4.8 Article

A 5-fluorouracil-loaded polydioxanone weft-knitted stent for the treatment of colorectal cancer

Journal

BIOMATERIALS
Volume 34, Issue 37, Pages 9451-9461

Publisher

ELSEVIER SCI LTD
DOI: 10.1016/j.biomaterials.2013.08.055

Keywords

5-FU-loaded weft-knitted stents; Intestinal stenosis; Drug release; Anti-tumour effect; In vitro and in vivo

Funding

  1. Hong Kong Research Grant Council
  2. Hong Kong Polytechnic University [PolyU5242/09E]
  3. Guangdong Provincial Department of Science and Technology through the Guangdong-Hong Kong International Textile Bioengineering Joint Research Center [2011B090400586, 2012B091000143]

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In-stents restenosis caused by tumour ingrowth is a major problem for patients undergoing stent displacement because the conventional stents often lack a sustained anti-tumour capability. The aim of this paper was to develop a weft-knitted polydioxanone stent which can slow release 5-fluorouracil (5-FU). In order to determine the most suitable drug concentration, the 5-FU safe concentration in vivo and appropriate loading percentage in the membranes were investigated, and then 5-FU-loaded tide membranes at concentration of 3.2%, 6.4% and 12.8% were coated onto the stent using electrospinning method, respectively. The morphology, chemical structure and in vitro drug release property of the coating membranes were subsequently examined. Their anti-tumour activity and mechanism were assessed in vitro and in vivo using a human colorectal cancer cell line HCT-116 and tumour-bearing BALB/c nude mice. The half maximal inhibitory concentration (IC50) and the median lethal dose (LD50) demonstrated that the 6.4% and 12.8% membranes had better anti-tumour effects than pure 5-FU due to the sustainable drug releasing property of the coated membranes on the stent. The membranes possessing appropriate drug loading doses, such as 6.4% or 12.8% also provided better anti-in-stents restenosis effects than other groups tested. Therefore, it is concluded that the drug-loaded stents have great potential for the use in the treatment of intestinal cancers in the future. (C) 2013 Elsevier Ltd. All rights reserved.

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