Your search keyword '"Jorge D. Brioni"' showing total 7 results

1. Use of the H3 receptor antagonist radioligand [3H]-A-349821 to reveal in vivo receptor occupancy of cognition enhancing H3 receptor antagonists

Author

Kennan C. Marsh, Marlon D. Cowart, Jorge D. Brioni, Ivan Milicic, Timothy A. Esbenshade, J Bauch, J Du, Thomas R. Miller, Kaitlin E. Browman, and Bruce W. Surber

Subjects

Pharmacology, medicine.medical_specialty, Biology, Radioligand Assay, chemistry.chemical_compound, Endocrinology, chemistry, In vivo, Competitive antagonist, Internal medicine, Radioligand, medicine, Histamine H3 receptor, Receptor, H3 receptor antagonist, ABT-239, medicine.drug

Abstract

Background and purpose: The histamine H3 receptor antagonist radioligand [3H]-A-349821 was characterized as a radiotracer for assessing in vivo receptor occupancy by H3 receptor antagonists that affect behaviour. This model was established as an alternative to ex vivo binding methods, for relating antagonist H3 receptor occupancy to blood levels and efficacy in preclinical models. Experimental approach: In vivo cerebral cortical H3 receptor occupancy by [3H]-A-349821 was determined in rats from differences in [3H]-A-349821 levels in the isolated cortex and cerebellum, a brain region with low levels of H3 receptors. Comparisons were made to relate antagonist H3 receptor occupancy to blood levels and efficacy in a preclinical model of cognition, the five-trial inhibitory avoidance response in rat pups. Key results: In adult rats, [3H]-A-349821, 1.5 µg·kg−1, penetrated into the brain and cleared more rapidly from cerebellum than cortex; optimally, [3H]-A-349821 levels were twofold higher in the latter. With increasing [3H]-A-349821 doses, cortical H3 receptor occupancy was saturable with a binding capacity consistent with in vitro binding in cortex membranes. In studies using tracer [3H]-A-349821 doses, ABT-239 and other H3 receptor antagonists inhibited H3 receptor occupancy by [3H]-A-349821 in a dose-dependent manner. Blood levels of the antagonists corresponding to H3 receptor occupancy were consistent with blood levels associated with efficacy in the five-trial inhibitory avoidance response. Conclusions and implications: When employed as an occupancy radiotracer, [3H]-A-349821 provided valid measurements of in vivo H3 receptor occupancy, which may be helpful in guiding and interpreting clinical studies of H3 receptor antagonists.

Published

2009

2. In vitro and in vivo characterization of A-940894: a potent histamine H4 receptor antagonist with anti-inflammatory properties

Author

J. L. Baranowski, David G. Witte, RM Adair, K. C. Marsh, Jorge D. Brioni, AM Manelli, Tracy L. Carr, Cowart, H. Liu, Jill M. Wetter, Carolyn A. Cuff, Betty B. Yao, Timothy A. Esbenshade, M. I. Strakhova, TA Vortherms, L Rundell, Auriléia Aparecida de Brito, Thomas R. Miller, Mcpherson Michael J, and BM Bettencourt

Subjects

Pharmacology, Histamine H1 receptor, Biology, Mast cell, chemistry.chemical_compound, Histamine receptor, medicine.anatomical_structure, chemistry, Histamine H2 receptor, medicine, Eosinophil chemotaxis, Prostaglandin D2, Histamine H4 receptor, Histamine

Abstract

Background and purpose: The histamine H4 receptor is widely expressed in cells of immune origin and has been shown to play a role in a variety of inflammatory processes mediated by histamine. In this report, we describe the in vitro and in vivo anti-inflammatory properties of a potent histamine H4 receptor antagonist, A-940894 (4-piperazin-1-yl-6,7-dihydro-5H-benzo[6,7]cyclohepta[1,2-d]pyrimidin-2-ylamine). Experimental approach: We have analysed the pharmacological profile of A-940894 at mouse native, rat recombinant and human recombinant and native, histamine H4 receptors by radioligand binding, calcium mobilization, mast cell shape change, eosinophil chemotaxis assays and in the mouse model of zymosan-induced peritonitis. Key results: A-940894 potently binds to both human and rat histamine H4 receptors and exhibits considerably lower affinity for the human histamine H1, H2 or H3 receptors. It potently blocked histamine-evoked calcium mobilization in the fluorometric imaging plate reader assays and inhibited histamine-induced shape change of mouse bone marrow-derived mast cells and chemotaxis of human eosinophils in vitro. In a mouse mast cell-dependent model of zymosan-induced peritonitis, A-940894 significantly blocked neutrophil influx and reduced intraperitoneal prostaglandin D2 levels. Finally, A-940894 has good pharmacokinetic properties, including half-life and oral bioavailability in rats and mice. Conclusions and Implications: These data suggest that A-940894 is a potent and selective histamine H4 receptor antagonist with pharmacokinetic properties suitable for long-term in vivo testing and could serve as a useful tool for the further characterization of histamine H4 receptor pharmacology.

Published

2009

3. The histamine H3receptor: an attractive target for the treatment of cognitive disorders

Author

Timothy A. Esbenshade, Jorge D. Brioni, Kaitlin E. Browman, M. I. Strakhova, Marlon D. Cowart, and R. S. Bitner

Subjects

Pharmacology, Cognitive disorder, Heteroreceptor, medicine.disease, chemistry.chemical_compound, chemistry, Autoreceptor, medicine, Histamine H3 receptor, Neurotransmitter Agents, H3 receptor antagonist, Neurotransmitter, Psychology, Neuroscience, Histamine

Abstract

The histamine H3 receptor, first described in 1983 as a histamine autoreceptor and later shown to also function as a heteroreceptor that regulates the release of other neurotransmitters, has been the focus of research by numerous laboratories as it represents an attractive drug target for a number of indications including cognition. The purpose of this review is to acquaint the reader with the current understanding of H3 receptor localization and function as a modulator of neurotransmitter release and its effects on cognitive processes, as well as to provide an update on selected H3 antagonists in various states of preclinical and clinical advancement. Blockade of centrally localized H3 receptors by selective H3 receptor antagonists has been shown to enhance the release of neurotransmitters such as histamine, ACh, dopamine and norepinephrine, among others, which play important roles in cognitive processes. The cognitive-enhancing effects of H3 antagonists across multiple cognitive domains in a wide number of preclinical cognition models also bolster confidence in this therapeutic approach for the treatment of attention deficit hyperactivity disorder, Alzheimer's disease and schizophrenia. However, although a number of clinical studies examining the efficacy of H3 receptor antagonists for a variety of cognitive disorders are currently underway, no clinical proof of concept for an H3 receptor antagonist has been reported to date. The discovery of effective H3 antagonists as therapeutic agents for the novel treatment of cognitive disorders will only be accomplished through continued research efforts that further our insights into the functions of the H3 receptor.

Published

2008

4. Characterization of a novel ATP-sensitive K+ channel opener, A-251179, on urinary bladder relaxation and cystometric parameters

Author

Char-Chang Shieh, William A. Carroll, Michael E. Brune, Matsushita K, Yoshihisa Kurachi, Kristi L. Whiteaker, Adebola Fabiyi, Jorge D. Brioni, Anthony V. Daza, Murali Gopalakrishnan, Eduardo J. Molinari, Steven A. Buckner, Mitsuhiko Yamada, and Milicic Ia

Subjects

Pharmacology, Urinary bladder, medicine.diagnostic_test, business.industry, Pig bladder, Cystometry, medicine.disease, Potassium channel, chemistry.chemical_compound, Muscle relaxation, medicine.anatomical_structure, Overactive bladder, chemistry, Anesthesia, Pinacidil, Medicine, Potassium channel opener, business

Abstract

Background and Purpose: ATP-sensitive K+ channels (KATP) play a pivotal role in contractility of urinary bladder smooth muscle. This study reports the characterization of 4-methyl-N-(2,2,2-trichloro-1-(3-pyridin-3-ylthioureido)ethyl)benzamide (A-251179) as a KATP channel opener. Experimental Approach: Glyburide-sensitive membrane potential, patch clamp and tension assays were employed to study the effect of A-251179 in vitro. The in vivo efficacy of A-251179 was characterized by suppression of spontaneous contractions in obstructed rat bladder and by measuring urodynamic function of urethane-anesthetized rat models. Key Results: A-251179 was about 4-fold more selective in activating SUR2B-Kir6.2 derived KATP channels compared to those derived from SUR2A-Kir6.2. In pig bladder smooth muscle strips, A-251179 suppressed spontaneous contractions, about 27- and 71-fold more potently compared to suppression of contractions evoked by low-frequency electrical stimulation and carbachol, respectively. In vivo, A-251179 suppressed spontaneous non-voiding bladder contractions from partial outlet-obstructed rats. Interestingly, in the neurogenic model where isovolumetric contractions were measured by continuous transvesical cystometry, A-251179 at a dose of 0.3 μmol kg-1, but not higher, was found to increase bladder capacity without affecting either the voiding efficiency or changes in mean arterial blood pressure. Conclusions and Implications: The thioureabenzamide analog, A-251179 is a potent novel KATP channel opener with selectivity for SUR2B/Kir6.2 containing KATP channels relative to pinacidil. The pharmacological profile of A-251179 is to increase bladder capacity and to prolong the time between voids without affecting voiding efficiency and represents an interesting characteristic to be explored for further investigations of KATP channel openers for the treatment of overactive bladder. British Journal of Pharmacology (2007) 151, 467–475; doi:10.1038/sj.bjp.0707249

Published

2007

5. Blockade of mGluR1 receptor results in analgesia and disruption of motor and cognitive performances: effects of A-841720, a novel non-competitive mGluR1 receptor antagonist

Author

C. Zhong, G Z Zheng, O El-Kouhen, Gerard B. Fox, R Chang, Prisca Honore, Mario Mezler, A O Stewart, Robert B. Moreland, Pramila Bhatia, S J Baker, T Kolasa, N M Rodell, Michael W. Decker, L N Miller, Jorge D. Brioni, E A Cronin, Katharine L. Chu, M E Uchic, M Patel, J. B. Pan, PR Hollingsworth, Steve McGaraughty, S G Lehto, and Joseph P. Mikusa

Subjects

Pharmacology, Metabotropic receptor, Neurotransmitter receptor, Metabotropic glutamate receptor, Chemistry, medicine.drug_class, Neuropathic pain, Analgesic, medicine, Metabotropic glutamate receptor 1, Receptor, Receptor antagonist

Abstract

Background and purpose: To further assess the clinical potential of the blockade of metabotropic glutamate receptors (mGluR1) for the treatment of pain. Experimental approach: We characterized the effects of A-841720, a novel, potent and non-competitive mGluR1 antagonist in models of pain and of motor and cognitive function. Key results: At recombinant human and native rat mGluR1 receptors, A-841720 inhibited agonist-induced calcium mobilization, with IC50 values of 10.7±3.9 and 1.0±0.2 nM, respectively, while showing selectivity over other mGluR receptors, in addition to other neurotransmitter receptors, ion channels, and transporters. Intraperitoneal injection of A-841720 potently reduced complete Freund's adjuvant-induced inflammatory pain (ED50=23 μmol kg−1) and monoiodoacetate-induced joint pain (ED50=43 μmol kg−1). A-841720 also decreased mechanical allodynia observed in both the sciatic nerve chronic constriction injury and L5-L6 spinal nerve ligation (SNL) models of neuropathic pain (ED50=28 and 27 μmol kg−1, respectively). Electrophysiological studies demonstrated that systemic administration of A-841720 in SNL animals significantly reduced evoked firing in spinal wide dynamic range neurons. Significant motor side effects were observed at analgesic doses and A-841720 also impaired cognitive function in the Y-maze and the Water Maze tests. Conclusions and implications. The analgesic effects of a selective mGluR1 receptor antagonist are associated with motor and cognitive side effects. The lack of separation between efficacy and side effects in pre-clinical models indicates that mGluR1 antagonism may not provide an adequate therapeutic window for the development of such antagonists as novel analgesic agents in humans. British Journal of Pharmacology (2006) 149, 761–774. doi:10.1038/sj.bjp.0706877

Published

2006

6. Enhancement of apomorphine-induced penile erection in the rat by a selective α1D -adrenoceptor antagonist

Author

Karl-Erik Andersson, Hiroya Mizusawa, Jorge D. Brioni, James P. Sullivan, Petter Hedlund, and Johan Sjunnesson

Subjects

Pharmacology, medicine.medical_specialty, Adrenergic receptor, Chemistry, Antagonist, Alpha (ethology), Erectile tissue, Yohimbine, Apomorphine, Endocrinology, medicine.anatomical_structure, Internal medicine, medicine, Prazosin, medicine.symptom, Vasoconstriction, medicine.drug

Abstract

1. Effects of A-322312 (alpha(1B)-adrenoceptor (AR) antagonist), A-119637 (alpha(1D)-AR antagonist), prazosin (non-selective alpha(1)-AR antagonist), and yohimbine (alpha(2)-AR antagonist) were studied in rat corpus cavernosum (CC) and cavernous artery (Acc) preparations. Effects of intracavernous (i.c.) or intraperitoneal (i.p.) administration of alpha(1)-AR antagonists on apomorphine-induced erections were investigated. 2. A-119637 attenuated electrically induced contractions in isolated CC (-logIC(50); 8.12+/-0.15), and relaxed noradrenaline (NA)-contracted preparations by more than 90% at 10(-7) M. At the same concentration, the -logEC(50) value for NA in Acc was altered from 6.79+/-0.07 to 4.86+/-0.13. In the CC and Acc, prazosin similarly inhibited contractile responses. 3. Inhibitory effects of A-322312 (10(-7) M) in electrically activated CC were 32.3+/-5.1%, whereas no effect on concentration-response curves for NA was observed in the Acc. Yohimbine (10(-8) M and 10(-7) M), enhanced electrically-induced contractions in isolated CC by 20 to 50%. At 10(-6) M, inhibitory effects of yohimbine were obtained. 4. A-119637 (0.3 micromol kg(-1), i.p.) tripled the number of erections, and produced a 6 fold increase in the duration of apomorphine-induced erectile responses. A-322312, prazosin, or yohimbine did not enhance erections induced by apomorphine. None of the alpha(1)-AR antagonists significantly increased ICP upon i.c. administration. Decreases in blood pressure were seen with A-119637 and prazosin. 5. The present findings show that there is a functional predominance of the alpha(1D)-AR subtype in the rat erectile tissue, and that blockade of this receptor facilitates rat penile erection induced by a suboptimal dose of apomorphine.

Published

2002

7. Pharmacology of human sulphonylurea receptor SUR1 and inward rectifier K+channel Kir6.2 combination expressed in HEK-293 cells

Author

Victoria E. Scott, Eduardo J. Molinari, Lisa M. Monteggia, Jorge D. Brioni, Jean M. Roch, Kristi L. Whiteaker, Char Chang Shieh, James P. Sullivan, and Murali Gopalakrishnan

Subjects

Pharmacology, Membrane potential, endocrine system, ATP-sensitive potassium channel, Chemistry, Inward-rectifier potassium ion channel, Kir6.2, Potassium channel, Biochemistry, Biophysics, Diazoxide, medicine, Sulfonylurea receptor, Patch clamp, medicine.drug

Abstract

1. The pharmacological properties of K(ATP) channels generated by stable co-expression of the sulphonylurea receptor SUR1 and the inwardly rectifying K(+) channel Kir6.2 were characterized in HEK-293 cells. 2. [(3)H]-Glyburide (glibenclamide) bound to transfected cells with a B(max) value of 18.5 pmol mg(-1) protein and with a K(D) value of 0.7 nM. Specific binding was displaced by a series of sulphonylurea analogues with rank order potencies consistent with those observed in pancreatic RINm5F insulinoma and in the brain. 3. Functional activity of K(ATP) channels was assessed by whole cell patch clamp, cation efflux and membrane potential measurements. Whole cell currents were detected in transfected cells upon depletion of internal ATP or by exposure to 500 microM diazoxide. The currents showed weak inward rectification and were sensitive to inhibition by glyburide (IC(50)=0.92 nM). 4. Metabolic inhibition by 2-deoxyglucose and oligomycin treatment triggered (86)Rb(+) efflux from transfected cells that was sensitive to inhibition by glyburide (IC(50)=3.6 nM). 5. Diazoxide, but not levcromakalim, evoked concentration-dependen decreases in DiBAC(4)(3) fluorescence responses with an EC(50) value of 14.1 microM which were attenuated by the addition of glyburide. Diazoxide-evoked responses were inhibited by various sulphonylurea analogues with rank order potencies that correlated well with their binding affinities. 6. In summary, results from ligand binding and functional assays demonstrate that the pharmacological properties of SUR1 and Kir6.2 channels co-expressed in HEK-293 cells resemble those typical of native K(ATP) channels described in pancreatic and neuronal tissues.

Published

2000