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基因靶向治疗缺血性心脏病和心力衰竭:转化和临床研究。

Gene targeting in ischemic heart disease and failure: translational and clinical studies.

机构信息

Division of Cardiothoracic Surgery, Medical University of South Carolina, SC, USA.

出版信息

Biochem Pharmacol. 2013 Jan 1;85(1):1-11. doi: 10.1016/j.bcp.2012.08.018. Epub 2012 Aug 28.

Abstract

Alternative and innovative targeted strategies hold relevance in improving the current treatments for ischemic heart disease (IHD). One potential treatment modality, gene targeting, may provide a unique alternative to current IHD therapies. The principal function of gene targeting in IHD is to augment the expression of an endogenous gene through amplification of an exogenous gene, delivered by a plasmid or a viral vector to enhance myocardial perfusion, and limit the long-term sequelae. The initial clinical studies of gene targeting in IHD were focused upon induction of angiogenic factors and the outcomes were equivocal. Nevertheless, significant advancements have been made in viral vectors, mode of delivery, and potentially relevant targets for IHD. Several of these advancements, particularly with a focus on translational large animal studies, are the focus of this review. The development of novel vectors with prolonged transduction efficiency and minimal inflammation, coupled with hybrid perfusion-mapping delivery devices, and improving the safety of vector use and efficacy of gene systems are but a few of the exciting progresses that are likely to proceed to clinical studies in the near future.

摘要

在改善缺血性心脏病 (IHD) 的当前治疗方法方面,替代和创新的靶向策略具有相关性。基因靶向作为一种潜在的治疗方式,可能为当前的 IHD 治疗提供独特的选择。基因靶向在 IHD 中的主要功能是通过质粒或病毒载体增强内源性基因的表达,从而增强心肌灌注并限制长期后遗症。最初的基因靶向治疗 IHD 的临床研究集中在诱导血管生成因子上,结果存在争议。然而,在病毒载体、给药方式以及与 IHD 相关的潜在靶点方面已经取得了重大进展。这些进展中的几个,特别是针对转化大型动物研究的进展,是本综述的重点。具有延长转导效率和最小炎症的新型载体的开发,结合混合灌注映射输送装置,以及提高载体使用的安全性和基因系统的疗效,只是在不久的将来可能进入临床研究的一些令人兴奋的进展。

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