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反义CD44S cDNA的导入可下调总体CD44异构体的表达,并抑制高转移性结肠癌细胞的肿瘤生长和转移。

Introduction of antisense CD44S CDNA down-regulates expression of overall CD44 isoforms and inhibits tumor growth and metastasis in highly metastatic colon carcinoma cells.

作者信息

Harada N, Mizoi T, Kinouchi M, Hoshi K, Ishii S, Shiiba K, Sasaki I, Matsuno S

机构信息

First Department of Surgery, Tohoku University School of Medicine, Sendai, Japan.

出版信息

Int J Cancer. 2001 Jan 1;91(1):67-75. doi: 10.1002/1097-0215(20010101)91:1<67::aid-ijc1011>3.0.co;2-d.

Abstract

We created antisense CD44 transfectants using LS174T, a colon adenocarcinoma cell line and assessed the effects of overall CD44 down-regulation on colorectal tumor growth and metastasis. The expression of antisense CD44s (the standard form of CD44) cDNA markedly inhibited the overall expression of CD44 variants. In vitro studies showed a significantly reduced ability of the stable antisense transfectants (LS174TAS1 and LS174TAS2) to bind hyaluronate and osteopontin, ligands for CD44. These cells developed tumors more slowly than controls (parental LS174T and mock transfectants) when the cells were subcutaneously injected into SCID mice. However, in vitro proliferation assays demonstrated no significant difference between the antisense transfectants and the controls on a hyaluronate-coated surface, suggesting the participation of ligands other than hyaluronate in tumor growth in vivo. Intrasplenic injection of parental LS174T cells produced colonies in the liver in 10 of 11 mice, whereas mice injected with the antisense transfectants were completely free of metastasis. In peritoneal dissemination, the weight of nodules and amount of ascites were significantly reduced in LS174TAS1 and AS2 compared with the controls. In vitro adhesion assays between the transfectants or controls and human peritoneal mesothelial cells revealed that the binding of LS174T cells to mesothelial cells was partly mediated by CD44-hyaluronate interaction. These data suggest that CD44-hyaluronate interaction plays a crucial role in peritoneal dissemination in colorectal carcinoma. The results of our study demonstrate the possible application of antisense CD44s to the treatment of colorectal carcinoma.

摘要

我们使用结肠腺癌细胞系LS174T构建了反义CD44转染细胞,并评估了CD44整体下调对结直肠癌生长和转移的影响。反义CD44s(CD44的标准形式)cDNA的表达显著抑制了CD44变体的整体表达。体外研究表明,稳定的反义转染细胞(LS174TAS1和LS174TAS2)与透明质酸和骨桥蛋白(CD44的配体)结合的能力显著降低。当将这些细胞皮下注射到SCID小鼠体内时,它们形成肿瘤的速度比对照(亲本LS174T和空载体转染细胞)慢。然而,体外增殖试验表明,在透明质酸包被的表面上,反义转染细胞与对照之间没有显著差异,这表明除透明质酸外的其他配体参与了体内肿瘤生长。脾内注射亲本LS174T细胞后,11只小鼠中有10只在肝脏中形成了菌落,而注射反义转染细胞的小鼠则完全没有转移。在腹膜播散中,与对照相比,LS174TAS1和AS2中的结节重量和腹水量显著减少。转染细胞或对照与人腹膜间皮细胞之间的体外黏附试验表明,LS174T细胞与间皮细胞的结合部分是由CD44-透明质酸相互作用介导的。这些数据表明,CD44-透明质酸相互作用在结直肠癌的腹膜播散中起关键作用。我们的研究结果证明了反义CD44s在结直肠癌治疗中的可能应用。

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