Joseph M. Pawluczyk | Researchain

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Featured researches published by Joseph M. Pawluczyk.

Bioorganic & Medicinal Chemistry Letters | 1999

Nonpeptide oxytocin antagonists: Analogs of L-371,257 with improved potency

Peter D. Williams; Mark G. Bock; Ben E. Evans; Roger M. Freidinger; Steven N. Gallicchio; Maribeth T. Guidotti; Marlene A. Jacobson; Michelle S. Kuo; Michelle R. Levy; Edward V. Lis; Stuart R. Michelson; Joseph M. Pawluczyk; Debra S. Perlow; Douglas J. Pettibone; Amy G. Quigley; Duane R. Reiss; Christopher A. Salvatore; Kenneth J. Stauffer; Carla J. Woyden

Structure-activity studies on the oxytocin antagonist 1 (L-371,257; Ki = 9.3 nM) have led to the identification of a related series of compounds containing an ortho-trifluoroethoxyphenylacetyl core which are orally bioavailable and have significantly improved potency in vitro and in vivo, e.g., compound 8 (L-374,943; Ki = 1.4 nM).

Bioorganic & Medicinal Chemistry Letters | 1998

Nonpeptide oxytocin antagonists : Potent, orally bioavailable analogs of L-371,257 containing a 1-R-(pyridyl)ethyl ether terminus

Michelle S. Kuo; Mark G. Bock; Roger M. Freidinger; Maribeth T. Guidotti; Edward V. Lis; Joseph M. Pawluczyk; Debra S. Perlow; Douglas J. Pettibone; Amy G. Quigley; Duane R. Reiss; Peter D. Williams; Carla J. Woyden

Structure-activity studies on the oxytocin antagonist 1 (L-371,257) have identified a new series of high affinity, receptor-selective OT antagonists in which the N-acetyl-4-piperidinyl ether terminus in 1 has been replaced with a 1-(aryl)ethoxy group.

Bioorganic & Medicinal Chemistry | 1994

Conformationally constrained o-tolylpiperazine camphorsulfonamide oxytocin antagonists. Structural modifications that provide high receptor affinity and suggest a bioactive conformation.

Peter D. Williams; Richard G. Ball; Bradley V. Clineschmidt; J. Chris Culberson; Jill M. Erb; Roger M. Freidinger; Joseph M. Pawluczyk; Debra S. Perlow; Douglas J. Pettibone; Daniel F. Veber

A series of new o-tolylpiperazine camphorsulfonamide OT antagonists is described. Analogs containing conformationally constrained 1-acylamino-2-propyl substituents at the camphor C2 endo position exhibit high affinity for OT and AVP-V1a receptors or high affinity and selectivity for OT receptors, depending on functionalities present in the acyl group. Determination of the preferred conformation of potency-enhancing 1-acylamino-2-propyl substituents using molecular mechanics energy calculations and X-ray crystallography, along with topological similarities to a conformationally constrained cyclic hexapeptide OT antagonist, suggests a receptor-bound conformation for this series of non-peptide OT antagonists.

Journal of Medicinal Chemistry | 1998

Development of orally active oxytocin antagonists: studies on 1-(1-[4-[1-(2-methyl-1-oxidopyridin-3-ylmethyl)piperidin-4-yloxy]-2- methoxybenzoyl]piperidin-4-yl)-1,4-dihydrobenz[d][1,3]oxazin-2-one (L-372,662) and related pyridines.

Ian M. Bell; Jill M. Erb; Roger M. Freidinger; Steven N. Gallicchio; James P. Guare; Maribeth T. Guidotti; Rita A. Halpin; Doug W. Hobbs; Carl F. Homnick; Michelle S. Kuo; Edward V. Lis; David J. Mathre; Stuart R. Michelson; Joseph M. Pawluczyk; Douglas J. Pettibone; Duane R. Reiss; Stanley Vickers; Peter D. Williams; Carla J. Woyden

Journal of Medicinal Chemistry | 1995

1-(1-[4-[(N-acetyl-4-piperidinyl)oxy]-2-methoxybenzoyl]piperidin-4- yl)-4H-3,1-benzoxazin-2(1H)-one (L-371,257): a new, orally bioavailable, non-peptide oxytocin antagonist.

Peter D. Williams; Bradley V. Clineschmidt; Jill M. Erb; Roger M. Freidinger; Maribeth T. Guidotti; Edward V. Lis; Joseph M. Pawluczyk; Douglas J. Pettibone; Duane R. Reiss; Daniel F. Veber

Journal of Medicinal Chemistry | 2002

Design and Synthesis of a Pro-Drug of Vinblastine Targeted at Treatment of Prostate Cancer with Enhanced Efficacy and Reduced Systemic Toxicity

Stephen F. Brady; Joseph M. Pawluczyk; Patricia K. Lumma; Dong-Mei Feng; Jenny M. Wai; Raymond E. Jones; Deborah Defeo-Jones; Bradley K. Wong; Cynthia Miller-Stein; Jiunn H. Lin; Allen Oliff; Roger M. Freidinger; Victor M. Garsky

Journal of Medicinal Chemistry | 1993

Nanomolar-affinity, non-peptide oxytocin receptor antagonists

Ben E. Evans; George F. Lundell; Kevin F. Gilbert; Mark G. Bock; Kenneth E. Rittle; Leigh Anne Carroll; Peter D. Williams; Joseph M. Pawluczyk; James L. Leighton

Molecular Cancer Therapeutics | 2002

A Prostate-specific Antigen (PSA)-activated Vinblastine Prodrug Selectively Kills PSA-secreting Cells in Vivo

Deborah Defeo-Jones; Stephen F. Brady; Dong-Mei Feng; Bradly K. Wong; Trina Bolyar; Kathleen M. Haskell; David M. Kiefer; Karen R. Leander; Elizabeth McAvoy; Patricia K. Lumma; Joseph M. Pawluczyk; Jenny M. Wai; Sherri L. Motzel; Kevin P. Keenan; Matthew J. van Zwieten; Jiunn H. Lin; Victor M. Garsky; Roger M. Freidinger; Allen Oliff; Raymond E. Jones

Tetrahedron Letters | 2007