Your search keyword '"Bradley S. Evans"' showing total 62 results

1. SIMPEL: using stable isotopes to elucidate dynamics of context specific metabolism

Author

Shrikaar Kambhampati, Allen H. Hubbard, Somnath Koley, Javier D. Gomez, Frédéric Marsolais, Bradley S. Evans, Jamey D. Young, and Doug K. Allen

Subjects

Biology (General), QH301-705.5

Abstract

Abstract The capacity to leverage high resolution mass spectrometry (HRMS) with transient isotope labeling experiments is an untapped opportunity to derive insights on context-specific metabolism, that is difficult to assess quantitatively. Tools are needed to comprehensively mine isotopologue information in an automated, high-throughput way without errors. We describe a tool, Stable Isotope-assisted Metabolomics for Pathway Elucidation (SIMPEL), to simplify analysis and interpretation of isotope-enriched HRMS datasets. The efficacy of SIMPEL is demonstrated through examples of central carbon and lipid metabolism. In the first description, a dual-isotope labeling experiment is paired with SIMPEL and isotopically nonstationary metabolic flux analysis (INST-MFA) to resolve fluxes in central metabolism that would be otherwise challenging to quantify. In the second example, SIMPEL was paired with HRMS-based lipidomics data to describe lipid metabolism based on a single labeling experiment. Available as an R package, SIMPEL extends metabolomics analyses to include isotopologue signatures necessary to quantify metabolic flux.

Published

2024

2. Commercial implementation of genomic selection in Tasmanian Atlantic salmon: Scheme evolution and validation

Author

Klara L. Verbyla, Peter D. Kube, and Bradley S. Evans

Subjects

Atlantic salmon, breeding, commercial implementation, genomic prediction, Evolution, QH359-425

Abstract

Abstract Genomic information was included for the first time in the prediction of breeding values for Atlantic salmon within the Australian Salmon Enterprises of Tasmania Pty Ltd selective breeding program in 2016. The process to realize genomic selection in the breeding program begun in 2014 with the scheme finalized and fully implemented for the first time in 2018. The high potential of within family selection to accelerate genetic gain, something not possible using the traditional pedigree‐based approach, provided the impetus for implementation. Efficient and effective genotyping platforms are essential for genomic selection. Genotype data from high density arrays revealed extensive persistence of linkage disequilibrium in the Tasmania Atlantic salmon population, resulting in high accuracies of both imputation and genomic breeding values when using imputed data. Consequently, a low‐density novel genotype‐by‐sequence assay was designed and incorporated into the scheme. Through the use of a static high‐ and dynamic low‐density genotyping platforms, an optimized genotyping scheme was devised and implemented such that all individuals in every year class are genotyped efficiently while maximizing the genetic gains and minimizing costs. The increase in the rates of genetic gain attributed to the implementation of genomic selection is significant across both the breeding programs primary and secondary traits. Substantial improvement in the ability to select parents prior to progeny testing is observed across multiple years. The resultant economic impacts for the industry are considerable based on the increases in genetic gain for traits achieved within the breeding program and the use of genomic selection for commercial production.

Published

2022

3. Accurate and efficient amino acid analysis for protein quantification using hydrophilic interaction chromatography coupled tandem mass spectrometry

Author

Shrikaar Kambhampati, Jia Li, Bradley S. Evans, and Doug K. Allen

Subjects

HILIC, Chromatography, Isobaric compounds, Amino acids, Protein hydrolysis, Protein quantification, Plant culture, SB1-1110, Biology (General), QH301-705.5

Abstract

Abstract Background Methods used to quantify protein from biological samples are often inaccurate with significant variability that requires care to minimize. The errors result from losses during protein preparation and purification and false detection of interfering compounds or elements. Amino acid analysis (AAA) involves a series of chromatographic techniques that can be used to measure protein levels, avoiding some difficulties and providing specific compositional information. However, unstable derivatives, that are toxic and can be costly, incomplete reactions, inadequate chromatographic separations, and the lack of a single hydrolysis method with sufficient recovery of all amino acids hinder precise protein quantitation using AAA. Results In this study, a hydrophilic interaction chromatography based method was used to separate all proteinogenic amino acids, including isobaric compounds leucine and isoleucine, prior to detection by multiple reaction monitoring with LC–MS/MS. Through inclusion of commercially available isotopically labeled (13C, 15N) amino acids as internal standards we adapted an isotopic dilution strategy for amino acid-based quantification of proteins. Three hydrolysis methods were tested with ubiquitin, bovine serum albumin, (BSA), and a soy protein biological reference material (SRM 3234; NIST) resulting in protein estimates that were 86–103%, 82–94%, and 90–99% accurate for the three protein samples respectively. The methane sulfonic acid hydrolysis approach provided the best recovery of labile amino acids including: cysteine, methionine and tryptophan that are challenging to accurately quantify. Conclusions Accurate determination of protein quantity and amino acid composition in heterogeneous biological samples is non-trivial. Recent advances in chromatographic phases and LC–MS/MS based methods, along with the availability of isotopic standards can minimize difficulties in analysis and improve protein quantitation. A robust method is described for high-throughput protein quantification and amino acid compositional analysis. Since accurate measurement of protein quality and quantity are a requirement for many biological studies that relate to crop improvement or more generally, our understanding of metabolism in living systems, we envision this method will have broad applicability.

Published

2019

4. Program for Integration and Rapid Analysis of Mass Isotopomer Distributions (PIRAMID).

Author

Javier D. Gomez, Martha L. Wall, Mohsin Rahim, Shrikaar Kambhampati, Bradley S. Evans, Doug K. Allen, Maciek R. Antoniewicz, and Jamey D. Young

Published

2023

5. Pan-cancer analysis identifies tumor-specific antigens derived from transposable elements

Author

Nakul M. Shah, H. Josh Jang, Yonghao Liang, Ju Heon Maeng, Shin-Cheng Tzeng, Angela Wu, Noah L. Basri, Xuan Qu, Changxu Fan, Amy Li, Benjamin Katz, Daofeng Li, Xiaoyun Xing, Bradley S. Evans, and Ting Wang

Subjects

Genetics

Published

2023

6. COLD REGULATED GENE 27 and 28 antagonize the transcriptional activity of the RVE8/LNK1/LNK2 circadian complex

Author

Maria L Sorkin, Shin-Cheng Tzeng, Stefanie King, Andrés Romanowski, Nikolai Kahle, Rebecca Bindbeutel, Andreas Hiltbrunner, Marcelo J Yanovsky, Bradley S Evans, Dmitri A Nusinow, Sub Plant-Environment Signaling, and Plant-Environment Signaling

Subjects

Cor27, Light, Clock, Physiology, Arabidopsis, Genetics, Proteins, Expression, Recruitment, Plant Science, Rhythms, Statistical-model, Time

Abstract

Many molecular and physiological processes in plants occur at a specific time of day. These daily rhythms are coordinated in part by the circadian clock, a timekeeper that uses daylength and temperature to maintain rhythms of ∼24 h in various clock-regulated phenotypes. The circadian MYB-like transcription factor REVEILLE 8 (RVE8) interacts with its transcriptional coactivators NIGHT LIGHT-INDUCIBLE AND CLOCK-REGULATED 1 (LNK1) and LNK2 to promote the expression of evening-phased clock genes and cold tolerance factors. While genetic approaches have commonly been used to discover connections within the clock and between clock elements and other pathways, here, we used affinity purification coupled with mass spectrometry (APMS) to identify time-of-day–specific protein interactors of the RVE8-LNK1/LNK2 complex in Arabidopsis (Arabidopsis thaliana). Among the interactors of RVE8/LNK1/LNK2 were COLD-REGULATED GENE 27 (COR27) and COR28, which coprecipitated in an evening-specific manner. In addition to COR27 and COR28, we found an enrichment of temperature-related interactors that led us to establish a previously uncharacterized role for LNK1 and LNK2 in temperature entrainment of the clock. We established that RVE8, LNK1, and either COR27 or COR28 form a tripartite complex in yeast (Saccharomyces cerevisiae) and that the effect of this interaction in planta serves to antagonize transcriptional activation of RVE8 target genes, potentially through mediating RVE8 protein degradation in the evening. Together, these results illustrate how a proteomic approach can be used to identify time-of-day–specific protein interactions. Discovery of the RVE8-LNK-COR protein complex indicates a previously unknown regulatory mechanism for circadian and temperature signaling pathways.

Published

2023

7. The unknown lipids project: harmonized methods improve compound identification and data reproducibility in an inter-laboratory untargeted lipidomics study

Author

Tong Shen, Ciara Conway, Kaitlin R. Rempfert, Jennifer E. Kyle, Sean M. Colby, David A. Gaul, Hani Habra, Fanzhou Kong, Kent J. Bloodsworth, Douglas Allen, Bradley S. Evans, Xiuxia Du, Facundo M. Fernandez, Thomas O. Metz, Oliver Fiehn, and Charles R. Evans

Subjects

Article

Abstract

Untargeted lipidomics allows analysis of a broader range of lipids than targeted methods and permits discovery of unknown compounds. Previous ring trials have evaluated the reproducibility of targeted lipidomics methods, but inter-laboratory comparison of compound identification and unknown feature detection in untargeted lipidomics has not been attempted. To address this gap, five laboratories analyzed a set of mammalian tissue and biofluid reference samples using both their own untargeted lipidomics procedures and a common chromatographic and data analysis method. While both methods yielded informative data, the common method improved chromatographic reproducibility and resulted in detection of more shared features between labs. Spectral search against the LipidBlast in silico library enabled identification of over 2,000 unique lipids. Further examination of LC-MS/MS and ion mobility data, aided by hybrid search and spectral networking analysis, revealed spectral and chromatographic patterns useful for classification of unknown features, a subset of which were highly reproducible between labs. Overall, our method offers enhanced compound identification performance compared to targeted lipidomics, demonstrates the potential of harmonized methods to improve inter-site reproducibility for quantitation and feature alignment, and can serve as a reference to aid future annotation of untargeted lipidomics data.

Published

2023

8. An Improved Top-Down Mass Spectrometry Characterization of Chlamydomonas reinhardtii Histones and Their Post-translational Modifications

Author

James J. Pesavento, James G. Umen, Henna Shaghasi, Mowei Zhou, Bradley S. Evans, Sarah R Rommelfanger, Shin-Cheng Tzeng, and Ljiljana Paša-Tolić

Subjects

animal structures, biology, Chemistry, 010401 analytical chemistry, Chlamydomonas reinhardtii, 010402 general chemistry, biology.organism_classification, Mass spectrometry, 01 natural sciences, 0104 chemical sciences, Histone H4, Histone, Histone H1, Biochemistry, Structural Biology, Acetylation, biology.protein, Fragmentation (cell biology), Linker, Spectroscopy

Abstract

We present an updated analysis of the linker and core histone proteins and their proteoforms in the green microalga Chlamydomonas reinhardtii by top-down mass spectrometry (TDMS). The combination of high-resolution liquid chromatographic separation, robust fragmentation, high mass spectral resolution, the application of a custom search algorithm, and extensive manual analysis enabled the characterization of 86 proteoforms across all four core histones H2A, H2B, H3, and H4 and the linker histone H1. All canonical H2A paralogs, which vary in their C-termini, were identified, along with the previously unreported noncanonical variant H2A.Z that had high levels of acetylation and C-terminal truncations. Similarly, a majority of the canonical H2B paralogs were identified, along with a smaller noncanonical variant, H2B.v1, that was highly acetylated. Histone H4 exhibited a novel acetylation profile that differs significantly from that found in other organisms. A majority of H3 was monomethylated at K4 with low levels of co-occuring acetylation, while a small fraction of H3 was trimethylated at K4 with high levels of co-occuring acetylation.

Published

2021

9. COR27/28 Regulate the Evening Transcriptional Activity of the RVE8-LNK1/2 Circadian Complex

Author

Maria L. Sorkin, Shin-Cheng Tzeng, Andrés Romanowski, Nikolai Kahle, Rebecca Bindbeutel, Andreas Hiltbrunner, Marcelo J. Yanovsky, Bradley S. Evans, and Dmitri A. Nusinow

Abstract

The timing of many molecular and physiological processes in plants occurs at a specific time of day. These daily rhythms are driven by the circadian clock, a master timekeeper that uses daylength and temperature to maintain rhythms of approximately 24 hours in various clock-regulated phenotypes. The circadian MYB-like transcription factor REVEILLE 8 (RVE8) interacts with its transcriptional coactivators NIGHT LIGHT INDUCIBLE AND CLOCK REGULATED 1 (LNK1) and LNK2 to promote the expression of evening-phased clock genes and cold tolerance factors. While genetic approaches have commonly been used to discover new connections within the clock and between other pathways, here we use affinity purification coupled with mass spectrometry to discover time-of-day-specific protein interactors of the RVE8-LNK1/2 complex. Among the interactors of RVE8/LNK1/LNK2 were COLD REGULATED GENE 27 (COR27) and COR28, which were coprecipitated in an evening-specific manner. In addition to COR27/28, we found an enrichment of temperature-related interactors that led us to establish a novel role for LNK1/2 in temperature entrainment of the clock. We established that RVE8, LNK1, and either COR27 or COR28 form a tripartite complex in yeast and that the effect of this interaction in planta serves to antagonize transcriptional activation of RVE8 target genes through mediating RVE8 protein degradation in the evening. Together, these results illustrate how a proteomic approach identified time-of-day-specific protein interactions and a novel RVE8-LNK-COR protein complex that implicates a new regulatory mechanism for circadian and temperature signaling pathways.

Published

2022

10. N1-methylpseudouridine found within COVID-19 mRNA vaccines produces faithful protein products

Author

Kyusik Q. Kim, Bhagyashri D. Burgute, Shin-Cheng Tzeng, Crystal Jing, Courtney Jungers, Junya Zhang, Liewei L. Yan, Richard D. Vierstra, Sergej Djuranovic, Bradley S. Evans, and Hani S. Zaher

Subjects

Vaccines, Synthetic, COVID-19 Vaccines, Nucleotides, COVID-19, Humans, Proteins, RNA, RNA, Messenger, mRNA Vaccines, General Biochemistry, Genetics and Molecular Biology, Pseudouridine

Abstract

Synthetic mRNA technology is a promising avenue for treating and preventing disease. Key to the technology is the incorporation of modified nucleotides such as N1-methylpseudouridine (m1Ψ) to decrease immunogenicity of the RNA. However, relatively few studies have addressed the effects of modified nucleotides on the decoding process. Here, we investigate the effect of m1Ψ and the related modification pseudouridine (Ψ) on translation. In a reconstituted system, we find that m1Ψ does not significantly alter decoding accuracy. More importantly, we do not detect an increase in miscoded peptides when mRNA containing m1Ψ is translated in cell culture, compared with unmodified mRNA. We also find that m1Ψ does not stabilize mismatched RNA-duplex formation and only marginally promotes errors during reverse transcription. Overall, our results suggest that m1Ψ does not significantly impact translational fidelity, a welcome sign for future RNA therapeutics.

Published

2021

11. A bifunctional salvage pathway for two distinct S‐adenosylmethionine by‐products that is widespread in bacteria, including pathogenicEscherichia coli

Author

Justin A. North, John A. Wildenthal, Tobias J. Erb, Fred Robert Tabita, Bradley S. Evans, John A. Gerlt, and Kathryn M. Byerly

Subjects

S-Adenosylmethionine, Phosphorylases, Rhodospirillum rubrum, medicine.disease_cause, Microbiology, Article, 03 medical and health sciences, chemistry.chemical_compound, Methionine, Bacterial Proteins, Fructose-Bisphosphate Aldolase, Escherichia coli, medicine, Isomerases, N-Glycosyl Hydrolases, Molecular Biology, Nucleotide salvage, 030304 developmental biology, Dihydroxyacetone phosphate, 0303 health sciences, Extraintestinal Pathogenic Escherichia coli, Thionucleosides, Deoxyadenosines, biology, 030306 microbiology, Phosphotransferases, Aldolase A, biology.organism_classification, Carbon, Oxygen, chemistry, Biochemistry, Dihydroxyacetone Phosphate, biology.protein, bacteria, Radical SAM, Metabolic Networks and Pathways, Bacteria

Abstract

S-adenosyl-l-methionine (SAM) is a necessary cosubstrate for numerous essential enzymatic reactions including protein and nucleotide methylations, secondary metabolite synthesis and radical-mediated processes. Radical SAM enzymes produce 5'-deoxyadenosine, and SAM-dependent enzymes for polyamine, neurotransmitter and quorum sensing compound synthesis produce 5'-methylthioadenosine as by-products. Both are inhibitory and must be addressed by all cells. This work establishes a bifunctional oxygen-independent salvage pathway for 5'-deoxyadenosine and 5'-methylthioadenosine in both Rhodospirillum rubrum and Extraintestinal Pathogenic Escherichia coli. Homologous genes for this pathway are widespread in bacteria, notably pathogenic strains within several families. A phosphorylase (Rhodospirillum rubrum) or separate nucleoside and kinase (Escherichia coli) followed by an isomerase and aldolase sequentially function to salvage these two wasteful and inhibitory compounds into adenine, dihydroxyacetone phosphate and acetaldehyde or (2-methylthio)acetaldehyde during both aerobic and anaerobic growth. Both SAM by-products are metabolized with equal affinity during aerobic and anaerobic growth conditions, suggesting that the dual-purpose salvage pathway plays a central role in numerous environments, notably the human body during infection. Our newly discovered bifunctional oxygen-independent pathway, widespread in bacteria, salvages at least two by-products of SAM-dependent enzymes for carbon and sulfur salvage, contributing to cell growth.

Published

2020

12. A General Method for Quantification and Discovery of Acyl Groups Attached to Acyl Carrier Proteins in Fatty Acid Metabolism Using LC-MS/MS

Author

Jeong-Won Nam, Jan G. Jaworski, Douglas K. Allen, Bradley S. Evans, Jia Li, and Lauren M Jenkins

Subjects

0106 biological sciences, 0301 basic medicine, Acylation, Plant Science, Mitochondrion, 01 natural sciences, In Brief, 03 medical and health sciences, chemistry.chemical_compound, stomatognathic system, Tandem Mass Spectrometry, Lc ms ms, Acyl Carrier Protein, Amino Acid Sequence, Peptide sequence, Conserved Sequence, biology, Fatty acid metabolism, Fatty Acids, Lipid metabolism, Cell Biology, biology.organism_classification, humanities, Biosynthetic Pathways, Plant Leaves, Chloroplast, 030104 developmental biology, Biochemistry, chemistry, Carrier protein, Brassicaceae, Seeds, lipids (amino acids, peptides, and proteins), Bacteria, Chromatography, Liquid, 010606 plant biology & botany

Abstract

Acyl carrier proteins (ACPs) are the scaffolds for fatty acid biosynthesis in living systems, rendering them essential to a comprehensive understanding of lipid metabolism. However, accurate quantitative methods to assess individual acyl-ACPs do not exist. We developed a robust method to quantify acyl-ACPs to the picogram level. We successfully identified acyl-ACP elongation intermediates (3-hydroxyacyl-ACPs and 2,3-trans-enoyl-ACPs) and unexpected medium-chain (C10:1, C14:1) and polyunsaturated long-chain (C16:3) acyl-ACPs, indicating both the sensitivity of the method and how current descriptions of lipid metabolism and ACP function are incomplete. Such ACPs are likely important to medium-chain lipid production for fuels and highlight poorly understood lipid remodeling events in the chloroplast. The approach is broadly applicable to type II fatty acid synthase systems found in plants and bacteria as well as mitochondria from mammals and fungi because it capitalizes on a highly conserved Asp-Ser-Leu-Asp amino acid sequence in ACPs to which acyl groups attach. Our method allows for sensitive quantification using liquid chromatography-tandem mass spectrometry with de novo-generated standards and an isotopic dilution strategy and will fill a gap in our understanding, providing insights through quantitative exploration of fatty acid biosynthesis processes for optimal biofuels, renewable feedstocks, and medical studies in health and disease.

Published

2020

13. Metabolic Analysis of Regionally Distinct Gut Microbial Communities Using an In Vitro Platform

Author

Ceylan Tanes, Kyle Bittinger, Bradley S. Evans, Pieter Van den Abbeele, Elliot S. Friedman, LinShu Liu, Jenni Firrman, and Scott G. Daniel

Subjects

0106 biological sciences, chemistry.chemical_classification, 010401 analytical chemistry, Fatty acid, General Chemistry, Biology, Gut flora, biology.organism_classification, 01 natural sciences, In vitro, 0104 chemical sciences, Untargeted metabolomics, Nutrient, Biochemistry, chemistry, Community composition, Metagenomics, General Agricultural and Biological Sciences, 010606 plant biology & botany

Abstract

The colon gut microbiota is responsible for complex chemical conversions of nutrients and subsequent release of metabolites that have diverse biological consequences. However, information on the metabolic dynamics that occur longitudinally through the colon is limited. Here, gas and liquid chromatographies coupled with mass spectrometry were applied to generate metabolic profiles of the region-specific microbial communities cultured using an in vitro platform simulating the ascending (AC), transverse (TC), and descending (DC) colon regions. Comparative analysis revealed a large divergence between metabolic profiles of the AC and the TC and DC regions in terms of short-chain fatty acid production, metabolic spectrum, and conversion of bile acids. Metagenomic evaluation revealed that the regionally derived metabolic profiles had strong correlation to community composition and genetic potential. Together, the results provide key insights regarding the metabolic divergence of the regional communities that are integral to understand the structure-function relationship of the gut microbiota.

Published

2019

14. Systems-wide Analysis Revealed Shared and Unique Responses to Moderate and Acute High Temperatures in the Green Alga Chlamydomonas reinhardtii

Author

Ru Zhang, Eric Becker, Kirk J. Czymmek, Ningning Zhang, Ming Xia, Frederick R. Cross, Cheyenne M. Anderson, Chen Chen, Erin M. Mattoon, Benedikt Venn, Leila Pazouki, Timo Mühlhaus, Bradley S. Evans, David Zimmer, Michael Schroda, Will McHargue, Jeffrey C. Berry, Jianlin Cheng, Jooyeon Jeong, Kresti Pecani, and Shin-Cheng Tzeng

Subjects

biology, Chemistry, Photoprotection, Thylakoid, Glyoxylate cycle, Chlamydomonas reinhardtii, Cell cycle, Photosynthetic efficiency, Photosynthesis, biology.organism_classification, Pyrenoid, Cell biology

Abstract

Different intensities of high temperatures affect the growth of photosynthetic cells in nature. To elucidate the underlying mechanisms, we cultivated the unicellular green alga Chlamydomonas reinhardtii under highly controlled photobioreactor conditions and revealed systems-wide shared and unique responses to 24-hour moderate (35°C) and acute (40°C) high temperatures and subsequent recovery at 25°C. We identified previously overlooked unique elements in response to moderate high temperature. Heat at 35°C transiently arrested the cell cycle followed by partial synchronization, up-regulated transcripts/proteins involved in gluconeogenesis/glyoxylate-cycle for carbon uptake, promoted growth, and increased starch accumulation. Heat at 40°C arrested the cell cycle, inhibited growth, resulting in carbon uptake over usage and increased starch accumulation. Both high temperatures induced photoprotection, while 40°C decreased photosynthetic efficiency, distorted thylakoid/pyrenoid ultrastructure, and affected the carbon concentrating mechanism. We demonstrated increased transcript/protein correlation during both heat treatments, suggesting reduced post-transcriptional regulation during heat may help coordinate heat tolerance activities efficiently. During recovery after both heat treatments, transcripts/proteins related to DNA synthesis increased while those involved in photosynthetic light reactions decreased. We propose down-regulating photosynthetic light reactions during DNA replication benefits cell cycle resumption by reducing ROS production. Our results provide potential targets to increase thermotolerance in algae and crops.

Published

2021

15. An Improved Top-Down Mass Spectrometry Characterization of

Author

Sarah R, Rommelfanger, Mowei, Zhou, Henna, Shaghasi, Shin-Cheng, Tzeng, Bradley S, Evans, Ljiljana, Paša-Tolić, James G, Umen, and James J, Pesavento

Subjects

Histones, Algal Proteins, Acetylation, Protein Processing, Post-Translational, Cells, Cultured, Chlamydomonas reinhardtii, Mass Spectrometry

Abstract

We present an updated analysis of the linker and core histone proteins and their proteoforms in the green microalga

Published

2021

16. Quantification of Acyl-Acyl Carrier Proteins for Fatty Acid Synthesis Using LC-MS/MS

Author

Lauren M, Jenkins, Jeong-Won, Nam, Bradley S, Evans, and Doug K, Allen

Subjects

Bacteria, Lipogenesis, Fatty Acids, Plants, Lipid Metabolism, Lipids, Mitochondria, Tandem Mass Spectrometry, Acyl Carrier Protein, Acyl Coenzyme A, Amino Acid Sequence, Chromatography, High Pressure Liquid, Conserved Sequence, Chromatography, Liquid

Abstract

The fatty acid biosynthetic cycle is predicated on an acyl carrier protein (ACP) scaffold where two carbon acetyl groups are added in a chain elongation process through a series of repeated enzymatic steps. The chain extension is terminated by hydrolysis with a thioesterase or direct transfer of the acyl group to a glycerophospholipid by an acyltransferase. Methods for analysis of the concentrations of acyl chains attached to ACPs are lacking but would be informative for studies in lipid metabolism. We describe a method to profile and quantify the levels of acyl-ACPs in plants, bacteria and mitochondria of animals and fungi that represent Type II fatty acid biosynthetic systems. ACPs of Type II systems have a highly conserved Asp-Ser-Leu-Asp (DSLD) amino acid sequence at the attachment site for 4'-phosphopantetheinyl arm carrying the acyl chain. Three amino acids of the conserved sequence can be cleaved away from the remainder of the protein using an aspartyl protease. Thus, partially purified protein can be enzymatically hydrolyzed to produce an acyl chain linked to a tripeptide via the 4'-phosphopantetheinyl group. After ionization and fragmentation, the corresponding fragment ion is detected by a triple quadrupole mass spectrometer using a multiple reaction monitoring method.

Published

2021

17. Quantification of Acyl-Acyl Carrier Proteins for Fatty Acid Synthesis Using LC-MS/MS

Author

Jeong-Won Nam, Lauren M Jenkins, Bradley S. Evans, and Doug K. Allen

Subjects

0106 biological sciences, 0301 basic medicine, chemistry.chemical_classification, biology, Stereochemistry, Fatty acid, 01 natural sciences, Amino acid, 03 medical and health sciences, chemistry.chemical_compound, Acyl carrier protein, 030104 developmental biology, chemistry, Acyltransferase, Glycerophospholipid, biology.protein, lipids (amino acids, peptides, and proteins), Peptide sequence, Fatty acid synthesis, Acyl group, 010606 plant biology & botany

Abstract

The fatty acid biosynthetic cycle is predicated on an acyl carrier protein (ACP) scaffold where two carbon acetyl groups are added in a chain elongation process through a series of repeated enzymatic steps. The chain extension is terminated by hydrolysis with a thioesterase or direct transfer of the acyl group to a glycerophospholipid by an acyltransferase. Methods for analysis of the concentrations of acyl chains attached to ACPs are lacking but would be informative for studies in lipid metabolism. We describe a method to profile and quantify the levels of acyl-ACPs in plants, bacteria and mitochondria of animals and fungi that represent Type II fatty acid biosynthetic systems. ACPs of Type II systems have a highly conserved Asp-Ser-Leu-Asp (DSLD) amino acid sequence at the attachment site for 4'-phosphopantetheinyl arm carrying the acyl chain. Three amino acids of the conserved sequence can be cleaved away from the remainder of the protein using an aspartyl protease. Thus, partially purified protein can be enzymatically hydrolyzed to produce an acyl chain linked to a tripeptide via the 4'-phosphopantetheinyl group. After ionization and fragmentation, the corresponding fragment ion is detected by a triple quadrupole mass spectrometer using a multiple reaction monitoring method. 15N isotopically labeled acyl-ACPs generated in high amounts are used with an isotope dilution strategy to quantify the absolute levels of each acyl group attached to the acyl carrier protein scaffold.

Published

2021

18. Polygenic and sex specific architecture for two maturation traits in farmed Atlantic salmon

Author

Bradley S. Evans, Amin R. Mohamed, Sean McWilliam, Hawlader A. Al-Mamun, Harry King, James Kijas, Peter D. Kube, and Klara L. Verbyla

Subjects

0106 biological sciences, Male, Multifactorial Inheritance, Gene Expression, Genome-wide association study, Fresh Water, Breeding, 01 natural sciences, PICALM, Gene Frequency, Genotype, Databases, Genetic, Sexual maturity, GWAS, 0303 health sciences, Monomeric Clathrin Assembly Proteins, Female, Biotechnology, Research Article, Atlantic salmon (Salmo salar), lcsh:QH426-470, lcsh:Biotechnology, Salmo salar, Fisheries, Sexual maturation, SNP, Single-nucleotide polymorphism, Biology, Polymorphism, Single Nucleotide, Tasmania, Picalm, 03 medical and health sciences, Sex Factors, lcsh:TP248.13-248.65, Genetics, Genetic architecture, Animals, Seawater, Gene, 030304 developmental biology, Base Sequence, Whole Genome Sequencing, Genetic Variation, lcsh:Genetics, Evolutionary biology, Guanylate Kinases, 010606 plant biology & botany, Genome-Wide Association Study

Abstract

Background A key developmental transformation in the life of all vertebrates is the transition to sexual maturity, whereby individuals are capable of reproducing for the first time. In the farming of Atlantic salmon, early maturation prior to harvest size has serious negative production impacts. Results We report genome wide association studies (GWAS) using fish measured for sexual maturation in freshwater or the marine environment. Genotypic data from a custom 50 K single nucleotide polymorphism (SNP) array was used to identify 13 significantly associated SNP for freshwater maturation with the most strongly associated on chromosomes 10 and 11. A higher number of associations (48) were detected for marine maturation, and the two peak loci were found to be the same for both traits. The number and broad distribution of GWAS hits confirmed a highly polygenetic nature, and GWAS performed separately within males and females revealed sex specific genetic behaviour for loci co-located with positional candidate genes phosphatidylinositol-binding clathrin assembly protein-like (picalm) and membrane-associated guanylate kinase, WW and PDZ domain-containing protein 2 (magi2). Conclusions The results extend earlier work and have implications for future applied breeding strategies to delay maturation in this important aquaculture species. Electronic supplementary material The online version of this article (10.1186/s12864-019-5525-4) contains supplementary material, which is available to authorized users.

Published

2019

19. Proteomic and Transcriptomic Analysis of Exosomes in COPD

Author

D. Steinberg, Shin-Cheng Tzeng, Bradley S. Evans, E. Katz, Jennifer Alexander-Brett, Colin E. Kluender, and E. Roberson

Subjects

Computational biology, Microvesicles

Published

2020

20. Quantitative Proteomics and Phosphoproteomics Supports a Role for Mut9-Like Kinases in Multiple Metabolic and Signaling Pathways in Arabidopsis

Author

Dmitri A. Nusinow, Jae H. Choi, John C. Rogers, Toni M. Kutchan, Xiaoyue Jiang, Margaret Wilson, Matthew Meyer, Shin-Chen Tzeng, Bradley S. Evans, and Megan M. Augustin

Subjects

Proteomics, ABA, abscisic acid, Biochemistry, Analytical Chemistry, SYD, SPLAYED, GLS, glucosinolate, Arabidopsis, Protein phosphorylation, 0303 health sciences, FDR, false discover rate, plants, BRM, Brahma, Kinase, 030302 biochemistry & molecular biology, Phosphoproteomics, Cell biology, quantitative phosphoproteomics, Proteome, ZT14, Zeitgeber 14, Phosphorylation, Signal transduction, Metabolic Networks and Pathways, Signal Transduction, quantitative proteomics, RVE8, Reveille 8, kinase, DDR, DNA damage repair, Quantitative proteomics, Protein Serine-Threonine Kinases, Biology, 03 medical and health sciences, Stress, Physiological, CCA1, circadian clock associated, HY5, elongated hypocotyl 5, Molecular Biology, GO, gene ontology, 030304 developmental biology, Abiotic stress, Arabidopsis Proteins, Research, TMT, tandem mass tag, Phosphoproteins, biology.organism_classification, arabidopsis, circadian, Mutation, DNA damage, ZT12, Zeitgeber 12, phyB, phytochrome B, MLK, Mut9-like kinase

Abstract

Protein phosphorylation is one of the most prevalent posttranslational modifications found in eukaryotic systems. It serves as a key molecular mechanism that regulates protein function in response to environmental stimuli. The Mut9-like kinases (MLKs) are a plant-specific family of Ser/Thr kinases linked to light, circadian, and abiotic stress signaling. Here we use quantitative phosphoproteomics in conjunction with global proteomic analysis to explore the role of the MLKs in daily protein dynamics. Proteins involved in light, circadian, and hormone signaling, as well as several chromatin-modifying enzymes and DNA damage response factors, were found to have altered phosphorylation profiles in the absence of MLK family kinases. In addition to altered phosphorylation levels, mlk mutant seedlings have an increase in glucosinolate metabolism enzymes. Subsequently, we show that a functional consequence of the changes to the proteome and phosphoproteome in mlk mutant plants is elevated glucosinolate accumulation and increased sensitivity to DNA damaging agents. Combined with previous reports, this work supports the involvement of MLKs in a diverse set of stress responses and developmental processes, suggesting that the MLKs serve as key regulators linking environmental inputs to developmental outputs., Graphical abstract, Highlights • MUT9-LIKE KINASE mutant quantitative proteome and phosphoproteome measured. • Changes to proteome and phosphoproteome are specific to genotype and environment. • Loss of MLKs alters glucosinolate enzyme abundance and metabolism. • Loss of MLKs increases plant sensitivity to UV radiation and DNA damage agents., In Brief The MUT9-like kinases are a family of plant-specific nuclear-localized kinases with roles in diverse signaling pathways, including light sensing, phytohormone perception, and the circadian clock. The proteome and phosphoproteome of compound mlk mutant seedlings have been determined under light and dark conditions. These experiments identify new roles for these kinases regulating secondary plant metabolism and stress responses, tested through metabolite analysis and assaying seedling sensitivity to DNA damaging agents.

Published

2020

21. Quantification and Discovery of Acyl-ACPs by LC-MS/MS

Author

Jia Li, Jeong-Won Nam, Douglas K. Allen, Jan G. Jaworski, Lauren M Jenkins, and Bradley S. Evans

Subjects

0303 health sciences, Fatty acid biosynthesis, biology, Chemistry, 030302 biochemistry & molecular biology, Lipid metabolism, Mitochondrion, biology.organism_classification, humanities, Chloroplast, 03 medical and health sciences, Biochemistry, stomatognathic system, Lc ms ms, lipids (amino acids, peptides, and proteins), Peptide sequence, Function (biology), Bacteria, 030304 developmental biology

Abstract

Acyl carrier proteins (ACPs) are the scaffolds for fatty acid biosynthesis in living systems, rendering them essential to a comprehensive understanding of lipid metabolism; however, accurate quantitative methods to assess individual acyl-ACPs do not exist. A robust method was developed to quantify acyl-ACPs at picogram levels. Acyl-ACP elongation intermediates (3-hydroxyacyl-ACPs and 2, 3-trans-enoyl-ACPs), and unexpected medium chain (C10:1, C14:1) and polyunsaturated long chain acyl-ACPs (C16:3) were also identified, indicating the sensitivity of the method and that descriptions of lipid metabolism and ACP function are incomplete. Such ACPs are likely important to medium chain lipid production for fuels and highlight poorly understood lipid remodeling events in the chloroplast. The approach is broadly applicable to Type II FAS systems found in plants, bacteria, and mitochondria of animal and fungal systems because it uses a strategy that capitalizes on a highly conserved Asp-Ser-Leu-Asp (DSLD) amino acid sequence in ACPs to which acyl groups are attached. This allows for sensitive quantification using LC-MS/MS withde novogenerated standards and an isotopic dilution strategy and will fill a gap in understanding, providing insights through quantitative exploration of fatty acid biosynthesis processes for optimal biofuels, renewable feed stocks, and medical studies in health and disease.

Published

2019

22. Bacteriophage φEf11 ORF28 Endolysin, a Multifunctional Lytic Enzyme with Properties Distinct from All Other Identified Enterococcus faecalis Phage Endolysins

Author

Derrick E. Fouts, Hongming Zhang, Roy H. Stevens, Bettina A. Buttaro, Salar Sanjari, and Bradley S. Evans

Subjects

Lysis, Lysin, Siphoviridae, Applied Microbiology and Biotechnology, Enterococcus faecalis, Microbiology, Amidase, Bacteriophage, 03 medical and health sciences, chemistry.chemical_compound, Viral Proteins, Endopeptidases, Amino Acid Sequence, Enzymology and Protein Engineering, 030304 developmental biology, 0303 health sciences, Ecology, biology, Base Sequence, 030306 microbiology, Chemistry, biology.organism_classification, Lytic cycle, Peptidoglycan, Sequence Alignment, Food Science, Biotechnology

Abstract

ϕEf11 is a temperate Siphoviridae bacteriophage that infects strains of Enterococcus faecalis. The ϕEf11 genome, encompassing 65 open reading frames (ORFs), is contained within 42,822 bp of DNA. Within this genome, a module of six lysis-related genes was identified. Based upon sequence homology, one of these six genes, ORF28, was predicted to code for an N-acetylmuramoyl-l-alanine amidase endolysin of 46.133 kDa, composed of 421 amino acids. The PCR-amplified ORF28 was cloned and expressed, and the resulting gene product was affinity purified to homogeneity. The purified protein was obtained from a fusion protein that exhibited a molecular mass of 72.5 kDa, consistent with a 46.1-kDa protein combined with a fused 26.5-kDa glutathione S-transferase tag. It produced rapid, profound lysis in E. faecalis populations and was active against 73 of 103 (71%) E. faecalis strains tested. In addition, it caused substantial destruction of E. faecalis biofilms. The lysin was quite stable, retaining its activity for three years in refrigerated storage, was stable over a wide range of pHs, and was unaffected by the presence of a reducing agent; however, it was inhibited by increasing concentrations of Ca2+. Liquid chromatography-mass spectrometry analysis of E. faecalis cell wall digestion products produced by the ORF28 endolysin indicated that the lysin acted as an N-acetylmuramidase, an endo-β-N-acetylglucosaminidase, and an endopeptidase, rather than an N-acetylmuramoyl-l-alanine amidase. The ϕEf11 ORF28 lysin shared 10% to 37% amino acid identity with the lytic enzymes of all other characterized E. faecalis bacteriophages. IMPORTANCE The emergence of multidrug-resistant pathogenic microorganisms has brought increasing attention to the urgent need for the development of alternative antimicrobial strategies. One such alternative to conventional antibiotics employs lytic enzymes (endolysins) that are produced by bacteriophages in the course of lytic infection. During lytic infection by a bacteriophage, these enzymes hydrolyze the cell wall peptidoglycan, resulting in the lysis of the host cell. However, external endolysin application can result in lysis from without. In this study, we have cloned, expressed, purified, and characterized an endolysin produced by a bacteriophage infecting strains of Enterococcus faecalis. The lysin is broadly active against most of the tested E. faecalis strains and exhibits multifunctional enzymatic specificities that differ from all other characterized endolysins produced by E. faecalis bacteriophages.

Published

2019

23. Abstract 2225: Transposable elements are an abundant and pan-cancer source of shared tumor-specific antigens and membrane targets

Author

Hyo Sik Jang, Xiaoyun Xing, Daofeng Li, Noah L. Basri, Angela Wu, Ting Wang, Bradley S. Evans, Shin-Cheng Tzeng, Changxu Fan, Nakul M. Shah, Benjamin Katz, and Ju Heon Maeng

Subjects

Transposable element, Cancer Research, Cancer, Computational biology, Biology, medicine.disease_cause, medicine.disease, Genome, Oncology, Cancer cell, medicine, Gene silencing, Epigenetics, Carcinogenesis, Gene

Abstract

Transposable elements (TEs) represent close to half of the genome and are generally disregarded in genomic studies due to their silencing in somatic tissues and difficulty in mapping to their repetitive sequences. Recent studies have revealed that epigenetic dysregulation in cancer can unlock the regulatory potential of transposable elements (TEs), and they can play an important role in cancer progression and oncogenesis. One important consequence of this phenomenon is the pervasive activation of TEs' intrinsic promoters, which leads to generation of thousands of unique transcripts. Many of these transcripts splice into downstream genes and lead to the generation of TE-gene chimeric transcripts. These transcripts can alter the main reading frame of the original transcript to generate unique isoforms of the target gene or generate novel out-of-frame peptides that could be therapeutic targets. In this study, we analyzed the transcriptomes of 11,092 samples from 33 TCGA cancer types and 675 cancer cell lines to comprehensively profile all TE-gene fusion transcripts. Using somatic tissues from FANTOM5 and GTEx, we filtered these transcripts for tumor-specificity and discovered 2,642 tumor-specific TE-gene transcripts that promiscuously occur in nearly all TCGA tumor samples. Computational prediction of reading frames of these transcripts identified 1,202 candidates with the potential to generate tumor-specific TE-derived antigens (TS-TEAs). We further analyzed tumor mass spectrometry data from breast adenocarcinoma and ovarian cancer and confirmed that unique peptide sequences from TS-TEAs could be detected. In addition, we performed HLA-pulldown mass spectrometry and confirmed that TS-TEAs are presented on the cell surface in cancer cell lines. Given that these antigens are highly shared within and across cancer types, we assessed their potential to generate universal antigen-based therapies. Optimal combinations of 5, 10, and 20 TS-TEAs could generate unique peptides that bind to patient-specific HLA alleles for 39.2%, 50.8%, and 60.8% of all TCGA tumors respectively. Lastly, we highlight the tumor-specific membrane proteins transcribed from TE-exapted promoters that can potentially expose novel epitopes on the extracellular surface of cancer cells. These can be valuable targets of CAR-T or alternative antibody-based therapies. In conclusion, we showcase the high prevalence of TE-derived promoter activation in cancer and suggest multiple avenues by which this phenomenon can be targeted therapeutically. Citation Format: Nakul M. Shah, Hyo Sik Jang, Ju Heon Maeng, Shin-Cheng Tzeng, Angela Wu, Changxu Fan, Noah L. Basri, Benjamin Katz, Daofeng Li, Xiaoyun Xing, Bradley S. Evans, Ting Wang. Transposable elements are an abundant and pan-cancer source of shared tumor-specific antigens and membrane targets [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2021; 2021 Apr 10-15 and May 17-21. Philadelphia (PA): AACR; Cancer Res 2021;81(13_Suppl):Abstract nr 2225.

Published

2021

24. Mesencephalic Astrocyte–Derived Neurotrophic Factor as a Urine Biomarker for Endoplasmic Reticulum Stress–Related Kidney Diseases

Author

Maria Lindahl, Ying Maggie Chen, Heedoo Lee, Bradley S. Evans, Jeffrey H. Miner, Yeawon Kim, Scott R. Manson, and Fumihiko Urano

Subjects

0301 basic medicine, medicine.medical_specialty, Podocyte, Mice, 03 medical and health sciences, 0302 clinical medicine, Downregulation and upregulation, Neurotrophic factors, Internal medicine, medicine, Animals, Nerve Growth Factors, Kidney, business.industry, Endoplasmic reticulum, General Medicine, Endoplasmic Reticulum Stress, 3. Good health, 030104 developmental biology, medicine.anatomical_structure, Proteostasis, Endocrinology, Nephrology, 030220 oncology & carcinogenesis, Cancer research, Unfolded protein response, Biomarker (medicine), Kidney Diseases, Brief Communications, business, Biomarkers

Abstract

Endoplasmic reticulum (ER) stress and disrupted proteostasis contribute to the pathogenesis of a variety of glomerular and tubular diseases. Thus, it is imperative to develop noninvasive biomarkers for detecting ER stress in podocytes or tubular cells in the incipient stage of disease, when a kidney biopsy is not yet clinically indicated. Mesencephalic astrocyte–derived neurotrophic factor (MANF) localizes to the ER lumen and is secreted in response to ER stress in several cell types. Here, using mouse models of human nephrotic syndrome caused by mutant laminin β2 protein–induced podocyte ER stress and AKI triggered by tunicamycin– or ischemia-reperfusion–induced tubular ER stress, we examined MANF as a potential urine biomarker for detecting ER stress in podocytes or renal tubular cells. ER stress upregulated MANF expression in podocytes and tubular cells. Notably, urinary MANF excretion concurrent with podocyte or tubular cell ER stress preceded clinical or histologic manifestations of the corresponding disease. Thus, MANF can potentially serve as a urine diagnostic or prognostic biomarker in ER stress–related kidney diseases to help stratify disease risk, predict disease progression, monitor treatment response, and identify subgroups of patients who can be treated with ER stress modulators in a highly targeted manner.

Published

2016

25. Discovery of phosphonic acid natural products by mining the genomes of 10,000 actinomycetes

Author

Christopher J. Thibodeaux, Kwo Kwang A. Wang, Ryuichi Hirota, Joel P. Cioni, Joleen Su, Emily Metzger, Steven S. L. Li, Bradley S. Evans, Wilfred A. van der Donk, Jun Kai Zhang, Jiangtao Gao, Kou San Ju, David P. Labeda, William W. Metcalf, Jaeheon Lee, James R. Doroghazi, and John Fudala

Subjects

Genetics, Biological Products, Multidisciplinary, Natural product, Base Sequence, Phosphorous Acids, Drug discovery, Molecular Sequence Data, Genomics, Sequence Analysis, DNA, Biological Sciences, Biology, Phosphonate, Genome, DNA sequencing, Actinobacteria, chemistry.chemical_compound, chemistry, Drug Discovery, Genomic library, Gene, Genome, Bacterial, Gene Library

Abstract

Although natural products have been a particularly rich source of human medicines, activity-based screening results in a very high rate of rediscovery of known molecules. Based on the large number of natural product biosynthetic genes in microbial genomes, many have proposed "genome mining" as an alternative approach for discovery efforts; however, this idea has yet to be performed experimentally on a large scale. Here, we demonstrate the feasibility of large-scale, high-throughput genome mining by screening a collection of over 10,000 actinomycetes for the genetic potential to make phosphonic acids, a class of natural products with diverse and useful bioactivities. Genome sequencing identified a diverse collection of phosphonate biosynthetic gene clusters within 278 strains. These clusters were classified into 64 distinct groups, of which 55 are likely to direct the synthesis of unknown compounds. Characterization of strains within five of these groups resulted in the discovery of a new archetypical pathway for phosphonate biosynthesis, the first (to our knowledge) dedicated pathway for H-phosphinates, and 11 previously undescribed phosphonic acid natural products. Among these compounds are argolaphos, a broad-spectrum antibacterial phosphonopeptide composed of aminomethylphosphonate in peptide linkage to a rare amino acid N(5)-hydroxyarginine; valinophos, an N-acetyl l-Val ester of 2,3-dihydroxypropylphosphonate; and phosphonocystoximate, an unusual thiohydroximate-containing molecule representing a new chemotype of sulfur-containing phosphonate natural products. Analysis of the genome sequences from the remaining strains suggests that the majority of the phosphonate biosynthetic repertoire of Actinobacteria has been captured at the gene level. This dereplicated strain collection now provides a reservoir of numerous, as yet undiscovered, phosphonate natural products.

Published

2015

26. Elucidating steroid alkaloid biosynthesis in Veratrum californicum: production of verazine in Sf9 cells

Author

Jörg M. Augustin, Toni M. Kutchan, Bradley S. Evans, Ann Smithson, Ashutosh K. Shukla, Mark O’Neil-Johnson, David A. Mann, Dan R. Ruzicka, Michael R. McKain, Michael K. Deyholos, Megan M. Augustin, Patrick P. Edger, Courtney M. Starks, James H. Leebens-Mack, Gane Ka-Shu Wong, J. Chris Pires, and Matthew D. Barrett

Subjects

Cyclopamine, Veratrum californicum, medicine.medical_treatment, Plant Science, Article, Steroid, chemistry.chemical_compound, Cytochrome P-450 Enzyme System, Biosynthesis, Sf9 Cells, Genetics, medicine, Animals, Veratrum, Plant Proteins, chemistry.chemical_classification, biology, Sequence Analysis, RNA, Gene Expression Profiling, Alkaloid, Veratrum Alkaloids, Cell Biology, biology.organism_classification, Biosynthetic Pathways, Enzymes, Veratrum alkaloid, Enzyme, Biochemistry, chemistry, 4-Aminobutyrate Transaminase, Transcriptome, Algorithms

Abstract

Steroid alkaloids have been shown to elicit a wide range of pharmacological effects that include anticancer and antifungal activities. Understanding the biosynthesis of these molecules is essential to bioengineering for sustainable production. Herein, we investigate the biosynthetic pathway to cyclopamine, a steroid alkaloid that shows promising antineoplastic activities. Supply of cyclopamine is limited, as the current source is solely derived from wild collection of the plant Veratrum californicum. To elucidate the early stages of the pathway to cyclopamine, we interrogated a V. californicum RNA-seq dataset using the cyclopamine accumulation profile as a predefined model for gene expression with the pattern-matching algorithm Haystack. Refactoring candidate genes in Sf9 insect cells led to discovery of four enzymes that catalyze the first six steps in steroid alkaloid biosynthesis to produce verazine, a predicted precursor to cyclopamine. Three of the enzymes are cytochromes P450 while the fourth is a γ-aminobutyrate transaminase; together they produce verazine from cholesterol.

Published

2015

27. Purification and Characterization of Phosphonoglycans from Glycomyces sp. Strain NRRL B-16210 and Stackebrandtia nassauensis NRRL B-16338

Author

Neil P. J. Price, William W. Metcalf, Bradley S. Evans, and Xiaomin Yu

Subjects

Magnetic Resonance Spectroscopy, Molecular Sequence Data, Organophosphonates, Xylose, Polysaccharide, Microbiology, chemistry.chemical_compound, Mutase, Bacterial Proteins, Actinomycetales, Hexose, Molecular Biology, chemistry.chemical_classification, biology, Polysaccharides, Bacterial, Articles, biology.organism_classification, Phosphonate, Molecular Weight, Carbohydrate Sequence, chemistry, Biochemistry, Phosphotransferases (Phosphomutases), Galactose, Acid hydrolysis

Abstract

Two related actinomycetes, Glycomyces sp. strain NRRL B-16210 and Stackebrandtia nassauensis NRRL B-16338, were identified as potential phosphonic acid producers by screening for the gene encoding phosphoenolpyruvate (PEP) mutase, which is required for the biosynthesis of most phosphonates. Using a variety of analytical techniques, both strains were subsequently shown to produce phosphonate-containing exopolysaccharides (EPS), also known as phosphonoglycans. The phosphonoglycans were purified by sequential organic solvent extractions, methanol precipitation, and ultrafiltration. The EPS from the Glycomyces strain has a mass of 40 to 50 kDa and is composed of galactose, xylose, and five distinct partially O -methylated galactose residues. Per-deutero-methylation analysis indicated that galactosyl residues in the polysaccharide backbone are 3,4-linked Gal, 2,4-linked 3-MeGal, 2,3-linked Gal, 3,6-linked 2-MeGal, and 4,6-linked 2,3-diMeGal. The EPS from the Stackebrandtia strain is comprised of glucose, galactose, xylose, and four partially O -methylated galactose residues. Isotopic labeling indicated that the O -methyl groups in the Stackebrandtia phosphonoglycan arise from S -adenosylmethionine. The phosphonate moiety in both phosphonoglycans was shown to be 2-hydroxyethylphosphonate (2-HEP) by 31 P nuclear magnetic resonance (NMR) and mass spectrometry following strong acid hydrolysis of the purified molecules. Partial acid hydrolysis of the purified EPS from Glycomyces yielded 2-HEP in ester linkage to the O -5 or O -6 position of a hexose and a 2-HEP mono(2,3-dihydroxypropyl)ester. Partial acid hydrolysis of Stackebrandtia EPS also revealed the presence of 2-HEP mono(2,3-dihydroxypropyl)ester. Examination of the genome sequences of the two strains revealed similar pepM -containing gene clusters that are likely to be required for phosphonoglycan synthesis.

Published

2014

28. General Method for Quantification and Discovery of Acyl Groups Attached to Acyl Carrier Proteins in Fatty Acid Metabolism Using LC-MS/MS[OPEN].

Author

1, Jeong-Won Nam, 1, Lauren M. Jenkins, Li, Jia, 2, Bradley S. Evans, 2, Jan G. Jaworski, and 2, Doug K. Allen

Published

2020

29. SOD2 to SOD1 Switch in Breast Cancer

Author

Doris Germain, Ellen L. Marsh, Luena Papa, Bradley S. Evans, and Mary Hahn

Subjects

Epithelial-Mesenchymal Transition, SIRT3, animal diseases, SOD1, SOD2, Down-Regulation, Breast Neoplasms, Mitochondrion, Biology, Biochemistry, Gene Expression Regulation, Enzymologic, chemistry.chemical_compound, Superoxide Dismutase-1, Superoxides, Cell Line, Tumor, Sirtuin 3, Humans, Enzyme Inhibitors, skin and connective tissue diseases, Molecular Biology, chemistry.chemical_classification, Reactive oxygen species, Superoxide Dismutase, Superoxide, nutritional and metabolic diseases, Cell Biology, Molecular biology, nervous system diseases, Neoplasm Proteins, Cell biology, Gene Expression Regulation, Neoplastic, chemistry, Cancer cell, cardiovascular system, Female, Intermembrane space, Reports

Abstract

Cancer cells are characterized by elevated levels of reactive oxygen species, which are produced mainly by the mitochondria. The dismutase SOD2 localizes in the matrix and is a major antioxidant. The activity of SOD2 is regulated by the deacetylase SIRT3. Recent studies indicated that SIRT3 is decreased in 87% of breast cancers, implying that the activity of SOD2 is compromised. The resulting elevation in reactive oxygen species was shown to be essential for the metabolic reprograming toward glycolysis. Here, we show that SOD2 itself is down-regulated in breast cancer cell lines. Further, activation of oncogenes, such as Ras, promotes the rapid down-regulation of SOD2. Because in the absence of SOD2, superoxide levels are elevated in the matrix, we reasoned that mechanisms must exist to retain low levels of superoxide in other cellular compartments especially in the intermembrane space of the mitochondrial to avoid irreversible damage. The dismutase SOD1 also acts as an antioxidant, but it localizes to the cytoplasm and the intermembrane space of the mitochondria. We report here that loss of SOD2 correlates with the overexpression of SOD1. Further, we show that mitochondrial SOD1 is the main dismutase activity in breast cancer cells but not in non-transformed cells. In addition, we show that the SOD1 inhibitor LCS-1 leads to a drastic fragmentation and swelling of the matrix, suggesting that in the absence of SOD2, SOD1 is required to maintain the integrity of the organelle. We propose that by analogy to the cadherin switch during epithelial-mesenchymal transition, cancer cells also undergo a SOD switch during transformation.

Published

2014

30. Negative Feedback Regulation of Fatty Acid Production Based on a Malonyl-CoA Sensor–Actuator

Author

Fuzhong Zhang, Yi Xiao, Bradley S. Evans, and Di Liu

Subjects

Biomedical Engineering, Biology, Biochemistry, Genetics and Molecular Biology (miscellaneous), Mass Spectrometry, chemistry.chemical_compound, Synthetic biology, Bacterial Proteins, Negative feedback, Gene expression, Escherichia coli, Promoter Regions, Genetic, Chromatography, High Pressure Liquid, chemistry.chemical_classification, Base Sequence, Cell growth, Fatty Acids, Fatty acid, General Medicine, Pyruvate carboxylase, Malonyl Coenzyme A, Malonyl-CoA, Metabolic Engineering, Biochemistry, chemistry, Genetic Engineering, Intracellular, Acetyl-CoA Carboxylase, Bacillus subtilis

Abstract

Engineering metabolic biosynthetic pathways has enabled the microbial production of many useful chemicals. However, pathway productivities and yields are often limited by metabolic imbalances. Synthetic regulatory circuits have been shown to be able to balance engineered pathways, improving titers and productivities. Here we developed a negative feedback regulatory circuit based on a malonyl-CoA-based sensor-actuator. Malonyl-CoA is biosynthesized from acetyl-CoA by the acetyl-CoA carboxylase, which is the rate-limiting step for fatty acid biosynthesis. Overexpression of acetyl-CoA carboxylase improves fatty acid production, but slows down cell growth. We have devised a malonyl-CoA sensor-actuator that controls gene expression levels based on intracellular malonyl-CoA concentrations. This sensor-actuator is used to construct a negative feedback circuit to regulate the expression of acetyl-CoA carboxylase. The negative feedback circuit is able to up-regulate acetyl-CoA carboxylase expression when the malonyl-CoA concentration is low and down-regulate acetyl-CoA carboxylase expression when excess amounts of malonyl-CoA have accumulated. We show that the regulatory circuit effectively alleviates the toxicity associated with acetyl-CoA carboxylase overexpression. When used to regulate the fatty acid pathway, the feedback circuit increases fatty acid titer and productivity by 34% and 33%, respectively.

Published

2014

31. Use of a Phosphonate Methyltransferase in the Identification of the Fosfazinomycin Biosynthetic Gene Cluster

Author

Wilfred A. van der Donk, Bradley S. Evans, James R. Doroghazi, Jaeheon Lee, Jiangtao Gao, Kou San Ju, Xiaomin Yu, Juan Esteban Velasquez, William W. Metcalf, Subha Mukherjee, and Changming Zhao

Subjects

S-Adenosylmethionine, Methyltransferase, Stereochemistry, Carboxylic acid, Organophosphonates, Article, Catalysis, Open Reading Frames, chemistry.chemical_compound, Organophosphorus Compounds, Biosynthesis, Gene cluster, DNA, Fungal, chemistry.chemical_classification, Biological Products, Natural product, Methionine, Computational Biology, General Medicine, Methyltransferases, General Chemistry, Phosphonate, Streptomyces, Anti-Bacterial Agents, Hydrazines, chemistry, Biochemistry, Isotope Labeling, Multigene Family, Linker

Abstract

Natural product discovery has been boosted by genome mining approaches, but compound purification is often still challenging. We report an enzymatic strategy for "stable isotope labeling of phosphonates in extract" (SILPE) that facilitates their purification. We used the phosphonate methyltransferase DhpI involved in dehydrophos biosynthesis to methylate a variety of phosphonate natural products in crude spent medium with a mixture of labeled and unlabeled S-adenosyl methionine. Mass-guided fractionation then allowed straightforward purification. We illustrate its utility by purifying a phosphonate that led to the identification of the fosfazinomycin biosynthetic gene cluster. This unusual natural product contains a hydrazide linker between a carboxylic acid and a phosphonic acid. Bioinformatic analysis of the gene cluster provides insights into how such a structure might be assembled.

Published

2013

32. Discovery of the Antibiotic Phosacetamycin via a New Mass Spectrometry-Based Method for Phosphonic Acid Detection

Author

Wilfred A. van der Donk, Changming Zhao, Neil L. Kelleher, Bradley S. Evans, James R. Doroghazi, William W. Metcalf, Jiangtao Gao, Courtney M. Evans, and Kou San Ju

Subjects

Biocide, Magnetic Resonance Spectroscopy, Phosphorous Acids, Metabolite, Molecular Sequence Data, Drug Evaluation, Preclinical, Microbial Sensitivity Tests, Fosfomycin, Phosphinate, Biochemistry, Streptomyces, Chromatography, Affinity, Mass Spectrometry, Article, Phosphates, chemistry.chemical_compound, Acetamides, Gene cluster, Escherichia coli, medicine, Molecular Structure, biology, General Medicine, biology.organism_classification, Phosphonate, Anti-Bacterial Agents, Biosynthetic Pathways, Glufosinate, chemistry, Multigene Family, Molecular Medicine, Genome, Bacterial, medicine.drug

Abstract

Naturally occurring phosphonates such as phosphinothricin (Glufosinate, a commercially used herbicide) and fosfomycin (Monurol, a clinically used antibiotic) have proved to be potent and useful biocides. Yet this class of natural products is still an under explored family of secondary metabolites. Discovery of the biosynthetic pathways responsible for the production of these compounds has been simplified by using gene based screening approaches, but detection and identification of the natural products the genes produce have been hampered by a lack of high-throughput methods for screening potential producers under various culture conditions. Here, we present an efficient mass-spectrometric method for the selective detection of natural products containing phosphonate and phosphinate functional groups. We have used this method to identify a new phosphonate metabolite, phosacetamycin, whose structure, biological activity, and biosynthetic gene cluster are reported.

Published

2013

33. Diversity and linkage disequilibrium in farmed Tasmanian Atlantic salmon

Author

H.R. King, Natasha A. Botwright, Klara L. Verbyla, Bradley S. Evans, Peter D. Kube, Craig R. Primmer, James Kijas, and N. Elliot

Subjects

0301 basic medicine, Male, Linkage disequilibrium, Population, Salmo salar, Aquaculture, Biology, Polymorphism, Single Nucleotide, Linkage Disequilibrium, Tasmania, 03 medical and health sciences, Gene Frequency, Genetics, Animals, Salmo, education, Allele frequency, education.field_of_study, Genetic diversity, ta1184, 04 agricultural and veterinary sciences, General Medicine, biology.organism_classification, SNP genotyping, Minor allele frequency, 030104 developmental biology, Evolutionary biology, 040102 fisheries, 0401 agriculture, forestry, and fisheries, Animal Science and Zoology, Female, Imputation (genetics)

Abstract

Summary Farmed Atlantic salmon (Salmo salar) is a globally important production species, including in Australia where breeding and selection has been in progress since the 1960s. The recent development of SNP genotyping platforms means genome-wide association and genomic prediction can now be implemented to speed genetic gain. As a precursor, this study collected genotypes at 218 132 SNPs in 777 fish from a Tasmanian breeding population to assess levels of genetic diversity, the strength of linkage disequilibrium (LD) and imputation accuracy. Genetic diversity in Tasmanian Atlantic salmon was lower than observed within European populations when compared using four diversity metrics. The distribution of allele frequencies also showed a clear difference, with the Tasmanian animals carrying an excess of low minor allele frequency variants. The strength of observed LD was high at short distances (

Published

2016

34. A RubisCO like protein links SAM metabolism with isoprenoid biosynthesis

Author

Benjamin P. Warlick, F. Robert Tabita, John A. Gerlt, Heidi Imker, Bradley S. Evans, Kyuil Cho, Jonathan V. Sweedler, B. Mc Kay Wood, Jaya Sriram, and Tobias J. Erb

Subjects

Proteomics, Oxygenase, S-Adenosylmethionine, Magnetic Resonance Spectroscopy, Ribulose-Bisphosphate Carboxylase, Rhodospirillum rubrum, DNA sequencing, Article, 03 medical and health sciences, Metabolomics, Polyamines, Molecular Biology, 030304 developmental biology, 0303 health sciences, Thionucleosides, biology, Deoxyadenosines, Molecular Structure, 030306 microbiology, Terpenes, RuBisCO, Cell Biology, Metabolism, biology.organism_classification, Pyruvate carboxylase, Biochemistry, biology.protein, Transcriptome

Abstract

Functional assignment of uncharacterized proteins is a challenge in the era of large-scale genome sequencing. Here, we combine in extracto-NMR, proteomics, and transcriptomics with a newly developed (knock-out) metabolomics platform to determine a potential physiological role for a ribulose-1,5-bisphosphate carboxylase/oxygenase (RubisCO)-like protein (RLP) from Rhodospirillum rubrum. Our studies unravelled an unexpected link in bacterial central carbon metabolism between S-adenosylmethionine (SAM)-dependent polyamine metabolism and isoprenoid biosynthesis and also provide an alternative approach to assign enzyme function at the organismic level.

Published

2012

35. Mechanistic Investigation of Methylphosphonate Synthase, a Non-Heme Iron-Dependent Oxygenase

Author

Wilfred A. van der Donk, Spencer C. Peck, Heather A. Cooke, and Bradley S. Evans

Subjects

Oxygenase, Hydrogen, Stereochemistry, Iron, Kinetics, chemistry.chemical_element, Substrate analog, 010402 general chemistry, Photochemistry, 01 natural sciences, Biochemistry, Catalysis, Mass Spectrometry, chemistry.chemical_compound, Colloid and Surface Chemistry, Stereospecificity, Nuclear Magnetic Resonance, Biomolecular, Fourier Analysis, 010405 organic chemistry, Chemistry, Communication, Substrate (chemistry), General Chemistry, 0104 chemical sciences, Heme Oxygenase (Decyclizing), Oxygenases, Methyl group

Abstract

Methylphosphonate synthase is a non-heme iron-dependent oxygenase that converts 2-hydroxyethylphosphonate (2-HEP) to methylphosphonate. On the basis of experiments with two enantiomers of a substrate analog, 2-hydroxypropylphosphonate, catalysis is proposed to commence with stereospecific abstraction of the pro-S hydrogen on C2 of the substrate. Experiments with isotopologues of 2-HEP indicate stereospecific hydrogen transfer of the pro-R hydrogen at C2 of the substrate to the methyl group of methylphosphonate. Kinetic studies with these substrate isotopologues reveal that neither hydrogen transfer is rate limiting under saturating substrate conditions. A mechanism is proposed that is consistent with the available data.

Published

2012

36. Structure Determination and Interception of Biosynthetic Intermediates for the Plantazolicin Class of Highly Discriminating Antibiotics

Author

Stefanie B. Bumpus, Katie J. Molohon, Bradley S. Evans, Jaeheon Lee, Joel O. Melby, Douglas A. Mitchell, Neil L. Kelleher, and Kyle L. Dunbar

Subjects

Plantazolicin, Bacillus amyloliquefaciens, Stereochemistry, Metabolite, Molecular Sequence Data, Bacillus, Biochemistry, Article, chemistry.chemical_compound, Bacteriocins, Bacteriocin, Amino Acid Sequence, Thiazole, Oxazoles, Oxazole, biology, General Medicine, Microcin, biology.organism_classification, Anti-Bacterial Agents, Bacillus anthracis, Thiazoles, chemistry, Multigene Family, Molecular Medicine, Oligopeptides

Abstract

The soil-dwelling, plant growth-promoting bacterium Bacillus amyloliquefaciens FZB42 is a prolific producer of complex natural products. Recently, a new FZB42 metabolite, plantazolicin (PZN), has been described as a member of the growing thiazole/oxazole-modified microcin (TOMM) family. TOMMs are biosynthesized from inactive, ribosomal peptides and undergo a series of cyclodehydrations, dehydrogenations, and other modifications to become bioactive natural products. Using high-resolution mass spectrometry, chemoselective modification, genetic interruptions, and other spectroscopic tools, we have determined the molecular structure of PZN. In addition to two conjugated polyazole moieties, the amino-terminus of PZN has been modified to N(α),N(α)-dimethylarginine. PZN exhibited a highly selective antibiotic activity toward Bacillus anthracis, but no other tested human pathogen. By altering oxygenation levels during fermentation, PZN analogues were produced that bear variability in their heterocycle content, which yielded insight into the order of biosynthetic events. Lastly, genome-mining has revealed the existence of four additional PZN-like biosynthetic gene clusters. Given their structural uniqueness and intriguing antimicrobial specificity, the PZN class of antibiotics may hold pharmacological value.

Published

2011

37. Complexity Generation in Fungal Peptidyl Alkaloid Biosynthesis: Oxidation of Fumiquinazoline A to the Heptacyclic Hemiaminal Fumiquinazoline C by the Flavoenzyme Af12070 from Aspergillus fumigatus

Author

Neil L. Kelleher, Yi Tang, Stuart W. Haynes, Brian D. Ames, Bradley S. Evans, Christopher T. Walsh, and Xue Gao

Subjects

Alanine, Indole test, chemistry.chemical_classification, Annulation, Flavoproteins, biology, Stereochemistry, Aspergillus fumigatus, Flavoprotein, biology.organism_classification, Biochemistry, Article, Amino acid, Fungal Proteins, chemistry.chemical_compound, Alkaloids, chemistry, Quinazolines, biology.protein, Hemiaminal, Aminal, Peptide Synthases, Oxidoreductases, Oxidation-Reduction

Abstract

The human pathogen Aspergillus fumigatus makes a series of fumiquinazoline (FQ) peptidyl alkaloids of increasing scaffold complexity using L-Trp, two equivalents of L-Ala, and the non-proteinogenic amino acid anthranilate as building blocks. The FQ gene cluster encodes two nonribosomal peptide synthetases (NRPS) and two flavoproteins. The trimodular NRPS Af12080 assembles FQF (the first level of complexity) while the next two enzymes, Af12060 and Af12050, act in tandem in an oxidative annulation sequence to couple alanine to the indole side chain of FQF to yield the imidazolindolone-containing FQA. In this study we show that the fourth enzyme, the mono-covalent flavoprotein Af12070, introduces a third layer of scaffold complexity by converting FQA to the spirohemiaminal FQC, presumably by catalyzing the formation of a transient imine within the pyrazinone ring (and therefore acting in an unprecedented manner as an FAD-dependent amide oxidase). FQC subsequently converts non-enzymatically to the known cyclic aminal FQD. We also investigated the effect of substrate structure on Af12070 activity and subsequent cyclization with a variety of FQA analogues, including an FQA diastereomer (2′-epi-FQA) which is an intermediate in the fungal biosynthesis of the tremorgenic tryptoquialanine. 2′-epi-FQA is processed by Af12070 to epi-FQD, not epi-FQC, illustrating that the delicate balance in product cyclization regiochemistry can be perturbed by a remote stereochemical center.

Published

2011

38. Directed Evolution of the Nonribosomal Peptide Synthetase AdmK Generates New Andrimid Derivatives In Vivo

Author

Yunqiu Chen, Neil L. Kelleher, William W. Metcalf, Huimin Zhao, and Bradley S. Evans

Subjects

Clinical Biochemistry, Sequence alignment, Microbial Sensitivity Tests, Polyenes, medicine.disease_cause, 01 natural sciences, Biochemistry, Article, Small Molecule Libraries, 03 medical and health sciences, Bacterial Proteins, Nonribosomal peptide, Drug Discovery, medicine, Pyrroles, Amino Acid Sequence, Peptide Synthases, Secondary metabolism, Molecular Biology, Escherichia coli, 030304 developmental biology, Pharmacology, chemistry.chemical_classification, 0303 health sciences, biology, Pantoea, 010405 organic chemistry, General Medicine, biology.organism_classification, Directed evolution, Pantoea agglomerans, Anti-Bacterial Agents, 0104 chemical sciences, chemistry, Mutation, Molecular Medicine, Directed Molecular Evolution, Sequence Alignment

Abstract

Many lead compounds in the search for new drugs derive from peptides and polyketides whose similar biosynthetic enzymes have been difficult to engineer for production of new derivatives. Problems with generating multiple analogs in a single experiment along with lack of high-throughput methods for structure-based screening have slowed progress in this area. Here, we use directed evolution and a multiplexed assay to screen a library of >14,000 members to generate three new derivatives of the antibacterial compound, andrimid. Another limiting factor in reengineering these mega-enzymes of secondary metabolism has been that commonly used hosts such as Escherichia coli often give lower product titers, so our reengineering was performed in the native producer, Pantoea agglomerans. This integrated “in vivo” approach can be extended to larger enzymes to create analogues of natural products for bioactivity testing.

Published

2011

39. Surveys of non-ribosomal peptide and polyketide assembly lines in fungi and prospects for their analysis in vitro and in vivo

Author

Neil L. Kelleher, Sarah J. Robinson, and Bradley S. Evans

Subjects

Proteomics, Fungi, Ribosomal RNA, Biology, Microbiology, Mass Spectrometry, Article, Polyketide, chemistry.chemical_compound, Biosynthesis, chemistry, Biochemistry, Proteome, Peptide Biosynthesis, Nucleic Acid-Independent, Genetics, Macrolides, Peptide Biosynthesis, Peptides, Secondary metabolism, Gene

Abstract

With many bioactive non-ribosomal peptides and polyketides produced in fungi, studies of their biosyntheses are an active area of research. Practical limitations of working with mega-dalton synthetases including cell lysis and protein extraction to recombinant gene and pathway expression has slowed understanding of many secondary metabolic processes relative to bacterial counterparts. Recent advances in accessing fungal biosynthetic machinery are beginning to change this. Here we describe the successes of some studies of thiotemplate biosynthesis in fungal systems, along with very recent advances in chemical tagging and mass spectrometric strategies to selectively study biosynthetic conveyer belts in isolation, and within a few years, in endogenous fungal proteomes.

Published

2011

40. A Proteomics Approach to Discovery of Natural Products and Their Biosynthetic Pathways

Author

Paul M. Thomas, Ioanna Ntai, Stefanie B. Bumpus, Bradley S. Evans, and Neil L. Kelleher

Subjects

Proteomics, Biomedical Engineering, Bioengineering, Bacillus, Computational biology, Biology, 01 natural sciences, Applied Microbiology and Biotechnology, Article, Mass Spectrometry, 03 medical and health sciences, chemistry.chemical_compound, Polyketide, Lipopeptides, Nonribosomal peptide, Gene cluster, Cluster Analysis, Gene Regulatory Networks, Peptide Biosynthesis, Peptide Synthases, Gene, 030304 developmental biology, chemistry.chemical_classification, 0303 health sciences, Biological Products, 010405 organic chemistry, Peptide Fragments, Streptomyces, 0104 chemical sciences, chemistry, Biochemistry, Proteome, Pantetheine, Peptide Biosynthesis, Nucleic Acid-Independent, Molecular Medicine, Zwittermicin A, Polyketide Synthases, Metabolic Networks and Pathways, Biotechnology

Abstract

Many natural products with antibiotic, anticancer and antifungal properties are synthesized by nonribosomal peptide synthetases (NRPSs) and polyketide synthases (PKSs). Although genome sequencing has revealed the diversity of these enzymes, identifying new products and their biosynthetic pathways remains challenging. By taking advantage of the size of these enzymes (often >2,000 amino acids) and unique marker ions derived from their common phosphopantetheinyl cofactor, we adapted mass spectrometry-based proteomics to selectively detect NRPS and PKS gene clusters in microbial proteomes without requiring genome sequence information. We detected known NRPS systems in members of the genera Bacillus and Streptomyces, and screened 22 environmental isolates to uncover production of unknown natural products from the hybrid NRPS-PKS zwittermicin A biosynthetic gene cluster. We also discovered an NRPS cluster that generates a seven-residue lipopeptide. This 'protein-first' strategy complements bioassay- and sequence-based approaches by finding expressed gene clusters that produce new natural products.

Published

2009

41. Family by environment interactions in shell size of 43-day old silver-lip pearl oyster (Pinctada maxima), five families reared under different nursery conditions

Author

Renate Kvingedal, Bradley S. Evans, Joseph J. Taylor, Dean R. Jerry, and Jens Knauer

Subjects

biology, business.industry, Pteriidae, fungi, Zoology, Aquatic Science, equipment and supplies, Bivalvia, biology.organism_classification, Selective breeding, Hatchery, Fishery, Aquaculture, Pinctada maxima, bacteria, Gene–environment interaction, business, Food quality

Abstract

To understand the influence the environment and associated genotype by environment interactions will exert on future silver-lip pearl oyster (Pinctada maxima) selective breeding programs, this study assessed the relative performance in four shell growth traits of spat from five full-sib families, when spat were communally reared at different salinities (29, 34 and 40 ppt), food availability (high, medium and low), food quality (high, medium and low), and in a hatchery vs. ocean environment for 43 days. Rearing environment was found to influence growth expression, with significant differences evident when oysters were grown at different salinities in the ocean instead of hatchery, or when fed algae of differing nutritional quality. As indicated by MANOVA, family comparative growth performances were also altered when the environment changed, with significant environment by family interactions apparent in the food quality, food availability and hatchery vs. ocean rearing treatments. Changes in salinity, however, did not affect relevant family performances. These results indicate that growth and relative family performance in P. maxima may change dependent on local environmental conditions and that genotype by environment effects may need to be considered in breeding programs for this species.

Published

2008

42. PCH1 integrates circadian and light-signaling pathways to control photoperiod-responsive growth in Arabidopsis

Author

Bradley S. Evans, Sophie Alvarez, Chan Yul Yoo, Rebecca K. Bindbeutel, Allison Tielking, Dmitri A. Nusinow, He Huang, Jessica S. Goldsworthy, Michael J. Naldrett, and Meng Chen

Subjects

0301 basic medicine, circadian rhythm, Light, QH301-705.5, Science, photobody, Photoperiod, Circadian clock, Arabidopsis, Plant Biology, Gene Expression, Plant Development, Biology, A. thaliana, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Gene Knockout Techniques, Gene Expression Regulation, Plant, Phytochrome B, Circadian Clocks, Botany, Gene expression, Circadian rhythm, Biology (General), photoperiodism, phytochrome, General Immunology and Microbiology, Phytochrome, Arabidopsis Proteins, General Neuroscience, General Medicine, plant growth, biology.organism_classification, Cell biology, Metallochaperones, 030104 developmental biology, Medicine, Signal transduction, Biogenesis, signal transduction, Research Article

Abstract

Plants react to seasonal change in day length through altering physiology and development. Factors that function to harmonize growth with photoperiod are poorly understood. Here we characterize a new protein that associates with both circadian clock and photoreceptor components, named PHOTOPERIODIC CONTROL OF HYPOCOTYL1 (PCH1). pch1 seedlings have overly elongated hypocotyls specifically under short days while constitutive expression of PCH1 shortens hypocotyls independent of day length. PCH1 peaks at dusk, binds phytochrome B (phyB) in a red light-dependent manner, and co-localizes with phyB into photobodies. PCH1 is necessary and sufficient to promote the biogenesis of large photobodies to maintain an active phyB pool after light exposure, potentiating red-light signaling and prolonging memory of prior illumination. Manipulating PCH1 alters PHYTOCHROME INTERACTING FACTOR 4 levels and regulates light-responsive gene expression. Thus, PCH1 is a new factor that regulates photoperiod-responsive growth by integrating the clock with light perception pathways through modulating daily phyB-signaling. DOI: http://dx.doi.org/10.7554/eLife.13292.001, eLife digest Most living things possess an internal “circadian” clock that synchronizes many behaviors, such as eating, resting or growing, with the day-night cycle. With the help of proteins that can detect light, known as photoreceptors, the clock also coordinates these behaviors as the number of daylight hours changes during the year. However, it is not known how the clock and photoreceptors are able to work together. The circadian clocks of animals and plants have evolved separately and use different proteins. In plants, a photoreceptor called phytochrome B responds to red light and regulates the ability of plants to grow. Most plants harness sunlight during the day, but grow fastest in the dark just before dawn. In 2015, researchers identified a new protein in a plant called Arabidopsis that is associated with several plant clock proteins and photoreceptors, including phytochrome B. However, the role of this new protein was not clear. Now, Huang et al. – including many of the researchers from the 2015 work – studied the new protein, named PCH1, in more detail. The experiments show that PCH1 is a critical link that regulates the daily growth of Arabidopsis plants in response to the number of daylight hours. PCH1 stabilizes the structure of phytochrome B so that it remains active, even in the dark. This prolonged activity acts as a molecular memory of prior exposure to light and helps to prevent plants from growing too much in the winter when there are fewer hours of daylight. Since PCH1 is also found in other species of plants, it may play the same role in regulating growth of major crop plants. The next challenge is to understand how the binding of PCH1 to phytochrome B alters the photoreceptor’s activity. In the future, Huang et al. hope to find out if manipulating the activity of PCH1 can improve the growth of crops in places where there is a large change in day length across the seasons. DOI: http://dx.doi.org/10.7554/eLife.13292.002

Published

2016

43. Author response: PCH1 integrates circadian and light-signaling pathways to control photoperiod-responsive growth in Arabidopsis

Author

He Huang, Bradley S. Evans, Chan Yul Yoo, Dmitri A. Nusinow, Jessica S. Goldsworthy, Allison Tielking, Rebecca K. Bindbeutel, Michael J. Naldrett, Meng Chen, and Sophie Alvarez

Subjects

photoperiodism, biology, Arabidopsis, Circadian rhythm, Signal transduction, biology.organism_classification, Cell biology

Published

2016

44. Nonribosomal Peptide and Polyketide Biosynthesis

Author

Bradley S. Evans

Subjects

chemistry.chemical_classification, Polyketide, Biochemistry, Chemistry, Nonribosomal peptide, Polyketide biosynthesis, Peptide

Published

2016

45. Synergism between Inositol Polyphosphates and TOR Kinase Signaling in Nutrient Sensing, Growth Control, and Lipid Metabolism in Chlamydomonas

Author

Yu Liu, James G. Umen, Bradley S. Evans, Doug K. Allen, Spencer Diamond, Jia Li, Inmaculada Couso, and Fangfang Ma

Subjects

0301 basic medicine, Cell signaling, biology, Kinase, Chlamydomonas, Chlamydomonas reinhardtii, Lipid metabolism, Cell Biology, Plant Science, Nutrient sensing, biology.organism_classification, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, Biochemistry, chemistry, Breakthrough Reports, Inositol, Kinase activity

Abstract

The networks that govern carbon metabolism and control intracellular carbon partitioning in photosynthetic cells are poorly understood. Target of Rapamycin (TOR) kinase is a conserved growth regulator that integrates nutrient signals and modulates cell growth in eukaryotes, though the TOR signaling pathway in plants and algae has yet to be completely elucidated. We screened the unicellular green alga Chlamydomonas reinhardtii using insertional mutagenesis to find mutants that conferred hypersensitivity to the TOR inhibitor rapamycin. We characterized one mutant, vip1-1, that is predicted to encode a conserved inositol hexakisphosphate kinase from the VIP family that pyrophosphorylates phytic acid (InsP6) to produce the low abundance signaling molecules InsP7 and InsP8. Unexpectedly, the rapamycin hypersensitive growth arrest of vip1-1 cells was dependent on the presence of external acetate, which normally has a growth-stimulatory effect on Chlamydomonas. vip1-1 mutants also constitutively overaccumulated triacylglycerols (TAGs) in a manner that was synergistic with other TAG inducing stimuli such as starvation. vip1-1 cells had reduced InsP7 and InsP8, both of which are dynamically modulated in wild-type cells by TOR kinase activity and the presence of acetate. Our data uncover an interaction between the TOR kinase and inositol polyphosphate signaling systems that we propose governs carbon metabolism and intracellular pathways that lead to storage lipid accumulation

Published

2016

46. Identification of Evening Complex Associated Proteins in Arabidopsis by Affinity Purification and Mass Spectrometry

Author

Leslie M. Hicks, Sophie Alvarez, Steve A. Kay, Dmitri A. Nusinow, He Huang, Steven P. Briggs, Michael J. Naldrett, Rebecca K. Bindbeutel, Zhouxin Shen, and Bradley S. Evans

Subjects

Proteomics, 0301 basic medicine, Light Signal Transduction, Proteome, Green Fluorescent Proteins, Circadian clock, TOC1, Arabidopsis, Protein degradation, Biochemistry, Analytical Chemistry, 03 medical and health sciences, Tandem Mass Spectrometry, Two-Hybrid System Techniques, Botany, Circadian rhythm, Molecular Biology, Transcription factor, Microscopy, Confocal, biology, Phytochrome, Arabidopsis Proteins, Research, food and beverages, Plants, Genetically Modified, biology.organism_classification, Circadian Rhythm, Cell biology, 030104 developmental biology, Mutation, Chromatography, Liquid, Protein Binding, Transcription Factors

Abstract

Many species possess an endogenous circadian clock to synchronize internal physiology with an oscillating external environment. In plants, the circadian clock coordinates growth, metabolism and development over daily and seasonal time scales. Many proteins in the circadian network form oscillating complexes that temporally regulate myriad processes, including signal transduction, transcription, protein degradation and post-translational modification. In Arabidopsis thaliana, a tripartite complex composed of EARLY FLOWERING 4 (ELF4), EARLY FLOWERING 3 (ELF3), and LUX ARRHYTHMO (LUX), named the evening complex, modulates daily rhythms in gene expression and growth through transcriptional regulation. However, little is known about the physical interactions that connect the circadian system to other pathways. We used affinity purification and mass spectrometry (AP-MS) methods to identify proteins that associate with the evening complex in A. thaliana. New connections within the circadian network as well as to light signaling pathways were identified, including linkages between the evening complex, TIMING OF CAB EXPRESSION1 (TOC1), TIME FOR COFFEE (TIC), all phytochromes and TANDEM ZINC KNUCKLE/PLUS3 (TZP). Coupling genetic mutation with affinity purifications tested the roles of phytochrome B (phyB), EARLY FLOWERING 4, and EARLY FLOWERING 3 as nodes connecting the evening complex to clock and light signaling pathways. These experiments establish a hierarchical association between pathways and indicate direct and indirect interactions. Specifically, the results suggested that EARLY FLOWERING 3 and phytochrome B act as hubs connecting the clock and red light signaling pathways. Finally, we characterized a clade of associated nuclear kinases that regulate circadian rhythms, growth, and flowering in A. thaliana. Coupling mass spectrometry and genetics is a powerful method to rapidly and directly identify novel components and connections within and between complex signaling pathways.

Published

2016

47. In Vivo Studies in Rhodospirillum rubrum Indicate That Ribulose-1,5-bisphosphate Carboxylase/Oxygenase (Rubisco) Catalyzes Two Obligatorily Required and Physiologically Significant Reactions for Distinct Carbon and Sulfur Metabolic Pathways*♦

Author

Swati Dey, Justin A. North, F. Robert Tabita, Jaya Sriram, and Bradley S. Evans

Subjects

inorganic chemicals, Ribulose-Bisphosphate Carboxylase, Photosynthesis, Rhodospirillum rubrum, Biochemistry, chemistry.chemical_compound, Bacterial Proteins, Light-independent reactions, Molecular Biology, Ribulose 1,5-bisphosphate, Thionucleosides, biology, Deoxyadenosines, RuBisCO, Carbon fixation, fungi, food and beverages, Cell Biology, Carbon Dioxide, biology.organism_classification, Carbon, Metabolic pathway, Carboxysome, Metabolism, chemistry, biology.protein, Biocatalysis, Metabolic Networks and Pathways, Sulfur

Abstract

All organisms possess fundamental metabolic pathways to ensure that needed carbon and sulfur compounds are provided to the cell in the proper chemical form and oxidation state. For most organisms capable of using CO2 as sole source of carbon, ribulose-1,5-bisphosphate (RuBP) carboxylase/oxygenase (Rubisco) catalyzes primary carbon dioxide assimilation. In addition, sulfur salvage pathways are necessary to ensure that key sulfur-containing compounds are both available and, where necessary, detoxified in the cell. Using knock-out mutations and metabolomics in the bacterium Rhodospirillum rubrum, we show here that Rubisco concurrently catalyzes key and essential reactions for seemingly unrelated but physiologically essential central carbon and sulfur salvage metabolic pathways of the cell. In this study, complementation and mutagenesis studies indicated that representatives of all known extant functional Rubisco forms found in nature are capable of simultaneously catalyzing reactions required for both CO2-dependent growth as well as growth using 5-methylthioadenosine as sole sulfur source under anaerobic photosynthetic conditions. Moreover, specific inactivation of the CO2 fixation reaction did not affect the ability of Rubisco to support anaerobic 5-methylthioadenosine metabolism, suggesting that the active site of Rubisco has evolved to ensure that this enzyme maintains both key functions. Thus, despite the coevolution of both functions, the active site of this protein may be differentially modified to affect only one of its key functions.

Published

2015

48. 1-Methylthio-<scp>d</scp>-xylulose 5-Phosphate Methylsulfurylase: A Novel Route to 1-Deoxy-<scp>d</scp>-xylulose 5-Phosphate in Rhodospirillum rubrum

Author

Jaya Sriram, Bradley S. Evans, Jonathan S. Sweedler, Heidi Imker, Benjamin P. Warlick, Udipi A. Ramagopal, Jeffrey B. Bonanno, John A. Gerlt, Stephen K. Burley, Tobias J. Erb, Steven C. Almo, F. Robert Tabita, and J. Michael Sauder

Subjects

Pentosephosphates, biology, Chemistry, Stereochemistry, Methyl disulfide, Rhodospirillum rubrum, Active site, biology.organism_classification, Biochemistry, Article, Terpenoid, D-xylulose-5-phosphate, 1-deoxy-D-xylulose 5-phosphate, Thioglycosides, Sulfurtransferases, biology.protein, Ribosemonophosphates, Polyamine biosynthesis, Nuclear Magnetic Resonance, Biomolecular, Methionine salvage pathway, Metabolic Networks and Pathways

Abstract

Rhodospirillum rubrum produces 5-methylthioadenosine (MTA) from S-adenosylmethionine in polyamine biosynthesis; however, R. rubrum lacks the classical methionine salvage pathway. Instead, MTA is converted to 5-methylthio-d-ribose 1-phosphate (MTR 1-P) and adenine; MTR 1-P is isomerized to 1-methylthio-d-xylulose 5-phosphate (MTXu 5-P) and reductively dethiomethylated to 1-deoxy-d-xylulose 5-phosphate (DXP), an intermediate in the nonmevalonate isoprenoid pathway [Erb, T. J., et al. (2012) Nat. Chem. Biol., in press]. Dethiomethylation, a novel route to DXP, is catalyzed by MTXu 5-P methylsulfurylase. An active site Cys displaces the enolate of DXP from MTXu 5-P, generating a methyl disulfide intermediate.

Published

2012

49. Cross-species complementation reveals conserved functions for EARLY FLOWERING 3 between monocots and dicots

Author

Todd C. Mockler, John Gierer, Michael J. Naldrett, Sophie Alvarez, Rebecca K. Bindbeutel, He Huang, Ellen L. Gruebbling, Malia A. Gehan, Bradley S. Evans, Sarah E. Huss, Dmitri A. Nusinow, and Cesar Lizarraga

Subjects

0106 biological sciences, 0301 basic medicine, Setaria, growth, Circadian clock, Plant Science, Biology, 01 natural sciences, Biochemistry, Genetics and Molecular Biology (miscellaneous), circadian RNA‐seq, 03 medical and health sciences, Arabidopsis, circadian clock, Botany, Arabidopsis thaliana, Gene, Ecology, Evolution, Behavior and Systematics, Original Research, 030304 developmental biology, Genetics, flowering, 0303 health sciences, Ecology, Setaria viridis, fungi, food and beverages, biology.organism_classification, Phenotype, ELF3, Complementation, CLOCK, 030104 developmental biology, Brachypodium, Brachypodium distachyon, Function (biology), 010606 plant biology & botany

Abstract

Plant responses to the environment are shaped by external stimuli and internal signaling pathways. In both the model plant Arabidopsis thaliana and crop species, circadian clock factors have been identified as critical for growth, flowering and circadian rhythms. Outside of A. thaliana, however, little is known about the molecular function of clock genes. Therefore, we sought to compare the function of Brachypodium distachyon and Seteria viridis orthologs of EARLY FLOWERING3, a key clock gene in A. thaliana. To identify both cycling genes and putative ELF3 functional orthologs in S. viridis, a circadian RNA-seq dataset and online query tool (Diel Explorer) was generated as a community resource to explore expression profiles of Setaria genes under constant conditions after photo- or thermo-entrainment. The function of ELF3 orthologs from A. thaliana, B. distachyon, and S. viridis were tested for complementation of an elf3 mutation in A. thaliana. Despite comparably low sequence identity versus AtELF3 (less than 37%), both monocot orthologs were capable of rescuing hypocotyl elongation, flowering time and arrhythmic clock phenotypes. Molecular analysis using affinity purification and mass spectrometry to compare physical interactions also found that BdELF3 and SvELF3 could be integrated into similar complexes and networks as AtELF3, including forming a composite evening complex. Thus, we find that, despite 180 million years of separation, BdELF3 and SvELF3 can functionally complement loss of ELF3 at the molecular and physiological level.One Sentence SummaryOrthologs of a key circadian clock component ELF3 from grasses functionally complement the Arabidopsis counterpart at the molecular and physiological level, in spite of high sequence divergence.

Published

2017

50. To Cyclize or Not To Cyclize: Catching Enzyme Evolution in the Act

Author

Neil L. Kelleher and Bradley S. Evans

Subjects

Biochemistry, Molecular Medicine, General Medicine, Biochemical engineering, Microbial genome, Biology

Abstract

If you look at the biggest genes in soil and marine bacteria, you tend to see the chemical blueprints for making natural products such as peptides and polyketides. Over the past decade, collective efforts of enzymologists working with synthetic and analytical chemists have been catching up with the data dump from microbial genome sequencing. Following this story line, we now understand how cyanobacteria construct scaffolds for the related natural products curacin and jamaicamide using subtle tweaks to non-standard biosynthetic machinery.

Published

2009