Dongliang Zhuang
Amylin Pharmaceuticals
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Publication
Featured researches published by Dongliang Zhuang.
The Lancet | 2008
Daniel J. Drucker; John B. Buse; Kristin Taylor; David M. Kendall; Michael Trautmann; Dongliang Zhuang; Lisa Porter
BACKGROUND Exenatide is an incretin mimetic that shares glucoregulatory properties with glucagon-like peptide 1 (GLP-1), and improves glycaemic control, with progressive bodyweight reductions, when administered twice a day in patients with type 2 diabetes. We compared the efficacy of a once-weekly formulation of exenatide to that of a twice daily dose. METHODS A 30-week, randomised, non-inferiority study compared a long-acting release formulation of exenatide 2 mg administered once weekly to 10 mug exenatide administered twice a day, in 295 patients with type 2 diabetes (haemoglobin A(1c) [HbA(1c)] 8.3% [SD 1.0], mean fasting plasma glucose 9 [SD 2] mmol/L, weight 102 [SD 20] kg, diabetes duration 6.7 [SD 5.0] years). The patients were naive to drug therapy, or on one or more oral antidiabetic agents. The primary endpoint was the change in HbA(1c) at 30 weeks. This study is registered with ClinicalTrials.gov, number NCT00308139. FINDINGS At 30 weeks, the patients given exenatide once a week had significantly greater changes in HbA(1c) than those given exenatide twice a day (-1.9 [SE 0.1%] vs -1.5 [0.1%], 95% CI -0.54% to -0.12%; p=0.0023). A significantly greater proportion of patients receiving treatment once a week versus twice a day achieved target HbA(1c) levels of 7.0% or less (77%vs 61% of evaluable patients, p=0.0039). INTERPRETATION Exenatide once weekly resulted in significantly greater improvements in glycaemic control than exenatide given twice a day, with no increased risk of hypoglycaemia and similar reductions in bodyweight.
Diabetes, Obesity and Metabolism | 2017
Shawn E. McCandless; Jack A. Yanovski; Jennifer L. Miller; Cary Fu; Lynne M. Bird; Parisa Salehi; Christine L. Chan; Diane E. J. Stafford; M. Jennifer Abuzzahab; David H. Viskochil; Sarah E. Barlow; Moris Angulo; Susan E. Myers; Barbara Y. Whitman; Dennis M. Styne; Elizabeth Roof; Elisabeth M. Dykens; Ann O. Scheimann; Jaret Malloy; Dongliang Zhuang; Kristin Taylor; Thomas E. Hughes; Dennis Kim; Merlin G. Butler
There are no treatments for the extreme hyperphagia and obesity in Prader–Willi syndrome (PWS). The bestPWS clinical trial assessed the efficacy, safety and tolerability of the methionine aminopeptidase 2 (MetAP2) inhibitor, beloranib.
Diabetes, Obesity and Metabolism | 2018
Jaret Malloy; Dongliang Zhuang; Terri Kim; Phil Inskeep; Dennis Kim; Kristin Taylor
Methionine aminopeptidase 2 (MetAP2) inhibition has been shown to result in significant weight loss and improved glucose control. This Phase 1 clinical trial assessed the safety and tolerability, pharmacokinetics and preliminary efficacy of a novel MetAP2 inhibitor, ZGN‐1061.
Diabetes Care | 2005
David M. Kendall; Matthew C. Riddle; Julio Rosenstock; Dongliang Zhuang; Dennis Kim; Mark Fineman; Alain D. Baron
Diabetes Care | 2007
Dennis Kim; Leigh MacConell; Dongliang Zhuang; Prajakti A. Kothare; Michael Trautmann; Mark Fineman; Kristin Taylor
Diabetologie Und Stoffwechsel | 2008
Michael Trautmann; L MacConell; K Taylor; Dongliang Zhuang; Prajakti A. Kothare; Wi Li; Fineman
Diabetologia | 2018
Joseph Proietto; Jaret Malloy; Dongliang Zhuang; Mark Arya; Neale Cohen; Ferdinandus de Looze; Christopher Gilfillan; Paul Griffin; Stephen Hall; Thomas Nathow; Geoffrey S. Oldfield; David O’Neal; Adam Roberts; Bronwyn Stuckey; Dennis K. Yue; Kristin Taylor; Dennis Kim
Diabetes | 2018
Terri Kim; Dongliang Zhuang; Thomas Edward Hughes; Dennis Kim; Kristin Taylor
Diabetologie Und Stoffwechsel | 2010
T Kim; K Taylor; K Wilhelm; Michael Trautmann; Dongliang Zhuang; O Bachmann; Lisa Porter
Diabetologie Und Stoffwechsel | 2009
Christof M Kazda; Oliver P. Bachmann; John B. Buse; Daniel J. Drucker; Ken C. Taylor; Tae Wan Kim; Kay A. Wilhelm; David M. Kendall; Michael Trautmann; Dongliang Zhuang; Lisa Porter