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利用免疫染色对正常细胞和转化细胞中X射线及热诱导产生的多个微管组织中心进行定量分析。

The use of immunostaining to quantify x-ray and heat-induced multiple microtubule organizing centers in normal and transformed cells.

作者信息

Lobreau A U, Raaphorst G P, Szekely J G

机构信息

Medical Biophysics Branch, Atomic Energy of Canada Limited Research Company, Manitoba.

出版信息

Basic Appl Histochem. 1988;32(2):263-78.

PMID:3046599
Abstract

Microtubule organizing centers (MTOC) in control, irradiated and heated C3H 10T1/2 mouse embryo cells and two radiation-transformed sublines, R1 and R25, were made visible by indirect immunofluorescence using antibody against tubulin. The MTOC were reformed by 5-min incubation in fresh medium after the microtubules were depolymerized with nocodazole. The R1 line had a different distribution of MTOC/cell than the parent 10T1/2 line or R25, which had similar distributions. After irradiation, multiple MTOC appeared in the normal and radiation-transformed cells irradiated to 10 Gy and incubated for 24 or 48 h. The multiple foci of microtubule reformation in the irradiated cells indicate that radiation damage is expressed in structural elements in the cytoplasm. After heat treatment of the three cell lines (43 degrees C for 93 min and 45 degrees C for 25 min), the MTOC were disrupted and many cells did not have visible organizing centers at 24 or 48 h, while others had a large number of small centers of microtubule reformation. The distribution of MTOC/cell seen in R25 cells after the treatment had similar patterns to those of the 10T1/2 line rather than to those of the other radiation-transformed line, R1. Thus, the radiation or heat response seen in the MTOC is not dependent upon cell transformation.

摘要

使用抗微管蛋白抗体通过间接免疫荧光法使对照、辐照和加热处理后的C3H 10T1/2小鼠胚胎细胞以及两个辐射转化亚系R1和R25中的微管组织中心(MTOC)可见。在用诺考达唑使微管解聚后,通过在新鲜培养基中孵育5分钟使MTOC重新形成。R1亚系细胞中MTOC/细胞的分布与亲代10T1/2细胞系或R25不同,而后两者的分布相似。辐照后,接受10 Gy辐照并孵育24或48小时的正常细胞和辐射转化细胞中出现了多个MTOC。辐照细胞中微管重新形成的多个焦点表明辐射损伤在细胞质的结构成分中得以体现。对这三种细胞系进行热处理(43℃处理93分钟和45℃处理25分钟)后,MTOC被破坏,许多细胞在24或48小时时没有可见的组织中心,而其他细胞则有大量小的微管重新形成中心。处理后在R25细胞中观察到的MTOC/细胞分布模式与10T1/2细胞系相似,而与另一个辐射转化细胞系R1不同。因此,在MTOC中观察到的辐射或热反应并不依赖于细胞转化。

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