Guozhang Xu
Johnson & Johnson Pharmaceutical Research and Development
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Publication
Featured researches published by Guozhang Xu.
Bioorganic & Medicinal Chemistry Letters | 2008
Guozhang Xu; Marta C. Abad; Peter J. Connolly; Michael P. Neeper; Geoffrey T. Struble; Barry A. Springer; Stuart L. Emanuel; Niranjan Pandey; Robert H. Gruninger; Mary Adams; Sandra Moreno-Mazza; Angel R. Fuentes-Pesquera; Steven A. Middleton
Members of a novel class of 4-amino-6-arylamino-pyrimidine-5-carbaldehyde hydrazones were identified as potent dual ErbB-2/EGFR kinase inhibitors using concept-guided design approach. These compounds inhibited the growth of ErbB-2 over-expressing human tumor cell lines (BT474, N87, and SK-BR-3) in vitro. Compound 15 emerged as a key lead and showed significant ability to inhibit growth factor-induced receptor phosphorylation in SK-BR-3 cells (IC(50)=54 nM) and cellular proliferation in vitro (IC(50)=14, 58, and 58 nM for BT474, N87, and SK-BR-3 respectively). The X-ray co-crystal structure of EGFR with a close analog (17) was determined and validated our design rationale.
Bioorganic & Medicinal Chemistry Letters | 2008
Guozhang Xu; Lily Lee Searle; Terry V. Hughes; Amanda K. Beck; Peter J. Connolly; Marta C. Abad; Michael P. Neeper; Geoffrey T. Struble; Barry A. Springer; Stuart L. Emanuel; Robert H. Gruninger; Niranjan Pandey; Mary Adams; Sandra Moreno-Mazza; Angel R. Fuentes-Pesquera; Steven A. Middleton; Lee M. Greenberger
We herein disclose a novel series of 4-aminopyrimidine-5-carbaldehyde oximes that are potent and selective inhibitors of both EGFR and ErbB-2 tyrosine kinases, with IC(50) values in the nanomolar range. Structure-activity relationship (SAR) studies elucidated a critical role for the 4-amino and C-6 arylamino moieties. The X-ray co-crystal structure of EGFR with 37 was determined and validated our design rationale.
Bioorganic & Medicinal Chemistry Letters | 2008
Kevin D. Kreutter; Tianbao Lu; Lily Lee; Edward C. Giardino; Sharmila Patel; Hui Huang; Guozhang Xu; Mark Fitzgerald; Barbara J. Haertlein; Venkatraman Mohan; Carl Crysler; Stephen H. Eisennagel; Malini Dasgupta; Martin McMillan; John C. Spurlino; Norman Huebert; Bruce E. Maryanoff; Bruce E. Tomczuk; Bruce P. Damiano; Mark R. Player
2-Cyano-6-fluorophenylacetamide was explored as a novel P2 scaffold in the design of thrombin inhibitors. Optimization around this structural motif culminated in 14, which is a potent thrombin inhibitor (K(i)=1.2nM) that exhibits robust efficacy in canine anticoagulation and thrombosis models upon oral administration.
Bioorganic & Medicinal Chemistry Letters | 2008
Terry V. Hughes; Guozhang Xu; Steven K. Wetter; Peter J. Connolly; Stuart L. Emanuel; Prabha Karnachi; Niranjan Pandey; Mary Adams; Sandra Moreno-Mazza; Steven A. Middleton; Lee M. Greenberger
A novel 5-[1,3,4-oxadiazol-2-yl]-N-aryl-4,6-pyrimidine diamine was synthesized and found to have potent dual EGFR/HER2 kinase inhibitory activity. The structure-based drug design of this molecule as well as the kinase and cellular inhibition of HER2 kinase dependent cell lines will be discussed.
Archive | 2008
Michael David Gaul; Alexander Kim; Lily Lee Searle; Raymond J. Patch; Dionisios Rentzeperis; Guozhang Xu; Xizhen Zhu
Bioorganic & Medicinal Chemistry Letters | 2006
Shenlin Huang; Ronghua Li; Peter J. Connolly; Guozhang Xu; Michael Gaul; Stuart L. Emanuel; Kenneth R. LaMontagne; Lee M. Greenberger
Bioorganic & Medicinal Chemistry Letters | 2007
Micheal D. Gaul; Guozhang Xu; Jennifer Kirkpatrick; Heidi Ott; Christian Andrew Baumann
Archive | 2004
Kevin D. Kreutter; Lily Lee; Tianbao Lu; Venkatraman Mohan; Sharmila Patel; Hui Huang; Guozhang Xu; Mark Fitzgerald
Archive | 2010
Gilles Bignan; Micheal D. Gaul; Guozhang Xu; Bao-Ping Zhao
Archive | 2012
Devraj Chakravarty; Kevin D. Kreutter; Mark T. Powell; Brian C. Shook; Fengbin Song; Guozhang Xu; Shyh-Ming Yang; Rui Zhang; Bao-Ping Zhao
