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转染c-Ha-Ras的人Caco-2细胞作为大肠内分泌分化的模型。

Human Caco-2 cells transfected with c-Ha-Ras as a model for endocrine differentiation in the large intestine.

作者信息

de Bruïne A P, de Vries J E, Dinjens W N, Moerkerk P T, van der Linden E P, Pijls M M, ten Kate J, Bosman F T

机构信息

Department of Pathology, University Hospital Maastricht, The Netherlands.

出版信息

Differentiation. 1993 May;53(1):51-60. doi: 10.1111/j.1432-0436.1993.tb00645.x.

Abstract

Endocrine cells occur in approximately 30% of all colorectal adenocarcinomas, and this feature appears to correlate with a relatively poor prognosis. To study the factors regulating endocrine differentiation in colorectal cancer, which may bear resemblance to the regulation of endocrine differentiation in normal intestinal mucosa, models in which differentiation can be manipulated are essential. However, endocrine features in colorectal cancer cell lines are scarce and are almost exclusively observed in xenografts, presumably as a result of differentiation induction by stromal components. We attempted to demonstrate endocrine differentiation in the colonic adenocarcinoma cell line Caco-2, which is frequently used as a model for enterocytic differentiation. In vitro endocrine tumor cells were not encountered. In vivo studies were cumbersome, because of the low take rate of Caco-2 cells. We did manage to establish nude mouse xenografts of Caco-2 cells by inoculating cells in collagen gel and by suppressing natural killer cell activity. In an attempt to induce a better take rate and to investigate the effect of Ras oncoprotein overexpression on endocrine differentiation, Caco-2 cells were transfected with a point-mutated c-Ha-Ras gene. The cell line Caco-2 EJ6, generated from these experiments, could be xenografted in nude mice with a high take rate, yielding a moderately well differentiated adenocarcinoma, morphologically identical to the tumors derived from untransfected Caco-2 cells. The xenografts displayed goblet cell, enterocytic, Paneth cell and endocrine differentiation. In vitro endocrine differentiation was observed neither under standard conditions nor with extracellular matrix components as differentiation inducers. We conclude that the Caco-2 cell line and its c-Ha-Ras transfected subline Caco-2 EJ6 in vivo display endocrine differentiation. Ras overexpression does not enhance endocrine differentiation. Due to its favorable growth properties in vivo, Caco-2 EJ6 is a suitable model for studies on endocrine differentiation in colorectal cancer.

摘要

内分泌细胞出现在约30%的结直肠癌中,这一特征似乎与相对较差的预后相关。为了研究调节结直肠癌内分泌分化的因素,这些因素可能与正常肠黏膜内分泌分化的调节相似,能够操纵分化的模型至关重要。然而,结直肠癌细胞系中的内分泌特征稀少,几乎仅在异种移植中观察到,推测这是基质成分诱导分化的结果。我们试图在结肠腺癌细胞系Caco-2中证明内分泌分化,该细胞系常用于肠细胞分化模型。在体外未遇到内分泌肿瘤细胞。由于Caco-2细胞的接种成功率低,体内研究很麻烦。我们通过在胶原凝胶中接种细胞并抑制自然杀伤细胞活性,成功建立了Caco-2细胞的裸鼠异种移植模型。为了提高接种成功率并研究Ras癌蛋白过表达对内分泌分化的影响,用点突变的c-Ha-Ras基因转染Caco-2细胞。从这些实验中产生的细胞系Caco-2 EJ6能够以高接种成功率异种移植到裸鼠中,产生中度分化良好的腺癌,形态上与未转染的Caco-2细胞衍生的肿瘤相同。异种移植显示有杯状细胞、肠细胞、潘氏细胞和内分泌分化。在标准条件下以及用细胞外基质成分作为分化诱导剂时,均未观察到体外内分泌分化。我们得出结论,Caco-2细胞系及其c-Ha-Ras转染的亚系Caco-2 EJ6在体内显示内分泌分化。Ras过表达不会增强内分泌分化。由于其在体内良好的生长特性,Caco-2 EJ6是研究结直肠癌内分泌分化的合适模型。

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