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大鼠腹水肝癌细胞与培养的间皮细胞层的相互作用:肿瘤侵袭模型

Interaction of rat ascites hepatoma cells with cultured mesothelial cell layers: a model for tumor invasion.

作者信息

Akedo H, Shinkai K, Mukai M, Mori Y, Tateishi R, Tanaka K, Yamamoto R, Morishita T

出版信息

Cancer Res. 1986 May;46(5):2416-22.

PMID:3697985
Abstract

Interactions of rat ascites hepatoma cells with primary cultured layers of rat mesentery-derived cells were studied. The mesentery-derived cells were isolated from rat mesentery and cultured in Eagle's minimum essential medium with a 2-fold concentration of amino acids and vitamins supplemented with 10% calf serum. The primary cultured cells, consisting mainly of mesothelial cells in polygonal shape, forms a "paving stone" sheet. Upon seeding the tumor cells on the mesentery-derived cell layers, three different types of tumor cell growth were observed. Type 1 was the formation of piled-up tumor cell nests on mesothelial cell layers. Type 2 was the formation of flattened tumor cell islands underneath mesothelial cell layers. This island formation was clearly observed under a phase contrast microscope 2 days after the tumor cell seeding. Protrusion of cellular processes of the tumor cells beneath mesothelial cells was occasionally seen. Type 3 was the growth of tumor cells in suspension. These types of tumor cell growth closely resemble those in the peritoneal cavity observed after i.p. implantation of the tumor cells. When the tumor cells recovered from the blood of tumor-bearing rats were seeded, flattened tumor cell islands were formed 15 times more frequently than when the tumor cells isolated from host peritoneal cavity were seeded. Shortly after the appearance of small flattened tumor cell islands, a distinct morphological change of mesothelial cells from polygonal to spindle shape was seen preferentially at the marginal area of the cell layers (a partial retraction of cell edges). The retraction of mesothelial cells was induced not only by seeding the tumor cells but by adding the tumor ascites fluid or the medium conditioned by the tumor cell culture. The morphological change was reversed by changing the culture medium to remove the effectors. These results indicate that the system described in this study can provide a useful model to study tumor cell invasion.

摘要

研究了大鼠腹水肝癌细胞与大鼠肠系膜来源细胞原代培养层之间的相互作用。从大鼠肠系膜中分离出肠系膜来源细胞,并在含有两倍浓度氨基酸和维生素且补充有10%小牛血清的伊格尔最低必需培养基中培养。原代培养细胞主要由多边形间皮细胞组成,形成“铺路石”样薄片。将肿瘤细胞接种到肠系膜来源细胞层上后,观察到三种不同类型的肿瘤细胞生长。类型1是在间皮细胞层上形成堆积的肿瘤细胞巢。类型2是在间皮细胞层下方形成扁平的肿瘤细胞岛。在接种肿瘤细胞2天后,在相差显微镜下可清楚观察到这种岛状形成。偶尔可见间皮细胞下方肿瘤细胞的细胞突起。类型3是肿瘤细胞悬浮生长。这些类型的肿瘤细胞生长与腹腔内接种肿瘤细胞后观察到的生长非常相似。当接种从荷瘤大鼠血液中回收的肿瘤细胞时,形成扁平肿瘤细胞岛的频率比接种从宿主腹腔分离的肿瘤细胞时高15倍。在小的扁平肿瘤细胞岛出现后不久,优先在细胞层边缘区域观察到间皮细胞从多边形到纺锤形的明显形态变化(细胞边缘部分回缩)。间皮细胞的回缩不仅由接种肿瘤细胞引起,还由添加肿瘤腹水或肿瘤细胞培养条件培养基引起。通过更换培养基去除效应物可使形态变化逆转。这些结果表明,本研究中描述的系统可为研究肿瘤细胞侵袭提供有用的模型。

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