Search

Your search keyword '"potent"' showing total 279 results
Start Over Descriptor "potent"
279 results on '"potent"'

251. Comparative pharmacokinetic, immunologic and hematologic studies on the anti-HIV-1/2 compounds aconitylated and succinylated HSA

Author

H. Schuitemaker, E Beljaars, A. Pasma, Dirk K. F. Meijer, C Smit, Pieter Swart, and Other departments

Subjects
Male, Receptors, Drug, Serum albumin, Pharmaceutical Science, Lymphocyte proliferation, Pharmacology, immunogenicity, Antiviral Agents, Iodine Radioisotopes, Succinylation, medicine, Animals, Humans, Tissue Distribution, Carbon Radioisotopes, Lymphocytes, Rats, Wistar, Scavenger receptor, Receptor, Blood Coagulation, Serum Albumin, chemistry.chemical_classification, Drug Carriers, Dose-Response Relationship, Drug, biology, HUMAN SERUM ALBUMINS, POTENT, Aco-HSA, Aconitic Acid, Albumin, Suc-HSA, HIV, toxicity, Human serum albumin, Rats, Amino acid, AIDS, RECEPTORS, polyanions, Biochemistry, chemistry, HIV-2, HIV-1, biology.protein, MONOCLONAL-ANTIBODIES, pharmacokinetics, Fluorescein-5-isothiocyanate, medicine.drug
Abstract

Charge modification by succinylation or cis-aconitylation of the terminal epsilon NH2 functions of the amino acid lysine in human serum albumin, resulted in polyanionic compounds with an anti-HIV-1 activity in the low nanomolar concentration range. After iv injections in rats of the negatively charged albumins (NCAs), a dose dependent elimination pattern was observed indicating a saturable eliminations pathway. The Michaelis-Menten parameters V-max and K-m were 62 +/- 8 mu g.min(-1).k(-1) and 16 +/- 4 mu g.ml(-1) (Cl-intr 3.9 +/- 1.1 ml.min(-1).kg(-1)) and 74 +/- 6 mu g.min(-1).kg(-1) and 11 +/- 2 mu g.ml(-1) (Cl-intr 6.7 +/- 1.2 ml.min(-1).kg(-1)) for aconitylated-HSA (Aco-HSA) and succinylated-HSA (Suc-HSA) respectively, using I-125-labelled proteins. The volume of distribution (V) of both compounds was approximately 60 ml.kg(-1). Coadministration of poly-inosinic acid and formaldehyde treated albumin showed a marked inhibition of blood clearance indicating that the compounds are mainly cleared from the bloodstream by scavenger receptors on liver and spleen endothelial cells and macrophages.The Michaelis-Menten constant K-m was remarkably higher when the hydrophobic fluorophore fluorescein was covalently linked to the protein, indicating that the affinity for the scavenger receptors is largely decreased by FiTC conjugation. The latter observation may have implications for the kinetic behavior of drug-carrier preparations if antiviral drugs like AZT or PMEA are linked to these intrinsic active carriers.In contrast to other polyanionic compounds like heparins and dextran sulfate, these NCAs did not exhibit acute toxicity and had no effect on blood coagulation. They neither had an effect on the lymphocyte proliferation. Studies on immunogenicity of the homologous derivatized albumins in rats did not show a significant response.The present pharmacokinetic and toxicologic data of Suc-HSA and Aco-HSA show that both compounds are interesting preparations for studies in SIV infected monkeys and AIDS patients.

Published
1996

252. STRUCTURE-ACTIVITY-RELATIONSHIPS IN THE 8-AMINO-6,7,8,9-TETRAHYDRO-3H-BENZ[E]INDOLE RING-SYSTEM .1. EFFECTS OF SUBSTITUENTS IN THE AROMATIC SYSTEM ON SEROTONIN AND DOPAMINE-RECEPTOR SUBTYPES

Author

STJERNLOF, P, ENNIS, MD, HANSSON, LO, HOFFMAN, RL, GHAZAL, NB, SUNDELL, S, SMITH, MW, SVENSSON, K, CARLSSON, A, WIKSTROM, H, and Groningen Research Institute of Pharmacy

Subjects
AGONISTS, DESIGN, DERIVATIVES, POTENT, 8-HYDROXY-2-(DI-NORMAL-PROPYLAMINO)TETRALIN, ANTAGONIST
Abstract

A series of 1-, 3-, and 4-substituted analogs to the potent 5-HT1A agonist 8-(dipropylamino)-6,7,8,9-tetrahydro-3H-benz[e]indole-1-carbaldehyde (5) were prepared and tested in vitro at 5-HT1A, 5-HT1D alpha, 5-HT1D beta, D-2, and D-3 receptors and in vivo for agonist activity in the 5-HTP and DOPA accumulation assays in reserpine-pretreated rats. Some of the compounds were resolved. The substituents used in the 1-position were chosen from a principal component analysis (PCA) plot constructed from both tabulated variables and variables calculated by semiempirical methods (PM3) and molecular mechanics software (MMX). Among the analogs prepared, some, e.g., compound 21, were equipotent to compound 5 with respect to 5-HT1A effects. All compounds were more or less selective for the 5-HT1A receptor, but-many of the compounds displayed higher affinities for 5-HT1D alpha than for 5-HT1D beta receptors.

Published
1995

254. Age-dependent appearance of synaptic currents in rat neocortical neurons in culture

Author

Massimo Avoli, Cristina Zona, Eleonora Palma, and Aldo Brancati

Subjects
nmda, Aging, Patch-Clamp Techniques, 6-Cyano-7-nitroquinoxaline-2, Cells, Wistar, cortical-neurons, glutamate, Tetrodotoxin, Neurotransmission, Biology, cell-culture, Synaptic Transmission, Settore BIO/09, Cellular and Molecular Neuroscience, chemistry.chemical_compound, Kynurenic acid, 3-dione, morphology, acid, cortex, hippocampal-neurons, miniature synaptic currents, mouse spinal-cord, potent, synaptic transmission, Animals, Glutamate receptor antagonist, Rats, Wistar, Cells, Cultured, 6-Cyano-7-nitroquinoxaline-2,3-dione, Cerebral Cortex, Neurons, Cultured, GABAA receptor, Rats, Electrophysiology, chemistry, 2-Amino-5-phosphonovalerate, Competitive antagonist, Synapses, CNQX, Excitatory postsynaptic potential, Biophysics, NMDA receptor, Cadmium, Excitatory Amino Acid Antagonists, Neuroscience
Abstract

Rat neocortical neurons grown in dissociated cell culture were recorded with the whole-cell patch-clamp technique. Spontaneous inward currents were observed in cells that were held at a membrane potential of -80 mV in medium containing tetrodotoxin and Cd2+. These currents displayed amplitudes up to 140 pA and rise time of 1.8 +/- 0.2 ms (mean +/- SD, n = 15). They reversed near 0 mV and showed no voltage-dependent frequency of occurrence. Hence, they were presumably due to spontaneous release of transmitter. The inward currents appeared around day 10 in culture and were detected up to 4 weeks. When cells of different ages were compared, the maximal probability of recording these inward events occurred at around 3 weeks in culture. The inward currents were not reduced by application of bicuculline methiodide which is a competitive antagonist of the GABAA receptor, but were blocked by the broad-spectrum glutamate receptor antagonist kynurenic acid. Moreover, spontaneous inward events were not affected by DL-2-aminophosphono-valerate (NMDA receptor antagonist) but disappeared following application of the non-NMDA receptors antagonist 6-cyano-7-nitroquinoxaline-2,3-dione (CNQX). Our observations indicate that the inward currents represent miniature synaptic events that are primarily mediated by non-NMDA excitatory amino acid receptor subtypes. Furthermore, our findings indicate that they develop over time and are not present in neurons that are grown in culture for less than 10 days.

Published
1994

255. 1,2,3-TRIAZOLE-[2',5'-BIS-O-(TERT-BUTYLDIMETHYLSILYL)-BETA-D-RIBOFURANOSYL]-3'-SPIRO-5'-(4'-AMINO-1',2'-OXATHIOL 2',2'-DIOXIDE) (TSAO) ANALOGS - SYNTHESIS AND ANTI-HIV-1 ACTIVITY

Author

Stefano Aquaro, María-José Camarasa, Anna Karlsson, Rosa Alvarez, Ana San-Félix, Carlo Federico Perno, Erik De Clercq, Sonsoles Velázquez, and Jan Balzarini

Subjects
1,2,3-Triazole, Stereochemistry, Molecular Sequence Data, SELECTIVE INHIBITORS, Antiviral Agents, Chemical synthesis, TIBO DERIVATIVES, Structure-Activity Relationship, chemistry.chemical_compound, Drug Discovery, Humans, Structure–activity relationship, Spiro Compounds, PYRIMIDINE NUCLEOSIDES, Uridine, Cells, Cultured, REVERSE-TRANSCRIPTASE INHIBITORS, INVITRO, Base Sequence, POTENT, ANTIVIRAL ACTIVITY, Triazoles, Orders of magnitude (numbers), IMMUNODEFICIENCY-VIRUS TYPE-1, Settore MED/07 - Microbiologia e Microbiologia Clinica, HIV Reverse Transcriptase, Cycloaddition, Thymine, chemistry, HIV-1 REPLICATION, STEREOSPECIFIC SYNTHESIS, HIV-1, Reverse Transcriptase Inhibitors, Molecular Medicine, Nucleoside, Lead compound, Thymidine
Abstract

Several 4- or 5-monosubsituted and 4,5-disubstituted 1,2,3-triazole analogues of the anti-HIV-1 lead compound [1-[2',5'-bis-O-(tert-butyldimethylsilyl)-beta-D- ribofuranosyl]thymine]-3'-spiro-5"-(4"-amino-1",2"-oxathiole 2",2"-dioxide) (TSAO-T) have been prepared and evaluated as inhibitors of HIV-1-induced cytopathicity. These analogues have been prepared by 1,3-diplar cycloaddition of [2,5-bis-O-(tert-butyldimethylsilyl)-beta-D-ribofuranosyl]- 3-spiro-5'-(4'-amino- and 4'-(N-acetylamino)-1',2'-oxathiole 2',2'-dioxide) (TSAO) azides to various substituted acetylenes. Several 4- and 5-substituted 1,2,3-triazole-TSAO analogues proved superior to the unsubstituted derivative by 1-2 orders of magnitude. In particular the 5-substituted amido-, (methylamido)-, and (dimethylamido)-1,2,3-triazole derivatives of TSAO were endowed with potent anti-HIV-1 activity (50% effective concentration: 0.056-0.52 microM). They show a similar resistance spectrum as previously noted for TSAO-T and related derivatives.

Published
1994

256. ORALLY-ACTIVE CENTRAL DOPAMINE AND SEROTONIN RECEPTOR LIGANDS - 5-[[(TRIFLUOROMETHYL)SULFONYL]OXY]-2-(DI-N-PROPYLAMINO)TETRALINS, 6-[[(TRIFLUOROMETHYL)SULFONYL]OXY]-2-(DI-N-PROPYLAMINO)TETRALINS, 7-[[(TRIFLUOROMETHYL)SULFONYL]OXY]-2-(DI-N-PROPYLAMINO)TETRALINS, AND 8-[[(TRIFLUOROMETHYL)SULFONYL]OXY]-2-(DI-N-PROPYLAMINO)TETRALINS AND THE FORMATION OF ACTIVE METABOLITES IN-VIVO

Author

SONESSON, C, BOIJE, M, SVENSSON, K, EKMAN, A, CARLSSON, A, ROMERO, AG, MARTIN, IJ, DUNCAN, JN, KING, LJ, WIKSTROM, H, and Groningen Research Institute of Pharmacy

Subjects
AGONIST N-0437, DERIVATIVES, POTENT, STIMULATING ACTIVITY, BINDING, SUBSTITUENT CONSTANTS, 2-(N-PROPYL-N-2-THIENYLETHYLAMINO)-5-HYDROXYTETRALIN, 8-HYDROXY-2-(DI-NORMAL-PROPYLAMINO)TETRALIN, ESTER PRODRUGS, 2-AMINOTETRALINS
Abstract

The racemic triflate derivatives 5-8 of the 5-, 6-, 7-, and 8-hydroxylated 2-(di-n-propylamino)-tetralins 1-4 were shown to possess similar pharmacological profiles to their phenolic counterparts in in vitro binding and in vivo biochemical and behavioral assays in rats. Consequently, subcutaneous administration of the 5-, 6-, and 7-triflates displayed essentially dopaminergic agonist properties, while the 8-triflate was shown to be a selective 5-HT1A receptor agonist. With respect to their agonist activities, the triflates were less potent than their phenolic analogs. The absolute oral bioavailability of compound 8 (8-triflate) was 4-5 times greater than the corresponding hydroxylated compound. Interestingly, in the in vivo biochemical assay compound 8 was found to be more potent after oral than after subcutaneous administration, indicating formation of one or more active metabolites. Following a study of the metabolism of compound 8 in rat hepatocytes, the monopropyl analog 9 was identified as the major metabolite and was suprisingly found to be more potent than compound 8. Oral administration of compound 5 (5-triflate) resulted in behavioral and biochemical effects indicative of mixed DA/5-HT1A agonist properties not seen after subcutaneous administration. These results may also be indicative of the formation of active metabolites.

Published
1993

257. Synthesis and in Vivo Distribution in the Rat of Several fluorine-18 Labeled N-fluoroalkylaporphines

Author

S. Zijlstra, Willem Vaalburg, Gm Visser, and Jakob Korf

Subjects
Male, Fluorine Radioisotopes, Apomorphine, Stereochemistry, DOPAMINE RECEPTOR, Dopamine Agents, Striatum, Dopamine, In vivo, medicine, Potency, Animals, Tissue Distribution, Rats, Wistar, BRAIN, Radiation, Chemistry, POTENT, Radiochemistry, Reserpine, Rats, Dopamine receptor, Isotope Labeling, Specific activity, medicine.drug
Abstract

A method is described for the rapid production and purification of new potential dopamine agonists. Via microwave heating 10,11-dihydroxy-N-(n-2-fluoroethyl)norapomorphine (FNEA), 10,11-dihydroxy-N-(n-3-fluoropropyl)norapomorphine (FNPA) and 2,10,11-trihydroxy-N-(n-3-fluoropropyl)norapomorphine (FTNPA) and their isotopic fluorine-18 derivatives were synthesized. The fluorine-18 label was introduced via N-fluoroalkylation of acylated noraporphine derivatives with no-carrier-added (n.c.a.) (FCH2CH2I)-F-18 and (FCH2CH2CH2I)-F-18. Within 160 min (E.O.B.), radiochemical yields of 13-29% (corrected for decay) were achieved based on [F-18]fluoroalkyliodide. The specific activity obtained, ranged from 15 to 75 GBq/mumol. The fluorine-18 labeled compounds were investigated for their in vivo binding potency to the D2-receptors. After i.v. injection, the distribution was studied in rats. High uptakes of the N-[F-18]fluoroalkylaporphines were found in the lungs, liver, adrenals and kidneys. No significant different radioactive accumulation was observed in striatum, cerebellum and frontal cortex. Dopamine depletion with reserpine did not affect the striatum to cerebellum ratio at low dosage of N-[F-18]fluoroalkylaporphines (10 nmol/kg).

Published
1993

258. Generalized Free Products of $\pi_c$ Groups

Author

H.L. Koay and P.C. Wong

Subjects
Algebra, one-relator group residually finite, 20F05, Generalized free product, Free product, 20E25, General Mathematics, potent, $\pi_c$, 20E30, Mathematics
Published
1992

259. Enantiomers of monohydroxy-2-aminotetralin derivatives and their activity at dopamine autoreceptors as studied by brain dialysis

Author

Pieter G. Tepper, H Stoelwinder, As Horn, W Timmerman, Bhc Westerink, Cor J. Grol, and Durk Dijkstra

Subjects
Male, N-0437 (2-(N-PROPYL-N-2-THIENYLETHYLAMINO)-5-HYDROXYTETRALIN, Dopamine, Dopamine Agents, Statistics as Topic, N-DI-N-PROPYLAMINO)TETRALIN), METABOLITES, DOPAMINE-D2 RECEPTOR AGONISTS, Receptors, Dopamine, DOPAMINE RELEASE, Chromatography, High Pressure Liquid, STRIATUM, Chemistry, MICRODIALYSIS, Stereoisomerism, SELECTIVITY, Dopamine receptor, Autoreceptor, PHNO (4-PROPYL-9-HYDROXYNAPHTHOXAZINE), INTRACEREBRAL DIALYSIS, N,N-DISUBSTITUTED 2-AMINOTETRALINS, medicine.drug, Microdialysis, Tetrahydronaphthalenes, Stereochemistry, INVIVO MEASUREMENT, TRANS-STRIATAL DIALYSIS, Thiophenes, 7-OH-DPAT (7-HYDROXY-2-(N, Dopamine agonist, (STEREOISOMERS), 7-OH-DPAT (7-HYDROXY-2-(N,N-DI-N-PROPYLAMINO)TETRALIN), Oxazines, medicine, Animals, RELEASE, Pharmacology, N-0438 (2-(N-PROPYL-N-2-THIENYLETHYLAMINO)-7-HYDROXYTETRALIN), POTENT, N-DISUBSTITUTED 2-AMINOTETRALINS, Rats, Inbred Strains, PERFORMANCE LIQUID-CHROMATOGRAPHY, RECEPTOR AGONISTS, 2-Aminotetralin, Corpus Striatum, Rats, Enantiomer, Dialysis
Abstract

The enantiomers of a series of dopamine (DA) agonists, monohydroxy-2-aminotetralin derivatives, were investigated using brain microdialysis. We used a 5-OH-substituted derivative, N-0437 (2-(N-propyl-N-2-thienylethylamino)-5-hydroxytetralin), and three 7-OH-substituted derivatives, N-0438 (2-(N-propyl-N-2-thienylethylamino)-7-hydroxytetralin), 7-OH-DPAT (7-hydroxy-2-(N,N-di-n-propylamino)tetralin) and PHNO (4-propyl-9-hydroxynaphthoxazine; position 9 of the naphtoxazines corresponds to position 7 of the aminotetralins). We studied the activity of the enantiomers at autoreceptors regulating the release of DA following their local infusion into the striatum of the rat. We were particularly interested in the activity of R(+)-N-0437, S(-)-N-0438, S(-)-7-OH-DPAT and S(-)-PHNO, which are enantiomers that have been classified as less potent or inactive in previous studies. S(-)-N-0437, R(+)-N-0438, R(+)-7-OH-DPAT and R(+)-PHNO decreased DA release by 45-60%. Thus, these enantiomers are potent agonists at autoreceptors regulating the release of DA. The R(+) enantiomer of the 5-OH-substituted derivative N-0437 possessed antagonistic activity at autoreceptors controlling DA release, increasing DA release by 100%. This finding is consistent with reports showing that one enantiomer of other 5-OH DA agonists displays agonistic activity, while the other has antagonistic properties at DA autoreceptors. The less potent enantiomers of the 7-OH-substituted derivatives S(-)-N-0438, S(-)-7-OH-DPAT and S(-)-PHNO, however, all showed weak agonistic activity at DA autoreceptors. They decreased DA release by maximally 40%. Thus, considering these results and the findings from the literature, the position of the hydroxyl group may determine the action profile of the enantiomers. Apparently, not only the R(+) configuration but also the S(-) configuration of the 7-OH-substituted derivatives can bind and activate the autoreceptor regulating DA release, whereas only the S(-) configuration of 5-OH-substituted derivatives is capable of doing so.

Published
1991

260. MESANGIAL CELL IMMUNE INJURY - EFFECTS OF THROMBOXANE RECEPTOR ANTAGONISM

Author

Elias A. Lianos, Barbara A. Bresnahan, W M Bagchus, and Richard J. Roman

Subjects
Male, medicine.medical_specialty, IMMUNE INJURY, Thromboxane, Glomerular Mesangial Cell, Receptors, Prostaglandin, Receptors, Thromboxane, Carbazoles, urologic and male genital diseases, ARGININE VASOPRESSIN, Thromboxane receptor, Thromboxane A2, chemistry.chemical_compound, Internal medicine, CONTRACTION, medicine, Animals, Antilymphocyte Serum, biology, Mesangial cell, POTENT, PROSTAGLANDIN, Rats, Inbred Strains, General Medicine, Bridged Bicyclo Compounds, Heterocyclic, MESANGIAL CELL, Glomerular Mesangium, Prostaglandin Endoperoxides, Synthetic, Rats, Thromboxane B2, ANGIOTENSIN-II, Endocrinology, Hydrazines, chemistry, THROMBOXANE, Nephrology, Renal blood flow, 15-Hydroxy-11 alpha,9 alpha-(epoxymethano)prosta-5,13-dienoic Acid, biology.protein, Fatty Acids, Unsaturated, Eicosanoids, RAT, Thromboxane-A synthase, Glomerular Filtration Rate
Abstract

We assessed the renal hemodynamic changes occurring acutely after glomerular mesangial cell immune injury and the effects of thromboxane receptor antagonism on these changes. A single intravenous proteinuric dose of a monoclonal antibody raised against the rat thymocyte antigen Thy 1.1 (ER4), which is also expressed in rat mesangial cells, induced acute decrements in glomerular filtration rate and in renal blood flow in male Munich-Wistar rats. One hour after administration of 4 to 6 mg/kg of ER4 antibody, glomerular filtration rate and renal blood flow decreased by 80 and 36%, respectively. These decrements were associated with significant increments in basal thromboxane B2 synthesis in isolated glomeruli and no changes in glomerular prostaglandin E2 synthesis. Pretreatment of animals with the thromboxane receptor antagonist SQ-29, 548 (2 mg/kg) significantly ameliorated decrements in glomerular filtration rate and renal blood flow. Pretreatment with a structurally dissimilar thromboxane receptor antagonist, L-670,596 (3 mg/kg) had no effect. Both antagonists at the doses employed abolished the decrements in renal blood flow induced by systemic administration of the thromboxane mimetic U-46619. Whereas the SQ-29,548 antagonist had no effect on glomerular leukotriene B4 and 12-hydroxyeicosate-traenoic acid synthesis, the L-670,596 thromboxane receptor antagonist significantly inhibited glomerular synthesis of these eicosanoids in immunologically injured glomeruli. These observations indicate that in mesangial cell immune injury the protective effect of thromboxane A2 receptor antagonism on glomerular filtration rate and renal blood flow is not solely due to inhibition of the vasoconstrictor effects of thromboxane A2. An effect on the synthesis of arachidonate lipoxygenation products may also play a role.

Published
1991

261. In search of selective and potent Golgi alpha -mannosidase II inhibitors as potential anticancer agents: Synthesis of 3-substituted-swainsonine analogs and preparation of immobilized swainsonine analogs on solid support.

Author

Guo, Luyi

Subjects
Analogs, Anticancer Agents, Golgi Alpha-mannosidase Ii, Immobilized, Inhibitors, Mannosidases, Potent, Potential, Preparation, Search, Selective, Solid, Substituted, Support, Swainsonine, Synthesis
Abstract

The major goal of this thesis research is to design and synthesize analogs of swainsonine that may be more selective and potent inhibitors for Golgi alpha-mannosidase II, but devoid of inhibitory activities toward lysosomal alpha-mannosidase. Alpha-3-benzyloxymethyl substitutions on swainsonine were tolerated well by mannosidases, while the respective beta-substitution rendered the analogs inactive. The first synthesis of a pseudodisaccharide with swainsonine at the glycone portion was accomplished. Although the pseudodisaccharide mimics the Man(alpha-1,6)Man disaccharide portion of the natural substrate, it showed low biological activities toward mannosidases. Polyethylene glycol linked swainsonine analogs were designed to bind both the active site and the putative GlcNAc binding site of Golgi alpha-mannosidase II. However, they were only weak inhibitors of mannosidases. Also, C3- and C6-derivatized swainsonine analogs were synthesized and used to prepare affinity columns for the purification of alpha-mannosidases. The C3-alpha-swainsonine affinity analogs were found to be potent alpha-mannosidase inhibitors. None of the synthesized C3-substituted swainsonine analogs showed significant selectivity in favor of Golgi alpha-mannosidase II.

Published
2003

262. SAR studies on a weak delta opioid dipeptide antagonist (Tyr-Tic) and a potent mu opioid peptidomimetic agonist.

Author

Ma, Wenli

Subjects
Agonist, Antagonist, Delta, Dipeptide, Mu, Opioid Receptors, Peptidomimetic, Potent, Sar, Structure Activity Relationship, Structure-activity Relationship, Studies, Tic, Tyr, Weak
Abstract

The existence of three types of opioid receptors, delta, mu and kappa, as well as their analgesic effects, and associated side effects are well known. Although thousands of opioid peptides and non-peptides have been synthesized, an understanding of the individual pharmacological activity of each receptor type, and the development of analgesics with no adverse side effects are still great challenges. A detailed knowledge of opioid receptor structure and the interaction of opioids at the receptor-binding site are keys for meeting these challenges. This thesis describes structure activity relationship (SAR) studies on two potentially valuable classes of small opioid ligands, Tyr-Tic and BTTQ (6-benzyl-4-tyrosyl-1,2,3,4-tetrahydroquinoline) and relates the observed results to our evolving opioid receptor models. In the Tyr-Tic series, extensive structural modifications performed on the Ti(c) (1,2,3,4-tetrahydroisoquinoline-(3-carboxylic acid)) benzene ring lead to generally decreased delta binding affinities, although lipophilic substituents such as Cl, F and Me are better tolerated. Modifications on various other positions fail to produce promising binding results. Conformational analysis of Tyr-Ti(c) using a grid scan search method with dihedral angles chi 1, y and o as variables identified low energy conformers, which were grouped into conformational families. Comparison with the structurally rigid opiate naltrindole and docking to our receptor model identifies the delta bound conformation of Tyr-Ti(c) as containing trans and gauche (+) orientations of Tyr1 and Tic2 side chains, respectively, a y angle of Tyr1 ∼ 130° and a cis peptide bond. Interactions of ligands with opioid receptor binding sites were also examined. The results are in general agreement with the observed SAR data. BTTQ was designed based on a pharmacophore model derived from the cyclic tetrapeptide peptide cyclo[Tyr-D-Cys-Phe-D-Pen] (JOM-13) with the entire cyclic portion of the peptide replaced by the tetrahydroquinoline scaffold. Various substituents were incorporated at the N1 position through a rationally designed synthetic pathway. The binding data are consistent with the modeling results that predict that a negatively charged group should improve mu binding affinity and decrease kappa binding affinity, while a positively charged group should increase kappa binding and diminish mu binding, although the magnitude of the changes observed is small.

Published
2000

263. Discovery of novel cyanamide-based inhibitors of cathepsin C.

Author

Lainé D, Palovich M, McCleland B, Petitjean E, Delhom I, Xie H, Deng J, Lin G, Davis R, Jolit A, Nevins N, Zhao B, Villa J, Schneck J, McDevitt P, Midgett R, Kmett C, Umbrecht S, Peck B, Davis AB, and Bettoun D

Abstract

The discovery of potent and selective cyanamide-based inhibitors of the cysteine protease cathepsin C is detailed. Optimization of the template with regard to plasma stability led to the identification of compound 17, a potent cathepsin C inhibitor with excellent selectivity over other cathepsins and potent in vivo activity in a cigarette smoke mouse model.

Published
2010
Full Text
View/download PDF

264. Preparation and characterization of conjugates of (modified) human serum albumin and liposomes: drug carriers with an intrinsic anti-HIV activity

Author

Hwm Morselt, M P deBéthune, R Pauwels, Dkf Meijer, Piet Swart, E Declercq, Gerrit L. Scherphof, Jaam Kamps, and Groningen University Institute for Drug Exploration (GUIDE)

Subjects
Anions, cis-Aconitic anhydride, PROTEINS, Biophysics, Serum albumin, RAT-LIVER, INHIBITION, Antiviral Agents, Biochemistry, Polyethylene Glycols, chemistry.chemical_compound, In vivo, Phosphatidylcholine, medicine, Humans, Tissue Distribution, ASSAY, Antiviral, IN-VIVO, Phosphatidylethanolamine, Drug Carriers, Liposome, INVITRO, Chromatography, biology, POTENT, Phosphatidylethanolamines, Aconitic Acid, Cell Biology, Human serum albumin, body regions, Kinetics, Liver, chemistry, Liposomes, Drug delivery, CELLS, REPLICATION, embryonic structures, biology.protein, HIV-1, (Human), Drug carrier, SATA, IMMUNOLIPOSOMES, medicine.drug
Abstract

Human serum albumin (HSA) derivatized with cis-aconitic anhydride (Aco-HSA) that was earlier shown to inhibit replication of human immunodeficiency virus type 1 (HIV-1), was covalently coupled to conventional liposomes, consisting of phosphatidylcholine, cholesterol and maleimido-4-(p-phenylbutyryl)phosphatidylethanolamine, using the heterobifunctional reagent N-succinimidyl-S-acetylthioacetate (SATA). The amount of HSA that could be coupled to the liposomes depended on derivatization of the HSA and ranged from 64.2 +/- microgram HSA/micromol total lipid for native HSA to 29.5 +/- 2.7 microgram HSA/micromol total lipid for HSA in which 53 of the epsilon amino groups of lysine were derivatized with cis-aconitic anhydride (Aco53-HSA). Incorporation of 3.8 mol% of total lipid of a poly(ethylene glycol) derivative of phosphatidylethanolamine (PEG-PE) in the liposomes resulted in a lower coupling efficiency of Aco-HSA. The elimination and distribution of the liposomal conjugates in rats in vivo was largely dependent on the modification of the HSA coupled to the liposomes. With native HSA-liposomes, more than 70% of the conjugate was still found in the blood plasma 30 min after i.v. injection in rats, while at this time Aco-HSA-liposomes were completely cleared from the circulation. The rapid clearance of conventional Aco-HSA-liposomes was due to a rapid uptake into the liver and could be considerably decreased by incorporating PEG-PE in the liposomal bilayer. After 3 h 60% of Aco-HSA-PEG-liposome conjugates were found in the blood. In an in vitro anti-HIV-1 assay, the 50% inhibitory concentrations (IC50) for Aco39-HSA-liposomes and Aco53-HSA-liposomes expressed as protein weight, were 2.87 microgram/ml and 0.154 microgram/ml, respectively. When PEG-PE was incorporated, the Aco53-HSA-liposomes retained anti HIV-1 activity (IC50:3.13 microgram/ml). The possibility to modulate the residence time in the bloodstream of Aco-HSA-liposomes and the potent anti-HIV-1 activity of these conjugates, may allow the development of an intrinsically active drug carrier system. By incorporating anti HIV-1 drugs such as AZT into such liposomes a drug delivery system can be designed that might act simultaneously on the virus/cell binding by virtue of the coupled Aco-HSA and on the RNA/DNA transcription of the HIV-1 replication cycle through the nucleoside analogue.

Full Text
View/download PDF

265. Synthetic constrained peptide selectively binds and antagonizes death receptor 5

Subjects
CYTOTOXIC LIGAND TRAIL, DECOY RECEPTORS, COMPLEX, POTENT, apoptosis, TRAIL, APOPTOSIS, ACTIVATION, CELL-DEATH, DOMAIN, R2C16, CRYSTAL-STRUCTURE, DR5, phage display
Abstract

Apoptosis or programmed cell death is an inherent part of the development and homeostasis of multicellular organisms. Dysregulation of apoptosis is implicated in the pathogenesis of diseases such as cancer, neurodegenerative diseases and autoimmune disorders. Tumour necrosis factor-related apoptosis-inducing ligand (TRAIL) is able to induce apoptosis by binding death receptor (DR)4 (TRAIL-R1) and DR5 (TRAIL-R2), which makes TRAIL an interesting and promising therapeutic target. To identify peptides that specifically interact with DR5, a disulfide-constrained phage display peptide library was screened for binders towards this receptor. Phage-displayed peptides were identified that bind specifically to DR5 and not to DR4, nor any of the decoy receptors. We show that the synthesized peptide, YCKVILTHRCY, in both monomeric and dimeric forms, binds specifically to DR5 in such a way that TRAIL binding to DR5 is inhibited. Surface plasmon resonance studies showed higher affinity towards DR5 for the dimeric form then the monomeric form of the peptide, with apparent K(d) values of 40 nm versus 272 nm, respectively. Binding studied on cell lines by flow cytometry analyses showed concentration-dependent binding. Upon co-incubation with increasing concentrations of TRAIL, the peptide binding was reduced. Moreover, both the monomeric and dimeric forms of the peptide reduced TRAIL-induced cell death in Colo205 colon carcinoma cells. The peptide, YCKVILTHRCY, or its derivates, may be a useful investigative tool for dissecting signalling via DR5 relative to DR4 or could act as a lead peptide for the development of therapeutic agents in diseases with dysregulated TRAIL-signalling.

266. Mdm2 and MdmX inhibitors for the treatment of cancer

Author

Alexander Dömling, Tad A. Holak, Lutz Weber, Grzegorz Dubin, Aleksandra Pecak, Krzysztof M. Zak, Barbara Rys, and Benedykt Wladyka

Subjects
p53, MDMX, HdmX, PROTEIN, Bioinformatics, protein-protein interaction, ACTIVATION, 0302 clinical medicine, ANTAGONISTS, DESIGN, Neoplasms, Drug Discovery, inhibitors, Molecular Targeted Therapy, Enzyme Inhibitors, IN-VIVO, 0303 health sciences, Molecular Structure, P53 PATHWAY, Proto-Oncogene Proteins c-mdm2, General Medicine, Small molecule, 3. Good health, 030220 oncology & carcinogenesis, Mdm2, Signal transduction, Signal Transduction, P53-MDM2 INTERACTION, tumor suppressor, Antineoplastic Agents, UBIQUITINATION, Biology, murine double minute, Patents as Topic, Structure-Activity Relationship, 03 medical and health sciences, Mdm4, medicine, Animals, Humans, cancer, 030304 developmental biology, Pharmacology, P53 pathway, POTENT, Cancer, medicine.disease, protein–protein interaction, The Hallmarks of Cancer, Cancer cell, biology.protein, Cancer research, Drug and Narcotic Control, SMALL-MOLECULE INHIBITORS, MdmX, Hdm2
Abstract

Introduction: One of the hallmarks of cancer cells is the inactivation of the p53 pathway either due to mutations in the p53 gene or over-expression of negative regulators, Mdm2 and/or MdmX. Pharmacological disruption of the Mdm2/X-p53 interaction to restore p53 activity is an attractive concept, aiming at a targeted and non-toxic cancer treatment. Areas covered: The introduction covers the biological role of p53 pathway and its regulation by Mdm2 and MdmX in normal and cancer cells and the current repertoire and development status of inhibitors of the Mdm2/X-p53 interaction for the treatment of cancer. The main part of the article covers patents and patent applications describing small molecule inhibitors of the Mdm2/X-p53 interaction published from 2011 until 2012. Expert opinion: The area of small molecule Mdm2/X-p53 interaction inhibitor development is progressing fast. Several Phase I clinical studies and preclinical programs are now in progress, however, the clinical proof concept has yet to be demonstrated. Multiple available compounds inhibit Mdm2-p53 interaction with nanomolar affinities, but MdmX is still missing such potent binders. Since research points to a complementary mode of Mdm2 and MdmX action, the future compound classes will possibly want to include dual actions versus Mdm2 and MdmX.

267. On p-saturable groups

Author

Jon González-Sánchez

Subjects
Normal subgroup, Lazard, Algebra and Number Theory, p-Saturable, p-Adic analytic, Combinatorics, Potent, Torsion (algebra), SUBGROUPS, Powerful, Finitely-generated abelian group, Pro-p groups, Uniformly powerful, PF-groups, Mathematics
Abstract

A pro-p group G is a PF-group if it has central series of closed subgroups {Ni}i∈N with trivial intersection satisfying N1=G and [Ni,G,…p−1,G]⩽Ni+1p. In this paper, we prove that a finitely generated pro-p group G is a p-saturable group, in the sense of Lazard, if and only if it is a torsion free PF-group. Using this characterization, we study certain families of subgroups of p-saturable groups. For example, we prove that any normal subgroup of a p-saturable group contained in the Frattini is again p-saturable.

Full Text
View/download PDF

268. Search for Potent Anthelmintics—Part VII. Hydrazones Derived from 4-substituted-7-coumarinyl Oxyaceticacid Hydrazides

Author

M. IMTIAZ HUSAIN, M. K. SHUKLA, and S. K. AGARWAL

Subjects
Potent, Oxyaceticacid, Hydrazones, Hydrazides
Abstract

Department of Chemistry, Lucknow University, Lucknow-226 007 Manuscript received 15 April 1977, accepted 21 December 1978 Twenty new N-(4-substituted-7-coumarinyloxyacetyl) hydrazones have been synthe­sised as possible anthelmintic agents, &nbsp

Published
1979
Full Text
View/download PDF

270. Structural basis of the activation of the CC chemokine receptor 5 by a chemokine agonist

Author

Isaikina, Polina, Tsai, Ching-Ju, Dietz, Nikolaus, Pamula, Filip, Grahl, Anne, Goldie, Kenneth N., Guixà-González, Ramon, Branco, Camila, Paolini-Bertrand, Marianne, Calo, Nicolas, Cerini, Fabrice, Schertler, Gebhard F. X., Hartley, Oliver, Stahlberg, Henning, Maier, Timm, Deupi, Xavier, and Grzesiek, Stephan

Subjects
Models, Molecular, Receptors, CCR5, Protein Conformation, Cryoelectron Microscopy, rantes, virus diseases, SciAdv r-articles, dynamics, Molecular Dynamics Simulation, inhibition, stomatognathic diseases, Structure-Activity Relationship, stomatognathic system, Structural Biology, parasitic diseases, potent, Humans, amino-terminus, recognition, human activities, Chemokine CCL5, Research Articles, Research Article, Signal Transduction
Abstract

The human CC chemokine receptor 5 (CCR5) is a G protein–coupled receptor (GPCR) that plays a major role in inflammation and is involved in cancer, HIV, and COVID-19. Despite its importance as a drug target, the molecular activation mechanism of CCR5, i.e., how chemokine agonists transduce the activation signal through the receptor, is yet unknown. Here, we report the cryo-EM structure of wild-type CCR5 in an active conformation bound to the chemokine super-agonist [6P4]CCL5 and the heterotrimeric Gi protein. The structure provides the rationale for the sequence-activity relation of agonist and antagonist chemokines. The N terminus of agonist chemokines pushes onto specific structural motifs at the bottom of the orthosteric pocket that activate the canonical GPCR microswitch network. This activation mechanism differs substantially from other CC chemokine receptors that bind chemokines with shorter N termini in a shallow binding mode involving unique sequence signatures and a specialized activation mechanism., Science Advances, 7 (25), ISSN:2375-2548

271. Synthesis of [(2S,3S,4R)-3,4-dihydroxypyrrolidin-2-yl]-5-methylfuran-4-carboxylic acid derivatives: New leads as selective beta-galactosidase inhibitors

Author

Moreno-Vargas, A. J., Demange, R., Fuentes, J., Robina, I., and Vogel, P.

Subjects
disease, sugars, biological-activity, oligosaccharides, alpha-galactosidase, potent, glycosidase inhibitors, configuration, N-butyldeoxynojirimycin
Abstract

The preparation of [(2S,3S,4R)-3,4-dihydroxypyrrolidin-2-yl]furan derivatives in a stereoselective route starting from D-glucose and ethyl acetoacetate is presented. Ethyl ester (6), N,N-diethylamide (7) and N-isopropylamide (8) have been tested towards 25 glycosidases. Ester (6) is a selective inhibitor of beta-galactosidases. The new compounds represent a new type of imino-C-nucleoside analogues. (C) 2002 Published by Elsevier Science Ltd.

272. Biofunctional polymer nanoparticles for intra-articular targeting and retention in cartilage

Author

Rothenfluh, Dominique A., Bermudez, Harry, O'Neil, Conlin P., and Hubbell, Jeffrey A.

Subjects
Static Compression, Drug Carriers, Liposome-Incorporated Corticosteroids, Aggrecanase Inhibitors, Delivery System, Potent, Phage Display, Articular-Cartilage, Peptide Libraries, Albumin Microspheres
Abstract

The extracellular matrix of dense, avascular tissues presents a barrier to entry for polymer-based therapeutics, such as drugs encapsulated within polymeric particles. Here, we present an approach by which polymer nanoparticles, suffciently small to enter the matrix of the targeted tissue, here articular cartilage, are further modified with a biomolecular ligand for matrix binding. This combination of ultrasmall size and biomolecular binding converts the matrix from a barrier into a reservoir, resisting rapid release of the nanoparticles and clearance from the tissue site. Phage display of a peptide library was used to discover appropriate targeting ligands by biopanning on denuded cartilage. The ligand WYRGRL was selected in 94 of 96 clones sequenced after five rounds of biopanning and was demonstrated to bind to collagen II alpha 1. Peptide-functionalized nanoparticles targeted articular cartilage up to 72-fold more than nanoparticles displaying a scrambled peptide sequence following intra-articular injection in the mouse.

273. Apatinib Sensitizes Human Breast Cancer Cells against Navitoclax and Venetoclax Despite Up-regulated Bcl-2 and Mcl-1 Gene Expressions

Author

Kavakcioglu Yardimci, Berna, Ozgun Acar, Ozden, Semiz, Asli, Sen, Alaattin, AGÜ, Yaşam ve Doğa Bilimleri Fakültesi, Moleküler Biyoloji ve Genetik Bölümü, and Sen, Alaattin

Subjects
Cytotoxicity, Proliferation, Resistance, Apoptosis, Venetoclax, Bh3 Mimetics, chemistry.chemical_compound, Downregulation and upregulation, Medicine, Apatinib, Endothelial Growth-Factor, Gene, Navitoclax, business.industry, Inhibitors, Death, Potent, Oncology, chemistry, Abt-263, Cancer cell, Cancer research, business, Human breast, Apoptosis, Breast adenocarcinoma
Abstract

This study was supported by Scientific Research Projects Unit of Pamukkale University (PAU-BAP2019BSP008). OBJECTIVE Defects in apoptotic cell death which restrict the success of conventional cytotoxic therapies have pivotal roles in a number of pathological conditions including cancer. However, a novel drug class targeting pro-survival Bcl-2 protein family members has been developed with the understanding of the structures and interactions of Bcl-2 proteins. Within this new class, Bcl-2/Bcl-xL inhibitor Navitoclax and Bcl-2 specific inhibitor Venetoclax have been shown to demonstrate strong anticancer activities on several types of cancers. But their low affinity to other anti-apoptotic proteins limits their clinical usage. Here, we investigated the cytotoxic and apoptotic effects of Navitoclax/Venetoclax and their combinations with specific tyrosine kinase inhibitor Apatinib on estrogen receptor (ER)-positive MCF-7 and ER-negative MDA-MB-231 breast cancer cell lines. METHODS MTT assay was used for the evaluation of the inhibition of cancer cell proliferation. ELISA test and Quantitative real-time PCR assay was performed to determine the role of caspase-3, Bak, Bax, Bcl-2, Bcl-xL and Mcl-1 proteins in the inhibition of cell proliferation triggered by the tested agents. RESULTS We found that aggressive MDA-MB-231 cell line was more sensitive to all tested agents. Apatinib significantly enhanced Navitoclax/Venetoclax mediated inhibition of cell viability in both cancer cell lines despite up-regulation in the expression levels of Bcl-2 and Mcl-1 genes. We further demonstrated significant Bak/Bax and caspase-3 expression in less aggressive MCF-7 cells. CONCLUSION Our findings have impacts on Navitoclax/Venetoclax plus Apatinib based therapy for breast adenocarcinoma. On the other hand, further studies should be conducted to elucidate the mechanisms underlying synergistic effects of Navitoclax/Venetoclax plus Apatinib combinations. Pamukkale University PAU-BAP2019BSP008

274. Polyvalent Side Chain Peptide-Synthetic Polymer Conjugates as HIV-1 Entry Inhibitors

Author

Danial, Maarten, Root, Michael J., and Klok, Harm-Anton

Subjects
Design, Potent, Functionalized Polymers, Gp120, Cd4-Mimetic Miniproteins, Toxin, Infection, Fusion, Immunodeficiency-Virus Type-1, Hpma Copolymers
Abstract

This report describes the synthesis and properties of a series of polyvalent side chain peptide synthetic polymer conjugates designed to block the CD4 binding site on gp120 and inhibit HIV-1 entry into a host cell. The peptide sequences in the conjugates are based on the CDR H3 region of the neutralizing anti-HIV-1 antibody IgG1 b12. Using a consecutive ester-amide/thiol-ene postpolymerization modification strategy, a library of polymer conjugates was prepared. Evaluation of the HIV-1 inhibitory properties revealed that midsized polymer conjugates displayed the highest antiviral activity, while shorter and longer conjugates proved to be less efficacious inhibitors. The lower molecular weight conjugates may not have sufficient length to span the distance between two neighboring gp120 containing spikes, while the higher molecular weight conjugates may be compromised due to a higher entropic penalty that would accompany their binding to the viral envelope. Although the IC50 values for these polymer conjugates are higher than that of the parent IgG1 b12 antibody, the strategy presented here may represent an interesting antiviral approach due to the attractive properties of such polymer therapeutics (relatively inexpensive production and purification costs, high thermal and chemical stability in storage conditions, long half-life in biological tissues, low immunogenicity, and protection from proteolytic degradation).

275. Scaffolding protein functional sites using deep learning

Author

Jue Wang, Sidney Lisanza, David Juergens, Doug Tischer, Joseph L. Watson, Karla M. Castro, Robert Ragotte, Amijai Saragovi, Lukas F. Milles, Minkyung Baek, Ivan Anishchenko, Wei Yang, Derrick R. Hicks, Marc Expòsit, Thomas Schlichthaerle, Jung-Ho Chun, Justas Dauparas, Nathaniel Bennett, Basile I. M. Wicky, Andrew Muenks, Frank DiMaio, Bruno Correia, Sergey Ovchinnikov, and David Baker

Subjects
Protein Folding, Binding Sites, Multidisciplinary, binding, Proteins, crystal-structure, novo design, prediction, Protein Engineering, Catalysis, Protein Structure, Secondary, Deep Learning, potent, sequence design, complex, Protein Binding
Abstract

The binding and catalytic functions of proteins are generally mediated by a small number of functional residues held in place by the overall protein structure. Here, we describe deep learning approaches for scaffolding such functional sites without needing to prespecify the fold or secondary structure of the scaffold. The first approach, “constrained hallucination,” optimizes sequences such that their predicted structures contain the desired functional site. The second approach, “inpainting,” starts from the functional site and fills in additional sequence and structure to create a viable protein scaffold in a single forward pass through a specifically trained RoseTTAFold network. We use these two methods to design candidate immunogens, receptor traps, metalloproteins, enzymes, and protein-binding proteins and validate the designs using a combination of in silico and experimental tests.

276. Synthesis of novel pyrrolidine 3,4-diol derivatives as inhibitors of alpha-L-fucosidases

Author

Moreno-Clavijo, Elena, Carmona, Ana T., Vera-Ayoso, Yolanda, Moreno-Vargas, Antonio J., Bello, Claudia, Vogel, Pierre, and Robina, Inmaculada

Subjects
L-Fucose, Enantioselective Synthesis, Potent, Glycosidase Inhibitors, Stereoselective-Synthesis, Aza-C-Disaccharides, Cystic-Fibrosis, Biological Evaluation, Discovery, Colorectal-Cancer
Abstract

The stereoselective synthesis of new 3,4-dihydroxypyrrolidine derivatives starting from D-mannose, D-ribose and L-fucose is presented. Two synthetic strategies employing organometallic addition to hemiacetalic sugars followed by selective nucleophilic displacement or conjugate addition of ammonia to conjugate aldonic esters as key steps, are used. The new compounds were assayed for their inhibitory activity towards 13 commercially available glycosidases. Compounds that share the absolute configuration at C(2,3,4,5) of L-fucopyranosides and incorporate aromatic moieties are potent and selective inhibitors of alpha-L-fucosidases in the nM range.

277. Synthesis of tri-and tetramines containing two 2,3-dihydroxypyrrolidine moieties and their inhibitory activity toward alpha-mannosidases

Author

Gerber-Lemaire, S, Popowycz, F, Rodriguez-Garcia, E, Schutz, C, Asenjo, ATC, Robina, I, and Vogel, P

Subjects
advanced malignancies, galactosidase, processinginhibitor, mannostatin-a, potent, biologicalevaluation, 3 deoxy derivatives, glycosidase inhibitors, n-butyldeoxynojirimycin, swainsonine
Abstract

Through the reductive amination of N-[(tert-butoxy) carbonyl]-2,5-dideoxy-2,5-imino-3,4-O-isopropylidene-L-ribose with tetramethylenediamine, hexamethylenediamine, 2,7-diaminofluorene, 4,4'-diaminodiphenylmethane and 1,4-(diaminomethyl) benzene, five tetramines containing two (2R, 3R, 4S)-2-aminomethylpyrrolidine- 3,4- diol moieties have been prepared and assayed for their inhibitory activities toward 24 glycosidases. Tetramines containing the tetramethylene or benzene-1,4-dimethylene linkers are more potent amannosidase inhibitors than simple (2R, 3R, 4S)-2-aminomethylpyrrolidine- 3,4-diols. Triamines such as (2S, 3R, 4S)-bis(3,4-dihydroxy-pyrrolidin-2-ethyl) amine were also prepared and shown to be better alpha-mannosidase inhibitors than (2S, 3R, 4S)- 2-(2-aminoethyl) pyrrolidin-3,4-diol.

278. Design, synthesis, and biological evaluation of 1-ethyl-3-(thiazol-2-yl)urea derivatives as Escherichia coli DNA gyrase inhibitors

Author

Janez Ilaš, Nace Zidar, Tihomir Tomašič, Danijel Kikelj, Michaela Barančoková, Päivi Tammela, Faculty of Pharmacy, Bioactivity Screening Group, Division of Pharmaceutical Biosciences, and Drug Research Program

Subjects
Ethylurea, ANTIBACTERIAL ACTIVITY, Pharmaceutical Science, 01 natural sciences, DNA gyrase, STRUCTURE-GUIDED DESIGN, chemistry.chemical_compound, Drug Discovery, Enterococcus faecalis, Topoisomerase II Inhibitors, Urea, biology, Strain (chemistry), ATP-BINDING-SITE, Molecular Structure, THIAZOLE, INHIBITOR, 3. Good health, Anti-Bacterial Agents, IIA TOPOISOMERASES, Biochemistry, 317 Pharmacy, Pseudomonas aeruginosa, Efflux, Antibacterial activity, Staphylococcus aureus, Topoisomerase IV, N-PHENYLINDOLAMIDES, education, Microbial Sensitivity Tests, Acetic acid, Structure-Activity Relationship, Antibiotic resistance, Escherichia coli, B INHIBITORS, Thiazole, AGENTS, TOPOISOMERASE-IV, Dose-Response Relationship, Drug, 010405 organic chemistry, POTENT, antibacterial, DNA gyrase, ethylurea, inhibitor, thiazole, 0104 chemical sciences, udc:547.7/.8, Antibacterial, 010404 medicinal & biomolecular chemistry, Thiazoles, chemistry, DISCOVERY, Drug Design, biology.protein
Abstract

Discovery of novel DNA gyrase B inhibitors remains an attractive field in the search for new antibacterial drugs to overcome the known bacterial resistance mechanisms. In the present study, we designed and synthesized novel ethylurea derivatives of 4,5,6,7-tetrahydrobenzo[1,2-d]thiazole-2,6-diamine, 2-(2-aminothiazol-4-yl)acetic acid, and benzo[1,2-d]thiazole-2,6-diamine and evaluated their Escherichia coli DNA gyrase inhibition. The most potent DNA gyrase inhibitors in the prepared library of compounds were benzo[1,2-d]thiazoles 32-34, 36, and 37 with IC50 values in the low micromolar range. The most promising inhibitors identified were evaluated against selected Gram-positive and Gram-negative bacterial strains. Compound 33 showed a MIC of 50microM against an E. coli efflux pump-defective strain, which suggests that efflux decreases the on-target concentrations of these compounds. Nasl. z nasl. zaslona. Opis vira z dne 14. 12. 2017. Bibliografija: str. 15-16. Abstract. ARRS Marie Skłodowska-Curie ETN INTEGRATE Academy of Finland Academy of Finland

Full Text
View/download PDF

Catalog

Books, media, physical & digital resources
See catalog results