Your search keyword '"Coenzymes biosynthesis"' showing total 256 results

1. Shared functions of Fe-S cluster assembly and Moco biosynthesis.

Author

Hasnat MA and Leimkühler S

Subjects

Escherichia coli Proteins metabolism, Escherichia coli Proteins genetics, Iron metabolism, Sulfur metabolism, Escherichia coli genetics, Escherichia coli metabolism, Carbon-Sulfur Lyases metabolism, Carbon-Sulfur Lyases genetics, Gene Expression Regulation, Bacterial, Operon, Isomerases, Molybdenum Cofactors, Metalloproteins metabolism, Metalloproteins genetics, Metalloproteins biosynthesis, Iron-Sulfur Proteins metabolism, Iron-Sulfur Proteins genetics, Coenzymes metabolism, Coenzymes biosynthesis, Coenzymes genetics, Pteridines metabolism

Abstract

Molybdenum cofactor (Moco) biosynthesis is a complex process that involves the coordinated function of several proteins. In the recent years it has become evident that the availability of Fe-S clusters play an important role for the biosynthesis of Moco. First, the MoaA protein binds two [4Fe-4S] clusters per monomer. Second, the expression of the moaABCDE and moeAB operons is regulated by FNR, which senses the availability of oxygen via a functional [4Fe-4S] cluster. Finally, the conversion of cyclic pyranopterin monophosphate to molybdopterin requires the availability of the L-cysteine desulfurase IscS, which is an enzyme involved in the transfer of sulfur to various acceptor proteins with a main role in the assembly of Fe-S clusters. In this review, we dissect the dependence of the production of active molybdoenzymes in detail, starting from the regulation of gene expression and further explaining sulfur delivery and Fe-S cluster insertion into target enzymes. Further, Fe-S cluster assembly is also linked to iron availability. While the abundance of selected molybdoenzymes is largely decreased under iron-limiting conditions, we explain that the expression of the genes is dependent on an active FNR protein. FNR is a very important transcription factor that represents the master-switch for the expression of target genes in response to anaerobiosis. Moco biosynthesis is further directly dependent on the presence of ArcA and also on an active Fur protein., Competing Interests: Declaration of competing interest The authors declare the following financial interests/personal relationships which may be considered as potential competing interests: Silke Leimkuehler reports financial support and administrative support were provided by Deutsche Forschungsgemeinschaft. Silke Leimkuehler reports financial support was provided by German Research Foundation. If there are other authors, they declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 Elsevier B.V. All rights reserved.)

Published

2024

2. Coenzyme biosynthesis in response to precursor availability reveals incorporation of β-alanine from pantothenate in prototrophic bacteria.

Author

Ryback B and Vorholt JA

Subjects

Coenzyme A biosynthesis, Pyridoxal, Pyridoxal Phosphate metabolism, Vitamins metabolism, NAD metabolism, Culture Media chemistry, Culture Media metabolism, beta-Alanine metabolism, Coenzymes biosynthesis, Escherichia coli metabolism

Abstract

Coenzymes are important for all classes of enzymatic reactions and essential for cellular metabolism. Most coenzymes are synthesized from dedicated precursors, also referred to as vitamins, which prototrophic bacteria can either produce themselves from simpler substrates or take up from the environment. The extent to which prototrophs use supplied vitamins and whether externally available vitamins affect the size of intracellular coenzyme pools and control endogenous vitamin synthesis is currently largely unknown. Here, we studied coenzyme pool sizes and vitamin incorporation into coenzymes during growth on different carbon sources and vitamin supplementation regimes using metabolomics approaches. We found that the model bacterium Escherichia coli incorporated pyridoxal, niacin, and pantothenate into pyridoxal 5'-phosphate, NAD, and coenzyme A (CoA), respectively. In contrast, riboflavin was not taken up and was produced exclusively endogenously. Coenzyme pools were mostly homeostatic and not affected by externally supplied precursors. Remarkably, we found that pantothenate is not incorporated into CoA as such but is first degraded to pantoate and β-alanine and then rebuilt. This pattern was conserved in various bacterial isolates, suggesting a preference for β-alanine over pantothenate utilization in CoA synthesis. Finally, we found that the endogenous synthesis of coenzyme precursors remains active when vitamins are supplied, which is consistent with described expression data of genes for enzymes involved in coenzyme biosynthesis under these conditions. Continued production of endogenous coenzymes may ensure rapid synthesis of the mature coenzyme under changing environmental conditions, protect against coenzyme limitation, and explain vitamin availability in naturally oligotrophic environments., Competing Interests: Conflict of interest The authors declare no competing interests., (Copyright © 2023 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2023

3. The pathway for coenzyme M biosynthesis in bacteria.

Author

Wu HH, Pun MD, Wise CE, Streit BR, Mus F, Berim A, Kincannon WM, Islam A, Partovi SE, Gang DR, DuBois JL, Lubner CE, Berkman CE, Lange BM, and Peters JW

Subjects

Anaerobiosis, Archaea metabolism, Methane metabolism, Oxidation-Reduction, Phosphates metabolism, Bacteria metabolism, Coenzymes biosynthesis, Euryarchaeota metabolism, Mesna metabolism

Abstract

Mercaptoethane sulfonate or coenzyme M (CoM) is the smallest known organic cofactor and is most commonly associated with the methane-forming step in all methanogenic archaea but is also associated with the anaerobic oxidation of methane to CO 2 in anaerobic methanotrophic archaea and the oxidation of short-chain alkanes in Syntrophoarchaeum species. It has also been found in a small number of bacteria capable of the metabolism of small organics. Although many of the steps for CoM biosynthesis in methanogenic archaea have been elucidated, a complete pathway for the biosynthesis of CoM in archaea or bacteria has not been reported. Here, we present the complete CoM biosynthesis pathway in bacteria, revealing distinct chemical steps relative to CoM biosynthesis in methanogenic archaea. The existence of different pathways represents a profound instance of convergent evolution. The five-step pathway involves the addition of sulfite, the elimination of phosphate, decarboxylation, thiolation, and the reduction to affect the sequential conversion of phosphoenolpyruvate to CoM. The salient features of the pathway demonstrate reactivities for members of large aspartase/fumarase and pyridoxal 5'-phosphate-dependent enzyme families.

Published

2022

4. Sulfur amino acid metabolism and related metabotypes of autism spectrum disorder: A review of biochemical evidence for a hypothesis.

Author

Indika NR, Deutz NEP, Engelen MPKJ, Peiris H, Wijetunge S, and Perera R

Subjects

Brain, Humans, Molybdenum Cofactors, Pteridines, Autism Spectrum Disorder metabolism, Coenzymes biosynthesis, Cysteine metabolism, Metalloproteins biosynthesis, Oxidative Stress, S-Adenosylmethionine metabolism

Abstract

There are multiple lines of evidence for an impaired sulfur amino acid (SAA) metabolism in autism spectrum disorder (ASD). For instance, the concentrations of methionine, cysteine and S-adenosylmethionine (SAM) in body fluids of individuals with ASD is significantly lower while the concentration of S-adenosylhomocysteine (SAH) is significantly higher as compared to healthy individuals. Reduced methionine and SAM may reflect impaired remethylation pathway whereas increased SAH may reflect reduced S-adenosylhomocysteine hydrolase activity in the catabolic direction. Reduced SAM/SAH ratio reflects an impaired methylation capacity. We hypothesize multiple mechanisms to explain how the interplay of oxidative stress, neuroinflammation, mercury exposure, maternal use of valproate, altered gut microbiome and certain genetic variants may lead to these SAA metabotypes. Furthermore, we also propose a number of mechanisms to explain the metabolic consequences of abnormal SAA metabotypes. For instance in the brain, reduced SAM/SAH ratio will result in melatonin deficiency and hypomethylation of a number of biomolecules such as DNA, RNA and histones. In addition to previously proposed mechanisms, we propose that impaired activity of "radical SAM" enzymes will result in reduced endogenous lipoic acid synthesis, reduced molybdenum cofactor synthesis and impaired porphyrin metabolism leading to mitochondrial dysfunction, porphyrinuria and impaired sulfation capacity. Furthermore depletion of SAM may also lead to the disturbed mTOR signaling pathway in a subgroup of ASD. The proposed "SAM-depletion hypothesis" is an inclusive model to explain the relationship between heterogeneous risk factors and metabotypes observed in a subset of children with ASD., (Copyright © 2021 Elsevier B.V. and Société Française de Biochimie et Biologie Moléculaire (SFBBM). All rights reserved.)

Published

2021

5. Creating enzymes and self-sufficient cells for biosynthesis of the non-natural cofactor nicotinamide cytosine dinucleotide.

Author

Wang X, Feng Y, Guo X, Wang Q, Ning S, Li Q, Wang J, Wang L, and Zhao ZK

Subjects

Coenzymes chemistry, Cytidine Triphosphate metabolism, Enzyme Assays, Escherichia coli enzymology, Escherichia coli genetics, Escherichia coli Proteins metabolism, High-Throughput Screening Assays, Lactic Acid metabolism, Malates metabolism, Niacinamide chemistry, Nicotinamide Mononucleotide metabolism, Nicotinamide-Nucleotide Adenylyltransferase metabolism, Oxidation-Reduction, Substrate Specificity genetics, Synthetic Biology methods, Coenzymes biosynthesis, Escherichia coli Proteins genetics, Niacinamide biosynthesis, Nicotinamide-Nucleotide Adenylyltransferase genetics, Protein Engineering

Abstract

Nicotinamide adenine dinucleotide (NAD) and its reduced form are indispensable cofactors in life. Diverse NAD mimics have been developed for applications in chemical and biological sciences. Nicotinamide cytosine dinucleotide (NCD) has emerged as a non-natural cofactor to mediate redox transformations, while cells are fed with chemically synthesized NCD. Here, we create NCD synthetase (NcdS) by reprograming the substrate binding pockets of nicotinic acid mononucleotide (NaMN) adenylyltransferase to favor cytidine triphosphate and nicotinamide mononucleotide over their regular substrates ATP and NaMN, respectively. Overexpression of NcdS alone in the model host Escherichia coli facilitated intracellular production of NCD, and higher NCD levels up to 5.0 mM were achieved upon further pathway regulation. Finally, the non-natural cofactor self-sufficiency was confirmed by mediating an NCD-linked metabolic circuit to convert L-malate into D-lactate. NcdS together with NCD-linked enzymes offer unique tools and opportunities for intriguing studies in chemical biology and synthetic biology.

Published

2021

6. Molybdenum cofactor biology, evolution and deficiency.

Author

Mayr SJ, Mendel RR, and Schwarz G

Subjects

Coenzymes biosynthesis, Coenzymes classification, Gene Fusion genetics, Humans, Metalloproteins biosynthesis, Metalloproteins classification, Molybdenum Cofactors, Pteridines classification, Substrate Specificity, Coenzymes genetics, Eukaryota genetics, Metalloproteins genetics, Molybdenum metabolism

Abstract

The molybdenum cofactor (Moco) represents an ancient metal‑sulfur cofactor, which participates as catalyst in carbon, nitrogen and sulfur cycles, both on individual and global scale. Given the diversity of biological processes dependent on Moco and their evolutionary age, Moco is traced back to the last universal common ancestor (LUCA), while Moco biosynthetic genes underwent significant changes through evolution and acquired additional functions. In this review, focused on eukaryotic Moco biology, we elucidate the benefits of gene fusions on Moco biosynthesis and beyond. While originally the gene fusions were driven by biosynthetic advantages such as coordinated expression of functionally related proteins and product/substrate channeling, they also served as origin for the development of novel functions. Today, Moco biosynthetic genes are involved in a multitude of cellular processes and loss of the according gene products result in severe disorders, both related to Moco biosynthesis and secondary enzyme functions., (Copyright © 2020 Elsevier B.V. All rights reserved.)

Published

2021

7. Human riboflavin kinase: Species-specific traits in the biosynthesis of the FMN cofactor.

Author

Anoz-Carbonell E, Rivero M, Polo V, Velázquez-Campoy A, and Medina M

Subjects

Catalysis, Humans, Kinetics, Riboflavin metabolism, Species Specificity, Substrate Specificity, Coenzymes biosynthesis, Coenzymes metabolism, Flavin Mononucleotide biosynthesis, Flavin Mononucleotide metabolism, Phosphotransferases (Alcohol Group Acceptor) metabolism

Abstract

Human riboflavin kinase (HsRFK) catalyzes vitamin B 2 (riboflavin) phosphorylation to flavin mononucleotide (FMN), obligatory step in flavin cofactor synthesis. HsRFK expression is related to protection from oxidative stress, amyloid-β toxicity, and some malignant cancers progression. Its downregulation alters expression profiles of clock-controlled metabolic-genes and destroys flavins protection on stroke treatments, while its activity reduction links to protein-energy malnutrition and thyroid hormones decrease. We explored specific features of the mechanisms underlying the regulation of HsRFK activity, showing that both reaction products regulate it through competitive inhibition. Fast-kinetic studies show that despite HsRFK binds faster and preferably the reaction substrates, the complex holding both products is kinetically most stable. An intricate ligand binding landscape with all combinations of substrates/products competing with the catalytic complex and exhibiting moderate cooperativity is also presented. These data might contribute to better understanding the molecular bases of pathologies coursing with aberrant HsRFK availability, and envisage that interaction with its client-apoproteins might favor FMN release. Finally, HsRFK parameters differ from those of the so far evaluated bacterial counterparts, reinforcing the idea of species-specific mechanisms in RFK catalysis. These observations support HsRFK as potential therapeutic target because of its key functions, while also envisage bacterial RFK modules as potential antimicrobial targets., (© 2020 Federation of American Societies for Experimental Biology.)

Published

2020

8. The biosynthesis of the molybdenum cofactors in Escherichia coli.

Author

Leimkühler S

Subjects

Coenzymes chemistry, Metalloproteins chemistry, Molybdenum metabolism, Molybdenum Cofactors, Organophosphorus Compounds, Pteridines chemistry, Pterins chemistry, Coenzymes biosynthesis, Escherichia coli metabolism, Metalloproteins biosynthesis

Abstract

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'-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., (© 2020 The Author. Environmental Microbiology published by Society for Applied Microbiology and John Wiley & Sons Ltd.)

Published

2020

9. Heterologous Expression and Engineering of the Nitrogenase Cofactor Biosynthesis Scaffold NifEN.

Author

Solomon JB, Lee CC, Jasniewski AJ, Rasekh MF, Ribbe MW, and Hu Y

Subjects

Azotobacter vinelandii genetics, Gene Expression, Bacterial Proteins genetics, Coenzymes biosynthesis, Genetic Engineering, Nitrogenase metabolism

Abstract

NifEN plays a crucial role in the biosynthesis of nitrogenase, catalyzing the final step of cofactor maturation prior to delivering the cofactor to NifDK, the catalytic component of nitrogenase. The difficulty in expressing NifEN, a complex, heteromultimeric metalloprotein sharing structural/functional homology with NifDK, is a major challenge in the heterologous expression of nitrogenase. Herein, we report the expression and engineering of Azotobacter vinelandii NifEN in Escherichia coli. Biochemical and spectroscopic analyses demonstrate the integrity of the heterologously expressed NifEN in composition and functionality and, additionally, the ability of an engineered NifEN variant to mimic NifDK in retaining the matured cofactor at an analogous cofactor-binding site. This is an important step toward piecing together a viable pathway for the heterologous expression of nitrogenase and identifying variants for the mechanistic investigation of this enzyme., (© 2020 Wiley-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2020

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

Author

Zupok A, Gorka M, Siemiatkowska B, Skirycz A, and Leimkühler S

Subjects

Escherichia coli Proteins genetics, Molybdenum Cofactors, Proteomics, Pteridines, Coenzymes biosynthesis, Escherichia coli metabolism, Escherichia coli Proteins metabolism, Gene Expression Regulation, Bacterial physiology, Iron metabolism, Metalloproteins biosynthesis

Abstract

Molybdenum cofactor (Moco) biosynthesis is a complex process that involves the coordinated function of several proteins. In recent years it has become obvious that the availability of iron plays an important role in the biosynthesis of Moco. First, the MoaA protein binds two [4Fe-4S] clusters per monomer. Second, the expression of the moaABCDE and moeAB operons is regulated by FNR, which senses the availability of oxygen via a functional [4Fe-4S] cluster. Finally, the conversion of cyclic pyranopterin monophosphate to molybdopterin requires the availability of the l-cysteine desulfurase IscS, which is a shared protein with a main role in the assembly of Fe-S clusters. In this report, we investigated the transcriptional regulation of the moaABCDE operon by focusing on its dependence on cellular iron availability. While the abundance of selected molybdoenzymes is largely decreased under iron-limiting conditions, our data show that the regulation of the moaABCDE operon at the level of transcription is only marginally influenced by the availability of iron. Nevertheless, intracellular levels of Moco were decreased under iron-limiting conditions, likely based on an inactive MoaA protein in addition to lower levels of the l-cysteine desulfurase IscS, which simultaneously reduces the sulfur availability for Moco production. IMPORTANCE FNR is a very important transcriptional factor that represents the master switch for the expression of target genes in response to anaerobiosis. Among the FNR-regulated operons in Escherichia coli is the moaABCDE operon, involved in Moco biosynthesis. Molybdoenzymes have essential roles in eukaryotic and prokaryotic organisms. In bacteria, molybdoenzymes are crucial for anaerobic respiration using alternative electron acceptors. This work investigates the connection of iron availability to the biosynthesis of Moco and the production of active molybdoenzymes., (Copyright © 2019 American Society for Microbiology.)

Published

2019

11. Identification and characterization of the rice pre-harvest sprouting mutants involved in molybdenum cofactor biosynthesis.

Author

Liu X, Wang J, Yu Y, Kong L, Liu Y, Liu Z, Li H, Wei P, Liu M, Zhou H, Bu Q, and Fang J

Subjects

Adaptation, Physiological, Gene Expression Regulation, Plant, Molybdenum Cofactors, Oryza physiology, Osmosis, Phenotype, Plant Proteins genetics, Plant Proteins metabolism, Pteridines, Salt Stress genetics, Stress, Physiological genetics, Biosynthetic Pathways, Coenzymes biosynthesis, Metalloproteins biosynthesis, Mutation genetics, Oryza genetics, Oryza growth & development

Abstract

In cereal crops, ABA deficiency during seed maturation phase causes pre-harvest sprouting (PHS), and molybdenum cofactor (MoCo) is required for ABA biosynthesis. Here, two rice PHS mutants F254 and F5-1 were characterized. In addition to the PHS, these mutants showed pleiotropic phenotypes such as twisting and slender leaves, and then died when the seedling developed to four or five leaves. Map-based cloning showed that OsCNX6 and OsCNX1 encoding homologs of MoaE and MoeA were responsible for F254 and F5-1 mutants, respectively. Genetic complementation indicated that OsCNX6 not only rescued the PHS and seedling lethal phenotype of the cnx6 mutant, but also recovered the MoCo-dependent enzyme activities such as xanthine dehydrogenase (XDH), aldehyde oxidase (AO), nitrate reductase (NR) and sulfite oxidase (SO). Expression pattern showed that OsCNX6 was richly expressed in seed during embryo maturation by quantitative reverse transcriptase PCR and RNA in situ hybridization. Furthermore, the OsCNX6 overexpression plants can significantly enhance the MoCo-dependent enzyme activities, and improved the osmotic and salt stress tolerance without unfavorable phenotypes. Collectively, these data indicated that OsCNX6 participated in MoCo biosynthesis, and is essential for rice development, especially for seed dormancy and germination, and OsCNX6 could be an effective target for improving abiotic stress tolerance in rice., (© 2018 The Authors. New Phytologist © 2018 New Phytologist Trust.)

Published

2019

12. Guided cobamide biosynthesis for heterologous production of reductive dehalogenases.

Author

Schubert T, von Reuß SH, Kunze C, Paetz C, Kruse S, Brand-Schön P, Nelly AM, Nüske J, and Diekert G

Subjects

Cobamides biosynthesis, Coenzymes biosynthesis, Desulfitobacterium enzymology, Enterobacteriaceae enzymology, Hydrolases metabolism, Vitamin B Complex biosynthesis

Abstract

Cobamides (Cbas) are essential cofactors of reductive dehalogenases (RDases) in organohalide-respiring bacteria (OHRB). Changes in the Cba structure can influence RDase function. Here, we report on the cofactor versatility or selectivity of Desulfitobacterium RDases produced either in the native organism or heterologously. The susceptibility of Desulfitobacterium hafniense strain DCB-2 to guided Cba biosynthesis (i.e. incorporation of exogenous Cba lower ligand base precursors) was analysed. Exogenous benzimidazoles, azabenzimidazoles and 4,5-dimethylimidazole were incorporated by the organism into Cbas. When the type of Cba changed, no effect on the turnover rate of the 3-chloro-4-hydroxy-phenylacetate-converting enzyme RdhA6 and the 3,5-dichlorophenol-dehalogenating enzyme RdhA3 was observed. The impact of the amendment of Cba lower ligand precursors on RDase function was also investigated in Shimwellia blattae, the Cba producer used for the heterologous production of Desulfitobacterium RDases. The recombinant tetrachloroethene RDase (PceA Y51 ) appeared to be non-selective towards different Cbas. However, the functional production of the 1,2-dichloroethane-dihaloeliminating enzyme (DcaA) of Desulfitobacterium dichloroeliminans was completely prevented in cells producing 5,6-dimethylbenzimidazolyl-Cba, but substantially enhanced in cells that incorporated 5-methoxybenzimidazole into the Cba cofactor. The results of the study indicate the utilization of a range of different Cbas by Desulfitobacterium RDases with selected representatives apparently preferring distinct Cbas., (© 2018 The Authors. Microbial Biotechnology published by John Wiley & Sons Ltd and Society for Applied Microbiology.)

Published

2019

13. A multi-enzyme cascade reaction for the production of 6-hydroxyhexanoic acid.

Author

Srinivasamurthy VST, Böttcher D, and Bornscheuer UT

Subjects

Alcohol Dehydrogenase metabolism, Batch Cell Culture Techniques, Biocatalysis, Bioreactors, Caproates chemistry, Caproates metabolism, Coenzymes biosynthesis, Coenzymes chemistry, Escherichia coli genetics, Escherichia coli Proteins metabolism, Fungal Proteins metabolism, Gene Expression, Hydroxy Acids metabolism, Kinetics, Lactones chemistry, Lactones metabolism, Lipase metabolism, Mixed Function Oxygenases metabolism, NADP biosynthesis, NADP chemistry, Alcohol Dehydrogenase genetics, Caproates chemical synthesis, Escherichia coli enzymology, Escherichia coli Proteins genetics, Fungal Proteins chemistry, Hydroxy Acids chemical synthesis, Lipase chemistry, Mixed Function Oxygenases genetics

Abstract

Multi-enzyme cascade reactions capture the essence of nature's efficiency by increasing the productivity of a process. Here we describe one such three-enzyme cascade for the synthesis of 6-hydroxyhexanoic acid. Whole cells of Escherichia coli co-expressing an alcohol dehydrogenase and a Baeyer-Villiger monooxygenase (CHMO) for internal cofactor regeneration were used without the supply of external NADPH or NADP+. The product inhibition caused by the ε-caprolactone formed by the CHMO was overcome by the use of lipase CAL-B for in situ conversion into 6-hydroxyhexanoic acid. A stirred tank reactor under fed-batch mode was chosen for efficient catalysis. By using this setup, a product titre of >20 g L-1 was achieved in a 500 mL scale with an isolated yield of 81% 6-hydroxyhexanoic acid.

Published

2019

14. The peacefulness gene promotes aggression in Drosophila.

Author

Ramin M, Li Y, Chang WT, Shaw H, and Rao Y

Subjects

Animals, Avoidance Learning, Brain metabolism, Carbon-Carbon Lyases, Coenzymes biosynthesis, Drosophila Proteins metabolism, Gene Knockdown Techniques, Male, Metalloproteins biosynthesis, Molybdenum Cofactors, Motor Activity, Mutagenesis, Insertional genetics, Neurons metabolism, Nuclear Proteins metabolism, Pteridines, Sexual Behavior, Animal, Smell physiology, Aggression physiology, Drosophila Proteins genetics, Drosophila melanogaster genetics, Drosophila melanogaster physiology, Genes, Insect, Nuclear Proteins genetics

Abstract

Natural aggressiveness is commonly observed in all animal species, and is displayed frequently when animals compete for food, territory and mating. Aggression is an innate behaviour, and is influenced by both environmental and genetic factors. However, the genetics of aggression remains largely unclear. In this study, we identify the peacefulness (pfs) gene as a novel player in the control of male-male aggression in Drosophila. Mutations in pfs decreased intermale aggressiveness, but did not affect locomotor activity, olfactory avoidance response and sexual behaviours. pfs encodes for the evolutionarily conserved molybdenum cofactor (MoCo) synthesis 1 protein (Mocs1), which catalyzes the first step in the MoCo biosynthesis pathway. Neuronal-specific knockdown of pfs decreased aggressiveness. By contrast, overexpression of pfs greatly increased aggressiveness. Knocking down Cinnamon (Cin) catalyzing the final step in the MoCo synthesis pathway, caused a pfs-like aggression phenotype. In humans, inhibition of MoCo-dependent enzymes displays anti-aggressive effects. Thus, the control of aggression by Pfs-dependent MoCo pathways may be conserved throughout evolution.

Published

2019

15. From the Eukaryotic Molybdenum Cofactor Biosynthesis to the Moonlighting Enzyme mARC.

Author

Tejada-Jimenez M, Chamizo-Ampudia A, Calatrava V, Galvan A, Fernandez E, and Llamas A

Subjects

Animals, Cardiac Myosins metabolism, Coenzymes biosynthesis, Enzymes chemistry, Enzymes genetics, Eukaryotic Cells metabolism, Mammals, Metabolic Networks and Pathways, Metalloproteins biosynthesis, Molybdenum metabolism, Molybdenum Cofactors, Myosin Light Chains metabolism, Nitrate Reductase metabolism, Nitrites metabolism, Oxidoreductases genetics, Oxidoreductases metabolism, Coenzymes metabolism, Enzymes metabolism, Metalloproteins metabolism, Pteridines metabolism

Abstract

All eukaryotic molybdenum (Mo) enzymes contain in their active site a Mo Cofactor (Moco), which is formed by a tricyclic pyranopterin with a dithiolene chelating the Mo atom. Here, the eukaryotic Moco biosynthetic pathway and the eukaryotic Moco enzymes are overviewed, including nitrate reductase (NR), sulfite oxidase, xanthine oxidoreductase, aldehyde oxidase, and the last one discovered, the moonlighting enzyme mitochondrial Amidoxime Reducing Component (mARC). The mARC enzymes catalyze the reduction of hydroxylated compounds, mostly N-hydroxylated (NHC), but as well of nitrite to nitric oxide, a second messenger. mARC shows a broad spectrum of NHC as substrates, some are prodrugs containing an amidoxime structure, some are mutagens, such as 6-hydroxylaminepurine and some others, which most probably will be discovered soon. Interestingly, all known mARC need the reducing power supplied by different partners. For the NHC reduction, mARC uses cytochrome b5 and cytochrome b5 reductase, however for the nitrite reduction, plant mARC uses NR. Despite the functional importance of mARC enzymatic reactions, the structural mechanism of its Moco-mediated catalysis is starting to be revealed. We propose and compare the mARC catalytic mechanism of nitrite versus NHC reduction. By using the recently resolved structure of a prokaryotic MOSC enzyme, from the mARC protein family, we have modeled an in silico three-dimensional structure of a eukaryotic homologue., Competing Interests: The authors declare no conflict of interest.

Published

2018

16. Diversity of structures, catalytic mechanisms and processes of cofactor biosynthesis of tryptophylquinone-bearing enzymes.

Author

Yukl ET and Davidson VL

Subjects

Catalysis, Protein Conformation, Protein Processing, Post-Translational, Tryptophan metabolism, Coenzymes biosynthesis, Coenzymes chemistry, Indolequinones metabolism, Tryptophan analogs & derivatives

Abstract

Tryptophyquinone-bearing enzymes contain protein-derived cofactors formed by posttranslational modifications of Trp residues. Tryptophan tryptophylquinone (TTQ) is comprised of a di-oxygenated Trp residue, which is cross-linked to another Trp residue. Cysteine tryptophylquinone (CTQ) is comprised of a di-oxygenated Trp residue, which is cross-linked to a Cys residue. Despite the similarity of these cofactors, it has become evident in recent years that the overall structures of the enzymes that possess these cofactors vary, and that the gene clusters that encode the enzymes are quite diverse. While it had been long assumed that all tryptophylquinone enzymes were dehydrogenases, recently discovered classes of these enzymes are oxidases. A common feature of enzymes that have these cofactors is that the posttranslational modifications that form the mature cofactors are catalyzed by a modifying enzyme. However, it is now clear that modifying enzymes are different for different tryptophylquinone enzymes. For methylamine dehydrogenase a di-heme enzyme, MauG, is needed to catalyze TTQ biosynthesis. However, no gene similar to mauG is present in the gene clusters that encode the other enzymes, and the recently characterized family of CTQ-dependent oxidases, termed LodA-like proteins, require a flavoenzyme for cofactor biosynthesis., (Copyright © 2018. Published by Elsevier Inc.)

Published

2018

17. Mosaic patterns of B-vitamin synthesis and utilization in a natural marine microbial community.

Author

Gómez-Consarnau L, Sachdeva R, Gifford SM, Cutter LS, Fuhrman JA, Sañudo-Wilhelmy SA, and Moran MA

Subjects

Alphaproteobacteria genetics, Alphaproteobacteria metabolism, Bacteria genetics, Coenzymes biosynthesis, Coenzymes metabolism, Flavobacteriaceae genetics, Flavobacteriaceae metabolism, Transcriptome, Vitamin B Complex biosynthesis, Bacteria metabolism, Microbial Consortia, Vitamin B Complex metabolism

Abstract

Aquatic environments contain large communities of microorganisms whose synergistic interactions mediate the cycling of major and trace nutrients, including vitamins. B-vitamins are essential coenzymes that many organisms cannot synthesize. Thus, their exchange among de novo synthesizers and auxotrophs is expected to play an important role in the microbial consortia and explain some of the temporal and spatial changes observed in diversity. In this study, we analyzed metatranscriptomes of a natural marine microbial community, diel sampled quarterly over one year to try to identify the potential major B-vitamin synthesizers and consumers. Transcriptomic data showed that the best-represented taxa dominated the expression of synthesis genes for some B-vitamins but lacked transcripts for others. For instance, Rhodobacterales dominated the expression of vitamin-B 12 synthesis, but not of vitamin-B 7 , whose synthesis transcripts were mainly represented by Flavobacteria. In contrast, bacterial groups that constituted less than 4% of the community (e.g., Verrucomicrobia) accounted for most of the vitamin-B 1 synthesis transcripts. Furthermore, ambient vitamin-B 1 concentrations were higher in samples collected during the day, and were positively correlated with chlorophyll-a concentrations. Our analysis supports the hypothesis that the mosaic of metabolic interdependencies through B-vitamin synthesis and exchange are key processes that contribute to shaping microbial communities in nature., (© 2018 Society for Applied Microbiology and John Wiley & Sons Ltd.)

Published

2018

18. Translucent larval integument and flaccid paralysis caused by genome editing in a gene governing molybdenum cofactor biosynthesis in Bombyx mori.

Author

Fujii T, Yamamoto K, and Banno Y

Subjects

Animals, Larva, Molybdenum Cofactors, Bombyx genetics, Bombyx metabolism, Coenzymes biosynthesis, Coenzymes genetics, Gene Editing, Insect Proteins genetics, Insect Proteins metabolism, Metalloproteins biosynthesis, Metalloproteins genetics, Pteridines

Abstract

Translucency of the larval integument in Bombyx mori is caused by a lack of uric acid in the epidermis. Hime'nichi translucent (ohi) is a unique mutation causing intermediate translucency of the larval integument and male-specific flaccid paralysis. To determine the gene associated with the ohi mutation, the ohi locus was mapped to a 400-kb region containing 29 predicted genes. Among the genes in this region, we focused on Bombyx homolog of mammalian Gephyrin (BmGphn), which regulates molybdenum cofactor (MoCo) biosynthesis, because MoCo is indispensable for the activity of xanthine dehydrogenase (XDH), a key enzyme in uric acid biosynthesis. The translucent integument of ohi larvae turned opaque after injection of bovine xanthine oxidase, which is a mammalian equivalent to XDH, indicating that XDH activity is defective in ohi larvae. RT-PCR and sequencing analysis showed that (i) in ohi larvae, expression of the BmGphn gene was repressed in the fat body where uric acid is synthesized, and (ii) there was no amino acid substitution in the ohi mutant allele. Finally, we obtained BmGphn knockout alleles (hereafter denoted as BmGphn Δ ) by using CRISPR/Cas9. The resulting ohi/BmGphn Δ larvae had translucent integuments, demonstrating that BmGphn is the gene responsible for the ohi phenotype. Our results show that repressed expression of BmGphn is a causative factor for the defective MoCo biosynthesis and XDH activity observed in ohi larvae. Interestingly, all male BmGphn Δ homozygotes died before pupation and showed a flaccid paralysis phenotype. The genetic and physiological mechanisms underlying this flaccid paralysis phenotype are also discussed., (Copyright © 2018 Elsevier Ltd. All rights reserved.)

Published

2018

19. C-C bond forming radical SAM enzymes involved in the construction of carbon skeletons of cofactors and natural products.

Author

Yokoyama K and Lilla EA

Subjects

Adenine analogs & derivatives, Adenine biosynthesis, Bacterial Proteins chemistry, Bacterial Proteins metabolism, Bacteriochlorophylls biosynthesis, Biological Products metabolism, Carbon chemistry, Coenzymes chemistry, Endopeptidases chemistry, Endopeptidases metabolism, Hydrolases chemistry, Hydrolases metabolism, Molybdenum chemistry, Molybdenum metabolism, Tunicamycin biosynthesis, Vitamin K 2 metabolism, Biological Products chemistry, Coenzymes biosynthesis, Enzymes chemistry, Enzymes metabolism, S-Adenosylmethionine metabolism

Abstract

Covering: up to the end of 2017 C-C bond formations are frequently the key steps in cofactor and natural product biosynthesis. Historically, C-C bond formations were thought to proceed by two electron mechanisms, represented by Claisen condensation in fatty acids and polyketide biosynthesis. These types of mechanisms require activated substrates to create a nucleophile and an electrophile. More recently, increasing number of C-C bond formations catalyzed by radical SAM enzymes are being identified. These free radical mediated reactions can proceed between almost any sp3 and sp2 carbon centers, allowing introduction of C-C bonds at unconventional positions in metabolites. Therefore, free radical mediated C-C bond formations are frequently found in the construction of structurally unique and complex metabolites. This review discusses our current understanding of the functions and mechanisms of C-C bond forming radical SAM enzymes and highlights their important roles in the biosynthesis of structurally complex, naturally occurring organic molecules. Mechanistic consideration of C-C bond formation by radical SAM enzymes identifies the significance of three key mechanistic factors: radical initiation, acceptor substrate activation and radical quenching. Understanding the functions and mechanisms of these characteristic enzymes will be important not only in promoting our understanding of radical SAM enzymes, but also for understanding natural product and cofactor biosynthesis.

Published

2018

20. Genetic dissection of cyclic pyranopterin monophosphate biosynthesis in plant mitochondria.

Author

Kruse I, Maclean AE, Hill L, and Balk J

Subjects

ATP-Binding Cassette Transporters metabolism, Amino Acid Sequence, Ammonia pharmacology, Arabidopsis drug effects, Arabidopsis growth & development, Arabidopsis metabolism, Arabidopsis Proteins metabolism, Chromatography, Liquid, Coenzymes biosynthesis, Gene Deletion, Metalloproteins biosynthesis, Mitochondria ultrastructure, Molybdenum Cofactors, Plant Cells metabolism, Plant Cells ultrastructure, Polymorphism, Single Nucleotide, Protein Isoforms genetics, Protein Isoforms metabolism, Pteridines, Seedlings drug effects, Seedlings genetics, Seedlings growth & development, Seedlings metabolism, Sequence Alignment, Sequence Homology, Amino Acid, Signal Transduction, Tandem Mass Spectrometry, ATP-Binding Cassette Transporters genetics, Arabidopsis genetics, Arabidopsis Proteins genetics, Gene Expression Regulation, Plant, Mitochondria metabolism, Organophosphorus Compounds metabolism, Pterins metabolism

Abstract

Mitochondria play a key role in the biosynthesis of two metal cofactors, iron-sulfur (FeS) clusters and molybdenum cofactor (Moco). The two pathways intersect at several points, but a scarcity of mutants has hindered studies to better understand these links. We screened a collection of sirtinol-resistant Arabidopsis thaliana mutants for lines with decreased activities of cytosolic FeS enzymes and Moco enzymes. We identified a new mutant allele of ATM3 ( ABC transporter of the mitochondria 3 ), encoding the ATP-binding cassette transporter of the mitochondria 3 (systematic name ABCB25), confirming the previously reported role of ATM3 in both FeS cluster and Moco biosynthesis. We also identified a mutant allele in CNX2 , cofactor of nitrate reductase and xanthine dehydrogenase 2 , encoding GTP 3',8-cyclase, the first step in Moco biosynthesis which is localized in the mitochondria. A single-nucleotide polymorphism in cnx2-2 leads to substitution of Arg88 with Gln in the N-terminal FeS cluster-binding motif. cnx2-2 plants are small and chlorotic, with severely decreased Moco enzyme activities, but they performed better than a cnx2-1 knockout mutant, which could only survive with ammonia as a nitrogen source. Measurement of cyclic pyranopterin monophosphate (cPMP) levels by LC-MS/MS showed that this Moco intermediate was below the limit of detection in both cnx2-1 and cnx2-2 , and accumulated more than 10-fold in seedlings mutated in the downstream gene CNX5 Interestingly, atm3-1 mutants had less cPMP than wild type, correlating with previous reports of a similar decrease in nitrate reductase activity. Taken together, our data functionally characterize CNX2 and suggest that ATM3 is indirectly required for cPMP synthesis., (© 2018 The Author(s).)

Published

2018

21. Radical Breakthroughs in Natural Product and Cofactor Biosynthesis.

Author

Yokoyama K

Subjects

Carbon-Carbon Lyases, Crystallography, X-Ray, Guanosine Triphosphate metabolism, Humans, Models, Molecular, Molecular Structure, Molybdenum Cofactors, Protein Conformation, Pteridines, Recombinant Proteins metabolism, S-Adenosylmethionine metabolism, Biological Products, Coenzymes biosynthesis, Escherichia coli Proteins metabolism, Isomerases metabolism, Metalloproteins biosynthesis, Nuclear Proteins metabolism, Organophosphorus Compounds metabolism, Pterins metabolism

Abstract

The radical SAM (S-adenosyl-l-methionine) superfamily is one of the largest group of enzymes with >113000 annotated sequences [Landgraf, B. J., et al. (2016) Annu. Rev. Biochem. 85, 485-514]. Members of this superfamily catalyze the reductive cleavage of SAM using an oxygen sensitive 4Fe-4S cluster to transiently generate 5'-deoxyadenosyl radical that is subsequently used to initiate diverse free radical-mediated reactions. Because of the unique reactivity of free radicals, radical SAM enzymes frequently catalyze chemically challenging reactions critical for the biosynthesis of unique structures of cofactors and natural products. In this Perspective, I will discuss the impact of characterizing novel functions in radical SAM enzymes on our understanding of biosynthetic pathways and use two recent examples from my own group with a particular emphasis on two radical SAM enzymes that are responsible for carbon skeleton formation during the biosynthesis of a cofactor and natural products.

Published

2018

22. Lessons From the Studies of a CC Bond Forming Radical SAM Enzyme in Molybdenum Cofactor Biosynthesis.

Author

Pang H and Yokoyama K

Subjects

Escherichia coli Proteins isolation & purification, Hydrolases isolation & purification, Metabolic Networks and Pathways, Molybdenum Cofactors, Organophosphorus Compounds metabolism, Pteridines, Pterins metabolism, Recombinant Proteins isolation & purification, Recombinant Proteins metabolism, Coenzymes biosynthesis, Enzyme Assays methods, Escherichia coli Proteins metabolism, Hydrolases metabolism, Metalloproteins biosynthesis

Abstract

MoaA is one of the founding members of the radical S-adenosyl- L -methionine (SAM) superfamily, and together with the second enzyme, MoaC, catalyzes the construction of the pyranopterin backbone structure of the molybdenum cofactor (Moco). However, the exact functions of both MoaA and MoaC had remained ambiguous for more than 2 decades. Recently, their functions were finally elucidated through successful characterization of the MoaA product as 3',8-cyclo-7,8-dihydro-GTP (3',8-cH 2 GTP), which was shown to be converted to cyclic pyranopterin monophosphate (cPMP) by MoaC. 3',8-cH 2 GTP was produced in a small quantity and was highly oxygen sensitive, which explains why this compound had previously eluded characterization. This chapter describes the methodologies for the characterization of MoaA, MoaC, and 3',8-cH 2 GTP, which together significantly altered the view of the mechanism of the pyranopterin backbone construction during the Moco biosynthesis. Through this chapter, we hope to share not only the protocols to study the first step of Moco biosynthesis but also the lessons we learned from the characterization of the chemically labile biosynthetic intermediate, which would be informative for the study of many other metabolic pathways and enzymes., (© 2018 Elsevier Inc. All rights reserved.)

Published

2018

23. Horizontal acquisition of a hypoxia-responsive molybdenum cofactor biosynthesis pathway contributed to Mycobacterium tuberculosis pathoadaptation.

Author

Levillain F, Poquet Y, Mallet L, Mazères S, Marceau M, Brosch R, Bange FC, Supply P, Magalon A, and Neyrolles O

Subjects

Animals, Bacterial Proteins genetics, Bacterial Proteins metabolism, Female, Gene Expression Regulation, Bacterial, Humans, Hypoxia metabolism, Hypoxia microbiology, Mice, Mice, Inbred C57BL, Molybdenum Cofactors, Mycobacterium genetics, Mycobacterium metabolism, Nitrates metabolism, Pteridines, Tuberculosis metabolism, Coenzymes biosynthesis, Gene Transfer, Horizontal, Metalloproteins biosynthesis, Mycobacterium tuberculosis genetics, Mycobacterium tuberculosis metabolism, Oxygen metabolism, Tuberculosis microbiology

Abstract

The unique ability of the tuberculosis (TB) bacillus, Mycobacterium tuberculosis, to persist for long periods of time in lung hypoxic lesions chiefly contributes to the global burden of latent TB. We and others previously reported that the M. tuberculosis ancestor underwent massive episodes of horizontal gene transfer (HGT), mostly from environmental species. Here, we sought to explore whether such ancient HGT played a part in M. tuberculosis evolution towards pathogenicity. We were interested by a HGT-acquired M. tuberculosis-specific gene set, namely moaA1-D1, which is involved in the biosynthesis of the molybdenum cofactor. Horizontal acquisition of this gene set was striking because homologues of these moa genes are present all across the Mycobacterium genus, including in M. tuberculosis. Here, we discovered that, unlike their paralogues, the moaA1-D1 genes are strongly induced under hypoxia. In vitro, a M. tuberculosis moaA1-D1-null mutant has an impaired ability to respire nitrate, to enter dormancy and to survive in oxygen-limiting conditions. Conversely, heterologous expression of moaA1-D1 in the phylogenetically closest non-TB mycobacterium, Mycobacterium kansasii, which lacks these genes, improves its capacity to respire nitrate and grants it with a marked ability to survive oxygen depletion. In vivo, the M. tuberculosis moaA1-D1-null mutant shows impaired survival in hypoxic granulomas in C3HeB/FeJ mice, but not in normoxic lesions in C57BL/6 animals. Collectively, our results identify a novel pathway required for M. tuberculosis resistance to host-imposed stress, namely hypoxia, and provide evidence that ancient HGT bolstered M. tuberculosis evolution from an environmental species towards a pervasive human-adapted pathogen.

Published

2017

24. Differential carriage of virulence-associated loci in the New Zealand Rangipo outbreak strain of Mycobacterium tuberculosis.

Author

Gautam SS, Mac Aogáin M, Bower JE, Basu I, and O'Toole RF

Subjects

Bacterial Proteins genetics, Coenzymes biosynthesis, Coenzymes genetics, Genetic Variation, Genotype, High-Throughput Nucleotide Sequencing, Humans, Metalloproteins biosynthesis, Metalloproteins genetics, Molybdenum Cofactors, New Zealand epidemiology, Pteridines, Tuberculosis epidemiology, Virulence genetics, Whole Genome Sequencing, Carrier State microbiology, Disease Outbreaks, Genetic Loci, Genome, Bacterial, Mycobacterium tuberculosis genetics, Mycobacterium tuberculosis pathogenicity, Tuberculosis microbiology

Abstract

Background: The Rangipo strain of Mycobacterium tuberculosis achieved notoriety in New Zealand due to its role in several tuberculosis (TB) outbreaks. Why this strain should be the source of relatively large clusters of the disease is unknown. In this work, we performed an in-depth analysis of the genome of the Rangipo strain to determine whether it offers clues to understanding its prevalence., Methods: Next-generation sequencing was performed on nine isolates which matched the Rangipo genotypic profile. Sequence reads were assembled against the H37Rv reference genome and single-locus variants identified. Unmapped reads were compared against the genome sequences of other M. tuberculosis strains, in particular CDC1551, Haarlem and Erdman., Results: Across the nine Rangipo strains, a total of 727 single-locus variants were identified with respect to H37Rv, of which 700 were common to all Rangipo strains sequenced. Within the common variants, 386 were non-synonymous, with 12 occurring in genes associated with M. tuberculosis virulence. Next-generation and Sanger sequencing determined the presence of three genes in the Rangipo isolates, which are absent in H37Rv, but which have been reported to be important for the pathogenicity of M. tuberculosis. The differentially encoded Rangipo genes consisted of transcriptional regulator EmbR2, and molybdopterin cofactor biosynthesis proteins A and B. The Rangipo strain also harbours an extended DNA helicase and an additional adenylate cyclase., Conclusions: Our study provides new insights into the genomic content of the New Zealand Rangipo strain of M. tuberculosis and highlights the presence of additional virulence-related loci not found in H37Rv.

Published

2017

25. Functional Complementation Studies Reveal Different Interaction Partners of Escherichia coli IscS and Human NFS1.

Author

Bühning M, Friemel M, and Leimkühler S

Subjects

Binding Sites, Humans, Molybdenum Cofactors, Nucleotidyltransferases metabolism, RNA, Bacterial genetics, RNA, Bacterial metabolism, RNA, Transfer metabolism, Sulfurtransferases metabolism, Carbon-Sulfur Lyases genetics, Carbon-Sulfur Lyases metabolism, Coenzymes biosynthesis, Coenzymes genetics, Escherichia coli enzymology, Escherichia coli genetics, Genetic Complementation Test, Metalloproteins biosynthesis, Metalloproteins genetics, Pteridines

Abstract

The trafficking and delivery of sulfur to cofactors and nucleosides is a highly regulated and conserved process among all organisms. All sulfur transfer pathways generally have an l-cysteine desulfurase as an initial sulfur-mobilizing enzyme in common, which serves as a sulfur donor for the biosynthesis of sulfur-containing biomolecules like iron-sulfur (Fe-S) clusters, thiamine, biotin, lipoic acid, the molybdenum cofactor (Moco), and thiolated nucleosides in tRNA. The human l-cysteine desulfurase NFS1 and the Escherichia coli homologue IscS share a level of amino acid sequence identity of ∼60%. While E. coli IscS has a versatile role in the cell and was shown to have numerous interaction partners, NFS1 is mainly localized in mitochondria with a crucial role in the biosynthesis of Fe-S clusters. Additionally, NFS1 is also located in smaller amounts in the cytosol with a role in Moco biosynthesis and mcm 5 s 2 U34 thio modifications of nucleosides in tRNA. NFS1 and IscS were conclusively shown to have different interaction partners in their respective organisms. Here, we used functional complementation studies of an E. coli iscS deletion strain with human NFS1 to dissect their conserved roles in the transfer of sulfur to a specific target protein. Our results show that human NFS1 and E. coli IscS share conserved binding sites for proteins involved in Fe-S cluster assembly like IscU, but not with proteins for tRNA thio modifications or Moco biosynthesis. In addition, we show that human NFS1 was almost fully able to complement the role of IscS in Moco biosynthesis when its specific interaction partner protein MOCS3 from humans was also present.

Published

2017

26. Shared function and moonlighting proteins in molybdenum cofactor biosynthesis.

Author

Leimkühler S

Subjects

Animals, Humans, Molybdenum Cofactors, Organophosphorus Compounds metabolism, Pteridines, Pterins metabolism, Archaeal Proteins metabolism, Bacterial Proteins metabolism, Coenzymes biosynthesis, Metalloproteins biosynthesis

Abstract

The biosynthesis of the molybdenum cofactor (Moco) is a highly conserved pathway in bacteria, archaea and eukaryotes. The molybdenum atom in Moco-containing enzymes is coordinated to the dithiolene group of a tricyclic pyranopterin monophosphate cofactor. The biosynthesis of Moco can be divided into three conserved steps, with a fourth present only in bacteria and archaea: (1) formation of cyclic pyranopterin monophosphate, (2) formation of molybdopterin (MPT), (3) insertion of molybdenum into MPT to form Mo-MPT, and (4) additional modification of Mo-MPT in bacteria with the attachment of a GMP or CMP nucleotide, forming the dinucleotide variants of Moco. While the proteins involved in the catalytic reaction of each step of Moco biosynthesis are highly conserved among the Phyla, a surprising link to other cellular pathways has been identified by recent discoveries. In particular, the pathways for FeS cluster assembly and thio-modifications of tRNA are connected to Moco biosynthesis by sharing the same protein components. Further, proteins involved in Moco biosynthesis are not only shared with other pathways, but additionally have moonlighting roles. This review gives an overview of Moco biosynthesis in bacteria and humans and highlights the shared function and moonlighting roles of the participating proteins.

Published

2017

27. Whole transcriptomic and proteomic analyses of an isogenic M. tuberculosis clinical strain with a naturally occurring 15 Kb genomic deletion.

Author

Duncan C, Jamieson FB, Troudt J, Izzo L, Bielefeldt-Ohmann H, Izzo A, and Mehaffy C

Subjects

Animals, Bacterial Proteins biosynthesis, Bacterial Proteins genetics, Coenzymes biosynthesis, Coenzymes genetics, DNA-Binding Proteins, Disease Models, Animal, Gene Expression Profiling, Guinea Pigs, Humans, Lipid Metabolism genetics, Metalloproteins biosynthesis, Metalloproteins genetics, Molybdenum Cofactors, Multigene Family, Mycobacterium tuberculosis metabolism, Mycobacterium tuberculosis pathogenicity, Protein Kinases genetics, Proteomics, Pteridines, Regulon, Tuberculosis, Pulmonary microbiology, Virulence genetics, Gene Deletion, Genome, Bacterial, Mycobacterium tuberculosis genetics

Abstract

Tuberculosis remains one of the most difficult to control infectious diseases in the world. Many different factors contribute to the complexity of this disease. These include the ability of the host to control the infection which may directly relate to nutritional status, presence of co-morbidities and genetic predisposition. Pathogen factors, in particular the ability of different Mycobacterium tuberculosis strains to respond to the harsh environment of the host granuloma, which includes low oxygen and nutrient availability and the presence of damaging radical oxygen and nitrogen species, also play an important role in the success of different strains to cause disease. In this study we evaluated the impact of a naturally occurring 12 gene 15 Kb genomic deletion on the physiology and virulence of M. tuberculosis. The strains denominated ON-A WT (wild type) and ON-A NM (natural mutant) were isolated from a previously reported TB outbreak in an inner city under-housed population in Toronto, Canada. Here we subjected these isogenic strains to transcriptomic (via RNA-seq) and proteomic analyses and identified several gene clusters with differential expression in the natural mutant, including the DosR regulon and the molybdenum cofactor biosynthesis genes, both of which were found in lower abundance in the natural mutant. We also demonstrated lesser virulence of the natural mutant in the guinea pig animal model. Overall, our findings suggest that the ON-A natural mutant is less fit to cause disease, but nevertheless has the potential to cause extended transmission in at-risk populations.

Published

2017

28. Optimization of overexpression of a chaperone protein of steroid C25 dehydrogenase for biochemical and biophysical characterization.

Author

Niedzialkowska E, Mrugała B, Rugor A, Czub MP, Skotnicka A, Cotelesage JJH, George GN, Szaleniec M, Minor W, and Lewiński K

Subjects

Escherichia coli chemistry, Escherichia coli genetics, Molybdenum Cofactors, Nitrosomonadaceae metabolism, Recombinant Proteins biosynthesis, Recombinant Proteins chemistry, Recombinant Proteins genetics, Recombinant Proteins isolation & purification, Bacterial Proteins biosynthesis, Bacterial Proteins chemistry, Bacterial Proteins genetics, Bacterial Proteins isolation & purification, Coenzymes biosynthesis, Coenzymes chemistry, Coenzymes genetics, Coenzymes isolation & purification, Escherichia coli metabolism, Gene Expression, Metalloproteins biosynthesis, Metalloproteins chemistry, Metalloproteins genetics, Metalloproteins isolation & purification, Molecular Chaperones biosynthesis, Molecular Chaperones chemistry, Molecular Chaperones genetics, Molecular Chaperones isolation & purification, Nitrosomonadaceae genetics, Pteridines chemistry, Pteridines isolation & purification

Abstract

Molybdenum is an essential nutrient for metabolism in plant, bacteria, and animals. Molybdoenzymes are involved in nitrogen assimilation and oxidoreductive detoxification, and bioconversion reactions of environmental, industrial, and pharmaceutical interest. Molybdoenzymes contain a molybdenum cofactor (Moco), which is a pyranopterin heterocyclic compound that binds a molybdenum atom via a dithiolene group. Because Moco is a large and complex compound deeply buried within the protein, molybdoenzymes are accompanied by private chaperone proteins responsible for the cofactor's insertion into the enzyme and the enzyme's maturation. An efficient recombinant expression and purification of both Moco-free and Moco-containing molybdoenzymes and their chaperones is of paramount importance for fundamental and applied research related to molybdoenzymes. In this work, we focused on a D1 protein annotated as a chaperone of steroid C25 dehydrogenase (S25DH) from Sterolibacterium denitrificans Chol-1S. The D1 protein is presumably involved in the maturation of S25DH engaged in oxygen-independent oxidation of sterols. As this chaperone is thought to be a crucial element that ensures the insertion of Moco into the enzyme and consequently, proper folding of S25DH optimization of the chaperon's expression is the first step toward the development of recombinant expression and purification methods for S25DH. We have identified common E. coli strains and conditions for both expression and purification that allow us to selectively produce Moco-containing and Moco-free chaperones. We have also characterized the Moco-containing chaperone by EXAFS and HPLC analysis and identified conditions that stabilize both forms of the protein. The protocols presented here are efficient and result in protein quantities sufficient for biochemical studies., (Copyright © 2017 Elsevier Inc. All rights reserved.)

Published

2017

29. The Role of SufS Is Restricted to Fe-S Cluster Biosynthesis in Escherichia coli.

Author

Bühning M, Valleriani A, and Leimkühler S

Subjects

Carbon-Sulfur Lyases genetics, Coenzymes biosynthesis, Escherichia coli genetics, Escherichia coli Proteins genetics, Escherichia coli Proteins metabolism, Iron-Sulfur Proteins genetics, Isomerases genetics, Isomerases metabolism, Lyases genetics, Metalloproteins biosynthesis, Molybdenum Cofactors, Operon, Pteridines, RNA, Transfer genetics, RNA, Transfer metabolism, Recombinant Proteins genetics, Recombinant Proteins metabolism, Sulfurtransferases genetics, Sulfurtransferases metabolism, Thiouridine analogs & derivatives, Thiouridine metabolism, Carbon-Sulfur Lyases metabolism, Escherichia coli metabolism, Gene Expression Regulation, Bacterial, Iron-Sulfur Proteins metabolism, Lyases metabolism

Abstract

In Escherichia coli, two different systems that are important for the coordinate formation of Fe-S clusters have been identified, namely, the ISC and SUF systems. The ISC system is the housekeeping Fe-S machinery, which provides Fe-S clusters for numerous cellular proteins. The IscS protein of this system was additionally revealed to be the primary sulfur donor for several sulfur-containing molecules with important biological functions, among which are the molybdenum cofactor (Moco) and thiolated nucleosides in tRNA. Here, we show that deletion of central components of the ISC system in addition to IscS leads to an overall decrease in Fe-S cluster enzyme and molybdoenzyme activity in addition to a decrease in the number of Fe-S-dependent thiomodifications of tRNA, based on the fact that some proteins involved in Moco biosynthesis and tRNA thiolation are Fe-S-dependent. Complementation of the ISC deficient strains with the suf operon restored the activity of Fe-S-containing proteins, including the MoaA protein, which is involved in the conversion of 5'GTP to cyclic pyranopterin monophosphate in the fist step of Moco biosynthesis. While both systems share a high degree of similarity, we show that the function of their respective l-cysteine desulfurase IscS or SufS is specific for each cellular pathway. It is revealed that SufS cannot play the role of IscS in sulfur transfer for the formation of 2-thiouridine, 4-thiouridine, or the dithiolene group of molybdopterin, being unable to interact with TusA or ThiI. The results demonstrate that the role of the SUF system is exclusively restricted to Fe-S cluster assembly in the cell.

Published

2017

30. Iron assimilation and utilization in anaerobic ammonium oxidizing bacteria.

Author

Ferousi C, Lindhoud S, Baymann F, Kartal B, Jetten MS, and Reimann J

Subjects

Biological Transport, Coenzymes biosynthesis, Oxidation-Reduction, Ammonium Compounds metabolism, Bacteria, Anaerobic metabolism, Iron metabolism

Abstract

The most abundant transition metal in biological systems is iron. It is incorporated into protein cofactors and serves either catalytic, redox or regulatory purposes. Anaerobic ammonium oxidizing (anammox) bacteria rely heavily on iron-containing proteins - especially cytochromes - for their energy conservation, which occurs within a unique organelle, the anammoxosome. Both their anaerobic lifestyle and the presence of an additional cellular compartment challenge our understanding of iron processing. Here, we combine existing concepts of iron uptake, utilization and metabolism, and cellular fate with genomic and still limited biochemical and physiological data on anammox bacteria to propose pathways these bacteria may employ., (Copyright © 2017 The Authors. Published by Elsevier Ltd.. All rights reserved.)

Published

2017

31. The conserved hypothetical protein PSPTO_3957 is essential for virulence in the plant pathogen Pseudomonas syringae pv. tomato DC3000.

Author

D'Amico K and Filiatrault MJ

Subjects

Base Sequence, Coenzymes biosynthesis, Coenzymes genetics, Conserved Sequence, Gene Expression Regulation, Bacterial, Metalloproteins biosynthesis, Metalloproteins genetics, Molybdenum Cofactors, Nitrates metabolism, Promoter Regions, Genetic, Pseudomonas syringae metabolism, Pteridines, Sigma Factor genetics, Virulence genetics, Bacterial Proteins genetics, Solanum lycopersicum microbiology, Plant Diseases microbiology, Pseudomonas syringae genetics, Pseudomonas syringae pathogenicity

Abstract

The plant pathogen Pseudomonas syringae accounts for substantial crop losses and is considered an important agricultural issue. To better manage disease in the field, it is important to have an understanding of the underlying genetic mechanisms that mediate virulence. There are a substantial number of genes in sequenced bacterial genomes, including P. syringae, that encode for conserved hypothetical proteins; some of these have been functionally characterized in other Pseudomonads and have been demonstrated to play important roles in disease. PSPTO_3957 encodes a conserved hypothetical protein of unknown function. To evaluate the role of PSPTO_3957 in P. syringae pv. tomato DC3000, a PSPTO_3957 deletion mutant was constructed. Here, we show that PSPTO_3957 does not influence growth on rich media, motility or biofilm formation but is necessary for nitrate assimilation and full virulence in P. syringae. Our results have revealed an important role for PSPTO_3957 in the biology of P. syringae. Given the conservation of this protein among many bacteria, this protein might serve as an attractive target for disease management of this and other bacterial plant pathogens., (Published by Oxford University Press on behalf of FEMS 2017. This work is written by (a) US Government employee(s) and is in the public domain in the US.)

Published

2017

32. Elucidation of the biosynthesis of the methane catalyst coenzyme F 430 .

Author

Moore SJ, Sowa ST, Schuchardt C, Deery E, Lawrence AD, Ramos JV, Billig S, Birkemeyer C, Chivers PT, Howard MJ, Rigby SE, Layer G, and Warren MJ

Subjects

Amidohydrolases genetics, Amidohydrolases metabolism, Coenzymes chemistry, Lyases genetics, Lyases metabolism, Metalloporphyrins chemistry, Methane analogs & derivatives, Methane metabolism, Methanosarcina barkeri genetics, Methanosarcina barkeri metabolism, Multigene Family, Nickel metabolism, Oxidoreductases genetics, Oxidoreductases metabolism, Tetrapyrroles chemistry, Uroporphyrins chemistry, Uroporphyrins metabolism, Biocatalysis, Biosynthetic Pathways genetics, Coenzymes biosynthesis, Metalloporphyrins metabolism, Methane biosynthesis, Methanosarcina barkeri enzymology, Tetrapyrroles biosynthesis

Abstract

Methane biogenesis in methanogens is mediated by methyl-coenzyme M reductase, an enzyme that is also responsible for the utilization of methane through anaerobic methane oxidation. The enzyme uses an ancillary factor called coenzyme F 430 , a nickel-containing modified tetrapyrrole that promotes catalysis through a methyl radical/Ni(ii)-thiolate intermediate. However, it is unclear how coenzyme F 430 is synthesized from the common primogenitor uroporphyrinogen iii, incorporating 11 steric centres into the macrocycle, although the pathway must involve chelation, amidation, macrocyclic ring reduction, lactamization and carbocyclic ring formation. Here we identify the proteins that catalyse the biosynthesis of coenzyme F 430 from sirohydrochlorin, termed CfbA-CfbE, and demonstrate their activity. The research completes our understanding of how the repertoire of tetrapyrrole-based pigments are constructed, permitting the development of recombinant systems to use these metalloprosthetic groups more widely.

Published

2017

33. The methanogenic redox cofactor F 420 is widely synthesized by aerobic soil bacteria.

Author

Ney B, Ahmed FH, Carere CR, Biswas A, Warden AC, Morales SE, Pandey G, Watt SJ, Oakeshott JG, Taylor MC, Stott MB, Jackson CJ, and Greening C

Subjects

Aerobiosis, Archaea classification, Archaea enzymology, Archaea isolation & purification, Archaeal Proteins genetics, Archaeal Proteins metabolism, Bacteria classification, Bacteria enzymology, Bacteria isolation & purification, Bacterial Proteins genetics, Bacterial Proteins metabolism, Coenzymes genetics, Ecosystem, Metagenome, Oxidation-Reduction, Phylogeny, Soil chemistry, Archaea metabolism, Bacteria metabolism, Coenzymes biosynthesis, Methane metabolism, Soil Microbiology

Abstract

F 420 is a low-potential redox cofactor that mediates the transformations of a wide range of complex organic compounds. Considered one of the rarest cofactors in biology, F 420 is best known for its role in methanogenesis and has only been chemically identified in two phyla to date, the Euryarchaeota and Actinobacteria. In this work, we show that this cofactor is more widely distributed than previously reported. We detected the genes encoding all five known F 420 biosynthesis enzymes (cofC, cofD, cofE, cofG and cofH) in at least 653 bacterial and 173 archaeal species, including members of the dominant soil phyla Proteobacteria, Chloroflexi and Firmicutes. Metagenome datamining validated that these genes were disproportionately abundant in aerated soils compared with other ecosystems. We confirmed through high-performance liquid chromatography analysis that aerobically grown stationary-phase cultures of three bacterial species, Paracoccus denitrificans, Oligotropha carboxidovorans and Thermomicrobium roseum, synthesized F 420 , with oligoglutamate sidechains of different lengths. To understand the evolution of F 420 biosynthesis, we also analyzed the distribution, phylogeny and genetic organization of the cof genes. Our data suggest that although the F o precursor to F 420 originated in methanogens, F 420 itself was first synthesized in an ancestral actinobacterium. F 420 biosynthesis genes were then disseminated horizontally to archaea and other bacteria. Together, our findings suggest that the cofactor is more significant in aerobic bacterial metabolism and soil ecosystem composition than previously thought. The cofactor may confer several competitive advantages for aerobic soil bacteria by mediating their central metabolic processes and broadening the range of organic compounds they can synthesize, detoxify and mineralize.

Published

2017

34. Identification of a protein-protein interaction network downstream of molybdenum cofactor biosynthesis in Arabidopsis thaliana.

Author

Kaufholdt D, Baillie CK, Meyer MH, Schwich OD, Timmerer UL, Tobias L, van Thiel D, Hänsch R, and Mendel RR

Subjects

Arabidopsis enzymology, Arabidopsis Proteins metabolism, Biosynthetic Pathways, Fluorescence, Molybdenum Cofactors, Plants, Genetically Modified, Protein Binding, Pteridines, Sulfite Oxidase metabolism, Arabidopsis metabolism, Coenzymes biosynthesis, Metalloproteins biosynthesis, Protein Interaction Maps

Abstract

The molybdenum cofactor (Moco) is ubiquitously present in all kingdoms of life and vitally important for survival. Among animals, loss of the Moco-containing enzyme (Mo-enzyme) sulphite oxidase is lethal, while for plants the loss of nitrate reductase prohibits nitrogen assimilation. Moco is highly oxygen-sensitive, which obviates a freely diffusible pool and necessitates protein-mediated distribution. During the highly conserved Moco biosynthesis pathway, intermediates are channelled through a multi-protein complex facilitating protected transport. However, the mechanism by which Moco is subsequently transferred to apo-enzymes is still unclear. Moco user enzymes can be divided into two families: the sulphite oxidase (SO) and the xanthine oxidoreductase (XOR) family. The latter requires a final sulphurisation of Moco catalysed via ABA3. To examine Moco transfer towards apo-Mo-enzymes, two different and independent protein-protein interaction assays were performed in vivo: bimolecular fluorescence complementation and split luciferase. The results revealed a direct contact between Moco producer molybdenum insertase CNX1, which represents the last biosynthesis step, and members of the SO family. However, no protein contact was observed between Moco producer CNX1 and apo-enzymes of the XOR family or between CNX1 and the Moco sulphurase ABA3. Instead, the Moco-binding protein MOBP2 was identified as a mediator between CNX1 and ABA3. This interaction was followed by contact between ABA3 and enzymes of the XOR family. These results allow to describe an interaction matrix of proteins beyond Moco biosynthesis and to demonstrate the complexity of transferring a prosthetic group after biosynthesis., (Copyright © 2016 Elsevier GmbH. All rights reserved.)

Published

2016

35. Structure of the Reduced Copper Active Site in Preprocessed Galactose Oxidase: Ligand Tuning for One-Electron O 2 Activation in Cofactor Biogenesis.

Author

Cowley RE, Cirera J, Qayyum MF, Rokhsana D, Hedman B, Hodgson KO, Dooley DM, and Solomon EI

Subjects

Electron Transport, Ligands, Models, Molecular, Quantum Theory, Catalytic Domain, Coenzymes biosynthesis, Copper metabolism, Galactose Oxidase chemistry, Galactose Oxidase metabolism, Oxygen metabolism

Abstract

Galactose oxidase (GO) is a copper-dependent enzyme that accomplishes 2e - substrate oxidation by pairing a single copper with an unusual cysteinylated tyrosine (Cys-Tyr) redox cofactor. Previous studies have demonstrated that the post-translational biogenesis of Cys-Tyr is copper- and O 2 -dependent, resulting in a self-processing enzyme system. To investigate the mechanism of cofactor biogenesis in GO, the active-site structure of Cu(I)-loaded GO was determined using X-ray absorption near edge structure (XANES) and extended X-ray absorption fine structure (EXAFS) spectroscopy, and density-functional theory (DFT) calculations were performed on this model. Our results show that the active-site tyrosine lowers the Cu potential to enable the thermodynamically unfavorable 1e - reduction of O 2 , and the resulting Cu(II)-O 2 •- is activated toward H atom abstraction from cysteine. The final step of biogenesis is a concerted reaction involving coordinated Tyr ring deprotonation where Cu(II) coordination enables formation of the Cys-Tyr cross-link. These spectroscopic and computational results highlight the role of the Cu(I) in enabling O 2 activation by 1e - and the role of the resulting Cu(II) in enabling substrate activation for biogenesis.

Published

2016

36. Genetic dissection of chlorate respiration in Pseudomonas stutzeri PDA reveals syntrophic (per)chlorate reduction.

Author

Clark IC, Youngblut M, Jacobsen G, Wetmore KM, Deutschbauer A, Lucas L, and Coates JD

Subjects

Coenzymes biosynthesis, DNA Transposable Elements, Metalloproteins biosynthesis, Molybdenum Cofactors, Oxidation-Reduction, Pseudomonas stutzeri genetics, Pteridines, Rhodocyclaceae growth & development, Rhodocyclaceae metabolism, Chlorates metabolism, Oxidoreductases genetics, Perchlorates metabolism, Pseudomonas stutzeri growth & development, Pseudomonas stutzeri metabolism

Abstract

Genes important for growth of Pseudomonas stutzeri PDA on chlorate were identified using a randomly DNA bar-coded transposon mutant library. During chlorate reduction, mutations in genes encoding the chlorate reductase clrABC, predicted molybdopterin cofactor chaperon clrD, molybdopterin biosynthesis and two genes of unknown function (clrE, clrF) had fitness defects in pooled mutant assays (Bar-seq). Markerless in-frame deletions confirmed that clrA, clrB and clrC were essential for chlorate reduction, while clrD, clrE and clrF had less severe growth defects. Interestingly, the key detoxification gene cld was essential for chlorate reduction in isogenic pure culture experiments, but showed only minor fitness defects in Bar-seq experiments. We hypothesized this was enabled through chlorite dismutation by the community, as most strains in the Bar-seq library contained an intact cld. In support of this, Δcld grew with wild-type PDA or ΔclrA, and purified Cld also restored growth to the Δcld mutant. Expanding on this, wild-type PDA and a Δcld mutant of the perchlorate reducer Azospira suillum PS grew on perchlorate in co-culture, but not individually. These results demonstrate that co-occurrence of cld and a chloroxyanion reductase within a single organism is not necessary and raises the possibility of syntrophic (per)chlorate respiration in the environment., (© 2015 Society for Applied Microbiology and John Wiley & Sons Ltd.)

Published

2016

37. Molybdate uptake by Agrobacterium tumefaciens correlates with the cellular molybdenum cofactor status.

Author

Hoffmann MC, Ali K, Sonnenschein M, Robrahn L, Strauss D, Narberhaus F, and Masepohl B

Subjects

Agrobacterium tumefaciens genetics, Amino Acid Sequence, Base Sequence, Coenzymes biosynthesis, Coenzymes genetics, Escherichia coli genetics, Escherichia coli Proteins metabolism, Inverted Repeat Sequences, Metalloproteins biosynthesis, Metalloproteins genetics, Molybdenum Cofactors, Operon, Promoter Regions, Genetic, Transcription Factors metabolism, Agrobacterium tumefaciens metabolism, Coenzymes metabolism, Metalloproteins metabolism, Molybdenum metabolism, Pteridines metabolism

Abstract

Many enzymes require the molybdenum cofactor, Moco. Under Mo-limiting conditions, the high-affinity ABC transporter ModABC permits molybdate uptake and Moco biosynthesis in bacteria. Under Mo-replete conditions, Escherichia coli represses modABC transcription by the one-component regulator, ModE, consisting of a DNA-binding and a molybdate-sensing domain. Instead of a full-length ModE protein, many bacteria have a shorter ModE protein, ModE(S) , consisting of a DNA-binding domain only. Here, we asked how such proteins sense the intracellular molybdenum status. We show that the Agrobacterium tumefaciens ModE(S) protein Atu2564 is essential for modABC repression. ModE(S) binds two Mo-boxes in the modA promoter as shown by electrophoretic mobility shift assays. Northern analysis revealed cotranscription of modE(S) with the upstream gene, atu2565, which was dispensable for ModE(S) activity. To identify genes controlling ModE(S) function, we performed transposon mutagenesis. Tn5 insertions resulting in derepressed modA transcription mapped to the atu2565-modE(S) operon and several Moco biosynthesis genes. We conclude that A. tumefaciens ModE(S) activity responds to Moco availability rather than to molybdate concentration directly, as is the case for E. coli ModE. Similar results in Sinorhizobium meliloti suggest that Moco dependence is a common feature of ModE(S) regulators., (© 2016 John Wiley & Sons Ltd.)

Published

2016

38. Mouse model for molybdenum cofactor deficiency type B recapitulates the phenotype observed in molybdenum cofactor deficient patients.

Author

Jakubiczka-Smorag J, Santamaria-Araujo JA, Metz I, Kumar A, Hakroush S, Brueck W, Schwarz G, Burfeind P, Reiss J, and Smorag L

Subjects

Animals, Apoptosis genetics, Carbon-Carbon Lyases, Coenzymes biosynthesis, Cysteine analogs & derivatives, Cysteine urine, Disease Models, Animal, Gene Expression, Humans, Hypoxanthine blood, Hypoxanthine urine, Metal Metabolism, Inborn Errors blood, Metal Metabolism, Inborn Errors physiopathology, Metal Metabolism, Inborn Errors urine, Metalloproteins biosynthesis, Mice, Mice, Knockout, Molybdenum Cofactors, Mutation, Nuclear Proteins biosynthesis, Phenotype, Pteridines, Xanthine blood, Xanthine urine, Coenzymes genetics, Metal Metabolism, Inborn Errors genetics, Metalloproteins genetics, Nuclear Proteins genetics

Abstract

Molybdenum cofactor (MoCo) deficiency is a rare, autosomal-recessive disorder, mainly caused by mutations in MOCS1 (MoCo deficiency type A) or MOCS2 (MoCo deficiency type B) genes; the absence of active MoCo results in a deficiency in all MoCo-dependent enzymes. Patients with MoCo deficiency present with neonatal seizures, feeding difficulties, severe developmental delay, brain atrophy and early childhood death. Although substitution therapy with cyclic pyranopterin monophosphate (cPMP) has been successfully used in both Mocs1 knockout mice and in patients with MoCo deficiency type A, there is currently no Mocs2 knockout mouse and no curative therapy for patients with MoCo deficiency type B. Therefore, we generated and characterized a Mocs2-null mouse model of MoCo deficiency type B. Expression analyses of Mocs2 revealed a ubiquitous expression pattern; however, at the cellular level, specific cells show prominent Mocs2 expression, e.g., neuronal cells in cortex, hippocampus and brainstem. Phenotypic analyses demonstrated that Mocs2 knockout mice failed to thrive and died within 11 days after birth. None of the tested MoCo-dependent enzymes were active in Mocs2-deficient mice, leading to elevated concentrations of purines, such as hypoxanthine and xanthine, and non-detectable levels of uric acid in the serum and urine. Moreover, elevated concentrations of S-sulfocysteine were measured in the serum and urine. Increased levels of xanthine resulted in bladder and kidney stone formation, whereas increased concentrations of toxic sulfite triggered neuronal apoptosis. In conclusion, Mocs2-deficient mice recapitulate the severe phenotype observed in humans and can now serve as a model for preclinical therapeutic approaches for MoCo deficiency type B.

Published

2016

39. Structural Framework for Metal Incorporation during Molybdenum Cofactor Biosynthesis.

Author

Kasaragod VB and Schindelin H

Subjects

Adenosine Diphosphate metabolism, Adenosine Monophosphate metabolism, Binding Sites, Carrier Proteins genetics, Carrier Proteins metabolism, Coenzymes biosynthesis, Humans, Membrane Proteins genetics, Membrane Proteins metabolism, Metalloproteins biosynthesis, Molybdenum Cofactors, Mutation, Protein Binding, Carrier Proteins chemistry, Coenzymes chemistry, Membrane Proteins chemistry, Metalloproteins chemistry, Molybdenum metabolism, Pteridines chemistry

Abstract

The molybdenum cofactor (Moco) is essential for the catalytic activity of all molybdenum-containing enzymes with the exception of nitrogenase. Moco biosynthesis follows an evolutionarily highly conserved pathway and genetic deficiencies in the corresponding human enzymes result in Moco deficiency, which manifests itself in severe neurological symptoms and death in childhood. In humans the final steps of Moco biosynthesis are catalyzed by gephyrin, specifically the penultimate adenylation of molybdopterin (MPT) by its N-terminal G domain (GephG) and the final metal incorporation by its C-terminal E domain (GephE). To better understand the poorly defined molecular framework of this final step, we determined high-resolution crystal structures of GephE in the apo state and in complex with ADP, AMP, and molybdate. Our data provide novel insights into the catalytic steps leading to final Moco maturation, namely deadenylation as well as molybdate binding and insertion., (Copyright © 2016 Elsevier Ltd. All rights reserved.)

Published

2016

40. Construction and evaluation of a novel bifunctional phenylalanine-formate dehydrogenase fusion protein for bienzyme system with cofactor regeneration.

Author

Jiang W and Fang BS

Subjects

Amino Acid Oxidoreductases chemistry, Amino Acid Oxidoreductases genetics, Bacillus enzymology, Candida enzymology, Coenzymes metabolism, Enzyme Stability, Formate Dehydrogenases chemistry, Formate Dehydrogenases genetics, Formates metabolism, Hydrogen-Ion Concentration, Kinetics, Phenylalanine biosynthesis, Phenylalanine metabolism, Phenylpyruvic Acids metabolism, Recombinant Fusion Proteins genetics, Stereoisomerism, Temperature, Amino Acid Oxidoreductases metabolism, Coenzymes biosynthesis, Formate Dehydrogenases metabolism, Recombinant Fusion Proteins metabolism

Abstract

Phenylalanine dehydrogenase (PheDH) plays an important role in enzymatic synthesis of L-phenylalanine for aspartame (sweetener) and detection of phenylketonuria (PKU), suggesting that it is important to obtain a PheDH with excellent characteristics. Gene fusion of PheDH and formate dehydrogenase (FDH) was constructed to form bifunctional multi-enzymes for bioconversion of L-phenylalanine coupled with coenzyme regeneration. Comparing with the PheDH monomer from Microbacterium sp., the bifunctional PheDH-FDH showed noteworthy stability under weakly acidic and alkaline conditions (pH 6.5-9.0). The bifunctional enzyme can produce 153.9 mM L-phenylalanine with remarkable performance of enantiomers choice by enzymatic conversion with high molecular conversion rate (99.87 %) in catalyzing phenylpyruvic acid to L-phenylalanine being 1.50-fold higher than that of the separate expression system. The results indicated the potential application of the PheDH and PheDH-FDH with coenzyme regeneration for phenylpyruvic acid analysis and L-phenylalanine biosynthesis in medical diagnosis and pharmaceutical field.

Published

2016

41. The molybdenum cofactor biosynthesis complex interacts with actin filaments via molybdenum insertase Cnx1 as anchor protein in Arabidopsis thaliana.

Author

Kaufholdt D, Baillie CK, Bikker R, Burkart V, Dudek CA, von Pein L, Rothkegel M, Mendel RR, and Hänsch R

Subjects

Coenzymes metabolism, Genetic Vectors, Metalloproteins metabolism, Molybdenum Cofactors, Pteridines metabolism, Actin Cytoskeleton metabolism, Arabidopsis metabolism, Arabidopsis Proteins metabolism, Calnexin metabolism, Coenzymes biosynthesis, Metalloproteins biosynthesis

Abstract

The pterin based molybdenum cofactor (Moco) plays an essential role in almost all organisms. Its biosynthesis is catalysed by six enzymes in a conserved four step reaction pathway. The last three steps are located in the cytoplasm, where a multimeric protein complex is formed to protect the intermediates from degradation. Bimolecular fluorescence complementation was used to test for cytoskeleton association of the Moco biosynthesis enzymes with actin filaments and microtubules using known cytoskeleton associated proteins, thus permitting non-invasive in vivo studies. Coding sequences of binding proteins were cloned via the GATEWAY system. No Moco biosynthesis enzyme showed any interaction with microtubules. However, alone the two domain protein Cnx1 exhibited interaction with actin filaments mediated by both domains with the Cnx1G domain displaying a stronger interaction. Cnx6 showed actin association only if unlabelled Cnx1 was co-expressed in comparable amounts. So Cnx1 is likely to be the anchor protein for the whole biosynthesis complex on actin filaments. A stabilization of the whole Moco biosynthesis complex on the cytoskeleton might be crucial. In addition a micro-compartmentation might either allow a localisation near the mitochondrial ATM3 exporter providing the first Moco intermediate or near one of the three molybdate transporters enabling efficient molybdate incorporation., (Copyright © 2016 Elsevier Ireland Ltd. All rights reserved.)

Published

2016

42. Moco biosynthesis and the ATAC acetyltransferase engage translation initiation by inhibiting latent PKR activity.

Author

Suganuma T, Swanson SK, Florens L, Washburn MP, and Workman JL

Subjects

Animals, Cell Line, Eukaryotic Initiation Factor-2 metabolism, Guanine Nucleotide Exchange Factors metabolism, Humans, JNK Mitogen-Activated Protein Kinases metabolism, Molybdenum Cofactors, Phosphorylation, Protein Biosynthesis, Pteridines, Sulfurtransferases metabolism, Acetyltransferases metabolism, Coenzymes biosynthesis, Metalloproteins biosynthesis, eIF-2 Kinase metabolism

Abstract

Molybdenum cofactor (Moco) biosynthesis is linked to c-Jun N-terminal kinase (JNK) signaling in Drosophila through MoaE, a molybdopterin (MPT) synthase subunit that is also a component of the Ada Two A containing (ATAC) acetyltransferase complex. Here, we show that human MPT synthase and ATAC inhibited PKR, a double-stranded RNA-dependent protein kinase, to facilitate translation initiation of iron-responsive mRNA. MPT synthase and ATAC directly interacted with PKR and suppressed latent autophosphorylation of PKR and its downstream phosphorylation of JNK and eukaryotic initiation factor 2α (eIF2α). The suppression of eIF2α phosphorylation via MPT synthase and ATAC prevented sequestration of the guanine nucleotide exchange factor eIF2B, which recycles eIF2-GDP to eIF2-GTP, resulting in the promotion of translation initiation. Indeed, translation of the iron storage protein, ferritin, was reduced in the absence of MPT synthase or ATAC subunits. Thus, MPT synthase and ATAC regulate latent PKR signaling and link transcription and translation initiation., (© The Author (2015). Published by Oxford University Press on behalf of Journal of Molecular Cell Biology, IBCB, SIBS, CAS. All rights reserved.)

Published

2016

43. Bacterial molybdoenzymes: old enzymes for new purposes.

Author

Leimkühler S and Iobbi-Nivol C

Subjects

Coenzymes metabolism, Environmental Microbiology, Metalloproteins metabolism, Molybdenum Cofactors, Pteridines metabolism, Apoenzymes metabolism, Bacteria enzymology, Bacterial Proteins metabolism, Coenzymes biosynthesis, Metalloproteins biosynthesis, Molecular Chaperones metabolism

Abstract

Molybdoenzymes are widespread in eukaryotic and prokaryotic organisms where they play crucial functions in detoxification reactions in the metabolism of humans and bacteria, in nitrate assimilation in plants and in anaerobic respiration in bacteria. To be fully active, these enzymes require complex molybdenum-containing cofactors, which are inserted into the apoenzymes after folding. For almost all the bacterial molybdoenzymes, molybdenum cofactor insertion requires the involvement of specific chaperones. In this review, an overview on the molybdenum cofactor biosynthetic pathway is given together with the role of specific chaperones dedicated for molybdenum cofactor insertion and maturation. Many bacteria are involved in geochemical cycles on earth and therefore have an environmental impact. The roles of molybdoenzymes in bioremediation and for environmental applications are presented., (© FEMS 2015. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com.)

Published

2016

44. Mechanistic Investigation of cPMP Synthase in Molybdenum Cofactor Biosynthesis Using an Uncleavable Substrate Analogue.

Author

Hover BM, Lilla EA, and Yokoyama K

Subjects

Coenzymes biosynthesis, Escherichia coli Proteins metabolism, Hydrolases chemistry, Hydrolases metabolism, Mass Spectrometry, Metalloproteins biosynthesis, Molybdenum Cofactors, Organophosphorus Compounds metabolism, Pterins metabolism, Staphylococcus aureus enzymology, Coenzymes chemistry, Escherichia coli enzymology, Escherichia coli Proteins chemistry, Metalloproteins chemistry, Organophosphorus Compounds chemistry, Pteridines chemistry, Pterins chemistry

Abstract

Molybdenum cofactor (Moco) is essential for all kingdoms of life, plays central roles in various biological processes, and must be biosynthesized de novo. During its biosynthesis, the characteristic pyranopterin ring is constructed by a complex rearrangement of guanosine 5'-triphosphate (GTP) into cyclic pyranopterin monophosphate (cPMP) through the action of two enzymes, MoaA and MoaC. Recent studies revealed that MoaC catalyzes the majority of the transformation and produces cPMP from a unique cyclic nucleotide, 3',8-cyclo-7,8-dihydro-GTP (3',8-cH2GTP). However, the mechanism by which MoaC catalyzes this complex rearrangement is largely unexplored. Here, we report the mechanistic characterization of MoaC using an uncleavable substrate analogue, 3',8-cH2GMP[CH2]PP, as a probe to investigate the timing of cyclic phosphate formation. Using partially active MoaC variants, 3',8-cH2GMP[CH2]PP was found to be accepted by MoaC as a substrate and was converted to an analogue of the previously described MoaC reaction intermediate, suggesting that the early stage of catalysis proceeds without cyclic phosphate formation. In contrast, when it was incubated with wt-MoaC, 3',8-cH2GMP[CH2]PP caused mechanism-based inhibition. Detailed characterization of the inhibited MoaC suggested that 3',8-cH2GMP[CH2]PP is mainly converted to a molecule (compound Y) with an acid-labile triaminopyrimidinone base without an established pyranopterin structure. MS analysis of MoaC treated with 3',8-cH2GMP[CH2]PP provided strong evidence that compound Y forms a tight complex with MoaC likely through a covalent linkage. These observations are consistent with a mechanism in which cyclic phosphate ring formation proceeds in concert with the pterin ring formation. This mechanism would provide a thermodynamic driving force to complete the formation of the unique tetracyclic structure of cPMP.

Published

2015

45. Molybdopterin biosynthesis-Mechanistic studies on a novel MoaA catalyzed insertion of a purine carbon into the ribose of GTP.

Author

Mehta AP, Abdelwahed SH, and Begley TP

Subjects

Carbon, Humans, Molybdenum Cofactors, Pteridines, Biocatalysis, Coenzymes biosynthesis, Escherichia coli Proteins physiology, Guanosine Triphosphate chemistry, Isomerases physiology, Metalloproteins biosynthesis, Purines chemistry, Ribose chemistry

Abstract

The first step in the biosynthesis of the molybdopterin cofactor involves an unprecedented insertion of the purine C8 carbon between the C2' and C3' carbons of the ribose moiety of GTP. Here we review mechanistic studies on this remarkable transformation. This article is part of a Special Issue entitled: Cofactor-dependent proteins: evolution, chemical diversity and bio-applications., (Copyright © 2015 Elsevier B.V. All rights reserved.)

Published

2015

46. The role of FeS clusters for molybdenum cofactor biosynthesis and molybdoenzymes in bacteria.

Author

Yokoyama K and Leimkühler S

Subjects

Bacteria metabolism, Bacterial Proteins chemistry, Coenzymes chemistry, Iron-Sulfur Proteins chemistry, Metalloproteins chemistry, Models, Biological, Models, Chemical, Molecular Structure, Molybdenum chemistry, Molybdenum Cofactors, Oxidoreductases chemistry, Pteridines chemistry, Bacterial Proteins metabolism, Coenzymes biosynthesis, Iron-Sulfur Proteins metabolism, Metalloproteins biosynthesis, Molybdenum metabolism, Oxidoreductases metabolism

Abstract

The biosynthesis of the molybdenum cofactor (Moco) has been intensively studied, in addition to its insertion into molybdoenzymes. In particular, a link between the assembly of molybdoenzymes and the biosynthesis of FeS clusters has been identified in the recent years: 1) the synthesis of the first intermediate in Moco biosynthesis requires an FeS-cluster containing protein, 2) the sulfurtransferase for the dithiolene group in Moco is also involved in the synthesis of FeS clusters, thiamin and thiolated tRNAs, 3) the addition of a sulfido-ligand to the molybdenum atom in the active site additionally involves a sulfurtransferase, and 4) most molybdoenzymes in bacteria require FeS clusters as redox active cofactors. In this review we will focus on the biosynthesis of the molybdenum cofactor in bacteria, its modification and insertion into molybdoenzymes, with an emphasis to its link to FeS cluster biosynthesis and sulfur transfer., (Copyright © 2014 Elsevier B.V. All rights reserved.)

Published

2015

47. Shared-intermediates in the biosynthesis of thio-cofactors: Mechanism and functions of cysteine desulfurases and sulfur acceptors.

Author

Black KA and Dos Santos PC

Subjects

Bacterial Proteins biosynthesis, Bacterial Proteins chemistry, Bacterial Proteins metabolism, Biosynthetic Pathways, Carbon-Sulfur Lyases chemistry, Coenzymes biosynthesis, Iron-Sulfur Proteins biosynthesis, Metalloproteins biosynthesis, Models, Molecular, Molybdenum Cofactors, Protein Structure, Tertiary, Pteridines, Carbon-Sulfur Lyases metabolism, Cysteine metabolism, Pyridoxal Phosphate metabolism, Sulfur metabolism

Abstract

Cysteine desulfurases utilize a PLP-dependent mechanism to catalyze the first step of sulfur mobilization in the biosynthesis of sulfur-containing cofactors. Sulfur activation and integration into thiocofactors involve complex mechanisms and intricate biosynthetic schemes. Cysteine desulfurases catalyze sulfur-transfer reactions from l-cysteine to sulfur acceptor molecules participating in the biosynthesis of thio-cofactors, including Fe-S clusters, thionucleosides, thiamin, biotin, and molybdenum cofactor. The proposed mechanism of cysteine desulfurases involves the PLP-dependent cleavage of the C-S bond from l-cysteine via the formation of a persulfide enzyme intermediate, which is considered the hallmark step in sulfur mobilization. The subsequent sulfur transfer reaction varies with the class of cysteine desulfurase and sulfur acceptor. IscS serves as a mecca for sulfur incorporation into a network of intertwined pathways for the biosynthesis of thio-cofactors. The involvement of a single enzyme interacting with multiple acceptors, the recruitment of shared-intermediates partaking roles in multiple pathways, and the participation of Fe-S enzymes denote the interconnectivity of pathways involving sulfur trafficking. In Bacillus subtilis, the occurrence of multiple cysteine desulfurases partnering with dedicated sulfur acceptors partially deconvolutes the routes of sulfur trafficking and assigns specific roles for these enzymes. Understanding the roles of promiscuous vs. dedicated cysteine desulfurases and their partnership with shared-intermediates in the biosynthesis of thio-cofactors will help to map sulfur transfer events across interconnected pathways and to provide insight into the hierarchy of sulfur incorporation into biomolecules. This article is part of a Special Issue entitled: Fe/S proteins: Analysis, structure, function, biogenesis and diseases., (Copyright © 2014 Elsevier B.V. All rights reserved.)

Published

2015

48. Mechanism of pyranopterin ring formation in molybdenum cofactor biosynthesis.

Author

Hover BM, Tonthat NK, Schumacher MA, and Yokoyama K

Subjects

Carbon Isotopes, Escherichia coli Proteins chemistry, Escherichia coli Proteins genetics, Escherichia coli Proteins isolation & purification, Hydrolases chemistry, Hydrolases isolation & purification, Magnetic Resonance Spectroscopy, Molecular Structure, Molybdenum Cofactors, Mutagenesis, Site-Directed, Protein Conformation, Pteridines, Coenzymes biosynthesis, Escherichia coli Proteins metabolism, Hydrolases metabolism, Metalloproteins biosynthesis, Models, Molecular, Pterins chemistry

Abstract

The molybdenum cofactor (Moco) is essential for all kingdoms of life, plays central roles in various biological processes, and must be biosynthesized de novo. During Moco biosynthesis, the characteristic pyranopterin ring is constructed by a complex rearrangement of guanosine 5'-triphosphate (GTP) into cyclic pyranopterin (cPMP) through the action of two enzymes, MoaA and MoaC (molybdenum cofactor biosynthesis protein A and C, respectively). Conventionally, MoaA was considered to catalyze the majority of this transformation, with MoaC playing little or no role in the pyranopterin formation. Recently, this view was challenged by the isolation of 3',8-cyclo-7,8-dihydro-guanosine 5'-triphosphate (3',8-cH2GTP) as the product of in vitro MoaA reactions. To elucidate the mechanism of formation of Moco pyranopterin backbone, we performed biochemical characterization of 3',8-cH2GTP and functional and X-ray crystallographic characterizations of MoaC. These studies revealed that 3',8-cH2GTP is the only product of MoaA that can be converted to cPMP by MoaC. Our structural studies captured the specific binding of 3',8-cH2GTP in the active site of MoaC. These observations provided strong evidence that the physiological function of MoaA is the conversion of GTP to 3',8-cH2GTP (GTP 3',8-cyclase), and that of MoaC is to catalyze the rearrangement of 3',8-cH2GTP into cPMP (cPMP synthase). Furthermore, our structure-guided studies suggest that MoaC catalysis involves the dynamic motions of enzyme active-site loops as a way to control the timing of interaction between the reaction intermediates and catalytically essential amino acid residues. Thus, these results reveal the previously unidentified mechanism behind Moco biosynthesis and provide mechanistic and structural insights into how enzymes catalyze complex rearrangement reactions.

Published

2015

49. Protein-pyridinol thioester precursor for biosynthesis of the organometallic acyl-iron ligand in [Fe]-hydrogenase cofactor.

Author

Fujishiro T, Kahnt J, Ermler U, and Shima S

Subjects

Acid Anhydride Hydrolases metabolism, Bacterial Proteins metabolism, Catalysis, Crystallography, X-Ray, Esters metabolism, Methanobacteriaceae, Methanocaldococcus, Molecular Docking Simulation, Nucleotidyltransferases metabolism, Acid Anhydride Hydrolases genetics, Adenosine Monophosphate metabolism, Bacterial Proteins genetics, Coenzymes biosynthesis, Hydrogenase, Iron-Sulfur Proteins, Nucleotidyltransferases genetics, Organometallic Compounds, Pyridines metabolism, Sulfur Compounds metabolism

Abstract

The iron-guanylylpyridinol (FeGP) cofactor of [Fe]-hydrogenase contains a prominent iron centre with an acyl-Fe bond and is the only acyl-organometallic iron compound found in nature. Here, we identify the functions of HcgE and HcgF, involved in the biosynthesis of the FeGP cofactor using structure-to-function strategy. Analysis of the HcgE and HcgF crystal structures with and without bound substrates suggest that HcgE catalyses the adenylylation of the carboxy group of guanylylpyridinol (GP) to afford AMP-GP, and subsequently HcgF catalyses the transesterification of AMP-GP to afford a Cys (HcgF)-S-GP thioester. Both enzymatic reactions are confirmed by in vitro assays. The structural data also offer plausible catalytic mechanisms. This strategy of thioester activation corresponds to that used for ubiquitin activation, a key event in the regulation of multiple cellular processes. It further implicates a nucleophilic attack onto the acyl carbon presumably via an electron-rich Fe(0)- or Fe(I)-carbonyl complex in the Fe-acyl formation.

Published

2015

50. Overexpression of a GmCnx1 gene enhanced activity of nitrate reductase and aldehyde oxidase, and boosted mosaic virus resistance in soybean.

Author

Zhou Z, He H, Ma L, Yu X, Mi Q, Pang J, Tang G, and Liu B

Subjects

Agrobacterium tumefaciens, Coenzymes biosynthesis, Conserved Sequence, DNA, Complementary genetics, DNA, Plant genetics, Disease Resistance, Genetic Vectors, Metalloproteins biosynthesis, Molecular Sequence Data, Molybdenum Cofactors, Phylogeny, Plant Diseases virology, Plant Leaves metabolism, Plant Leaves virology, Plant Proteins genetics, Plant Roots metabolism, Plants, Genetically Modified, Protein Structure, Tertiary, Pteridines, Recombinant Fusion Proteins metabolism, Sequence Alignment, Sequence Homology, Amino Acid, Soybean Proteins genetics, Glycine max genetics, Glycine max virology, Up-Regulation, Xanthine Dehydrogenase genetics, Aldehyde Oxidase metabolism, Mosaic Viruses physiology, Nitrate Reductase metabolism, Plant Diseases genetics, Plant Proteins physiology, Soybean Proteins physiology, Glycine max metabolism, Xanthine Dehydrogenase physiology

Abstract

Molybdenum cofactor (Moco) is required for the activities of Moco-dependant enzymes. Cofactor for nitrate reductase and xanthine dehydrogenase (Cnx1) is known to be involved in the biosynthesis of Moco in plants. In this work, a soybean (Glycine max L.) Cnx1 gene (GmCnx1) was transferred into soybean using Agrobacterium tumefaciens-mediated transformation method. Twenty seven positive transgenic soybean plants were identified by coating leaves with phosphinothricin, bar protein quick dip stick and PCR analysis. Moreover, Southern blot analysis was carried out to confirm the insertion of GmCnx1 gene. Furthermore, expression of GmCnx1 gene in leaf and root of all transgenic lines increased 1.04-2.12 and 1.55-3.89 folds, respectively, as compared to wild type with GmCnx1 gene and in line 10 , 22 showing the highest expression. The activities of Moco-related enzymes viz nitrate reductase (NR) and aldehydeoxidase (AO) of T1 generation plants revealed that the best line among the GmCnx1 transgenic plants accumulated 4.25 μg g(-1) h(-1) and 30 pmol L(-1), respectively (approximately 2.6-fold and 3.9-fold higher than non-transgenic control plants).In addition, overexpression ofGmCnx1boosted the resistance to various strains of soybean mosaic virus (SMV). DAS-ELISA analysis further revealed that infection rate of GmCnx1 transgenic plants were generally lower than those of non-transgenic plants among two different virus strains tested. Taken together, this study showed that overexpression of a GmCnx1 gene enhanced NR and AO activities and SMV resistance, suggesting its important role in soybean genetic improvement.

Published

2015