Inagaki Katsuya, Fuess Sally, Storm Theresa A, Gibson Gregory A, Mctiernan Charles F, Kay Mark A, Nakai Hiroyuki
Department of Molecular Genetics & Biochemistry, University of Pittsburgh School of Medicine, Pittsburgh, PA 15261, USA.
Mol Ther. 2006 Jul;14(1):45-53. doi: 10.1016/j.ymthe.2006.03.014. Epub 2006 May 19.
It has been recently shown that recombinant adeno-associated virus serotype 8 (rAAV8) is a robust alternative serotype vector that overcomes many of the limitations of rAAV2 and transduces various tissues efficiently and globally through systemic vector administration. AAV9 is a serotype newly isolated from human tissues, but our knowledge of the biology of rAAV9 in vivo is currently limited. Here, we demonstrate by a series of comprehensive side-by-side experiments with rAAV8 and 9 vectors delivered via different routes or at various doses in mice that rAAV9 vectors share the robustness of rAAV8, i.e., (1) very high liver transduction efficiency irrespective of whether vectors are administered intravascularly or extravascularly and (2) substantial transduction in the heart, skeletal muscle, and pancreas by peripheral vein injection. Importantly, rAAV9 transduced myocardium 5- to 10-fold higher than rAAV8, resulting in over 80% cardiomyocyte transduction following tail vein injection of as low as 1.0 x 10(11) particles per mouse. Thus rAAV9, as well as rAAV8, is a robust vector for gene therapy applications and rAAV9 is superior to rAAV8 specifically for cardiac gene delivery by systemic vector administration.
最近的研究表明,重组腺相关病毒8型(rAAV8)是一种强大的替代血清型载体,它克服了rAAV2的许多局限性,并通过全身载体给药有效地、广泛地转导各种组织。AAV9是一种新从人类组织中分离出的血清型,但我们目前对rAAV9体内生物学特性的了解有限。在这里,我们通过一系列全面的并行实验,在小鼠中以不同途径或不同剂量递送rAAV8和9载体,证明rAAV9载体具有与rAAV8相同的强大功能,即:(1)无论载体是通过血管内还是血管外给药,肝脏转导效率都非常高;(2)通过外周静脉注射,心脏、骨骼肌和胰腺中有大量转导。重要的是,rAAV9对心肌的转导比rAAV8高5至10倍,在每只小鼠尾静脉注射低至1.0×10¹¹个颗粒后,心肌细胞转导率超过80%。因此,rAAV9以及rAAV8都是用于基因治疗的强大载体,并且rAAV9在通过全身载体给药进行心脏基因递送方面特别优于rAAV8。
