Synthesis and degradation of FtsZ quantitatively predict the first cell division in starved bacteria

Karthik Sekar; Roberto Rusconi; John T. Sauls; Tobias Fuhrer; Elad Noor; Jen Nguyen; Vicente I. Fernandez; Marieke F. Buffing; Michael Berney; Suckjoon Jun; Roman Stocker; Uwe Sauer

doi:10.15252/msb.20188623

Synthesis and degradation of FtsZ quantitatively predict the first cell division in starved bacteria

Karthik Sekar, Roberto Rusconi, John T. Sauls, Tobias Fuhrer, Elad Noor, Jen Nguyen, Vicente I. Fernandez, Marieke F. Buffing, Michael Berney, Suckjoon Jun, Roman Stocker, Uwe Sauer

Microbiology & Immunology

Research output: Contribution to journal › Article › peer-review

31 Scopus citations

Abstract

In natural environments, microbes are typically non-dividing and gauge when nutrients permit division. Current models are phenomenological and specific to nutrient-rich, exponentially growing cells, thus cannot predict the first division under limiting nutrient availability. To assess this regime, we supplied starving Escherichia coli with glucose pulses at increasing frequencies. Real-time metabolomics and microfluidic single-cell microscopy revealed unexpected, rapid protein, and nucleic acid synthesis already from minuscule glucose pulses in non-dividing cells. Additionally, the lag time to first division shortened as pulsing frequency increased. We pinpointed division timing and dependence on nutrient frequency to the changing abundance of the division protein FtsZ. A dynamic, mechanistic model quantitatively relates lag time to FtsZ synthesis from nutrient pulses and FtsZ protease-dependent degradation. Lag time changed in model-congruent manners, when we experimentally modulated the synthesis or degradation of FtsZ. Thus, limiting abundance of FtsZ can quantitatively predict timing of the first cell division.

Original language	English (US)
Article number	e8623
Journal	Molecular Systems Biology
Volume	14
Issue number	11
DOIs	https://doi.org/10.15252/msb.20188623
State	Published - Nov 2018

Keywords

Escherichia coli
FtsZ
division
protein degradation
starvation

ASJC Scopus subject areas

General Biochemistry, Genetics and Molecular Biology
General Immunology and Microbiology
General Agricultural and Biological Sciences
Applied Mathematics

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10.15252/msb.20188623

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title = "Synthesis and degradation of FtsZ quantitatively predict the first cell division in starved bacteria",

abstract = "In natural environments, microbes are typically non-dividing and gauge when nutrients permit division. Current models are phenomenological and specific to nutrient-rich, exponentially growing cells, thus cannot predict the first division under limiting nutrient availability. To assess this regime, we supplied starving Escherichia coli with glucose pulses at increasing frequencies. Real-time metabolomics and microfluidic single-cell microscopy revealed unexpected, rapid protein, and nucleic acid synthesis already from minuscule glucose pulses in non-dividing cells. Additionally, the lag time to first division shortened as pulsing frequency increased. We pinpointed division timing and dependence on nutrient frequency to the changing abundance of the division protein FtsZ. A dynamic, mechanistic model quantitatively relates lag time to FtsZ synthesis from nutrient pulses and FtsZ protease-dependent degradation. Lag time changed in model-congruent manners, when we experimentally modulated the synthesis or degradation of FtsZ. Thus, limiting abundance of FtsZ can quantitatively predict timing of the first cell division.",

keywords = "Escherichia coli, FtsZ, division, protein degradation, starvation",

author = "Karthik Sekar and Roberto Rusconi and Sauls, {John T.} and Tobias Fuhrer and Elad Noor and Jen Nguyen and Fernandez, {Vicente I.} and Buffing, {Marieke F.} and Michael Berney and Suckjoon Jun and Roman Stocker and Uwe Sauer",

note = "Publisher Copyright: {\textcopyright} 2018 The Authors. Published under the terms of the CC BY 4.0 license",

year = "2018",

month = nov,

doi = "10.15252/msb.20188623",

language = "English (US)",

volume = "14",

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AU - Sekar, Karthik

AU - Rusconi, Roberto

AU - Sauls, John T.

AU - Fuhrer, Tobias

AU - Noor, Elad

AU - Nguyen, Jen

AU - Fernandez, Vicente I.

AU - Buffing, Marieke F.

AU - Berney, Michael

AU - Jun, Suckjoon

AU - Stocker, Roman

AU - Sauer, Uwe

PY - 2018/11

Y1 - 2018/11

N2 - In natural environments, microbes are typically non-dividing and gauge when nutrients permit division. Current models are phenomenological and specific to nutrient-rich, exponentially growing cells, thus cannot predict the first division under limiting nutrient availability. To assess this regime, we supplied starving Escherichia coli with glucose pulses at increasing frequencies. Real-time metabolomics and microfluidic single-cell microscopy revealed unexpected, rapid protein, and nucleic acid synthesis already from minuscule glucose pulses in non-dividing cells. Additionally, the lag time to first division shortened as pulsing frequency increased. We pinpointed division timing and dependence on nutrient frequency to the changing abundance of the division protein FtsZ. A dynamic, mechanistic model quantitatively relates lag time to FtsZ synthesis from nutrient pulses and FtsZ protease-dependent degradation. Lag time changed in model-congruent manners, when we experimentally modulated the synthesis or degradation of FtsZ. Thus, limiting abundance of FtsZ can quantitatively predict timing of the first cell division.

AB - In natural environments, microbes are typically non-dividing and gauge when nutrients permit division. Current models are phenomenological and specific to nutrient-rich, exponentially growing cells, thus cannot predict the first division under limiting nutrient availability. To assess this regime, we supplied starving Escherichia coli with glucose pulses at increasing frequencies. Real-time metabolomics and microfluidic single-cell microscopy revealed unexpected, rapid protein, and nucleic acid synthesis already from minuscule glucose pulses in non-dividing cells. Additionally, the lag time to first division shortened as pulsing frequency increased. We pinpointed division timing and dependence on nutrient frequency to the changing abundance of the division protein FtsZ. A dynamic, mechanistic model quantitatively relates lag time to FtsZ synthesis from nutrient pulses and FtsZ protease-dependent degradation. Lag time changed in model-congruent manners, when we experimentally modulated the synthesis or degradation of FtsZ. Thus, limiting abundance of FtsZ can quantitatively predict timing of the first cell division.

KW - Escherichia coli

KW - FtsZ

KW - division

KW - protein degradation

KW - starvation

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Synthesis and degradation of FtsZ quantitatively predict the first cell division in starved bacteria

Abstract

Keywords

ASJC Scopus subject areas

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