首页> 美国卫生研究院文献>The Journal of Biophysical and Biochemical Cytology >Manipulation of cell-cell and cell-substratum interactions in mouse mammary tumor epithelial cells using broad spectrum antisera
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Manipulation of cell-cell and cell-substratum interactions in mouse mammary tumor epithelial cells using broad spectrum antisera

机译:使用广谱抗血清处理小鼠乳腺肿瘤上皮细胞中的细胞-细胞和细胞-基质相互作用

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摘要

Two antisera were raised in goats against material shed by two different mammary epithelial cell lines into serum-free culture medium. These antisera, when added to the medium of intact, growing mouse mammary tumor cells in the absence of complement, cause distinct and dramatic alterations in cell morphology and adhesiveness. One antiserum (anti-SFM I) causes mouse mammary tumor epithelial cells to round and detach from the substratum. Treatment with the other antiserum (anti- SFM II) does not affect cell-substratum interactions, but causes the cells to convert from an epitheloid to a fibroblastic morphology. Statistical analysis of transmission electron micrographs of control and antibody-treated cells indicates that treatment with anti-SFM II is associated with a substantial reduction in the extent of intercellular junctions, particularly desmosomes. To identify the components with which the two antisera interact, nonionic detergent extracts of mouse mammary tumor cells were fractionated, and the ability of various fractions to block the morphological effects of either antiserum was determined. The whole Nonidet P40 (NP40) extract of the epithelial cells blocked the effects of both antisera. After the extract was subjected to ion exchange and lectin affinity chromatography, two separate fractions were obtained. One fraction blocks and anti-SFM I induced rounding and detachment of cells from the substratum. The second fraction blocks the effects of both antisera. The isolation of the former fraction, which has highly restricted number of components, represents a significant first step toward identifying the surface membrane molecule(s) involved in cell-substratum adhesion in epithelial cells.
机译:针对两种不同的乳腺上皮细胞系脱落的物质,在山羊体内培养了两种抗血清,将其制成无血清培养基。当将这些抗血清添加到完整的,在没有补体的情况下生长的小鼠乳腺肿瘤细胞的培养基中时,会引起细胞形态和粘附性的明显变化。一种抗血清(抗SFM I)可导致小鼠乳腺肿瘤上皮细胞变圆并脱离基质。用其他抗血清(抗SFM II)处理不会影响细胞-基质相互作用,但会导致细胞从表皮转化为成纤维细胞形态。对照和经抗体处理的细胞的透射电子显微照片的统计分析表明,用抗SFM II处理与细胞间连接,尤其是桥粒连接程度的显着降低有关。为了鉴定与两种抗血清相互作用的成分,将小鼠乳腺肿瘤细胞的非离子去污剂提取物进行分级,并确定了各种级分阻断任一抗血清的形态学作用的能力。上皮细胞的整个Nonidet P40(NP40)提取物均阻断了两种抗血清的作用。将提取物进行离子交换和凝集素亲和层析后,获得两个分离的级分。一小部分阻滞和抗SFM I诱导细胞从基底圆化和脱离。第二部分阻断两种抗血清的作用。前一部分的分离具有高度受限的成分数量,是朝着鉴定上皮细胞中细胞-基质粘附所涉及的表面膜分子迈出的重要第一步。

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