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采用基因治疗优化的基因递送方法靶向心脏。

Targeting the heart with gene therapy-optimized gene delivery methods.

作者信息

Müller Oliver J, Katus Hugo A, Bekeredjian Raffi

机构信息

Internal Medicine III, University of Heidelberg, Germany.

出版信息

Cardiovasc Res. 2007 Feb 1;73(3):453-62. doi: 10.1016/j.cardiores.2006.09.021. Epub 2006 Oct 3.

Abstract

With evolving knowledge in molecular and cellular cardiology, cardiac gene therapy has already been investigated in clinical studies. Different vector systems for cardiac gene therapy have been developed in recent years. While non-viral vectors, such as plasmid DNA, allow remarkable organ specificity, they are often limited by low transfection efficiency and transient gene expression. In contrast, adenoviral or adeno-associated virus-based vectors transfer the transgene more efficiently, but organ specificity may be reduced and immunogenic properties can limit their applicability. Using advanced transcriptional and transductional targeting strategies, viral vectors have been improved in the last few years. Recently, more efficient serotypes of adeno-associated viruses have been identified that show increased transduction rates, thus reducing the necessity for high virus titers. Combination with specific application techniques, such as intramyocardial injection, catheter-based perfusion, ultrasound targeted microbubble destruction, or retroinfusion may further enhance vector efficiency. This review article will give a broad overview of different gene delivery strategies that have been applied in experimental and clinical studies targeting the heart.

摘要

随着分子和细胞心脏病学知识的不断发展,心脏基因治疗已在临床研究中得到探索。近年来,已开发出用于心脏基因治疗的不同载体系统。虽然非病毒载体,如质粒DNA,具有显著的器官特异性,但它们往往受到转染效率低和基因表达短暂的限制。相比之下,基于腺病毒或腺相关病毒的载体能更有效地转移转基因,但器官特异性可能降低,免疫原性可能限制其适用性。在过去几年中,通过使用先进的转录和转导靶向策略,病毒载体得到了改进。最近,已鉴定出更有效的腺相关病毒血清型,其转导率有所提高,从而降低了对高病毒滴度的需求。与特定应用技术,如心肌内注射、基于导管的灌注、超声靶向微泡破坏或逆向灌注相结合,可能会进一步提高载体效率。本文将广泛概述已应用于针对心脏的实验和临床研究中的不同基因递送策略。

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