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局部应用重组血管内皮生长因子(rVEGF)后,受照射手术部位的游离血管移植物存活情况得到改善。

Improved free vascular graft survival in an irradiated surgical site following topical application of rVEGF.

作者信息

Schultze-Mosgau Stefan, Wehrhan Falk, Rödel Franz, Amann Kerstin, Radespiel-Tröger Martin, Grabenbauer Gerhard G

机构信息

Department of Oral and Maxillofacial Surgery, University of Erlangen-Nuremberg, Erlangen, Germany.

出版信息

Int J Radiat Oncol Biol Phys. 2003 Nov 1;57(3):803-12. doi: 10.1016/s0360-3016(03)00636-9.

Abstract

PURPOSE

Wound healing disorders following surgery in preirradiated tissue are clinically well known and may even become more crucial with the increasing use of neoadjuvant chemoradiation protocols. Both the expression of vascular endothelial growth factor (VEGF) and endoglin (CD105) play a key role in neovascularization and wound healing after soft tissue grafts in irradiated and nonirradiated tissue. Modulation of neovascularization through the application of recombinant VEGF (rVEGF) may be a therapeutic option to reduce wound healing disorders in irradiated tissue. An experimental in vivo model was used to study the possible role of rVEGF for reduction of wound healing disorders and the promotion of neovascularization.

METHODS AND MATERIALS

A free myocutaneous gracilis flap was transplanted from the groin into the neck region of Wistar rats (weight 300-500 g) with and without previous irradiation of the neck region with 40 Gy: Group 1 (n = 7) radiotherapy alone; Group 2 (n = 14) flap transplantation alone and rVEGF; Group 3 (n = 14) radiotherapy, transplantation, and rVEGF. Time interval between irradiation and grafting was 10 +/- 1 day. 1.0 micro g rVEGF/500 microL phosphate-buffered saline was applied s.c. intraoperatively and on Days 1 through 7. Neovascularization (CD105) and endogenous VEGF expression were analyzed by means of immunohistochemistry on Days 3, 5, 7, 14, and 28 postoperatively and quantified as labeling indices (LI).

RESULTS

After irradiation there was a continuous significant reduction of the cytoplasmic VEGF expression (MEAN LI: 0.018 +/- 0.048) compared with the nonirradiated control (mean LI: 0.042 +/- 0.006) (p < 0.001). VEGF expression after flap transplantation without irradiation after VEGF application was at a constantly higher level from Day 3 (mean LI: 0.044 +/- 0.01) to Day 28 postoperatively compared with the control group (Day 3, mean LI: 0.028 +/- 0.006) (p < 0.001). As an indication of increased neovascularization after the local application of rVEGF, a significantly increased expression of CD105 was found in the transition area and graft bed from Day 7 on (p < 0.001). After irradiation and grafting there was a significant overall increase in the VEGF- and CD105-expression throughout Day 28 after rVEGF in the transition area (p < 0.001).

CONCLUSION

Whereas irradiation alone led to a downregulation of the endogenous VEGF expression, rVEGF application resulted in an increased expression and in a CD105 associated neovascularization after soft tissue grafting in irradiated tissues. Application of rVEGF may enable modulation of wound healing by influencing neovascularization. This could indicate a possible clinical approach for reducing fibrosis and chronic wound healing disorders in irradiated tissues.

摘要

目的

先前接受过放疗的组织术后伤口愈合障碍在临床上已广为人知,并且随着新辅助放化疗方案使用的增加,这一问题可能变得更加关键。血管内皮生长因子(VEGF)和内皮糖蛋白(CD105)的表达在照射和未照射组织的软组织移植后的新生血管形成和伤口愈合中均起关键作用。通过应用重组VEGF(rVEGF)来调节新生血管形成可能是减少照射组织中伤口愈合障碍的一种治疗选择。本研究使用一种体内实验模型来研究rVEGF在减少伤口愈合障碍及促进新生血管形成方面的可能作用。

方法和材料

将游离股薄肌皮瓣从腹股沟区移植到体重300 - 500 g的Wistar大鼠颈部区域,颈部区域之前分别接受40 Gy照射和未照射:第1组(n = 7)单纯放疗;第2组(n = 14)单纯皮瓣移植及rVEGF;第3组(n = 14)放疗、移植及rVEGF。照射与移植之间的时间间隔为10±1天。术中及术后第1至7天,将1.0 μg rVEGF/500 μL磷酸盐缓冲盐水皮下注射。术后第3、5、7、14和28天通过免疫组织化学分析新生血管形成(CD105)和内源性VEGF表达,并将其量化为标记指数(LI)。

结果

与未照射对照组(平均LI:0.042±0.006)相比,照射后细胞质VEGF表达持续显著降低(平均LI:0.018±0.048)(p < 0.001)。应用VEGF后,未照射情况下皮瓣移植后VEGF表达从术后第3天(平均LI:0.044±0.01)至第28天持续高于对照组(第3天,平均LI:0.028±0.006)(p < 0.001)。作为局部应用rVEGF后新生血管形成增加的指标,从第7天起在移行区和移植床发现CD105表达显著增加(p < 0.001)。照射和移植后,在移行区,rVEGF作用后第28天VEGF和CD105表达总体显著增加(p < 0.001)。

结论

单独照射导致内源性VEGF表达下调,而应用rVEGF导致照射组织软组织移植后VEGF表达增加及与CD105相关的新生血管形成。应用rVEGF可能通过影响新生血管形成来调节伤口愈合。这可能提示一种减少照射组织中纤维化和慢性伤口愈合障碍的可能临床方法。

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