John Wityak
Bristol-Myers Squibb
Network
Latest external collaboration on country level. Dive into details by clicking on the dots.
Publication
Featured researches published by John Wityak.
Bioorganic & Medicinal Chemistry Letters | 2003
Jagabandhu Das; Robert V. Moquin; James Lin; Chunjian Liu; Arthur M. Doweyko; Henry F. DeFex; Qiong Fang; Suhong Pang; Sidney Pitt; Ding Ren Shen; Gary L. Schieven; Joel C. Barrish; John Wityak
A series of structurally novel benzothiazole based small molecule inhibitors of p56(lck) was prepared to elucidate their structure-activity relationships (SAR), selectivity and cell activity in the T-cell proliferation assay. BMS-350751 (2) and BMS-358233 (3) are identified as potent Lck inhibitors with excellent cellular activities against T-cell proliferation.
Bioorganic & Medicinal Chemistry Letters | 2003
Jagabandhu Das; James Lin; Robert V. Moquin; Zhongqi Shen; Steven H. Spergel; John Wityak; Arthur M. Doweyko; Henry F. DeFex; Qiong Fang; Suhong Pang; Sidney Pitt; Ding Ren Shen; Gary L. Schieven; Joel C. Barrish
A series of structurally novel benzothiazole based small molecule inhibitors of p56(lck) were prepared to elucidate their structure-activity relationships (SARs), selectivity and cell activity in the T-cell proliferation assay. BMS-243117 (compound 2) is identified as a potent, and selective Lck inhibitor with good cellular activity (IC(50)=1.1 microM) against T-cell proliferation.
Bioorganic & Medicinal Chemistry Letters | 2002
Ping Chen; Derek J. Norris; Edwin J. Iwanowicz; Steven H. Spergel; James Lin; Henry H. Gu; Zhongqi Shen; John Wityak; Tai-An Lin; Suhong Pang; Henry de Fex; Sidney Pitt; Ding Ren Shen; Arthur M. Doweyko; Donna A. Bassolino; Jacques Y. Roberge; Michael A. Poss; Bang-Chi Chen; Gary L. Schieven; Joel C. Barrish
We have identified a novel series of 1,5-imidazoquinoxalines as inhibitors of Lck with excellent potency (IC50s<5 nM) as well as good cellular activity against T-cell proliferation (IC50s<1 microM). Structure-activity studies demonstrate the requirement for the core heterocycle in addition to an optimal 2,6-disubstituted aniline group.
Bioorganic & Medicinal Chemistry Letters | 2002
Ping Chen; Edwin J. Iwanowicz; Derek J. Norris; Henry H. Gu; James Lin; Robert V. Moquin; Jagabandhu Das; John Wityak; Steven H. Spergel; Henry de Fex; Suhong Pang; Sydney Pitt; Ding Ren Shen; Gary L. Schieven; Joel C. Barrish
A series of anilino(imidazoquinoxaline) analogues bearing solubilizing side chains at the 6- and 7-positions of the fused phenyl ring has been prepared and evaluated for inhibition against Lck enzyme and of T-cell proliferation. Significant improvement of the cellular activity was achieved over the initial lead, compound 2.
Archive | 2000
Jagabandhu Das; Ramesh Padmanabha; Ping Chen; Derek J. Norris; Arthur M. Doweyko; Joel C. Barrish; John Wityak
Archive | 2003
Joel C. Barrish; Jagabandhu Das; Steven B. Kanner; Chunjian Liu; Steven H. Spergel; John Wityak; Arthur M. Doweyko; Joseph A. Furch
Journal of Medicinal Chemistry | 2000
William J. Pitts; John Wityak; Joanne M. Smallheer; A. Ewa Tobin; James W. Jetter; Jennifer S. Buynitsky; Patricia P. Harlow; Kimberly A. Solomon; Martha H. Corjay; Shaker A. Mousa; and Ruth R. Wexler; Prabhakar K. Jadhav
Archive | 1997
John Wityak; Aleksandra Ewa Tobin
Bioorganic & Medicinal Chemistry Letters | 2006
Jagabandhu Das; Joseph A. Furch; Chunjian Liu; Robert V. Moquin; James Lin; Steven H. Spergel; Kim W. McIntyre; David J. Shuster; Kathleen D. O’Day; Becky Penhallow; Chen-Yi Hung; Arthur M. Doweyko; Amrita Kamath; Hongjian Zhang; Punit Marathe; Steven B. Kanner; Tai-An Lin; John H. Dodd; Joel C. Barrish; John Wityak
Bioorganic & Medicinal Chemistry Letters | 2005
Ashok V. Purandare; Aiming Gao; Honghe Wan; John E. Somerville; Christine Burke; Carrie Seachord; Wayne Vaccaro; John Wityak; Michael A. Poss
