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表型异质性遵循生长-活力权衡,以响应氨基酸同一性。

Phenotypic heterogeneity follows a growth-viability tradeoff in response to amino acid identity.

机构信息

Department of Bioengineering and Imperial College Centre for Synthetic Biology, Imperial College London, London, SW7 2AZ, UK.

London Biofoundry, Imperial College Translation & Innovation Hub, London, UK.

出版信息

Nat Commun. 2024 Aug 2;15(1):6515. doi: 10.1038/s41467-024-50602-8.

Abstract

In their natural environments, microorganisms mainly operate at suboptimal growth conditions with fluctuations in nutrient abundance. The resulting cellular adaptation is subject to conflicting tasks: growth or survival maximisation. Here, we study this adaptation by systematically measuring the impact of a nitrogen downshift to 24 nitrogen sources on cellular metabolism at the single-cell level. Saccharomyces lineages grown in rich media and exposed to a nitrogen downshift gradually differentiate to form two subpopulations of different cell sizes where one favours growth while the other favours viability with an extended chronological lifespan. This differentiation is asymmetrical with daughter cells representing the new differentiated state with increased viability. We characterise the metabolic response of the subpopulations using RNA sequencing, metabolic biosensors and a transcription factor-tagged GFP library coupled to high-throughput microscopy, imaging more than 800,000 cells. We find that the subpopulation with increased viability is associated with a dormant quiescent state displaying differences in MAPK signalling. Depending on the identity of the nitrogen source present, differentiation into the quiescent state can be actively maintained, attenuated, or aborted. These results establish amino acids as important signalling molecules for the formation of genetically identical subpopulations, involved in chronological lifespan and growth rate determination.

摘要

在自然环境中,微生物主要在营养物质丰度波动的亚最优生长条件下运作。由此产生的细胞适应受到相互冲突的任务的影响:生长或生存的最大化。在这里,我们通过系统地测量在单细胞水平上氮减少到 24 种氮源对细胞代谢的影响来研究这种适应。在富含营养的培养基中生长并暴露于氮减少的酿酒酵母谱系逐渐分化为两种不同细胞大小的亚群,其中一种有利于生长,而另一种有利于具有延长的时序寿命的生存能力。这种分化是不对称的,子细胞代表具有更高生存能力的新分化状态。我们使用 RNA 测序、代谢生物传感器和转录因子标记 GFP 文库结合高通量显微镜来表征亚群的代谢反应,对超过 800,000 个细胞进行成像。我们发现,具有更高生存能力的亚群与休眠静止状态相关,表现出 MAPK 信号的差异。根据存在的氮源的身份,向静止状态的分化可以被主动维持、减弱或中止。这些结果将氨基酸确立为形成遗传上相同的亚群的重要信号分子,参与时序寿命和生长速率的决定。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/33ad/11297284/25db312b00fd/41467_2024_50602_Fig1_HTML.jpg

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