Zixia Feng
Novartis
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Publication
Featured researches published by Zixia Feng.
Tetrahedron Letters | 2000
Zixia Feng; Mark Hellberg
Abstract A novel class of prostaglandins containing a boronate in the α chain have been synthesized. The key steps in the synthesis were the preparation of the ylide containing the boronate and the subsequent Wittig reaction using the ylide.
Chemical Biology & Drug Design | 2016
Rajkumar V. Patil; Shouxi Xu; Alfred N. Van Hoek; Andrew Rusinko; Zixia Feng; Jesse A. May; Mark Hellberg; Najam A. Sharif; M. B. Wax; Macarena Irigoyen; Grant J. Carr; Tom Brittain; Peter M. Brown; Damon Colbert; S. Sindhu Kumari; K. Varadaraj; Alok K. Mitra
Aquaporins (AQPs) are a family of membrane proteins that function as channels facilitating water transport in response to osmotic gradients. These play critical roles in several normal physiological and pathological states and are targets for drug discovery. Selective inhibition of the AQP1 water channel may provide a new approach for the treatment of several disorders including ocular hypertension/glaucoma, congestive heart failure, brain swelling associated with a stroke, corneal and macular edema, pulmonary edema, and otic disorders such as hearing loss and vertigo. We developed a high‐throughput assay to screen a library of compounds as potential AQP1 modulators by monitoring the fluorescence dequenching of entrapped calcein in a confluent layer of AQP1‐overexpressing CHO cells that were exposed to a hypotonic shock. Promising candidates were tested in a Xenopus oocyte‐swelling assay, which confirmed the identification of two lead classes of compounds belonging to aromatic sulfonamides and dihydrobenzofurans with IC50s in the low micromolar range. These selected compounds directly inhibited water transport in AQP1‐enriched stripped erythrocyte ghosts and in proteoliposomes reconstituted with purified AQP1. Validation of these lead compounds, by the three independent assays, establishes a set of attractive AQP1 blockers for developing novel, small‐molecule functional modulators of human AQP1.
Bioorganic & Medicinal Chemistry | 2009
Zixia Feng; Mark R. Hellberg; Najam A. Sharif; Marsha A. McLaughlin; Gary W. Williams; Daniel Scott; Tony Wallace
FP-Class prostaglandin analogs have demonstrated utility for the treatment of glaucoma and ocular hypertension. A series of novel FP prostaglandin analogs was designed to optimize topical ocular activity and reduce ocular side-effects by replacing 13-carbon with oxygen. A facile synthesis was successfully developed for synthesis of the 13-oxa prostaglandins from the commercially available Corey aldehyde benzoate. Among the compounds synthesized, AL-16082 was the most potent prostaglandin FP agonist in vitro. In a prostaglandin FP receptor-linked second-messenger assay, phosphoinositide (PI) turnover, it exhibited a potency value (EC(50)) of 1.9 nM (78% max. response relative to fluprostenol). The isopropyl ester of AL-16082, compound AL-16049, significantly lowered intraocular pressure (IOP) in the ocular hypertensive monkey eyes by 30%. In the study of acute ocular irritation response in New Zealand albino rabbits, AL-16049 produced lower incidence of hyperemia, swelling, and discharge than PGF(2alpha) (1 microg), and a similar incidence of hyperemia, swelling, and discharge to latanoprost (1.8 microg). AL-16049 also produced no signs of ocular irritation or discomfort in the cat at the doses evaluated.
Archive | 1998
Abdelmoula Namil; Andrew Hoffman; Mark R. Hellberg; Thomas R. Dean; Zixia Feng; Hwang-Hsing Chen; Najam A. Sharif; Anura P. Dantanarayana
Archive | 2000
Jesse A. May; Zixia Feng
Bioorganic & Medicinal Chemistry Letters | 2007
Zixia Feng; Suchismita Mohapatra; Peter G. Klimko; Mark R. Hellberg; Jesse A. May; Curtis R. Kelly; Gary W. Williams; Marsha A. McLaughlin; Najam A. Sharif
Archive | 2002
Zixia Feng; Mark R. Hellberg
Archive | 2006
Mark R. Hellberg; Abdelmoula Namil; Zixia Feng; Jennifer Ward
Archive | 2007
Suchismita Mohapatra; Mark R. Hellberg; Zixia Feng
Archive | 2001
Zixia Feng; Mark R. Hellberg; Steven T. Miller