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基底膜成分(基质胶)可促进人乳腺腺癌MCF7细胞的致瘤性,并提供一个体内模型来评估细胞对雌激素的反应性。

Basement membrane components (matrigel) promote the tumorigenicity of human breast adenocarcinoma MCF7 cells and provide an in vivo model to assess the responsiveness of cells to estrogen.

作者信息

Noel A, Simon N, Raus J, Foidart J M

机构信息

Laboratory of Biology, University of Liege, Diepenbeek, Belgium.

出版信息

Biochem Pharmacol. 1992 Mar 17;43(6):1263-7. doi: 10.1016/0006-2952(92)90501-9.

Abstract

The ability to transplant human tumors into athymic nude mice allows studies of tumor cells in vivo. However, after s.c. injection the incidence of tumor and metastases in nude mice is frequently low. We have studied the tumorigenicity in nude mice of estradiol (E2)-sensitive breast adenocarcinoma MCF7 cells. Matrigel, an extract of basement membrane proteins, induces rapid tumor development after s.c. injection of MCF7 cells. In the absence of this matrice, MCF7 cells failed to induce tumor growth. In this in vivo model, MCF7 cells were analysed for their E2 sensitivity. Two weeks after inoculation in the presence of matrigel, cells formed growing tumors in intact mice supplemented with E2. In ovariectomized or untreated mice, tumor appearance was delayed and the growth level was very low. Thus, MCF7 cells formed tumors in the absence of E2 but retained in vivo their responsiveness to estrogen. Growing human tumors in nude mice provides a rapid and useful model for testing the sensitivity of cells to hormone.

摘要

将人类肿瘤移植到无胸腺裸鼠体内的能力使得在体内研究肿瘤细胞成为可能。然而,皮下注射后,裸鼠体内肿瘤和转移的发生率通常较低。我们研究了对雌二醇(E2)敏感的乳腺腺癌MCF7细胞在裸鼠中的致瘤性。基质胶是一种基底膜蛋白提取物,皮下注射MCF7细胞后可诱导肿瘤快速生长。在没有这种基质的情况下,MCF7细胞无法诱导肿瘤生长。在这个体内模型中,分析了MCF7细胞对E2的敏感性。在有基质胶存在的情况下接种两周后,细胞在补充了E2的完整小鼠体内形成了生长中的肿瘤。在去卵巢或未处理的小鼠中,肿瘤出现延迟且生长水平非常低。因此,MCF7细胞在没有E2的情况下形成肿瘤,但在体内保留了对雌激素的反应性。在裸鼠体内培养人类肿瘤为测试细胞对激素的敏感性提供了一个快速且有用的模型。

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