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Dive into the research topics where Xianming Jin is active.

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Featured researches published by Xianming Jin.


ACS Medicinal Chemistry Letters | 2015

Structure-Based Drug Design of Novel, Potent, and Selective Azabenzimidazoles (ABI) as ATR Inhibitors

Paul A. Barsanti; Yue Pan; Yipin Lu; Rama Jain; Matthew Cox; Robert Aversa; Michael P. Dillon; Robert A. Elling; Cheng Hu; Xianming Jin; Mark Knapp; Jiong Lan; Savithri Ramurthy; Patrick Rudewicz; Lina Setti; Sharadha Subramanian; Michelle Mathur; Lorena Taricani; George Thomas; Linda Xiao; Qin Yue

Compound 13 was discovered through morphing of the ATR biochemical HTS hit 1. The ABI series was potent and selective for ATR. Incorporation of a 6-azaindole afforded a marked increase in cellular potency but was associated with poor PK and hERG ion channel inhibition. DMPK experiments established that CYP P450 and AO metabolism in conjunction with Pgp and BCRP efflux were major causative mechanisms for the observed PK. The series also harbored the CYP3A4 TDI liability driven by the presence of both a morpholine and an indole moiety. Incorporation of an adjacent fluorine or nitrogen into the 6-azaindole addressed many of the various medicinal chemistry issues encountered.


ACS Medicinal Chemistry Letters | 2015

Structure-Based Drug Design of Novel Potent and Selective Tetrahydropyrazolo[1,5-a]pyrazines as ATR Inhibitors.

Paul A. Barsanti; Robert Aversa; Xianming Jin; Yue Pan; Yipin Lu; Robert A. Elling; Rama Jain; Mark Knapp; Jiong Lan; Xiaodong Lin; Patrick Rudewicz; Janet Sim; Lorena Taricani; George Thomas; Linda Xiao; Qin Yue

A saturation strategy focused on improving the selectivity and physicochemical properties of ATR inhibitor HTS hit 1 led to a novel series of highly potent and selective tetrahydropyrazolo[1,5-a]pyrazines. Use of PI3Kα mutants as ATR crystal structure surrogates was instrumental in providing cocrystal structures to guide the medicinal chemistry designs. Detailed DMPK studies involving cyanide and GSH as trapping agents during microsomal incubations, in addition to deuterium-labeled compounds as mechanistic probes uncovered the molecular basis for the observed CYP3A4 TDI in the series.


Archive | 2012

PYRIDINE BIARYL AMINE COMPOUNDS AND THEIR USES

William R. Antonios-Mccrea; Paul A. Barsanti; Cheng Hu; Xianming Jin; Xiaodong Lin; Eric J. Martin; Yue Pan; Keith B. Pfister; Paul A. Renhowe; Martin Sendzik; James C. Sutton; Lifeng Wan


Archive | 2012

N-acyl pyridine biaryl compounds and their uses

Paul A. Barsanti; Cheng Hu; Xianming Jin; Simon Ng; Keith B. Pfister; Martin Sendzik; James C. Sutton


Archive | 2012

N-acyl pyrimidine biaryl compounds as protein kinase inhibitors

Paul A. Barsanti; Cheng Hu; Xianming Jin; Simon Ng; Keith B. Pfister; Martin Sendzik; James C. Sutton


Archive | 2011

Phenyl-heteroaryl amine compounds and their uses

William R. Antonios-Mccrea; Paul A. Barsanti; Cheng Hu; Xianming Jin; Eric J. Martin; Yue Pan; Keith B. Pfister; Martin Sendzik; James C. Sutton; Lifeng Wan


Archive | 2011

3-(AMINOARYL)-PYRIDINE COMPOUNDS

William R. Antonios-McCrea; Paul A. Barsanti; Cheng Hu; Xianming Jin; Eric J. Martin; Yue Pan; Keith B. Pfister; Martin Sendzik; James Sutton; Lifeng Wan


Archive | 2012

Substituted bi-heteroaryl compounds as cdk9 inhibitors and their uses

William R. Antonios-McCrea; Paul A. Barsanti; Cheng Hu; Xianming Jin; Eric J. Martin; Yue Pan; Xiaodong Lin; Keith B. Pfister; Paul A. Renhowe; Martin Sendzik; James Sutton; Lifeng Wan


Archive | 2012

Pyrimidine biaryl amine compounds and their use as cdk9 inhibitors

William R. Antonios-Mccrea; Paul A. Barsanti; Cheng Hu; Xianming Jin; Xiaodong Lin; Eric J. Martin; Yue Pan; Keith B. Pfister; Paul A. Renhowe; Martin Sendzik; James C. Sutton; Lifeng Wan


Archive | 2010

Bipyridines useful for the treatment of proliferative diseases

Paul A. Barsanti; Zheng Chen; Cheng Hu; Xianming Jin; Simon Ng; Keith B. Pfister; Martin Sendzik; James C. Sutton

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