Iron-Dependent Regulation of Molybdenum Cofactor Biosynthesis Genes in Escherichia coli

Zupok, Arkadiusz; Górka, Michał; Siemiatkowska, Beata; Skirycz, Aleksandra; Leimkühler, Silke

doi:10.1128/jb.00382-19

Cited by 11 publications

(7 citation statements)

References 77 publications

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“…The moaABCDE operon is involved in the Molybdenum cofactor (Moco) biosynthesis. This cofactor serves as the catalytic centre of Molybdoenzymes that are essential for anaerobic respiration (Zupok et al, 2019). Similarly, the uvrC gene increased the fitness of 4/74 in all environments except in InSPI2 ( Figure 10 ).…”

Section: Resultsmentioning

confidence: 99%

Evolutionary barriers to horizontal gene transfer in macrophage associated Salmonella

Bhatia

Kirit

Bollback

2022

Preprint

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Horizontal Gene Transfer (HGT) is a powerful evolutionary force facilitating bacterial adaptation and emergence of novel phenotypes. Several factors, including environmental ones, are predicted to restrict HGT, but we lack data supporting these predictions. Here, we address this gap by measuring the relative fitness of 44 genes horizontally transferred from E. coli to S. Typhimurium strain 4/74 in four infection relevant environments and estimated the distribution of fitness effects (DFE) in each environment. Roughly half of the genes, 40-50%, had significant fitness effects in at least one environment, with most genes showing significant gene by environment (G x E) interactions. We further identified 12 genes with dosage-dependent effects across the four environments, indicating that intolerance of the recipient strain to high protein dosage is a significant barrier to HGT. We also found longer genes had stronger fitness detriments than shorter ones, showing that gene length can significantly hinder HGT. In summary, a substantial fraction of transferred genes had a significant fitness cost on the recipient, with both gene characteristics and the environment providing barriers to HGT.

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Section: Resultsmentioning

confidence: 99%

Evolutionary barriers to horizontal gene transfer in macrophage associated Salmonella

Bhatia

Kirit

Bollback

2022

Preprint

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“… 94 In E. coli , Fe-S cluster insertion to MoaA is mediated by the Isc system and an A-type carrier protein ErpA under oxygen-limiting condition. 95 E. coli grown under iron limiting conditions show significantly reduced intracellular Moco production due to the dysfunctional [4Fe-4S] assembly and failure to produce functional MoaA and the downregulation of l -cysteine desulfurase essential for MPT synthase 96 ( Figure 1 ). Therefore, specific inhibition of Fe-S cluster biosynthesis or sulfur trafficking in pathogenic bacteria may provide potent growth inhibition by pleiotropic loss of both FeS cluster and Moco.…”

Section: Translating the Mechanistic And Structural Understanding To ...mentioning

confidence: 99%

Resolving the Multidecade-Long Mystery in MoaA Radical SAM Enzyme Reveals New Opportunities to Tackle Human Health Problems

Yokoyama

Pang

2021

ACS Bio Med Chem Au

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MoaA is one of the most conserved radical S -adenosyl- l -methionine (SAM) enzymes, and is found in most organisms in all three kingdoms of life. MoaA contributes to the biosynthesis of molybdenum cofactor (Moco), a redox enzyme cofactor used in various enzymes such as purine and sulfur catabolism in humans and anaerobic respiration in bacteria. Unlike many other cofactors, in most organisms, Moco cannot be taken up as a nutrient and requires de novo biosynthesis. Consequently, Moco biosynthesis has been linked to several human health problems, such as human Moco deficiency disease and bacterial infections. Despite the medical and biological significance, the biosynthetic mechanism of Moco’s characteristic pyranopterin structure remained elusive for more than two decades. This transformation requires the actions of the MoaA radical SAM enzyme and another protein, MoaC. Recently, MoaA and MoaC functions were elucidated as a radical SAM GTP 3′,8-cyclase and cyclic pyranopterin monophosphate (cPMP) synthase, respectively. This finding resolved the key mystery in the field and revealed new opportunities in studying the enzymology and chemical biology of MoaA and MoaC to elucidate novel mechanisms in enzyme catalysis or to address unsolved questions in Moco-related human health problems. Here, we summarize the recent progress in the functional and mechanistic studies of MoaA and MoaC and discuss the field’s future directions.

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“…In E. coli, transcription of the moaABCDE operon is also upregulated by FNR (fumarate and nitrate reduction regulatory protein) (Anderson et al, 2000;Zupok et al, 2019a). FNR is a transcriptional regulator that is essential for expressing anaerobic respiratory processes (Unden et al, 2002).…”

Section: The Regulation Of Moco Biosynthesismentioning

confidence: 99%

The biosynthesis of the molybdenum cofactors in Escherichia coli

Leimkühler

2020

Environmental Microbiology

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The biosynthesis of the molybdenum cofactor (Moco) is highly conserved among all kingdoms of life. In all molybdoenzymes containing Moco, the molybdenum atom is coordinated to a dithiolene group present in the pterin-based 6-alkyl side chain of molybdopterin (MPT). In general, the biosynthesis of Moco can be divided into four steps in in bacteria: (i) the starting point is the formation of the cyclic pyranopterin monophosphate (cPMP) from 5 0 -GTP, (ii) in the second step the two sulfur atoms are inserted into cPMP leading to the formation of MPT, (iii) in the third step the molybdenum atom is inserted into MPT to form Moco and (iv) in the fourth step bis-Mo-MPT is formed and an additional modification of Moco is possible with the attachment of a nucleotide (CMP or GMP) to the phosphate group of MPT, forming the dinucleotide variants of Moco. This review presents an update on the well-characterized Moco biosynthesis in the model organism Escherichia coli including novel discoveries from the recent years.

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Iron-Dependent Regulation of Molybdenum Cofactor Biosynthesis Genes in Escherichia coli

Cited by 11 publications

References 77 publications

Evolutionary barriers to horizontal gene transfer in macrophage associated Salmonella

Evolutionary barriers to horizontal gene transfer in macrophage associated Salmonella

Resolving the Multidecade-Long Mystery in MoaA Radical SAM Enzyme Reveals New Opportunities to Tackle Human Health Problems

The biosynthesis of the molybdenum cofactors in Escherichia coli

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