4.1 Article

A Novel Antiproliferative Drug Coating for Glaucoma Drainage Devices

期刊

JOURNAL OF GLAUCOMA
卷 23, 期 8, 页码 526-534

出版社

LIPPINCOTT WILLIAMS & WILKINS
DOI: 10.1097/IJG.0b013e318294869b

关键词

glaucoma surgery; wound healing; biodegradable polymer; mitomycin C; 5-fluorouracil

资金

  1. Louisiana Board of Regents [LEQSF(2010-12)-RD-B-05]
  2. Department of Defense [W81XWH-10-1-0377]

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Purpose: The implantation of a glaucoma drainage device (GDD) is often necessary for intractable cases of glaucoma. Currently, the success rate of GDD implants is relatively low because fibrosis that develops during the wound-healing process ultimately blocks fluid drainage. We describe herein a novel porous coating for Ahmed glaucoma valves based on biodegradable poly(lactic-co-glycolic acid) (PLGA). Materials and Methods: Thin films of PLGA were fabricated using a spin-coating technique. The procedure led to an asymmetric pore structure that was exploited to control the rate of dissolution. Double-layered porous films were constructed to achieve continuous drug release. A cell culture system was used to test the efficacy of these coatings. Results: Double-layered films were manufactured to provide a burst of mitomycin C (MMC) release followed by a slow release of 5-fluorouracil (5-FU), which together prevented fibrosis over the most active period of postoperative wound healing (0 to 28 d). Double-layered films containing 5-FU only in the bottom layer showed a 3- to 5-day delay in drug release, followed by a sharp increase that continued for (similar to)28 days. MMC was stable only when surface-loaded, and this drug was therefore surface-loaded onto the top PLGA layer to provide a continuous release of antifibrotics over the wound-healing period. Conclusions: The combined use of both MMC and 5-FU in a biodegradable device inhibits cell proliferation in a tissue culture model and has the potential to reduce fibrosis and increase the success rate of GDD implants. The design is simple and can be scaled for commercial production.

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