Localized arterial wall drug delivery from a polymer-coated removable metallic stent. Kinetics, distribution, and bioactivity of forskolin. | Zendy

Thomas Lambert | Zendy; V. Dev | Zendy; Eldad Rechavia | Zendy; James S. Forrester | Zendy; Frank Litvack | Zendy; Neal Eigler | Zendy

Open Access

Localized arterial wall drug delivery from a polymer-coated removable metallic stent. Kinetics, distribution, and bioactivity of forskolin.

Author(s) -

Thomas Lambert,

V. Dev,

Eldad Rechavia,

James S. Forrester,

Frank Litvack,

Neal Eigler

Publication year - 1994

Publication title -

circulation

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 7.795

H-Index - 607

eISSN - 1524-4539

pISSN - 0009-7322

DOI - 10.1161/01.cir.90.2.1003

Subject(s) - forskolin , medicine , restenosis , blood flow , stent , cardiology , stimulation

Coronary stenting is associated with two major complications: subacute thrombosis and neointimal proliferation resulting in restenosis. Our hypothesis is that the biocompatibility of metallic stents can be improved by coating with a polymer membrane that delivers agents that favorably modify the local arterial microenvironment. This study evaluates the kinetics, distribution, and bioactivity of the model drug forskolin delivered to the local arterial wall by a polyurethane-coated removable metallic stent.

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