ABSTRACT
Fibrosis of the lung constitutes a major clinical challenge and novel therapies are required to alleviate the associated morbidity and mortality. Investigating the antifibrotic efficacy of drugs that are already in clinical practice offers an efficient strategy to identify new therapies. The phosphodiesterase 4 (PDE4) inhibitors, approved for the treatment of chronic obstructive pulmonary disease, harbor therapeutic potential for pulmonary fibrosis by augmenting the activity of endogenous antifibrotic mediators that signal through cyclic AMP. In this study, we tested the efficacy of several PDE4 inhibitors including a novel compound (Compound 1) in a murine model of lung fibrosis that results from a targeted type II alveolar epithelial cell injury. We also compared the antifibrotic activity of PDE4 inhibition to the two therapies that are FDA-approved for idiopathic pulmonary fibrosis (pirfenidone and nintedanib). We found that both preventative (day 0-21) and therapeutic (day 11-21) dosing regimens of the PDE4 inhibitors significantly ameliorated the weight loss and lung collagen accumulation that are the sequelae of targeted epithelial cell damage. In a therapeutic protocol, the reduction in lung fibrosis with PDE4 inhibitor administration was equivalent to pirfenidone and nintedanib. Treatment with this class of drugs also resulted in a decrease in plasma surfactant protein D concentration, a reduction in the plasma levels of several chemokines implicated in lung fibrosis, and an in vitro inhibition of fibroblast profibrotic gene expression. These results motivate further investigation of PDE4 inhibition as a treatment for patients with fibrotic lung disease.
Subject(s)
Alveolar Epithelial Cells/pathology , Benzamides/therapeutic use , Isoquinolines/therapeutic use , Phosphodiesterase 4 Inhibitors/therapeutic use , Pulmonary Fibrosis/drug therapy , Aminopyridines/therapeutic use , Animals , Benzamides/administration & dosage , Benzamides/blood , Cells, Cultured , Chemokines/blood , Cyclic AMP/metabolism , Cyclopropanes/therapeutic use , Dose-Response Relationship, Drug , Drug Evaluation, Preclinical/methods , Fibroblasts/metabolism , Humans , Isoquinolines/administration & dosage , Isoquinolines/blood , Mice, Inbred C57BL , Mice, Transgenic , Phosphodiesterase 4 Inhibitors/administration & dosage , Phosphodiesterase 4 Inhibitors/blood , Pulmonary Fibrosis/blood , Pulmonary Fibrosis/prevention & control , Pulmonary Surfactant-Associated Protein D/blood , Pyridines/therapeutic use , Tumor Necrosis Factor-alpha/metabolismABSTRACT
Many of the drugs currently marketed for the treatment of schizophrenia are dopamine D2 receptor antagonists or partial agonists with or without mixed receptor pharmacology, and primarily treat the positive symptoms of schizophrenia. These drugs, depending on their pharmacological profile, have been categorized as typical (with low or no serotonergic component) and atypical (with a high serotonergic, 5-HT2A and 5-HT1A component) antipsychotics. Atypical antipsychotics have increased tolerability compared with typical antipsychotics, particularly against extrapyramidal side effects which are caused by D2 receptor antagonism, and an increased efficacy for the treatment of the negative symptoms associated with schizophrenia. However, over the course of treatment, adverse effects such as weight gain, metabolic disorders, QT prolongation and sexual dysfunction have been observed, and thus current research efforts are being directed to the identification of new antipsychotics that have better tolerability and efficacy against the positive and negative symptoms of schizophrenia.
Subject(s)
Antipsychotic Agents/therapeutic use , Dopamine/metabolism , Schizophrenia/drug therapy , Antipsychotic Agents/classification , Antipsychotic Agents/pharmacology , Dopamine Agonists/therapeutic use , Humans , Schizophrenia/metabolismABSTRACT
There is growing pressure to find more effective therapies for major psychiatric disorders, such as schizophrenia and depressive disorder. The repeated disappointments that have been experienced with highly selective, single-target agents have prompted questions about their relative merits. In contrast, a multi-target agent (MTA) approach, discovered either by serendipity or by judicious design, might offer a more rational way to address the complex clinical demands of patients and their co-morbidities. Rather than being mutually exclusive, a balanced portfolio of the two approaches may offer a beneficial and synergistic outcome toward identification of novel antipsychotic and antidepressant therapies. With improvements in biomarker technology, translational biology and a growing understanding of psychopathology, there is optimism that the new generation of MTAs will finally shed the stigma of 'dirty drugs' and progress to the concept of intentionally designed and tailored psychopharmacological agents.
Subject(s)
Antipsychotic Agents/therapeutic use , Depressive Disorder, Major/drug therapy , Schizophrenia/drug therapy , Antidepressive Agents/pharmacology , Antidepressive Agents/therapeutic use , Antipsychotic Agents/pharmacology , Drug Design , HumansABSTRACT
As part of an on-going effort to investigate the chemical space requirements for D(2)/5-HT(2A) receptor antagonists as atypical antipsychotics, new 1-aminoindanes were synthesized. The replacement of the heterocycle (oxindole) in ziprasidone with a carbocycle (indane) was well tolerated and was found to retain binding affinities for dopamine D(2), serotonin 5-HT(2A), and serotonin 5-HT(1A). Such compounds hold promise as a new chemical motif with atypical antipsychotic properties for the treatment of schizophrenia and related disorders.
Subject(s)
Antipsychotic Agents/pharmacology , Indans/pharmacology , Antipsychotic Agents/chemistry , Antipsychotic Agents/metabolism , ERG1 Potassium Channel , Ether-A-Go-Go Potassium Channels/drug effects , Humans , Indans/chemistry , Indans/metabolism , Molecular Structure , Receptor, Serotonin, 5-HT1A/metabolism , Receptor, Serotonin, 5-HT2A/metabolism , Receptors, Dopamine D2/metabolismABSTRACT
Compound 1a (6-chloro-5-{3-[4-(1H-indazol-3-yl)-piperazin-1-yl]-propyl}-3,3-dimethyl-1,3-dihydro-indol-2-one) was mutagenic to Salmonella typhimurium TA98 in the presence of rat liver S9 subcellular fraction. The metabolism of 1a in rat liver S9 or microsomes demonstrated that it underwent a P450-mediated N-deindazolation (loss of indazole ring) as a predominant metabolic pathway. To investigate a possible link between metabolism and mutagenicity, a structural analogue 1b (6-chloro-5-{3-[4-(1H-indazol-3-yl)-piperidin-1-yl]-propyl}-3,3-dimethyl-1,3-dihydro-indol-2-one), the cleaved product 2a (6-chloro-3,3-dimethyl-5-(3-piperazin-1-yl-propyl)-1,3-dihydro-indol-2-one), and the core motif 3a (3-piperazinyl indazole) were evaluated in the Ames assay. It was found that 1b was not mutagenic to Salmonella typhimurium TA98 in the absence or presence of a metabolic activating system. In contrast to 1a, 1b did not undergo the metabolic cleavage (loss of indazole ring). Marginal mutagenicity of 2a to TA98 was observed with rat liver S9, whereas 3a was shown to be a promutagen. It was further demonstrated that 1a inactivated P450 3A, the principle enzyme catalyzing the N-deindazolation reaction, in an NADPH-, time-, and concentration-dependent manner. The kinetics of inactivation was characterized by a K(I) of 8.1 microM and k(inact) of 0.114 min(-1). The differences in mutagenicity between 1a and 1b suggest that a chemical bond extending from the 3-position of the indazole to a heteroatom (as part of another cyclic ring) is a prerequisite for the toxicity. The metabolic process leading to the elimination of the indazole from the rest of the molecule apparently plays a key role in causing mutagenicity. It is postulated that the N-deindazolation of 1a proceeds via an oxaziridine intermediate, the formation of which is indirectly inferred from the presence of benzoic acid in microsomal incubations. Benzoic acid is thought to be derived from the hydrolysis of 3-indazolone, an unstable product generated from the oxaziridine. Evidence suggests that the electrophilic oxaziridine intermediate may be responsible for the mutagenicity and inactivation of P450 3A.
Subject(s)
Aziridines/metabolism , Cytochrome P-450 Enzyme System/metabolism , Indazoles/chemistry , Mutagenesis/genetics , Piperazines/chemistry , Animals , Aziridines/chemistry , Cytochrome P-450 Enzyme System/genetics , Enzyme Activation/drug effects , Indazoles/chemical synthesis , Indazoles/toxicity , Kinetics , Liver/drug effects , Liver/metabolism , Microsomes/drug effects , Microsomes/metabolism , Molecular Structure , Oxidation-Reduction , Piperazines/chemical synthesis , Piperazines/toxicity , Rats , Salmonella typhimurium/drug effects , Salmonella typhimurium/genetics , Structure-Activity Relationship , Testosterone/chemistry , Testosterone/metabolismABSTRACT
A series of 3-imino-2-indolones are the first published, high-affinity antagonists of the galanin GAL3 receptor. One example, 1,3-dihydro-1-phenyl-3-[[3-(trifluoromethyl)phenyl]imino]-2H-indol-2-one (9), was shown to have high affinity for the human GAL3 receptor (Ki=17 nM) and to be highly selective for GAL3 over a broad panel of targets, including GAL1 and GAL2. Compound 9 was also shown to be an antagonist in a human GAL3 receptor functional assay (Kb=29 nM).
Subject(s)
Imines/chemical synthesis , Indoles/chemical synthesis , Receptor, Galanin, Type 3/antagonists & inhibitors , Animals , Binding, Competitive , Brain/metabolism , COS Cells , Chlorocebus aethiops , Cyclic AMP/biosynthesis , Humans , Imines/pharmacokinetics , Imines/pharmacology , Indoles/pharmacokinetics , Indoles/pharmacology , Ligands , Radioligand Assay , Rats , Receptor, Galanin, Type 1/drug effects , Receptor, Galanin, Type 2/drug effects , Stereoisomerism , Structure-Activity RelationshipABSTRACT
A benzylpiperidine analogue with an acetylenic linker, 5-(3-[4-(4-fluorobenzyl)-piperidin-1-yl]-prop-1-ynyl)-1,3-dihydrobenzimidazol-2-one (3), was identified as a chemical lead with excellent activity at the NR1A/2B receptor (IC50=3 nM). Efforts to optimize this activity led to focused modifications around the structural motif of 3. The synthesis and SAR studies are discussed.
Subject(s)
Alkynes/chemistry , Excitatory Amino Acid Antagonists/chemistry , Receptors, N-Methyl-D-Aspartate/antagonists & inhibitors , Alkynes/metabolism , Alkynes/pharmacology , Animals , Brain/drug effects , Brain/metabolism , Drug Evaluation, Preclinical/methods , Excitatory Amino Acid Antagonists/metabolism , Excitatory Amino Acid Antagonists/pharmacology , Rats , Receptors, N-Methyl-D-Aspartate/metabolismABSTRACT
NR2B antagonists have received considerable attention in recent years. In this class of excitatory amino acid receptor antagonists NR2B antagonists have shown efficacy in neuroprotection, anti-hyperalgesic and anti-Parkinson animal models. Several groups are involved in developing these compounds as therapeutic agents and evaluating newer therapeutic targets for these agents. Until recently benzylpiperidine and phenylpiperidine templates, which were based on the structures of Ifenprodil and Eliprodil, formed the basis of most SAR in this area. A few chemical leads in this class such as CP-101,606, Ro25,6981 and PD0196860 have been identified as possible development leads which have generated significant interest in this area. In addition to the efforts of Pfizer (Parke-Davis), Roche and E.Merck, several other industrial and academic research groups have continued to work in the NR2B area and recently Merck and Roche have reported new chemical leads as NR2B antagonists with significantly different biaryl templates. These new advances have raised hope, for potential success of the NR2B antagonists as new therapeutic agents, for the treatment of several pathophysiological indications.
