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α-连环蛋白阳性的HCT-8人结肠癌细胞体内侵袭的诱导

Induction of invasion in vivo of alpha-catenin-positive HCT-8 human colon-cancer cells.

作者信息

Van Hoorde L, Pocard M, Maryns I, Poupon M F, Mareel M

机构信息

Laboratory of Experimental Cancerology, Department of Radiotherapy and Nuclear Medicine, Ghent University Hospital, Gent, Belgium.

出版信息

Int J Cancer. 2000 Dec 1;88(5):751-8. doi: 10.1002/1097-0215(20001201)88:5<751::aid-ijc11>3.0.co;2-b.

Abstract

Variants from the HCT-8 colon-cancer cell line were implanted s.c. and orthotopically into nude mice. Well-differentiated HCT-8/E11 and HCT-8/E41 cells have a functional E-cadherin-catenin complex and are non-invasive into pre-cultured chick heart fragments in vitro, whereas poorly differentiated HCT-8/E11R1 cells are deficient in alpha-catenin protein and invasive in heart fragments. We investigated whether these differences were maintained in vivo. In contrast with in vitro observations, in vivo the 3 HCT-8 variants behaved very similarly and all formed undifferentiated tumors. The in vivo invasive behavior of HCT-8 cells was site-dependently modulated: HCT-8 cells invaded when injected into the cecum but not when injected s.c. Metastases to the liver or lungs were not observed. The composition and expression of the E-cadherin-catenin complex in nude mouse HCT-8 tumors was the same as in HCT-8 cells in culture on solid substrate. We conclude that the in vivo invasive behavior of HCT-8 cells is not determined by whether alpha-catenin is expressed or not but by as yet unidentified host factors.

摘要

将来自HCT - 8结肠癌细胞系的变体皮下和原位植入裸鼠体内。高分化的HCT - 8/E11和HCT - 8/E41细胞具有功能性E - 钙黏蛋白 - 连环蛋白复合物,在体外对预培养的鸡心脏组织块无侵袭性,而低分化的HCT - 8/E11R1细胞缺乏α - 连环蛋白蛋白,对心脏组织块有侵袭性。我们研究了这些差异在体内是否依然存在。与体外观察结果相反,在体内这3种HCT - 8变体的行为非常相似,均形成未分化肿瘤。HCT - 8细胞的体内侵袭行为受部位依赖性调节:注入盲肠时HCT - 8细胞会发生侵袭,而皮下注射时则不会。未观察到肝或肺转移。裸鼠HCT - 8肿瘤中E - 钙黏蛋白 - 连环蛋白复合物的组成和表达与在固体基质上培养的HCT - 8细胞相同。我们得出结论,HCT - 8细胞的体内侵袭行为不是由α - 连环蛋白是否表达决定的,而是由尚未确定的宿主因素决定的。

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