Your search keyword '"Blumberg PM"' showing total 22 results

1. 4-Aminophenyl acetamides and propanamides as potent transient receptor potential vanilloid 1 (TRPV1) ligands.

Author

Kim C, Ann J, Lee S, Kim E, Choi S, Blumberg PM, Frank-Foltyn R, Bahrenberg G, Stockhausen H, Christoph T, and Lee J

Subjects

Acetamides chemistry, Acetamides pharmacology, Acetamides therapeutic use, Amides pharmacology, Amides therapeutic use, Binding Sites, Capsaicin chemistry, Capsaicin toxicity, Humans, Hydrogen-Ion Concentration, Hypothermia pathology, Hypothermia prevention & control, Ligands, Molecular Docking Simulation, Protein Structure, Tertiary, Structure-Activity Relationship, TRPV Cation Channels metabolism, Amides chemistry, TRPV Cation Channels antagonists & inhibitors

Abstract

A series of 2-(3,5-substituted 4-aminophenyl)acetamide and propanamide derivatives were investigated as human TRPV1 antagonists. The analysis of the structure-activity relationship indicated that 2-(3,5-dihalo 4-aminophenyl)acetamide analogues displayed excellent antagonism of hTRPV1 activation by capsaicin and showed improved potency compared to the corresponding propanamides. The most potent antagonist (36) exhibited potent and selective antagonism for hTRPV1 not only to capsaicin but also to NADA and elevated temperature; however, it only displayed weak antagonism to low pH. Further studies indicated that oral administration of antagonist 36 blocked the hypothermic effect of capsaicin in vivo but demonstrated hyperthermia at that dose. A docking study of 36 was performed in our established hTRPV1 homology model to understand its binding interactions with the receptor and to compare with that of previous antagonist 1., (Copyright © 2018 Elsevier Ltd. All rights reserved.)

Published

2018

2. Exploring the influence of indololactone structure on selectivity for binding to the C1 domains of PKCα, PKCε, and RasGRP.

Author

Elhalem E, Donadío LG, Zhou X, Lewin NE, Garcia LC, Lai CC, Kelley JA, Peach ML, Blumberg PM, and Comin MJ

Subjects

DNA-Binding Proteins chemistry, Guanine Nucleotide Exchange Factors chemistry, Humans, Molecular Docking Simulation, Protein Binding, Protein Domains, Protein Kinase C-alpha chemistry, Protein Kinase C-epsilon chemistry, Structure-Activity Relationship, DNA-Binding Proteins metabolism, Guanine Nucleotide Exchange Factors metabolism, Indoles chemistry, Indoles pharmacology, Lactones chemistry, Lactones pharmacology, Protein Kinase C-alpha metabolism, Protein Kinase C-epsilon metabolism

Abstract

C1 domain-containing proteins, such as protein kinase C (PKC), have a central role in cellular signal transduction. Their involvement in many diseases, including cancer, cardiovascular disease, and immunological and neurological disorders has been extensively demonstrated and has prompted a search for small molecules to modulate their activity. By employing a diacylglycerol (DAG)-lactone template, we have been able to develop ultra potent analogs of diacylglycerol with nanomolar binding affinities approaching those of complex natural products such as phorbol esters and bryostatins. One current challenge is the development of selective ligands capable of discriminating between different protein family members. Recently, structure-activity relationship studies have shown that the introduction of an indole ring as a DAG-lactone substituent yielded selective Ras guanine nucleotide-releasing protein (RasGRP1) activators when compared to PKCα and PKCε. In the present work, we examine the effects of ligand selectivity relative to the orientation of the indole ring and the nature of the DAG-lactone template itself. Our results show that the indole ring must be attached to the lactone moiety through the sn-2 position in order to achieve RasGRP1 selectivity., (Copyright © 2017 Elsevier Ltd. All rights reserved.)

Published

2017

3. t-Butyl pyridine and phenyl C-region analogues of 2-(3-fluoro-4-methylsulfonylaminophenyl)propanamides as potent TRPV1 antagonists.

Author

Lee S, Kang DW, Ryu H, Kim C, Ann J, Lee H, Kim E, Hong S, Choi S, Blumberg PM, Frank-Foltyn R, Bahrenberg G, Stockhausen H, Christoph T, and Lee J

Subjects

Amides chemistry, Animals, Humans, Molecular Docking Simulation, Structure-Activity Relationship, Amides pharmacology, Pyridines chemistry, TRPV Cation Channels antagonists & inhibitors

Abstract

A series of 2-substituted 6-t-butylpyridine and 4-t-butylphenyl C-region analogues of 2-(3-fluoro-4-methylsulfonamidophenyl)propanamides were investigated for hTRPV1 antagonism. The analysis of structure activity relationships indicated that the pyridine derivatives generally exhibited a little better antagonism than did the corresponding phenyl surrogates for most of the series. Among the compounds, compound 7 showed excellent antagonism toward capsaicin activation with K i =0.1nM and compound 60S demonstrated a strong antiallodynic effect with 83% MPE at 10mg/kg in the neuropathic pain model. The docking study of 7S in our hTRPV1 homology model indicated that the interactions between the A/B-regions of 7S with Tyr511 and the interactions between the t-butyl and ethyl groups in the C-region of 7S with the two hydrophobic binding pockets of hTRPV1 contributed to the high potency., (Copyright © 2017 Elsevier Ltd. All rights reserved.)

Published

2017

4. 2-Sulfonamidopyridine C-region analogs of 2-(3-fluoro-4-methylsulfonamidophenyl)propanamides as potent TRPV1 antagonists.

Author

Ann J, Ki Y, Yoon S, Kim MS, Lee JU, Kim C, Lee S, Jung A, Baek J, Hong S, Choi S, Pearce LV, Esch TE, Turcios NA, Lewin NE, Ogunjirin AE, Herold BK, McCall AK, Blumberg PM, and Lee J

Subjects

Dose-Response Relationship, Drug, Humans, Models, Molecular, Molecular Structure, Pyridines chemistry, Structure-Activity Relationship, Sulfonamides chemistry, Pyridines pharmacology, Sulfonamides pharmacology, TRPV Cation Channels antagonists & inhibitors

Abstract

A series of 2-sulfonamidopyridine C-region derivatives of 2-(3-fluoro-4-methylsulfonamidophenyl)propanamide were investigated as hTRPV1 ligands. Systematic modification on the 2-sulfonamido group provided highly potent TRPV1 antagonists. The N-benzyl phenylsulfonamide derivatives 12 and 23 in particular showed higher affinities than that of lead compound 1. Compound 12 exhibited strong analgesic activity in the formalin pain model. Docking analysis of its chiral S-form 12S in our hTRPV1 homology model indicated that its high affinity might arise from additional hydrophobic interactions not present in lead compound 1S., (Copyright © 2016 Elsevier Ltd. All rights reserved.)

Published

2016

5. Structure activity relationships of benzyl C-region analogs of 2-(3-fluoro-4-methylsulfonamidophenyl)propanamides as potent TRPV1 antagonists.

Author

Ann J, Jung A, Kim MY, Kim HM, Ryu H, Kim S, Kang DW, Hong S, Cui M, Choi S, Blumberg PM, Frank-Foltyn R, Bahrenberg G, Stockhausen H, Christoph T, and Lee J

Subjects

Amides chemical synthesis, Amides therapeutic use, Analgesics chemical synthesis, Animals, Binding Sites, Capsaicin toxicity, Humans, Hypothermia chemically induced, Hypothermia drug therapy, Mice, Molecular Conformation, Molecular Docking Simulation, Structure-Activity Relationship, TRPV Cation Channels metabolism, Amides chemistry, Analgesics chemistry, TRPV Cation Channels antagonists & inhibitors

Abstract

A series of 2-substituted 4-(trifluoromethyl)benzyl C-region analogs of 2-(3-fluoro-4-methylsulfonamidophenyl)propanamides were investigated for hTRPV1 antagonism. The analysis indicated that the phenyl C-region derivatives exhibited better antagonism than those of the corresponding pyridine surrogates for most of the series examined. Among the phenyl C-region derivatives, the two best compounds 43 and 44S antagonized capsaicin selectively relative to their antagonism of other activators and showed excellent potencies with K(i(CAP))=0.3 nM. These two compounds blocked capsaicin-induced hypothermia, consistent with TRPV1 as their site of action, and they demonstrated promising analgesic activities in a neuropathic pain model without hyperthermia. The docking study of 44S in our hTRPV1 homology model indicated that its binding mode was similar with that of its pyridine surrogate in the A- and B-regions but displayed a flipped configuration in the C-region., (Copyright © 2015 Elsevier Ltd. All rights reserved.)

Published

2015

6. Synthesis, biological, and biophysical studies of DAG-indololactones designed as selective activators of RasGRP.

Author

Garcia LC, Donadío LG, Mann E, Kolusheva S, Kedei N, Lewin NE, Hill CS, Kelsey JS, Yang J, Esch TE, Santos M, Peach ML, Kelley JA, Blumberg PM, Jelinek R, Marquez VE, and Comin MJ

Subjects

Animals, CHO Cells, Cell Membrane metabolism, Cells, Cultured, Cricetulus, Diglycerides chemistry, Fluorescence Polarization, Fluorescence Resonance Energy Transfer, HEK293 Cells, Humans, Indoles chemistry, Lactones chemistry, Male, Models, Molecular, Prostatic Neoplasms drug therapy, Prostatic Neoplasms metabolism, Protein Isoforms, DNA-Binding Proteins metabolism, Diglycerides pharmacology, Guanine Nucleotide Exchange Factors metabolism, Indoles pharmacology, Lactones pharmacology, Prostatic Neoplasms pathology, Protein Kinase C metabolism

Abstract

The development of selective agents capable of discriminating between protein kinase C (PKC) isoforms and other diacylglycerol (DAG)-responsive C1 domain-containing proteins represents an important challenge. Recent studies have highlighted the role that Ras guanine nucleotide-releasing protein (RasGRP) isoforms play both in immune responses as well as in the development of prostate cancer and melanoma, suggesting that the discovery of selective ligands could have potential therapeutic value. Thus far, the N-methyl-substituted indololactone 1 is the agonist with the highest reported potency and selectivity for RasGRP relative to PKC. Here we present the synthesis, binding studies, cellular assays and biophysical analysis of interactions with model membranes of a family of regioisomers of 1 (compounds 2-5) that differ in the position of the linkage between the indole ring and the lactone moiety. These structural variations were studied to explore the interaction of the active complex (C1 domain-ligand) with cellular membranes, which is believed to be an important factor for selectivity in the activation of DAG-responsive C1 domain containing signaling proteins. All compounds were potent and selective activators of RasGRP when compared to PKCα with selectivities ranging from 6 to 65 fold. However, the parent compound 1 was appreciably more selective than any of the other isomers. In intact cells, modest differences in the patterns of translocation of the C1 domain targets were observed. Biophysical studies using giant vesicles as model membranes did show substantial differences in terms of molecular interactions impacting lipid organization, dynamics and membrane insertion. However, these differences did not yield correspondingly large changes in patterns of biological response, at least for the parameters examined., (Copyright © 2014 Elsevier Ltd. All rights reserved.)

Published

2014

7. TRPV1 antagonist with high analgesic efficacy: 2-Thio pyridine C-region analogues of 2-(3-fluoro-4-methylsulfonylaminophenyl)propanamides.

Author

Ha TH, Ryu H, Kim SE, Kim HS, Ann J, Tran PT, Hoang VH, Son K, Cui M, Choi S, Blumberg PM, Frank R, Bahrenberg G, Schiene K, Christoph T, Frormann S, and Lee J

Subjects

Amides metabolism, Amides therapeutic use, Analgesics metabolism, Analgesics therapeutic use, Animals, Benzeneacetamides metabolism, Benzeneacetamides therapeutic use, Binding Sites, Disease Models, Animal, Humans, Mice, Molecular Docking Simulation, Neuralgia drug therapy, Protein Binding, Protein Structure, Tertiary, Rats, Structure-Activity Relationship, Sulfonamides metabolism, Sulfonamides therapeutic use, TRPV Cation Channels metabolism, Amides chemistry, Analgesics chemistry, Benzeneacetamides chemistry, Pyridines chemistry, Sulfonamides chemistry, TRPV Cation Channels antagonists & inhibitors

Abstract

A series of 2-thio pyridine C-region analogues of 2-(3-fluoro-4-methylsulfonylaminophenyl)propanamides were investigated as hTRPV1 antagonists. Among them, compound 24S showed stereospecific and excellent TRPV1 antagonism of capsaicin-induced activation. Further, it demonstrated strong anti-allodynic in a rat neuropathic pain model. Consistent with its action in vitro being through TRPV1, compound 24S blocked capsaicin-induced hypothermia in mice. Docking analysis of 24S with our hTRPV1 homology model was performed to identify its binding mode., (Copyright © 2013 Elsevier Ltd. All rights reserved.)

Published

2013

8. 2-(4-Methylsulfonylaminophenyl) propanamide TRPV1 antagonists: Structure-activity relationships in the B and C-regions.

Author

Sun W, Liu K, Ryu H, Kang DW, Kim YS, Kim MS, Cho Y, Bhondwe RS, Thorat SA, Kim HS, Pearce LV, Pavlyukovets VA, Tran R, Morgan MA, Lazar J, Ryder CB, Toth A, Blumberg PM, and Lee J

Subjects

Animals, CHO Cells, Cricetinae, Humans, Rats, Structure-Activity Relationship, TRPV Cation Channels metabolism, Analgesics chemistry, Analgesics pharmacology, Mesylates chemistry, Mesylates pharmacology, Phenylpropionates chemistry, Phenylpropionates pharmacology, TRPV Cation Channels antagonists & inhibitors

Abstract

On the basis of the previous lead N-4-t-butylbenzyl 2-(3-fluoro-4-methylsulfonylaminophenyl) propanamide (3) as a potent TRPV1 antagonist, structure-activity relationships for the B (propanamide part) and C-region (4-t-butylbenzyl part) have been investigated for rTRPV1 in CHO cells. The B-region was modified with dimethyl, cyclopropyl and reverse amides and then the C-region was replaced with 4-substituted phenyl, aryl alkyl and diaryl alkyl derivatives. Among them, compound 50 showed high binding affinity with K(i)=21.5nM, which was twofold more potent than 3 and compound 54 exhibited potent antagonism with K(i(ant))=8.0nM comparable to 3., (Copyright © 2011 Elsevier Ltd. All rights reserved.)

Published

2012

9. N-4-t-Butylbenzyl 2-(4-methylsulfonylaminophenyl) propanamide TRPV1 antagonists: Structure-activity relationships in the A-region.

Author

Kim YS, Kil MJ, Kang SU, Ryu H, Kim MS, Cho Y, Bhondwe RS, Thorat SA, Sun W, Liu K, Lee JH, Choi S, Pearce LV, Pavlyukovets VA, Morgan MA, Tran R, Lazar J, Blumberg PM, and Lee J

Subjects

Amides chemical synthesis, Animals, Binding Sites, CHO Cells, Computer Simulation, Cricetinae, Cricetulus, Humans, Hydrogen Bonding, Protein Binding drug effects, Protein Structure, Tertiary, Rats, Stereoisomerism, Structure-Activity Relationship, TRPV Cation Channels metabolism, Amides chemistry, Amides pharmacology, TRPV Cation Channels antagonists & inhibitors

Abstract

Structure-activity relationships for the A-region in a series of N-4-t-butylbenzyl 2-(4-methylsulfonylaminophenyl) propanamides as TRPV1 antagonists have been investigated. Among them, the 3-fluoro analogue 54 showed high binding affinity and potent antagonism for both rTRPV1 and hTRPV1 in CHO cells. Its stereospecific activity was demonstrated with marked selectivity for the (S)-configuration (54S versus 54R). A docking study of 54S with our hTRPV1 homology model highlighted crucial hydrogen bonds between the ligand and the receptor contributing to its potency., (Copyright © 2011 Elsevier Ltd. All rights reserved.)

Published

2012

10. Halogenation of 4-hydroxy/amino-3-methoxyphenyl acetamide TRPV1 agonists showed enhanced antagonism to capsaicin.

Author

Kang DW, Kim YS, Lim KS, Kim MS, Pearce LV, Pavlyukovets VA, Tao AK, Lang-Kuhs KA, Blumberg PM, and Lee J

Subjects

Acetamides chemical synthesis, Acetamides pharmacology, Animals, Benzamides chemical synthesis, Benzamides pharmacology, CHO Cells, Cricetinae, Cricetulus, Halogenation, Rats, Structure-Activity Relationship, TRPV Cation Channels antagonists & inhibitors, TRPV Cation Channels metabolism, Thiourea analogs & derivatives, Thiourea chemical synthesis, Thiourea pharmacology, Acetamides chemistry, Benzamides chemistry, Capsaicin pharmacology, TRPV Cation Channels agonists

Abstract

As an extension of our analysis of the effect of halogenation on thiourea TRPV1 agonists, we have now modified selected 4-hydroxy(or 4-amino)-3-methoxyphenyl acetamide TRPV1 agonists by 5- or 6-halogenation on the aromatic A-region and evaluated them for potency for TRPV1 binding and regulation and for their pattern of agonism/antagonism (efficacy). Halogenation shifted the functional activity at TRPV1 toward antagonism with a greater extent of antagonism as the size of the halogen increased (I>Br>Cl), as previously observed for the thiourea series. The extent of antagonism was greater for halogenation at the 5-position than at the 6-position, in contrast to SAR for the thiourea series. In this series, compounds 55 and 75 showed the most potent antagonism, with K(i) (ant)=2.77 and 2.19nM, respectively, on rTRPV1 expressed in Chinese hamster ovary cells. The compounds were thus ca. 40-60-fold more potent than 6'-iodononivamide., (Copyright © 2010 Elsevier Ltd. All rights reserved.)

Published

2010

11. Non-vanillyl resiniferatoxin analogues as potent and metabolically stable transient receptor potential vanilloid 1 agonists.

Author

Choi HK, Choi S, Lee Y, Kang DW, Ryu H, Maeng HJ, Chung SJ, Pavlyukovets VA, Pearce LV, Toth A, Tran R, Wang Y, Morgan MA, Blumberg PM, and Lee J

Subjects

Animals, CHO Cells, Calcium metabolism, Cricetinae, Cricetulus, Diterpenes blood, Diterpenes chemistry, Diterpenes pharmacokinetics, Microsomes, Liver metabolism, Models, Molecular, Rats, Structure-Activity Relationship, Diterpenes pharmacology, TRPV Cation Channels agonists

Abstract

A series of non-vanillyl resiniferatoxin analogues, having 4-methylsulfonylaminophenyl and fluorophenyl moieties as vanillyl surrogates, have been investigated as ligands for rat TRPV1 heterologously expressed in Chinese hamster ovary cells. Although lacking the metabolically problematic 4-hydroxy substituent on the A-region phenyl ring, the compounds retained substantial agonist potency. Indeed, the 3-methoxy-4-methylsulfonylaminophenyl analog (1) was modestly (2.5-fold) more potent than RTX, with an EC(50)=0.106 nM. Further, it resembled RTX in its kinetics and pattern of stimulation of the levels of intracellular calcium in individual cells, as revealed by imaging. Compound 1 displayed modestly enhanced in vitro stability in rat liver microsomes and in plasma, suggesting that it might be a pharmacokinetically more favorable surrogate of resiniferatoxin. Molecular modeling analyses with selected analogues provide evidence that the conformational differences could affect their binding affinities, especially for the ester versus amide at the B-region.

Published

2009

12. Alpha-substituted N-(4-tert-butylbenzyl)-N'-[4-(methylsulfonylamino)benzyl]thiourea analogues as potent and stereospecific TRPV1 antagonists.

Author

Chung JU, Kim SY, Lim JO, Choi HK, Kang SU, Yoon HS, Ryu H, Kang DW, Lee J, Kang B, Choi S, Toth A, Pearce LV, Pavlyukovets VA, Lundberg DJ, and Blumberg PM

Subjects

Animals, CHO Cells, Calcium metabolism, Capsaicin pharmacology, Cells, Cultured, Cricetinae, Cricetulus, Models, Molecular, Molecular Structure, Rats, Stereoisomerism, Structure-Activity Relationship, Thiourea chemical synthesis, Thiourea chemistry, TRPV Cation Channels antagonists & inhibitors, Thiourea pharmacology

Abstract

A series of alpha-substituted N-(4-tert-butylbenzyl)-N'-[4-(methylsulfonylamino)benzyl]thiourea analogues have been investigated as TRPV1 receptor antagonists. alpha-Methyl substituted analogues showed potent and stereospecific antagonism to the action of capsaicin on rat TRPV1 heterologously expressed in Chinese hamster ovary cells. In particular, compounds 14 and 18, which possess the R-configuration, exhibited excellent potencies (respectively, K(i)=41 and 39.2 nM and K(i(ant))=4.5 and 37 nM).

Published

2007

13. 2-Benzyl and 2-phenyl-3-hydroxypropyl pivalates as protein kinase C ligands.

Author

Lee J, Lee JH, Kim SY, Perry NA, Lewin NE, Ayres JA, and Blumberg PM

Subjects

Binding Sites, Ligands, Models, Molecular, Molecular Structure, Pentanoic Acids chemical synthesis, Pentanoic Acids metabolism, Phorbols chemistry, Phorbols metabolism, Protein Kinase C-alpha drug effects, Protein Kinase C-alpha metabolism, Structure-Activity Relationship, Pentanoic Acids chemistry, Protein Kinase C-alpha chemistry

Abstract

A series of 2-benzyl and 2-phenyl-3-hydroxypropyl pivalates designed to incorporate the principal pharmacophores of phorbol esters have been synthesized and tested as PKC-alpha ligands. Among the analogues, 13c exhibited the most potent binding affinity with a Ki = 0.7 microM. The synthesized analogues were subjected to molecular modeling analysis based on two alternative models of the phorbol pharmacophore and a docking study of 13c was carried out.

Published

2006

14. Analysis of structure-activity relationships with the N-(3-acyloxy-2-benzylpropyl)-N'-[4-(methylsulfonylamino)benzyl]thiourea template for vanilloid receptor 1 antagonism.

Author

Lee J, Kim SY, Lee J, Kang M, Kil MJ, Choi HK, Jin MK, Wang Y, Toth A, Pearce LV, Lundberg DJ, Tran R, and Blumberg PM

Subjects

Amides chemistry, Animals, Benzyl Compounds chemical synthesis, CHO Cells, Calcium metabolism, Cricetinae, Ligands, Models, Molecular, Molecular Conformation, Molecular Structure, Phenylthiourea chemical synthesis, Rats, Receptors, Drug genetics, Receptors, Drug metabolism, Structure-Activity Relationship, Thiourea chemical synthesis, Benzyl Compounds chemistry, Benzyl Compounds pharmacology, Phenylthiourea analogs & derivatives, Phenylthiourea chemistry, Phenylthiourea pharmacology, Receptors, Drug antagonists & inhibitors, Thiourea analogs & derivatives, Thiourea chemistry, Thiourea pharmacology

Abstract

In a continuing effort to elucidate the structure-activity relationships of the lead antagonist N-[2-(3,4-dimethylbenzyl)-3-pivaloyloxypropyl]-N'-[4-(methylsulfonylamino)benzyl]thiourea (1), the distances between the proposed four pharmacophores in 1 have been varied by insertion or deletion of one carbon to optimize their fit to the receptor. In addition, the acyloxy group of the C region was replaced with amide and N-hydroxy amide to identify the pharmacophoric importance of the ester group in the C2 region. The results indicated that the pharmacophoric arrangement of 1 was optimal for receptor binding affinity and antagonism, and the ester of the C2 region was significant for receptor binding. Among the derivatives, compound 19 showed distinct behavior with a 2-fold improvement in antagonism but a 13-fold reduction in binding affinity compared to 1. The partial separation of pharmacophoric requirements of these two assays has been noted before and compound 19 is thus selective for the calcium entry-linked receptor population. The conformational analysis of 1 generated three distinct conformers having different types of hydrophobic interactions, which will be utilized for exploring the active conformation of the VR1 ligand.

Published

2004

15. Structure-activity relationships of simplified resiniferatoxin analogues with potent VR1 agonism elucidates an active conformation of RTX for VR1 binding.

Author

Lee J, Kim SY, Park S, Lim JO, Kim JM, Kang M, Lee J, Kang SU, Choi HK, Jin MK, Welter JD, Szabo T, Tran R, Pearce LV, Toth A, and Blumberg PM

Subjects

Amides chemistry, Amides metabolism, Animals, CHO Cells, Calcium metabolism, Cricetinae, Diterpenes chemistry, Diterpenes metabolism, Ligands, Models, Molecular, Protein Binding drug effects, Protein Conformation drug effects, Rats, Receptors, Drug metabolism, Structure-Activity Relationship, Thiourea chemistry, Thiourea metabolism, Amides chemical synthesis, Receptors, Drug chemistry, Thiourea chemical synthesis

Abstract

We previously described a series of N-(3-acyloxy-2-benzylpropyl) homovanillate and N'-(4-hydroxy-3-methoxybenzyl) thiourea derivatives that were potent VR1 agonists with high-affinities and excellent analgesic profiles. The design of these simplified RTX analogues was based on our RTX-derived pharmacophore model which incorporates the 4-hydroxy-3-methoxyphenyl (A-region), C(20)-ester (B-region), orthophenyl (C1-region) and C(3)-keto (C2-region) groups of RTX. For the purpose of optimizing the spatial arrangement of the four principal pharmacophores on the lead agonists (1-4), we have modified the distances in the parent C-region, 3-acyloxy-2-benzylpropyl groups, by lengthening or shortening one carbon to vary the distances between the pharmacophores. We find that two of the amides, 4 and 19, possess EC(50) values <1 nM for induction of calcium influx in the VR1-CHO cells. As observed previously, the structure-activity relations for inhibition of RTX binding to VR1 and for induction of calcium uptake were distinct, presumably reflecting both intrinsic and methodological factors. In order to find the active conformation of VR1 ligands, the energy-minimized conformations of seven selected agonists were determined and the positions of their four pharmacophores were matched with those of five low energy RTX conformations. The rms values for the overlaps in the pharmacophores were calculated and correlated with the measured binding affinities (K(i)) and calcium influx (EC(50)) values. The binding affinities of the agonists correlated best with the RMS values derived from RTX conformation E (r(2)=0.92), predicting a model of the active conformation of RTX and related vanilloids for binding to VR1. Poorer correlation was obtained between any of the conformations and the EC(50) values for calcium influx.

Published

2004

16. N-[4-(methylsulfonylamino)benzyl]thiourea analogues as vanilloid receptor antagonists: analysis of structure-activity relationships for the "C-Region".

Author

Lee J, Kang SU, Lim JO, Choi HK, Jin MK, Toth A, Pearce LV, Tran R, Wang Y, Szabo T, and Blumberg PM

Subjects

Animals, Biochemistry methods, CHO Cells, Capsaicin pharmacology, Cricetinae, Drug Evaluation, Preclinical methods, Rats, Receptors, Drug metabolism, Structure-Activity Relationship, Receptors, Drug antagonists & inhibitors, Thiourea analogs & derivatives

Abstract

We recently reported that N-(4-t-butylbenzyl)-N'-[4-(methylsulfonylamino)benzyl] thiourea (2) was a high affinity antagonist of the vanilloid receptor with a binding affinity of K(i)=63 nM and an antagonism of K(i)=53.9 nM in rat VR1 heterologously expressed in Chinese hamster ovary (CHO) cells (Mol. Pharmacol. 2002, 62, 947-956). In an effort to further improve binding affinity and antagonistic potency, we have modified the C-region of the lead 4-t-butylbenzyl group with diverse surrogates, such as araalkyl, alkyl, 4-alkynylbenzyl, indanyl, 3,3-diarylpropyl, 4-alkoxybenzyl, 4-substituted piperazine and piperidine. The lipophilic surrogates, arylalkyl and alkyl, conferred modest decreases in binding affinities and antagonistic potencies; the groups having heteroatoms resulted in dramatic decreases. Our findings indicate that 4-t-butylbenzyl is one of the most favorable groups for high receptor binding and potent antagonism to VR1 in this structural series.

Published

2004

17. Conformationally constrained analogues of diacylglycerol (DAG). Effect on protein kinase C (PK-C) binding by the isosteric replacement of sn-1 and sn-2 esters in DAG-lactones.

Author

Kang JH, Chung HE, Kim SY, Kim Y, Lee J, Lewin NE, Pearce LV, Blumberg PM, and Marquez VE

Subjects

Amides chemistry, Amides metabolism, Esters chemistry, Esters metabolism, Hydrogen Bonding, Isomerism, Ligands, Models, Molecular, Molecular Conformation, Recombinant Proteins metabolism, Structure-Activity Relationship, Diglycerides chemistry, Diglycerides metabolism, Lactones chemistry, Lactones metabolism, Protein Kinase C metabolism

Abstract

In order to determine the importance of the two ester pharmacophores in high affinity, conformationally constrained DAG-lactones (Lac-1-5) as PK-C ligands, we have independently replaced the sn-1 and sn-2 carbonyl esters in these compounds by ketone (2, 10, 11), amide (3, 25-28), and hydroxyl (12, 13) isosteres. Although the ketone analogue of the sn-1 ester (2) exhibited comparable activity to the parent Lac-1 when taking into account the difference in lipophilicities, the other isosteres were significantly poorer PK-C alpha ligands compared to the parent DAG-lactones. This study demonstrates that the ester functionality in DAG-lactone plays an important role in the ligand's capacity to form a strong hydrogen bond with Gly253 at the active site. The discrete K(i) analysis from the sn-1 and sn-2 isosteres further confirms that the DAG-lactones bind preferentially to the C1-domain in the sn-2 binding mode, as previously suggested.

Published

2003

18. Phenolic modification as an approach to improve the pharmacology of the 3-acyloxy-2-benzylpropyl homovanillic amides and thioureas, a promising class of vanilloid receptor agonists and analgesics.

Author

Lee J, Lee J, Kang MS, Kim KP, Chung SJ, Blumberg PM, Yi JB, and Park YH

Subjects

Amides chemistry, Amides pharmacokinetics, Amides pharmacology, Analgesics blood, Analgesics chemistry, Analgesics pharmacokinetics, Animals, Calcium metabolism, Homovanillic Acid chemical synthesis, Homovanillic Acid pharmacokinetics, Male, Neurons drug effects, Phenol chemistry, Rats, Rats, Sprague-Dawley, Structure-Activity Relationship, Thiourea chemistry, Thiourea pharmacokinetics, Thiourea pharmacology, Analgesics pharmacology, Homovanillic Acid analogs & derivatives, Receptors, Drug agonists

Abstract

In order to improve the analgesic activity and pharmacokinetics of thioureas 2 and 3, which we previously developed as potent vanilloid receptor (VR) agonists, we prepared and characterized phenolic modifications of them and of their amide surrogates (7, 8). The aminoethyl analogue of the amide template 13 was a potent analgesic with an EC50=0.96 microg/kg in the AA-induced writhing test and with better in vivo stability than the parent phenol.

Published

2002

19. N-(3-acyloxy-2-benzylpropyl)-N'-dihydroxytetrahydrobenzazepine and tetrahydroisoquinoline thiourea analogues as vanilloid receptor ligands.

Author

Lee J, Lee J, Szabo T, Gonzalez AF, Welter JD, and Blumberg PM

Subjects

Animals, Benzazepines chemistry, Isoquinolines chemistry, Ligands, Magnetic Resonance Spectroscopy, Rats, Spectrophotometry, Infrared, Thiourea chemistry, Benzazepines metabolism, Isoquinolines metabolism, Receptors, Drug metabolism, Thiourea metabolism

Abstract

The vanilloid receptor represents a promising target for drug development. Building on our previous strategies which have generated potent agonists for VR1, we now describe a series of novel N-(3-acyloxy-2-benzylpropyl)-N'-dihydroxytetrahydrobenzazepine and tetrahydroisoquinoline thiourea analogues, several of which are potent VR1 antagonists. We report here the rationale for the design, the synthesis, and the in vitro characterization of activity in assays for [(3)H]resiniferatoxin binding and (45)Ca influx using heterologously expressed rat VR1.

Published

2001

20. N-(3-Acyloxy-2-benzylpropyl)-N'-(4-hydroxy-3-methoxybenzyl) thiourea derivatives as potent vanilloid receptor agonists and analgesics.

Author

Lee J, Lee J, Kim J, Kim SY, Chun MW, Cho H, Hwang SW, Oh U, Park YH, Marquez VE, Beheshti M, Szabo T, and Blumberg PM

Subjects

Animals, Capsaicin chemistry, Male, Mice, Mice, Inbred ICR, Models, Animal, Receptors, Drug chemistry, Structure-Activity Relationship, Thiourea pharmacology, Analgesics chemical synthesis, Receptors, Drug agonists, Thiourea chemical synthesis

Abstract

A series of N-(3-acyloxy-2-benzylpropyl)-N'-(4-hydroxy-3-methoxybenzyl) thiourea derivatives were investigated as vanilloid receptor ligands in an effort to discover a novel class of analgesics. The proposed pharmacophore model of resiniferatoxin. which includes the C20 homovanillic moiety, the C3-carbonyl and the orthoester phenyl ring as key pharmacophoric groups, was utilized as a guide for drug design. The compounds were synthesized after several steps from diethylmalonate and evaluated in vitro in a receptor binding assay and in a capsaicin-activated channel assay. Additional evaluation of analgesic activity, anti-inflammatory activity and pungency was conducted in animal models by the writhing test, the ear edema assay, and the eye-wiping test, respectively. Among the new compounds, 23 and 28 were found to be the most potent receptor agonists of the series with Ki values of 19 nM and 11 nM, respectively. Their strong in vitro potencies were also reflected by an excellent analgesic profile in animal tests with ED50 values of 0.5 microg kg for 23 and 1.0 microg/kg for 28. Relative to capsaicin these compounds appear to be ca. 600 and 300 times more potent. Both 23 and 28 were found to be less pungent than capsaicin based on the eye-wiping test. However, the compounds did not show significant anti-inflammatory activity. A molecular modeling study comparing the energy-minimized structures of resiniferatoxin and 35 demonstrated a good correlation in the spatial disposition of the corresponding key pharmacophores. The thioureas described in this investigation, which were designed as simplified resiniferatoxin surrogates, represent a novel class of potent vanilloid receptor agonists endowed with potent analgesic activity and reduced pungency.

Published

2001

21. Synthesis of bis-gamma-butyrolactones containing conformationally constrained (S)- and (R)-diacylglycerol structures.

Author

Lee J, Lewin NE, Blumberg PM, and Marquez VE

Subjects

Kinetics, Magnetic Resonance Spectroscopy, Molecular Conformation, Phorbol 12,13-Dibutyrate metabolism, Protein Kinase C metabolism, Stereoisomerism, 4-Butyrolactone chemistry, Diglycerides chemistry

Abstract

The synthesis of two sets of rigid diacylglycerol (DAG) analogues with either the (S)-DAG or (R)-DAG enantiomer embedded into a bis-gamma-butyrolactone template was accomplished stereoselectively from di-O-isopropylidene-alpha-D-apiose. The key step in both syntheses was the assemblage of the bicyclic perhydrofuro[3,4-b]furan ring system via a radical exo-dig intramolecular cyclization. A lipophilic undecanyl alkyl chain attached at C-3 of the fully assembled perhydrofuro[3,4-b]furan-2,4-dione (bis-gamma-butyrolactone) template can adopt two orientations with the one directed away from the concave face of the bicyclic system favored by a 4 to 1 ratio in each case. Evaluation of the final target pairs of enantiomers as PK-C alpha ligands revealed that the template containing an embedded (R)-DAG structure was more effective. The difference in binding affinity was also modulated by the direction of the alkyl chain.

Published

1996

22. Conformationally constrained analogues of diacylglycerol (DAG)--II. Differential interaction of delta-lactones and gamma-lactones with protein kinase C (PK-C).

Author

Lee J, Marquez VE, Blumberg PM, Krausz KW, and Kazanietz MG

Subjects

Binding Sites, Chromatography, Thin Layer, Diglycerides metabolism, Diglycerides pharmacology, Enzyme Activation, Kinetics, Magnetic Resonance Spectroscopy, Myristates chemistry, Myristates metabolism, Phosphorylation, Pyrones chemistry, Pyrones metabolism, Stereoisomerism, Diglycerides chemistry, Myristates pharmacology, Phorbol 12,13-Dibutyrate metabolism, Protein Kinase C metabolism, Pyrones pharmacology

Abstract

Starting with L- or D-tri-O-acetylglucal, the corresponding L- and D-isomers of 4-O-tetradecanoyl-2,3-dideoxyglucono-1,5-lactone (2a and 2b) were synthesized as rigid diacylglycerol (DAG) analogues. Consistent with results obtained previously with the equivalent L- and D-1,4-lactones (1a and 1b), the L-isomer (2a) was more potent in activating protein kinase C (PK-C) and inhibiting the binding of [3H]phorbol-12,13-dibutyrate to the enzyme's regulatory domain. In these experiments the difference in potency observed between the optical antipodes of the gluconolactones (2a and 2b) was greatly increased relative to the corresponding ribonolactones (1a and 1b). These results indicate that PK-C is more able to discriminate between optical antipodes, in favor of the L-isomer, as the lactone ring increases from five to six.

Published

1993