Search

Your search keyword '"ELMORE, S. W."' showing total 19 results
Start Over Author "ELMORE, S. W."
19 results on '"ELMORE, S. W."'

2. Potent and selective small-molecule MCL-1 inhibitors demonstrate on-target cancer cell killing activity as single agents and in combination with ABT-263 (navitoclax)

Author

Leverson, J D, primary, Zhang, H, additional, Chen, J, additional, Tahir, S K, additional, Phillips, D C, additional, Xue, J, additional, Nimmer, P, additional, Jin, S, additional, Smith, M, additional, Xiao, Y, additional, Kovar, P, additional, Tanaka, A, additional, Bruncko, M, additional, Sheppard, G S, additional, Wang, L, additional, Gierke, S, additional, Kategaya, L, additional, Anderson, D J, additional, Wong, C, additional, Eastham-Anderson, J, additional, Ludlam, M J C, additional, Sampath, D, additional, Fairbrother, W J, additional, Wertz, I, additional, Rosenberg, S H, additional, Tse, C, additional, Elmore, S W, additional, and Souers, A J, additional

Published
2015
Full Text
View/download PDF

5. Bcl-2 family proteins are essential for platelet survival

Author

Zhang, H, primary, Nimmer, P M, additional, Tahir, S K, additional, Chen, J, additional, Fryer, R M, additional, Hahn, K R, additional, Iciek, L A, additional, Morgan, S J, additional, Nasarre, M C, additional, Nelson, R, additional, Preusser, L C, additional, Reinhart, G A, additional, Smith, M L, additional, Rosenberg, S H, additional, Elmore, S W, additional, and Tse, C, additional

Published
2007
Full Text
View/download PDF

11. Discovery of Potent Antagonists of the Antiapoptotic Protein XIAP for the Treatment of Cancer

Author

Oost, T. K., Sun, C., Armstrong, R. C., Al-Assaad, A.-S., Betz, S. F., Deckwerth, T. L., Ding, H., Elmore, S. W., Meadows, R. P., Olejniczak, E. T., Oleksijew, A., Oltersdorf, T., Rosenberg, S. H., Shoemaker, A. R., Tomaselli, K. J., Zou, H., and Fesik, S. W.

Abstract

Inhibitor of apoptosis (IAP) proteins are overexpressed in many cancers and have been implicated in tumor growth, pathogenesis, and resistance to chemo- or radiotherapy. On the basis of the NMR structure of a SMAC peptide complexed with the BIR3 domain of X-linked IAP (XIAP), a novel series of XIAP antagonists was discovered. The most potent compounds in this series bind to the baculovirus IAP repeat 3 (BIR3) domain of XIAP with single-digit nanomolar affinity and promote cell death in several human cancer cell lines. In a MDA-MB-231 breast cancer mouse xenograft model, these XIAP antagonists inhibited the growth of tumors. Close structural analogues that showed only weak binding to the XIAP−BIR3 domain were inactive in the cellular assays and showed only marginal in vivo activity. Our results are consistent with a mechanism in which ligands for the BIR3 domain of XIAP induce apoptosis by freeing up caspases. The present study validates the BIR3 domain of XIAP as a target and supports the use of small molecule XIAP antagonists as a potential therapy for cancers that overexpress XIAP.

Published
2004

12. Nonsteroidal Selective Glucocorticoid Modulators:  The Effect of C-10 Substitution on Receptor Selectivity and Functional Potency of 5-Allyl-2,5-dihydro-2,2,4-trimethyl-1H-[1]benzopyrano[3,4-f]quinolines

Author

Kym, P. R., Kort, M. E., Coghlan, M. J., Moore, J. L., Tang, R., Ratajczyk, J. D., Larson, D. P., Elmore, S. W., Pratt, J. K., Stashko, M. A., Falls, H. D., Lin, C. W., Nakane, M., Miller, L., Tyree, C. M., Miner, J. N., Jacobson, P. B., Wilcox, D. M., Nguyen, P., and Lane, B. C.

Abstract

The preparation and characterization of a series of C-10 substituted 5-allyl-2,5-dihydro-2,2,4-trimethyl-1H-[1]benzopyrano[3,4-f]quinolines as a novel class of selective ligands for the glucocorticoid receptor is described. Substitution at the C-10 position of the tetracyclic core with linear, two-atom appendages (OCH3, OCF2H, NHMe, SMe, CH&dbd;CH2, C&tbd1;CH, CH2OH) provided molecules of high affinity (Ki = 2−8 nM) for the human glucocorticoid receptor (hGR) with limited cross-reactivity with other steroid receptors (PR, MR, AR, ER). Optimal analogues showed slightly less potent but highly efficacious E-selectin repression with reduced levels of GRE activation efficacy in reporter gene assays relative to prednisolone. Preliminary SAR of analogues containing substitution at the C-9 and C-10 positions identified the 9-OH, 10-OMe analogue 50 and the 9-OH, 10-Cl analogue 58 as compounds that demonstrated potent, GR-mediated inhibition in a conconavalin A stimulated T-cell proliferation assay in both rodent and human whole blood monocytes. When evaluated for their in vivo effects in carrageenan-induced paw edema in rats, 50, 58, and 10-OCF2H analogue 35 showed dose-dependent anti-inflammatory effects (50, ED50 = 16 mg/kg; 58, ED50 = 15 mg/kg; 35, ED50 = 21 mg/kg vs ED50 = 15 mg/kg for 18 and ED50 = 4 mg/kg for prednisolone).

Published
2003

13. Nonsteroidal Selective Glucocorticoid Modulators:  the Effect of C-5 Alkyl Substitution on the Transcriptional Activation/Repression Profile of 2,5-Dihydro-10-methoxy-2,2,4-trimethyl-1H-[1]benzopyrano[3,4-f]quinolines

Author

Elmore, S. W., Coghlan, M. J., Anderson, D. D., Pratt, J. K., Green, B. E., Wang, A. X., Stashko, M. A., Lin, C. W., Tyree, C. M., Miner, J. N., Jacobson, P. B., Wilcox, D. M., and Lane, B. C.

Abstract

The preparation and characterization of a series of selective glucocorticoid receptor modulators are described. The preliminary structure−activity relationship of nonaromatic C-5 substitution on the tetracyclic quinoline core showed a preference for small lipophilic side chains. Proper substitution at this position maintained the transcriptional repression of proinflammatory transcription factors while diminishing the transcriptional activation activity of the ligand/glucocorticoid receptor complex. The optimal compounds described in this study were the allyl analogue 18 and cyclopentyl analogue 32. These candidates showed slightly less potent, highly efficacious E-selectin repression with significantly reduced levels of glucocorticoid response element activation in reporter gene assays vs prednisolone. Allyl analogue 18 was evaluated in vivo. An oral dose of 18 showed an ED50 = 1.7 mg/kg as compared to 1.2 mg/kg for prednisolone in the Sephadex-induced pulmonary eosinophilia model and an ED50 = 15 mg/kg vs 4 mg/kg for prednisolone in the carrageenan-induced paw edema model.

Published
2001

14. Synthesis and Characterization of Non-Steroidal Ligands for the Glucocorticoid Receptor:  Selective Quinoline Derivatives with Prednisolone-Equivalent Functional Activity

Author

Coghlan, M. J., Kym, P. R., Elmore, S. W., Wang, A. X., Luly, J. R., Wilcox, D., Stashko, M., Lin, C.-W., Miner, J., Tyree, C., Nakane, M., Jacobson, P., and Lane, B. C.

Abstract

A novel class of functional ligands for the human glucocorticoid receptor is described. Substituents in the C-10 position of the tetracyclic core are essential for glucocorticoid receptor (GR) selectivity versus other steroid receptors. The C-5 position is derivatized with meta-substituted aromatic groups, resulting in analogues with a high affinity for GR (Ki = 2.4−9.3 nM) and functional activity comparable to prednisolone in reporter gene assays of glucocorticoid-mediated gene transcription. The biological activity of these novel quinolines was also prednisolone-equivalent in whole cell assays of glucocorticoid function, and compound 13 was similar to prednisolone (po ED50 = 2.8 mpk for 13 vs ED50 = 1.2 mpk for prednisolone) in a rodent model of asthma (sephadex-induced eosinophil influx).

Published
2001

15. Structure−Activity Studies for a Novel Series of Tricyclic Substituted Hexahydrobenz[e]isoindole α<INF>1A</INF> Adrenoceptor Antagonists as Potential Agents for the Symptomatic Treatment of Benign Prostatic Hyperplasia (BPH)

Author

Meyer, M. D., Altenbach, R. J., Basha, F. Z., Carroll, W. A., Condon, S., Elmore, S. W., Kerwin, J. F., Jr., Sippy, K. B., Tietje, K., Wendt, M. D., Hancock, A. A., Brune, M. E., Buckner, S. A., and Drizin, I.

Abstract

In search of a uroselective agent that exhibits a high level of selectivity for the α1A receptor, a novel series of tricyclic hexahydrobenz[e]isoindoles was synthesized. A generic pharmacophoric model was developed requiring the presence of a basic amine core and a fused heterocyclic side chain separated by an alkyl chain. It was shown that the 6-OMe substitution with R, R stereochemistry of the ring junction of the benz[e]isoindole and a two-carbon spacer chain were optimal. In contrast to the highly specific requirements for the benz[e]isoindole portion and linker chain, a wide variety of tricyclic fused heterocyclic attachments were tolerated with retention of potency and selectivity. In vitro functional assays for the α1 adrenoceptor subtypes were used to further characterize these compounds, and in vivo models of vascular vs prostatic tone were used to assess uroselectivity.

Published
2000

16. Synthesis and Pharmacological Characterization of 3-[2-((3aR,9bR)-cis-6-Methoxy- 2,3,3a,4,5,9b-hexahydro-1H- benz[e]isoindol-2-yl)ethyl]pyrido[3‘,4‘:4,5]thieno[3,2-d]pyrimidine- 2,4(1H,3H)-dione (A-131701):  A Uroselective α<INF>1A</INF> Adrenoceptor Antagonist for the Symptomatic Treatment of Benign Prostatic Hyperplasia<SUP>1</SUP><BBR RID="jm970364ab00001">

Author

Meyer, M. D., Altenbach, R. J., Basha, F. Z., Carroll, W. A., Drizin, I., Elmore, S. W., Ehrlich, P. P., Lebold, S. A., Tietje, K., Sippy, K. B., Wendt, M. D., Plata, D. J., Plagge, F., Buckner, S. A., Brune, M. E., Hancock, A. A., and Kerwin, J. F., Jr.

Published
1997

18. Structure-activity studies for a novel series of tricyclic substituted hexahydrobenz[e]isoindole alpha(1A) adrenoceptor antagonists as potential agents for the symptomatic treatment of benign prostatic hyperplasia (BPH).

Author

Meyer MD, Altenbach RJ, Basha FZ, Carroll WA, Condon S, Elmore SW, Kerwin JF Jr, Sippy KB, Tietje K, Wendt MD, Hancock AA, Brune ME, Buckner SA, and Drizin I

Subjects
Adrenergic alpha-Antagonists chemistry, Adrenergic alpha-Antagonists metabolism, Adrenergic alpha-Antagonists pharmacology, Animals, Blood Pressure drug effects, Cell Line, Dogs, Heterocyclic Compounds, 3-Ring chemistry, Heterocyclic Compounds, 3-Ring metabolism, Heterocyclic Compounds, 3-Ring pharmacology, Indoles chemistry, Indoles metabolism, Indoles pharmacology, Male, Pressure, Prostatic Hyperplasia drug therapy, Radioligand Assay, Rats, Rats, Inbred SHR, Stereoisomerism, Structure-Activity Relationship, Urethra drug effects, Urethra physiology, Adrenergic alpha-Antagonists chemical synthesis, Heterocyclic Compounds, 3-Ring chemical synthesis, Indoles chemical synthesis
Abstract

In search of a uroselective agent that exhibits a high level of selectivity for the alpha(1A) receptor, a novel series of tricyclic hexahydrobenz[e]isoindoles was synthesized. A generic pharmacophoric model was developed requiring the presence of a basic amine core and a fused heterocyclic side chain separated by an alkyl chain. It was shown that the 6-OMe substitution with R, R stereochemistry of the ring junction of the benz[e]isoindole and a two-carbon spacer chain were optimal. In contrast to the highly specific requirements for the benz[e]isoindole portion and linker chain, a wide variety of tricyclic fused heterocyclic attachments were tolerated with retention of potency and selectivity. In vitro functional assays for the alpha(1) adrenoceptor subtypes were used to further characterize these compounds, and in vivo models of vascular vs prostatic tone were used to assess uroselectivity.

Published
2000
Full Text
View/download PDF

19. Synthesis and pharmacological characterization of 3-[2-((3aR,9bR)-cis-6-methoxy-2,3,3a,4,5,9b-hexahydro-1H-benz[e] isoindol-2-yl)ethyl]pyrido-[3',4':4,5]thieno[3,2-d]pyrimidine-2,4 (1H,3H)-dione (A-131701): a uroselective alpha 1A adrenoceptor antagonist for the symptomatic treatment of benign prostatic hyperplasia.

Author

Meyer MD, Altenbach RJ, Basha FZ, Carroll WA, Drizin I, Elmore SW, Ehrlich PP, Lebold SA, Tietje K, Sippy KB, Wendt MD, Plata DJ, Plagge F, Buckner SA, Brune ME, Hancock AA, and Kerwin JF Jr

Subjects
Adrenergic alpha-Antagonists therapeutic use, Animals, Dogs, Humans, Indoles therapeutic use, Isoindoles, Male, Models, Chemical, Prazosin analogs & derivatives, Prazosin therapeutic use, Pyrimidinones therapeutic use, Rats, Receptors, Adrenergic, alpha-1, Sulfonamides therapeutic use, Tamsulosin, Adrenergic alpha-1 Receptor Antagonists, Adrenergic alpha-Antagonists chemical synthesis, Indoles chemical synthesis, Prostatic Hyperplasia drug therapy, Pyrimidinones chemical synthesis
Published
1997
Full Text
View/download PDF

Catalog

Books, media, physical & digital resources
See catalog results