Chihyuan Chuang
University of California, San Francisco
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Publication
Featured researches published by Chihyuan Chuang.
British Journal of Haematology | 2016
Donna Oksenberg; Kobina Dufu; Mira Patel; Chihyuan Chuang; Zhe Li; Qing Xu; Abel Silva-Garcia; Chengjing Zhou; Athiwat Hutchaleelaha; Larysa N. Patskovska; Yury Patskovsky; Steven C. Almo; Uma Sinha; Brian Metcalf; David R. Archer
A major driver of the pathophysiology of sickle cell disease (SCD) is polymerization of deoxygenated haemoglobin S (HbS), which leads to sickling and destruction of red blood cells (RBCs) and end‐organ damage. Pharmacologically increasing the proportion of oxygenated HbS in RBCs may inhibit polymerization, prevent sickling and provide long term disease modification. We report that GBT440, a small molecule which binds to the N‐terminal α chain of Hb, increases HbS affinity for oxygen, delays in vitro HbS polymerization and prevents sickling of RBCs. Moreover, in a murine model of SCD, GBT440 extends the half‐life of RBCs, reduces reticulocyte counts and prevents ex vivo RBC sickling. Importantly, oral dosing of GBT440 in animals demonstrates suitability for once daily dosing in humans and a highly selective partitioning into RBCs, which is a key therapeutic safety attribute. Thus, GBT440 has the potential for clinical use as a disease‐modifying agent in sickle cell patients.
ACS Medicinal Chemistry Letters | 2017
Brian Metcalf; Chihyuan Chuang; Kobina Dufu; Mira Patel; Abel Silva-Garcia; Carl Johnson; Qing Lu; James R. Partridge; Larysa N. Patskovska; Yury Patskovsky; Steven C. Almo; Matthew P. Jacobson; Lan Hua; Qing Xu; Stephen L Gwaltney; Calvin Yee; Jason R. Harris; Bradley P. Morgan; Joyce James; Donghong Xu; Athiwat Hutchaleelaha; Kumar Paulvannan; Donna Oksenberg; Zhe Li
We report the discovery of a new potent allosteric effector of sickle cell hemoglobin, GBT440 (36), that increases the affinity of hemoglobin for oxygen and consequently inhibits its polymerization when subjected to hypoxic conditions. Unlike earlier allosteric activators that bind covalently to hemoglobin in a 2:1 stoichiometry, 36 binds with a 1:1 stoichiometry. Compound 36 is orally bioavailable and partitions highly and favorably into the red blood cell with a RBC/plasma ratio of ∼150. This partitioning onto the target protein is anticipated to allow therapeutic concentrations to be achieved in the red blood cell at low plasma concentrations. GBT440 (36) is in Phase 3 clinical trials for the treatment of sickle cell disease (NCT03036813).
Archive | 2011
Zhe Yang; Alex Muci; Jeffrey Warrington; Gustave Bergnes; Bradley P. Morgan; Chihyuan Chuang; Antonio Romero; Scott Collibee; Xiangping Qian; Pu-Ping Lu
Archive | 2011
Luke W. Ashcraft; Gustave Bergnes; Scott Collibee; Chihyuan Chuang; Jeff Gardina; Bradley P. Morgan; Alex Muci; Xiangping Qian; Jeffrey Warrington; Zhe Yang; Pu-Ping Lu; Antonio Romero
Archive | 2012
Brian Metcalf; Chihyuan Chuang; Jeffrey Warrington; Kumar Paulvannan; Matthew P. Jacobson; Lan Hua; Bradley Morgan
Archive | 2011
Luke W. Ashcraft; Gustave Bergnes; Scott Collibee; Chihyuan Chuang; Jeff Gardina; Bradley P. Morgan; Alex Muci; Xiangping Qian; Antonio Romero; Jeffrey Warrington; Zhe Yang
Archive | 2012
Luke W. Ashcraft; Gustave Bergnes; Chihyuan Chuang; Scott Collibee; Pu-Ping Lu; Bradley P. Morgan; Alex Muci; Xiangping Qian; Jeffrey Warrington; Zhe Yang
Archive | 2011
Luke W. Ashcraft; Gustave Bergnes; Scott Collibee; Chihyuan Chuang; Jeff Gardina; Bradley P. Morgan; Alex Muci; Xiangping Qian; Jeffrey Warrington; Zhe Yang; Pu-Ping Lu; Antonio Romero
american thoracic society international conference | 2010
Zhiheng Jia; Guillermo Godinez; Nickie Durham; Xi Wang; Chihyuan Chuang; Pu-Ping Lu; Wenyue Wang; Bing Yao; Jeffrey Warrington; James J. Hartman; David J. Morgans; Bradley P. Morgan; Xiangping Qian; Fady Malik; Malar Pannirselvam
Archive | 2016
Luke W. Ashcraft; Bergnes Gustave; Scott Collibee; Chihyuan Chuang; Jeff Gardina; Morgan Bradley P; Alex Muci; Qian Xiangping; Jeffrey Warrington; Yang Zhe; Lu Pu-Ping; Antonio Romero