在大型内膜增生动物模型中向主动脉冠状动脉大隐静脉移植物进行基因递送。
Gene delivery to aortocoronary saphenous vein grafts in a large animal model of intimal hyperplasia.
作者信息
Petrofski Jason A, Hata Jonathan A, Gehrig Thomas R, Hanish Steven I, Williams Matthew L, Thompson Richard B, Parsa Cyrus J, Koch Walter J, Milano Carmelo A
机构信息
Department of Surgery, Duke University Medical Center, Durham, NC 27703, USA.
出版信息
J Thorac Cardiovasc Surg. 2004 Jan;127(1):27-33. doi: 10.1016/j.jtcvs.2003.07.032.
OBJECTIVE
More than 50% of aortocoronary saphenous vein grafts are occluded 10 years after surgery. Intimal hyperplasia is an initial, critical step in the progression toward occlusion. To date, no clinically relevant large animal models of aortocoronary saphenous vein graft intimal hyperplasia have been fully characterized. Gene therapy holds promise as a novel treatment for aortocoronary saphenous vein graft intimal hyperplasia. The 2 objectives of this study are to characterize a canine model of aortocoronary saphenous vein graft intimal hyperplasia and to demonstrate that ex vivo gene delivery is possible in these grafts using adenoviral vectors.
METHODS
Ten dogs underwent aortocoronary bypass grafting using saphenous veins. Six dogs underwent serial arteriograms to monitor graft patency. On postoperative day 90, the dogs were killed and their grafted and nongrafted saphenous veins were studied histologically. Four dogs underwent the same procedure, but their saphenous veins were treated with 1 x 10(12) total viral particles of a replication-deficient, recombinant adenovirus containing beta-galactosidase (n = 2) or the beta-adrenergic receptor kinase carboxyl terminus (n = 2). These animals were killed on postoperative day 7 for determination of transgene expression.
RESULTS
All grafts were demonstrated patent by arteriogram before the animals were killed. The mean intimal area of the saphenous vein grafts was increased when compared with that of the nongrafted saphenous veins (2.83 mm(2) vs 0.09 mm(2), P <.0008). Adenoviral-treated saphenous vein grafts demonstrated positive transgene expression either by X-gal staining (beta-galactosidase) or Northern analysis (beta-adrenergic receptor kinase carboxyl terminus).
CONCLUSION
This study characterizes a clinically relevant canine model of aortocoronary saphenous vein graft intimal hyperplasia. In addition, it demonstrates that adenoviral vectors can be delivered ex vivo to the saphenous vein graft vessel wall at subphysiologic distension pressures. This model may be used in future studies to manipulate molecular targets critical in aortocoronary saphenous vein graft intimal hyperplasia.
目的
超过50%的主动脉冠状动脉大隐静脉移植血管在术后10年发生闭塞。内膜增生是其向闭塞进展的起始关键步骤。迄今为止,尚无已充分表征的与临床相关的主动脉冠状动脉大隐静脉移植内膜增生的大型动物模型。基因治疗有望成为治疗主动脉冠状动脉大隐静脉移植内膜增生的新方法。本研究的两个目的是表征主动脉冠状动脉大隐静脉移植内膜增生的犬模型,并证明使用腺病毒载体在这些移植血管中进行离体基因递送是可行的。
方法
10只犬接受了使用大隐静脉的主动脉冠状动脉旁路移植术。6只犬接受了系列动脉造影以监测移植血管通畅情况。术后第90天,处死犬并对其移植和未移植的大隐静脉进行组织学研究。4只犬接受相同手术,但它们的大隐静脉用含β-半乳糖苷酶(n = 2)或β-肾上腺素能受体激酶羧基末端(n = 2)的复制缺陷型重组腺病毒的1×10¹²个总病毒颗粒进行处理。这些动物在术后第7天处死以测定转基因表达。
结果
在处死动物前,所有移植血管经动脉造影显示通畅。与未移植的大隐静脉相比,大隐静脉移植血管的平均内膜面积增加(2.83平方毫米对0.09平方毫米,P <.0008)。经腺病毒处理的大隐静脉移植血管通过X-gal染色(β-半乳糖苷酶)或Northern分析(β-肾上腺素能受体激酶羧基末端)显示转基因表达阳性。
结论
本研究表征了一种与临床相关的主动脉冠状动脉大隐静脉移植内膜增生的犬模型。此外,它证明了腺病毒载体可在低于生理扩张压力下离体递送至大隐静脉移植血管壁。该模型可用于未来研究以操控在主动脉冠状动脉大隐静脉移植内膜增生中起关键作用的分子靶点。
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