A Two-Enzyme Adaptive Unit within Bacterial Folate Metabolism

Andrew F. Schober; Andrew D. Mathis; Christine Ingle; Junyoung O. Park; Li Chen; Joshua D. Rabinowitz; Ivan Junier; Olivier Rivoire; Kimberly A. Reynolds

doi:10.1016/j.celrep.2019.05.030

A Two-Enzyme Adaptive Unit within Bacterial Folate Metabolism

Andrew F. Schober, Andrew D. Mathis, Christine Ingle, Junyoung O. Park, Li Chen, Joshua D. Rabinowitz, Ivan Junier, Olivier Rivoire, Kimberly A. Reynolds

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

18 Scopus citations

Abstract

Enzyme function and evolution are influenced by the larger context of a metabolic pathway. Deleterious mutations or perturbations in one enzyme can often be compensated by mutations to others. We used comparative genomics and experiments to examine evolutionary interactions with the essential metabolic enzyme dihydrofolate reductase (DHFR). Analyses of synteny and co-occurrence across bacterial species indicate that DHFR is coupled to thymidylate synthase (TYMS) but relatively independent from the rest of folate metabolism. Using quantitative growth rate measurements and forward evolution in Escherichia coli, we demonstrate that the two enzymes adapt as a relatively independent unit in response to antibiotic stress. Metabolomic profiling revealed that TYMS activity must not exceed DHFR activity to prevent the depletion of reduced folates and the accumulation of the intermediate dihydrofolate. Comparative genomics analyses identified >200 gene pairs with similar statistical signatures of modular co-evolution, suggesting that cellular pathways may be decomposable into small adaptive units.

Original language	English (US)
Pages (from-to)	3359-3370.e7
Journal	Cell Reports
Volume	27
Issue number	11
DOIs	https://doi.org/10.1016/j.celrep.2019.05.030
State	Published - Jun 11 2019

Keywords

DHFR
TYMS
adaptive unit
co-evolution
comparative genomics
dihydrofolate reductase
experimental evolution
folate metabolism
forward evolution
synteny
thymidylate synthase
trimethoprim

ASJC Scopus subject areas

General Biochemistry, Genetics and Molecular Biology

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10.1016/j.celrep.2019.05.030

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title = "A Two-Enzyme Adaptive Unit within Bacterial Folate Metabolism",

abstract = "Enzyme function and evolution are influenced by the larger context of a metabolic pathway. Deleterious mutations or perturbations in one enzyme can often be compensated by mutations to others. We used comparative genomics and experiments to examine evolutionary interactions with the essential metabolic enzyme dihydrofolate reductase (DHFR). Analyses of synteny and co-occurrence across bacterial species indicate that DHFR is coupled to thymidylate synthase (TYMS) but relatively independent from the rest of folate metabolism. Using quantitative growth rate measurements and forward evolution in Escherichia coli, we demonstrate that the two enzymes adapt as a relatively independent unit in response to antibiotic stress. Metabolomic profiling revealed that TYMS activity must not exceed DHFR activity to prevent the depletion of reduced folates and the accumulation of the intermediate dihydrofolate. Comparative genomics analyses identified >200 gene pairs with similar statistical signatures of modular co-evolution, suggesting that cellular pathways may be decomposable into small adaptive units.",

keywords = "DHFR, TYMS, adaptive unit, co-evolution, comparative genomics, dihydrofolate reductase, experimental evolution, folate metabolism, forward evolution, synteny, thymidylate synthase, trimethoprim",

author = "Schober, {Andrew F.} and Mathis, {Andrew D.} and Christine Ingle and Park, {Junyoung O.} and Li Chen and Rabinowitz, {Joshua D.} and Ivan Junier and Olivier Rivoire and Reynolds, {Kimberly A.}",

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AU - Schober, Andrew F.

AU - Mathis, Andrew D.

AU - Ingle, Christine

AU - Park, Junyoung O.

AU - Chen, Li

AU - Rabinowitz, Joshua D.

AU - Junier, Ivan

AU - Rivoire, Olivier

AU - Reynolds, Kimberly A.

PY - 2019/6/11

Y1 - 2019/6/11

N2 - Enzyme function and evolution are influenced by the larger context of a metabolic pathway. Deleterious mutations or perturbations in one enzyme can often be compensated by mutations to others. We used comparative genomics and experiments to examine evolutionary interactions with the essential metabolic enzyme dihydrofolate reductase (DHFR). Analyses of synteny and co-occurrence across bacterial species indicate that DHFR is coupled to thymidylate synthase (TYMS) but relatively independent from the rest of folate metabolism. Using quantitative growth rate measurements and forward evolution in Escherichia coli, we demonstrate that the two enzymes adapt as a relatively independent unit in response to antibiotic stress. Metabolomic profiling revealed that TYMS activity must not exceed DHFR activity to prevent the depletion of reduced folates and the accumulation of the intermediate dihydrofolate. Comparative genomics analyses identified >200 gene pairs with similar statistical signatures of modular co-evolution, suggesting that cellular pathways may be decomposable into small adaptive units.

AB - Enzyme function and evolution are influenced by the larger context of a metabolic pathway. Deleterious mutations or perturbations in one enzyme can often be compensated by mutations to others. We used comparative genomics and experiments to examine evolutionary interactions with the essential metabolic enzyme dihydrofolate reductase (DHFR). Analyses of synteny and co-occurrence across bacterial species indicate that DHFR is coupled to thymidylate synthase (TYMS) but relatively independent from the rest of folate metabolism. Using quantitative growth rate measurements and forward evolution in Escherichia coli, we demonstrate that the two enzymes adapt as a relatively independent unit in response to antibiotic stress. Metabolomic profiling revealed that TYMS activity must not exceed DHFR activity to prevent the depletion of reduced folates and the accumulation of the intermediate dihydrofolate. Comparative genomics analyses identified >200 gene pairs with similar statistical signatures of modular co-evolution, suggesting that cellular pathways may be decomposable into small adaptive units.

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KW - TYMS

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KW - comparative genomics

KW - dihydrofolate reductase

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KW - folate metabolism

KW - forward evolution

KW - synteny

KW - thymidylate synthase

KW - trimethoprim

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ER -

A Two-Enzyme Adaptive Unit within Bacterial Folate Metabolism

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