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Stent-based delivery of adeno-associated viral vectors with sustained vascular transduction and iNOS-mediated inhibition of in-stent restenosis

机译:腺相关病毒载体的基于支架的递送具有持续的血管转导和iNOS介导的支架内再狭窄抑制

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摘要

In-stent restenosis remains an important clinical problem in the era of drug eluting stents. Development of clinical gene therapy protocols for the prevention and treatment of in-stent restenosis is hampered by the lack of adequate local delivery systems. Herein we describe a novel stent-based gene delivery platform capable of providing local arterial gene transfer with adeno-associated viral (AAV) vectors. This system exploits the natural affinity of protein G (PrG) to bind to the Fc region of mammalian IgG, making PrG a universal adaptor for surface immobilization of vector-capturing antibodies (Ab). Our results: 1) demonstrate the feasibility of reversible immobilization of AAV2 vectors using vector tethering by AAV2-specific Ab appended to the stent surface through covalently attached PrG, 2) show sustained release kinetics of PrG/Ab-immobilized AAV2 vector particles into simulated physiological medium in vitro and site-specific transduction of cultured cells, 3) provide evidence of long-term (12 weeks) arterial expression of luciferase with PrG/Ab-tethered AAV2Luc, and 4) show anti-proliferative activity and anti-restenotic efficacy of stent-immobilized AAV2iNOS in the rat carotid artery model of stent angioplasty.
机译:支架内再狭窄仍然是药物洗脱支架时代的重要临床问题。缺乏适当的局部递送系统阻碍了预防和治疗支架内再狭窄的临床基因治疗方案的开发。在这里,我们描述了一种新型的基于支架的基因传递平台,该平台能够提供与腺相关病毒(AAV)载体的局部动脉基因转移。该系统利用蛋白G(PrG)的天然亲和力与哺乳动物IgG的Fc区结合,从而使PrG成为载体捕获抗体(Ab)表面固定的通用适配器。我们的结果:1)证明了通过通过共价连接的PrG附加到支架表面的AAV2特异性抗体进行载体束缚,可逆地固定AAV2载体的可行性,2)显示了固定化PrG / Ab的AAV2矢量颗粒在模拟生理学中的持续释放动力学3)提供长期(12周)荧光素酶与PrG / Ab相连的AAV2Luc的动脉表达的证据,以及4)显示抗增殖活性和抗再狭窄功效支架血管成形术的大鼠颈动脉模型中固定有支架的AAV2iNOS。

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