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Dive into the research topics where Joan-En Chang-Lin is active.

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Featured researches published by Joan-En Chang-Lin.


Investigative Ophthalmology & Visual Science | 2011

Pharmacokinetics of a Sustained-Release Dexamethasone Intravitreal Implant in Vitrectomized and Nonvitrectomized Eyes

Joan-En Chang-Lin; James A. Burke; Qing Peng; Ton Lin; Werhner C. Orilla; C. Ghosn; Kai-Ming Zhang; Baruch D. Kuppermann; Michael R. Robinson; Scott M. Whitcup; Devin F. Welty

PURPOSE To evaluate dexamethasone pharmacokinetics after implantation of a sustained-release dexamethasone (DEX) intravitreal implant in nonvitrectomized and vitrectomized eyes. METHODS The right eyes of 25 rabbits underwent vitrectomy; contralateral eyes served as nonvitrectomy controls. The 0.7-mg DEX implant was injected into both eyes, and drug concentrations were determined in the vitreous humor and retina for 31 days (on days 2, 8, 15, 22, and 31). RESULTS DEX was present in nonvitrectomized and vitrectomized eyes for at least 31 days. There were no statistically significant differences in DEX concentration between nonvitrectomized and vitrectomized eyes at any time point (P > 0.05). The maximum concentration of DEX in nonvitrectomized versus vitrectomized eyes for vitreous humor was 791 ng/mL (day 22) versus 731 ng/mL (day 22), respectively, and for retina it was 4110 ng/mL (day 15) versus 3670 ng/mL (day 22), respectively. Mean absorption (AUC(0-tlast)) of dexamethasone in nonvitrectomized and vitrectomized eyes was not different for both the vitreous humor (13,600 vs. 15,000 ng/day/mL; P = 0.73) and retina (67,600 vs. 50,200 ng/day/mL; P = 0.47). CONCLUSIONS The vitreoretinal pharmacokinetic profiles were similar between nonvitrectomized and vitrectomized eyes. These observations are consistent with clinical findings of the DEX implant in patients who have undergone vitrectomy and should reduce concerns about the use of the DEX implant in eyes that have undergone vitrectomy.


Advanced Drug Delivery Reviews | 2005

Topical and systemic drug delivery to the posterior segments

Patrick M. Hughes; Orest Olejnik; Joan-En Chang-Lin; Clive G. Wilson


Archive | 2006

Methods for treating ocular conditions with cyclic lipid contraining microparticles

Patrick M. Hughes; Joan-En Chang-Lin; Devin F. Welty


Archive | 2008

Sustained release intraocular implants containing tyrosine kinase inhibitors and related methods

Patrick M. Hughes; Thomas C. Malone; Gerald W. De Vries; Jeffrey L. Edelman; Joan-En Chang-Lin; Jane Guo Shiah; Thierry Nivaggioli


Archive | 2006

Compositions and methods for the intraocular transport of therapeutic agents

Patrick M. Hughes; Orest Olejnik; Joan-En Chang-Lin


Archive | 2007

Method for determining optimum intraocular locations for drug delivery systems

Michael R. Robinson; Joan-En Chang-Lin; Devin F. Welty; Scott M. Whitcup; Patrick M. Hughes


Archive | 2007

Ocular therapy using alpha-2 adrenergic receptor anterior compounds having enhanced clearance rates

Patrick M. Hughes; James A. Burke; Joan-En Chang-Lin


Archive | 2006

Ocular therapy using alpha-2 adrenergic receptor compounds having enhanced anterior clearance rates

Patrick M. Hughes; James A. Burke; Joan-En Chang-Lin


Archive | 2005

Retinoid-containing sustained release intraocular drug delivery system and related methods

Patrick M. Hughes; Orest Olejnik; Glenn T. Huang; Joan-En Chang-Lin; Thierry Nivaggioli; Jane-Guo Shiah; Michele Boix; Christian Sarrazin


Archive | 2005

Biodegradable intravitreal tyrosine kinase implants

Jeffrey L. Edelman; Patrick M. Hughes; Thomas C. Malone; Gerald W. Devries; Joan-En Chang-Lin; Jane Guo Shiah; Thierry Nivaggioli; Lon T. Spada; Wendy M. Blanda

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