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作 者:牛桂莲[1] 方伟岗[1] 郑杰[1] 由江峰[1] 吴秉铨[1]
机构地区:[1]北京医科大学病理学系
出 处:《中华病理学杂志》1998年第6期421-424,共4页Chinese Journal of Pathology
基 金:国家自然科学基金;国家教委跨世纪优秀人才计划基金
摘 要:目的探讨金属蛋白酶组织抑制因子3(TIMP3)对高转移性人肺巨细胞癌细胞系(BE1)恶性表型的影响。方法构建含全长人TIMP3cDNA的真核表达载体,用脂质体法转入BE1细胞。检测转染后BE1细胞的体外侵袭及裸鼠体内成瘤性及转移能力的变化。结果BE1细胞在转入TIMP3cDNA后表达TIMP3mRNA,与母系及空载体对照相比,体外侵袭力降低,在裸鼠体内成瘤率降低(对照组6/6只,实验组9/12只),成瘤潜伏期延长,转移至肺和淋巴结的能力降低(对照组分别为5/6只和6/6只;实验组分别为1/12只和5/12只)。Objective The purpose of this study is to determine if increasing levels of tissue inhibitor of metalloproteinase 3 (TIMP 3) expression could suppress the malignant phenotype of human cancer cells. Methods The recombinant expression vector, which contains full length cDNA of human TIMP 3, was constructed and transfected into BE1 cell line by lipofectin technique. The invasive and spontaneous metastatic potential was examined. Results TIMP 3 mRNA expression in TIMP 3 gene transfected BE1 cells was upregulated as detected by Northern blot. The invasion of TIMP 3 gene transfected cells across matrigel coated filters was significantly decreased when compared with controls. Following subcutaneous injection into nude mice, the TIMP 3 transfected cells suppressed primary tumor growth, as characterized by reduced tumor incidence (9/12 vs 6/6), longer latency and reduced metastatic potential to the lungs (1/12 vs 5/6) and lymph nodes (5/12 vs 6/6). Conclusion The results suggest that upregulation of TIMP 3 expression in BE1 cells resulted in suppression of the invasive potential of BE1 cells in vitro as well as tumorigenic and metastatic potential in nude mice.
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