John J. Piwinski
Merck & Co.
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Publication
Featured researches published by John J. Piwinski.
Bioorganic & Medicinal Chemistry Letters | 2010
Wensheng Yu; Zhuyan Guo; Peter Orth; Madison; Liya Chen; Chaoyang Dai; Robert J. Feltz; Viyyoor Moopil Girijavallabhan; Seongkon Kim; Joseph A. Kozlowski; Brian J. Lavey; Dansu Li; Daniel Lundell; Xiaoda Niu; John J. Piwinski; Janeta Popovici-Muller; Razia Rizvi; Kristin E. Rosner; Bandarpalle B. Shankar; Neng-Yang Shih; M.A Siddiqui; Jing Sun; Ling Tong; Shelby Umland; Michael K.C. Wong; De-Yi Yang; Guowei Zhou
We disclose inhibitors of TNF-alpha converting enzyme (TACE) designed around a hydantoin zinc binding moiety. Crystal structures of inhibitors bound to TACE revealed monodentate coordination of the hydantoin to the zinc. SAR, X-ray, and modeling designs are described. To our knowledge, these are the first reported X-ray structures of TACE with a hydantoin zinc ligand.
Bioorganic & Medicinal Chemistry Letters | 2010
Wensheng Yu; Ling Tong; Seong Heon Kim; Michael K.C. Wong; Lei Chen; De-Yi Yang; Bandarpalle B. Shankar; Brian J. Lavey; Guowei Zhou; Aneta Kosinski; Razia Rizvi; Dansu Li; Robert J. Feltz; John J. Piwinski; Kristin E. Rosner; Neng-Yang Shih; M. Arshad Siddiqui; Zhuyan Guo; Peter Orth; Himanshu Shah; Jing Sun; Shelby Umland; Daniel Lundell; Xiaoda Niu; Joseph A. Kozlowski
We disclose further optimization of hydantoin TNF-alpha convertase enzyme (TACE) inhibitors. SAR with respect to the non-prime region of TACE active site was explored. A series of biaryl substituted hydantoin compounds was shown to have sub-nanomolar K(i), good rat PK, and good selectivity versus MMP-1, -2, -3, -7, -9, and -13.
Bioorganic & Medicinal Chemistry Letters | 2011
Chaoyang Dai; Dansu Li; Janeta Popovici-Muller; Lianyun Zhao; Vinay Girijavallabhan; Kristin E. Rosner; Brian J. Lavey; Razia Rizvi; Bandarpalle B. Shankar; Michael K.C. Wong; Zhuyan Guo; Peter Orth; Corey O. Strickland; Jing Sun; Xiaoda Niu; Shiying Chen; Joseph A. Kozlowski; Daniel Lundell; John J. Piwinski; Neng-Yang Shih; M. Arshad Siddiqui
TNF-α converting enzyme (TACE) inhibitors are promising agents to treat inflammatory disorders and cancer. We have investigated novel tartrate diamide TACE inhibitors where the tartrate core binds to zinc in a unique tridentate fashion. Incorporating (R)-2-(2-N-alkylaminothiazol-4-yl)pyrrolidines into the left hand side amide of the tartrate scaffold led to the discovery of potent and selective TACE inhibitors, some of which exhibited good rat oral bioavailability.
Bioorganic & Medicinal Chemistry Letters | 2010
Vinay Girijavallabhan; Lei Chen; Chaoyang Dai; Robert J. Feltz; Luke Firmansjah; Dansu Li; Seong Heon Kim; Joseph A. Kozlowski; Brian J. Lavey; Aneta Kosinski; John J. Piwinski; Janeta Popovici-Muller; Razia Rizvi; Kristin E. Rosner; Banderpalle B. Shankar; Neng-Yang Shih; M. Arshad Siddiqui; Ling Tong; Michael K.C. Wong; De-Yi Yang; Liping Yang; Wensheng Yu; Guowei Zhou; Zhuyan Guo; Peter Orth; Vincent Madison; Hong Bian; Daniel Lundell; Xiaoda Niu; Himanshu Shah
Our research on hydantoin based TNF-α converting enzyme (TACE) inhibitors has led to an acetylene containing series that demonstrates sub-nanomolar potency (K(i)) as well as excellent activity in human whole blood. These studies led to the discovery of highly potent TACE inhibitors with good DMPK profiles.
Bioorganic & Medicinal Chemistry Letters | 2012
Rongze Kuang; Ho-Jane Shue; Li Xiao; David J. Blythin; Neng-Yang Shih; Xiao Chen; Danlin Gu; John Schwerdt; Ling Lin; Pauline C. Ting; Jianhua Cao; Robert Aslanian; John J. Piwinski; Daniel Prelusky; Ping Wu; Ji Zhang; Xiang Zhang; Chander S. Celly; Motasim Billah; Peng Wang
Optimization of oxazole-based PDE4 inhibitors has led to the discovery of a series of quinolyl oxazoles, with 4-benzylcarboxamide and 5-α-aminoethyl groups which exhibit picomolar potency against PDE4. Selectivity profiles and in vivo biological activity are also reported.
Bioorganic & Medicinal Chemistry Letters | 2010
Dansu Li; Janeta Popovici-Muller; David B. Belanger; John P. Caldwell; Chaoyang Dai; Maria David; Vinay Girijavallabhan; Brian J. Lavey; Joe F. Lee; Zhidan Liu; Rob Mazzola; Razia Rizvi; Kristin E. Rosner; Bandarpalle B. Shankar; Jim Spitler; Pauline C. Ting; Henry M. Vaccaro; Wensheng Yu; Guowei Zhou; Zhaoning Zhu; Xiaoda Niu; Jing Sun; Zhuyan Guo; Peter Orth; Shiying Chen; Joseph A. Kozlowski; Daniel Lundell; Vincent Madison; Brian A. McKittrick; John J. Piwinski
The syntheses and structure-activity relationships of the tartrate-based TACE inhibitors are discussed. The optimization of both the prime and non-prime sites led to compounds with picomolar activity. Several analogs demonstrated good rat pharmacokinetics.
Bioorganic & Medicinal Chemistry Letters | 2012
Cecil D. Kwong; Jeremy L. Clark; Anita T. Fowler; Feng Geng; Hollis S. Kezar; Abhijit Roychowdhury; Robert C. Reynolds; Joseph A. Maddry; Subramaniam Ananthan; John A. Secrist; Neng-Yang Shih; John J. Piwinski; Cheng Li; Boris Feld; Hsueh-Cheng Huang; Xiao Tong; F. George Njoroge; Ashok Arasappan
Compound 1 was identified as a HCV replication inhibitor from screening/early SAR triage. Potency improvement was achieved via modulation of substituent on the 5-azo linkage. Due to potential toxicological concern, the 5-azo linkage was replaced with 5-alkenyl or 5-alkynyl moiety. Analogs containing the 5-alkynyl linkage were found to be potent inhibitors of HCV replication. Further evaluation identified compounds 53 and 63 with good overall profile, in terms of replicon potency, selectivity and in vivo characteristics. Initial target engagement studies suggest that these novel carbanucleoside-like derivatives may inhibit the HCV replication complex (replicase).
Bioorganic & Medicinal Chemistry Letters | 2012
Ashok Arasappan; Frank Bennett; Vinay Girijavallabhan; Yuhua Huang; Regina Huelgas; Carmen Alvarez; Lei Chen; Stephen Gavalas; Seong-Heon Kim; Aneta Kosinski; Patrick Pinto; Razia Rizvi; Randall R. Rossman; Bandarpalle B. Shankar; Ling Tong; Francisco Velazquez; Srikanth Venkatraman; Vishal Verma; Joseph A. Kozlowski; Neng-Yang Shih; John J. Piwinski; Malcolm Maccoss; Cecil D. Kwong; Jeremy L. Clark; Anita T. Fowler; Feng Geng; Hollis S. Kezar; Abhijit Roychowdhury; Robert C. Reynolds; Joseph A. Maddry
Based on a previously identified HCV replication (replicase) inhibitor 1, SAR efforts were conducted around the pyrimidine core to improve the potency and pharmacokinetic profile of the inhibitors. A benzothiazole moiety was found to be the optimal substituent at the pyrimidine 5-position. Due to potential reactivity concern, the 4-chloro residue was replaced by a methyl group with some loss in potency and enhanced rat in vivo profile. Extensive investigations at the C-2 position resulted in identification of compound 16 that demonstrated very good replicon potency, selectivity and rodent plasma/target organ concentration. Inhibitor 16 also demonstrated good plasma levels and oral bioavailability in dogs, while monkey exposure was rather low. Chemistry optimization towards a practical route to install the benzothiazole moiety resulted in an efficient direct C-H arylation protocol.
Bioorganic & Medicinal Chemistry Letters | 2012
Vinay Girijavallabhan; Carmen Alvarez; Frank Bennett; Lei Chen; Stephen Gavalas; Yuhua Huang; Seong-Heon Kim; Aneta Kosinski; Patrick Pinto; Razia Rizvi; Randall R. Rossman; Bandarpalle B. Shankar; Ling Tong; Francisco Velazquez; Srikanth Venkatraman; Vishal Verma; Joseph A. Kozlowski; Neng-Yang Shih; John J. Piwinski; Malcolm Maccoss; Cecil D. Kwong; Namita Bansal; Jeremy L. Clark; Anita T. Fowler; Hollis S. Kezar; Jacob Valiyaveettil; Robert C. Reynolds; Joseph A. Maddry; Subramaniam Ananthan; John A. Secrist
Introduction of a nitrogen atom into the benzene ring of a previously identified HCV replication (replicase) benzothiazole inhibitor 1, resulted in the discovery of the more potent pyridothiazole analogues 3. The potency and PK properties of the compounds were attenuated by the introductions of various functionalities at the R(1), R(2) or R(3) positions of the molecule (compound 3). Inhibitors 38 and 44 displayed excellent potency, selectivity (GAPDH/MTS CC(50)), PK parameters in all species studied, and cross genotype activity.
Bioorganic & Medicinal Chemistry Letters | 2012
Frank Bennett; Hollis S. Kezar; Vinay Girijavallabhan; Yuhua Huang; Regina Huelgas; Randall R. Rossman; Neng-Yang Shih; John J. Piwinski; Malcolm Maccoss; Cecil D. Kwong; Jeremy L. Clark; Anita T. Fowler; Feng Geng; Abhijit Roychowdhury; Robert C. Reynolds; Joseph A. Maddry; Subramaniam Ananthan; John A. Secrist; Cheng Li; Robert Chase; Stephanie Curry; Hsueh-Cheng Huang; Xiao Tong; F. George Njoroge; Ashok Arasappan
Introduction of nitrogen atom into the benzene ring of a previously identified HCV replication (replicase) benzofuran inhibitor 2, resulted in the discovery of the more potent pyridofuran analogue 5. Subsequent introduction of small alkyl and alkoxy ligands into the pyridine ring resulted in further improvements in replicon potency. Replacement of the 4-chloro moiety on the pyrimidine core with a methyl group, and concomitant monoalkylation of the C-2 amino moiety resulted in the identification of several inhibitors with desirable characteristics. Inhibitor 41, from the monosubstituted pyridofuran and inhibitor 50 from the disubstituted series displayed excellent potency, selectivity (GAPDH/MTS CC(50)) and PK parameters in all species studied, while the selectivity in the thymidine incorporation assay (DNA·CC(50)) was low.
