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地塞米松和依托泊苷可诱导处于细胞周期不同阶段的大鼠胸腺细胞凋亡。

Dexamethasone and etoposide induce apoptosis in rat thymocytes from different phases of the cell cycle.

作者信息

Fearnhead H O, Chwalinski M, Snowden R T, Ormerod M G, Cohen G M

机构信息

MRC Toxicology Unit, University of Leicester, U.K.

出版信息

Biochem Pharmacol. 1994 Sep 15;48(6):1073-9. doi: 10.1016/0006-2952(94)90142-2.

Abstract

Dexamethasone and etoposide both induce apoptosis in immature rat thymocytes. We investigated the dependence of apoptosis on the phase of the cell cycle after incubation with these drugs. Cell cycle progression was followed by a combination of pulse labelling with 5-bromo-2'-deoxyuridine (BrdU), labelling fixed cells with an anti-BrdU antibody and flow cytometry. Dexamethasone had little effect on the cell cycle progression of proliferating thymocytes, while etoposide caused cell cycle arrest. Normal and apoptotic thymocytes were separated by centrifugation on discontinuous Percoll gradients into four fractions (F1-F4). It was found that both dexamethasone and etoposide induced apoptosis in cells in G0/G1 and G2/M of the cell cycle, whereas only etoposide induced apoptosis of cells in S phase. These results demonstrated that dexamethasone induced apoptosis in quiescent cells while only etoposide could induce apoptosis in cells from the proliferative compartment. Following treatment of thymocytes with etoposide, some of the proliferating thymocytes (F1) were converted to cells with intermediate size and density (F3). We have recently identified these cells as a population of preapoptotic thymocytes, at an early stage of apoptosis. These cells then further progressed to fully apoptotic cells (F4). These data support the hypothesis that normal thymocytes (F1) became apoptotic (F4) via an intermediate population (F3).

摘要

地塞米松和依托泊苷均可诱导未成熟大鼠胸腺细胞凋亡。我们研究了用这些药物孵育后凋亡对细胞周期阶段的依赖性。通过用5-溴-2'-脱氧尿苷(BrdU)进行脉冲标记、用抗BrdU抗体标记固定细胞以及流式细胞术相结合的方法来跟踪细胞周期进程。地塞米松对增殖性胸腺细胞的细胞周期进程影响很小,而依托泊苷导致细胞周期停滞。通过在不连续的Percoll梯度上离心,将正常和凋亡的胸腺细胞分离为四个组分(F1 - F4)。发现地塞米松和依托泊苷均可诱导细胞周期G0/G1期和G2/M期的细胞凋亡,而只有依托泊苷可诱导S期细胞凋亡。这些结果表明,地塞米松诱导静止细胞凋亡,而只有依托泊苷可诱导增殖区室的细胞凋亡。用依托泊苷处理胸腺细胞后,一些增殖性胸腺细胞(F1)转变为具有中等大小和密度的细胞(F3)。我们最近将这些细胞鉴定为处于凋亡早期的预凋亡胸腺细胞群体。这些细胞随后进一步发展为完全凋亡的细胞(F4)。这些数据支持正常胸腺细胞(F1)通过中间群体(F3)转变为凋亡细胞(F4)这一假说。

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