YAP 的活化对稀释作用很强

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC ACS Applied Electronic Materials Pub Date : 2024-08-14 DOI:10.1039/D4MO00100A
Ian Jones, Mar Arias-Garcia, Patricia Pascual-Vargas, Melina Beykou, Lucas Dent, Tara Pal Chaudhuri, Theodoros Roumeliotis, Jyoti Choudhary, Julia Sero and Chris Bakal
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摘要

由于合成、降解和细胞大小的不同,许多转录因子在细胞间的浓度变化很大。人们对这些因子的功能是否受浓度波动的影响以及如何实现这一点知之甚少。在两组独立的乳腺癌细胞中,我们发现 YAP 的平均全细胞浓度随着细胞面积的增加而降低。然而,在按大小分组的细胞中,核浓度分布在约 4-8 倍的大小范围内保持不变,这意味着尽管细胞范围内的浓度下降,核转位却没有受到干扰。在 DNA 和 CycA/PCNA 表达较多的细胞中,全细胞浓度和核浓度都较高,这表明 YAP 在细胞周期中的周期性合成抵消了细胞生长和/或细胞扩散造成的稀释。细胞面积与 YAP 的比例关系扩展到黑色素瘤和 RPE 细胞。对成像和磷酸蛋白组数据的综合分析表明,不同细胞系的平均核YAP浓度可通过RAS/MAPK信号传导、病灶粘附成熟和核转运过程的差异来预测。对MEK或CDK4/6的化学抑制增加了YAP的平均核浓度,验证了RAS/MAPK和细胞周期调控YAP转位的观点。总之,这项研究提供了一个实例,说明蛋白质的细胞质稀释(例如通过细胞生长)并不会限制同源的细胞功能。在这里,同样的蛋白质转位到细胞核中。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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YAP activation is robust to dilution†

The concentration of many transcription factors exhibits high cell-to-cell variability due to differences in synthesis, degradation, and cell size. Whether the functions of these factors are robust to fluctuations in concentration, and how this may be achieved, is poorly understood. Across two independent panels of breast cancer cells, we show that the average whole cell concentration of YAP decreases as a function of cell area. However, the nuclear concentration distribution remains constant across cells grouped by size, across a 4–8 fold size range, implying unperturbed nuclear translocation despite the falling cell wide concentration. Both the whole cell and nuclear concentration was higher in cells with more DNA and CycA/PCNA expression suggesting periodic synthesis of YAP across the cell cycle offsets dilution due to cell growth and/or cell spreading. The cell area – YAP scaling relationship extended to melanoma and RPE cells. Integrative analysis of imaging and phospho-proteomic data showed the average nuclear YAP concentration across cell lines was predicted by differences in RAS/MAPK signalling, focal adhesion maturation, and nuclear transport processes. Validating the idea that RAS/MAPK and cell cycle regulate YAP translocation, chemical inhibition of MEK or CDK4/6 increased the average nuclear YAP concentration. Together, this study provides an example case, where cytoplasmic dilution of a protein, for example through cell growth, does not limit a cognate cellular function. Here, that same proteins translocation into the nucleus.

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来源期刊
CiteScore
7.20
自引率
4.30%
发文量
567
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