Your search keyword '"Nadzan AM"' showing total 42 results

1. Novel trifluoroacetophenone derivatives as malonyl-CoA decarboxylase inhibitors.

Author

Wallace DM, Haramura M, Cheng JF, Arrhenius T, and Nadzan AM

Subjects

Indicators and Reagents, Malonyl Coenzyme A metabolism, Propanols chemistry, Structure-Activity Relationship, Acetophenones chemical synthesis, Acetophenones pharmacology, Carboxy-Lyases antagonists & inhibitors, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors pharmacology

Abstract

A series of trifluoroacetophenone derivatives were prepared and evaluated as malonyl-CoA decarboxylase (MCD) inhibitors. Some of the 'reverse amide' analogs were found to be potent inhibitors of MCD enzyme activity. The trifluoroacetyl group may interact with the MCD active site as the hydrate in a similar fashion to the hexafluoroisopropanol analogs reported previously. Adding electron-withdrawing groups to the phenyl ring stabilizes the hydrated species and enhances this interaction.

Published

2007

2. Discovery of potent and orally available malonyl-CoA decarboxylase inhibitors as cardioprotective agents.

Author

Cheng JF, Huang Y, Penuliar R, Nishimoto M, Liu L, Arrhenius T, Yang G, O'leary E, Barbosa M, Barr R, Dyck JR, Lopaschuk GD, and Nadzan AM

Subjects

Administration, Oral, Animals, Biological Availability, Cardiotonic Agents pharmacokinetics, Cardiotonic Agents pharmacology, Crystallography, X-Ray, Isoxazoles pharmacokinetics, Isoxazoles pharmacology, Molecular Conformation, Myocardial Ischemia drug therapy, Myocardial Ischemia physiopathology, Myocardial Reperfusion, Rats, Rats, Sprague-Dawley, Stereoisomerism, Structure-Activity Relationship, Carboxy-Lyases antagonists & inhibitors, Cardiotonic Agents chemical synthesis, Isoxazoles chemical synthesis

Abstract

Discovery of 5-(1,1,1,3,3,3-hexafluoro-2-hydroxypropan-2-yl)-4,5-dihydroisoxazole-3-carboxamides as a new class of malonyl-coenzyme A decarboxylase (MCD) inhibitors is described. tert-Butyl 3-(5-(1,1,1,3,3,3-hexafluoro-2-hydroxypropan-2-yl)-4,5-dihydroisoxazole-3-carboxamido)butanoate (5, CBM-301940) exhibited excellent potency and in vivo PK/ADME properties. It is the most powerful stimulant of glucose oxidation reported to date in isolated working rat hearts. Compound 5 improved the cardiac efficiency and function in a rat heart global ischemia/reperfusion model, suggesting MCD inhibitors may be useful for the treatment of ischemic heart diseases.

Published

2006

3. Heteroaryl substituted bis-trifluoromethyl carbinols as malonyl-CoA decarboxylase inhibitors.

Author

Cheng JF, Mak CC, Huang Y, Penuliar R, Nishimoto M, Zhang L, Chen M, Wallace D, Arrhenius T, Chu D, Yang G, Barbosa M, Barr R, Dyck JR, Lopaschuk GD, and Nadzan AM

Subjects

Animals, Drug Evaluation, Preclinical, Enzyme Activation drug effects, Enzyme Inhibitors chemistry, Glucose chemistry, Glucose metabolism, Heart drug effects, In Vitro Techniques, Methanol analogs & derivatives, Molecular Structure, Oxidation-Reduction, Rats, Stereoisomerism, Structure-Activity Relationship, Carboxy-Lyases antagonists & inhibitors, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors pharmacology, Heterocyclic Compounds chemistry, Methanol chemical synthesis, Methanol pharmacology

Abstract

A series of heteroaryl-substituted bis-trifluoromethyl carbinols were prepared and evaluated as malonyl-CoA decarboxylase (MCD) inhibitors. Some thiazole-based derivatives showed potent in vitro MCD inhibitory activities and significantly increased glucose oxidation rates in isolated working rat hearts.

Published

2006

4. Aza-retinoids as novel retinoid X receptor-specific agonists.

Author

Farmer LJ, Marron KS, Canan Koch SS, Hwang CK, Kallel EA, Zhi L, Nadzan AM, Robertson DW, and Bennani YL

Subjects

Aza Compounds chemical synthesis, Aza Compounds chemistry, Molecular Structure, Retinoids chemical synthesis, Retinoids chemistry, Stereoisomerism, Structure-Activity Relationship, Aza Compounds pharmacology, Retinoid X Receptors agonists, Retinoids pharmacology

Abstract

A new structurally simple series of potent lipophilic aza-retinoids RXR agonists has been developed. SAR studies for the N-alkyl-azadienoic acids described here demonstrate that the RXR activity profile is sensitive to the N-alkyl chain length. Further, we have expanded the work to include azadienoic acids, which exhibited many accessible conformations leading to a better understanding of the SAR around the series.

Published

2006

5. Synthesis and structure-activity relationship of small-molecule malonyl coenzyme A decarboxylase inhibitors.

Author

Cheng JF, Chen M, Wallace D, Tith S, Haramura M, Liu B, Mak CC, Arrhenius T, Reily S, Brown S, Thorn V, Harmon C, Barr R, Dyck JR, Lopaschuk GD, and Nadzan AM

Subjects

Animals, Energy Metabolism drug effects, Fatty Acids metabolism, Glucose metabolism, In Vitro Techniques, Male, Malonyl Coenzyme A metabolism, Morpholines chemistry, Morpholines pharmacology, Myocardial Ischemia drug therapy, Myocardium enzymology, Myocardium metabolism, Oxidation-Reduction, Phenylurea Compounds chemistry, Phenylurea Compounds pharmacology, Rats, Rats, Sprague-Dawley, Structure-Activity Relationship, Swine, Carboxy-Lyases antagonists & inhibitors, Morpholines chemical synthesis, Phenylurea Compounds chemical synthesis

Abstract

The discovery and structure-activity relationship of first-generation small-molecule malonyl-CoA decarboxylase (MCD; CoA = coenzyme A) inhibitors are reported. We demonstrated that MCD inhibitors increased malonyl-CoA concentration in the isolated working rat hearts. Malonyl-CoA is a potent, endogenous, and allosteric inhibitor of carnitine palmitoyltransferase-I (CPT-I), a key enzyme for mitochondrial fatty acid oxidation. As a result of the increase in malonyl-CoA levels, fatty acid oxidation rates were decreased and the glucose oxidation rates were significantly increased. Demonstration of in vivo efficacy of methyl 5-(N-(4-(1,1,1,3,3,3-hexafluoro-2-hydroxypropan-2-yl)phenyl)morpholine-4-carboxamido)pentanoate (6u) in a pig ischemia model indicated that MCD inhibitors may be useful for treating ischemic heart diseases.

Published

2006

6. Design and synthesis of heterocyclic malonyl-CoA decarboxylase inhibitors.

Author

Cheng JF, Chen M, Liu B, Hou Z, Arrhenius T, and Nadzan AM

Subjects

Animals, Cardiotonic Agents pharmacology, Drug Design, Energy Metabolism, Enzyme Inhibitors pharmacology, Fatty Acids metabolism, Glucose metabolism, Imidazoles chemistry, Models, Chemical, Myocardial Ischemia drug therapy, Myocardial Ischemia metabolism, Oxidation-Reduction, Rats, Swine, Carboxy-Lyases antagonists & inhibitors, Cardiotonic Agents chemical synthesis, Enzyme Inhibitors chemical synthesis

Abstract

We have previously reported the discovery of small molecule inhibitors of malonyl-CoA decarboxylase (MCD) as novel metabolic modulators, which inhibited fatty acid oxidation and consequently increased the glucose oxidation rates in the isolated working rat hearts. MCD inhibitors were also shown to improve cardiac efficiency in rat and pig demand-induced ischemic models through the mechanism-based modulation of energy metabolism. Herein, we describe the design and synthesis of a series of novel heterocyclic MCD inhibitors with a preference for substituted imidazole and isoxazole.

Published

2006

7. Discovery and structure-activity relationship of coumarin derivatives as TNF-alpha inhibitors.

Author

Cheng JF, Chen M, Wallace D, Tith S, Arrhenius T, Kashiwagi H, Ono Y, Ishikawa A, Sato H, Kozono T, Sato H, and Nadzan AM

Subjects

Cells, Cultured, Dose-Response Relationship, Drug, Humans, Inhibitory Concentration 50, Leukocytes, Mononuclear metabolism, Lipopolysaccharides pharmacology, Structure-Activity Relationship, Tumor Necrosis Factor-alpha metabolism, Coumarins chemical synthesis, Coumarins pharmacology, Tumor Necrosis Factor-alpha antagonists & inhibitors

Abstract

The discovery and structure-activity relationship of a novel series of coumarin-based TNF-alpha inhibitors is described. Starting from the initial lead 1a, various derivatives were prepared surrounding the coumarin core structure to optimize the in vitro inhibitory activity of TNF-alpha production by human peripheral blood mononuclear cells (hPBMC), stimulated by bacterial lipopolysaccharide (LPS). Selected compounds also demonstrated in vivo inhibition of TNF-alpha production in rats.

Published

2004

8. Malonyl coenzyme a decarboxylase inhibition protects the ischemic heart by inhibiting fatty acid oxidation and stimulating glucose oxidation.

Author

Dyck JR, Cheng JF, Stanley WC, Barr R, Chandler MP, Brown S, Wallace D, Arrhenius T, Harmon C, Yang G, Nadzan AM, and Lopaschuk GD

Subjects

Acetyl Coenzyme A, Animals, Cardiotonic Agents pharmacology, Energy Metabolism, Enzyme Inhibitors pharmacology, Esters metabolism, Glycolysis, Malonyl Coenzyme A metabolism, Mitochondria, Heart drug effects, Mitochondria, Heart metabolism, Models, Animal, Myocardial Ischemia metabolism, Oxidation-Reduction, Rats, Rats, Sprague-Dawley, Swine, Carboxy-Lyases antagonists & inhibitors, Cardiotonic Agents therapeutic use, Enzyme Inhibitors therapeutic use, Fatty Acids metabolism, Glucose metabolism, Myocardial Ischemia drug therapy, Myocardium metabolism

Abstract

Abnormally high rates of fatty acid oxidation and low rates of glucose oxidation are important contributors to the severity of ischemic heart disease. Malonyl coenzyme A (CoA) regulates fatty acid oxidation by inhibiting mitochondrial uptake of fatty acids. Malonyl CoA decarboxylase (MCD) is involved in the decarboxylation of malonyl CoA to acetyl CoA. Therefore, inhibition of MCD may decrease fatty acid oxidation and protect the ischemic heart, secondary to increasing malonyl CoA levels. Ex vivo working rat hearts aerobically perfused in the presence of newly developed MCD inhibitors showed an increase in malonyl CoA levels, which was accompanied by both a significant decrease in fatty acid oxidation rates and an increase in glucose oxidation rates compared with controls. Using a model of demand-induced ischemia in pigs, MCD inhibition significantly increased glucose oxidation rates and reduced lactate production compared with vehicle-treated hearts, which was accompanied by a significant increase in cardiac work compared with controls. In a more severe rat heart global ischemia/reperfusion model, glucose oxidation was significantly increased and cardiac function was significantly improved during reperfusion in hearts treated with the MCD inhibitor compared with controls. Together, our data show that MCD inhibitors, which increase myocardial malonyl CoA levels, decrease fatty acid oxidation and accelerate glucose oxidation in both ex vivo rat hearts and in vivo pig hearts. This switch in energy substrate preference improves cardiac function during and after ischemia, suggesting that pharmacological inhibition of MCD may be a novel approach to treating ischemic heart disease.

Published

2004

9. Expression, purification, and characterization of human malonyl-CoA decarboxylase.

Author

Zhou D, Yuen P, Chu D, Thon V, McConnell S, Brown S, Tsang A, Pena M, Russell A, Cheng JF, Nadzan AM, Barbosa MS, Dyck JR, Lopaschuk GD, and Yang G

Subjects

Amino Acid Sequence, Carboxy-Lyases genetics, Carboxy-Lyases isolation & purification, Cloning, Molecular, Escherichia coli genetics, Humans, Hydrogen-Ion Concentration, Molecular Sequence Data, Recombinant Proteins genetics, Recombinant Proteins isolation & purification, Recombinant Proteins metabolism, Sequence Homology, Substrate Specificity, Carboxy-Lyases metabolism

Abstract

The recombinant human malonyl-CoA decarboxylase (hMCD) was overexpressed in Escherichia coli with and without the first 39 N-terminal amino acids via a cleavable MBP-fusion construct. Proteolytic digestion using genenase I to remove the MBP-fusion tag was optimized for both the full length and truncated hMCD. The apo-hMCD enzymes were solubilized and purified to homogeneity. Steady-state kinetic characterization showed similar kinetic parameters for the MBP-fused and apo-hMCD enzymes with an apparent Km value of approximately 330-520 microM and a turnover rate kcat of 13-28s(-1). For the apo-hMCD enzymes, the N-terminal truncated hMCD was well tolerated over a broad pH range (pH 4-10); whereas the full-length hMCD appeared to be stable only at pH >/= 8.5. Our results showed that the N-terminal region of hMCD has no effect on the catalytic activity of the enzyme but plays a role in the folding process and conformation stability of hMCD.

Published

2004

10. Retinoic acid receptor ligands based on the 6-cyclopropyl-2,4-hexadienoic acid.

Author

Farmer LJ, Zhi L, Jeong S, Lamph WW, Osburn DL, Croston G, Flatten KS, Heyman RA, and Nadzan AM

Subjects

Binding, Competitive drug effects, Cell Differentiation drug effects, Cell Division drug effects, Humans, Indicators and Reagents, Ligands, Receptors, Retinoic Acid agonists, Receptors, Retinoic Acid genetics, Sorbic Acid chemical synthesis, Sorbic Acid pharmacology, Transfection, Tumor Cells, Cultured, Cyclopropanes chemical synthesis, Cyclopropanes pharmacology, Receptors, Retinoic Acid drug effects, Sorbic Acid analogs & derivatives

Abstract

A series of novel cyclopropanyl methyl hexadienoic acid retinoids was designed and prepared. These compounds exhibited either selective activity as RXR agonists or pan-agonists on one or more of each of the RAR and RXR isoforms. The most potent pan-agonist 5a (RAR's EC(50)=17-59 nM; RXR's EC(50)=6-14 nM) showed good antiproliferative properties in the in vitro cancer cell lines, ME 180 and RPMI 8226.

Published

2003

11. Analysis of combinatorial chemistry samples by micellar electrokinetic chromatography.

Author

Simms PJ, Jeffries CT, Huang Y, Zhang L, Arrhenius T, and Nadzan AM

Subjects

Chromatography, High Pressure Liquid, Indicators and Reagents, Spectrophotometry, Ultraviolet, Chromatography, Micellar Electrokinetic Capillary methods, Combinatorial Chemistry Techniques methods

Abstract

A micellar electrokinetic chromatography (MEKC) method has been developed that can evaluate the purity of samples generated in combinatorial chemistry libraries. This method uses an open tube capillary (27 cm x 50 microm) along with a run buffer composed of sodium dodecyl sulfate (SDS), hydroxypropyl-beta-cyclodextrin, and sodium tetraborate coupled with UV detection. Neutral compounds and compounds that were insoluble in aqueous buffers could be analyzed under these conditions in approximately 3 min. The concentration of SDS and the concentration of hydroxypropyl-beta-cyclodextrin effected the separation. The affect on selectivity resulting from the addition of an organic modifier to the run buffer was examined. The low background absorbency of the run buffer made for easy detection of compounds that absorbed at low UV wavelengths. The quick analysis time made this suitable for analysis of combinatorial chemistry samples.

Published

2001

12. Novel nonsecosteroidal vitamin D mimics exert VDR-modulating activities with less calcium mobilization than 1,25-dihydroxyvitamin D3.

Author

Boehm MF, Fitzgerald P, Zou A, Elgort MG, Bischoff ED, Mere L, Mais DE, Bissonnette RP, Heyman RA, Nadzan AM, Reichman M, and Allegretto EA

Subjects

Animals, Biological Transport, Breast Neoplasms pathology, Calcitriol pharmacology, Calcium Channel Agonists pharmacology, Cell Differentiation drug effects, Cell Division drug effects, Female, HL-60 Cells, Humans, Keratinocytes cytology, Keratinocytes drug effects, Ketones pharmacology, Macrophages cytology, Macrophages drug effects, Male, Mice, Molecular Mimicry, Phenyl Ethers pharmacology, Prostatic Neoplasms pathology, Rats, Receptors, Calcitriol metabolism, Transcriptional Activation, Vitamin D analogs & derivatives, Vitamin D chemical synthesis, Vitamin D-Binding Protein metabolism, Antineoplastic Agents pharmacology, Calcium metabolism, Receptors, Calcitriol physiology, Vitamin D pharmacology

Abstract

Background: The secosteroid 1,25-dihydroxyvitamin D3 (1,25(OH)2D3) acts through the vitamin D receptor (VDR) to elicit many activities that make it a promising drug candidate for the treatment of a number of diseases, including cancer and psoriasis. Clinical use of 1,25(OH)2D3 has been limited by hypercalcemia elicited by pharmacologically effective doses. We hypothesized that structurally distinct, nonsecosteroidal mimics of 1,25(OH)2D3 might have different activity profiles from vitamin D analogs, and set out to discover such compounds by screening small-molecule libraries., Results: A bis-phenyl derivative was found to activate VDR in a transactivation screening assay. Additional related compounds were synthesized that mimicked various activities of 1,25(OH)2D3, including growth inhibition of cancer cells and keratinocytes, as well as induction of leukemic cell differentiation. In contrast to 1, 25(OH)2D3, these synthetic compounds did not demonstrate appreciable binding to serum vitamin D binding protein, a property that is correlated with fewer calcium effects in vivo. Two mimics tested in mice showed greater induction of a VDR target gene with less elevation of serum calcium than 1,25(OH)2D3., Conclusions: These novel VDR modulators may have potential as therapeutics for cancer, leukemia and psoriasis with less calcium mobilization side effects than are associated with secosteroidal 1,25(OH)2D3 analogs.

Published

1999

13. Synthesis of retinoid X receptor-specific ligands that are potent inducers of adipogenesis in 3T3-L1 cells.

Author

Canan Koch SS, Dardashti LJ, Cesario RM, Croston GE, Boehm MF, Heyman RA, and Nadzan AM

Subjects

3T3 Cells, Adipocytes metabolism, Adipocytes physiology, Animals, Benzoates chemistry, Benzoates metabolism, Benzoates pharmacology, Binding, Competitive, Cell Differentiation drug effects, Cell Line, Crystallography, X-Ray, Ligands, Mice, Oximes chemistry, Oximes metabolism, Oximes pharmacology, Receptors, Cytoplasmic and Nuclear agonists, Receptors, Cytoplasmic and Nuclear biosynthesis, Receptors, Retinoic Acid biosynthesis, Receptors, Retinoic Acid metabolism, Recombinant Proteins agonists, Recombinant Proteins biosynthesis, Recombinant Proteins metabolism, Retinoid X Receptors, Transcription Factors biosynthesis, Transcription Factors metabolism, Transfection, Triglycerides metabolism, Adipocytes drug effects, Benzoates chemical synthesis, DNA-Binding Proteins metabolism, Oximes chemical synthesis, Receptors, Retinoic Acid agonists, Transcription Factors agonists

Abstract

A novel series of oxime ligands has been synthesized that displays potent, specific activation of the retinoid X receptors (RXRs). The oximes of 3-substituted (tetramethyltetrahydronaphthyl)carbonylbenzoic acids are readily available by condensation with hydroxyl- or methoxylamine; alkylation of the hydroxyl oxime provides a variety of analogues. Oximes and variously substituted oxime derivatives demonstrate high binding affinity for the RXRs and specific RXR activation and, hence, are called rexinoids. These oxime rexinoids are activators of the RXR:PPARgamma heterodimer and are potent inducers of differentiation of 3T3-L1 preadipocytes to adipocytes. We have recently reported that ligands which activate the RXR:PPARgamma heterodimer in this manner are effective in the treatment of type II diabetes (non-insulin-dependent diabetes mellitus, NIDDM). Thus, these new oxime rexinoids are potential therapeutic agents for the treatment of metabolic disorders, such as obesity and diabetes.

Published

1999

14. Synthesis and Characterization of a Highly Potent and Selective Isotopically Labeled Retinoic Acid Receptor Ligand, ALRT1550.

Author

Bennani YL, Marron KS, Mais DE, Flatten K, Nadzan AM, and Boehm MF

Abstract

The syntheses of two labeled homologues of (2E,4E,6E)-7-(3,5-di-tert-butylphenyl)-3-methylocta-2,4,6-trienoic acid (ALRT1550, 2), [(13)CD(3)]ALRT1550 (3) and [(3)H]ALRT1550 (4), are described in this report. ALRT1550 is an exceptionally potent antiproliferative agent which is currently in phase I/II clinical trials for acute chemotherapy. Both homologues were prepared from commercially available 3,5-di-tert-butylbenzoic acid. Homologue [(13)CD(3)]ALRT1550 was labeled at the 7-position of the trienoic acid chain via addition of [(13)CD(3)]MgI to a Weinreb amide precursor. The preparation of [(3)H]ALRT1550 utilized novel methodology to synthesize a sterically hindered and site-specific tritium-labeled tert-butyl group. Saturation binding and Scatchard analysis of this ligand at the retinoic acid receptors are also described, along with competition binding (K(i)) values for a series of known retinoids using [(3)H]ALRT1550 or [(3)H]ATRA as the labeled probes.

Published

1998

15. Sensitization of diabetic and obese mice to insulin by retinoid X receptor agonists.

Author

Mukherjee R, Davies PJ, Crombie DL, Bischoff ED, Cesario RM, Jow L, Hamann LG, Boehm MF, Mondon CE, Nadzan AM, Paterniti JR Jr, and Heyman RA

Subjects

Animals, Bexarotene, Blood Glucose metabolism, Cells, Cultured, Diabetes Mellitus, Type 2 blood, Female, Glucose Tolerance Test, Hypoglycemic Agents pharmacology, Insulin blood, Ligands, Mice, Mice, Inbred C57BL, Mice, Obese, Nicotinic Acids pharmacology, Obesity blood, Receptors, Cytoplasmic and Nuclear genetics, Receptors, Cytoplasmic and Nuclear metabolism, Receptors, Retinoic Acid genetics, Receptors, Retinoic Acid metabolism, Retinoid X Receptors, Rosiglitazone, Tetrahydronaphthalenes pharmacology, Thiazoles pharmacology, Transcription Factors genetics, Transcription Factors metabolism, Transfection, Diabetes Mellitus, Type 2 metabolism, Insulin pharmacology, Insulin Resistance, Obesity metabolism, Receptors, Retinoic Acid agonists, Thiazolidinediones, Transcription Factors agonists

Abstract

Retinoic acid receptors (RAR), thyroid hormone receptors (TR), peroxisome proliferator activated receptors (PPARs) and the orphan receptor, LXR, bind preferentially to DNA as heterodimers with a common partner, retinoid X receptor (RXR), to regulate transcription. We investigated whether RXR-selective agonists replicate the activity of ligands for several of these receptors? We demonstrate here that RXR-selective ligands (referred to as rexinoids) function as RXR heterodimer-selective agonists, activating RXR: PPARgamma and RXR:LXR dimers but not RXR:RAR or RXR:TR heterodimers. Because PPARgamma is a target for antidiabetic agents, we investigated whether RXR ligands could alter insulin and glucose signalling. In mouse models of noninsulin-dependent diabetes mellitus (NIDDM) and obesity, RXR agonists function as insulin sensitizers and can decrease hyperglycaemia, hypertriglyceridaemia and hyperinsulinaemia. This antidiabetic activity can be further enhanced by combination treatment with PPARgamma agonists, such as thiazolidinediones. These data suggest that the RXR:PPARgamma heterodimer is a single-function complex serving as a molecular target for treatment of insulin resistance. Activation of the RXR:PPARgamma dimer with rexinoids may provide a new and effective treatment for NIDDM.

Published

1997

16. A novel retinoic acid receptor-selective retinoid, ALRT1550, has potent antitumor activity against human oral squamous carcinoma xenografts in nude mice.

Author

Shalinsky DR, Bischoff ED, Lamph WW, Zhang L, Boehm MF, Davies PJ, Nadzan AM, and Heyman RA

Subjects

Animals, Carcinoma, Squamous Cell metabolism, Drug Screening Assays, Antitumor, Humans, Mice, Mice, Nude, Mouth Neoplasms metabolism, Receptors, Retinoic Acid metabolism, Transplantation, Heterologous, Antineoplastic Agents therapeutic use, Carcinoma, Squamous Cell drug therapy, Mouth Neoplasms drug therapy, Receptors, Retinoic Acid agonists, Retinoids therapeutic use

Abstract

We have identified a novel retinoid, ALRT1550, that potently and selectively activates retinoic acid receptors (RARs). ALRT1550 binds RARs with Kd values of approximately equal to 1-4 nM, and retinoid X receptors with low affinities (Kd approximately equal to 270-556 nM). We studied the effects of ALRT1550 on cellular proliferation in squamous carcinoma cells. ALRT1550 inhibited in vitro proliferation of UMSCC-22B cells in a concentration-dependent manner with an IC50 value of 0.22 +/- 0.1 (SE) nM. 9-cis-Retinoic acid (ALRT1057), a pan agonist retinoid that activates RARs and retinoid X receptors, inhibited proliferation with an IC50 value of 81 +/- 29 nM. In vivo, as tumor xenografts in nude mice, UMSCC-22B formed well-differentiated squamous carcinomas, and oral administration (daily, 5 days/week) of ALRT1550, begun 3 days after implanting tumor cells, inhibited tumor growth by up to 89% in a dose-dependent manner over the range of 3-75 micrograms/kg. ALRT1550 (30 micrograms/kg) also inhibited growth of established tumors by 72 +/- 3% when tumors were allowed to grow to approximately equal to 100 mm3 before dosing began. In comparison, 9-cis retinoic acid at 30 mg/kg inhibited growth of established tumors by 73 +/- 5%. Interestingly, retinoids did not appear to alter tumor morphologies in UMSCC-22B tumors. Notably, ALRT1550 produced a therapeutic index of approximately equal to 17 in this model, indicating a separation between doses that inhibited tumor growth and that induced symptoms of hypervitaminosis A. In summary, ALRT1550 potently inhibits cellular proliferation in vitro and in vivo in this squamous cell carcinoma tumor model. These data support additional study of ALRT1550 for its potential for improving anticancer therapy in human clinical trials.

Published

1997

17. Activation of specific RXR heterodimers by an antagonist of RXR homodimers.

Author

Lala DS, Mukherjee R, Schulman IG, Koch SS, Dardashti LJ, Nadzan AM, Croston GE, Evans RM, and Heyman RA

Subjects

DNA-Binding Proteins metabolism, Dimerization, Gene Expression Regulation, Ligands, Nuclear Receptor Co-Repressor 2, Receptors, Cytoplasmic and Nuclear metabolism, Receptors, Retinoic Acid agonists, Receptors, Retinoic Acid antagonists & inhibitors, Receptors, Retinoic Acid chemistry, Repressor Proteins metabolism, Retinoid X Receptors, Retinoids metabolism, TATA-Box Binding Protein, Trans-Activators metabolism, Transcription Factors agonists, Transcription Factors antagonists & inhibitors, Transcription Factors chemistry, Transcription, Genetic physiology, Transfection, Tumor Cells, Cultured, Drosophila Proteins, Nicotinic Acids pharmacology, Receptors, Retinoic Acid metabolism, Retinoids pharmacology, TATA-Binding Protein Associated Factors, Tetrahydronaphthalenes pharmacology, Transcription Factor TFIID, Transcription Factors metabolism

Abstract

Retinoid X receptor (RXR) plays a central role in the regulation of many intracellular receptor signalling pathways and can mediate ligand-dependent transcription, acting as a homodimer or as a heterodimer. Here we identify an antagonist towards RXR homodimers which also functions as an agonist when RXR is paired as a heterodimer to specific partners, including peroxisome proliferator-activated receptor and retinoic acid receptor. This dimer-selective ligand confers differential interactions on the transcription machinery: the antagonist promotes association with TAF110 (TATA-binding protein (TBP)-associated factor 110) and the co-repressor SMRT, but not with TBP, and these properties are distinct from pure RXR agonists. This unique class of RXR ligands will provide a means to control distinct target genes at the level of transcription and allow the development of retinoids with a new pharmacological action.

Published

1996

18. Identification of the first retinoid X, receptor homodimer antagonist.

Author

Canan Koch SS, Dardashti LJ, Hebert JJ, White SK, Croston GE, Flatten KS, Heyman RA, and Nadzan AM

Subjects

Animals, Cell Line, Chlorocebus aethiops, DNA-Binding Proteins antagonists & inhibitors, HL-60 Cells, Humans, Indicators and Reagents, Kinetics, Molecular Structure, Receptors, Retinoic Acid biosynthesis, Recombinant Proteins antagonists & inhibitors, Recombinant Proteins biosynthesis, Retinoid X Receptors, Retinoids chemistry, Structure-Activity Relationship, Transcription Factors biosynthesis, Transcriptional Activation, Transfection, Receptors, Retinoic Acid antagonists & inhibitors, Retinoids chemical synthesis, Retinoids pharmacology, Transcription Factors antagonists & inhibitors

Published

1996

19. Discovery of novel retinoic acid receptor agonists having potent antiproliferative activity in cervical cancer cells.

Author

Zhang L, Nadzan AM, Heyman RA, Love DL, Mais DE, Croston G, Lamph WW, and Boehm MF

Subjects

Cell Division drug effects, Drug Screening Assays, Antitumor, Female, Humans, Molecular Structure, Receptors, Retinoic Acid metabolism, Retinoid X Receptors, Retinoids chemistry, Thymidine metabolism, Transcription Factors metabolism, Tumor Cells, Cultured, Uterine Cervical Neoplasms, Antineoplastic Agents pharmacology, Receptors, Retinoic Acid agonists, Retinoids pharmacology

Abstract

Retinoic acid receptor (RAR) active retinoids have proven therapeutically useful for treating certain cancers and dermatological diseases. Herein, we describe the discovery of two new RAR active trienoic acid retinoids, (2E,4E,6E)-7-(3,5-di-tert-butylphenyl)-3-methylocta-2, 4,6-trienoic acid (10a, ALRT1550) and (2E,4E,6Z)-7-(3,5-di-tert-butylphenyl)-3-methylocta-2, 4,6-trienoic acid (10b, LG100567). ALRT1550 is a RAR selective retinoid which exhibits exceptional potency in both competitive binding and cotransfection assays. Moreover, it is the most potent antiproliferative retinoid described to date and thus has implications for the treatment of certain cancers. LG100567 is a potent panagonist which activates both RARs and retinoid X receptors.

Published

1996

20. Intracellular receptors and signal transducers and activators of transcription superfamilies: novel targets for small-molecule drug discovery.

Author

Rosen J, Day A, Jones TK, Jones ET, Nadzan AM, and Stein RB

Subjects

Base Sequence, DNA, Humans, Molecular Sequence Data, Structure-Activity Relationship, Transcription, Genetic, Gene Expression Regulation, Receptors, Cytoplasmic and Nuclear metabolism, Signal Transduction, Transcription Factors metabolism

Published

1995

21. Characterization of the novel CCK analogs JMV-180, JMV-320, and JMV-332 in H345 cells.

Author

Witte DG, Nadzan AM, Martinez J, Rodriguez M, and Lin CW

Subjects

Amino Acid Sequence, Cholecystokinin analysis, Molecular Sequence Data, Receptors, Cholecystokinin antagonists & inhibitors, Sincalide analogs & derivatives, Sincalide analysis, Tumor Cells, Cultured, Carcinoma, Small Cell chemistry, Cholecystokinin analogs & derivatives, Lung Neoplasms chemistry, Receptors, Cholecystokinin drug effects

Abstract

The interaction of the novel CCK analogs JMV-180, JMV-320, and JMV-332 with CCK-B/gastrin receptors on small cell lung cancer (SCLC) cells was investigated. JMV-180, JMV-320, and JMV-332 potently inhibited specific binding of 125I-CCK-8 to CCK-B/gastrin receptors expressed on the SCLC cell line NCI-H345 (H345) with IC50 values of 4.9, 1.8, and 7.0 nM, respectively. JMV-320 and JMV-332 stimulated intracellular calcium ([Ca2+]i) release in a dose-dependent manner in cells preloaded with indo-1. JMV-180 did not stimulate [Ca2+]i but inhibited the [Ca2+]i release elicited by 10 nM CCK-8 in a dose-dependent manner. These data indicate that JMV-320 and JMV-332 function as CCK-B/gastrin receptor agonists while JMV-180 functions as a CCK-B/gastrin receptor antagonist in H345 cells.

Published

1992

22. Intraventricular CCK-8 reduces single meal size in the baboon by interaction with type-A CCK receptors.

Author

Figlewicz DP, Nadzan AM, Sipols AJ, Green PK, Liddle RA, Porte D Jr, and Woods SC

Subjects

Animals, Blood Glucose analysis, Cholecystokinin blood, Fasting, Injections, Intraventricular, Insulin blood, Male, Oligopeptides pharmacology, Papio, Receptors, Cholecystokinin drug effects, Tetragastrin analogs & derivatives, Tetragastrin pharmacology, Eating drug effects, Receptors, Cholecystokinin physiology, Sincalide pharmacology

Abstract

Intraventricular cholecystokinin COOH-terminal octapeptide (CCK-8) decreases meal size in the meal-trained baboon. In the present study, we tested whether this action is mediated by CCK-A receptors, CCK-B receptors, or both. Intraventricular administration of the selective CCK-A receptor agonist A71623 at 1 and 10 nmol/kg suppressed 30-min meal size 69 +/- 22% and 75 +/- 7%, respectively. Additionally, intraventricular A71623 was equipotent to CCK-8 at 1 nmol/kg (% suppression of meal by CCK = 59 +/- 17). However, intraventricular administration of the CCK-B receptor agonist A63387 at 10 nmol/kg had no effect on 30-min meal size (% suppression = 18 +/- 29). Intravenous administration of 10 nmol/kg A71623 did not result in an alteration of meal size, but prandial plasma insulin and glucose responses were delayed and blunted. Basal plasma insulin levels doubled after intravenous administration of A71623. Both behavioral and metabolic responses to A71623 in the baboon are virtually identical to those we have previously observed after CCK-8 treatment. Thus we conclude that the predominant receptor population with which intraventricular CCK-8 interacts are type-A CCK receptors that are accessible to the ventricular system of the baboon.

Published

1992

23. A-71623, a selective CCK-A receptor agonist, suppresses food intake in the mouse, dog, and monkey.

Author

Asin KE, Bednarz L, Nikkel AL, Gore PA Jr, and Nadzan AM

Subjects

Animals, Cholecystokinin pharmacology, Depression, Chemical, Dogs, Macaca fascicularis, Male, Mice, Quinolines pharmacology, Receptors, Cholecystokinin drug effects, Species Specificity, Tetragastrin pharmacology, Eating drug effects, Receptors, Cholecystokinin physiology, Tetragastrin analogs & derivatives

Abstract

The anorectic actions of cholecystokinin (CCK)-8 and of a selective CCK-A agonist, A-71623, were examined in CD1 mice, beagle dogs, and cynomolgus monkeys. A-71623 suppressed intakes in all species tested, and the effects were blocked by a selective CCK-A antagonist, A-70104. In the dog only, CCK-8 was more potent on a molar basis compared to A-71623, although the effects of both CCK agonists were more short-lived in the dog compared to the other species tested. Our results support other evidence suggesting that the anorectic actions of exogenous application of CCK-8 in these species are mediated via stimulation of the CCK-A receptor subtype.

Published

1992

24. Behavioral effects of A71623, a highly selective CCK-A agonist tetrapeptide.

Author

Asin KE, Bednarz L, Nikkel AL, Gore PA Jr, Montana WE, Cullen MJ, Shiosaki K, Craig R, and Nadzan AM

Subjects

Animals, Anorexia chemically induced, Body Weight drug effects, Circadian Rhythm, Eating drug effects, Food Deprivation physiology, Male, Motor Activity drug effects, Peptides pharmacology, Rats, Rats, Inbred Strains, Sincalide pharmacology, Tetragastrin administration & dosage, Tetragastrin pharmacology, Time Factors, Behavior, Animal drug effects, Cholecystokinin physiology, Tetragastrin analogs & derivatives

Abstract

We studied the behavioral effects of a novel cholecystokinin tetrapeptide (CCK-4) analogue, A71623, with full agonist activity and high affinity and selectivity for the CCK-A receptor subtype relative to the CCK-B receptor. In tests for anorectic activity, A71623 was found to suppress 60-min intakes of a liquid diet in both deprived and sated rats, and the effects were blocked by a selective CCK-A antagonist, A70104. Compared with CCK-8, A71623 was found to have improved potency and duration of action; the most potent route of administration was intraperitoneal. A71623 also suppressed the intake of a liquid diet and a 0.2 M sucrose solution in lean and obese Zucker rats. In daily injection studies, the anorectic activity of CCK-8 diminished rapidly, whereas the suppressant effects of A71623 on food intakes and body weight gains persisted throughout the 11-day treatment period. Finally, A71623 reduced the spontaneous locomotor activity of rats at doses above those required to suppress intakes. These studies are the first to describe the behavioral effects of a potent and highly selective CCK-A receptor agonist.

Published

1992

25. Development of potent and selective CCK-A receptor agonists from Boc-CCK-4: tetrapeptides containing Lys(N epsilon)-amide residues.

Author

Shiosaki K, Lin CW, Kopecka H, Craig RA, Bianchi BR, Miller TR, Witte DG, Stashko M, and Nadzan AM

Subjects

Amino Acid Sequence, Amylases metabolism, Animals, Formic Acid Esters metabolism, Guinea Pigs, Molecular Sequence Data, Molecular Structure, Oligopeptides metabolism, Oligopeptides pharmacology, Pancreas drug effects, Pancreas metabolism, Sincalide chemistry, Sincalide metabolism, Sincalide pharmacology, Structure-Activity Relationship, Formic Acid Esters chemistry, Oligopeptides chemical synthesis, Receptors, Cholecystokinin metabolism

Abstract

A series of Boc-CCK-4 derivatives represented by the general structure Boc-Trp-Lys(N epsilon-COR)-Asp-Phe-NH2, where R is an aromatic, heterocyclic, or aliphatic group, are potent and selective CCK-A receptor agonists. These amide-bearing compounds complement the previously described urea-based tetrapeptides (Shiosaki et al. J. Med. Chem. 1991, 34, 2837-2842); structure-activity studies revealed parallel as well as divergent trends between these two series. A significant correlation was observed between pancreatic binding affinity and the resonance constant R of the phenyl substituent in one particular series of derivatives. Sulfation of phenolic amides appended onto the epsilon-amino group of the lysine did not affect affinity for the CCK-A receptor in contrast to the 500-fold increase in binding potency observed upon sulfation of CCK-8, suggesting that the lysine appendage and the sulfated tyrosine in CCK-8, both key structural elements that impart high affinity for the CCK-A receptor, are interacting differently with the receptor. The amide-bearing tetrapeptides are full agonists relative to CCK-8 in stimulating pancreatic amylase release while being partial agonists in eliciting phosphoinositide (PI) hydrolysis. Both effects were blocked by selective CCK-A receptor antagonists.

Published

1992

26. Effects of selective CCK receptor agonists on food intake after central or peripheral administration in rats.

Author

Asin KE, Gore PA Jr, Bednarz L, Holladay M, and Nadzan AM

Subjects

Analysis of Variance, Animals, Anorexia chemically induced, Dose-Response Relationship, Drug, Injections, Intraperitoneal, Injections, Intraventricular, Male, Oligopeptides pharmacology, Rats, Rats, Inbred Strains, Receptors, Cholecystokinin classification, Tetragastrin administration & dosage, Tetragastrin pharmacology, Time Factors, Brain physiology, Eating drug effects, Oligopeptides administration & dosage, Receptors, Cholecystokinin physiology, Tetragastrin analogs & derivatives

Abstract

In this paper report the effects of peripheral (intraperitoneal, i.p.) and central (intracerebroventricular, i.c.v.) injection of selective cholecystokinin (CCK) receptor agonists on food intake in the rat. Stimulation of peripheral and central CCK-A receptors by the selective CCK-A receptor agonist A-71623 suppressed intakes of a liquid diet in both deprived and sated rats. In contrast, i.c.v., but not i.p., injections of the selective CCK-B receptor agonist A-63387, reduced food intakes, although on a molar basis the effect was much less than that seen with A-71623. Although these results stress the relative importance of the CCK-A receptor in the effects of exogenous CCK-8 administration on feeding, stimulation of the CCK-B receptor may still be involved in the control of feeding following the endogenous release of CCK.

Published

1992

27. Cholecystokinin antagonists: (R)-tryptophan-based hybrid antagonists of high affinity and selectivity for CCK-A receptors.

Author

Kerwin JF Jr, Wagenaar F, Kopecka H, Lin CW, Miller T, Witte D, Stashko M, and Nadzan AM

Subjects

Animals, Benzamides pharmacology, Binding, Competitive, Glutamates chemical synthesis, Glutamates pharmacology, Guinea Pigs, In Vitro Techniques, Receptors, Cholecystokinin metabolism, Stereoisomerism, Structure-Activity Relationship, Tryptophan chemical synthesis, Tryptophan pharmacology, Benzamides chemical synthesis, Cholecystokinin antagonists & inhibitors, Receptors, Cholecystokinin drug effects, Tryptophan analogs & derivatives

Abstract

The intriguing structural similarities of glutamic acid based cholecystokinin (CCK) antagonists (A-64718 and A-65186) and the benzodiazepine CCK antagonist MK-329 (L-364,718) have been reported. Efforts to include the weak CCK antagonist benzotript into this construct utilizing a similar approach have resulted in a novel series of benzotript-based hybrid antagonists N alpha-(3'-quinolylcarbonyl)-(R)-tryptophan di-n-pentylamide (9, A-67396), N alpha-(4',8'-dihydroxy-2'-quinolylcarbonyl)-(R)-tryptophan di-n-pentylamide (23, A-70276), and N alpha-(3'-quinolylcarbonyl)-(R)-5'-hydroxytryptophan di-n-pentylamide (36, A-71134) which possess respectively binding affinities of 23, 21, and 11 nM for the pancreatic CCK-A receptor and which inhibit CCK8-induced amylase secretion. Compound 9 possesses a selectivity of greater than 500-fold for the pancreatic CCK-A receptor over the CCK-B receptor.

Published

1991

28. Boc-CCK-4 derivatives containing side-chain ureas as potent and selective CCK-a receptor agonists.

Author

Shiosaki K, Lin CW, Kopecka H, Tufano MD, Bianchi BR, Miller TR, Witte DG, and Nadzan AM

Subjects

Amino Acid Sequence, Amylases metabolism, Animals, Guinea Pigs, Hydrolysis, Molecular Sequence Data, Pancreas drug effects, Pancreas enzymology, Phosphatidylinositols metabolism, Tetragastrin chemistry, Tetragastrin pharmacology, Receptors, Cholecystokinin drug effects, Tetragastrin analogs & derivatives, Urea chemistry

Abstract

Novel Boc-CCK-4 derivatives were communicated recently as having high potency and selectivity for the CCK-A receptor (Shiosaki et al. J. Med. Chem. 1990, 33, 2950-2952). While Boc-CCK-4 binds selectively to the CCK-B receptor, replacement of the methionine with an N epsilon-substituted lysine dramatically reversed receptor selectivity, leading to the development of this novel series of tetrapeptides. A detailed structure-activity analysis of a series of urea-substituted tetrapeptides, represented by the general structure Boc-Trp-Lys(N epsilon-CO-NHR)-Asp-Phe-NH2, revealed that a number of substituted phenyl, naphthyl, and aliphatic urea residues in the lysine side chain yielded potent and selective CCK-A ligands. These tetrapeptides elicit full agonist responses in stimulating pancreatic amylase release that are effectively blocked by a selective CCK-A receptor antagonist. Conversion of the urea to a thiourea significantly reduced CCK-A binding potency as did replacement of the lysine with the homologous ornithine or homolysine. Tetrapeptides that were partial agonists (less than 80% efficacy) in phosphoinositide (PI) hydrolysis relative to CCK-8 did not exhibit high-dose inhibition of amylase secretion in guinea pig acini.

Published

1991

29. Characterization of two novel cholecystokinin tetrapeptide (30-33) analogues, A-71623 and A-70874, that exhibit high potency and selectivity for cholecystokinin-A receptors.

Author

Lin CW, Shiosaki K, Miller TR, Witte DG, Bianchi BR, Wolfram CA, Kopecka H, Craig R, Wagenaar F, and Nadzan AM

Subjects

Amylases metabolism, Animals, Cerebral Cortex metabolism, Cholecystokinin chemistry, Guinea Pigs, In Vitro Techniques, Oligopeptides chemistry, Oligopeptides metabolism, Pancreas metabolism, Phosphatidylinositols metabolism, Radioligand Assay, Secretory Rate drug effects, Structure-Activity Relationship, Tetragastrin metabolism, Cholecystokinin metabolism, Receptors, Cholecystokinin metabolism, Tetragastrin analogs & derivatives

Abstract

Based on their relative affinities for cholecystokinin octapeptide (26-33) (CCK-8), cholecystokinin tetrapeptide (30-33) (CCK-4), desulfated CCK-8, and gastrin, cholecystokinin (CCK) receptors have been classified as CCK-A (alimentary) and CCK-B (brain). Selective nonpeptide antagonists of CCK-A and CCK-B receptors, as well as highly selective CCK-A and CCK-B peptide agonists, have been described. We report here the characterization of two novel CCK-4-based peptides, A-71623 and A-70874. In radioligand binding assays, the IC50 values for A-71623 and A-70874 were 3.7 and 4.9 nM in guinea pig pancreas (CCK-A) and 4500 and 710 nM in cerebral cortex (CCK-B), respectively. Both were agonists in stimulating pancreatic amylase release, and their stimulatory effects were potently inhibited by the CCK-A antagonist L-364,718. A-71623 was a full agonist and A-70874 was a partial agonist (approximately 80%) in stimulating phosphoinositide breakdown in pancreas. Both peptides also were potent agonists in stimulating CCK-A receptors in the ileum. They were, however, weak and behaved as partial agonists in calcium studies in NCI-H345 cells, which possess CCK-B/gastrin receptors. In guinea pig gastric glands, the affinities of A-71623 and A-70874 for the CCK-B/gastrin receptor were 11 and 1.6 microM, respectively. These results demonstrate that A-71623 and A-70874 are potent and selective agonists at CCK-A receptors. The preferential interaction of these novel CCK-4 analogs with CCK-A receptors is in contrast to other CCK-4-based peptides, which are primarily selective for CCK-B receptors. In addition, A-71623 and A-70874 are the first two examples of potent CCK-A agonists that do not contain a tyrosine residue whose sulfation is required for potent CCK-A agonist activity of larger peptides.

Published

1991

30. trans-3-n-propyl-L-proline is a highly favorable, conformationally restricted replacement for methionine in the C-terminal tetrapeptide of cholecystokinin. Stereoselective synthesis of 3-allyl- and 3-n-propyl-L-proline derivatives from 4-hydroxy-L-proline.

Author

Holladay MW, Lin CW, May CS, Garvey DS, Witte DG, Miller TR, Wolfram CA, and Nadzan AM

Subjects

Animals, Cerebral Cortex metabolism, Guinea Pigs, Hydroxyproline, Indicators and Reagents, Molecular Structure, Pancreas metabolism, Proline chemical synthesis, Structure-Activity Relationship, Tetragastrin metabolism, Tetragastrin pharmacology, Methionine, Proline analogs & derivatives, Receptors, Cholecystokinin metabolism, Tetragastrin analogs & derivatives, Tetragastrin chemical synthesis

Published

1991

31. Development of CCK-tetrapeptide analogues as potent and selective CCK-A receptor agonists.

Author

Shiosaki K, Lin CW, Kopecka H, Craig R, Wagenaar FL, Bianchi B, Miller T, Witte D, and Nadzan AM

Subjects

Amino Acid Sequence, Amylases metabolism, Animals, Cerebral Cortex metabolism, Cholecystokinin chemical synthesis, Cholecystokinin metabolism, Cholecystokinin pharmacology, Guinea Pigs, Molecular Sequence Data, Molecular Structure, Oligopeptides chemical synthesis, Oligopeptides metabolism, Oligopeptides pharmacology, Pancreas drug effects, Pancreas metabolism, Peptide Fragments chemical synthesis, Peptide Fragments pharmacology, Receptors, Cholecystokinin drug effects, Structure-Activity Relationship, Cholecystokinin analogs & derivatives, Peptide Fragments metabolism, Receptors, Cholecystokinin metabolism, Tetragastrin analogs & derivatives

Published

1990

32. A71378: a CCK agonist with high potency and selectivity for CCK-A receptors.

Author

Lin CW, Holladay MW, Witte DG, Miller TR, Wolfram CA, Bianchi BR, Bennett MJ, and Nadzan AM

Subjects

Amino Acid Sequence, Animals, Binding, Competitive, Calcium metabolism, Guinea Pigs, Kinetics, Molecular Sequence Data, Muscle, Smooth metabolism, Oligopeptides metabolism, Organ Specificity, Pancreas metabolism, Receptors, Cholecystokinin drug effects, Sincalide analogs & derivatives, Sincalide metabolism, Sincalide pharmacology, Gastric Mucosa metabolism, Ileum metabolism, Oligopeptides pharmacology, Receptors, Cholecystokinin metabolism

Abstract

Receptors for the brain and gut peptide cholecystokinin (CCK) have been classified into two classes, CCK-A and CCK-B. To date, peptide analogues with selectivity for the CCK-B receptors have been identified, and selective antagonists for CCK-A and CCK-B receptors have been reported as well; until now, there have been no reports of highly selective CCK-A agonists. Herein we describe the properties of A71378 [desamino-Try(SO3H)-Nle-Gly-Trp-Nle-(N-methyl)Asp-Phe-NH2], a highly selective CCK-A receptor ligand. Characterization of A71378 was carried out in the guinea pig pancreas, cortex, gastric gland, and ileum, as well as in NCI-H345 cells. The IC50 values of A71378 for the pancreatic CCK-A, cortical CCK-B, and gastrin receptor were 0.4 nM, 300 nM, and 1,200 nM, respectively. A71378 proved to be a potent agonist in eliciting pancreatic amylase secretion (EC50 = 0.16 nM) and ileal muscle contraction (EC50 = 3.7 nM). In contrast, A71378 was relatively weak (EC50 = 600 nM) in mobilizing intracellular calcium from NCI-H345 cells, which express CCK-B/gastrin receptors. The high potency and selectivity of A71378 for the CCK-A over CCK-B and gastrin receptors is unprecedented among CCK peptides. Studies on CCK-7 analogues indicate that N-methylation of the Asp residue is responsible for the observed selectivity for CCK-A receptors. This discovery of a selective CCK-A agonist should prove valuable for studies aimed at understanding the physiological roles of CCK-A receptors in the brain and periphery.

Published

1990

33. Hydroxynybomycin: isolation, structure and bioactivity.

Author

Nadzan AM, Rinehart KL Jr, and Sokolski WT

Subjects

Anti-Bacterial Agents pharmacology, Bacteria drug effects, Chemical Phenomena, Chemistry, Magnetic Resonance Spectroscopy, Mass Spectrometry, Spectrophotometry, Infrared, Anti-Bacterial Agents isolation & purification

Published

1977

34. Evidence that type A CCK receptors facilitate dopamine efflux in rat brain.

Author

Vickroy TW, Bianchi BR, Kerwin JF Jr, Kopecka H, and Nadzan AM

Subjects

Animals, Brain drug effects, In Vitro Techniques, Male, Nucleus Accumbens drug effects, Nucleus Accumbens metabolism, Rats, Rats, Inbred Strains, Brain metabolism, Cholecystokinin pharmacology, Dopamine metabolism, Receptors, Cholecystokinin metabolism

Published

1988

35. Thyrotropin releasing hormone augments growth of spinal cord transplants in oculo.

Author

Henschen A, Zerbe G, Nadzan AM, McKelvy JF, Olson L, and Hoffer B

Subjects

Amino Acids pharmacology, Animals, Female, Fetus physiology, Rats, Rats, Inbred Strains, Spinal Cord embryology, Spinal Cord growth & development, Time Factors, Ocular Physiological Phenomena, Spinal Cord transplantation, Thyrotropin-Releasing Hormone pharmacology

Abstract

The effects of thyrotropin releasing hormone (TRH) on spinal cord growth were evaluated using the in oculo transplant model. The growth of fetal spinal cord allografts, placed into the anterior eye chamber of Sprague-Dawley rats, was markedly augmented by acute exposure of the graft and host animal to TRH at the time of transplantation. No significant growth augmentation was seen after equimolar administration of a mixture of the amino acids that comprise the TRH molecule. It is concluded that acutely administered TRH, at the time of grafting, elicits a significant stimulation of the growth of spinal cord tissue. Our data strengthen the rationale for continued clinical trials of this peptide in spinal cord injury.

Published

1988

36. Nybomycin. 9. Synthetic and biosynthetic incorporation of 15N as a means of assigning the 13C nuclear magnetic resonance spectrum of nybomycin 1,2.

Author

Nadzan AM and Rinehart KL Jr

Subjects

Butyrates, Carbon Isotopes, Isotope Labeling, Magnetic Resonance Spectroscopy, Nitrogen Isotopes, Pyridines biosynthesis, Pyridines chemical synthesis, Quinolones, Anti-Bacterial Agents biosynthesis, Anti-Bacterial Agents chemical synthesis, Quinolines biosynthesis, Quinolines chemical synthesis

Published

1977

37. Hybrid cholecystokinin (CCK) antagonists: new implications in the design and modification of CCK antagonists.

Author

Kerwin JF Jr, Nadzan AM, Kopecka H, Lin CW, Miller T, Witte D, and Burt S

Subjects

Benzodiazepines chemical synthesis, Benzodiazepinones chemical synthesis, Benzodiazepinones pharmacology, Chemical Phenomena, Chemistry, Devazepide, Drug Design, Molecular Conformation, Receptors, Cholecystokinin drug effects, Stereoisomerism, Structure-Activity Relationship, Benzodiazepines pharmacology, Cholecystokinin antagonists & inhibitors, Glutamine analogs & derivatives, Proglumide analogs & derivatives, Proglumide chemical synthesis, Proglumide pharmacology

Published

1989

38. Distinct requirements for activation at CCK-A and CCK-B/gastrin receptors: studies with a C-terminal hydrazide analogue of cholecystokinin tetrapeptide (30-33).

Author

Lin CW, Holladay MW, Barrett RW, Wolfram CA, Miller TR, Witte D, Kerwin JF Jr, Wagenaar F, and Nadzan AM

Subjects

Amino Acid Sequence, Animals, Benzodiazepinones pharmacology, Calcium metabolism, Devazepide, Gastrins, Guinea Pigs, Molecular Sequence Data, Proglumide analogs & derivatives, Proglumide pharmacology, Tetragastrin pharmacology, Cholecystokinin antagonists & inhibitors, Peptide Fragments pharmacology, Receptors, Cholecystokinin drug effects, Tetragastrin analogs & derivatives

Abstract

We describe here the properties of tert-butyloxycarbonyl-Trp-Leu-Asp-Phe-NHNH2 (A-57696), a C-terminal hydrazide analogue of tert-butyloxycarbonyl-CCK4 (Boc-Trp-Met-Asp-Phe-NH2), at four cholecystokinin (CCK) receptor-bearing tissues, the guinea pig pancreas and gall bladder (Type A), guinea pig cortex (Type B), and NCI-H345 cells, a human small cell lung cancer cell line that expresses CCK-B/gastrin receptors. Using 125I-Bolton-Hunter-cholecystokinin octapeptide (26-33) (125I-Bolton-Hunter-CCK8) as the radioligand, A-57696 was found to be selective for cortical CCK-B receptors (IC50 = 25 nM), compared with pancreatic CCK-A receptors (IC50 = 15 microM). A-57696 behaved as a competitive antagonist in reversing CCK8-stimulated pancreatic amylase secretion and phosphoinositide breakdown. By Schild analysis, its Kd was determined to be 4.7 and 6.8 microM in amylase and phosphoinositide assays, respectively. A-57696 (100 microM) did not elicit gall bladder contraction, and it inhibited contractions induced by CCK8. The Kd of A-57696 at gall bladder CCK-A receptors was 19 microM. In contrast, A-57696 behaved as a partial agonist (80% of maximal CCK8 response) in stimulating calcium mobilization at CCK-B/gastrin receptors on NCI-H345 cells. A-57696 and CCK8 inhibited each other in calcium mobilization experiments utilizing the fluorescent dye Indo-1. Stimulatory actions of CCK8 and A-57696 were reversed by the CCK-B-selective (R)-L-365,260 (100 nM), whereas at the same concentration, the CCK-A-selective (S)-L-365,260 was ineffective. Binding studies using 125I-Bolton-Hunter-CCK8 and 125I-gastrin indicated that binding sites labeled by these two ligands displayed similar affinities for CCK8, desulfated CCK8, gastrin, A-57696, and both enantiomers of L-365,260. A-57696 represents a new class of CCK-A peptide antagonist at guinea pig pancreas a new class of CCK-A peptide antagonist at guinea pig pancreas and gall bladder. Its contrasting functional activities at guinea pig CCK-A and CCK-B/gastrin receptors in a human tumor cell demonstrate that, in addition to the previously described differences in binding specificity for selective agonists and antagonists, CCK-A receptors and CCK-B/gastrin receptors have different requirements for activation.

Published

1989

39. Structural identification of the major DNA adduct formed by aflatoxin B1 in vitro.

Author

Essigmann JM, Croy RG, Nadzan AM, Busby WF Jr, Reinhold VN, Büchi G, and Wogan GN

Subjects

Animals, Chromatography, High Pressure Liquid, Guanine metabolism, Magnetic Resonance Spectroscopy, Male, Rats, Spectrophotometry, Ultraviolet, Aflatoxins metabolism, DNA metabolism, Microsomes, Liver metabolism

Abstract

The covalent binding of the hepatocarcinogen aflatoxin B1 by rat liver microsomes to calf thymus DNA resulted in a binding level equal to one aflatoxin residue per 60 DNA nucleotides. An aflatoxin derivative-guanine adduct was efficiently liberated from DNA with formic acid. Analytical reversed-phase high-pressure liquid chromatography of the DNA hydrolysate revealed that approximately 90% of the carcinogen bound to DNA could be accounted for as a single component. Preparative high-pressure liquid chromatography was used to isolate sufficient quantities of the adduct for structural analysis from large quantities (340 mg) of DNA. A combination of spectral and chemical data indicates that the major product of the interaction of metabolically activated aflatoxin B1 and DNA is 2,3-dihydro-2-(N7-guanyl)-3-hydroxyaflatoxin B1 with the guanine and hydroxyl functions possessing a trans configuration. The structural data support the hypothesis that the putative 2,3-oxide of aflatoxin B1 is quantitatively important as an intermediate in the binding of aflatoxin B1 to nucleic acids.

Published

1977

40. Cholecystokinin receptors: relationships among phosphoinositide breakdown, amylase release and receptor affinity in pancreas.

Author

Lin CW, Bianchi BR, Grant D, Miller T, Danaher EA, Tufano MD, Kopecka H, and Nadzan AM

Subjects

Animals, Cholecystokinin pharmacology, Dose-Response Relationship, Drug, Guinea Pigs, In Vitro Techniques, Male, Pancreas metabolism, Peptide Fragments pharmacology, Receptors, Cell Surface metabolism, Receptors, Cholecystokinin, Amylases metabolism, Pancreas drug effects, Phosphatidylinositols metabolism, Receptors, Cell Surface drug effects

Abstract

The gut hormone cholecystokinin (CCK) octapeptide stimulates the release of amylase from exocrine pancreas, a process believed to be the result of the breakdown of phosphatidylinositol lipids. To examine further the relationship between phosphoinositide (PI) breakdown and amylase release, we have investigated the effect of N-terminally protected CCK C-terminal fragments in these systems using guinea-pig pancreatic lobules. There was a good correlation between the ability of these fragments to elicit amylase release and their potency in enhancing PI breakdown. In general, the EC50 for amylase release is 10-fold lower than the EC50 for PI breakdown. In addition, a good correlation existed between amylase release and the affinity of CCK fragments for [125I]Bolton Hunter-CCK octapeptide binding sites in pancreatic membranes. We also discovered that N-carbobenzyloxy-CCK tetrapeptide was relatively inefficient in causing PI breakdown, but it caused a near maximal stimulation in amylase release. These findings might reflect an amplification mechanism between PI breakdown and amylase release or that N-carbobenzyloxy-CCK tetrapeptide-induced amylase release is independent of PI breakdown.

Published

1986

41. Centrally administered CCK-8 suppresses activity in mice by a "peripheral-type" CCK receptor.

Author

Britton DR, Yahiro L, Cullen MJ, Kerwin JF Jr, Kopecka H, and Nadzan AM

Subjects

Animals, Dose-Response Relationship, Drug, Drug Interactions, Injections, Intraperitoneal, Injections, Intraventricular, Male, Mice, Quinolines pharmacology, Sincalide administration & dosage, Sincalide analogs & derivatives, Tetragastrin analogs & derivatives, Tetragastrin pharmacology, Motor Activity drug effects, Receptors, Cholecystokinin drug effects, Sincalide pharmacology

Abstract

Cholecystokinin octapeptide (CCK-8) administered either systemically (IP) or centrally (ICV) suppresses several types of behavior in mice including exploratory locomotion, rearing and grooming. At doses equimolar to those active for CCK-8, neither desulfated CCK-8 (CCK-8-DS), nor the protected C-terminus tetrapeptide fragment, BOC-CCK-4, is behaviorally active when administered either centrally or systemically. A potent and selective antagonist to the peripheral type (Type A) CCK receptor, A-65186, when given systemically, blocked the effects of systemically administered CCK-8, but failed to block the effects of ICV administered CCK-8. Central administration of A-65186 blocked the effects of ICV administered CCK-8. These results demonstrate that administration of exogenous CCK-8 to mice can suppress exploratory locomotion by acting either centrally or peripherally and that in either case the demonstrated behavioral effects are mediated via a "peripheral" type (Type A) CCK receptor.

Published

1989

42. Letter: Nybomycin. 8. Biosynthetic origin of the central ring carbons studied by 13C-labeled substrates.

Author

Nadzan AM and Rinehart KL Jr

Subjects

Carbon Isotopes, Chemical Phenomena, Chemistry, Isotope Labeling, Pyridines biosynthesis, Quinolines biosynthesis, Quinolones, Anti-Bacterial Agents biosynthesis

Published

1976