Inhibition of human in-stent restenosis: a molecular view

Abstract

The current management of the stenosis of the coronary arteries relies on the insertion of a metal mesh tube, namely stent, into the obstructed vessel. Coronary stents have been envisaged to reduce the restenosis after balloon angioplasty. Nonetheless, one of the major complications after successful revascularization is the late in-stent restenosis. Such lesion consists mainly of inflammatory reaction and neointima formation as a consequence of the mechanical injury of the vessel. In this review, we examine the molecular players underlying the in-stent restenosis, with particular reference to the role of the mTOR pathway and the intracellular receptor immunophilins. The 'limus' based drugs, which are developed or are under development in drug-eluting stent technology, will be also discussed.