同时应用碱性成纤维细胞生长因子和肝细胞生长因子以增强血管形成。
Simultaneous application of basic fibroblast growth factor and hepatocyte growth factor to enhance the blood vessels formation.
作者信息
Marui Akira, Kanematsu Akihiro, Yamahara Kenichi, Doi Kazuhiko, Kushibiki Toshihiro, Yamamoto Masaya, Itoh Hiroshi, Ikeda Tadashi, Tabata Yasuhiko, Komeda Masashi
机构信息
Department of Cardiovascular Surgery, Kyoto University Graduate School of Medicine, 54 Shogoin Kawahara, Sakyo, Kyoto, Japan 606-8507.
出版信息
J Vasc Surg. 2005 Jan;41(1):82-90. doi: 10.1016/j.jvs.2004.10.029.
OBJECTIVE
The present study investigated whether the simultaneous application of basic fibroblast growth factor (bFGF) and hepatocyte growth factor (HGF) enhances blood vessel formation in murine ischemic hindlimb compared with bFGF or HGF applied alone.
METHODS
Unilateral hindlimb ischemia was created in C57BL/6 mice. Hindlimb blood flow was evaluated by laser Doppler perfusion image index (LDPII) (ratio (%) of ischemic-to-normal-limb blood flow). The ischemic limbs were treated with bFGF and HGF separately, or bFGF and HGF together, and their therapeutic effects were assessed. Collagen microspheres (CM) were used as a sustained-release carrier for bFGF and HGF.
RESULTS
A single intramuscular injection of 5 microg or less of bFGF-incorporated CM (bFGF/CM) into the ischemic limb did not significantly increase the LDPII compared with the control (no treatment) 4 weeks after the treatment. Similarly, 20 microg or less of HGF/CM did not increase LDPII. Based on these results, we compared the dual release of CM incorporating 5 microg of bFGF and 20 microg of HGF with either the single release of 5 mug of bFGF/CM alone or 20 microg of HGF/CM alone. The LDPII of the dual release (94.2% +/- 10.9%) was higher than either single release (51.2% +/- 5.8% or 52.5% +/- 8.0%, P < .01). Furthermore, the LDPII in the dual release (94.2% +/- 10.9%) was equivalent to that with 80 microg of bFGF/CM (95.1% +/- 7.6%) alone or 80 microg of HGF/CM (92.8% +/- 7.6%) alone. A histologic evaluation at 4 weeks showed capillary density in the dual release (868 +/- 173 vessels/mm(2)) was higher than that in either single release (204 +/- 68 vessels/mm(2) or 185 +/- 98 vessels/mm(2) , P < .01). The percentage of mature vessels assessed by alpha-smooth muscle actin staining was also higher in the dual release (43.8% +/- 7.8% vs 9.5% +/- 3.0% or 11.7% +/- 3.8%, respectively; P < .01).
CONCLUSIONS
This study demonstrates that the sustained dual release of a lower dose of bFGF and HGF from a carrier matrix can achieve equivalent blood perfusion recovery and more mature vasculature in the ischemic limb than a higher dose of bFGF or HGF alone. This approach may be a highly promising strategy for the future treatment of peripheral vascular disease.
目的
本研究旨在探讨与单独应用碱性成纤维细胞生长因子(bFGF)或肝细胞生长因子(HGF)相比,同时应用这两种因子是否能增强小鼠缺血后肢的血管生成。
方法
在C57BL/6小鼠中制造单侧后肢缺血。通过激光多普勒灌注图像指数(LDPII)(缺血肢体与正常肢体血流的比率(%))评估后肢血流。分别用bFGF和HGF,或bFGF与HGF联合处理缺血肢体,并评估其治疗效果。胶原微球(CM)用作bFGF和HGF的缓释载体。
结果
治疗后4周,向缺血肢体单次肌内注射5微克或更少的含bFGF的CM(bFGF/CM)与对照组(未治疗)相比,未显著增加LDPII。同样,20微克或更少的HGF/CM也未增加LDPII。基于这些结果,我们将含5微克bFGF和20微克HGF的CM双释放与单独单次释放5微克bFGF/CM或20微克HGF/CM进行了比较。双释放组的LDPII(94.2%±10.9%)高于单释放组(51.2%±5.8%或52.5%±8.0%,P<.01)。此外,双释放组的LDPII(94.2%±10.9%)与单独使用80微克bFGF/CM(95.1%±7.6%)或80微克HGF/CM(92.8%±7.6%)时相当。4周时的组织学评估显示,双释放组的毛细血管密度(868±173个血管/mm²)高于单释放组(204±68个血管/mm²或185±98个血管/mm²,P<.01)。通过α-平滑肌肌动蛋白染色评估的成熟血管百分比在双释放组中也更高(分别为43.8%±7.8%,而单释放组为9.5%±3.0%或11.7%±3.8%;P<.01)。
结论
本研究表明,从载体基质中持续双释放较低剂量的bFGF和HGF与单独使用较高剂量的bFGF或HGF相比,能在缺血肢体中实现同等的血流灌注恢复和更成熟的脉管系统。这种方法可能是未来治疗外周血管疾病的一种非常有前景的策略。
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