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Metalloprotein switches that display chemical-dependent electron transfer in cells.


ABSTRACT: Biological electron transfer is challenging to directly regulate using environmental conditions. To enable dynamic, protein-level control over energy flow in metabolic systems for synthetic biology and bioelectronics, we created ferredoxin logic gates that utilize transcriptional and post-translational inputs to control energy flow through a synthetic electron transfer pathway that is required for bacterial growth. These logic gates were created by subjecting a thermostable, plant-type ferredoxin to backbone fission and fusing the resulting fragments to a pair of proteins that self-associate, a pair of proteins whose association is stabilized by a small molecule, and to the termini of a ligand-binding domain. We show that the latter domain insertion design strategy yields an allosteric ferredoxin switch that acquires an oxygen-tolerant [2Fe-2S] cluster and can use different chemicals, including a therapeutic drug and an environmental pollutant, to control the production of a reduced metabolite in Escherichia coli and cell lysates.

SUBMITTER: Atkinson JT 

PROVIDER: S-EPMC6898983 | biostudies-literature | 2019 Feb

REPOSITORIES: biostudies-literature

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Metalloprotein switches that display chemical-dependent electron transfer in cells.

Atkinson Joshua T JT   Campbell Ian J IJ   Thomas Emily E EE   Bonitatibus Sheila C SC   Elliott Sean J SJ   Bennett George N GN   Silberg Jonathan J JJ  

Nature chemical biology 20181217 2


Biological electron transfer is challenging to directly regulate using environmental conditions. To enable dynamic, protein-level control over energy flow in metabolic systems for synthetic biology and bioelectronics, we created ferredoxin logic gates that utilize transcriptional and post-translational inputs to control energy flow through a synthetic electron transfer pathway that is required for bacterial growth. These logic gates were created by subjecting a thermostable, plant-type ferredoxi  ...[more]

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