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首页> 外文期刊>The Journal of Thoracic and Cardiovascular Surgery >Therapeutic angiogenesis in the ischemic canine heart induced by myocardial injection of naked complementary DNA plasmid encoding hepatocyte growth factor.
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Therapeutic angiogenesis in the ischemic canine heart induced by myocardial injection of naked complementary DNA plasmid encoding hepatocyte growth factor.

机译:心肌注射编码肝细胞生长因子的裸互补DNA质粒在缺血犬心脏中产生的治疗性血管生成。

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OBJECTIVE: We investigated the efficacy of directly injecting a plasmid with complementary DNA encoding human hepatocyte growth factor into ischemic canine myocardium to induce angiogenesis. METHODS: Four weeks after ligation of the left anterior descending coronary artery, 125 microg of a complementary DNA plasmid encoding the gene for either hepatocyte growth factor (n = 8) or LacZ (transfection control group, n = 8) was injected directly into the myocardium at the border between the normal tissue and the infarction. Eight other dogs were used as a sham control group. Regional thickening fraction, which indicated contractile function, and blood flow in the normal (circumflex branch territory) and ischemic areas were evaluated under dobutamine administration just before and 4 weeks after transfection. The animals were killed, and capillary numbers in both areas were assessed. These data in the ischemic area were evaluated as the percentage of those in the normal. RESULTS: The number of myocardial capillaries in the ischemic area was successfully increased to approximately 140% of usual in the hepatocyte growth factor group, whereas no change was observed in the other groups (P =.0017 by analysis of variance). Furthermore, regional thickening fraction and blood flow in the ischemic area, which had deteriorated after coronary ligation, showed significant improvement in the hepatocyte growth factor group relative to the other groups (thickening fraction P <.0001 by analysis of variance, blood flow P =.0005 by analysis of variance). CONCLUSIONS: These results support the efficacy of the direct injection of plasmid complementary DNA encoding human hepatocyte growth factor to induce therapeutic angiogenesis in the ischemic myocardium.
机译:目的:我们研究了将编码人肝细胞生长因子的互补DNA质粒直接注射入缺血性犬心肌的诱导血管生成的功效。方法:结扎左冠状动脉前降支后四周,将125微克编码肝细胞生长因子(n = 8)或LacZ(转染对照组,n = 8)基因的互补DNA质粒直接注射到小鼠体内。心肌位于正常组织和梗塞之间的边界。将另外八只狗用作假对照组。转染前和转染后4周,在多巴酚丁胺的管理下,评估了指示收缩功能的区域增厚分数以及正常(回旋支区域)和缺血区域的血流量。处死动物,并评估两个区域的毛细血管数目。将缺血区域的这些数据评估为正常区域的百分比。结果:在肝细胞生长因子组中,缺血区域的心肌毛细血管数目成功增加至通常的140%,而其他组则未观察到变化(通过方差分析,P = .0017)。此外,与其他组相比,冠状动脉结扎后局部缺血区的局部增厚分数和血流量显着改善(通过方差分析,增厚分数P <.0001,血流量P = .0005(通过方差分析)。结论:这些结果支持直接注射编码人肝细胞生长因子的质粒互补DNA在缺血性心肌中诱导治疗性血管生成的功效。

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