Lokmic Zerina, Thomas James L, Morrison Wayne A, Thompson Erik W, Mitchell Geraldine M
Bernard O'Brien Institute of Microsurgery, Melbourne, Australia.
J Vasc Surg. 2008 Oct;48(4):974-85. doi: 10.1016/j.jvs.2008.05.021. Epub 2008 Aug 23.
An arteriovenous loop (AVL) enclosed in a polycarbonate chamber in vivo, produces a fibrin exudate which acts as a provisional matrix for the development of a tissue engineered microcirculatory network.
By administering enoxaparin sodium - an inhibitor of fibrin polymerization, the significance of fibrin scaffold formation on AVL construct size (including the AVL, fibrin scaffold, and new tissue growth into the fibrin), growth, and vascularization were assessed and compared to controls.
In Sprague Dawley rats, an AVL was created on femoral vessels and inserted into a polycarbonate chamber in the groin in 3 control groups (Series I) and 3 experimental groups (Series II). Two hours before surgery and 6 hours post-surgery, saline (Series I) or enoxaparin sodium (0.6 mg/kg, Series II) was administered intra-peritoneally. Thereafter, the rats were injected daily with saline (Series I) or enoxaparin sodium (1.5 mg/kg, Series II) until construct retrieval at 3, 10, or 21 days. The retrieved constructs underwent weight and volume measurements, and morphologic/morphometric analysis of new tissue components.
Enoxaparin sodium treatment resulted in the development of smaller AVL constructs at 3, 10, and 21 days. Construct weight and volume were significantly reduced at 10 days (control weight 0.337 +/- 0.016 g [Mean +/- SEM] vs treated 0.228 +/- 0.048, [P < .001]: control volume 0.317 +/- 0.015 mL vs treated 0.184 +/- 0.039 mL [P < .01]) and 21 days (control weight 0.306 +/- 0.053 g vs treated 0.198 +/- 0.043 g [P < .01]: control volume 0.285 +/- 0.047 mL vs treated 0.148 +/- 0.041 mL, [P < .01]). Angiogenesis was delayed in the enoxaparin sodium-treated constructs with the absolute vascular volume significantly decreased at 10 days (control vascular volume 0.029 +/- 0.03 mL vs treated 0.012 +/- 0.002 mL [P < .05]).
In this in vivo tissue engineering model, endogenous, extra-vascularly deposited fibrin volume determines construct size and vascular growth in the first 3 weeks and is, therefore, critical to full construct development.
体内包裹在聚碳酸酯腔室中的动静脉环(AVL)会产生纤维蛋白渗出物,该渗出物作为组织工程化微循环网络发育的临时基质。
通过给予依诺肝素钠(一种纤维蛋白聚合抑制剂),评估纤维蛋白支架形成对AVL构建体大小(包括AVL、纤维蛋白支架以及长入纤维蛋白的新组织)、生长和血管化的意义,并与对照组进行比较。
在Sprague Dawley大鼠中,在股血管上创建AVL,并将其插入腹股沟的聚碳酸酯腔室中,分为3个对照组(系列I)和3个实验组(系列II)。手术前2小时和手术后6小时,腹腔内注射生理盐水(系列I)或依诺肝素钠(0.6mg/kg,系列II)。此后,每天给大鼠注射生理盐水(系列I)或依诺肝素钠(1.5mg/kg,系列II),直到在第3、10或21天取出构建体。取出的构建体进行重量和体积测量,以及新组织成分的形态学/形态计量学分析。
依诺肝素钠治疗导致在第3、10和21天时AVL构建体变小。在第10天(对照重量0.337±0.016g[平均值±标准误],治疗组0.228±0.048g,[P<.001];对照体积0.317±0.015mL,治疗组0.184±0.039mL[P<.01])和第21天(对照重量0.306±0.053g,治疗组0.198±0.043g[P<.01];对照体积0.285±0.047mL,治疗组0.148±0.041mL,[P<.01]),构建体重量和体积显著降低。依诺肝素钠治疗的构建体中血管生成延迟,在第10天时绝对血管体积显著减少(对照血管体积0.029±0.03mL,治疗组0.012±0.002mL[P<.05])。
在这个体内组织工程模型中,内源性血管外沉积的纤维蛋白体积在前3周决定构建体大小和血管生长,因此对构建体的完全发育至关重要。
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