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Single Cell Analysis of Yeast Replicative Aging Using a New Generation of Microfluidic Device

Overview of attention for article published in PLOS ONE, November 2012
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Title
Single Cell Analysis of Yeast Replicative Aging Using a New Generation of Microfluidic Device
Published in
PLOS ONE, November 2012
DOI 10.1371/journal.pone.0048275
Pubmed ID
Authors

Yi Zhang, Chunxiong Luo, Ke Zou, Zhengwei Xie, Onn Brandman, Qi Ouyang, Hao Li

Abstract

A major limitation to yeast aging study has been the inability to track mother cells and observe molecular markers during the aging process. The traditional lifespan assay relies on manual micro-manipulation to remove daughter cells from the mother, which is laborious, time consuming, and does not allow long term tracking with high resolution microscopy. Recently, we have developed a microfluidic system capable of retaining mother cells in the microfluidic chambers while removing daughter cells automatically, making it possible to observe fluorescent reporters in single cells throughout their lifespan. Here we report the development of a new generation of microfluidic device that overcomes several limitations of the previous system, making it easier to fabricate and operate, and allowing functions not possible with the previous design. The basic unit of the device consists of microfluidic channels with pensile columns that can physically trap the mother cells while allowing the removal of daughter cells automatically by the flow of the fresh media. The whole microfluidic device contains multiple independent units operating in parallel, allowing simultaneous analysis of multiple strains. Using this system, we have reproduced the lifespan curves for the known long and short-lived mutants, demonstrating the power of the device for automated lifespan measurement. Following fluorescent reporters in single mother cells throughout their lifespan, we discovered a surprising change of expression of the translation elongation factor TEF2 during aging, suggesting altered translational control in aged mother cells. Utilizing the capability of the new device to trap mother-daughter pairs, we analyzed mother-daughter inheritance and found age dependent asymmetric partitioning of a general stress response reporter between mother and daughter cells.

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Geographical breakdown

Country Count As %
United States 5 3%
China 2 1%
Canada 1 <1%
Switzerland 1 <1%
Spain 1 <1%
France 1 <1%
Unknown 147 93%

Demographic breakdown

Readers by professional status Count As %
Student > Ph. D. Student 46 29%
Researcher 31 20%
Student > Bachelor 18 11%
Student > Master 17 11%
Student > Doctoral Student 9 6%
Other 21 13%
Unknown 16 10%
Readers by discipline Count As %
Agricultural and Biological Sciences 59 37%
Biochemistry, Genetics and Molecular Biology 43 27%
Engineering 16 10%
Physics and Astronomy 6 4%
Chemistry 4 3%
Other 11 7%
Unknown 19 12%