Wild R, Dhanabal M, Olson T A, Ramakrishnan S
SUGEN Inc, 230 East Grand Avenue, South San Francisco, CA 94080-4811, USA.
Br J Cancer. 2000 Oct;83(8):1077-83. doi: 10.1054/bjoc.2000.1439.
Vascular endothelial growth factor (VEGF) plays an important role in tumour angiogenesis. VEGF binds to tyrosine kinase receptors, which are expressed almost exclusively on tumour endothelium. Therefore, VEGF can be used to target toxin molecules to tumour vessels for anti-angiogenic therapy. However, recent evidence suggests that VEGF can also bind in an isoform-specific fashion to a newly identified neuropilin-1 (NP-1) receptor. NP-1 is widely expressed in normal tissue and presents a potential target for unwanted toxicity. As a consequence, we investigated whether the VEGF121 isoform, which lacks the NP-1 binding domain, could be used to target toxin polypeptides to tumour vasculature. Treatment of endothelial cells with a VEGF121-diphtheria toxin (DT385) conjugate selectively inhibited proliferating endothelial cells, whereas confluent cultures were completely resistant to the construct. In addition, VEGF121-DT385 conjugate treatment completely prevented tumour cell induced angiogenesis in vivo. Most importantly, the conjugate inhibited tumour growth in athymic mice and induced tumour-specific vascular damage. There was also no apparent toxicity associated with the treatment. Our results suggest that proliferating endothelial cells are highly sensitive to VEGF121-toxin conjugates and that the binding to NP-1 receptors is not necessary for efficient inhibition of tumour growth.
血管内皮生长因子(VEGF)在肿瘤血管生成中起重要作用。VEGF与酪氨酸激酶受体结合,这些受体几乎仅在肿瘤内皮细胞上表达。因此,VEGF可用于将毒素分子靶向肿瘤血管以进行抗血管生成治疗。然而,最近的证据表明,VEGF也可以以异构体特异性的方式与新发现的神经纤毛蛋白-1(NP-1)受体结合。NP-1在正常组织中广泛表达,是产生不必要毒性的潜在靶点。因此,我们研究了缺乏NP-1结合域的VEGF121异构体是否可用于将毒素多肽靶向肿瘤脉管系统。用VEGF121-白喉毒素(DT385)偶联物处理内皮细胞可选择性抑制增殖的内皮细胞,而汇合培养物对该构建体完全耐药。此外,VEGF121-DT385偶联物处理在体内完全阻止了肿瘤细胞诱导的血管生成。最重要的是,该偶联物抑制了无胸腺小鼠的肿瘤生长并诱导了肿瘤特异性血管损伤。该治疗也没有明显的毒性。我们的结果表明,增殖的内皮细胞对VEGF121-毒素偶联物高度敏感,并且与NP-1受体的结合对于有效抑制肿瘤生长不是必需的。
