基因转移作为实现永久性心脏保护的策略 I:AAV 介导的诱导型一氧化氮合酶基因治疗可在 1 年后限制梗死面积,而无不良功能后果。
Gene transfer as a strategy to achieve permanent cardioprotection I: rAAV-mediated gene therapy with inducible nitric oxide synthase limits infarct size 1 year later without adverse functional consequences.
机构信息
Division of Cardiovascular Medicine, Institute of Molecular Cardiology, University of Louisville, 550 S Jackson Street, Louisville, KY 40292, USA.
出版信息
Basic Res Cardiol. 2011 Nov;106(6):1355-66. doi: 10.1007/s00395-011-0207-7. Epub 2011 Jul 21.
The ultimate goal of prophylactic gene therapy is to confer permanent protection against ischemia. Although gene therapy with inducible nitric oxide synthase (iNOS) is known to protect against myocardial infarction at 3 days and up to 2 months, the long-term effects on myocardial ischemic injury and function are unknown. To address this issue, we created a recombinant adeno-associated viral vector carrying the iNOS gene (rAAV/iNOS), which enables long-lasting transgene expression. The ability of rAAV/iNOS to direct the expression of functional iNOS protein was confirmed in COS-7 cells before in vivo gene transfer. Mice received injections in the anterior LV wall of rAAV/LacZ or rAAV/iNOS; 1 year later, they underwent a 30-min coronary occlusion (O) and 4 h of reperfusion (R). iNOS gene transfer resulted in elevated iNOS protein expression (+3-fold vs. the LacZ group, n = 6; P < 0.05) and iNOS activity (+4.4-fold vs. the LacZ group, n = 6; P < 0.05) 1 year later. Infarct size (% of risk region) was dramatically reduced at 1 year after iNOS gene transfer (13.5 ± 2.2%, n = 12, vs. 41.7 ± 2.9%, n = 10, in the LacZ group; P < 0.05). The infarct-sparing effect of iNOS gene therapy at 1 year was as powerful as that observed 24 h after ischemic preconditioning (six 4-min O/4-min R cycles) (19.3 ± 2.3%, n = 11; P < 0.05). Importantly, compared with the LacZ group (n = 11), iNOS gene transfer (n = 10) had no effect on LV dimensions or function for up to 1 year (at 1 year: FS 34.5 ± 2.0 vs. 34.6 ± 2.6%, EF 57.0 ± 2.0 vs. 59.7 ± 2.9%, LVEDD 4.3 ± 0.1 vs. 4.2 ± 0.2 mm, LVESD 2.8 ± 0.1 vs. 2.9 ± 0.2 mm) (echocardiography). These data demonstrate, for the first time, that rAAV-mediated iNOS gene transfer affords long-term, probably permanent (1 year), cardioprotection without adverse functional consequences, providing a strong rationale for further preclinical testing of prophylactic gene therapy.
基因治疗的最终目标是提供对缺血的永久性保护。虽然诱导型一氧化氮合酶(iNOS)的基因治疗已知在 3 天和长达 2 个月内可预防心肌梗死,但对心肌缺血性损伤和功能的长期影响尚不清楚。为了解决这个问题,我们创建了携带 iNOS 基因的重组腺相关病毒载体(rAAV/iNOS),它可以实现长期的转基因表达。在体内基因转移之前,rAAV/iNOS 能够在 COS-7 细胞中指导功能性 iNOS 蛋白的表达,这一点已经得到了证实。在 LV 前壁注射 rAAV/LacZ 或 rAAV/iNOS;1 年后,它们接受 30 分钟的冠状动脉闭塞(O)和 4 小时的再灌注(R)。1 年后,iNOS 基因转移导致 iNOS 蛋白表达增加(与 LacZ 组相比增加 3 倍,n=6;P<0.05)和 iNOS 活性增加(与 LacZ 组相比增加 4.4 倍,n=6;P<0.05)。1 年后,iNOS 基因转移可显著减少梗死面积(占危险区域的百分比)(与 LacZ 组相比,n=12,为 13.5±2.2%;n=10,为 41.7±2.9%;P<0.05)。1 年后 iNOS 基因治疗的梗死保护作用与缺血预处理后 24 小时观察到的作用一样强大(6 个 4 分钟 O/4 分钟 R 循环)(n=11,19.3±2.3%;P<0.05)。重要的是,与 LacZ 组(n=11)相比,iNOS 基因转移(n=10)在 1 年内对 LV 尺寸或功能没有影响(1 年后:FS 34.5±2.0%与 34.6±2.6%,EF 57.0±2.0%与 59.7±2.9%,LVEDD 4.3±0.1mm 与 4.2±0.2mm,LVESD 2.8±0.1mm 与 2.9±0.2mm)(超声心动图)。这些数据首次表明,rAAV 介导的 iNOS 基因转移可提供长期、可能是永久性的(1 年)心脏保护作用,而无不良功能后果,为预防性基因治疗的进一步临床前测试提供了强有力的依据。
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