Baldwin Zachary K, Chandiwal Amito, Balasubramanian Viji, Pearce Benjamin J, Curi Michael A, Skelly Christopher L, Huang Wendy W, Vosicky James E, Roizman Bernard, Weichselbaum Ralph R, Schwartz Lewis B
Section of Vascular Surgery, Department of Surgery, University of Chicago, 5841 South Maryland Avenue, Chicago, IL, USA.
J Vasc Surg. 2005 Jan;41(1):115-21. doi: 10.1016/j.jvs.2004.10.026.
Vascular remodeling in response to injury or low shear stress (or both) is characterized by neointimal hyperplasia and luminal contraction. When profound, the response leads to restenosis after percutaneous endovascular intervention as well as to de novo stenosis in vein grafts. It has recently been reported that exposure of vein patches to neurovirulence-attenuated Herpes simplex virus-1 (HSV-1) decreases neointimal hyperplasia and increases luminal area. This experiment tested the hypothesis that R7020, a more highly attenuated mutant of HSV-1, would modulate the vascular remodeling response of experimental vein grafts chronically exposed to low shear stress.
The external jugular veins of 31 New Zealand white rabbits were clamped and intraluminally exposed to vehicle (phospate-buffered saline solution, n = 11), R7020 2.5 x 10(8) plaque forming units [PFU]/mL (n = 8), or R7020 2.5 x 10(9) PFU/mL (n = 12) for 10 or 30 minutes at an average pressure of 80 mm Hg. After exposure, an end-to-side distal external jugular-to-common carotid artery anastomosis was created, resulting in a widely patent arteriovenous fistula. The external jugular was suture-ligated just proximal to the thoracic inlet, distal to a small 10- to 50-microm venous tributary, creating a reversed vein "graft" segment immediately and abruptly exposed to arterial pressure (48 +/- 3 mm Hg) and low shear stress (0.12 +/- .02 dyne/cm(2)). In the 29 animals (N = 31) that survived to harvest, 26 grafts were found to be patent and were analyzed further. Nine grafts were harvested within the first week after operation, snap frozen in liquid nitrogen, and assayed for the presence of the Herpes viral immediate-response protein ICP0 by Western blot analysis. The 17 remaining grafts were perfusion-fixed, excised, stained, and analyzed morphometrically by digital planimetry.
In patent grafts, the hemodynamic environment of low shear stress was maintained (shear stress at harvest, 0.26 +/- .06 dyne/cm(2)). Western blot analysis revealed the presence of ICP0 in R7020-exposed vein grafts after 2, 3, 7, and 14 days; ICP0 was not detected in unexposed vein grafts or adjacent carotid arteries. After 4 weeks, vein grafts exposed to R7020 exhibited a statistically significantly increased ratio of luminal radius to wall thickness, indicating altered remodeling (vehicle, 6.7 +/- 1.3; R7020 2.5 x 10(8), 9.1 +/- 1.3; R7020 2.5 x 10(9) ratio, 11.3 +/- 1.4; P < .05 for high dose compared with vehicle).
A brief exposure of the neurovirulence-attenuated HSV-1 strain R7020 results in an increased ratio of luminal radius to wall thickness in experimental vein grafts chronically exposed to low shear stress.
对损伤或低切应力(或二者兼具)产生的血管重塑表现为内膜增生和管腔狭窄。严重时,这种反应会导致经皮血管腔内介入术后再狭窄以及静脉移植物新生狭窄。最近有报道称,将静脉补片暴露于神经毒力减弱的单纯疱疹病毒1型(HSV-1)可减少内膜增生并增加管腔面积。本实验检验了以下假设:HSV-1的一种高度减毒突变体R7020,可调节长期暴露于低切应力的实验性静脉移植物的血管重塑反应。
钳夹31只新西兰白兔的颈外静脉,并在平均压力80 mmHg下向管腔内分别注入赋形剂(磷酸盐缓冲盐溶液,n = 11)、2.5×10⁸ 蚀斑形成单位[PFU]/mL的R7020(n = 8)或2.5×10⁹ PFU/mL的R7020(n = 12),持续10或30分钟。暴露后,进行端侧远端颈外静脉至颈总动脉吻合术,形成一个通畅的动静脉瘘。在胸廓入口近端、一条10至50微米小静脉分支远端将颈外静脉缝合结扎,立即形成一个反向静脉 “移植物” 段,并突然使其暴露于动脉压(48±3 mmHg)和低切应力(0.12±0.02达因/cm²)下。在存活至取材的29只动物(N = 31)中,发现26个移植物通畅,并进一步进行分析。9个移植物在术后第一周内取材,在液氮中速冻,通过蛋白质免疫印迹分析检测疱疹病毒即刻反应蛋白ICP0的存在情况。其余17个移植物进行灌注固定、切除、染色,并通过数字平面测量法进行形态学分析。
在通畅的移植物中,低切应力的血流动力学环境得以维持(取材时的切应力,0.26±0.06达因/cm²)。蛋白质免疫印迹分析显示,在暴露于R7020的静脉移植物中,术后2、3、7和14天均检测到ICP0;在未暴露的静脉移植物或相邻颈动脉中未检测到ICP0。4周后,暴露于R7020的静脉移植物的管腔半径与壁厚之比在统计学上显著增加,表明重塑改变(赋形剂组,6.7±1.3;2.5×10⁸ 的R7020组,9.1±1.3;2.5×10⁹ 的R7020组,11.3±1.4;高剂量组与赋形剂组相比,P < 0.05)。
短暂暴露于神经毒力减弱的HSV-1毒株R7020,可使长期暴露于低切应力的实验性静脉移植物的管腔半径与壁厚之比增加。
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