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A novel combretastatin A-4 derivative, AC7700, strongly stanches tumour blood flow and inhibits growth of tumours developing in various tissues and organs

机译:新型康普他汀A-4衍生物AC7700可以强烈抑制肿瘤血流并抑制各种组织器官中肿瘤的生长

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摘要

In a previous study, we used subcutaneous LY80 tumours (a subline of Yoshida sarcoma), Sato lung carcinoma, and methylcholanthrene-induced primary tumours, to demonstrate that a novel water-soluble combretastatin A-4 derivative, AC7700, abruptly and irreversibly stopped tumour blood flow. As a result of this interrupted supply of nutrients, extensive necrosis was induced within the tumour. In the present study, we investigated whether AC7700 acts in the same way against solid tumours growing in the liver, stomach, kidney, muscle, and lymph nodes. Tumour blood flow and the change in tumour blood flow induced by AC7700 were measured by the hydrogen clearance method. In a model of cancer chemotherapy against metastases, LY80 cells (2×106) were injected into the lateral tail vein, and AC7700 at 10 mg kg−1 was injected i.v. five times at intervals of 2 days, starting on day 7 after tumour cell injection. The number and size of tumours were compared with those in the control group. The change in tumour blood flow and the therapeutic effect of AC7700 on microtumours were observed directly by using Sato lung carcinoma implanted in a rat transparent chamber. AC7700 caused a marked decrease in the tumour blood flow of all LY80 tumours developing in various tissues and organs and growth of all tumours including lymph node metastases and microtumours was inhibited. In every tumour, tumour blood flow began to decrease immediately after AC7700 administration and reached a minimum at approximately 30 min after injection. In many tumour capillaries, blood flow completely stopped within 3 min after AC7700 administration. These results demonstrate that AC7700 is effective for tumours growing in various tissues and organs and for metastases. We conclude that tumour blood flow stanching induced by AC7700 may become an effective therapeutic strategy for all cancers, including refractory cancers because the therapeutic effect is independent of tumour site and specific type of cancer.
机译:在先前的研究中,我们使用了皮下LY80肿瘤(吉田肉瘤的一个亚系),佐藤肺癌和甲基胆固醇诱发的原发性肿瘤,证明了一种新型的水溶性康他汀A-4衍生物AC7700能够以不可逆转的方式终止肿瘤。血流(量。由于这种营养供应的中断,在肿瘤内诱发了广泛的坏死。在本研究中,我们调查了AC7700是否以相同的方式作用于在肝,胃,肾,肌肉和淋巴结中生长的实体瘤。用氢清除法测量AC7700诱导的肿瘤血流量和肿瘤血流量的变化。在针对转移的癌症化学疗法模型中,将LY80细胞(2×106)注入尾侧静脉,并静脉内注入10μmgkg-1的AC7700。从注射肿瘤细胞后的第7天开始,每2天间隔5次。将肿瘤的数量和大小与对照组进行比较。通过将Sato肺癌植入大鼠透明腔室,可直接观察到肿瘤血流的变化以及AC7700对微肿瘤的治疗效果。 AC7700导致在各种组织和器官中发育的所有LY80肿瘤的肿瘤血流量明显减少,并且所有肿瘤(包括淋巴结转移和微瘤)的生长均受到抑制。在每种肿瘤中,AC7700给药后肿瘤血流量立即开始减少,并在注射后约30分钟达到最小。在许多肿瘤毛细血管中,AC7700给药后3分钟内血流完全停止。这些结果证明AC7700对在各种组织和器官中生长的肿瘤和转移有效。我们的结论是,AC7700引起的肿瘤血流停滞可能成为所有癌症(包括难治性癌症)的有效治疗策略,因为治疗效果与肿瘤部位和特定类型的癌症无关。

著录项

  • 作者

    Hori, K; Saito, S; Kubota, K;

  • 作者单位
  • 年度 2002
  • 总页数
  • 原文格式 PDF
  • 正文语种 {"code":"en","name":"English","id":9}
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