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卤夫酮抑制植入性转移性大鼠脑肿瘤模型中的血管生成和生长——一项磁共振成像研究。

Halofuginone inhibits angiogenesis and growth in implanted metastatic rat brain tumor model--an MRI study.

作者信息

Abramovitch Rinat, Itzik Anna, Harel Hila, Nagler Arnon, Vlodavsky Israel, Siegal Tali

机构信息

The Goldyne Savad Institute of Gene Therapy, MRI/MRS Laboratory, HBRC, Hadassah Hebrew University Medical Center, Jerusalem, Israel.

出版信息

Neoplasia. 2004 Sep-Oct;6(5):480-9. doi: 10.1593/neo.03520.

Abstract

Tumor growth and metastasis depend on angiogenesis; therefore, efforts are made to develop specific angiogenic inhibitors. Halofuginone (HF) is a potent inhibitor of collagen type alpha1(I). In solid tumor models, HF has a potent antitumor and antiangiogenic effect in vivo, but its effect on brain tumors has not yet been evaluated. By employing magnetic resonance imaging (MRI), we monitored the effect of HF on tumor progression and vascularization by utilizing an implanted malignant fibrous histiocytoma metastatic rat brain tumor model. Here we demonstrate that treatment with HF effectively and dose-dependently reduced tumor growth and angiogenesis. On day 13, HF-treated tumors were fivefold smaller than control (P < .001). Treatment with HF significantly prolonged survival of treated animals (142%; P = .001). In HF-treated rats, tumor vascularization was inhibited by 30% on day 13 and by 37% on day 19 (P < .05). Additionally, HF treatment inhibited vessel maturation (P = .03). Finally, in HF-treated rats, we noticed the appearance of a few clusters of satellite tumors, which were distinct from the primary tumor and usually contained vessel cores. This phenomenon was relatively moderate when compared to previous reports of other antiangiogenic agents used to treat brain tumors. We therefore conclude that HF is effective for treatment of metastatic brain tumors.

摘要

肿瘤的生长和转移依赖于血管生成;因此,人们致力于开发特异性血管生成抑制剂。常山酮(HF)是α1(I)型胶原蛋白的强效抑制剂。在实体瘤模型中,HF在体内具有强效的抗肿瘤和抗血管生成作用,但其对脑肿瘤的作用尚未得到评估。通过采用磁共振成像(MRI),我们利用植入的恶性纤维组织细胞瘤转移性大鼠脑肿瘤模型,监测了HF对肿瘤进展和血管生成的影响。在此我们证明,HF治疗可有效且剂量依赖性地降低肿瘤生长和血管生成。在第13天,接受HF治疗的肿瘤比对照组小5倍(P <.001)。HF治疗显著延长了治疗动物的生存期(142%;P =.001)。在接受HF治疗的大鼠中,第13天肿瘤血管生成受到30%的抑制,第19天受到37%的抑制(P <.05)。此外,HF治疗抑制了血管成熟(P =.03)。最后,在接受HF治疗的大鼠中,我们注意到出现了一些卫星肿瘤簇,它们与原发性肿瘤不同,通常含有血管核心。与先前关于用于治疗脑肿瘤的其他抗血管生成药物的报道相比,这种现象相对较轻。因此,我们得出结论,HF对转移性脑肿瘤的治疗有效。

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