Drug Delivery (Dec 2022)

Microchannel-embedded implantable device with fibrosis suppression for prolonged controlled drug delivery

  • Han Bi Ji,
  • Jae Young Hong,
  • Cho Rim Kim,
  • Chang Hee Min,
  • Jae Hoon Han,
  • Min Ji Kim,
  • Se-Na Kim,
  • Cheol Lee,
  • Young Bin Choy

DOI
https://doi.org/10.1080/10717544.2022.2032873
Journal volume & issue
Vol. 29, no. 1
pp. 489 – 498

Abstract

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For the prolonged, controlled delivery of systemic drugs, we propose an implantable drug-delivery chip (DDC) embedded with pairs of a microchannel and drug-reservoir serving as a drug diffusion barrier and depot, respectively. We pursued a DDC for dual drugs: a main-purpose drug, diclofenac (DF), for systemic exposure, and an antifibrotic drug, tranilast (TR), for local delivery. Thus, the problematic fibrotic tissue formation around the implanted device could be diminished, thereby less hindrance in systemic exposure of DF released from the DDC. First, we separately prepared DDCs for DF or TR delivery, and sought to find a proper microchannel length for a rapid onset and sustained pattern of drug release, as well as the required drug dose. Then, two distinct DDCs for DF and TR delivery, respectively, were assembled to produce a Dual_DDC for the concurrent delivery of DF and TR. When the Dual_DDC was implanted in living rats, the DF concentration in blood plasma did not drop significantly in the later periods after implantation relative to that in the early periods before fibrotic tissue formation. When the Dual_DDC was implanted without TR, there was a significant decrease in the blood plasma DF concentration as the time elapsed after implantation. Biopsied tissues around the Dual_DDC exhibited a significant decrease in the fibrotic capsule thickness and collagen density relative to the Dual_DDC without TR, owing to the effect of the local, sustained release of the TR.

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