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Long-term microfluidic tracking of coccoid cyanobacterial cells reveals robust control of division timing

Overview of attention for article published in BMC Biology, February 2017
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Title
Long-term microfluidic tracking of coccoid cyanobacterial cells reveals robust control of division timing
Published in
BMC Biology, February 2017
DOI 10.1186/s12915-016-0344-4
Pubmed ID
Authors

Feiqiao Brian Yu, Lisa Willis, Rosanna Man Wah Chau, Alessandro Zambon, Mark Horowitz, Devaki Bhaya, Kerwyn Casey Huang, Stephen R. Quake

Abstract

Cyanobacteria are important agents in global carbon and nitrogen cycling and hold great promise for biotechnological applications. Model organisms such as Synechocystis sp. and Synechococcus sp. have advanced our understanding of photosynthetic capacity and circadian behavior, mostly using population-level measurements in which the behavior of individuals cannot be monitored. Synechocystis sp. cells are small and divide slowly, requiring long-term experiments to track single cells. Thus, the cumulative effects of drift over long periods can cause difficulties in monitoring and quantifying cell growth and division dynamics. To overcome this challenge, we enhanced a microfluidic cell-culture device and developed an image analysis pipeline for robust lineage reconstruction. This allowed simultaneous tracking of many cells over multiple generations, and revealed that cells expand exponentially throughout their cell cycle. Generation times were highly correlated for sister cells, but not between mother and daughter cells. Relationships between birth size, division size, and generation time indicated that cell-size control was inconsistent with the "sizer" rule, where division timing is based on cell size, or the "timer" rule, where division occurs after a fixed time interval. Instead, single cell growth statistics were most consistent with the "adder" rule, in which division occurs after a constant increment in cell volume. Cells exposed to light-dark cycles exhibited growth and division only during the light period; dark phases pause but do not disrupt cell-cycle control. Our analyses revealed that the "adder" model can explain both the growth-related statistics of single Synechocystis cells and the correlation between sister cell generation times. We also observed rapid phenotypic response to light-dark transitions at the single cell level, highlighting the critical role of light in cyanobacterial cell-cycle control. Our findings suggest that by monitoring the growth kinetics of individual cells we can build testable models of circadian control of the cell cycle in cyanobacteria.

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Geographical breakdown

Country Count As %
Unknown 89 100%

Demographic breakdown

Readers by professional status Count As %
Student > Ph. D. Student 20 22%
Researcher 18 20%
Student > Master 13 15%
Student > Doctoral Student 8 9%
Student > Bachelor 7 8%
Other 13 15%
Unknown 10 11%
Readers by discipline Count As %
Agricultural and Biological Sciences 26 29%
Biochemistry, Genetics and Molecular Biology 21 24%
Engineering 10 11%
Physics and Astronomy 3 3%
Medicine and Dentistry 3 3%
Other 16 18%
Unknown 10 11%