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5-溴脱氧尿苷在S期早期掺入对Friend小鼠红白血病细胞生长和分化的扰动

Perturbation of growth and differentiation of Friend murine erythroleukemia cells by 5-bromodeoxyuridine incorporation in early S phase.

作者信息

Brown E H, Schildkraut C L

出版信息

J Cell Physiol. 1979 May;99(2):261-78. doi: 10.1002/jcp.1040990213.

Abstract

Cultured Friend murine erythroleukemia cells (Friend cells) are induced to undergo erythroid differentiation when grown in the presence of dimethylsulfoxide (DMSO) and other compounds. The effects of unifilar substitution of bromouracil (BU) for thymidine in the DNA (BU-DNA) of Friend cells were examined. Cells were grown in the presence of 5-bromodeoxy-uridine (BrdU) for one generation, then centrifuged and resuspended in medium containing DMSO without BrdU. These cells exhibited a delay in the appearance of heme-producing, benzidine-reative (B+) cells and a decreased rate of cell proliferation in comparison to the control not containing BU-DNA. A transient inhibition of entry into S phase was observed when control cells or cells containing BU-DNA were grown in the presence of DMSO) for 10 to 20 hours. This transient inhibition was increased in the BrdU culture. Thus BU-substitution in Friend cells alters other cellular functions in addition to erythroid differentiation. The rate of increase in the percent of cells committed to differentiate (those forming B+ colonies in plasma clots) was similar in the BrdU and control cultures until 40 to 50 hours. After this time, a delay in the appearance of committed cells was observed in the BrdU culture. The effect of BrdU on the appearance of B+ cells was more pronounced and occurred earlier than its effect on the rate of commitment. Therefore, the delay in the appearance of B+ cells in the BrdU culture was due primarily to perturbation of post-commitment events such as the accumulation of hemoglobin. We also examined the effect on growth and differentiation after BrdU was incorporated during different intervals of S phase in cells synchronized by centrifugal elutriation or by double thymidine block and hydroxyurea treatment. The delay in the appearance of B+ cells and inhibition of cell proliferation were only observed when BrdU was incorporated in the first half of S phase. BrdU (10 muM) had no effect on growth or differentiation when present during late S or G1 and G2. These results, using two very different methods to achieve cell synchrony, indicate that the effects of BrdU on growth and differentiation described above are due to its incorporation into DNA sequences replicating during early S.

摘要

培养的弗氏小鼠红白血病细胞(弗氏细胞)在二甲基亚砜(DMSO)和其他化合物存在下生长时会被诱导进行红系分化。研究了在弗氏细胞的DNA中用溴尿嘧啶(BU)单链取代胸腺嘧啶的影响(BU-DNA)。细胞在5-溴脱氧尿苷(BrdU)存在下生长一代,然后离心并重悬于不含BrdU的含DMSO的培养基中。与不含BU-DNA的对照相比,这些细胞中产生血红素的、联苯胺反应阳性(B+)细胞的出现延迟,细胞增殖速率降低。当对照细胞或含BU-DNA的细胞在DMSO存在下生长10至20小时时,观察到进入S期的短暂抑制。在BrdU培养物中这种短暂抑制增强。因此,弗氏细胞中的BU取代除了影响红系分化外,还改变了其他细胞功能。在BrdU培养物和对照培养物中,直到40至50小时,承诺分化的细胞百分比(在血浆凝块中形成B+集落的细胞)的增加速率相似。在此之后,在BrdU培养物中观察到承诺细胞出现延迟。BrdU对B+细胞出现的影响比其对承诺速率的影响更明显且更早发生。因此,BrdU培养物中B+细胞出现延迟主要是由于承诺后事件的扰动,如血红蛋白的积累。我们还研究了在通过离心淘析或双胸腺嘧啶阻断和羟基脲处理同步化的细胞中,在S期不同间隔掺入BrdU后对生长和分化的影响。仅当在S期上半段掺入BrdU时,才观察到B+细胞出现延迟和细胞增殖抑制。当在S期末期或G1期和G2期存在时,10μM的BrdU对生长或分化没有影响。使用两种非常不同的方法实现细胞同步化的这些结果表明,上述BrdU对生长和分化的影响是由于其掺入早期S期复制的DNA序列中。

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