Enhanced Reendothelialization and Thrombosis Prevention with a New Drug-Eluting Stent.

Cardiovasc Drugs Ther

Departments of Surgery, University of Missouri School of Medicine, 1 Hospital Drive, Columbia, MO, 65212, USA.

Published: June 2024

AI Article Synopsis

  • - The study investigates the effects of cyclopentenyl cytosine (CPEC)-coated stents on preventing artery narrowing, encouraging blood vessel healing, and reducing blood clots.
  • - Researchers used advanced microscopy and drug release tests to evaluate the CPEC-coated stents against traditional everolimus-coated stents in lab settings and within animal models, finding CPEC stents led to less stenosis and promoted better healing.
  • - Results showed that CPEC-coated stents significantly lowered blood clot formation without requiring anticoagulant medications, suggesting they could improve treatment outcomes for cardiovascular diseases.

Article Abstract

Purpose: The objective of the study is to test the efficacy of cyclopentenyl cytosine (CPEC)-coated stents on blocking artery stenosis, promoting reendothelialization, and reducing thrombosis.

Methods: Scanning electron microscopy was employed to observe the morphological characteristics of stents coated with a mixture of CPEC and poly(lactic-co-glycolic acid) (PLGA) copolymer. PLGA has been used in various Food and Drug Administration (FDA)-approved therapeutic devices. In vitro release of CPEC was tested to measure the dynamic drug elution. Comparison between CPEC- and everolimus-coated stents on neointimal formation and thrombosis formation was conducted after being implanted into the human internal mammary artery and grafted to the mouse aorta.

Results: Optimization in stent coating resulted in uniform and consistent coating with minimal variation. In vitro drug release tests demonstrated a gradual and progressive discharge of CPEC. CPEC- or everolimus-coated stents caused much less stenosis than bare-metal stents. However, CPEC stent-implanted arteries exhibited enhanced reendothelialization compared to everolimus stents. Mechanistically, CPEC-coated stents reduced the proliferation of vascular smooth muscle cells while simultaneously promoting reendothelialization. More significantly, unlike everolimus-coated stents, CPEC-coated stents showed a significant reduction in thrombosis formation even in the absence of ongoing anticoagulant treatment.

Conclusions: The study establishes CPEC-coated stent as a promising new device for cardiovascular interventions. By enhancing reendothelialization and preventing thrombosis, CPEC offers advantages over conventional approaches, including the elimination of the need for anti-clogging drugs, which pave the way for improved therapeutic outcomes and management of atherosclerosis-related medical procedures.

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Source
http://dx.doi.org/10.1007/s10557-024-07584-yDOI Listing

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