Jiang Wen G, Grimshaw David, Martin Tracey A, Davies Gaynor, Parr Christian, Watkins Gareth, Lane Jane, Abounader Roger, Laterra John, Mansel Robert E
Metastasis Research Group, University Department of Surgery, University of Wales College of Medicine, Cardiff CF14 4XN, Wales, UK.
Clin Cancer Res. 2003 Sep 15;9(11):4274-81.
Hepatocyte growth factor/scatter factor (HGF/SF) is known to increase the invasiveness and migration of cancer cells in vitro and induce angiogenesis. This study examined if inhibition of HGF/SF receptor expression by cancer cells and HGF/SF expression by stromal fibroblasts affects the growth of mammary cancer.
Transgenes encoding ribozymes to specifically target human HGF/SF receptor (pLXSN-MET) or HGF/SF (pLXSN-HGF) were constructed using a pLXSN retroviral vector. Human mammary cancer cells MDA MB 231 was transduced with pLXSN-MET (MDA(+/+)). A human fibroblast cell line MRC5, which produces bioactive HGF/SF, was transduced with pLXSN-HGF (MRC5(+/+)). These cells were used in a nude mice breast tumor model.
HGF receptor in MDA(+/+) cells and HGF in MRC5(+/+)cells were successfully removed with respective ribozymes as shown by reverse transcription-PCR and Western blotting, respectively. MDA(+/+) was found to have reduced invasiveness when stimulated with HGF/SF. MRC5(+/+) exhibited a significant reduction in HGF/SF production. When injected into athymic nude mice, MDA(+/+) exhibited a slower rate of growth, compared with the wild type (MDA(-/-)), and the cells transduced with control viral vector (MDA(+/-)). The growth of MDA(-/-) tumor was significantly enhanced when coimplanted with wild-type MRC5 (MRC5(-/-)), and the stimulatory effect was reduced when MRC5(+/+) cells were coimplanted instead of MRC5(-/-). The reduction of tumor growth was accompanied by reduction of angiogenesis, as demonstrated by the staining of VE-cadherin in primary tumor tissues.
Retroviral ribozyme transgenes targeting HGF/SF in fibroblasts or its receptor cMET in mammary cancer cells can reduce the growth of mammary cancer and associated angiogenesis by inhibiting paracrine stromal-tumor cell interactions.
已知肝细胞生长因子/离散因子(HGF/SF)可在体外增加癌细胞的侵袭性和迁移能力并诱导血管生成。本研究检测了癌细胞对HGF/SF受体表达的抑制以及基质成纤维细胞对HGF/SF表达的抑制是否会影响乳腺癌的生长。
使用pLXSN逆转录病毒载体构建编码核酶的转基因,以特异性靶向人HGF/SF受体(pLXSN-MET)或HGF/SF(pLXSN-HGF)。用人pLXSN-MET转导人乳腺癌细胞MDA MB 231(MDA(+/+))。用pLXSN-HGF转导产生生物活性HGF/SF的人成纤维细胞系MRC5(MRC5(+/+))。将这些细胞用于裸鼠乳腺肿瘤模型。
如逆转录-PCR和蛋白质印迹分别所示,MDA(+/+)细胞中的HGF受体和MRC5(+/+)细胞中的HGF分别被各自的核酶成功去除。发现MDA(+/+)在用HGF/SF刺激时侵袭性降低。MRC5(+/+)的HGF/SF产生显著减少。当注射到无胸腺裸鼠体内时,与野生型(MDA(-/-))和用对照病毒载体转导的细胞(MDA(+/-))相比,MDA(+/+)的生长速率较慢。当与野生型MRC5(MRC5(-/-))共同植入时,MDA(-/-)肿瘤的生长显著增强,而当植入MRC5(+/+)细胞而非MRC5(-/-)时,刺激作用减弱。如原发性肿瘤组织中VE-钙黏蛋白染色所示,肿瘤生长的减少伴随着血管生成的减少。
靶向成纤维细胞中HGF/SF或乳腺癌细胞中其受体cMET的逆转录病毒核酶转基因可通过抑制旁分泌基质-肿瘤细胞相互作用来减少乳腺癌的生长及相关血管生成。
