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使用RO3306在RPE-1细胞中从G2/M期检查点进行可控退出:富集特定阶段细胞群体以深入分析有丝分裂事件。

Controlled Exit from the G2/M Checkpoint in RPE-1 Cells Using RO3306: Enrichment of Phase-Specific Cell Populations for In-Depth Analyses of Mitotic Events.

作者信息

Anglada Teresa, Pulido-Artola Núria, Rodriguez-Muñoz Marina, Genesca Anna

机构信息

Department of Cell Biology, Physiology, and Immunology, Universitat Autònoma de Barcelona, 08193 Barcelona, Spain.

出版信息

Int J Mol Sci. 2025 May 21;26(10):4951. doi: 10.3390/ijms26104951.

Abstract

Studying the cell cycle is essential for understanding the molecular mechanisms that regulate cell division, growth, and differentiation in living organisms. However, mitosis constitutes only a brief phase of the overall cell cycle, making its analysis challenging in asynchronous cell populations due to its transient and dynamic nature. Cell synchronization methods help to enrich populations at specific cell cycle stages, including mitosis, typically by using chemical inhibitors to arrest cells at defined checkpoints. However, many existing protocols rely on combinations of inhibitors that interfere with normal mitotic progression, disrupting dynamics and causing side effects such as chromosome non-disjunction or lagging chromosomes, which limit their applicability. In this study, we present an RO3306 block-and-release strategy to selectively enrich cell populations at defined mitotic stages without compromising cell viability or disrupting their progression to mitotic exit. This approach provides a reliable method for studying mitotic events with high temporal resolution. Furthermore, by preserving mitotic integrity, it offers a valuable framework for investigating the molecular mechanisms of cell division and the processes driving genomic instability in human cells.

摘要

研究细胞周期对于理解调节生物体细胞分裂、生长和分化的分子机制至关重要。然而,有丝分裂仅占整个细胞周期的一个短暂阶段,由于其短暂和动态的性质,在异步细胞群体中对其进行分析具有挑战性。细胞同步化方法有助于在特定细胞周期阶段富集细胞群体,包括有丝分裂阶段,通常是通过使用化学抑制剂在特定检查点阻滞细胞。然而,许多现有方案依赖于干扰正常有丝分裂进程的抑制剂组合,破坏动态过程并导致诸如染色体不分离或滞后染色体等副作用,这限制了它们的适用性。在本研究中,我们提出了一种RO3306阻滞与释放策略,以在不损害细胞活力或不破坏其进入有丝分裂退出进程的情况下,在特定有丝分裂阶段选择性富集细胞群体。这种方法为以高时间分辨率研究有丝分裂事件提供了一种可靠的方法。此外,通过保持有丝分裂的完整性,它为研究细胞分裂的分子机制以及驱动人类细胞基因组不稳定的过程提供了一个有价值的框架。

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