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细胞活性分解揭示细胞周期在驱动生物功能异质性中的作用。

Decomposition of cell activities revealing the role of the cell cycle in driving biofunctional heterogeneity.

机构信息

Innovation Research Institute of Traditional Chinese Medicine, Shandong University of Traditional Chinese Medicine, Jinan, 250355, Shandong, China.

Department of Chemical Engineering, University of Florida, Gainesville, FL, 32611, USA.

出版信息

Sci Rep. 2021 Dec 6;11(1):23431. doi: 10.1038/s41598-021-02926-4.

Abstract

Heterogeneity of cell phenotypes remains a barrier in progressing cell research and a challenge in conquering cancer-related drug resistance. Cell morphology, the most direct property of cell phenotype, evolves along the progression of the cell cycle; meanwhile, cell motility, the dynamic property of cell phenotype, also alters over the cell cycle. However, a quantifiable research understanding the relationship between the cell cycle and cell migration is missing. Herein, we coordinate the migratory behaviours of NIH 3T3 fibroblasts to their corresponding phases of the cell cycle, the G1, the S, and the G2 phases, and explain the relationship through the spatiotemporal arrangements between the Rho GTPases' signals and cyclin-dependent kinase inhibitors, p21, and p27. Taken together, we demonstrate that both cell morphology and the dynamic subcellular behaviour are homogenous within each stage of the cell cycle phases but heterogenous between phases through quantitative cell analyses and an interactive molecular mechanism between the cell cycle and cell migration, posing potential implications in countering drug resistance.

摘要

细胞表型的异质性仍然是细胞研究进展的障碍,也是克服与癌症相关的耐药性的挑战。细胞形态是细胞表型最直接的特征,它沿着细胞周期的进展而演变;同时,细胞迁移性是细胞表型的动态特征,也会在细胞周期中发生变化。然而,目前缺乏对细胞周期与细胞迁移之间关系的可量化研究。在这里,我们协调 NIH 3T3 成纤维细胞的迁移行为与其细胞周期的相应阶段,即 G1、S 和 G2 期,通过 Rho GTPases 信号和细胞周期蛋白依赖性激酶抑制剂 p21 和 p27 之间的时空排列来解释这种关系。总之,我们通过定量细胞分析和细胞周期与细胞迁移之间的相互作用分子机制证明,细胞形态和细胞内动态行为在细胞周期各阶段内是同质的,但在各阶段之间是异质的,这对对抗耐药性具有潜在意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6b76/8648726/ccca667b4f47/41598_2021_2926_Fig1_HTML.jpg

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