Mattar Citra N Z, Gil-Farina Irene, Rosales Cecilia, Johana Nuryanti, Tan Yvonne Yi Wan, McIntosh Jenny, Kaeppel Christine, Waddington Simon N, Biswas Arijit, Choolani Mahesh, Schmidt Manfred, Nathwani Amit C, Chan Jerry K Y
Obstetrics & Gynaecology, Yong Loo Lin School of Medicine, National University of Singapore, Singapore 119077, Singapore.
Department of Translational Oncology, German Cancer Research Center and National Center for Tumor Diseases, 69120 Heidelberg, Germany.
Mol Ther. 2017 Aug 2;25(8):1843-1853. doi: 10.1016/j.ymthe.2017.04.003. Epub 2017 Apr 24.
The safe correction of an inherited bleeding disorder in utero prior to the onset of organ damage is highly desirable. Here, we report long-term transgene expression over more than 6 years without toxicity following a single intrauterine gene transfer (IUGT) at 0.9G using recombinant adeno-associated vector (AAV)-human factor IX (hFIX) in the non-human primate model we have previously described. Four of six treated animals monitored for around 74 months expressed hFIX at therapeutic levels (3.9%-120.0%). Long-term expression was 6-fold higher in males and with AAV8 compared to AAV5, mediated almost completely at this stage by random genome-wide hepatic proviral integrations, with no evidence of hotspots. Post-natal AAV challenge without immunosuppression was evaluated in two animals exhibiting chronic low transgene expression. The brief neutralizing immune reaction elicited had no adverse effect and, although expression was not improved at the dose administered, no clinical toxicity was observed. This long-term surveillance thus confirms the safety of late-gestation AAV-hFIX transfer and demonstrates that postnatal re-administration can be performed without immunosuppression, although it requires dose optimization for the desired expression. Nevertheless, eventual vector genotoxicity and the possibility of germline transmission will require lifelong monitoring and further evaluation of the reproductive function of treated animals.
在器官损伤发生之前对子宫内的遗传性出血性疾病进行安全矫正非常必要。在此,我们报告了在我们之前描述的非人灵长类动物模型中,使用重组腺相关病毒(AAV)-人凝血因子IX(hFIX)以0.9G进行单次子宫内基因转移(IUGT)后,超过6年的长期转基因表达且无毒性。在监测约74个月的6只接受治疗的动物中,有4只以治疗水平(3.9%-120.0%)表达hFIX。与AAV5相比,雄性动物以及使用AAV8时的长期表达高出6倍,现阶段几乎完全由全基因组随机肝脏前病毒整合介导,且无热点证据。在两只慢性低转基因表达的动物中评估了无免疫抑制情况下的产后AAV挑战。引发的短暂中和免疫反应没有不良影响,尽管在所给予的剂量下表达没有改善,但未观察到临床毒性。因此,这种长期监测证实了妊娠晚期AAV-hFIX转移的安全性,并表明产后重新给药可以在无免疫抑制的情况下进行,尽管需要对所需表达进行剂量优化。然而,最终的载体基因毒性和种系传播的可能性将需要对治疗动物的生殖功能进行终身监测和进一步评估。
