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Inhibition of Neovascularization and Tumor Growth and Facilitation of Wound Repair by Halofuginone an Inhibitor of Collagen Type I Synthesis

机译:Halofuginone(一种I型胶原合成抑制剂)抑制新血管形成和肿瘤生长并促进伤口修复

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摘要

Halofuginone, an inhibitor of collagen α1(I) gene expression was used for the treatment of subcutaneously implanted C6 glioma tumors. Halofuginone had no effect on the growth of C6 glioma spheroids in vitro, and these spheroids showed no collagen α1(I) expression and no collagen synthesis. However, a significant attenuation of tumor growth was observed in vivo, for spheroids implanted in CD-1 nude mice which were treated by oral or intraperitoneal (4 µg every 48 hours) administration of halofuginone. In these mice, treatment was associated with a dose-dependent reduction in collagen α1(I) expression and dose- and time-dependent inhibition of angiogenesis, as measured by MRI. Moreover, halofuginone treatment was associated with improved re-epithelialization of the chronic wounds that are associated with this experimental model. Oral administration of halofuginone was effective also in intervention in tumor growth, and here, too, the treatment was associated with reduced angiogenic activity and vessel regression. These results demonstrate the important role of collagen type I in tumor angiogenesis and tumor growth and implicate its role in chronic wounds. Inhibition of the expression of collagen type I provides an attractive new target for cancer therapy.
机译:Halofuginone,一种胶原α1(I)基因表达的抑制剂,被用于治疗皮下植入的C6胶质瘤肿瘤。 halofuginone在体外对C6胶质瘤球体的生长没有影响,并且这些球体没有胶原蛋白α1(I)的表达,也没有胶原蛋白的合成。但是,对于植入CD-1裸鼠中的类球体,通过口服或腹膜内(每48小时给药4 µg)卤氟甲酮治疗,可以观察到体内肿瘤生长的显着减弱。在这些小鼠中,治疗与MRI测得的胶原α1(I)表达的剂量依赖性降低以及血管生成的剂量依赖性和时间依赖性抑制有关。此外,卤氟胍酮治疗与与该实验模型有关的慢性伤口的再上皮化改善有关。口服氟氟胍酮在干预肿瘤生长方面也很有效,在这里,治疗也与降低血管生成活性和血管退化有关。这些结果证明了I型胶原在肿瘤血管生成和肿瘤生长中的重要作用,并暗示了其在慢性伤口中的作用。抑制I型胶原蛋白的表达为癌症治疗提供了一个有吸引力的新靶标。

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