ABSTRACT
A series of 1-indazol-3-(1-phenylpyrazol-5-yl)methyl ureas were investigated as hTRPV1 antagonists. The structure-activity relationship study was conducted systematically for both the indazole A-region and the 3-trifluoromethyl/t-butyl pyrazole C-region to optimize the antagonism toward the activation by capsaicin. Among them, the antagonists 26, 50 and 51 displayed highly potent antagonism with Ki(CAP) = 0.4-0.5 nM. Further, in vivo studies in mice indicated that these derivatives both antagonized capsaicin induced hypothermia, consistent with their in vitro activity, and themselves did not induce hyperthermia. In the formalin model, 51 showed anti-nociceptive activity in a dose-dependent manner.
Subject(s)
Indazoles/pharmacology , Methylurea Compounds/pharmacology , Pyrazoles/pharmacology , TRPV Cation Channels/antagonists & inhibitors , Analgesics/chemical synthesis , Analgesics/pharmacology , Animals , Body Temperature/drug effects , CHO Cells , Capsaicin/pharmacology , Cricetulus , Humans , Indazoles/chemical synthesis , Methylurea Compounds/chemical synthesis , Mice , Molecular Structure , Pyrazoles/chemical synthesis , Structure-Activity Relationship , TRPV Cation Channels/agonistsABSTRACT
Rapid hydrolysis of urea results in further fertilization frequency and excessive nitrogen (N) input. A modified urea, dimethylolurea (DMU), was synthesized in this study. The structure of the sample was characterized by Fourier transform infrared and nuclear magnetic resonance analysis, manifesting the formation of DMU. N release investigation confirmed that DMU enabling provided a gradual N supply. The N leaching experiment indicated that increasing the applied DMU significantly reduced the NH4+-N, NO3--N, and total N leaching, compared with urea application alone. The application effect on maize and wheat was evaluated. The results revealed that singly applied DMU with 100% or 80% N input, irrespective of the amount, promoted crop yield and agronomic characteristic and N use efficiency (NUE) of maize and wheat, beyond urea with two split applications at the recommended rate. Thus, the potential availability of DMU was proven; this could be widely used in agricultural fields as a slow-release fertilizer.
Subject(s)
Crops, Agricultural/growth & development , Fertilizers , Methylurea Compounds/administration & dosage , Nitrogen/administration & dosage , Agriculture/methods , Delayed-Action Preparations , Fertilizers/analysis , Methylurea Compounds/chemical synthesis , Methylurea Compounds/chemistry , Spectroscopy, Fourier Transform Infrared , Triticum/growth & development , Zea mays/growth & developmentABSTRACT
Functionally selective G protein-coupled receptor ligands are valuable tools for deciphering the roles of downstream signaling pathways that potentially contribute to therapeutic effects versus side effects. Recently, we discovered both Gi/o-biased and ß-arrestin2-biased D2 receptor agonists based on the Food and Drug Administration (FDA)-approved drug aripiprazole. In this work, based on another FDA-approved drug, cariprazine, we conducted a structure-functional selectivity relationship study and discovered compound 38 (MS1768) as a potent partial agonist that selectively activates the Gi/o pathway over ß-arrestin2. Unlike the dual D2R/D3R partial agonist cariprazine, compound 38 showed selective agonist activity for D2R over D3R. In fact, compound 38 exhibited potent antagonism of dopamine-stimulated ß-arrestin2 recruitment. In our docking studies, compound 38 directly interacts with S1935.42 on TM5 but has no interactions with extracellular loop 2, which appears to be in contrast to the binding poses of D2R ß-arrestin2-biased ligands. In in vivo studies, compound 38 showed high D2R receptor occupancy in mice and effectively inhibited phencyclidine-induced hyperlocomotion.
Subject(s)
Dopamine Agonists/pharmacology , GTP-Binding Protein alpha Subunits, Gi-Go/metabolism , Isoquinolines/pharmacology , Methylurea Compounds/pharmacology , Receptors, Dopamine D2/agonists , Animals , Antipsychotic Agents/chemical synthesis , Antipsychotic Agents/metabolism , Antipsychotic Agents/pharmacology , Dopamine Agonists/chemical synthesis , Dopamine Agonists/metabolism , Drug Design , Drug Partial Agonism , Female , HEK293 Cells , Humans , Isoquinolines/chemical synthesis , Isoquinolines/metabolism , Locomotion/drug effects , Male , Methylurea Compounds/chemical synthesis , Methylurea Compounds/metabolism , Mice, Inbred C57BL , Molecular Docking Simulation , Molecular Structure , Piperazines/chemistry , Receptors, Dopamine D2/metabolism , Signal Transduction/drug effects , Structure-Activity Relationship , beta-Arrestin 2/metabolismABSTRACT
By varying the molecular charge, shape and amphiphilicity of a series of conformationally distinct diarylureas it is possible to control the levels of phospholipid membrane lysis using membranes composed of bacterial lipid extracts. From the data obtained, it appears as though the lysis activity observed is not due to charge, conformation or amphiphilicity in isolation, but that surface aggregation, H-bonding and other factors may also play a part. The work provides evidence that this class of foldamer possesses potential for optimisation into new antibacterial agents.
Subject(s)
Anti-Bacterial Agents/pharmacology , Cell Membrane/drug effects , Methylurea Compounds/pharmacology , Phenylurea Compounds/pharmacology , Surface-Active Agents/pharmacology , Anti-Bacterial Agents/chemical synthesis , Anti-Bacterial Agents/chemistry , Cell Membrane/metabolism , Cell Membrane Permeability , Escherichia coli/drug effects , Methylurea Compounds/chemical synthesis , Methylurea Compounds/chemistry , Molecular Conformation , Molecular Structure , Phenylurea Compounds/chemical synthesis , Phenylurea Compounds/chemistry , Polymyxin B/pharmacology , Staphylococcus aureus/drug effects , Surface-Active Agents/chemical synthesis , Surface-Active Agents/chemistryABSTRACT
Novel 1-(1,3-disubstituted-imidazolidyn-2-ylidene)-3-ethoxycarbonylmethylurea derivatives (3a-3j) were obtained from appropriate 1-aryl-3-arylsulfonyl-1H-imidazolidine-2-imines (1a-1j) and ethyl isocyanatoacetate (2), which were subjected to condensation. Seven compounds were tested for their antiviral activity against HSV-1 and CVB3 viruses. Among the tested compounds, 3c was found to be active against HSV-1, proving that 4-methoxy substituent as R and 4-methyl substituent as R1 are most beneficial for activity against this virus. Furthermore, 3e and 3g were active against CVB3, which demonstrated that both 4-methyl and 4-chloro substitution is tolerated as R1, whereas 4-chloro and 2-methoxy substituents are best as R. It was also shown that the active compounds are characterized by relatively big surface area, small ovality, and greatest HOMO and LUMO energies in comparison to the rest of the compounds.
Subject(s)
Antiviral Agents/chemical synthesis , Antiviral Agents/pharmacology , Enterovirus B, Human/drug effects , Herpesvirus 1, Human/drug effects , Methylurea Compounds/pharmacology , Antiviral Agents/chemistry , Dose-Response Relationship, Drug , Methylurea Compounds/chemical synthesis , Methylurea Compounds/chemistry , Microbial Sensitivity Tests , Structure-Activity RelationshipABSTRACT
Emerging drug resistance and other drawbacks limit tubulin inhibitors' therapeutic applications and developing novel tubulin inhibitors still attracts intensive efforts. We describe the discovery and structure-activity relationship study of a series of benzimidazole-2-urea derivatives as novel ß tubulin inhibitors. The representative compound 6o potently suppressed the proliferation of a panel of human cancer cells (NCI-H460, Colo205, K562, A431, HepG2, Hela, MDA-MB-435S) with IC50 values of 0.040, 0.050, 0.006, 0.026, 1.774, 0.452 and 0.052 µM, respectively. Compound 6o obviously inhibited NCI-H460 spindles formation and induced cell cycle arrest at G2/M phase at 0.10 µM. Computational study suggested that 6o interacts with ß tubulin in a novel binding mode. Our results suggested that benzimidazole-2-urea derivatives might be promising tubulin inhibitors with novel binding mode for further development.
Subject(s)
Antineoplastic Agents/pharmacology , Benzimidazoles/pharmacology , Methylurea Compounds/pharmacology , Tubulin Modulators/chemistry , Tubulin Modulators/pharmacology , Tubulin/metabolism , Antineoplastic Agents/chemical synthesis , Antineoplastic Agents/chemistry , Benzimidazoles/chemical synthesis , Benzimidazoles/chemistry , Cell Cycle Checkpoints/drug effects , Cell Division/drug effects , Cell Line, Tumor , Cell Proliferation/drug effects , Dose-Response Relationship, Drug , Drug Screening Assays, Antitumor , G2 Phase/drug effects , HeLa Cells , Hep G2 Cells , Humans , K562 Cells , Methylurea Compounds/chemical synthesis , Methylurea Compounds/chemistry , Models, Molecular , Molecular Structure , Structure-Activity Relationship , Tubulin Modulators/chemical synthesisABSTRACT
This paper describes the identification and optimization of a novel series of DFG-out binding p38 inhibitors as inhaled agents for the treatment of chronic obstructive pulmonary disease. Structure based drug design and "inhalation by design" principles have been applied to the optimization of the lead series exemplied by compound 1a. Analogues have been designed to be potent and selective for p38, with an emphasis on slow enzyme dissociation kinetics to deliver prolonged lung p38 inhibition. Pharmacokinetic properties were tuned with high intrinsic clearance and low oral bioavailability in mind, to minimize systemic exposure and reduce systemically driven adverse events. High CYP mediated clearance and glucuronidation were targeted to achieve high intrinsic clearance coupled with multiple routes of clearance to minimize drug-drug interactions. Furthermore, pharmaceutical properties such as stability, crystallinity, and solubility were considered to ensure compatibility with a dry powder inhaler. 1ab (PF-03715455) was subsequently identified as a clinical candidate from this series with efficacy and safety profiles confirming its potential as an inhaled agent for the treatment of COPD.
Subject(s)
Anti-Inflammatory Agents, Non-Steroidal/chemical synthesis , Azabicyclo Compounds/chemical synthesis , Methylurea Compounds/chemical synthesis , Pulmonary Disease, Chronic Obstructive/drug therapy , Pyrazoles/chemical synthesis , p38 Mitogen-Activated Protein Kinases/antagonists & inhibitors , Administration, Inhalation , Animals , Anti-Inflammatory Agents, Non-Steroidal/pharmacokinetics , Anti-Inflammatory Agents, Non-Steroidal/pharmacology , Azabicyclo Compounds/pharmacokinetics , Azabicyclo Compounds/pharmacology , Binding Sites , Cell Membrane Permeability , Crystallography, X-Ray , Dogs , Drug Stability , Humans , In Vitro Techniques , Kinetics , Leukocytes, Mononuclear/drug effects , Leukocytes, Mononuclear/metabolism , Methylurea Compounds/pharmacokinetics , Methylurea Compounds/pharmacology , Models, Molecular , Protein Binding , Protein Conformation , Pyrazoles/pharmacokinetics , Pyrazoles/pharmacology , Rats , Solubility , Surface Plasmon Resonance , Tumor Necrosis Factor-alpha/biosynthesis , p38 Mitogen-Activated Protein Kinases/chemistryABSTRACT
The carbamoylating agents carbamoyl azides and carbamoyl cyanides (aka cyanoformamides) react with hydroxylamine in different ways, leading in the first case to N-hydroxyureas and, in the case of carbamoyl cyanides, to carbamoyl amidoxime derivatives. The synthetic procedure developed for the latter type of compound, which represents an interesting precursor for heterocyclic structures, allowed the highly efficient preparation of a wide selection of examples. The Z configuration of the double bond in the amidoxime moiety was proposed on the basis of comparison between experimental and calculated (13)C and (15)N NMR chemical shift values for the isopropyl and benzyl derivatives.
Subject(s)
Antineoplastic Agents/chemical synthesis , Azides/chemistry , Chelating Agents/chemistry , Formamides/chemistry , Hydroxylamine/chemistry , Methylurea Compounds/chemistry , Methylurea Compounds/chemical synthesis , Oximes/chemistry , Antineoplastic Agents/chemistry , Magnetic Resonance Spectroscopy , Molecular StructureABSTRACT
A preliminary library of novel N(6),5'-bis-ureidoadenosine analogs and related derivatives was prepared and tested for activity against the NCI 60 panel of human cancers. A 2'-O-TBS group was found to be necessary, but not sufficient, for optimal antiproliferative activity. Neither the N(6)- nor 5'-ureido substituents were sufficient to achieve significant antiproliferative effects when present in the absence of the other. The 2'-O-TBS, and N(6),5'-bis-ureido substitution patterns were found to be necessary for optimal antiproliferative activity.
Subject(s)
Adenosine/analogs & derivatives , Antineoplastic Agents/pharmacology , Methylurea Compounds/pharmacology , Adenosine/chemical synthesis , Adenosine/chemistry , Adenosine/pharmacology , Antineoplastic Agents/chemical synthesis , Antineoplastic Agents/chemistry , Cell Line, Tumor , Cell Proliferation/drug effects , Drug Screening Assays, Antitumor , Humans , Methylurea Compounds/chemical synthesis , Methylurea Compounds/chemistry , Molecular Structure , Stereoisomerism , Structure-Activity RelationshipABSTRACT
A family of 1,4-diarylpiperidine-4-methylureas were designed and synthesized as novel dual effectors on ACAT and LDL receptor expression. We examined SAR of the synthesized compounds focusing on substitution at the three aromatic parts of the starting compound 1 and succeeded in identifying essential substituents for inhibition of ACAT and up-regulation of hepatic LDL receptor expression. Especially, we found that compound 12f, which can easily be prepared, has biological properties comparable to those of SMP-797, a promising ACAT inhibitor. In addition, the in vitro effects of 12f on lipid metabolism were substantially superior to those of a known ACAT inhibitor, Avasimibe.
Subject(s)
Methylurea Compounds/chemical synthesis , Methylurea Compounds/pharmacology , Naphthyridines/pharmacology , Piperidines/chemical synthesis , Piperidines/pharmacology , Receptors, LDL/drug effects , Sterol O-Acyltransferase/drug effects , Combinatorial Chemistry Techniques , Humans , Methylurea Compounds/chemistry , Molecular Structure , Naphthyridines/chemistry , Piperidines/chemistry , Sterol O-Acyltransferase/antagonists & inhibitors , Structure-Activity RelationshipABSTRACT
Infections caused by hepatitis C virus (HCV) are a significant world health problem for which novel therapies are in urgent demand. The polymerase of HCV is responsible for the replication of viral RNA. We recently disclosed dihydroxypyrimidine carboxylates 2 as novel, reversible inhibitors of the HCV NS5B polymerase. This series was further developed into 5,6-dihydroxy-2-(2-thienyl)pyrimidine-4-carboxylic acids such as 34 (EC50 9.3 microM), which now show activity in the cell-based HCV replication assay. The structure-activity relationship of these inhibitors is discussed in the context of their physicochemical properties and of the polymerase crystal structure. We also report the results of mutagenesis experiments which support the proposed binding model, which involves pyrophosphate-like chelation of the active site Mg ions.
Subject(s)
Antiviral Agents/chemical synthesis , Hepacivirus/drug effects , Hepacivirus/enzymology , Methylurea Compounds/chemical synthesis , Models, Molecular , Pyrimidines/chemical synthesis , Thiophenes/chemical synthesis , Viral Nonstructural Proteins/antagonists & inhibitors , Viral Nonstructural Proteins/genetics , Antiviral Agents/chemistry , Antiviral Agents/pharmacology , Binding Sites , Cell Line , Chelating Agents/chemistry , Crystallization , Humans , Methylurea Compounds/chemistry , Methylurea Compounds/pharmacology , Mutagenesis , Protein Conformation , Pyrimidines/chemistry , Pyrimidines/pharmacology , Structure-Activity Relationship , Thiophenes/chemistry , Thiophenes/pharmacology , Viral Nonstructural Proteins/chemistry , Virus Replication/drug effectsABSTRACT
Pathogenic enterococci are becoming resistant to currently available antibiotics, including vancomycin, the drug of last resort for Gram-positive infections. Enterococci pose a significant public health threat, not least because of the risk of transferring vancomycin resistance to the ubiquitous Staphylococcus aureus. Vancomycin resistance is manifested by cell wall peptidoglycan precursors with altered termini that cannot bind the antibiotic. Small molecules with well-oriented nucleophile-electrophile assembly and complementary chirality to the peptidoglycan termini were identified as catalytic and selective cleavers of the peptidoglycan precursor depsipeptide. These molecules were tested in combination with vancomycin and were found to re-sensitize vancomycin-resistant bacteria to the antibiotic.
Subject(s)
Alanine/metabolism , Enterococcus/drug effects , Lactates/metabolism , Peptidoglycan/metabolism , Pyrrolidines/pharmacology , Vancomycin/pharmacology , Alanine/analogs & derivatives , Anti-Bacterial Agents/chemical synthesis , Anti-Bacterial Agents/chemistry , Anti-Bacterial Agents/metabolism , Anti-Bacterial Agents/pharmacology , Catalysis , Combinatorial Chemistry Techniques , Computer Simulation , Drug Design , Drug Synergism , Enterococcus/metabolism , Enterococcus faecalis/drug effects , Enterococcus faecalis/metabolism , Enterococcus faecium/drug effects , Enterococcus faecium/metabolism , Hydrolysis , Methylurea Compounds/chemical synthesis , Methylurea Compounds/metabolism , Methylurea Compounds/pharmacology , Microbial Sensitivity Tests , Models, Molecular , Oligopeptides/chemical synthesis , Oligopeptides/metabolism , Oligopeptides/pharmacology , Peptide Library , Peptidoglycan/chemistry , Protein Precursors/metabolism , Pyrrolidines/chemical synthesis , Pyrrolidines/metabolism , Stereoisomerism , Vancomycin/metabolism , Vancomycin ResistanceABSTRACT
The identification of L-739,943 (8b), a potent, orally bioavailable benzolactam growth hormone secretagogue, is obtained from zwitterionic L-692,429 through modification of its amino acid side chain and replacement of the acidic 2'-tetrazole with the neutral and potency enhancing 2'-(N-methylaminocarbonylamino)methyl substituent. L-739,943 is orally active for the release of growth hormone in beagle dogs at doses as low as 0.5 mg/kg. Oral bioavailability in dogs of 8b is 24% at a dose of 2 mg/kg with a mean drug Cmax of 145 +/- 46 ng/mL. L-739,943 represents a significant breakthrough in terms of both potency and oral bioavailability as compared to the prototype benzolactam L-692,429.
Subject(s)
Benzazepines , Growth Hormone/metabolism , Methylurea Compounds , Administration, Oral , Animals , Benzazepines/chemical synthesis , Benzazepines/chemistry , Benzazepines/pharmacokinetics , Benzazepines/pharmacology , Biological Availability , Cells, Cultured , Dogs , Female , Male , Methylurea Compounds/chemical synthesis , Methylurea Compounds/chemistry , Methylurea Compounds/pharmacokinetics , Methylurea Compounds/pharmacology , Pituitary Gland/cytology , Pituitary Gland/metabolism , Rats , Rats, Wistar , Structure-Activity Relationship , Tetrazoles/pharmacologyABSTRACT
A series of N-alkyl-N-biphenylylmethyl-N'-arylurea and related derivatives represented by 1 have been prepared and evaluated for their ability to inhibit acyl-CoA:cholesterol O-acyltransferase in vitro and to lower plasma cholesterol levels in cholesterol-fed rats in vivo. Linking of two phenyl groups via oxygen and introduction of fluorine at appropriate positions on the biphenyl moiety improved in vitro and in vivo activity. From this series of analogs, compound 40 (FR179254), which had potent in vitro potency (rabbit intestinal microsomes IC50 = 25 nM), showed excellent plasma cholesterol-lowering activity when administered via the diet (ED50 = 0.045 mg/kg). However, the hypocholesterolemic effect of this compound was moderate when dosed by oral gavage in PEG400 as a vehicle (ED50 = 5.3 mg/kg). Modification of the N'-aryl moiety led to the identification of compound 50 (FR182980) which was efficacious in both dosing models (ED50 = 0.034 mg/kg and 0.11 mg/kg, respectively).
Subject(s)
Biphenyl Compounds/pharmacology , Cholesterol/blood , Enzyme Inhibitors/pharmacology , Methylurea Compounds/pharmacology , Phenylurea Compounds/pharmacology , Sterol O-Acyltransferase/antagonists & inhibitors , Anilides/pharmacokinetics , Anilides/pharmacology , Animals , Biological Availability , Biphenyl Compounds/chemistry , Cholesterol, Dietary/administration & dosage , Enzyme Inhibitors/pharmacokinetics , In Vitro Techniques , Intestinal Mucosa/enzymology , Male , Methylurea Compounds/chemical synthesis , Methylurea Compounds/pharmacokinetics , Microsomes/enzymology , Phenylurea Compounds/chemical synthesis , Phenylurea Compounds/chemistry , Phenylurea Compounds/pharmacokinetics , Pyridines/pharmacokinetics , Pyridines/pharmacology , Rabbits , Rats , Rats, Sprague-Dawley , Structure-Activity RelationshipABSTRACT
This report describes a method for the assessment of inhibitor binding affinities to wild type HIV-1 aspartic protease and to its drug-resistant mutant forms. We have elaborated a refined method for molecular modeling of the 3D structures of mutant enzymes and enzyme-inhibitor complexes based on the crystal structure of the wild type form, which employs a full thermodynamic cycle. Model complexes of four HIV-1 aspartic protease mutants with ten analogs of the A77003 inhibitor were considered. Predictions of inhibition efficiency, resistance potential, and hydrophilicity of the redesigned A77003 analogs were obtained by employing molecular mechanics for the evaluation of enzyme-inhibitor complexation energy and the polarizable continuum model for the estimation of solvent effects. Simple qualitative indicators for structural modifications aimed at overcoming the emergence of HIV resistance to protease inhibitors and at increasing the bioavailability of pseudopeptide inhibitors are examined. A semi-quantitative method for the description of enzyme-ligand binding and its implications for the rational design of inhibitors with higher binding affinity towards emerging HIV PR mutants is presented.
Subject(s)
Aspartic Acid Endopeptidases/metabolism , Drug Design , Drug Resistance, Microbial/physiology , HIV Protease Inhibitors/pharmacology , HIV Protease/drug effects , Methylurea Compounds/pharmacology , Pyridines/pharmacology , Aspartic Acid Endopeptidases/genetics , Biological Availability , Crystallography , Methylurea Compounds/chemical synthesis , Models, Molecular , Molecular Structure , Mutation , Protein Binding , Pyridines/chemical synthesis , Solubility , Valine/analogs & derivativesABSTRACT
Derivatives of antitumour anthracycline antibiotics containing N-methylurea moiety in the carbohydrate ring were obtained by the interaction of methyl isocyanate with daunorubicin, doxorubicin, carminomycin and daunorubicin derivatives, substituted at C-13 or C-14 positions. N-Nitrosation of these compounds yielded modified anthracycline antibiotics containing the N-methyl-N-nitrosourea substituent at C-3' position. Alkaline degradation of these derivatives produced, through corresponding isocyanates cyclic 3'-N,4'-carbonylderivatives. In these anthracycline derivatives with sugar cycles conjugated with oxazoline-2-ones the predominant conformations of sugar ring has changed from 1C4 to 4C1, 2,5B, or B0,3 (shown by 1H NMR spectroscopy). It was demonstrated, both in vitro and in vivo, that introduction of methylurea or cytotoxic methylnitrosourea moieties does not potentiate antimicrobial, cytotoxic or antitumour properties of these compounds.
Subject(s)
Antibiotics, Antineoplastic/chemical synthesis , Daunorubicin/chemical synthesis , Leukemia P388/drug therapy , Leukemia, Experimental/drug therapy , Methylnitrosourea/chemical synthesis , Methylurea Compounds/chemical synthesis , Animals , Cell Division/drug effects , Chemical Phenomena , Chemistry , Daunorubicin/pharmacology , Male , Mice , Structure-Activity RelationshipABSTRACT
The design rationale for a new series of tripeptide derived angiotensin converting enzyme (ACE) inhibitors, which we term "ketomethylureas", is described. Analogs of tripeptide substrates (i.e. N-benzoyl-Phe-Ala-Pro) in which the nitrogen atom of the scissile amide bond and the adjacent asymmetric carbon atom of the penultimate amino acid residue are formally transposed give rise to this novel class of inhibitors. The most potent ketomethylureas inhibit ACE with I50 values in the nM range.
Subject(s)
Angiotensin-Converting Enzyme Inhibitors/chemical synthesis , Ketones/chemical synthesis , Methylurea Compounds/chemical synthesis , Animals , Indicators and Reagents , Ketones/pharmacology , Kinetics , Methylurea Compounds/pharmacology , Oligopeptides/chemical synthesis , Oligopeptides/pharmacology , Rats , Structure-Activity RelationshipABSTRACT
The use of isotopic substitution to retard the oxidative metabolism of the gastric antisecretory agent N,N-dimethyl-N'-[2-(diisopropylamino)ethyl]-N'-(4,6-dimethyl-2-pyridyl)urea (1) and improve its antisecretory potency was examined. The pyridine ring methyl hydrogens of 1 were replaced with either deuterium or fluorine. The hexadeuterated analogue (12) was found to be approximately 2.1 times more potent than the protio form (1) as an inhibitor of gastric acid secretion stimulated by gastrin tetrapeptide. The hexafluoro analogue (11) was 0.4 times as potent as 1. A useful pyridine ring synthesis was developed to prepare the metabolites of 1, 10a (4-hydroxymethyl) and 10b (6-hydroxymethyl), and the hexafluoro analogue 11. These syntheses involved the condensation of 1,3-diketones with an appropriately N-substituted amidinoacetate.
Subject(s)
Gastric Juice/metabolism , Methylurea Compounds/pharmacology , Animals , Biotransformation , Deuterium , Dogs , Gastric Juice/drug effects , Magnetic Resonance Spectroscopy , Methylurea Compounds/chemical synthesis , Methylurea Compounds/metabolism , Structure-Activity RelationshipABSTRACT
Methylurea, a precursor of carcinogenic nitroso compound, was formed by incubating methylamine and carbamyl phosphate in neutral buffer. The formation was checked on a radiochromatogram, as well as by color reaction. The presence of methylamine and carbamyl phosphate in preserved, fermented foods provided a suitable condition for the formation of methylurea.
