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Correction of hyperbilirubinemia in gunn rats by surgical delivery of low doses of helper-dependent adenoviral vectors

机译:低剂量辅助依赖型腺病毒载体的外科手术治疗对冈恩大鼠高胆红素血症的纠正

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Helper-dependent adenoviral (HDAd) vectors are attractive for liver-directed gene therapy because they can drive sustained high levels of transgene expression without chronic toxicity. However, high vector doses are required to achieve efficient hepatic transduction by systemic delivery because of a nonlinear dose response. Unfortunately, such high doses result in systemic vector dissemination and dose-dependent acute toxicity with potential lethal consequences. We have previously shown in nonhuman primates that delivery of HDAd in surgically isolated livers resulted in a significantly higher hepatic transduction with reduced systemic vector dissemination compared with intravenous delivery and multiyear transgene expression. Encouraged by these data, we have now employed a surgical vector delivery method in the Gunn rat, an animal model for Crigler-Najjar syndrome. After vector delivery into the surgically isolated liver, we show phenotypic correction at the low and clinically relevant vector dose of 1×1011 vp/kg. Correction of hyperbilirubinemia and increased glucuronidation of bilirubin in bile was achieved for up to 1 year after vector administration. Surgical delivery of the vector was well tolerated without signs of acute or chronic toxicity. This method of delivery could thereby be a safer alternative to liver transplantation for long-term treatment of Crigler-Najjar syndrome type I.
机译:辅助依赖型腺病毒(HDAd)载体对于肝定向基因治疗很有吸引力,因为它们可以驱动持续高水平的转基因表达而无慢性毒性。然而,由于非线性剂量响应,需要高载体剂量以通过全身递送实现有效的肝转导。不幸的是,如此高的剂量导致全身性载体传播和剂量依赖性急性毒性,并具有潜在的致命后果。先前我们在非人类灵长类动物中显示,与静脉内递送和多年转基因表达相比,HDAd在外科手术分离的肝脏中的递送导致肝脏转导显着更高,而系统载体的传播减少。受这些数据的鼓舞,我们现在在Gunn大鼠(一种Crigler-Najjar综合征的动物模型)中采用了外科载体输送方法。在将载体递送至手术分离的肝脏后,我们在低且临床相关的载体剂量1×1011 vp / kg下表现出表型校正。给予载体后长达一年的时间里,胆汁中高胆红素血症的纠正和胆红素的葡糖醛酸苷化增加。载体的手术递送耐受良好,没有急性或慢性毒性的迹象。因此,对于长期治疗I型Crigler-Najjar综合征,这种分娩方法可能是肝移植的更安全替代方案。

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