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血管内皮生长因子的可控递送促进了兔缺血模型中的新生血管形成并维持肢体功能。

Controlled delivery of vascular endothelial growth factor promotes neovascularization and maintains limb function in a rabbit model of ischemia.

作者信息

Hopkins S P, Bulgrin J P, Sims R L, Bowman B, Donovan D L, Schmidt S P

机构信息

Department of Surgery, Akron General Medical Center, Ohio, USA.

出版信息

J Vasc Surg. 1998 May;27(5):886-94; discussion 895. doi: 10.1016/s0741-5214(98)70269-1.

DOI:10.1016/s0741-5214(98)70269-1
PMID:9620141
Abstract

PURPOSE

Vascular endothelial growth factor (VEGF) modulates new blood vessel development and growth and has been suggested as a potential therapeutic agent that could alleviate debilitating claudication in patients. The objective of this study was to determine whether controlled, local delivery of a low dose of VEGF from an osmotic pump could promote neovascularization, limb perfusion, and functional improvements in the hind limbs of rabbits rendered partially ischemic by surgery. The effects of VEGF were compared with those of the vasodilator nitroglycerin (NTG) and to saline administered similarly.

METHODS

Thirty rabbits were randomly assigned to either VEGF (n = 10), NTG (n = 10), or saline (n = 10) treatment groups. Partial ischemia was induced in each left hind limb by surgical ligation of the common and superficial femoral arteries, leaving the internal iliac artery intact. The right limb of each animal served as a nonischemic control. Immediately after vessel ligations, a 28-day osmotic pump was implanted to deliver VEGF (0.22 microg/kg/day), NTG (17.8 microg/kg/day), or saline solution into the common iliac artery just proximal to the ligation site. Comparative vascularity between ischemic and nonischemic limbs within treatment groups and between groups was evaluated by (1) capillary counts from representative fields of hematoxylin and eosin stained muscle tissue taken from hind limbs at day 40; (2) digitized arteriograms of ischemic legs at day 40, which were used to quantify the complexity of vascular branching (fractal dimension index) and the total extent of vascularization (vascular density index); (3) measuring capillary refill times in ischemic limbs; and (4) observations of functional and trophic changes in ischemic limbs. Statistical differences between treatment groups were evaluated by one-way ANOVA.

RESULTS

Complexity of vascular branching and vascular density were significantly greater (p < 0.001) in VEGF-treated ischemic limbs compared with NTG- and saline-treated ischemic limbs. By postoperation day 14, all VEGF-treated ischemic limbs had restored capillary refill (p < 0.001), new hair growth, and greatly improved limb function and appearance. Saline-treated limbs exhibited ischemic changes, with poor capillary refill and negligible limb function. Capillary refill in NTG-treated ischemic limbs did not differ significantly from saline-treated limbs. Ischemic VEGF-treated limbs had significantly more capillaries compared with both ischemic and nonischemic limbs in saline-treated animals (p < 0.05). Ischemic NTG-treated limbs also had significantly more capillaries compared with ischemic limbs in saline-treated animals (p < 0.05). Because of high variability, however, capillary counts in VEGF-treated ischemic limbs did not differ significantly from those of contralateral nonischemic limbs, or from capillary counts in either ischemic or nonischemic limbs of NTG-treated rabbits.

CONCLUSIONS

Controlled release of microgram quantities of VEGF significantly enhanced neovascularization and vascular perfusion in ischemic limbs compared with controls in this rabbit model of partial ischemia. In addition, VEGF-treated ischemic limbs demonstrated near-normal function and appearance, whereas NTG- and saline-treated ischemic controls remained noticeably impaired. This novel approach of VEGF delivery may prove clinically useful either alone or combined with revascularization procedures.

摘要

目的

血管内皮生长因子(VEGF)可调节新血管的发育和生长,有人提出它可能是一种潜在的治疗药物,能够缓解患者使人衰弱的跛行症状。本研究的目的是确定通过渗透泵控制局部递送低剂量VEGF是否能促进新血管形成、肢体灌注,并改善手术造成部分缺血的兔后肢的功能。将VEGF的作用与血管扩张剂硝酸甘油(NTG)以及以类似方式给予的生理盐水的作用进行比较。

方法

30只兔子被随机分为VEGF治疗组(n = 10)、NTG治疗组(n = 10)或生理盐水治疗组(n = 10)。通过手术结扎股总动脉和股浅动脉,保留髂内动脉完整,在每只兔子的左后肢诱导部分缺血。每只动物的右肢作为非缺血对照。血管结扎后立即植入一个28天的渗透泵,将VEGF(0.22微克/千克/天)、NTG(17.8微克/千克/天)或生理盐水溶液输送到结扎部位近端的髂总动脉中。通过以下方法评估治疗组内缺血肢体与非缺血肢体之间以及各治疗组之间的相对血管生成情况:(1)在第40天时,从后肢苏木精-伊红染色的肌肉组织的代表性视野中进行毛细血管计数;(2)第40天时缺血腿部的数字化动脉造影,用于量化血管分支的复杂性(分形维数指数)和血管生成的总范围(血管密度指数);(3)测量缺血肢体的毛细血管再充盈时间;(4)观察缺血肢体的功能和营养变化。通过单因素方差分析评估治疗组之间的统计学差异。

结果

与NTG和生理盐水治疗的缺血肢体相比,VEGF治疗的缺血肢体的血管分支复杂性和血管密度显著更高(p < 0.001)。到术后第14天,所有VEGF治疗的缺血肢体都恢复了毛细血管再充盈(p < 0.001),有新毛发生长,并且肢体功能和外观有了极大改善。生理盐水治疗的肢体出现缺血变化,毛细血管再充盈不良,肢体功能可忽略不计。NTG治疗的缺血肢体的毛细血管再充盈与生理盐水治疗的肢体相比无显著差异。与生理盐水治疗动物的缺血和非缺血肢体相比,VEGF治疗的缺血肢体有明显更多的毛细血管(p < 0.05)。与生理盐水治疗动物的缺血肢体相比,NTG治疗的缺血肢体也有明显更多的毛细血管(p < 0.05)。然而,由于变异性高,VEGF治疗的缺血肢体的毛细血管计数与对侧非缺血肢体的毛细血管计数相比,或与NTG治疗兔子的缺血或非缺血肢体的毛细血管计数相比,无显著差异。

结论

在这个部分缺血的兔模型中,与对照组相比,微克量VEGF的控释显著增强了缺血肢体的新血管形成和血管灌注。此外,VEGF治疗的缺血肢体表现出接近正常的功能和外观,而NTG和生理盐水治疗的缺血对照仍明显受损。这种VEGF递送的新方法单独使用或与血管重建手术联合使用可能在临床上有用。

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