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The birth and death of proteins in a single cell
admin
2018-08-23
发布年2018
语种英语
国家美国
领域地球科学
正文(英文)
Embryonic stem cells expressing a fluorescent timer fused to the endogenous LaminB1 protein, which coats the nuclear envelope. Credit: Andrea Alber

The amount of proteins inside cells fluctuates over time, and this affects various functions of the cells. Cells are constantly synthesizing and degrading proteins, and studies have shown that this "see-saw" effect actually impacts the function of the cell.

When it comes to stem cells, the constant variation of transcription factors (proteins that regulate the expression of genes) has important consequences on their ability to differentiate into . But it is not well understood how and degradation work together to regulate these fluctuations.

The lab of David Suter at EPFL, in collaboration with the team of Félix Naef, has now developed a new method that can distinguish changes in protein synthesis from changes in protein degradation in single living cells. The method, published in Molecular Cell, uses a fluorescent timer combined with pulse-chase fluorescent labelling, which is a technique that can track a cellular process occurring over time.

Using their new method, the scientists made two discoveries. First, that protein synthesis and degradation rates change significantly during the cell cycle, with almost half of them stopping to be degraded during mitosis.

The second discovery was that rates differ largely between . This variability affects all proteins to a similar extent, suggesting fluctuations in the activity of proteasomes—the protein complexes that degrade unneeded or damaged proteins. Remarkably, these differences are offset by corresponding changes in protein synthesis rates, thereby minimizing variability in protein expression levels between .

"Think of it as two factories," explains David Suter. "Factory A makes a lot of bad quality product X, meaning they are quickly out of order. Factory B makes less of high-quality product Y, which works for a longer period of time."

Explore further: Similarities between the two gap phases of the cell cycle indicate a default biochemical program in living cells

More information: Andrea Brigitta Alber, Eric Raphael Paquet, Martina Biserni, Felix Naef, David Michael Suter. Single live cell monitoring of protein turnover reveals intercellular variability and cell cycle dependence of degradation rates. Molecular Cell 23 August 2018. DOI: 10.1016/j.molcel.2018.07.023

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来源平台Science X network
文献类型新闻
条目标识符http://119.78.100.173/C666/handle/2XK7JSWQ/114839
专题地球科学
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