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将血小板反应蛋白1互补DNA转染到人乳腺癌细胞系中可降低原发性肿瘤生长、转移潜能和血管生成。

Transfection of thrombospondin 1 complementary DNA into a human breast carcinoma cell line reduces primary tumor growth, metastatic potential, and angiogenesis.

作者信息

Weinstat-Saslow D L, Zabrenetzky V S, VanHoutte K, Frazier W A, Roberts D D, Steeg P S

机构信息

Women's Cancers Section, National Cancer Institute, Bethesda, Maryland 20892.

出版信息

Cancer Res. 1994 Dec 15;54(24):6504-11.

PMID:7527299
Abstract

Previous studies demonstrated that metastatic MDA-MB-435 breast carcinoma cells synthesized and secreted less of the extracellular matrix protein thrombospondin 1 (TSP1) than nonmetastatic breast carcinoma cell lines, a trend also observed for melanoma and lung carcinoma cell lines. To directly examine the effect of tumor cell TSP1 expression on tumor growth and metastasis. MDA-MB-435 cells were transfected with full length THBS-1 cDNA linked to a constitutive cytomegalovirus promoter, or with the cytomegalovirus vector alone. Injection of transfected clones that overexpressed TSP1 into the mammary fat pad of nude mice resulted in a dose-dependent inhibition of primary tumor size and an inhibition of spontaneous pulmonary metastases, which occurred in 21-30% of THBS-1 transfectants compared to 44-49% of controls (P = 0.007). An additional clone was identified that overexpressed a COOH-terminally truncated TSP1. This clone produced larger primary tumors and an increase in the occurrence of metastases relative to control transfectants, suggesting the participation of a previously understudied region of TSP1 in the regulation of tumor progression. The THBS-1 and control transfectants did not exhibit significant differences in growth, colonization, or motility in vitro. However, a relative reduction in capillary densities in primary tumors formed by the wild-type THBS-1 transfectants was observed, suggestive of an angiostatic effect. The data indicate that tumor cell production of TSP1 can exert a significant inhibitory effect on tumor progression in the MDA-MB-435 breast carcinoma cell line, which may be attributable in part to a reduction in angiogenesis.

摘要

先前的研究表明,转移性MDA-MB-435乳腺癌细胞合成和分泌的细胞外基质蛋白血小板反应蛋白1(TSP1)比非转移性乳腺癌细胞系少,黑色素瘤和肺癌细胞系也观察到这种趋势。为了直接检测肿瘤细胞TSP1表达对肿瘤生长和转移的影响,将与组成型巨细胞病毒启动子相连的全长THBS-1 cDNA转染到MDA-MB-435细胞中,或仅转染巨细胞病毒载体。将过表达TSP1的转染克隆注射到裸鼠的乳腺脂肪垫中,导致原发性肿瘤大小呈剂量依赖性抑制,并抑制自发性肺转移,THBS-1转染细胞中21%-30%发生肺转移,而对照组为44%-49%(P = 0.007)。另外鉴定出一个过表达COOH末端截短型TSP1的克隆。与对照转染细胞相比,该克隆产生更大的原发性肿瘤,转移发生率增加,这表明TSP1一个先前研究较少的区域参与了肿瘤进展的调控。THBS-1和对照转染细胞在体外生长、定植或运动性方面没有显著差异。然而,观察到野生型THBS-1转染细胞形成的原发性肿瘤中毛细血管密度相对降低,提示有血管生成抑制作用。数据表明,肿瘤细胞产生的TSP1可对MDA-MB-435乳腺癌细胞系的肿瘤进展产生显著抑制作用,这可能部分归因于血管生成的减少。

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Transfection of thrombospondin 1 complementary DNA into a human breast carcinoma cell line reduces primary tumor growth, metastatic potential, and angiogenesis.将血小板反应蛋白1互补DNA转染到人乳腺癌细胞系中可降低原发性肿瘤生长、转移潜能和血管生成。
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