Stanley L. Gaul
United States Military Academy
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Publication
Featured researches published by Stanley L. Gaul.
Bioorganic & Medicinal Chemistry Letters | 2003
Christopher F. Claiborne; John A. Mccauley; Brian E. Libby; Neil Roy Curtis; Helen J Diggle; Janusz Jozef Kulagowski; Stuart R. Michelson; Kenneth D. Anderson; David A. Claremon; Roger M. Freidinger; Rodney A. Bednar; Scott D. Mosser; Stanley L. Gaul; Thomas M. Connolly; Cindra Condra; Bohumil Bednar; Gary L. Stump; Joseph J. Lynch; Alison Macaulay; Keith A. Wafford; Kenneth S. Koblan; Nigel J. Liverton
A novel series of benzamidines was synthesized and shown to exhibit NR2B-subtype selective NMDA antagonist activity. Compound 31 is orally active in a carrageenan-induced rat hyperalgesia model of pain and shows no motor coordination side effects.
Bioorganic & Medicinal Chemistry Letters | 2002
Philippe G. Nantermet; James C. Barrow; George F Lundell; Janetta M. Pellicore; Kenneth E. Rittle; MaryBeth Young; Roger M. Freidinger; Thomas M. Connolly; Cindra Condra; Jerzy Karczewski; Rodney A. Bednar; Stanley L. Gaul; Robert J. Gould; Kris Prendergast; Harold G. Selnick
The synthesis and biological evaluation of a series of nonpeptidic small molecule antagonists of the human platelet thrombin receptor (PAR-1) are described. Optimization of the 5-amino-3-arylisoxazole lead resulted in an approximate 100-fold increase in potency. The most potent of these compounds (54) inhibits platelet activation with IC(50)s of 90 nM against the thrombin receptor agonist peptide (TRAP) and 510 nM against thrombin as the agonist. Further, antagonist 54 fully blocks platelet aggregation stimulated by 1 nM thrombin for 10 min.
Bioorganic & Medicinal Chemistry Letters | 2001
James C. Barrow; Philippe G. Nantermet; Harold G. Selnick; Kristen L Glass; Phung L. Ngo; Mary Beth Young; Janetta M. Pellicore; Michael J. Breslin; John H. Hutchinson; Roger M. Freidinger; Cindra Condra; Jerzy Karczewski; Rodney A. Bednar; Stanley L. Gaul; Andrew M. Stern; Robert J. Gould; Thomas M. Connolly
Thrombin is the most potent agonist of platelet activation, and its effects are predominantly mediated by platelet thrombin receptors. Therefore, antagonists of the thrombin receptor have potential utility for the treatment of thrombotic disorders. Screening of combinatorial libraries revealed 2 to be a potent antagonist of the thrombin receptor. Modifications of this structure produced 11k, which inhibits thrombin receptor stimulated secretion and aggregation of platelets.
Bioorganic & Medicinal Chemistry Letters | 1996
Melissa S. Egbertson; George D. Hartman; Robert J. Gould; Bohumil Bednar; Rodney A. Bednar; Jacquelynn J. Cook; Stanley L. Gaul; Marie A. Holahan; Laura A. Libby; J.J. Lynch; Robert J. Lynch; Gary R. Sitko; Maria T. Stranieri; Laura M. Vassallo
Abstract Potency enhancing features of two series of fibrinogen receptor antagonists were combined to give analogs with improved potency and oral activity. Antagonists containing either alkyl or aryl sulfonamides and a central isoindolinone structural constraint demonstrate high affinity for both activated and unactivated platelet receptors.
European Journal of Pharmacology | 1975
Charles S. Sweet; Stanley L. Gaul
Hydrochlorothiazide, administered at 1, 3 and 9 mg/kg/day p.o. for 4 days, produced a dose-dependent lowering of plasma potassium and an elevation in plasma renin activity in unanesthetized dogs. When plasma renin activity was suppressed in diuretic-treated dogs by the potent beta-adrenergic receptor-blocking drug, timolol (0.5, 2 mg/kg/day p.o. for 4 days), the hypokalemia and hyperreninemia were significantly less pronounced. The data suggest that beta-adrenergic blocking drugs can be used to antagonize these side effects of diuretics.
Bioorganic & Medicinal Chemistry Letters | 2009
Charles J. McIntyre; John A. Mccauley; Bohumil Bednar; Rodney A. Bednar; John W. Butcher; David A. Claremon; Michael E. Cunningham; Roger M. Freidinger; Stanley L. Gaul; Carl F. Homnick; Ken S. Koblan; Scott D. Mosser; Joseph J. Romano; Nigel J. Liverton
A novel series of annulated tricyclic compounds was synthesized and evaluated as NMDA/NR2B antagonists. Structure-activity development was directed towards in vitro optimization of NR2B activity and selectivity over the hERG K(+) channel. Preferred compounds were subsequently evaluated for selectivity in an alpha(1)-adrenergic receptor binding counter-screen and a cell-based assay of NR2B activity.
Biochemistry | 1994
Kurt Freund; Kundan P. Doshi; Stanley L. Gaul; David A. Claremon; David C. Remy; John J. Baldwin; Steven M. Pitzenberger; Andrew M. Stern
Journal of Medicinal Chemistry | 1997
Benny C. Askew; Rodney A. Bednar; Bohumil Bednar; David A. Claremon; Jacquelynn J. Cook; Charles J. Mcintyre; Cecila A. Hunt; Robert J. Gould; Robert J. Lynch; Joseph J. Lynch; Stanley L. Gaul; Maria T. Stranieri; Gary R. Sitko; Marie A. Holahan; Joan D. Glass; Terrence Hamill; Lynn M. Gorham; Thomayant Prueksaritanont; John J. Baldwin; George D. Hartman
Journal of Medicinal Chemistry | 2004
John A. McCauley; Cory R. Theberge; Joseph J. Romano; Susan B. Billings; Kenneth D. Anderson; David A. Claremon; Roger M. Freidinger; Rodney A. Bednar; Scott D. Mosser; Stanley L. Gaul; Thomas M. Connolly; Cindra Condra; Menghang Xia; Michael E. Cunningham; Bohumil Bednar; Gary L. Stump; Joseph J. Lynch; Alison Macaulay; Keith A. Wafford; Kenneth S. Koblan; Nigel J. Liverton
Journal of Medicinal Chemistry | 1999
Melissa S. Egbertson; Jacquelynn J. Cook; Bohumil Bednar; John D. Prugh; Rodney A. Bednar; Stanley L. Gaul; Robert J. Gould; George D. Hartman; Carl F. Homnick; Marie A. Holahan; Laura A. Libby; Joseph J. Lynch; Robert J. Lynch; Gary R. Sitko; Maria T. Stranieri; Laura M. Vassallo
