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Featured researches published by Yong-Liang Zhu.


Proceedings of the National Academy of Sciences of the United States of America | 2008

Discovery of a selective inhibitor of oncogenic B-Raf kinase with potent antimelanoma activity.

James H. Tsai; John T. Lee; Weiru Wang; Jiazhong Zhang; Hanna Cho; Shumeye Mamo; Ryan Bremer; Sam Gillette; Jun Kong; Nikolas K. Haass; Katrin Sproesser; Ling Li; Keiran S.M. Smalley; Daniel Fong; Yong-Liang Zhu; Adhirai Marimuthu; Hoa Nguyen; Billy Lam; Jennifer Liu; Ivana Cheung; Julie Rice; Yoshihisa Suzuki; Catherine Luu; Calvin Settachatgul; Rafe Shellooe; John Cantwell; Sung-Hou Kim; Joseph Schlessinger; Kam Y. J. Zhang; Brian L. West

BRAFV600E is the most frequent oncogenic protein kinase mutation known. Furthermore, inhibitors targeting “active” protein kinases have demonstrated significant utility in the therapeutic repertoire against cancer. Therefore, we pursued the development of specific kinase inhibitors targeting B-Raf, and the V600E allele in particular. By using a structure-guided discovery approach, a potent and selective inhibitor of active B-Raf has been discovered. PLX4720, a 7-azaindole derivative that inhibits B-RafV600E with an IC50 of 13 nM, defines a class of kinase inhibitor with marked selectivity in both biochemical and cellular assays. PLX4720 preferentially inhibits the active B-RafV600E kinase compared with a broad spectrum of other kinases, and potent cytotoxic effects are also exclusive to cells bearing the V600E allele. Consistent with the high degree of selectivity, ERK phosphorylation is potently inhibited by PLX4720 in B-RafV600E-bearing tumor cell lines but not in cells lacking oncogenic B-Raf. In melanoma models, PLX4720 induces cell cycle arrest and apoptosis exclusively in B-RafV600E-positive cells. In B-RafV600E-dependent tumor xenograft models, orally dosed PLX4720 causes significant tumor growth delays, including tumor regressions, without evidence of toxicity. The work described here represents the entire discovery process, from initial identification through structural and biological studies in animal models to a promising therapeutic for testing in cancer patients bearing B-RafV600E-driven tumors.


Journal of Chemical Information and Modeling | 2014

Including explicit water molecules as part of the protein structure in MM/PBSA calculations.

Yong-Liang Zhu; Paul Beroza; Dean R. Artis

Water is the natural medium of molecules in the cell and plays an important role in protein structure, function and interaction with small molecule ligands. However, the widely used molecular mechanics Poisson-Boltzmann surface area (MM/PBSA) method for binding energy calculation does not explicitly take account of water molecules that mediate key protein-ligand interactions. We have developed a protocol to include water molecules that mediate ligand-protein interactions as part of the protein structure in calculation of MM/PBSA binding energies (a method we refer to as water-MM/PBSA) for a series of JNK3 kinase inhibitors. Improved correlation between water-MM/PBSA binding energies and experimental IC50 values was obtained compared to that obtained from classical MM/PBSA binding energy. This improved correlation was further validated using sets of neuraminidase and avidin inhibitors. The observed improvement, however, appears to be limited to systems in which there are water-mediated ligand-protein hydrogen bond interactions. We conclude that the water-MM/PBSA method performs better than classical MM/PBSA in predicting binding affinities when water molecules play a direct role in mediating ligand-protein hydrogen bond interactions.


Archive | 2006

Pyrrolo [2, 3-b] pyridine derivatives as protein kinase inhibitors

Prabha N. Ibrahim; Dean R. Artis; Ryan Bremer; Gaston Habets; Shumeye Mamo; Marika Nespi; Chao Zhang; Jiazhong Zhang; Yong-Liang Zhu; Rebecca Zuckerman; Brian L. West; Yoshihisa Suzuki; James H. Tsai; Klaus-Peter Hirth; Gideon Bollag; Wayne Spevak; Hanna Cho; Samuel J. Gillette; Guoxian Wu; Hongyao Zhu; Shenghua Shi


Archive | 2004

Compounds and methods for development of Ret modulators

Prabha N. Ibrahim; Dean R. Artis; Ryan Bremer; Gaston Habets; Clarence R. Hurt; Shumeye Mamo; Marika Nespi; Chao Zhang; Jiazhong Zhang; Yong-Liang Zhu; Rebecca Zuckerman; Heike Krupka; Abhinav Kumar; Brian L. West


Archive | 2007

INHIBITORS OF POLO-LIKE KINASE

Robert A. Galemmo; Dean R. Artis; Xiaocong Michael Ye; Danielle L. Aubele; Anh P. Truong; Simeon Bowers; Yong-Liang Zhu; Jeffrey R. Neitz; Jennifer Sealy; Marc Adler; Paul Beroza; John P. Anderson


Archive | 2010

Pteridinones as inhibitors of polo-like kinase

Robert A. Galemmo; Dean R. Artis; Xiaocong Michael Ye; Danielle L. Aubele; Anh P. Truong; Simeon Bowers; Yong-Liang Zhu; R. Jeffrey Neitz; Jennifer Sealy; Marc Adler; Paul Beroza; John P. Anderson


Archive | 2010

Compounds and methods for inhibition of renin, and indications therefor

Guoxian Wu; Prabha N. Ibrahim; Yong Zhou; Shumeye Mamo; Samuel J. Gillette; Yong-Liang Zhu; Jinyu Liu; Chao Zhang; Kam Y. J. Zhang; Dean R. Artis


Archive | 2017

composto, composição farmacêutica, método para o tratamento de uma doença neurodegenerativa, método para reduzir a concentração de p-ser-alfa-sinucleina em tecido cerebral, e, método para o tratamento de um câncer

Anh P. Truong; Danielle L. Aubele; Dean R. Artis; Jennifer Sealy; John P. Anderson; Marc Adler; Paul Beroza; R. Jeffrey Neitz; Robert A. Galemmo; Simeon Bowers; Xiaocong Michael Ye; Yong-Liang Zhu


Archive | 2010

Ptéridinones en tant qu'inhibiteurs de polo-like kinase

Robert A. Galemmo; Dean R. Artis; Xiaocong Michael Ye; Danielle L. Aubele; Anh P. Truong; Simeon Bowers; Yong-Liang Zhu; R. Jeffrey Neitz; Jennifer Sealy; Marc Adler; Paul Beroza; John P. Anderson


Archive | 2010

Composés et procédés pour inhiber la rénine, et indications associées

Guoxian Wu; Prabha N. Ibrahim; Yong Zhou; Shumeye Mamo; Samuel J. Gillette; Yong-Liang Zhu; Jinyu Liu; Chao Zhang; Kam Y. J. Zhang; Dean R. Artis

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