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环磷酸腺苷(cAMP)介导的B淋巴细胞前体细胞系Reh的生长抑制与G2/M期早期短暂延迟相关,随后细胞在G1期积累。

cAMP-mediated growth inhibition of a B-lymphoid precursor cell line Reh is associated with an early transient delay in G2/M, followed by an accumulation of cells in G1.

作者信息

Blomhoff H K, Blomhoff R, Stokke T, deLange Davies C, Brevik K, Smeland E B, Funderud S, Godal T

机构信息

Department of Pathology, The Norwegian Radium Hospital, Oslo.

出版信息

J Cell Physiol. 1988 Dec;137(3):583-7. doi: 10.1002/jcp.1041370327.

Abstract

This study was undertaken to gain more insight into the effects of cyclic adenosine monophosphate (cAMP) on cell-cycle progression in the B-lymphoid precursor cell line Reh. The adenylate cyclase activator forskolin reduced the proliferation of asynchronously growing Reh cells by 50% after 72 hr culture. Growth inhibition was associated with an accumulation of cells in G1. Furthermore, we demonstrated that forskolin provoked a delay of cells for approximately 10 hr in G2/M prior to the G1 arrest. Two different methods were applied to elucidate how cells in different phases of the cell cycle were affected by an elevated cAMP level. One method was based on centrifugal elutriation, whereby synchronous cell populations from the different phases of the cell cycle were isolated. By the other method, S-phase cells were selectively stained by pulsing asynchronously growing cells with bromo-deoxyuridine (BrdU). The data demonstrate that the position of a cell in the cell cycle is critical in determining how the cell will respond to an elevated cAMP level. Thus cells in G1 at the time forskolin is added are not delayed in G2/M, but they will subsequently accumulate in G1 after 48 hr. Cells given forskolin in G2/m, however, are delayed for 10 hr in G2/M, but they do not accumulate in G1. Cells given forskolin in the S phase are delayed in G2/M as well as arrested in G1. The results suggest that cAMP inhibits growth of the Reh cells by preventing the cells from passing important restriction points located in the G1 and G2 phases of the cell cycle.

摘要

本研究旨在更深入地了解环磷酸腺苷(cAMP)对B淋巴细胞前体细胞系Reh细胞周期进程的影响。在培养72小时后,腺苷酸环化酶激活剂福斯高林使异步生长的Reh细胞增殖减少了50%。生长抑制与G1期细胞的积累有关。此外,我们证明福斯高林在G1期阻滞之前,使细胞在G2/M期延迟约10小时。应用两种不同的方法来阐明细胞周期不同阶段的细胞如何受到cAMP水平升高的影响。一种方法基于离心淘析,通过该方法分离出细胞周期不同阶段的同步细胞群体。另一种方法是通过用溴脱氧尿苷(BrdU)脉冲处理异步生长的细胞来选择性标记S期细胞。数据表明,细胞在细胞周期中的位置对于确定细胞如何响应升高的cAMP水平至关重要。因此,在添加福斯高林时处于G1期的细胞不会在G2/M期延迟,但在48小时后它们会在G1期积累。然而,在G2/M期给予福斯高林的细胞在G2/M期延迟10小时,但它们不会在G1期积累。在S期给予福斯高林的细胞在G2/M期延迟并且在G1期停滞。结果表明,cAMP通过阻止细胞通过位于细胞周期G1期和G2期的重要限制点来抑制Reh细胞的生长。

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