique , Pyridines/composition chimique , Thiazoles/composition chimique , Animaux , Modèles animaux de maladie humaine , Chiens , Évaluation préclinique de médicament , Femelle , I-kappa B Kinase/métabolisme , Souris , Souris de lignée BALB C , Inhibiteurs de protéines kinases/pharmacocinétique , Inhibiteurs de protéines kinases/usage thérapeutique , Pyridines/pharmacocinétique , Pyridines/usage thérapeutique , Rats , Relation structure-activitéRÉSUMÉ
The synthesis and structure-activity relationships (SAR) of p38α MAP kinase inhibitors based on a 5-amino-pyrazole scaffold are described. These studies led to the identification of compound 2j as a potent and selective inhibitor of p38α MAP kinase with excellent cellular potency toward the inhibition of TNFα production. Compound 2j was highly efficacious in vivo in inhibiting TNFα production in an acute murine model of TNFα production. X-ray co-crystallography of a 5-amino-pyrazole analog 2f bound to unphosphorylated p38α is also disclosed.