Your search keyword '"Stefania Meini"' showing total 19 results

1. MEN15596, a novel nonpeptide tachykinin NK2 receptor antagonist

Author

Claudio Catalani, Claudio Valenti, Cecilia Cialdai, Carlo Alberto Maggi, Manuela Tramontana, Stefania Meini, Sandro Giuliani, Rose-Marie Catalioto, Maria Altamura, Alessandro Lecci, and Riccardo Patacchini

Subjects

Male, Agonist, medicine.medical_specialty, Colon, Swine, medicine.drug_class, Bronchoconstriction, Neurokinin A, Guinea Pigs, Pig bladder, Substance P, CHO Cells, Thiophenes, In Vitro Techniques, Pharmacology, Binding, Competitive, Mice, Radioligand Assay, chemistry.chemical_compound, Cricetulus, In vivo, Cricetinae, Internal medicine, medicine, Animals, Humans, Potency, Rats, Wistar, Receptor, Aged, Dose-Response Relationship, Drug, Cell Membrane, Antagonist, Dipeptides, Receptors, Neurokinin-2, Middle Aged, Peptide Fragments, Rats, Endocrinology, chemistry, Vasoconstriction, Female, Rabbits, Muscle Contraction

Abstract

The pharmacological profile of MEN15596 or (6-methyl-benzo[b]thiophene-2-carboxylic acid [1-(2-phenyl-1R-{[1-(tetrahydropyran-4-ylmethyl)-piperidin-4-ylmethyl]-carbamoyl}-ethylcarbamoyl)-cyclopentyl]-amide), a novel potent and selective tachykinin NK2 receptor antagonist endowed with oral activity, is described. At the human recombinant tachykinin NK2 receptor, MEN15596 showed subnanomolar affinity (pKi 10.1) and potently antagonized (pKB 9.1) the neurokinin A-induced intracellular calcium release. MEN15596 selectivity for the tachykinin NK2 receptor was assessed by binding studies at the recombinant tachykinin NK1 (pKi 6.1) and NK3 (pKi 6.4) receptors, and at a number of 34 molecular targets including receptors, transporters and ion channels. In isolated smooth muscle preparations MEN15596 showed a marked species selectivity at the tachykinin NK2 receptor with the highest antagonist potency in guinea-pig colon, human and pig bladder (pKB 9.3, 9.2 and 8.8, respectively) whereas it was three orders of magnitude less potent in the rat and mouse urinary bladder (pKB 6.3 and 5.8, respectively). In agreement with binding experiments, MEN15596 showed low potency in blocking selective NK1 or NK3 receptor agonist-induced contractions of guinea-pig ileum preparations (pA2

Published

2006

2. A way to manage the thermal flexibility of ligand candidates for bioassays

Author

Cristina Nativi, Antonio Guidi, Francesco Cuda, Stefania Meini, Stefano Menichetti, Franco Pasqui, Giuseppe Balacco, Maria Altamura, and Annalisa Guerri

Subjects

chemistry.chemical_classification, Flexibility (engineering), Chemistry, Ligand, Organic Chemistry, Nuclear magnetic resonance spectroscopy, Biochemistry, Physical chemical, Drug Discovery, Thermal, Organic chemistry, Bioassay, Biological system, Thioamide

Abstract

An original way to manage both stereochemistry and conformational constraints in ligand candidates for bioassays is presented with reference to a group of model N,N′-tetrasubstituted o-phthalamides and thioamides. The study shows that a scale of thermal flexibility in solution can be envisaged, the divisions of which are represented by compounds sharing quite similar geometrical features. NMR spectroscopy and powder X-ray analysis were used for the physical chemical investigation. An attempt to exploit the conformational instability of a model thioamide in the medium of a bioassay was also performed.

Published

2006

3. Pharmacology of an original and selective nonpeptide antagonist ligand for the human tachykinin NK2 receptor

Author

Maria Altamura, Antonio Guidi, Paola Cucchi, Carlo Alberto Maggi, Alessandro Giolitti, Claudio Catalani, Luigi Rotondaro, Franco Pasqui, Stefania Meini, Sabrina Zappitelli, Sandro Giuliani, and Francesca Bellucci

Subjects

Indoles, Inositol Phosphates, Morpholines, Neurokinin A, Mutation, Missense, Phthalic Acids, Gene Expression, CHO Cells, Substance P, Biology, Ligands, Tritium, Binding, Competitive, Saredutant, Iodine Radioisotopes, Radioligand Assay, Cricetulus, Piperidines, Cricetinae, medicine, Animals, Humans, Protein Isoforms, Binding site, Receptor, G protein-coupled receptor, Pharmacology, Dose-Response Relationship, Drug, Cell Membrane, Antagonist, Receptors, Neurokinin-2, Ligand (biochemistry), Biochemistry, Competitive antagonist, Benzamides, Tachykinin receptor, medicine.drug

Abstract

The pharmacological outline of a novel and original antagonist at the human tachykinin NK 2 receptor is presented, namely MEN13510 ( N - N ′-bis-[2-(1 H -indol-3-yl)-ethyl]- N , N ′-bis-(3-thiomorpholin-4-yl-propyl)-phthalamide). MEN13510 retained nanomolar affinity for the human tachykinin NK 2 receptor ( K i 6.4 nM), and micromolar affinity for the human tachykinin NK 1 and NK 3 receptors. A competitive antagonism is indicated by the Schild analysis (p K B 7.8, slope − 0.94) of concentration–response curves of NKA induced inositolphosphates accumulation in Chinese hamster ovary (CHO) cells expressing the human NK 2 receptor in the presence of MEN13510 (30–300 nM concentration range). The MEN13510 interaction with the human NK 2 receptor was evaluated by means of heterologous inhibition binding experiments, by using agonist and antagonist radioligands ([ 125 I]NKA, [ 3 H]nepadutant, [ 3 H]saredutant) at a series of mutant receptors having single aminoacidic substitutions of residues located in transmembrane (TM) segments 3, 4, 5, 6, and 7. MEN13510 affinity was not affected by the mutations in TM 3 and 4 (Q109A, F112A, T171A, C167G), and it was reduced by 10-fold at the I202F mutant, but not at the Y206A (TM4). Amongst the investigated mutants bearing the mutated residues in TM6 (F270A, Y266F, W263A) only F270A decreased the MEN13510 affinity by 7-fold. Even mutations in TM7 did reduce MEN13510 affinity by 32-fold (Y289T, but not Y289F) and 13-fold (F293A). Studied mutations represent the human tachykinin NK 2 receptor discriminants involved in the binding of previously reported peptidic and nonpeptidic antagonists, against which results obtained with MEN13510 are compared. Results indicate that the binding site of this antagonist is, at least in part, overlapping to that described for NKA or saredutant. Finally we show that MEN13510 retains nanomolar affinity for the recently discovered splice variant of the human tachykinin NK 2 receptor, namely β isoform, as it has been described for the nonpeptide antagonist saredutant.

Published

2005

4. Pharmacological evaluation of α and β human tachykinin NK2 receptor splice variants expressed in CHO cells

Author

Luigi Rotondaro, Carlo Alberto Maggi, Stefania Meini, Rose-Marie Catalioto, Alessandro Giolitti, Sandro Giuliani, Angela Faiella, Francesca Bellucci, Laura Quartara, Claudio Catalani, Francisco M. Pinto, and María L. Candenas

Subjects

Gene isoform, Inositol Phosphates, Neurokinin A, Molecular Sequence Data, Intracellular Space, Substance P, CHO Cells, Biology, Transfection, Tritium, Binding, Competitive, Peptides, Cyclic, Iodine Radioisotopes, Radioligand Assay, chemistry.chemical_compound, Cricetulus, Piperidines, Cricetinae, Enzyme-linked receptor, Animals, Humans, Protein Isoforms, Amino Acid Sequence, Inositol phosphate, Receptor, Pharmacology, chemistry.chemical_classification, Sequence Homology, Amino Acid, musculoskeletal, neural, and ocular physiology, Chinese hamster ovary cell, Cell Membrane, Receptors, Neurokinin-2, Molecular biology, Alternative Splicing, chemistry, Biochemistry, Benzamides, Calcium, Tachykinin receptor

Abstract

In the present study, we have investigated, by binding and functional experiments, the pharmacological profile of a new human tachykinin NK(2) receptor splice variant named beta isoform. Neurokinin A, nepadutant, SR48968 [(S)-N-methyl-N[4-(4-acetylamino-4-phenyl piperidino)-2-(3,4-dichlorophenyl) butyl]benzamide] and substance P have been tested for binding on the receptor expressed in whole CHO transfected cells. Only SR48968 binds, but with an affinity about sixfold lower in respect to the alpha isoform. Moreover, neurokinin A was unable to inhibit the [(3)H]SR48968 binding to the beta isoform up to microM concentrations. In cells expressing the human tachykinin NK(2) receptor beta isoform, contrary to those expressing the alpha isoform, natural or selective tachykinin receptor agonists (1 microM) were unable to produce a significant activation of inositol phosphate (IP) production or increase of intracellular calcium concentration [Ca(2+)](i). The recently discovered tachykinins, endokinins C and D, did not activate IP production or [Ca(2+)](i) increase in cells expressing the alpha or beta isoform of the human tachykinin NK(2) receptor. The present data indicate that the human tachykinin NK(2) receptor beta isoform is poorly or not expressed on the cell membrane surface and that it may possibly act as a regulator of tachykinin NK(2) receptor function. We cannot exclude the possibility that this receptor could interact with other presently unknown ligands.

Published

2004

5. The N-terminal of Icatibant and bradykinin interact with the same Asp residues in the human B2 receptor

Author

Laura Quartara, Stefania Meini, Carlo Alberto Maggi, Paola Cucchi, Alessandro Giolitti, Luigi Rotondaro, Sandro Giuliani, Francesca Bellucci, Sabrina Zappitelli, and Claudio Catalani

Subjects

Pharmacology, Agonist, Aspartic Acid, Dose-Response Relationship, Drug, Receptor, Bradykinin B2, Bradykinin B2 Receptor Antagonists, Chemistry, Stereochemistry, medicine.drug_class, Bradykinin, Peptide Fragments, chemistry.chemical_compound, Icatibant, Cricetinae, Quinolines, medicine, Animals, Humans, Bradykinin receptor, B2 Bradykinin Receptor, Receptor, G protein-coupled receptor

Abstract

The pharmacology of peptide and non-peptide bradykinin B2 receptor ligands was evaluated in the inositol phosphate (IP) production assay in CHO cells expressing the human bradykinin B2 receptor. The effect of single and double alanine mutation of D266 and D284 residues at the human bradykinin B2 receptor was evaluated on the agonist profile of bradykinin (H-Arg-Pro-Pro-Gly-Phe-Ser-Pro-Phe-Arg-OH) and the synthetic agonist FR190997 (8-[2,6-dichloro-3-[N-methylcarbamoyl)cinnamidoacetyl]-N-methylamino]benzyloxy]-2-methyl-4-(2-pyridylmethoxy)quinoline). Bradykinin potency (EC50 0.5 nM at the wild-type receptor) was reduced by 16-fold at D266A and D284A mutants and by 2300-fold at the D266A/D284A double mutant. None of the mutants affected the potency or the efficacy of FR190997. Peptide antagonists, Icatibant (H-DArg-Arg-Pro-Hyp-Gly-Thi-Ser-Dtic-Oic-Arg-OH) and MEN11270 (H-DArg-Arg-Pro-Hyp-Gly-Thi-c(Dab-DTic-Oic-Arg)c(7gamma-10alpha)) (100 nM) similarly antagonized the concentration-response curve to bradykinin or FR190997 (pA2 values 8.5 and 8.4 versus bradykinin and 8.2 and 8.4 versus FR190997) at the wild-type receptor. Non-peptide antagonists FR173657 ((E)-3-(6-acetamido-3-pyridyl)-N-[N-[2,4-dichloro-3-[(2-methyl-8-quinolinyl) oxymethyl]phenyl]-N-methylaminocarbonyl methyl]acrylamide) and LF16-0687 (1-[[2,4-dichloro-3-[(2,4-dimethylquinolin-8-yl)oxy] methyl]-phenyl]sulfonyl]-N-[3-[[4-(aminoiminomethyl)-phenyl]carbonylamino]propyl]-(S)-pyrrolidine carboxamide) (100 nM) showed an equivalent potency values in blocking the IP production induced by bradykinin or FR190997 (pA2 values 8.7 and 8.8 versus bradykinin and 8.8 and 8.6 versus FR190997). Whilst the antagonist potency of FR173657 and LF16-0687 was not affected by D266A/D284A double mutation (IP production induced by the synthetic agonist), that of Icatibant and MEN11270 was reduced by 50- and 200-fold. The antagonist potency of [Ala1]-Icatibant and [Ala2]-Icatibant (pA2 values at wild-type 7.7 and 6.4) was significantly less reduced (20-fold and 13-fold, respectively) by the D266A/D284A double mutation. Our results highlight a crucial role for two aspartic residues, D266 and D284, located at the top of transmembrane segments 6 and 7, in the high-affinity interaction of peptide antagonists with the human bradykinin B2 receptor. An interaction of these receptor residues with the N-terminal basic residues of Icatibant is hypothesized.

Published

2004

6. Site-directed mutagenesis at the human B2 receptor and molecular modelling to define the pharmacophore of non-peptide bradykinin receptor antagonists

Author

Paola Cucchi, Stefania Meini, Angela Faiella, Luigi Rotondaro, Carlo Alberto Maggi, Laura Quartara, Alessandro Giolitti, Claudio Catalani, and Francesca Bellucci

Subjects

Models, Molecular, Agonist, Receptor, Bradykinin B2, Stereochemistry, medicine.drug_class, CHO Cells, Binding, Competitive, Peptides, Cyclic, Biochemistry, Benzamidine, chemistry.chemical_compound, Cricetinae, Bradykinin B2 Receptor Antagonists, medicine, Animals, Humans, Binding site, Bradykinin receptor, Receptor, G protein-coupled receptor, Pharmacology, Chemistry, Wild type, Mutagenesis, Site-Directed, Quinolines, Female, Pharmacophore, Oligopeptides

Abstract

Combining site-directed mutagenesis with information obtained from molecular modelling of the bradykinin (BK) human B 2 receptor (hB 2 R) as derived from the bovine rhodopsin crystal structure [Science 289 (2000) 739], we previously defined a putative binding mode for the non-peptide B 2 receptor antagonists, FR173657 and LF16-0687 [Can J Physiol Pharmacol 80 (2002) 303]. The present work is aimed to define the specific role of the quinoline moiety in the pharmacophore of these non-peptide antagonists. The effect of the mutations I110A, L114A (TM, transmembrane 3), W256A (TM6), F292A, Y295A and Y295F (TM7) was evaluated. None of the mutations affected the binding interaction of peptide ligands: the agonist BK and the peptide antagonist MEN 11270. The affinities in competing for [ 3 H ]-BK binding and in blocking the BK-induced IP production by the non-peptide antagonists LF16-0687 and FR173657 at the wild type and mutant receptors were analysed. While the affinities of LF16-0687 and FR173657 were crucially decreased at the I110A, Y295A, and Y295F mutants, the W256A mutation affected the affinity of the LF16-0687 only. The important contribution of the quinoline moiety was shown by the inability of an analogue of LF16-0687, lacking this moiety, to affect BK binding at the wild type receptor. On the other hand, the benzamidine group did not interact with mutated residues, since LF16-0687 analogues without this group or with an oxidated benzamidine displayed pairwise loss of affinity on wild type and mutated receptors. Further differences between FR173657 and LF16-0687 were highlighted at the I110 and Y295 mutants when comparing binding (p K i ) and functional antagonist (p K B ) affinity. First, the I110A mutation similarly impaired their binding affinity (250-fold), but at a less extent the antagonist potency of FR173657 only. Second, both the hydroxyl and the phenyl moieties of the Y295 residue had a specific role in the LF16-0687 interaction with the receptor, as demonstrated at the Y295F and Y295A mutants, respectively, but not in that of FR173657. Present data identify a receptor binding pocket comprised among TM3, 6, and 7, which concerns the interaction of the non-peptide antagonists FR173657 and LF16-0687, but not that of the peptide agonist or antagonist. Results indicate the quinoline group as the involved pharmacophoric element, and that the studied residues are differently involved in the interaction. The analysis performed by means of the GRID software led us to propose different spatial orientations of the quinoline moieties and partially overlapping binding pockets for the two ligands: that of LF16-0687 is located in the lipophilic environment amongst I110 (TM3), W256 (TM6), and Y295 (TM7) residues, whereas that of FR173657 lies essentially between I110 and Y295.

Published

2004

7. Serum biomarkers detection clusters improve the detection of symptomatic treatment effect in knee osteoarthitis patients: the results of a phase ib/iia study with the b2 receptor antagonist fasitibant

Author

Claudio Catalani, Cristina Rossi, Paola Cucchi, C.A. Maggi, Andrea Nizzardo, Francesca Bellucci, Stefania Meini, and Angela Capriati

Subjects

musculoskeletal diseases, medicine.medical_specialty, Pathology, business.industry, Symptomatic treatment, Antagonist, Biomedical Engineering, Gastroenterology, Fasitibant, B2 receptor, Rheumatology, Serum biomarkers, Internal medicine, medicine, Orthopedics and Sports Medicine, business

Published

2014

8. Ala scan analogues of HOE 140. Synthesis and biological activities

Author

Domenico Regoli, Carlo Alberto Maggi, Alessandro Giolitti, Stefania Meini, Riccardo Patacchini, Renzo Ricci, Katia Varani, Anna Rizzi, Caterina Rizzi, Laura Quartara, Pier Andrea Borea, and Silvia Amadesi

Subjects

bradykinin B(2) receptor peptide antagonist, Umbilical Veins, Receptor, Bradykinin B2, Stereochemistry, Guinea Pigs, Peptide, In Vitro Techniques, Bradykinin, Binding, Competitive, Chemical synthesis, Structure-Activity Relationship, chemistry.chemical_compound, Drug Discovery, Peptide synthesis, Animals, Humans, Bioassay, Potency, Bradykinin Receptor Antagonists, Pharmacology, chemistry.chemical_classification, Oligopeptide, Alanine, binding experiments, Receptors, Bradykinin, Organic Chemistry, Antagonist, Muscle, Smooth, General Medicine, Amino acid, chemistry, Biochemistry

Abstract

The role of the amino acids contained in the sequence of HOE 140 (H-DArg(1)-Arg(2)-Pro(3)-Hyp(4)-Gly(5)-Thi(6)-Ser(7)-DTic(8)-Oic(9 )-Arg(10)-OH), a potent and selective bradykinin B(2) receptor peptide antagonist, has been investigated by the replacement of each original residue (one by one) with Ala. The resulting set of decapeptides has been tested for the B(2) antagonist activity as well as for competition with the binding of [3H]BK to plasma membranes of the human umbilical vein (hUV). Positive correlations have been established between data obtained with the bioassay and with the binding in the hUV (same species, same tissue) and also between the two bioassays, the guinea-pig ileum (GPI) and the hUV (different species, different tissue). The structure-activity study has shown that the replacement of any of the residues that constitute HOE 140 with Ala is accompanied by a decrease of potency of at least 1 log unit. The analogues can be divided into three groups, with Ala(1) and Ala(7) showing affinities lower than HOE 140 by a factor of 10, Ala(4) and Ala(10) by a factor of 100 and Ala(2), Ala(5), Ala(6), Ala(8) and Ala(9) by a factor higher than 100 (100-1000). To verify the effect of chirality, the DAla(5) and DSer(7) analogues were synthesized and it was found that the substitution with a D-residue in position 5 is not tolerated while that in position 7 is favourable. The DSer(7) derivative is the most potent analogue found in this study: it shows potency as high as that of HOE 140 in the bioassays.

Published

2000

9. Nociceptin and the micturition reflex

Author

Sandro Giuliani, Stefania Meini, Carlo Alberto Maggi, and Alessandro Lecci

Subjects

Central Nervous System, medicine.medical_specialty, Time Factors, Physiology, Vasodilator Agents, media_common.quotation_subject, Urinary Bladder, Inhibitory postsynaptic potential, Models, Biological, Nervous System, Biochemistry, Urination, Nociceptin Receptor, Cellular and Molecular Neuroscience, chemistry.chemical_compound, Endocrinology, Internal medicine, Reflex, medicine, Animals, Opioid peptide, Injections, Spinal, Receptors, Tachykinin, media_common, Dose-Response Relationship, Drug, Rats, Kinetics, Nociceptin receptor, medicine.anatomical_structure, Opioid Peptides, Spinal Cord, chemistry, Capsaicin, Peripheral nervous system, Injections, Intravenous, Receptors, Opioid, Excitatory postsynaptic potential

Abstract

The i.v. administration of nociceptin (10-100 nmol/kg) inhibits the micturition reflex in a naloxone-resistant manner. The effects induced by i.v. nociceptin were not observed in capsaicin-pretreated animals indicating that i.v. nociceptin inhibits the micturition reflex by inhibiting afferent discharge from capsaicin-sensitive nerves. Supporting this interpretation, nociceptin also inhibited the reflex but not the local bladder contraction induced by topical capsaicin and protects this reflex (but not the local contraction) by desensitization. Intrathecal nociceptin (10 nmol/rat) produces urodynamic modifications similar to those induced by the i.v. administration. Intracerebroventricular (i.c.v.) administration of nociceptin (0.3-1 nmol/rat) also inhibited the micturition reflex in a naloxone-resistant manner suggesting a direct effect on supraspinal sites controlling the micturition. Beyond the inhibitory effects exerted by nociceptin on the micturition reflex, a peripheral excitatory effect mediated by capsaicin-sensitive fibers was also detected. The application of nociceptin (5-50 nmol/rat) onto the bladder serosa when the intravesical volume was subthreshold for the triggering of the micturition reflex, activated the reflex in a dose-dependent manner; the same treatment produced a biphasic effect on the ongoing reflex. In addition to the triggering of micturition reflex, topical nociceptin evokes a local tonic-type contraction that was abolished by the coadministration of tachykinin NK(1) and NK(2) receptor antagonists. Altogether these results indicate that ORL(1) receptors are present at several sites for the integration of the micturition reflex, and that their activation may produce both excitatory or inhibitory effects, depending on the route of administration and the experimental conditions.

Published

2000

10. Kinin B1 receptor-mediated motor responses in normal or inflamed rat urinary bladder in vivo

Author

Carlo Alberto Maggi, Sandro Giuliani, Stefania Meini, Alessandro Lecci, Manuela Tramontana, and Marco Criscuoli

Subjects

Male, Agonist, medicine.medical_specialty, Contraction (grammar), Physiology, medicine.drug_class, Administration, Topical, media_common.quotation_subject, Urinary Bladder, Clinical Biochemistry, Stimulation, Bradykinin, Receptor, Bradykinin B1, Urethane, Biochemistry, Urination, Cellular and Molecular Neuroscience, Endocrinology, Reference Values, Tetrahydroisoquinolines, Internal medicine, Cystitis, medicine, Animals, Rats, Wistar, Cyclophosphamide, Bradykinin Receptor Antagonists, media_common, Urinary bladder, Dose-Response Relationship, Drug, Chemistry, Receptors, Bradykinin, Anti-Inflammatory Agents, Non-Steroidal, Ganglia, Parasympathetic, Kinin, musculoskeletal system, Receptor antagonist, Ganglionectomy, Rats, medicine.anatomical_structure, Reflex, Anesthetics, Intravenous, Muscle Contraction

Abstract

The rat urinary bladder is one of the few in vivo preparations in which kinin B1 receptor-mediated contractile responses have been described, but the nature (local or reflex) of these responses has not been characterized. We have investigated the motor effects of i.v. or topical (onto the bladder serosa) administration of the selective kinin B1 receptor agonist [des-Arg9]-bradykinin ([des-Arg9]-BK) in the normal or inflamed (cyclophosphamide-induced) urinary bladder in urethane-anaesthetized rats. In both normal and inflamed bladders [des-Arg9]-BK produced a tonic contraction of low amplitude (15 mmHg) with phasic contractions of high amplitude (or = 15 mmHg) superimposed (micturition reflex contractions). In inflamed bladders, the response to [des-Arg9]-BK was more prominent than in controls. Similar observations were made after the topical administration of [des-Arg9]-BK. In order to evaluate any time-dependency in the expression of B1 receptor-mediated bladder responses, [des-Arg9]-BK was administered in separate groups of control animals at 30 and 240 min after the completion of surgical procedures required for set-up of the preparation: no bladder contraction was detected at 30 min whereas both local and reflex contractions could be elicited by [des-Arg9]-BK at 240 min after the set up. In ganglionectomized rats, the response to [des-Arg9]-BK or the selective tachykinin NK2 receptor agonist [betaAla8]NKA(4-10) was evaluated at 30 and 240 min after the set up in inflamed or in control animals. The response to [des-Arg9]-BK was greater after inflammation although a time-dependent increase was evident in both groups; in contrast, the response to [betaAla8]NKA(4-10) was similar in both groups and remained constant over the observation period. After induction of inflammation, the tonic contraction induced by [des-Arg9]-BK in ganglionectomized rats was dose-dependently reduced by the kinin B1 receptor antagonist [desArg10]Hoe 140. The contractile response (number of micturition reflex contractions) induced by [des-Arg9]-BK in normal rats with intact pelvic nerves at 240 min from the set up was not changed after the administration of the selective B2 receptor antagonist Hoe 140. These results indicate that stimulation of bladder kinin B1 receptors evokes a local, tonic-type contraction with reflex contractions superimposed in both normal and inflamed bladders, but in the latter situation the motor responses are magnified.

Published

1999

11. Synthesis and biological activity of new bradykinin pseudopeptide B1 receptor agonists containing alkylic spacers

Author

Claudia Galoppini, Mariella Tancredi, Stefania Meini, Paolo Rovero, Laura Quartara, and Carlo Alberto Maggi

Subjects

chemistry.chemical_classification, Agonist, Tetrapeptide, Stereochemistry, medicine.drug_class, Organic Chemistry, Clinical Biochemistry, Pharmaceutical Science, Bradykinin, Peptide, Biological activity, Biochemistry, In vitro, chemistry.chemical_compound, chemistry, Drug Discovery, medicine, Molecular Medicine, Bradykinin receptor, Receptor, Molecular Biology

Abstract

The tetrapeptide in the central portion of bradykinin and desArg10-kallidin was replaced by alkyl spacers of various lengths (-NH(CH2)nCO-, n=5–11). When tested as agonists at the kinins receptors, these pseudopeptides showed significant activity only at the B1 receptor. In particular, the introduction of a dodecanoic spacer in the central portion of desArg10-kallidin reduces only tenfold the agonist activity at the B1 receptor.

Published

1997

12. Nitric oxide is the mediator of tachykinin NK3 receptor-induced relaxation in the circular muscle of the guinea-pig ileum

Author

Stefania Meini, Sandro Giuliani, Riccardo Patacchini, and Carlo Alberto Maggi

Subjects

Male, Agonist, medicine.medical_specialty, medicine.drug_class, Muscle Relaxation, Guinea Pigs, In Vitro Techniques, Substance P, Arginine, Nitric Oxide, Inhibitory postsynaptic potential, Apamin, Nitroarginine, omega-Conotoxins, Nitric oxide, chemistry.chemical_compound, Ileum, Internal medicine, Isoprenaline, medicine, Animals, Receptor, Pharmacology, Voltage-dependent calcium channel, Muscle, Smooth, Receptors, Neurokinin-3, Peptide Fragments, Endocrinology, chemistry, Tetrodotoxin, Peptides, Vasoactive Intestinal Peptide, medicine.drug

Abstract

The tachykinin NK3 receptor agonist, senktide, produces concentration-dependent contraction of the circular muscle of the guinea-pig ileum (EC50 2.59 nM). In the presence of the blocker of neuronal type of voltage-sensitive calcium channels, omega-conotoxin (0.1 microM), the contractile response to a low concentration of senktide was converted to an inhibitory effect on spontaneous activity of the ileum. This inhibitory effect was further enhanced in the presence of atropine (1 microM) and was abolished by tetrodotoxin (1 microM), indicating its neural origin. In the presence of atropine and omega-conotoxin, the inhibitory response to senktide (1 nM) was greatly inhibited or even abolished by L-nitroarginine (30 microM), its effect being prevented by L-arginine but not by D-arginine (300 microM in each case). Apamin (0.1 microM) failed to significantly affect the inhibitory response to senktide. Apamin enhanced spontaneous activity of the preparation while L-nitroarginine had no effect. Neither apamin nor L-nitroarginine affected the inhibitory response to isoprenaline. These findings indicate that inhibition of circular muscle activity produced through NK3 receptor stimulation in the guinea-pig ileum is mediated through a neuronal pathway involving nitric oxide or a nitric oxide-like substance(s) generation.

Published

1993

13. Tachykinin control of ferret airways: Mucus secretion, bronchoconstriction and receptor mapping

Author

Judith C.W. Mak, D.F Rogers, Stefania Meini, and J.A.L Rohde

Subjects

Male, Agonist, medicine.medical_specialty, Neurokinin B, medicine.drug_class, Bronchoconstriction, Neurokinin A, Substance P, Biology, Cellular and Molecular Neuroscience, chemistry.chemical_compound, Endocrinology, Tachykinins, Internal medicine, medicine, Animals, Methacholine Chloride, Receptors, Tachykinin, Submucosal glands, Endocrine and Autonomic Systems, Ferrets, Reproducibility of Results, Muscle, Smooth, General Medicine, respiratory system, Mucus, Peptide Fragments, Stimulation, Chemical, Receptors, Neurotransmitter, Trachea, Neurology, chemistry, Methacholine, Capsaicin, medicine.symptom, Tachykinin receptor, medicine.drug

Abstract

The effects of synthetic tachykinin receptor agonists on mucus secretion by ferret trachea was determined in vitro in Ussing chambers using 35SO4 as a mucus marker and the synthetic peptides [Sar9,Met(O2)11]substance P (SarSP), [beta Ala8]neurokinin A-(4-10) and [MePhe7] neurokinin B which are selective for NK1, NK2 and NK3 tachykinin-receptors respectively. The bronchomotor effects of the same agonists were also studied in vitro and tachykinin receptors were localized by autoradiographic mapping. SarSP was the only synthetic agonist able to elicit a concentration-dependent increase in mucus secretion and was much more potent than SP. The EC50 for SarSP was 1.7 x 10(-6) M. Moreover, the maximal increase in release of 35SO4 produced by SarSP 10(-5) M was 95% of the increase produced by methacholine 10(-4) M indicating that this concentration of SarSP induced a near maximal secretory response. There was no significant difference in the secretory action of SP administered from the luminal or the submucosal side of the tissue. Only the NK2 agonist was able to produce a concentration-dependent contractility of bronchial ring preparations and its effect was relatively weak (EC50 6.4 x 10(-6) M). Capsaicin (10(-5) M) produced only a slight increase in tracheal mucus secretion (28 +/- 5%; n = 6) and was completely ineffective in inducing bronchoconstriction. Binding sites for [125I]-Bolton Hunter SP were more evident than sites for [125I]-NKA on submucosal glands and epithelium. In contrast, only binding sites to NKA could be observed over the smooth muscle.(ABSTRACT TRUNCATED AT 250 WORDS)

Published

1993

14. 220 BRADYKININ, THROUGH B2 RECEPTORS, ACTIVATES THE RELEASE OF THE CYTOKINE INTERLEUKIN 6, THE CHEMOKINE INTERLEUKIN 8, AND THE METALLOPROTEINASE 3 IN HUMAN KNEE CHONDROCYTES

Author

Claudio Catalani, S. Giuliani, C.A. Maggi, Stefania Meini, Paola Cucchi, and Francesca Bellucci

Subjects

medicine.medical_specialty, biology, Chemistry, Cartilage, medicine.medical_treatment, Biomedical Engineering, Interleukin, Interleukin 1 receptor, type II, Interleukin 20, medicine.anatomical_structure, Cytokine, Endocrinology, Rheumatology, Proteoglycan, Internal medicine, medicine, biology.protein, Orthopedics and Sports Medicine, Interleukin 8, Interleukin 1 receptor, type I

Abstract

Results: Cartilage cultured in the presence of blood showed a decrease of proteoglycan synthesis rate of 70%, an increase of proteoglycan release of 100%, and a decrease of proteoglycan content of 15% after 16 days of culture (all p

Published

2010

15. Characterization of the NK-2 receptor which mediates the motor response to tachykinins in human isolated bronchi

Author

C.A. Maggi, M. Astolfi, Stefania Meini, S. Treggiari, and Stefano Manzini

Subjects

Cellular and Molecular Neuroscience, Endocrinology, Neurology, Endocrine and Autonomic Systems, General Medicine, Anatomy, Biology, Receptor, Cell biology

Published

1993

16. Effect of selective tachykinin agonists on mucus secretion and smooth muscle contraction in ferret airways

Author

D.F. Rogers, Peter J. Barnes, Stefania Meini, and Stefano Manzini

Subjects

Cellular and Molecular Neuroscience, medicine.medical_specialty, Endocrinology, Neurology, Endocrine and Autonomic Systems, Chemistry, Internal medicine, medicine, Secretion, General Medicine, Smooth muscle contraction, Mucus

Published

1992

17. Antagonism by isbufylline, and its metabolite (1-methyl-7-isobutyl-xanthine), of capsaicin-induced motor and inflammatory effects in guinea pig airways

Author

Stefania Meini, Antonio Giachetti, Stefano Manzini, and Luigi Abelli

Subjects

Pharmacology, Guinea pig, chemistry.chemical_compound, chemistry, Capsaicin, Metabolite, ISBUFYLLINE, Antagonism, Xanthine

Published

1990

18. Sensory neuropeptides and asthma pathophysiology

Author

Lido Ballati, Francesca Perretti, Stefano Manzini, and Stefania Meini

Subjects

Pharmacology, business.industry, medicine, Neuropeptide, Sensory system, medicine.disease, business, Neuroscience, Pathophysiology, Asthma

Published

1990

19. Contractile effect of endothelin on isolated iris sphincter muscle of the pig

Author

Pierangelo Geppetti, Stefania Meini, Riccardo Patacchini, and Stefano Manzini

Subjects

Atropine, medicine.medical_specialty, Contraction (grammar), Swine, Iris sphincter muscle, Iris, Tetrodotoxin, In Vitro Techniques, Biology, chemistry.chemical_compound, Internal medicine, medicine, Animals, Pharmacology, Endothelins, Muscle, Smooth, medicine.anatomical_structure, Endocrinology, chemistry, Capsaicin, Sphincter, medicine.symptom, Peptides, Endothelin receptor, Muscle Contraction, medicine.drug, Muscle contraction

Abstract

Porcine endothelin (1 nM-0.3 microM) produced a concentration-dependent contraction of the isolated sphincter muscle of the pig iris. Neither atropine (1 microM) nor tetrodotoxin (1 microM) nor pre-exposure of the preparation to 10 microM capsaicin for 15 min affected the endothelin-induced response. We propose that the endothelin-induced contraction of the iris sphincter muscle of the pig is largely due to a direct action on smooth muscle cells and is unrelated to neurogenic myotic mechanisms.

Published

1989