Kinetic Modeling of the Genetic Information Processes in a Minimal Cell

Zane R. Thornburg; Marcelo C. R. Melo; David Bianchi; Troy A. Brier; Cole Crotty; Marian Breuer; Hamilton O. Smith; Clyde A. Hutchison; John I. Glass; Zaida Luthey-Schulten

doi:10.3389/fmolb.2019.00130

Kinetic Modeling of the Genetic Information Processes in a Minimal Cell

Zane R. Thornburg, Marcelo C. R. Melo, David Bianchi, Troy A. Brier, Cole Crotty, Marian Breuer, Hamilton O. Smith, Clyde A. Hutchison, John I. Glass, Zaida Luthey-Schulten^*

^*Corresponding author for this work

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

Abstract

JCVI-syn3A is a minimal bacterial cell with a 543 kbp genome consisting of 493 genes. For this slow growing minimal cell with a 105 min doubling time, we recently established the essential metabolism including the transport of required nutrients from the environment, the gene map, and genome-wide proteomics. Of the 452 protein-coding genes, 143 are assigned to metabolism and 212 are assigned to genetic information processing. Using genome-wide proteomics and experimentally measured kinetic parameters from the literature we present here kinetic models for the genetic information processes of DNA replication, replication initiation, transcription, and translation which are solved stochastically and averaged over 1,000 replicates/cells. The model predicts the time required for replication initiation and DNA replication to be 8 and 50 min on average respectively and the number of proteins and ribosomal components to be approximately doubled in a cell cycle. The model of genetic information processing when combined with the essential metabolic and cell growth networks will provide a powerful platform for studying the fundamental principles of life.

Original language	English
Article number	130
Number of pages	13
Journal	Frontiers in Molecular Biosciences
Volume	6
DOIs	https://doi.org/10.3389/fmolb.2019.00130
Publication status	Published - 28 Nov 2019

Keywords

minimal cells
stochastic simulations
kinetic parameters
DNA replication
transcription
translation
mRNA production
protein production
ESCHERICHIA-COLI
REPLICATION-ORIGIN
RIBOSOME BIOGENESIS
DNAA PROTEIN
POLYMERASE
SIMULATION
DYNAMICS
BALANCE
BINDING
GROWTH

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10.3389/fmolb.2019.00130Licence: CC BY

Cite this

@article{9fe98799761f461792e2869a2a30447b,

title = "Kinetic Modeling of the Genetic Information Processes in a Minimal Cell",

abstract = "JCVI-syn3A is a minimal bacterial cell with a 543 kbp genome consisting of 493 genes. For this slow growing minimal cell with a 105 min doubling time, we recently established the essential metabolism including the transport of required nutrients from the environment, the gene map, and genome-wide proteomics. Of the 452 protein-coding genes, 143 are assigned to metabolism and 212 are assigned to genetic information processing. Using genome-wide proteomics and experimentally measured kinetic parameters from the literature we present here kinetic models for the genetic information processes of DNA replication, replication initiation, transcription, and translation which are solved stochastically and averaged over 1,000 replicates/cells. The model predicts the time required for replication initiation and DNA replication to be 8 and 50 min on average respectively and the number of proteins and ribosomal components to be approximately doubled in a cell cycle. The model of genetic information processing when combined with the essential metabolic and cell growth networks will provide a powerful platform for studying the fundamental principles of life.",

keywords = "minimal cells, stochastic simulations, kinetic parameters, DNA replication, transcription, translation, mRNA production, protein production, ESCHERICHIA-COLI, REPLICATION-ORIGIN, RIBOSOME BIOGENESIS, DNAA PROTEIN, POLYMERASE, SIMULATION, DYNAMICS, BALANCE, BINDING, GROWTH",

author = "Thornburg, {Zane R.} and Melo, {Marcelo C. R.} and David Bianchi and Brier, {Troy A.} and Cole Crotty and Marian Breuer and Smith, {Hamilton O.} and Hutchison, {Clyde A.} and Glass, {John I.} and Zaida Luthey-Schulten",

note = "Funding Information: The authors thank Tyler Earnest for help with the gene map software. Funding. Partial support from NSF MCB 1818344 and 1840320, The Center for the Physics of Living Cells NSF PHY 1430124, NSF PHY 1505008, and NSF REU 1659598. Publisher Copyright: {\textcopyright} Copyright {\textcopyright} 2019 Thornburg, Melo, Bianchi, Brier, Crotty, Breuer, Smith, Hutchison, Glass and Luthey-Schulten.",

year = "2019",

month = nov,

day = "28",

doi = "10.3389/fmolb.2019.00130",

language = "English",

volume = "6",

journal = "Frontiers in Molecular Biosciences",

issn = "2296-889X",

publisher = "Frontiers Research Foundation",

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TY - JOUR

T1 - Kinetic Modeling of the Genetic Information Processes in a Minimal Cell

AU - Thornburg, Zane R.

AU - Melo, Marcelo C. R.

AU - Bianchi, David

AU - Brier, Troy A.

AU - Crotty, Cole

AU - Breuer, Marian

AU - Smith, Hamilton O.

AU - Hutchison, Clyde A.

AU - Glass, John I.

AU - Luthey-Schulten, Zaida

N1 - Funding Information: The authors thank Tyler Earnest for help with the gene map software. Funding. Partial support from NSF MCB 1818344 and 1840320, The Center for the Physics of Living Cells NSF PHY 1430124, NSF PHY 1505008, and NSF REU 1659598. Publisher Copyright: © Copyright © 2019 Thornburg, Melo, Bianchi, Brier, Crotty, Breuer, Smith, Hutchison, Glass and Luthey-Schulten.

PY - 2019/11/28

Y1 - 2019/11/28

N2 - JCVI-syn3A is a minimal bacterial cell with a 543 kbp genome consisting of 493 genes. For this slow growing minimal cell with a 105 min doubling time, we recently established the essential metabolism including the transport of required nutrients from the environment, the gene map, and genome-wide proteomics. Of the 452 protein-coding genes, 143 are assigned to metabolism and 212 are assigned to genetic information processing. Using genome-wide proteomics and experimentally measured kinetic parameters from the literature we present here kinetic models for the genetic information processes of DNA replication, replication initiation, transcription, and translation which are solved stochastically and averaged over 1,000 replicates/cells. The model predicts the time required for replication initiation and DNA replication to be 8 and 50 min on average respectively and the number of proteins and ribosomal components to be approximately doubled in a cell cycle. The model of genetic information processing when combined with the essential metabolic and cell growth networks will provide a powerful platform for studying the fundamental principles of life.

AB - JCVI-syn3A is a minimal bacterial cell with a 543 kbp genome consisting of 493 genes. For this slow growing minimal cell with a 105 min doubling time, we recently established the essential metabolism including the transport of required nutrients from the environment, the gene map, and genome-wide proteomics. Of the 452 protein-coding genes, 143 are assigned to metabolism and 212 are assigned to genetic information processing. Using genome-wide proteomics and experimentally measured kinetic parameters from the literature we present here kinetic models for the genetic information processes of DNA replication, replication initiation, transcription, and translation which are solved stochastically and averaged over 1,000 replicates/cells. The model predicts the time required for replication initiation and DNA replication to be 8 and 50 min on average respectively and the number of proteins and ribosomal components to be approximately doubled in a cell cycle. The model of genetic information processing when combined with the essential metabolic and cell growth networks will provide a powerful platform for studying the fundamental principles of life.

KW - minimal cells

KW - stochastic simulations

KW - kinetic parameters

KW - DNA replication

KW - transcription

KW - translation

KW - mRNA production

KW - protein production

KW - ESCHERICHIA-COLI

KW - REPLICATION-ORIGIN

KW - RIBOSOME BIOGENESIS

KW - DNAA PROTEIN

KW - POLYMERASE

KW - SIMULATION

KW - DYNAMICS

KW - BALANCE

KW - BINDING

KW - GROWTH

U2 - 10.3389/fmolb.2019.00130

DO - 10.3389/fmolb.2019.00130

M3 - Article

C2 - 31850364

SN - 2296-889X

VL - 6

JO - Frontiers in Molecular Biosciences

JF - Frontiers in Molecular Biosciences

M1 - 130

ER -