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正常及转化成纤维细胞的细胞周期依赖性凝集性、伴刀豆球蛋白A结合位点分布及表面形态

Cell cycle dependent agglutinability, distribution of concanavalin A binding sites and surface morphology of normal and transformed fibroblasts.

作者信息

Collard J G, Temmink J H

出版信息

Adv Exp Med Biol. 1975;55:221-44. doi: 10.1007/978-1-4684-0949-9_12.

DOI:10.1007/978-1-4684-0949-9_12
PMID:168744
Abstract

In studies on phenotypic reversion of transformed cells to normal growth patterns, we investigated the effect of dibutyryl cyclic AMP (dbc-AMP) and a protease inhibitor (TLCK) on growth of SV40-transformed mouse fibroblasts (3T3). The results did not support the hypothesis that transformed cells grown with dbc-AMP or TLCK are induced to contact-mediated growth control. The growth rate of SV-3T3 cells grown with the drugs was strongly reduced, due to accumulation of the cells in the G2 phase of the cell cycle. In addition, decreased agglutinability with concanavalin A (Con A) of those SV-3T3 cells was not caused by a direct effect of the drugs on the cell surface, but by partial synchronization of the cells in the G2 phase of the cycle. In synchronized cultures agglutinability of transformed cells reached a minimum in G2 and was maximal in mitosis and G1. Normal cells agglutinated only in mitosis. This suggested that agglutinability of cells is somehow cell cycle dependent. Cytochemical investigations on normal and transformed 3T3 cells had shown that Con A-induced redistribution of binding sites on the surface of these cells is not correlated with agglutinability. The present work on replicas confirmed this, but indicated also that normal 3T3 cells have more extended lamellipodia with less Con A binding sites than SV-3T3 cells. Preliminary scanning electron microscope data showed cell cycle dependent changes in 3T3 cells and also showed that confluent 3T3 and SV-3T3 cells suspended for agglutination tests had a different surface morphology. These results may represent additional factors important for differences in cell agglutinability by Con A.

摘要

在关于转化细胞向正常生长模式表型逆转的研究中,我们研究了二丁酰环磷腺苷(dbc - AMP)和一种蛋白酶抑制剂(TLCK)对SV40转化的小鼠成纤维细胞(3T3)生长的影响。结果不支持这样的假说,即与dbc - AMP或TLCK一起培养的转化细胞会被诱导进行接触介导的生长控制。用这些药物培养的SV - 3T3细胞的生长速率大幅降低,这是由于细胞在细胞周期的G2期积累所致。此外,那些SV - 3T3细胞与伴刀豆球蛋白A(Con A)的凝集性降低并非由药物对细胞表面的直接作用引起,而是由细胞在周期的G2期部分同步化导致的。在同步培养中,转化细胞的凝集性在G2期达到最低,在有丝分裂期和G1期达到最高。正常细胞仅在有丝分裂期凝集。这表明细胞的凝集性在某种程度上依赖于细胞周期。对正常和转化的3T3细胞的细胞化学研究表明,Con A诱导的这些细胞表面结合位点的重新分布与凝集性无关。关于复制品的当前研究证实了这一点,但也表明正常3T3细胞比SV - 3T3细胞具有更伸展的片状伪足且Con A结合位点更少。初步的扫描电子显微镜数据显示了3T3细胞中依赖于细胞周期的变化,并且还表明用于凝集试验而悬浮的汇合3T3和SV - 3T3细胞具有不同的表面形态。这些结果可能代表了对Con A引起的细胞凝集性差异很重要的其他因素。

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引用本文的文献

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Distribution of concanavalin A binding sites on normal human urinary bladder mucosa and bladder tumors by transmission and scanning electron microscopy and X-ray microanalysis.通过透射电子显微镜、扫描电子显微镜和X射线微分析研究伴刀豆球蛋白A结合位点在正常人类膀胱黏膜和膀胱肿瘤上的分布。
Urol Res. 1984;12(2):135-41. doi: 10.1007/BF00257180.