Gene Therapy Program, Department of Pathology and Laboratory Medicine, University of Pennsylvania, Philadelphia, Pennsylvania 19104, USA.
J Clin Invest. 2011 Jun;121(6):2427-35. doi: 10.1172/JCI57367. Epub 2011 May 16.
Vectors based on adeno-associated virus (AAV) serotype 9 are candidates for in vivo gene delivery to many organs, but the receptor(s) mediating these tropisms have yet to be defined. We evaluated AAV9 uptake by glycans with terminal sialic acids (SAs), a common mode of cellular entry for viruses. We found, however, that AAV9 binding increased when terminal SA was enzymatically removed, suggesting that galactose, which is the most commonly observed penultimate monosaccharide to SA, may mediate AAV9 transduction. This was confirmed in mutant CHO Pro-5 cells deficient in the enzymes involved in glycoprotein biogenesis, as well as lectin interference studies. Binding of AAV9 to glycans with terminal galactose was demonstrated via glycan binding assays. Co-instillation of AAV9 vector with neuraminidase into mouse lung resulted in exposure of terminal galactose on the apical surface of conducting airway epithelial cells, as shown by lectin binding and increased transduction of these cells, demonstrating the possible utility of this vector in lung-directed gene transfer. Increasing the abundance of the receptor on target cells and improving vector efficacy may improve delivery of AAV vectors to their therapeutic targets.
基于腺相关病毒(AAV)血清型 9 的载体是将基因递送至许多器官的体内的候选物,但介导这些趋向性的受体尚未确定。我们评估了末端唾液酸(SA)聚糖的 AAV9 摄取,这是病毒进入细胞的常见方式。然而,我们发现当末端 SA 被酶去除时,AAV9 结合增加,这表明最常见的 SA 前位单糖半乳糖可能介导 AAV9 的转导。在缺乏参与糖蛋白生物发生的酶的突变 CHO Pro-5 细胞以及凝集素干扰研究中证实了这一点。通过聚糖结合测定证明了 AAV9 与末端半乳糖的聚糖结合。将 AAV9 载体与神经氨酸酶共同注入小鼠肺中,导致气道上皮细胞的顶端表面暴露末端半乳糖,如凝集素结合和这些细胞的转导增加所示,证明了该载体在肺靶向基因转移中的可能用途。增加靶细胞上受体的丰度并提高载体效力可能会提高 AAV 载体递送至治疗靶标的效率。
