RÉSUMÉ
Farnesoid X receptor (FXR) agonists are emerging as important potential therapeutics for the treatment of nonalcoholic steatohepatitis (NASH) patients, as they exert positive effects on multiple aspects of the disease. FXR agonists reduce lipid accumulation in the liver, hepatocellular inflammation, hepatic injury, and fibrosis. While there are currently no approved therapies for NASH, the bile acid-derived FXR agonist obeticholic acid (OCA; 6-ethyl chenodeoxycholic acid) has shown promise in clinical studies. Previously, we described the discovery of tropifexor (LJN452), the most potent non-bile acid FXR agonist currently in clinical investigation. Here, we report the discovery of a novel chemical series of non-bile acid FXR agonists based on a tricyclic dihydrochromenopyrazole core from which emerged nidufexor (LMB763), a compound with partial FXR agonistic activity in vitro and FXR-dependent gene modulation in vivo. Nidufexor has advanced to Phase 2 human clinical trials in patients with NASH and diabetic nephropathy.
Sujet(s)
Benzothiazoles/usage thérapeutique , Chénodiol/analogues et dérivés , Alimentation riche en graisse/effets indésirables , Isoxazoles/usage thérapeutique , Stéatose hépatique non alcoolique/traitement médicamenteux , Récepteurs cytoplasmiques et nucléaires/agonistes , Animaux , Benzothiazoles/composition chimique , Chénodiol/composition chimique , Chénodiol/usage thérapeutique , Chiens , Humains , Isoxazoles/composition chimique , Mâle , Souris , Souris de lignée C57BL , Stéatose hépatique non alcoolique/sang , Stéatose hépatique non alcoolique/étiologie , Structure tertiaire des protéines , Rats , Résultat thérapeutiqueRÉSUMÉ
This corrects the article DOI: 10.1038/nrd.2018.97.
RÉSUMÉ
Danger signals are a hallmark of many common inflammatory diseases, and these stimuli can function to activate the cytosolic innate immune signalling receptor NLRP3 (NOD-, LRR- and pyrin domain-containing 3). Once activated, NLRP3 nucleates the assembly of an inflammasome, leading to caspase 1-mediated proteolytic activation of the interleukin-1ß (IL-1ß) family of cytokines, and induces an inflammatory, pyroptotic cell death. Pharmacological inhibition of NLRP3 activation results in potent therapeutic effects in a wide variety of rodent models of inflammatory diseases, effects that are mirrored by genetic ablation of NLRP3. Although these findings highlight the potential of NLRP3 as a drug target, an understanding of NLRP3 structure and activation mechanisms is incomplete, which has hampered the discovery and development of novel therapeutics against this target. Here, we review recent advances in our understanding of NLRP3 activation and regulation, highlight the evolving landscape of NLRP3 modulators and discuss opportunities for pharmacologically targeting NLRP3 with novel small molecules.
RÉSUMÉ
The farnesoid X receptor (FXR) is a nuclear receptor that acts as a master regulator of bile acid metabolism and signaling. Activation of FXR inhibits bile acid synthesis and increases bile acid conjugation, transport, and excretion, thereby protecting the liver from the harmful effects of bile accumulation, leading to considerable interest in FXR as a therapeutic target for the treatment of cholestasis and nonalcoholic steatohepatitis. We identified a novel series of highly potent non-bile acid FXR agonists that introduce a bicyclic nortropine-substituted benzothiazole carboxylic acid moiety onto a trisubstituted isoxazole scaffold. Herein, we report the discovery of 1 (tropifexor, LJN452), a novel and highly potent agonist of FXR. Potent in vivo activity was demonstrated in rodent PD models by measuring the induction of FXR target genes in various tissues. Tropifexor has advanced into phase 2 human clinical trials in patients with NASH and PBC.
Sujet(s)
Benzothiazoles/pharmacologie , Cholestase/traitement médicamenteux , Isoxazoles/pharmacologie , Stéatose hépatique non alcoolique/traitement médicamenteux , Récepteurs cytoplasmiques et nucléaires/agonistes , Administration par voie orale , Animaux , Benzothiazoles/usage thérapeutique , Biodisponibilité , Chiens , Évaluation préclinique de médicament/méthodes , Facteurs de croissance fibroblastique/génétique , Régulation de l'expression des gènes/effets des médicaments et des substances chimiques , Humains , Isoxazoles/usage thérapeutique , Mâle , Microsomes du foie/effets des médicaments et des substances chimiques , Pipéridines/composition chimique , Rat Sprague-Dawley , Récepteurs cytoplasmiques et nucléaires/génétique , Récepteurs cytoplasmiques et nucléaires/métabolisme , Relation structure-activité , Triglycéride/sangRÉSUMÉ
OBJECTIVES: Wnt signalling has been implicated in activating a fibrogenic programme in fibroblasts in systemic sclerosis (SSc). Porcupine is an O-acyltransferase required for secretion of Wnt proteins in mammals. Here, we aimed to evaluate the antifibrotic effects of pharmacological inhibition of porcupine in preclinical models of SSc. METHODS: The porcupine inhibitor GNF6231 was evaluated in the mouse models of bleomycin-induced skin fibrosis, in tight-skin-1 mice, in murine sclerodermatous chronic-graft-versus-host disease (cGvHD) and in fibrosis induced by a constitutively active transforming growth factor-ß-receptor I. RESULTS: Treatment with pharmacologically relevant and well-tolerated doses of GNF6231 inhibited the activation of Wnt signalling in fibrotic murine skin. GNF6231 ameliorated skin fibrosis in all four models. Treatment with GNF6231 also reduced pulmonary fibrosis associated with murine cGvHD. Most importantly, GNF6231 prevented progression of fibrosis and showed evidence of reversal of established fibrosis. CONCLUSIONS: These data suggest that targeting the Wnt pathway through inhibition of porcupine provides a potential therapeutic approach to fibrosis in SSc. This is of particular interest, as a close analogue of GNF6231 has already demonstrated robust pathway inhibition in humans and could be available for clinical trials.
Sujet(s)
Aminopyridines/usage thérapeutique , Protéines membranaires/antagonistes et inhibiteurs , Pipérazines/usage thérapeutique , Sclérodermie localisée/prévention et contrôle , Sclérodermie systémique/prévention et contrôle , Peau/anatomopathologie , Voie de signalisation Wnt/effets des médicaments et des substances chimiques , Acyltransferases , Aminopyridines/pharmacologie , Animaux , Bléomycine , Modèles animaux de maladie humaine , Évolution de la maladie , Femelle , Fibrose , Maladie du greffon contre l'hôte/complications , Souris de lignée BALB C , Pipérazines/pharmacologie , Protein-Serine-Threonine Kinases/génétique , Fibrose pulmonaire/étiologie , Fibrose pulmonaire/prévention et contrôle , Récepteur de type I du facteur de croissance transformant bêta , Récepteurs TGF-bêta/génétique , Sclérodermie localisée/étiologie , Sclérodermie localisée/métabolisme , Sclérodermie systémique/induit chimiquement , Sclérodermie systémique/métabolisme , Sclérodermie systémique/anatomopathologie , Peau/métabolisme , Facteur de croissance transformant bêta/métabolismeRÉSUMÉ
Blockade of aberrant Wnt signaling is an attractive therapeutic approach in multiple cancers. We developed and performed a cellular high-throughput screen for inhibitors of Wnt secretion and pathway activation. A lead structure (GNF-1331) was identified from the screen. Further studies identified the molecular target of GNF-1331 as Porcupine, a membrane bound O-acyl transferase. Structure-activity relationship studies led to the discovery of a novel series of potent and selective Porcupine inhibitors. Compound 19, GNF-6231, demonstrated excellent pathway inhibition and induced robust antitumor efficacy in a mouse MMTV-WNT1 xenograft tumor model.
RÉSUMÉ
Emerging approaches to treat immune disorders target positive regulatory kinases downstream of antigen receptors with small molecule inhibitors. Here we provide evidence for an alternative approach in which inhibition of the negative regulatory inositol kinase Itpkb in mature T lymphocytes results in enhanced intracellular calcium levels following antigen receptor activation leading to T cell death. Using Itpkb conditional knockout mice and LMW Itpkb inhibitors these studies reveal that Itpkb through its product IP4 inhibits the Orai1/Stim1 calcium channel on lymphocytes. Pharmacological inhibition or genetic deletion of Itpkb results in elevated intracellular Ca2+ and induction of FasL and Bim resulting in T cell apoptosis. Deletion of Itpkb or treatment with Itpkb inhibitors blocks T-cell dependent antibody responses in vivo and prevents T cell driven arthritis in rats. These data identify Itpkb as an essential mediator of T cell activation and suggest Itpkb inhibition as a novel approach to treat autoimmune disease.
Sujet(s)
Maladies auto-immunes/enzymologie , Maladies auto-immunes/thérapie , Lymphocytes T CD4+/métabolisme , Signalisation calcique , Phosphotransferases (Alcohol Group Acceptor)/antagonistes et inhibiteurs , Animaux , Apoptose/effets des médicaments et des substances chimiques , Apoptose/génétique , Maladies auto-immunes/anatomopathologie , Lymphocytes T CD4+/effets des médicaments et des substances chimiques , Lymphocytes T CD4+/immunologie , Canaux calciques/métabolisme , Signalisation calcique/effets des médicaments et des substances chimiques , Signalisation calcique/génétique , Régulation de l'expression des gènes/effets des médicaments et des substances chimiques , Cellules HEK293 , Humains , Inositol phosphates/métabolisme , Cellules Jurkat , Souris de lignée C57BL , Souris knockout , Protéine ORAI1 , Phosphotransferases (Alcohol Group Acceptor)/métabolisme , Inhibiteurs de protéines kinases/pharmacologie , Rats de lignée LEWRÉSUMÉ
Deregulated kinase activities of tropomyosin receptor kinase (TRK) family members have been shown to be associated with tumorigenesis and poor prognosis in a variety of cancer types. In particular, several chromosomal rearrangements involving TRKA have been reported in colorectal, papillary thyroid, glioblastoma, melanoma, and lung tissue that are believed to be the key oncogenic driver in these tumors. By screening the Novartis compound collection, a novel imidazopyridazine TRK inhibitor was identified that served as a launching point for drug optimization. Structure guided drug design led to the identification of (R)-2-phenylpyrrolidine substituted imidazopyridazines as a series of potent, selective, orally bioavailable pan-TRK inhibitors achieving tumor regression in rats bearing KM12 xenografts. From this work the (R)-2-phenylpyrrolidine has emerged as an ideal moiety to incorporate in bicyclic TRK inhibitors by virtue of its shape complementarity to the hydrophobic pocket of TRKs.
RÉSUMÉ
Systematic SAR optimization of the GPR119 agonist lead 1, derived from an internal HTS campaign, led to compound 29. Compound 29 displays significantly improved in vitro activity and oral exposure, leading to GLP1 elevation in acutely dosed mice and reduced glucose excursion in an OGTT study in rats at doses ⩾10 mg/kg.
Sujet(s)
Pyrimidines/synthèse chimique , Récepteurs couplés aux protéines G/effets des médicaments et des substances chimiques , Animaux , Découverte de médicament , Souris , Structure moléculaire , Rats , Relation structure-activitéRÉSUMÉ
Screening hit 5 was identified in a biochemical screen for GPR119 agonists. Compound 5 was structurally novel, displayed modest biochemical activity and no oral exposure, but was structurally distinct from typical GPR119 agonist scaffolds. Systematic optimization led to compound 36 with significantly improved in vitro activity and oral exposure, to elevate GLP1 acutely in an in vivo mouse model at a dose of 10mg/kg.
Sujet(s)
Pyrazoles/pharmacologie , Pyrimidines/pharmacologie , Récepteurs couplés aux protéines G/agonistes , Animaux , Diabète de type 2/traitement médicamenteux , Humains , Hypoglycémiants/composition chimique , Hypoglycémiants/pharmacologie , Souris , Souris de lignée C57BL , Pyrazoles/composition chimique , Pyrimidines/composition chimique , Relation structure-activitéRÉSUMÉ
Activation of the G-protein coupled receptor (GPCR) Takeda G-protein receptor 5 (TGR5), also known as G-protein bile acid receptor 1 (GPBAR1), has been shown to play a key role in pathways associated with diabetes, metabolic syndrome, and autoimmune disease. Nipecotamide 5 was identified as an attractive starting point after a high-throughput screen (HTS) for receptor agonists. A comprehensive hit-to-lead effort culminated in the discovery of 45h as a potent, selective, and bioavailable TGR5 agonist to test in preclinical metabolic disease models. In genetically obese mice (ob/ob), 45h was as effective as a dipeptidyl peptidase-4 (DPP-4) inhibitor at reducing peak glucose levels in an acute oral glucose tolerance test (OGTT), but this effect was lost upon chronic dosing.
Sujet(s)
Hypoglycémiants/synthèse chimique , Pipérazines/synthèse chimique , Récepteurs couplés aux protéines G/agonistes , Administration par voie orale , Animaux , Biodisponibilité , Découverte de médicament , Glucagon-like peptide 1/analyse , Humains , Hypoglycémiants/pharmacocinétique , Hypoglycémiants/pharmacologie , Mâle , Souris , Souris de lignée C57BL , Souris obèse , Pipérazines/pharmacologie , Relation structure-activitéRÉSUMÉ
Wnt signaling is one of the key oncogenic pathways in multiple cancers, and targeting this pathway is an attractive therapeutic approach. However, therapeutic success has been limited because of the lack of therapeutic agents for targets in the Wnt pathway and the lack of a defined patient population that would be sensitive to a Wnt inhibitor. We developed a screen for small molecules that block Wnt secretion. This effort led to the discovery of LGK974, a potent and specific small-molecule Porcupine (PORCN) inhibitor. PORCN is a membrane-bound O-acyltransferase that is required for and dedicated to palmitoylation of Wnt ligands, a necessary step in the processing of Wnt ligand secretion. We show that LGK974 potently inhibits Wnt signaling in vitro and in vivo, including reduction of the Wnt-dependent LRP6 phosphorylation and the expression of Wnt target genes, such as AXIN2. LGK974 is potent and efficacious in multiple tumor models at well-tolerated doses in vivo, including murine and rat mechanistic breast cancer models driven by MMTV-Wnt1 and a human head and neck squamous cell carcinoma model (HN30). We also show that head and neck cancer cell lines with loss-of-function mutations in the Notch signaling pathway have a high response rate to LGK974. Together, these findings provide both a strategy and tools for targeting Wnt-driven cancers through the inhibition of PORCN.
Sujet(s)
Protéines membranaires/antagonistes et inhibiteurs , Tumeurs/traitement médicamenteux , Pyrazines/pharmacologie , Pyridines/pharmacologie , Voie de signalisation Wnt/effets des médicaments et des substances chimiques , Acyltransferases , Animaux , Axine/antagonistes et inhibiteurs , Technique de Western , Lignée cellulaire tumorale , Clonage moléculaire , Tests de criblage à haut débit , Humains , Souris , Mutagenèse , Phosphorylation/effets des médicaments et des substances chimiques , Pyrazines/usage thérapeutique , Pyridines/usage thérapeutique , Dosage par compétition , Rats , Récepteurs Notch/génétique , RT-PCRRÉSUMÉ
The synthesis, preclinical profile, and in vivo efficacy in rat xenograft models of the novel and selective anaplastic lymphoma kinase inhibitor 15b (LDK378) are described. In this initial report, preliminary structure-activity relationships (SARs) are described as well as the rational design strategy employed to overcome the development deficiencies of the first generation ALK inhibitor 4 (TAE684). Compound 15b is currently in phase 1 and phase 2 clinical trials with substantial antitumor activity being observed in ALK-positive cancer patients.
Sujet(s)
Tumeurs/traitement médicamenteux , Inhibiteurs de protéines kinases/synthèse chimique , Pyrimidines/synthèse chimique , Récepteurs à activité tyrosine kinase/antagonistes et inhibiteurs , Sulfones/synthèse chimique , Kinase du lymphome anaplasique , Animaux , Essais cliniques de phase I comme sujet , Essais cliniques de phase II comme sujet , Chiens , Humains , Macaca fascicularis , Mâle , Inhibiteurs de protéines kinases/pharmacocinétique , Inhibiteurs de protéines kinases/usage thérapeutique , Pyrimidines/pharmacocinétique , Pyrimidines/usage thérapeutique , Rats , Relation structure-activité , Sulfones/pharmacocinétique , Sulfones/usage thérapeutique , Tests d'activité antitumorale sur modèle de xénogreffeRÉSUMÉ
Neurotrophins and their receptors (TRKs) play key roles in the development of the nervous system and the maintenance of the neural network. Accumulating evidence points to their role in malignant transformations, chemotaxis, metastasis, and survival signaling and may contribute to the pathogenesis of a variety of tumors of both neural and non-neural origin. By screening the GNF kinase collection, a series of novel oxindole inhibitors of TRKs were identified. Optimization led to the identification of GNF-5837 (22), a potent, selective, and orally bioavailable pan-TRK inhibitor that inhibited tumor growth in a mouse xenograft model derived from RIE cells expressing both TRKA and NGF. The properties of 22 make it a good tool for the elucidation of TRK biology in cancer and other nononcology indications.
RÉSUMÉ
Pharmacologic antagonism of cannabinoid 1 receptors (CB1 receptors) in the central nervous system (CNS) suppresses food intake, promotes weight loss, and improves the metabolic profile. Since the CB1 receptor is expressed both in the CNS and in peripheral tissues, therapeutic value may be gained with CB1 receptor inverse agonists acting on receptors in both domains. The present report examines the metabolic and CNS actions of a novel CB1 receptor inverse agonist, compound 64, a 1,5,6-trisubstituted pyrazolopyrimidinone. Compound 64 showed similar or superior binding affinity, in vitro potency, and pharmacokinetic profile compared to rimonabant. Both compounds improved the metabolic profile in diet-induced obese (DIO) rats and obese cynomolgus monkeys. Weight loss tended to be greater in compound 64-treated DIO rats compared to pair-fed counterparts, suggesting that compound 64 may have metabolic effects beyond those elicited by weight loss alone. In the CNS, reversal of agonist-induced hypothermia and hypolocomotion indicated that compound 64 possessed an antagonist activity in vivo. Dosed alone, compound 64 suppressed extinction of conditioned freezing (10 mg/kg) and rapid eye movement (REM) sleep (30 mg/kg), consistent with previous reports for rimonabant, although for REM sleep, compound 64 was greater than threefold less potent than for metabolic effects. Together, these data suggested that (1) impairment of extinction learning and REM sleep suppression are classic, centrally mediated responses to CB1 receptor inverse agonists, and (2) some separation may be achievable between central and peripheral effects with brain-penetrating CB1 receptor inverse agonists while maintaining metabolic efficacy. Furthermore, chronic treatment with compound 64 contributes to evidence that peripheral CB1 receptor blockade may yield beneficial outcomes that exceed those elicited by weight loss alone.
Sujet(s)
Obésité/traitement médicamenteux , Pipéridines/pharmacologie , Pyrazoles/pharmacologie , Pyrimidinones/pharmacologie , Récepteur cannabinoïde de type CB1/antagonistes et inhibiteurs , Animaux , Encéphale/métabolisme , Relation dose-effet des médicaments , Agonisme inverse des médicaments , Extinction (psychologie)/effets des médicaments et des substances chimiques , Macaca fascicularis , Mâle , Souris , Souris de lignée C57BL , Activité motrice/effets des médicaments et des substances chimiques , Obésité/métabolisme , Pipéridines/pharmacocinétique , Pyrazoles/administration et posologie , Pyrazoles/pharmacocinétique , Pyrimidinones/administration et posologie , Pyrimidinones/pharmacocinétique , Rats , Rat Sprague-Dawley , Rimonabant , Sommeil paradoxal/effets des médicaments et des substances chimiques , Distribution tissulaireRÉSUMÉ
The discovery, synthesis, and optimization of compound 1 from a high-throughput screening hit to highly potent and selective peroxisome proliferator-activated receptor delta (PPARdelta) agonists are reported. The synthesis and structure-activity relationship in this series are described in detail. On the basis of a general schematic PPAR pharmacophore model, scaffold 1 was divided into headgroup, linker, and tailgroup and successively optimized for PPAR activation using in vitro PPAR transactivation assays. A (2-methylphenoxy)acetic acid headgroup, a flexible linker, and a five-membered heteroaromatic center ring with two hydrophobic aryl substituents were required for efficient and selective PPARdelta activation. The fine-tuning of these aryl substituents led to an array of highly potent and selective compounds such as compound 38c, displaying an excellent pharmacokinetic profile in mouse. In an in vivo acute dosing model, selected members of this array were shown to induce the expression of pyruvate dehydrogenase kinase-4 (PDK4) and uncoupling protein-3 (UCP3), genes that are known to be involved in energy homeostasis and regulated by PPARdelta in skeletal muscle.
Sujet(s)
Oxazoles/pharmacologie , Récepteur PPAR delta/agonistes , Thiazoles/pharmacologie , Animaux , Évaluation préclinique de médicament , Transfert d'énergie par résonance de fluorescence , Tests de criblage à haut débit , Humains , Mâle , Souris , Souris de lignée BALB C , Souris de lignée C57BL , Structure moléculaire , Oxazoles/synthèse chimique , Oxazoles/composition chimique , Récepteur PPAR delta/génétique , Stéréoisomérie , Relation structure-activité , Thiazoles/synthèse chimique , Thiazoles/composition chimiqueRÉSUMÉ
A series of 4-amino-6-benzimidazole-pyrimidines was designed to target lymphocyte-specific tyrosine kinase (Lck), a member of the Src-family kinases (SFKs). These type II inhibitors were optimized using a cellular Lck-dependent proliferation assay and are capable of inhibiting Lck at single-digit nanomolar concentrations. This scaffold is likely to serve a valuable template for developing potent inhibitors of a number of SFKs.
Sujet(s)
Benzimidazoles/pharmacologie , Découverte de médicament , Protéine tyrosine kinase p56(lck) spécifique des lymphocytes/antagonistes et inhibiteurs , Inhibiteurs de protéines kinases/pharmacologie , Pyrimidines/pharmacologie , Animaux , Benzimidazoles/synthèse chimique , Benzimidazoles/composition chimique , Lignée cellulaire , Prolifération cellulaire/effets des médicaments et des substances chimiques , Conception de médicament , Souris , Modèles moléculaires , Structure moléculaire , Inhibiteurs de protéines kinases/synthèse chimique , Inhibiteurs de protéines kinases/composition chimique , Pyrimidines/synthèse chimique , Pyrimidines/composition chimique , Stéréoisomérie , Relation structure-activitéRÉSUMÉ
A novel series of benzo[a]carbazole-based small molecule agonists of the thrombopoietin (Tpo) receptor is reported. Starting from a 3.4 microM high throughput screen hit, members of this series have been identified which are full agonists with functional potency <50 nM and oral bioavailability in mice.
Sujet(s)
Dérivés du benzène/synthèse chimique , Dérivés du benzène/pharmacologie , Carbazoles/synthèse chimique , Carbazoles/pharmacologie , Récepteurs à la thrombopoïétine/agonistes , Thrombopoïétine , Administration par voie orale , Animaux , Dérivés du benzène/composition chimique , Carbazoles/composition chimique , Techniques de chimie combinatoire , Conception de médicament , Humains , Souris , Structure moléculaire , Résonance magnétique nucléaire biomoléculaire , Récepteurs à la thrombopoïétine/composition chimique , Relation structure-activité , Thrombopoïétine/composition chimique , Thrombopoïétine/métabolismeRÉSUMÉ
The lead optimization of a novel series of benzo[a]carbazole-based small molecule agonists of the thrombopoietin (Tpo) receptor is reported. The chemical instability of the dihydro-benzo[a]carbazole lead 2 was successfully addressed in the design and evaluation of compounds which also demonstrated improved potency compared to 2. Members of the scaffold have been identified which are full agonists that demonstrate cellular functional potency <50 nM. Analog 21 demonstrates equivalent efficacy in the human megakaryocyte differentiation (CFU-mega) assay compared to Eltrombopag.
Sujet(s)
Dérivés du benzène/synthèse chimique , Dérivés du benzène/pharmacologie , Carbazoles/synthèse chimique , Carbazoles/pharmacologie , Récepteurs à la thrombopoïétine/agonistes , Thrombopoïétine , Dérivés du benzène/composition chimique , Carbazoles/composition chimique , Techniques de chimie combinatoire , Conception de médicament , Humains , Concentration inhibitrice 50 , Mégacaryocytes/métabolisme , Structure moléculaire , Résonance magnétique nucléaire biomoléculaire , Récepteurs à la thrombopoïétine/composition chimique , Relation structure-activité , Thrombopoïétine/composition chimique , Thrombopoïétine/métabolismeRÉSUMÉ
We have identified a novel liver X receptor (LXR) agonist (2) that activates the LXRbeta subtype with selectivity over LXRalpha. LXRbeta selectivity was confirmed using macrophages derived from LXR mutant mice. Despite its selectivity and modest potency, the compound can induce APO-AI-dependent cholesterol efflux from macrophages with full efficacy. Our results indicate that it is possible to achieve significant LXRbeta selectivity in a small molecule while maintaining functional LXR activity.