Drug-Coated Balloon vs. Stent for Coronary Artery Disease: Authors Respond

Drug-Coated Balloon Angioplasty: Expanding ⁤Applications Beyond Small Vessels

The landscape of percutaneous coronary intervention (PCI) is continually evolving, with ⁣advancements aimed at minimizing stent-related complications and optimizing long-term outcomes. Among these innovations, drug-coated balloon (DCB) angioplasty has garnered significant attention ⁣as a compelling alternative to traditional stent-based procedures. Initially proposed by Scheller and colleagues in 2004,DCB technology has demonstrated efficacy in treating de novo small-vessel disease. However,a crucial debate persists: can⁤ the benefits of DCBs be consistently extended to larger,more complex coronary lesions? This article delves into‌ the current understanding of DCB angioplasty,exploring ⁤its mechanisms,established ⁣indications,emerging applications,and future directions,as of October 27,2025.

Understanding the Mechanism of Action

Unlike drug-eluting stents (DES), which provide a permanent metallic scaffold and sustained drug release, DCBs deliver a therapeutic agent ​directly to the ‌vessel wall during balloon inflation. This localized drug delivery aims to⁢ inhibit neointimal hyperplasia – ⁢the excessive growth of smooth muscle cells that can lead to restenosis (re-narrowing of the artery). the primary drugs utilized‌ in DCBs include paclitaxel ‍and​ sirolimus,both known for their anti-proliferative properties.

The process involves​ a balloon catheter⁣ coated with a drug-polymer ‍matrix. when ⁢inflated within the lesion, the balloon physically compresses the plaque, restoring blood flow, while simultaneously transferring the drug ⁤to the arterial wall. ​ Crucially, the absence of a stent eliminates‌ the risk‌ of stent thrombosis (blood clot formation within the stent) and⁤ late stent failure, complications associated with DES.However, this also means the vessel relies solely on the drug effect and the mechanical ‌benefit of the angioplasty to ‌maintain patency.

Established Indications for DCB Angioplasty

Current ⁢guidelines, supported by robust clinical evidence, primarily endorse DCB angioplasty for the treatment ‍of de novo (newly ⁤formed) small-vessel disease – typically defined as vessels with a diameter of 2.5 to 3.5 mm. Landmark trials, such ‌as the COMPARE II and ISAR-3 studies, demonstrated non-inferiority, and in some cases superiority, of DCBs compared to bare-metal stents (BMS) in this patient population.

These trials showed reduced rates of ⁤target lesion revascularization (TLR) – the need for repeat intervention⁣ – ​with DCBs, without an‍ increase in adverse events like myocardial infarction or stent thrombosis.Furthermore, DCBs have proven ⁤particularly valuable in patients with complex comorbidities, such as diabetes, where the ​risk of restenosis is elevated. A recent meta-analysis published in the ⁤ Journal of the American College of Cardiology ⁤ (September 2025) confirmed a consistent​ benefit of‍ DCBs in diabetic patients undergoing PCI ⁣for small vessel disease.

Expanding the Horizon: DCBs in Larger Vessels and Complex lesions

The central question driving current research is whether DCB angioplasty⁣ can be safely and effectively applied to larger vessels and more challenging lesion morphologies. Several factors contribute to this complexity. Larger vessels have a greater⁣ surface area requiring drug coverage,potentially⁣ leading to insufficient drug delivery. Moreover, ​lesions with significant⁢ calcium, long length, or severe stenosis may be less responsive to balloon angioplasty alone, necessitating a stent for⁤ adequate scaffolding.

However, emerging data suggest a potential role⁤ for DCBs in select cases. Studies are investigating ⁣the use of DCBs in:

* In-stent ​restenosis (ISR): DCBs have shown promise in treating restenosis within previously placed stents, offering a drug-eluting alternative to repeat