Your search keyword '"FUCOSE"' showing total 9,939 results

1. Head and neck cancer N-glycome traits are cell line and HPV status–dependent

Author

Mohammad Rasheduzzaman, Abarna V. M. Murugan, Xi Zhang, Tiago Oliveira, Riccardo Dolcetti, Liz Kenny, Newell W. Johnson, Daniel Kolarich, and Chamindie Punyadeera

Subjects

Squamous Cell Carcinoma of Head and Neck, Polysaccharides, Head and Neck Neoplasms, Papillomavirus Infections, Humans, Glycomics, Biochemistry, Fucose, Cell Line, Analytical Chemistry

Abstract

Glycosylation is the most common post-translational modification of proteins, and glycosylation changes at cell surfaces are frequently associated with malignant epithelia including head and neck squamous cell carcinoma (HNSCC). In HNSCC, 5-year survival remains poor, averaging around 50% globally: this is partly related to late diagnosis. Specific protein glycosylation signatures on malignant keratinocytes have promise as diagnostic and prognostic biomarkers and as therapeutic targets. Nevertheless, HNSCC-specific glycome is to date largely unknown. Herein, we tested six established HNSCC cell lines to capture the qualitative and semi-quantitative N-glycome using porous graphitized carbon liquid chromatography coupled to electrospray ionisation tandem mass spectrometry. Oligomannose-type N-glycans were the predominant features in all HNSCC cell lines analysed (57.5–70%). The levels of sialylated N-glycans showed considerable cell line-dependent differences ranging from 24 to 35%. Importantly, α2-6 linked sialylated N-glycans were dominant across most HNSCC cell lines except in SCC-9 cells where similar levels of α2-6 and α2-3 sialylated N-glycans were observed. Furthermore, we found that HPV-positive cell lines contained higher levels of phosphorylated oligomannose N-glycans, which hint towards an upregulation of lysosomal pathways. Almost all fucose-type N-glycans carried core-fucose residues with just minor levels (

Published

2022

2. Chemical Synthesis of the Nonreducing Hexasaccharide Fragment of Axinelloside A Based on a Stepwise Glycosylation Approach

Author

Su-Jia Li, Qing Fang, Ying-Wen Huang, Yi-Yang Luo, Xiao-Dong Mu, Ling Li, Xiao-Chen Yin, and Jin-Song Yang

Subjects

Lipopolysaccharides, Glycosylation, Organic Chemistry, Oligosaccharides, Glycosides, Physical and Theoretical Chemistry, Biochemistry, Fucose

Abstract

An expedient synthesis of the nonreducing hexasaccharide fragment of axinelloside A has been completed via a linear stepwise glycosylation approach. Challenges involved in the synthesis include the highly stereoselective construction of five consecutive 1,2-icis/i-glycosidic linkages and the formation of a sterically crowded 2,3-disubstituted l-fucoside subunit. Protecting group-directing glycosylation strategies such as the remote participation effect of the benzoyl substituent and the stereocontrolling effect of the 4,6-iO/i-benzylidene group were employed for the synthesis of the desired 1,2-icis/i-glycosidic linkages. Moreover, the 2,3-branched l-fucoside framework was established through a 3-iO/iand then 2-iO/iglycosylation sequence in which the 3-hydroxyl group of the core l-fucose unit was glycosylated first and then the 2-hydroxyl. The synthetic hexasaccharide is properly protected, so it can be employed as a precursor to synthesize its natural form.

Published

2022

3. Strategies for Enhancing Microbial Production of 2′-Fucosyllactose, the Most Abundant Human Milk Oligosaccharide

Author

Yuanlin Liu, Yingying Zhu, Hao Wang, Li Wan, Wenli Zhang, and Wanmeng Mu

Subjects

Prebiotics, Milk, Human, Guanosine Diphosphate Fucose, Humans, Oligosaccharides, Lactose, General Chemistry, Fucosyltransferases, General Agricultural and Biological Sciences, Trisaccharides, Fucose

Abstract

Human milk oligosaccharides (HMOs), a group of structurally diverse unconjugated glycans in breast milk, act as important prebiotics and have plenty of unique health effects for growing infants. 2'-Fucosyllactose (2'-FL) is the most abundant HMO, accounting for approximately 30%, among approximately 200 identified HMOs with different structures. 2'-FL can be enzymatically produced by α1,2-fucosyltransferase, using GDP-l-fucose as donor and lactose as acceptor. Metabolic engineering strategies have been widely used for enhancement of GDP-l-fucose supply and microbial production of 2'-FL with high productivity. GDP-l-fucose supply can be enhanced by two main pathways, including

Published

2022

4. Sargassum fusiforme fucoidan ameliorates diet-induced obesity through enhancing thermogenesis of adipose tissues and modulating gut microbiota

Author

Jihui, Zuo, Ya, Zhang, Yu, Wu, Jian, Liu, Qifang, Wu, Yizhe, Shen, Li, Jin, Mingjiang, Wu, Zengling, Ma, and Haibin, Tong

Subjects

Sargassum, Thermogenesis, General Medicine, Diet, High-Fat, Biochemistry, Gastrointestinal Microbiome, Mice, Inbred C57BL, Mice, Polysaccharides, Structural Biology, Animals, Female, Obesity, Molecular Biology, Fucose

Abstract

Obesity has become a global epidemic. Sargassum fusiforme fucoidan (Fuc) is a group of water-soluble heteropolysaccharides that exhibits a wide range of medicinal functions. It consists of l-fucose and sulfate groups, with l-fucose as the main monosaccharide. This study investigated the therapeutic effects of Fuc on diet-induced obesity (DIO) in C57BL/6J female mice. Fuc significantly alleviated obesity in mice induced by high-fat high-fructose (HFHF) feeding, inhibiting body weight gain, reducing fat accumulation, and improving hepatic steatosis. In addition, Fuc significantly improved glucose tolerance and insulin sensitivity by enhancing the phosphorylation level of AKT (at Ser473) in the adipose tissues. Mechanistically, although Fuc did not decrease the energy intake in DIO mice, it significantly increased the energy expenditure by up-regulating the expression of uncoupling protein 1 (UCP1) in the adipose tissues. Notably, Fuc also improved the obesity-driven dysbiosis of gut microbiota and decreased the relative abundance of the obesity-related intestinal bacteria. However, Fuc was unable to alleviate DIO-induced metabolic disorders in pseudo-sterile mice. Our findings suggested that Fuc might remodel gut microbiota and exert its weight loss and hypolipidemic effects by increasing the energy expenditure, thus providing a novel perspective for treating obesity and related complications.

Published

2022

5. Structure of a unique fucose-containing exopolysaccharide from Sayram ketteki yoghurt and its anti-MRSA biofilm effect

Author

Zhiwen, Ge, Xiaohong, Chen, Renqin, Yang, Wei, Li, Baixing, Yin, Zhiyu, Li, and Mingsheng, Dong

Subjects

Methicillin-Resistant Staphylococcus aureus, Structural Biology, Biofilms, Spectroscopy, Fourier Transform Infrared, Microbial Sensitivity Tests, General Medicine, Yogurt, Molecular Biology, Biochemistry, Anti-Bacterial Agents, Fucose

Abstract

In this work, we reported an in situ exopolysaccharide (in situ-EPS1) containing rare fucose produced by Lactobacillus helveticus MB2-1 in Sayram ketteki yoghurt, which made it unique. Its fine structure was characterized by GPC, HPLC, FT-IR, GC-MS

Published

2022

6. Monosaccharide profiling of glycoproteins by capillary electrophoresis with contactless conductivity detection

Author

Alice Tomnikova, Petr Kozlík, and Tomáš Křížek

Subjects

Acetylgalactosamine, Xylose, Cetrimonium, Monosaccharides, Clinical Biochemistry, Electrophoresis, Capillary, Galactose, Biochemistry, N-Acetylneuraminic Acid, Acetylglucosamine, Phosphates, Analytical Chemistry, Electrolytes, Glucose, Tandem Mass Spectrometry, Sodium Hydroxide, Fetuins, Mannose, Chromatography, Liquid, Fucose, Glycoproteins

Abstract

Saccharides form one of the major constituents of biological macromolecules in living organisms. Many biological processes including protein folding, stability, immune response and receptor activation are regulated by glycosylation. In this work, we optimized a capillary electrophoresis method with capacitively coupled contactless conductivity detection for the separation of eight monosaccharides commonly found in glycoproteins, namely D-glucose, D-galactose, D-mannose, N-acetyl-D-glucosamine, N-acetyl-D-galactosamine, D-fucose, N-acetylneuraminic acid, and D-xylose. A highly alkaline solution of 50 mM sodium hydroxide, 22.5 mM disodium phosphate, and 0.2 mM CTAB (pH 12.4) was used as a background electrolyte in a 10 µm id capillary. To achieve baseline separation of all analytes, a counter-directional pressure of -270 kPa was applied during the separation. The limits of detection of our method were below 7 µg/ml (i.e., 1.5 pg or 1 mg/g protein) and the limits of quantification were below 22 µg/ml (i.e., 5 pg or 3 mg/g protein). As a proof of concept of our methodology, we performed an analysis of monosaccharides released from fetuin glycoprotein by acid hydrolysis. The results show that, when combined with an appropriate pre-concentration technique, the developed method can be used as a monosaccharide profiling tool in glycoproteomics and complement the routinely used LC-MS/MS analysis.

Published

2022

7. Sialic Acid and Fucose Residues on the SARS-CoV-2 Receptor-Binding Domain Modulate IgG Antibody Reactivity

Author

Ebba Samuelsson, Ekaterina Mirgorodskaya, Kristina Nyström, Malin Bäckström, Jan-Åke Liljeqvist, and Rickard Nordén

Subjects

Cricetulus, Infectious Diseases, SARS-CoV-2, Cricetinae, Immunoglobulin G, Spike Glycoprotein, Coronavirus, Animals, COVID-19, Humans, CHO Cells, Antibodies, Viral, N-Acetylneuraminic Acid, Fucose

Abstract

The receptor-binding domain (RBD) of the SARS-CoV-2 spike protein is a conserved domain and a target for neutralizing antibodies. We defined the carbohydrate content of the recombinant RBD produced in different mammalian cells. We found a higher degree of complex-type N-linked glycans, with less sialylation and more fucosylation, when the RBD was produced in human embryonic kidney cells compared to the same protein produced in Chinese hamster ovary cells. The carbohydrates on the RBD proteins were enzymatically modulated, and the effect on antibody reactivity was evaluated with serum samples from SARS-CoV-2 positive patients. Removal of all carbohydrates diminished antibody reactivity, while removal of only sialic acids or terminal fucoses improved the reactivity. The RBD produced in Lec3.2.8.1-cells, which generate carbohydrate structures devoid of sialic acids and with reduced fucose content, exhibited enhanced antibody reactivity, verifying the importance of these specific monosaccharides. The results can be of importance for the design of future vaccine candidates, indicating that it is possible to enhance the immunogenicity of recombinant viral proteins.

Published

2022

8. Biochemical and Biophysical Characterization of Carbonic Anhydrase VI from Human Milk and Saliva

Author

Alma Yrjänäinen, Maarit S. Patrikainen, Latifeh Azizi, Martti E. E. Tolvanen, Mikko Laitaoja, Janne Jänis, Vesa P. Hytönen, Alessio Nocentini, Claudiu T. Supuran, Seppo Parkkila, Tampere University, BioMediTech, and Department of Clinical Chemistry

Subjects

Milk, Human, Organic Chemistry, Humans, Bioengineering, 3111 Biomedicine, Saliva, Biochemistry, Carbonic Anhydrases, Fucose, Analytical Chemistry

Abstract

Carbonic anhydrases (CA, EC 4.2.1.1) catalyze the hydration of carbon dioxide and take part in many essential physiological processes. In humans, 15 CAs are characterized, including the only secreted isoenzyme CA VI. CA VI has been linked to specific processes in the mouth, namely bitter taste perception, dental caries, and maintenance of enamel pellicle, and implicated in several immunity-related phenomena. However, little is known of the mechanisms of the above. In this study, we characterized human CA VI purified from saliva and milk with biophysical methods and measured their enzyme activities and acetazolamide inhibition. Size-exclusion chromatography showed peaks of salivary and milk CA VI corresponding to hexameric state or larger at pH 7.5. At pH 5.0 the hexamer peaks dominated. SDS- PAGE of milk CA VI protein treated with a bifunctional crosslinker further confirmed that a majority of CA VI is oligomers of similar sizes in solution. Mass spectrometry experiments confirmed that both of the two putative N-glycosylation sites, Asn67 and Asn256, are heterogeneously glycosylated. The attached glycans in milk CA VI were di- and triantennary complex-type glycans, carrying both a core fucose and 1 to 2 additional fucose units, whereas the glycans in salivary CA VI were smaller, seemingly degraded forms of core fucosylated complex- or hybrid-type glycans. Mass spectrometry also verified the predicted signal peptide cleavage site and the terminal residue, Gln 18, being in pyroglutamate form. Thorough characterization of CA VI paves way to better understanding of the biological function of the protein.

Published

2022

9. Fucose Binding Motifs on Mucin Core Glycopeptides Impact Bacterial Lectin Recognition**

Author

Sandra Behren, Jin Yu, Christian Pett, Manuel Schorlemer, Viktoria Heine, Thomas Fischöder, Lothar Elling, and Ulrika Westerlind

Subjects

Glycosylation, Microarrays, Lectins, Glycopeptides, Biochemistry and Molecular Biology, General Chemistry, General Medicine, Biokemi och molekylärbiologi, Catalysis, Fucose

Abstract

Mucin glycoproteins are essential components of the mucosal barrier, which protects the host from pathogens. Throughout evolution, bacteria have developed strategies to modulate and penetrate this barrier, and cause virulence by interacting with mucin O-glycans at the epithelial cell-surface. O-fucosylated glycan epitopes on mucins are key ligands of many bacterial lectins. Here, a chemoenzymatic synthesis strategy is described to prepare a library of fucosylated mucin core glycopeptides to enable studies of mucin-interacting and fucose-binding bacterial lectins. Glycan cores with biologically important Lewis and H-antigens were prepared decorating the peptide backbone at different sites and densities. The fucosylated mucin glycopeptides were applied in microarray binding studies to explore the importance of glycan core and peptide backbone presentation of these antigens in binding interactions with the P. aeruginosa lectin LecB and the C. difficile toxin A.

Published

2023

10. In Silico and In Vitro Investigation of the Distribution and Expression of Key Genes in the Fucose Operon of Escherichia coli

Author

Nehal A. Saif, Yomna A. Hashem, Heba M. Amin, and Ramy K. Aziz

Subjects

Microbiology (medical), Virology, E. coli, fucose, comparative genomic analysis, real-time PCR, subsystem, SEED, Microbiology

Abstract

Many gut bacteria degrade polysaccharides, providing nutritional advantages to their hosts. Fucose, a mucin degradation product, was suggested as a communication molecule between the resident microbiota and external pathogens. However, the precise role and variants of the fucose utilization pathway remain to be elucidated. Here, we computationally and experimentally investigated the fucose utilization operon of E.coli. While the operon is conserved among E.coli genomes, a variant pathway, in which an ABC transporter system replaces the fucose permease gene (fucP), was computationally identified in 50 out of 1058 genomes. Comparative genomics and subsystems analysis results were confirmed by polymerase chain reaction-based screening of 40 human E.coli isolates, which indicated the conservation of fucP in 92.5% of the isolates (vs. 7.5% of its suggested alternative, yjfF). The in silico predictions were confirmed by in vitro experiments comparing the growth of E.coli strains K12, BL21, and isogenic fucose-utilization K12 mutants. Additionally, fucP and fucI transcripts were quantified in E.coli K12 and BL21, after in silico analysis of their expression in 483 public transcriptomes. In conclusion, E.coli utilizes fucose by two pathway variants, with measurable transcriptional differences. Future studies will explore this variation’s impact on signaling and virulence.

Published

2023

11. Multi-omics unravel the compromised mucosal barrier function linked to aberrant mucin O-glycans in a pig model

Author

Bing Xia, Ruqing Zhong, Qingshi Meng, Weida Wu, Liang Chen, Xin Zhao, and Hongfu Zhang

Subjects

Proteome, Polysaccharides, Swine, Structural Biology, Mucins, Animals, General Medicine, Intestinal Mucosa, Molecular Biology, Biochemistry, Fucose

Abstract

Early weaning stress (EWS) in piglets is associated with intestinal dysfunction. Here, utilizing a pig EWS model to mimic early-life stress (ELS) in humans, we investigated the mechanism of ELS-induced intestinal diseases through integrated multi-omics analyses of proteome, glycome, and microbiome. Our results demonstrated that EWS resulted in disrupted the ileal barrier integrity by reducing tight junction-related gene expression and interfering with cell-cell adhesion paralleled the increased proportion of pathogens such as Escherichia_Shigella and Helicobacter. Furthermore, Proteome data revealed that the accumulation of unfolded proteins and insufficient unfolded protein response (UPR) process caused by EWS led to ER stress. Data from proteome and glycome found that EWS induced aberrant mucin O-glycans, including truncated glycans, reduction in acidic glycans, and increased in fucosylated glycans. In addition, correlation test by taking fucose and inflammatory response into account suggested that enhancement of fucose expression might be a compensatory host response. Taken together, these results extend the comprehensive knowledge of the detrimental impacts and pathogenesis of EWS and help to provide intervention targets for ELS-induced intestinal diseases in the future.

Published

2022

12. Characterization of the response of Escherichia coli to <scp>l</scp> ‐fucose in bacterial swimming motility

Author

Jingyun Li, Juan Chen, Lu Wang, Yan Lin, Xian Zhang, Jian Liu, and Fangbin Wang

Subjects

Bacterial Proteins, Flagella, Escherichia coli, General Medicine, Applied Microbiology and Biotechnology, Bacterial Adhesion, Swimming, Fucose

Abstract

l-Fucose, as a monosaccharide in nature, plays a crucial role in bacteria colonization. Escherichia coli (E. coli), as a common microorganism in environment, utilize bacterial flagellar motor to drive the rotation of flagella, which is regulated by chemotactic signal transduction signals. Yet the effect of l-fucose to bacterial motility remains unclear. The effect of l-fucose on the swimming motility of bacteria was investigated from the level of single flagellar motor to individual cell and cell population by employing a bead assay, a high-throughput 2D tracking assay and a high-throughput dark-field flicker microscopy. The results showed that the swimming motility of the bacteria cultured with l-fucose was decreased, while the tumble frequency increased. Furthermore, the behavioral alterations of bacteria affected by l-fucose were directly reveled by measuring the cell distribution of bacteria swimming near surfaces and bacterial surface adhesion, suggesting that l-fucose promotes bacterial surface aggregation and surface adhesion. The effect of l-fucose on bacterial swimming motility characterized in this study are consistent with the key role that l-fucose plays in bacterial colonization.

Published

2022

13. Structural characteristics and immune-enhancing activity of fractionated polysaccharides from Athyrium Multidentatum (Doll.) Ching

Author

Yang, Wang, Xiaoyan, Shen, Kaiyue, Yin, Changqing, Miao, Yanlong, Sun, Shumei, Mao, Dongmei, Liu, and Jiwen, Sheng

Subjects

Mice, RAW 264.7 Cells, Polysaccharides, Structural Biology, Animals, Galactose, General Medicine, Arabinose, Mannose, Molecular Biology, Biochemistry, Fucose

Abstract

Polysaccharides coded as CP were extracted from Athyrium Multidentatum (Doll.) Ching and then fractionated into five fractions (FP-1, FP-2, FP-3, FP-4 and FP-5). A purified polysaccharide designated as FP-3-4 was prepared from FP-3 by Sephadex G-100 column chromatography. Chemical analysis disclosed that CP and these fractions were heteropolysaccharides and mainly composed of glucose, galactose, arabinose, mannose, rhamnose, xylose, fucose, ribose and uronic acid with different molar ratios. They presented different images of SEM. FP-3-4 was highly branched polymers with sixteen types of linkages. The in vitro immunomodulatory results stated that CP and these fractions could promote macrophage proliferation, enhance macrophage phagocytosis and increase the production of NO, TNF-α, IFN-γ, IL-1β, IL-6, IL-10 and IL-2, indicating remarkable immune enhancement activities. RNA sequencing analysis revealed that CP and FP-3 induced macrophage activation mainly through MAPK and alternative NF-κΒ signaling pathways via CD14/TLR4 and Dectin-2 receptors, which were verified by RT-qPCR and western blot.

Published

2022

14. Role of Mucin 2 Glycoprotein and L-fucose in Interaction of Immunity and Microbiome within the Experimental Model of Inflammatory Bowel Disease

Author

Victoria D. Bets, Kseniya M. Achasova, Mariya A. Borisova, Elena N. Kozhevnikova, and Ekaterina A. Litvinova

Subjects

Mice, Knockout, Mucin-2, Bacteria, Microbiota, Forkhead Transcription Factors, General Medicine, Models, Theoretical, Inflammatory Bowel Diseases, Biochemistry, Anti-Bacterial Agents, Mice, Animals, Intestinal Mucosa, Fucose

Abstract

Many factors underlie the development of inflammatory bowel disease (IBD) in humans. In particular, imbalance of microbiota and thinning of the mucosal layer in the large intestine play a huge role. Pathogenic microorganisms also exacerbate the course of diseases. In this research the role of mucin 2 deficiency in the formation of intestinal microflora in the experimental model using the Muc2 gene knockout mice in the presence of Helicobacter spp. was investigated. Also, restorative and anti-inflammatory effect of the dietary L-fucose in the Muc2

Published

2022

15. Structure–function relationship of a novel fucoside-binding fruiting body lectin from Coprinopsis cinerea exhibiting nematotoxic activity

Author

Silvia Bleuler-Martinez, Annabelle Varrot, Vincent Olieric, Mario Schubert, Eva Vogt, Céline Fetz, Therese Wohlschlager, David Fernando Plaza, Martin Wälti, Yannick Duport, Guido Capitani, Markus Aebi, and Markus Künzler

Subjects

Binding Sites, nematode, defense, fucose, mushroom, toxin, Carbohydrates, Crystallography, X-Ray, Biochemistry, Fungal Proteins, Structure-Activity Relationship, X-Ray Diffraction, Lectins, Scattering, Small Angle, Animals, Agaricales, Caenorhabditis elegans

Abstract

Lectins are non-immunoglobulin-type proteins that bind to specific carbohydrate epitopes and play important roles in intra- and inter-organismic interactions. Here, we describe a novel fucose-specific lectin, termed CML1, which we identified from fruiting body extracts of Coprinopsis cinerea. For further characterization, the coding sequence for CML1 was cloned and heterologously expressed in Escherichia coli. Feeding of CML1-producing bacteria inhibited larval development of the bacterivorous nematode Caenorhabditis tropicalis, but not of C. elegans. The crystal structure of the recombinant protein in its apo-form and in complex with H type I or Lewis A blood group antigens was determined by X-ray crystallography. The protein folds as a sandwich of 2 antiparallel β-sheets and forms hexamers resulting from a trimer of dimers. The hexameric arrangement was confirmed by small-angle X-ray scattering (SAXS). One carbohydrate-binding site per protomer was found at the dimer interface with both protomers contributing to ligand binding, resulting in a hexavalent lectin. In terms of lectin activity of recombinant CML1, substitution of the carbohydrate-interacting residues His54, Asn55, Trp94, and Arg114 by Ala abolished carbohydrate-binding and nematotoxicity. Although no similarities to any characterized lectin were found, sequence alignments identified many non-characterized agaricomycete proteins. These results suggest that CML1 is the founding member of a novel family of fucoside-binding lectins involved in the defense of agaricomycete fruiting bodies against predation by fungivorous nematodes., Glycobiology, 32 (7), ISSN:0959-6658

Published

2022

16. A Cross-Sectional Assessment of Human Milk Oligosaccharide Composition of Vegan, Vegetarian, and Nonvegetarian Mothers

Author

Jessica Neville, Roman Pawlak, Melinda Chang, Annalee Furst, Lars Bode, and Maryanne T. Perrin

Subjects

Vegans, Milk, Human, Health Policy, Mothers, Oligosaccharides, Obstetrics and Gynecology, Pediatrics, Breast Feeding, Cross-Sectional Studies, Pregnancy, Maternity and Midwifery, Humans, Lactation, Female, Fucose, Vegetarians

Published

2022

17. Chemo-enzymatic synthesis and analysis of isomeric glycans

Author

Vos, Gael Martijn, Faculteit Betawetenschappen, Boons, Geert-Jan, and de Vries, Robert

Subjects

glycaan, glycan, ion-mobility, I-branch, ionmobiliteit, I-vertakking, chemo-enzymatische synthese, O-gllycaan, O-glycan, fucose, hypochlorite, isomeren, humane melksaccharide, bloodgroup antigen, human milk oligosaccharide, isomers, hypochloriet, bloedgroepantigeen, chemo-enzymatic synthesis

Abstract

Glycans, also known as carbohydrates, are an essential component of all living organisms and are, among other things, present on proteins and lipids in the cellular membrane. Glycan structure is not encoded in the genome, oppose to other biopolymers such as RNA and proteins, but is regulated by around 200 glycosyltransferase enzymes. As a result of substrate competition, glycans are generated that vary in composition, linkage positions and configurations. The large heterogeineity and diversity in glycan structure complicates the synthesis and characterization of glycans. The research described in this dissertation covers the synthesis of well-defined glycans and applies synthetic glycans in the development of analytical methodology for the detailed structural characterization of naturally occuring glycans. Chemically modified glycans are synthesized by employing glycosyltransferase enzymes. These modifications are manipulated to (de)activate certain positions on a glycan and thereby direct glycosyltransferase activity. Traceless removal of these modifications allows the synthesis of complex natural glycans with controlled architecture. These glycans are used to study differences in biological activity between isomeric glycans. Synthetic glycopeptides with various functionalities are used as model substrates to develop a method to release glycans from glycopeptides without damaging the glycan structure itself. This methodology conserves labile glycan modifications that are often lost in glycan analysis. Furthermore, synthetic complex glycans are applied as reference compounds for the development of analytical methodology that can structurally elucidate challenging glycan epitopes.

Published

2023

18. Chemo-enzymatic synthesis and analysis of isomeric glycans

Author

Vos, Gael Martijn, Faculteit Betawetenschappen, Boons, Geert-Jan, de Vries, Robert, and University Utrecht

Subjects

glycaan, glycan, ion-mobility, I-branch, ionmobiliteit, I-vertakking, chemo-enzymatische synthese, O-gllycaan, O-glycan, fucose, hypochlorite, isomeren, humane melksaccharide, bloodgroup antigen, human milk oligosaccharide, isomers, hypochloriet, bloedgroepantigeen, chemo-enzymatic synthesis

Abstract

Glycans, also known as carbohydrates, are an essential component of all living organisms and are, among other things, present on proteins and lipids in the cellular membrane. Glycan structure is not encoded in the genome, oppose to other biopolymers such as RNA and proteins, but is regulated by around 200 glycosyltransferase enzymes. As a result of substrate competition, glycans are generated that vary in composition, linkage positions and configurations. The large heterogeineity and diversity in glycan structure complicates the synthesis and characterization of glycans. The research described in this dissertation covers the synthesis of well-defined glycans and applies synthetic glycans in the development of analytical methodology for the detailed structural characterization of naturally occuring glycans. Chemically modified glycans are synthesized by employing glycosyltransferase enzymes. These modifications are manipulated to (de)activate certain positions on a glycan and thereby direct glycosyltransferase activity. Traceless removal of these modifications allows the synthesis of complex natural glycans with controlled architecture. These glycans are used to study differences in biological activity between isomeric glycans. Synthetic glycopeptides with various functionalities are used as model substrates to develop a method to release glycans from glycopeptides without damaging the glycan structure itself. This methodology conserves labile glycan modifications that are often lost in glycan analysis. Furthermore, synthetic complex glycans are applied as reference compounds for the development of analytical methodology that can structurally elucidate challenging glycan epitopes.

Published

2023

19. Chemo-enzymatic synthesis and analysis of isomeric glycans

Subjects

glycaan, glycan, ion-mobility, I-branch, ionmobiliteit, I-vertakking, chemo-enzymatische synthese, O-gllycaan, O-glycan, fucose, hypochlorite, isomeren, humane melksaccharide, bloodgroup antigen, human milk oligosaccharide, isomers, hypochloriet, bloedgroepantigeen, chemo-enzymatic synthesis

Abstract

Glycans, also known as carbohydrates, are an essential component of all living organisms and are, among other things, present on proteins and lipids in the cellular membrane. Glycan structure is not encoded in the genome, oppose to other biopolymers such as RNA and proteins, but is regulated by around 200 glycosyltransferase enzymes. As a result of substrate competition, glycans are generated that vary in composition, linkage positions and configurations. The large heterogeineity and diversity in glycan structure complicates the synthesis and characterization of glycans. The research described in this dissertation covers the synthesis of well-defined glycans and applies synthetic glycans in the development of analytical methodology for the detailed structural characterization of naturally occuring glycans. Chemically modified glycans are synthesized by employing glycosyltransferase enzymes. These modifications are manipulated to (de)activate certain positions on a glycan and thereby direct glycosyltransferase activity. Traceless removal of these modifications allows the synthesis of complex natural glycans with controlled architecture. These glycans are used to study differences in biological activity between isomeric glycans. Synthetic glycopeptides with various functionalities are used as model substrates to develop a method to release glycans from glycopeptides without damaging the glycan structure itself. This methodology conserves labile glycan modifications that are often lost in glycan analysis. Furthermore, synthetic complex glycans are applied as reference compounds for the development of analytical methodology that can structurally elucidate challenging glycan epitopes.

Published

2023

20. Synthesis and Application of Rare Deoxy Amino l-Sugar Analogues to Probe Glycans in Pathogenic Bacteria

Author

Phuong Luong, Antara Ghosh, Karen D. Moulton, Suvarn S. Kulkarni, and Danielle H. Dube

Subjects

Azides, Infectious Diseases, Bacteria, Polysaccharides, Bacterial, Humans, Sugars, Article, Fucose

Abstract

Bacterial cell envelope glycans are compelling antibiotic targets as they are critical for strain fitness and pathogenesis yet are virtually absent from human cells. However, systematic study and perturbation of bacterial glycans remains challenging due to their utilization of rare deoxy amino l-sugars, which impede traditional glycan analysis and are not readily available from natural sources. The development of chemical tools to study bacterial glycans is a crucial step toward understanding and altering these biomolecules. Here we report an expedient methodology to access azide-containing analogues of a variety of unusual deoxy amino l-sugars starting from readily available l-rhamnose and l-fucose. Azide-containing l-sugar analogues facilitated metabolic profiling of bacterial glycans in a range of Gram-negative bacteria and revealed differential utilization of l-sugars in symbiotic versus pathogenic bacteria. Further application of these probes will refine our knowledge of the glycan repertoire in diverse bacteria and aid in the design of novel antibiotics.

Published

2023

21. Pathogenic investigations of Streptococcus pasteurianus , an underreported zoonotic pathogen, isolated from a diseased piglet with meningitis

Author

Shuoyue Wang, Miaohang Ma, Zijing Liang, Xinchi Zhu, Huochun Yao, Liping Wang, and Zongfu Wu

Subjects

Swine Diseases, Mice, Inbred ICR, Streptococcus suis, General Veterinary, General Immunology and Microbiology, Swine, Virulence Factors, Clindamycin, Streptococcus, General Medicine, Erythromycin, Rodent Diseases, Mice, Doxycycline, Streptococcal Infections, Animals, Humans, Meningitis, Gentamicins, Fucose

Abstract

Streptococcus pasteurianus, an underreported opportunistic pathogen, is considered an increasingly recognized cause of meningitis and bacteremia in many animals and humans worldwide. However, except for some epidemiological studies, there is no report about the gene-deletion mutagenesis, virulence factors, reservoir niches or animal infection models for this pathogen. In this study, we first isolated an S. pasteurianus strain from a newly weaned piglet's brain with meningitis. The genomic sequence of this swine isolate WUSP067 shared high homology with that of two human strains. The comparative genome analysis showed that strain WUSP067 contained a fucose utilization cluster absent in human strains, and it shared 91% identity with that of an integrative and conjugative element (ICE) ICE

Published

2021

22. Tobramycin-loaded complexes to prevent and disrupt Pseudomonas aeruginosa biofilms

Author

Manuel Romero, Shaun Robertson, Greta Avancini, Francesca Mastrotto, Giuseppe Mantovani, Federica Sandrelli, Delia Boffoli, Miguel Cámara, Pratik Gurnani, Gokhan Yilmaz, Federica Bellato, Francesca Moret, Paolo Caliceti, and Stefano Salmaso

Subjects

Biofilm, Complexes, Lectins, Pseudomonas aeruginosa, Synthetic glycopolymers, Tobramycin, Pharmaceutical Science, Mannose, medicine.disease_cause, Fucose, chemistry.chemical_compound, medicine, Humans, Chemistry, Aminoglycoside, Combinatorial chemistry, Anti-Bacterial Agents, Bacterial adhesin, Targeted drug delivery, Biofilms, medicine.drug

Abstract

Carbohydrate-based materials are increasingly investigated for a range of applications spanning from healthcare to advanced functional materials. Synthetic glycopolymers are particularly attractive as they possess low toxicity and immunogenicity and can be used as multivalent ligands to target sugar-binding proteins (lectins). Here, we utilised RAFT polymerisation to synthesize two families of novel diblock copolymers consisting of a glycopolymers block containing either mannopyranose or galactopyranose pendant units, which was elongated with sodium 2-acrylamido-2-methyl-1-propanesulfonate (AMPS) to generate a polyanionic block. The latter enabled complexation of cationic aminoglycoside antibiotic tobramycin through electrostatic interactions (loading efficiency in the 0.5-6.3 wt% range, depending on the copolymer). The resulting drug vectors were characterized by dynamic light scattering, zeta-potential, and transmission electron microscopy. Tobramycin-loaded complexes were tested for their ability to prevent clustering or disrupt biofilm of the Pseudomonas aeruginosa Gram-negative bacterium responsible for a large proportion of nosocomial infection, especially in immunocompromised patients. P. aeruginosa possesses two specific tetrameric carbohydrate-binding adhesins, LecA (PA-IL, galactose/N-acetyl-D-galactosamine-binding) and LecB (PA-IIL, fucose/mannose-binding), and the cell-associated and extracellular adhesin CdrA (Psl/mannose-binding) thus ideally suited for targeted drug delivery using sugar-decorated tobramycin-loaded complexes here developed. Both aliphatic and aromatic linkers were utilised to link the sugar pendant units to the polyacrylamide polymer backbone to assess the effect of the nature of such linkers on bactericidal/bacteriostatic properties of the complexes. Results showed that tobramycin-loaded complexes efficiently suppressed (40 to 60% of inhibition) in vitro biofilm formation in PAO1-L P. aeruginosa and that preferential targeting of PAO1-L biofilm can be achieved using mannosylated glycopolymer-b-AMPSm.

Published

2021

23. The structure–activity mechanism of the changes in the physicochemical properties of <scp> Flammulina velutipes </scp> polysaccharides during ultrasonic extraction

Author

Liyan Zhao, Jinrong Xiao, Benard Muinde Kimatu, Xin Chen, Qiuhui Hu, and Huihua Zheng

Subjects

Nutrition and Dietetics, Chromatography, Chemistry, Extraction (chemistry), Galactose, Fucose, Viscosity, chemistry.chemical_compound, Rheology, Polysaccharides, Zeta potential, Ultrasonics, Thermal stability, Ultrasonic sensor, Particle size, Agronomy and Crop Science, Flammulina, Food Science, Biotechnology

Abstract

BACKGROUND The high yield of ultrasonic extraction has been widely studied. However, the effects of ultrasound on the properties of products has generally been ignored. In this study, the structural characteristics, rheological properties, and thermal stability of Flammulina velutipes polysaccharides (FVPs) under different ultrasonic power (200, 600, 1000 W) and time (10, 20, 30 min) were investigated to explore the effects of ultrasonic extraction on FVPs and the structure-physicochemical properties relationship. The ultrasonic intensity at the corresponding rated power was also measured. RESULTS The results showed that the molecular weight, particle size, and zeta potential of FVPs decreased as the ultrasonic intensity or time increased. The galactose, mannose, and fucose contents were increased, but the glucose content was decreased by ultrasonic extraction. Viscosity and weak gel strength were positively correlated with molecular weight. Thermal degradation enthalpy was positively correlated with the galactose and fucose contents. CONCLUSIONS Ultrasound reduced the viscosity and gel strength of FVPs by breaking the polysaccharide chain and improving the galactose and fucose contents, which improved the thermal stability of FVPs. This work provides a theoretical basis for the development of FVP foods with a clear structure-function relationship, which makes it possible to directionally produce FVPs by adjusting ultrasonic parameters during extraction. © 2021 Society of Chemical Industry.

Published

2021

24. Bacterial lectin BambL acts as a B cell superantigen

Author

Joern Dengjel, Isabel Wilhelm, Sarah Wehrum, Ana Valeria Meléndez, Peter Fritz Müller, Christina Jäger, Marco Frensch, Beate Fischer, Winfried Römer, Annamaria Tadic, Hermann Eibel, and Britta Diedrich

Subjects

Burkholderia, Adaptive immunity, B-cell receptor, Receptors, Antigen, B-Cell, Apoptosis, Multivalent lectins, CD19, Fucose, Cellular and Molecular Neuroscience, chemistry.chemical_compound, Bacterial Proteins, Polysaccharides, Lectins, hemic and lymphatic diseases, medicine, Superantigen, Humans, Molecular Biology, B cell, Pharmacology, CD86, B-Lymphocytes, Binding Sites, Superantigens, biology, Chemistry, CD69, breakpoint cluster region, Cell Biology, Cell biology, medicine.anatomical_structure, biology.protein, Molecular Medicine, Original Article, Bacterial pathogens, Immunoglobulin glycosylation, β-Propeller lectins, Protein Binding, Signal Transduction

Abstract

B cell superantigens crosslink conserved domains of B cell receptors (BCRs) and cause dysregulated, polyclonal B cell activation irrespective of normal BCR-antigen complementarity. The cells typically succumb to activation-induced cell death, which can impede the adaptive immune response and favor infection. In the present study, we demonstrate that the fucose-binding lectin of Burkholderia ambifaria, BambL, bears functional resemblance to B cell superantigens. By engaging surface glycans, the bacterial lectin activated human peripheral blood B cells, which manifested in the surface expression of CD69, CD54 and CD86 but became increasingly cytotoxic at higher concentrations. The effects were sensitive to BCR pathway inhibitors and excess fucose, which corroborates a glycan-driven mode of action. Interactome analyses in a model cell line suggest BambL binds directly to glycans of the BCR and regulatory coreceptors. In vitro, BambL triggered BCR signaling and induced CD19 internalization and degradation. Owing to the lectin’s six binding sites, we propose a BCR activation model in which BambL functions as a clustering hub for receptor glycans, modulates normal BCR regulation, and induces cell death through exhaustive activation. Supplementary Information The online version contains supplementary material available at 10.1007/s00018-021-04009-z.

Published

2021

25. Bisecting Lewis X in Hybrid-Type N-Glycans of Human Brain Revealed by Deep Structural Glycomics

Author

Clemens Grünwald-Gruber, Martin Pabst, Johannes Helm, Johannes Führer, Jonathan Urteil, Daniel Maresch, David Stenitzer, Friedrich Altmann, Andreas Thader, and Laura Neumann

Subjects

0303 health sciences, Glycan, biology, Chemistry, Stereochemistry, 010401 analytical chemistry, Hybrid type, Human brain, 01 natural sciences, Fucose, 0104 chemical sciences, Analytical Chemistry, Glycomics, 03 medical and health sciences, Residue (chemistry), chemistry.chemical_compound, medicine.anatomical_structure, Natural source, medicine, biology.protein, Graphitic carbon, 030304 developmental biology

Abstract

The importance of protein glycosylation in the biomedical field requires methods that not only quantitate structures by their monosaccharide composition, but also resolve and identify the many isomers expressed by mammalian cells. The art of unambiguous identification of isomeric structures in complex mixtures, however, did not yet catch up with the fast pace of advance of high-throughput glycomics. Here, we present a strategy for deducing structures with the help of a deci-minute accurate retention time library for porous graphitic carbon chromatography with mass spectrometric detection. We implemented the concept for the fundamental N-glycan type consisting of five hexoses, four N-acetylhexosamines and one fucose residue. Nearly all of the 40 biosynthetized isomers occupied unique elution positions. This result demonstrates the unique isomer selectivity of porous graphitic carbon. With the help of a rather tightly spaced grid of isotope-labeled internal N-glycan, standard retention times were transposed to a standard chromatogram. Application of this approach to animal and human brain N-glycans immediately identified the majority of structures as being of the bisected type. Most notably, it exposed hybrid-type glycans with galactosylated and even Lewis X containing bisected N-acetylglucosamine, which have not yet been discovered in a natural source. Thus, the time grid approach implemented herein facilitated discovery of the still missing pieces of the N-glycome in our most noble organ and suggests itself─in conjunction with collision induced dissociation─as a starting point for the overdue development of isomer-specific deep structural glycomics.

Published

2021

26. Comparative Characteristics of the Expression of Fucosylated Glycans and Morphometric Parameters of Terminal Placental Villi Depending on the Severity of Preeclampsia

Author

M. M. Ziganshina, G V Kulikova, Shchegolev Ai, and Gennady T. Sukhikh

Subjects

Glycan, Endothelium, General Medicine, Biology, medicine.disease, General Biochemistry, Genetics and Molecular Biology, Fucose, Preeclampsia, carbohydrates (lipids), Andrology, Glycocalyx, chemistry.chemical_compound, medicine.anatomical_structure, Syncytiotrophoblast, chemistry, Placenta, embryonic structures, Correlation analysis, medicine, biology.protein

Abstract

We performed a comparative analysis of the expression of fucosylated glycans and morphometric characteristics of the terminal villi of the placenta, depending on the severity of preeclampsia (PE). Similar patterns of the expression of fucosylated glycans in the syncytiotrophoblast glycocalyx were revealed in the placental tissue of patients with normal pregnancy and with mild and severe PE: predominance of glycans with α1,6-fucose in the core, clustered fucose residues, and LeX glycan over α1,2-fucose-containing glycans. The expression pattern of fucosylated glycans and the composition of the endothelial glycocalyx are normally close to the expression pattern and composition of the syncytiotrophoblast glycocalyx; in case of mild and severe PE, the expression pattern of fucosylated glycans was changed uniformly, and α1,2-fucose-containing glycans significantly prevailed in the endothelial glycocalyx. According to the results of Fisher's LSD test, in patients with severe PE, the total vascular area in the villus prevailed over the indices established during physiological course of pregnancy (p=0.04) and mild PE (p=0.04). Correlation analysis revealed direct and reciprocal relationships between the morphometric characteristics of the terminal villi of the placenta and the expression of fucosylated glycans in the syncytiotrophoblast and endothelium in PE. Our results indicate a changed expression of fucosylated glycans in the glycocalyx of placental barrier structures and the morphometric parameters of villi in PE of different severity, which can affect the function of the placental barrier.

Published

2021

27. Conformational alteration in glycan induces phospholipase Cβ1 activation and angiogenesis

Author

Sheng-Hung Wang, Jing-Yan Cheng, Hsiu-Hui Tsai, Tzu-Chi Lo, Jung-Tung Hung, Chun-Cheng Lin, Chien-Wei Lee, Yi-Hsuan Ho, Huan-Hsien Kuo, Alice L. Yu, and John Yu

Subjects

Endocrinology, Diabetes and Metabolism, Biochemistry (medical), Clinical Biochemistry, Phospholipase C beta, Cell Biology, General Medicine, Ceramides, DNA-Binding Proteins, Mice, Human Umbilical Vein Endothelial Cells, Animals, Humans, Pharmacology (medical), Molecular Biology, Fucose

Abstract

Background In endothelial cells, phospholipase C (PLC) β1-activated Ca2+ is a crucial second messenger for the signaling pathways governing angiogenesis. PLCβ1 is inactivated by complexing with an intracellular protein called translin-associated factor X (TRAX). This study demonstrates specific interactions between Globo H ceramide (GHCer) and TRAX, which highlight a new angiogenic control through PLCβ1 activation. Methods Globo-series glycosphingolipids (GSLs), including GHCer and stage-specific embryonic antigen-3 ceramide (SSEA3Cer), were analyzed using enzyme-linked immunosorbent assay (ELISA) and Biacore for their binding with TRAX. Angiogenic activities of GSLs in human umbilical vein endothelial cells (HUVECs) were evaluated. Molecular dynamics (MD) simulation was used to study conformations of GSLs and their molecular interactions with TRAX. Fluorescence resonance energy transfer (FRET) analysis of HUVECs by confocal microscopy was used to validate the release of PLCβ1 from TRAX. Furthermore, the in vivo angiogenic activity of extracellular vesicles (EVs) containing GHCer was confirmed using subcutaneous Matrigel plug assay in mice. Results The results of ELISA and Biacore analysis showed a stable complex between recombinant TRAX and synthetic GHCer with Kd of 40.9 nM. In contrast, SSEA3Cer lacking a fucose residue of GHCer at the terminal showed ~ 1000-fold decrease in the binding affinity. These results were consistent with their angiogenic activities in HUVECs. The MD simulation indicated that TRAX interacted with the glycan moiety of GHCer at amino acid Q223, Q219, L142, S141, and E216. At equilibrium the stable complex maintained 4.6 ± 1.3 H-bonds. TRAX containing double mutations with Q223A and Q219A lost its ability to interact with GHCer in both MD simulation and Biacore assays. Removal of the terminal fucose from GHCer to become SSEA3Cer resulted in decreased H-bonding to 1.2 ± 1.0 by the MD simulation. Such specific H-bonding was due to the conformational alteration in the whole glycan which was affected by the presence or absence of the fucose moiety. In addition, ELISA, Biacore, and in-cell FRET assays confirmed the competition between GHCer and PLCβ1 for binding to TRAX. Furthermore, the Matrigel plug assay showed robust vessel formation in the plug containing tumor-secreted EVs or synthetic GHCer, but not in the plug with SSEA3Cer. The FRET analysis also indicated the disruption of colocalization of TRAX and PLCβ1 in cells by GHCer derived from EVs. Conclusions Overall, the fucose residue in GHCer dictated the glycan conformation for its complexing with TRAX to release TRAX-sequestered PLCβ1, leading to Ca2+ mobilization in endothelial cells and enhancing angiogenesis in tumor microenvironments.

Published

2022

28. Human Milk Oligosaccharide 2′-Fucosyllactose Inhibits Ligand Binding to C-Type Lectin DC-SIGN but Not to Langerin

Author

Mukherjee, Reshmi, Somovilla, Victor J., Chiodo, Fabrizio, Bruijns, Sven, Pieters, Roland J., Garssen, Johan, van Kooyk, Yvette, Kraneveld, Aletta D., van Bergenhenegouwen, Jeroen, Afd Pharmacology, Afd Chemical Biology and Drug Discovery, Pharmacology, Chemical Biology and Drug Discovery, Molecular cell biology and Immunology, AII - Cancer immunology, Afd Pharmacology, Afd Chemical Biology and Drug Discovery, Pharmacology, and Chemical Biology and Drug Discovery

Subjects

Milk, Human, Organic Chemistry, Oligosaccharides, Receptors, Cell Surface, General Medicine, Ligands, DC-SIGN, Catalysis, lewis B antigen, Computer Science Applications, Inorganic Chemistry, langerin, Humans, 2′-FL, Lectins, C-Type, human milk oligosaccharides, Physical and Theoretical Chemistry, Molecular Biology, Spectroscopy, Fucose

Abstract

Human milk oligosaccharides (HMOs) and its most abundant component, 2’-Fucosyllactose (2’-FL), are known to be immunomodulatory. Previously, it was shown that HMOs and 2’-FL bind to the C-type lectin receptor DC-SIGN. Here we show, using a ligand-receptor competition assay, that a whole mixture of HMOs from pooled human milk (HMOS) and 2’-FL inhibit the binding of the carbohydrate-binding receptor DC-SIGN to its prototypical ligands, fucose and the oligosaccharide Lewis-B, (Leb) in a dose-dependent way. Interestingly, such inhibition by HMOS and 2’-FL was not detected for another C-type lectin, Langerin, evolutionary similar to DC-SIGN. The cell-ligand competition assay using DC-SIGN expressing cells confirmed that 2’-FL inhibits the binding of DC-SIGN to Leb. Molecular dynamics (MD) simulations show that 2’-FL exists in a preorganized bioactive conformation before binding to DC-SIGN and this conformation is retained after binding to DC-SIGN. Leb has more flexible conformations and utilizes two binding modes, which operate one at a time via its two fucoses to bind to DC-SIGN. 2’-FL may have a reduced entropic penalty due to its preorganized state compared to Leb, and it has lower binding enthalpy, suggesting better binding to DC-SIGN. Thus, due to the better binding to DC-SIGN, 2’-FL may replace Leb from its binding pocket in DC-SIGN. MD simulations also showed that 2’-FL does not bind to Langerin. Our studies confirm 2’-FL as a specific ligand for DC-SIGN and suggest that 2’-FL can replace other DC-SIGN ligands from its binding pocket during ligand-receptor interactions in possible immunomodulatory processes.

Published

2022

29. Neutron crystallography reveals mechanisms used by Pseudomonas aeruginosa for host-cell binding

Author

Lukas Gajdos, Matthew P. Blakeley, Michael Haertlein, V. Trevor Forsyth, Juliette M. Devos, and Anne Imberty

Subjects

Science, Genetic Vectors, Glycobiology, Carbohydrates, Gene Expression, General Physics and Astronomy, Crystallography, X-Ray, Ligands, Article, Bacterial Adhesion, General Biochemistry, Genetics and Molecular Biology, Lectins, Escherichia coli, Humans, Pseudomonas Infections, Cloning, Molecular, X-ray crystallography, Fucose, Neutrons, Bacterial structural biology, Cross Infection, Binding Sites, Multidisciplinary, Water, R735, Hydrogen Bonding, General Chemistry, Deuterium, R1, Recombinant Proteins, Pseudomonas aeruginosa, Calcium, Protein Binding

Abstract

The opportunistic pathogen Pseudomonas aeruginosa, a major cause of nosocomial infections, uses carbohydrate-binding proteins (lectins) as part of its binding to host cells. The fucose-binding lectin, LecB, displays a unique carbohydrate-binding site that incorporates two closely located calcium ions bridging between the ligand and protein, providing specificity and unusually high affinity. Here, we investigate the mechanisms involved in binding based on neutron crystallography studies of a fully deuterated LecB/fucose/calcium complex. The neutron structure, which includes the positions of all the hydrogen atoms, reveals that the high affinity of binding may be related to the occurrence of a low-barrier hydrogen bond induced by the proximity of the two calcium ions, the presence of coordination rings between the sugar, calcium and LecB, and the dynamic behaviour of bridging water molecules at room temperature. These key structural details may assist in the design of anti-adhesive compounds to combat multi-resistance bacterial infections., Pseudomonas aeruginosa employs lectins to bind to its host cells, and is known to be the major cause of lung infections. Lectin B (LecB) from Pseudomonas aeruginosa binds specifically to galactose and fucose and is important for pathogenicity, adhesion and biofilm formation. In this work, the neutron crystal structure (1.9 Å) of the deuterated LecB/Ca/fucose complex is reported. The structure, in combination with perdeuteration of the ligand and the receptor allowed the observation of hydrogen atoms, protonation states and hydrogen bonds involved in the interaction between pathogenic bacteria and host cells. Thus the study provides structural insights into the mechanism of high affinity binding of LecB to its targets.

Published

2022

30. Pyranose Ring Puckering Thermodynamics for Glycan Monosaccharides Associated with Vertebrate Proteins

Author

Guvench, Olgun, Martin, Devon, and Greene, Megan

Subjects

GlcNAc, QH301-705.5, glucose, galactose, GalNAc, mannose, xylose, fucose, Neu5Ac, glucuronate, iduronate, tetrahydropyran, Article, Catalysis, Inorganic Chemistry, Polysaccharides, Carbohydrate Conformation, Animals, Physical and Theoretical Chemistry, Biology (General), Molecular Biology, QD1-999, Spectroscopy, Monosaccharides, Organic Chemistry, General Medicine, Computer Science Applications, Chemistry, Thermodynamics

Abstract

The conformational properties of carbohydrates can contribute to protein structure directly through covalent conjugation in the cases of glycoproteins and proteoglycans and indirectly in the case of transmembrane proteins embedded in glycolipid-containing bilayers. However, there continue to be significant challenges associated with experimental structural biology of such carbohydrate-containing systems. All-atom explicit-solvent molecular dynamics simulations provide a direct atomic resolution view of biomolecular dynamics and thermodynamics, but the accuracy of the results depends on the quality of the force field parametrization used in the simulations. A key determinant of the conformational properties of carbohydrates is ring puckering. Here, we applied extended system adaptive biasing force (eABF) all-atom explicit-solvent molecular dynamics simulations to characterize the ring puckering thermodynamics of the ten common pyranose monosaccharides found in vertebrate biology (as represented by the CHARMM carbohydrate force field). The results, along with those for idose, demonstrate that the CHARMM force field reliably models ring puckering across this diverse set of molecules, including accurately capturing the subtle balance between 4C1 and 1C4 chair conformations in the cases of iduronate and of idose. This suggests the broad applicability of the force field for accurate modeling of carbohydrate-containing vertebrate biomolecules such as glycoproteins, proteoglycans, and glycolipids.

Published

2022

31. β-D-XYLOSIDASE 4 modulates systemic immune signaling in Arabidopsis thaliana

Author

Kornelia Bauer, Shahran Nayem, Martin Lehmann, Marion Wenig, Lin-Jie Shu, Stefanie Ranf, Peter Geigenberger, and A. Corina Vlot

Subjects

Plant Science, plant immunity, plant defense, systemic acquired resistance, cell wall, xylosidase, xylose, fucose, putrescine, ddc

Abstract

Pectin- and hemicellulose-associated structures of plant cell walls participate in defense responses against pathogens of different parasitic lifestyles. The resulting immune responses incorporate phytohormone signaling components associated with salicylic acid (SA) and jasmonic acid (JA). SA plays a pivotal role in systemic acquired resistance (SAR), a form of induced resistance that - after a local immune stimulus - confers long-lasting, systemic protection against a broad range of biotrophic invaders. β-D-XYLOSIDASE 4 (BXL4) protein accumulation is enhanced in the apoplast of plants undergoing SAR. Here, two independent Arabidopsis thaliana mutants of BXL4 displayed compromised systemic defenses, while local resistance responses to Pseudomonas syringae remained largely intact. Because both phloem-mediated and airborne systemic signaling were abrogated in the mutants, the data suggest that BXL4 is a central component in SAR signaling mechanisms. Exogenous xylose, a possible product of BXL4 enzymatic activity in plant cell walls, enhanced systemic defenses. However, GC-MS analysis of SAR-activated plants revealed BXL4-associated changes in the accumulation of certain amino acids and soluble sugars, but not xylose. In contrast, the data suggest a possible role of pectin-associated fucose as well as of the polyamine putrescine as regulatory components of SAR. This is the first evidence of a central role of cell wall metabolic changes in systemic immunity. Additionally, the data reveal a so far unrecognized complexity in the regulation of SAR, which might allow the design of (crop) plant protection measures including SAR-associated cell wall components.

Published

2022

32. Multivalent Fucosides Targeting β-Propeller Lectins from Lung Pathogens with Promising Anti-Adhesive Properties

Author

Duca, Margherita, Haksar, Diksha, van Neer, Jacq, Thies-Weesie, Dominique M E, Martínez-Alarcón, Dania, de Cock, Hans, Varrot, Annabelle, Pieters, Roland J, Molecular Microbiology, Afd Chemical Biology and Drug Discovery, Sub Molecular Microbiology, Sub Physical and Colloid Chemistry, Chemical Biology and Drug Discovery, Physical and Colloid Chemistry, Molecular Microbiology, Afd Chemical Biology and Drug Discovery, Sub Molecular Microbiology, Sub Physical and Colloid Chemistry, Chemical Biology and Drug Discovery, and Physical and Colloid Chemistry

Subjects

Lectins, Adhesives, Aspergillus fumigatus, Molecular Medicine, Humans, General Medicine, Biochemistry, Lung, Fucose

Abstract

Fungal and bacterial pathogens causing lung infections often use lectins to mediate adhesion to glycoconjugates at the surface of host tissues. Given the rapid emergence of resistance to the treatments in current use, β-propeller lectins such as FleA from Aspergillus fumigatus, SapL1 from Scedosporium apiospermum, and BambL from Burkholderia ambifaria have become appealing targets for the design of anti-adhesive agents. In search of novel and cheap anti-infectious agents, we synthesized multivalent compounds that can display up to 20 units of fucose, the natural ligand. We obtained nanomolar inhibitors that are several orders of magnitude stronger than their monovalent analogue according to several biophysical techniques (i.e., fluorescence polarization, isothermal titration calorimetry, and bio-layer interferometry). The reason for high affinity might be attributed to a strong aggregating mechanism, which was examined by analytical ultracentrifugation. Notably, the fucosylated inhibitors reduced the adhesion of A. fumigatus spores to lung epithelial cells when administered 1 h before or after the infection of human lung epithelial cells. For this reason, we propose them as promising anti-adhesive drugs for the prevention and treatment of aspergillosis and related microbial lung infections.

Published

2022

33. A Redox‐Controlled Substrate Engineering Strategy for Site‐Specific Enzymatic Fucosylation

Author

Na Lu, Yun Li, Hui Xia, Kan Zhong, Chenning Jia, Jinfeng Ye, Xianwei Liu, Chang‐Cheng Liu, and Hongzhi Cao

Subjects

Glycosylation, Polysaccharides, General Chemistry, General Medicine, Fucosyltransferases, Oxidation-Reduction, Catalysis, Fucose, Substrate Specificity

Abstract

Fucosylation is one of the most common modifications of oligo-N-acetyllactosamine (oligo-LacNAc) glycans. However, none of known fucosyltransferases (FucTs) could install the α1,3-linked fucose to the oligo-LacNAc substrates in a site-specific manner. Here, we report a facile and general redox-controlled substrate engineering strategy for the site-specific α1,3-fucosylation of complex glycans containing multiple LacNAc units. This strategy takes advantage of an operationally simple oxidation enzyme module by using galactose oxidase (GOase) to convert the LacNAc unit into oxidized C6'-aldehyde LacNAc sequence, which is not a good substrate for recombinant α1,3-FucT from Helicobacter pylori strain 26695 (Hpα1,3FucT), enabling the site-specific α1,3-fucosylation at intact LacNAc sites. The general applicability and robustness of this strategy were demonstrated by the synthesis of a variety of structurally well-defined fucosides of linear and branched O- and N-linked glycans.

Published

2022

34. A Sensitive and Reversible Labeling Strategy Enables Global Mapping of the Core‐Fucosylated Glycoproteome on Cell Surfaces

Author

Yinping Tian, Yuqiu Wang, Hongbo Yin, Yawen Luo, Fangyu Wei, Hu Zhou, and Liuqing Wen

Subjects

Glycosylation, Proteome, Polysaccharides, General Medicine, General Chemistry, Mass Spectrometry, Catalysis, Fucose, Glycoproteins, Acetylglucosamine

Abstract

Core fucosylation, the attachment of α1,6-fucose to the innermost N-acetylglucosamine (GlcNAc) residue of N-glycans, has a strong relationship with tumor growth, invasion, metastasis, prognosis, and immune evasion by regulating many membrane proteins. However, details about the functional mechanism are still largely unknown due to the lack of an effective analytical method to identify cell-surface core-fucosylated glycoproteins, and especially glycosylation sites. Here, we developed a sensitive and reversible labeling strategy for probing core fucosylation, by which core-fucosylated glycoproteins that located on cell-surface were selectively tagged by a biotinylated probe with high sensitivity. The labeled probe can be further broken enzymatically after the capture by affinity resin. The on-bead traceless cleavage allowed the global mapping of core-fucosylated glycoproteins and glycosylation sites by mass spectrometry (MS). The profile of core-fucosylated glycoproteome provides an in-depth understanding of the biological functions of core fucosylation.

Published

2022

35. Nanoparticles To Study Lectins in Caenorhabditis elegans: Multivalent Galactose β1-4 Fucose-Functionalized Dendrimers Provide Protection from Oxidative Stress

Author

Harrison W. VanKoten, Rebecca S. Moore, and Mary J. Cloninger

Subjects

Polymers and Plastics, biology, Nanoparticle, Bioengineering, biology.organism_classification, medicine.disease_cause, Fucose, Cell biology, Biomaterials, chemistry.chemical_compound, chemistry, RNA interference, Dendrimer, Galactose, Materials Chemistry, medicine, Caenorhabditis elegans, Oxidative stress, Galectin

Abstract

Galectins are galactoside-binding lectins that are functional dimers or higher-order oligomers. Multivalent binding has been shown to augment the relatively low affinity of the galectins for their galactoside-binding partners, enabling the galectins to play an important role in the global remodeling of cells that occurs during the stress conditions of disease states, including heart disease and cancer. The presence of galectins in the nematode Caenorhabditis elegans and their galactoside-binding properties have been demonstrated, but the role of multivalent interactions for C. elegans galectins is unknown. Here, we describe the synthesis of Galβ1-4Fuc-functionalized poly(amidoamine) dendrimers and their utility in studies using C. elegans during oxidative stress. C. elegans were fed Galβ1-4Fuc-functionalized dendrimers and RNA interference to knock down lectins lec-1 and lec-10 while undergoing oxidative stress. C. elegans that were pretreated with the glycodendrimers were less susceptible to oxidative stress than untreated controls. Worms that were fed fluorescently tagged glycodendrimers and imaged indicated that the dendrimers are primarily present in the digestive tract of the worms, and uptake into the vulva and proximal gonads could also be observed in some instances. This study suggests that multivalently presented Galβ1-4Fuc can protect C. elegans from oxidative stress.

Published

2021

36. Extraction and characterization of an exopolysaccharide from a marine bacterium

Author

Ashwini Prabhu, Punchappady-Devasya Rekha, and Bythadka Erappa Dhanya

Subjects

Microbiology (medical), chemistry.chemical_classification, Antioxidant, biology, Biocompatibility, DPPH, Biomolecule, medicine.medical_treatment, biology.organism_classification, Microbiology, Fucose, chemistry.chemical_compound, chemistry, medicine, Monosaccharide, Food science, Bacteria, Thermostability

Abstract

The marine bacterial exopolysaccharides (EPS) have transfigured the biotech sector with their myriad applications and prospects. This work was carried out to characterize and analyze the functional and biochemical properties of an EPS (EPS-DR3A) produced by a marine bacterium, Pseudoalteromonas sp. YU16-DR3A. The bacterium was cultured in Zobell marine broth for the production of EPS. The extracted EPS designated as EPS-DR3A was composed of 69% carbohydrates and 7.6% proteins with a molecular weight of 20 kDa. FT-IR spectra showed the presence of different functional groups. The monosaccharide analysis performed using GC-MS showed the presence of fucose, erythrotetrose, ribose, and glucose as monomers. EPS-DR3A showed excellent emulsifying activity against the tested hydrocarbons and food oils with stable emulsions. Rheological analysis of EPS-DR3A revealed the pseudoplastic behavior. The EPS-DR3A displayed good thermal stability with a degradation temperature of 249 °C and a melting point at 322 °C. Further, it had the ability to scavenge DPPH and nitric oxide free radicals with good total antioxidant activity. The in vitro biocompatibility study of EPS-DR3A showed high degree of biocompatibility with human dermal fibroblast cells at the tested concentrations. Taken together, the findings such as thermostability, emulsifying activity, pseudoplasticity, antioxidant activity, and biocompatibility of EPS-DR3A make this biomolecule an important candidate for a wide range of biomedical applications.

Published

2021

37. Transcriptomic profile of human erythroleukemia cells in response to Sargassum fusiforme polysaccharide and its structure analysis

Author

Ce Xie, Hao-Miao Ding, Rui-Jie Fu, Cai-Sheng Wang, and Guo-Ying Qian

Subjects

Cell growth, Chemistry, Sargassum, General Medicine, In vitro, Fucose, Transcriptome, Phosphatidylinositol 3-Kinases, chemistry.chemical_compound, Complementary and alternative medicine, Biochemistry, Polysaccharides, Drug Discovery, Cancer cell, Humans, Leukemia, Erythroblastic, Acute, Viability assay, KEGG, Gene

Abstract

Sargassum fusiforme (S. fusiforme) has been used as an ingredient in Chinese herbal medicine for thousands of years. However, there are a limited number of studies concerning its therapeutic mechanism. High performance gel permeation chromatography (HPGPC) analysis showed that the average molecular weight of the S. fusiforme polysaccharide, SFPS 191212, is 43 kDa. SFPS 191212 is composed of mannose, rhamnose, galactose, xylose, glucose, and fucose (at a molar ratio: 2.1 : 2.9 : 1.8 : 15.5 : 4.6 : 62.5) with α- and β-configurations. The present research evaluated the anti-tumor potential of the S. fusiforme polysaccharide in human erythroleukemia (HEL) cells in vitro. To explore the SFPS 191212's apoptosis mechanism in HEL cells, transcriptome analysis was performed on HEL cells that were incubated with SFPS 191212. The inhibitory effect of SFPS 191212 on HEL cell growth was also analyzed. It was found that SFPS 191212 inhibited HEL cell proliferation, reduced cell viability in a concentration-dependent manner, and induced an insignificant toxic effect on normal human embryonic lung (MRC-5) cells. Compared with the control group, transcriptome analysis identified a total of 598 differentially expressed genes (DEGs), including 243 up-regulated genes and 355 down-regulated genes. Gene Ontology (GO) and Kyoto Encyclopedia of Genes and Genomes (KEGG) enrichment analyses were performed on all DEGs, and 900 GO terms and 52 pathways were found to be significantly enriched. Finally, 23 DEGs were randomly selected and confirmed by quantitative real-time polymerase chain reaction (qRT-PCR). Moreover, SFPS 191212 down-regulated the PI3K/Akt signal transduction pathway. Our results provide a framework for understanding the effect of SFPS 191212 on cancer cells and can serve as a resource for delineating the anti-tumor mechanisms of S. fusiforme.

Published

2021

38. Tremella fuciformis TFCUV5 Mycelial Culture-derived Exopolysaccharide Production and Its Anti-aging Effects on Skin Cells

Author

Hansu Jang, Min-Ho Jo, Jung-Hyun Ju, Chul Ho Kim, Hyun-Sook Yeom, Min-Soo Kim, Keug-Hyun Ahn, Sun-Yeon Heo, Hye Ja Lee, Baek-Rock Oh, and Byeol Kim

Subjects

biology, Tremella fuciformis, Biomedical Engineering, Mannose, Bioengineering, Xylose, Glucuronic acid, biology.organism_classification, Applied Microbiology and Biotechnology, Fucose, chemistry.chemical_compound, chemistry, Fermentation, Food science, Industrial and production engineering, Mycelium, Biotechnology

Abstract

Tremella fuciformis TFC6 mycelia was isolated from its fruiting body. T. fuciformis TFCUV5 was obtained from TFC6 mycelia by ultraviolet mutagenesis to improve extracellular-polysaccharide (EPS) yield. In addition, we investigated the physicochemical properties and functionality of EPS for industrial applications and the effect of EPS on enhancement of the moisturizing factor and antiwrinkle effect in skin cells. The EPS yield was improved upon fermentation by the mutant strain through optimization of the medium composition and culture conditions to a maximum of 8.4 g/L; the productivity was 1.9 g/L-day under optimal culture conditions (initial pH 7.0 at 25°C, 300 rpm, 2 vvm). EPS with a molecular weight of 1.79 × 106 (± 0.721%) comprised mannose, xylose, glucuronic acid, fucose, and glucose. EPS extract increased both moisture and the antiwrinkle factor in skin cells. Therefore, EPS from TFCUV5 might have potential to be used in the cosmetics industry.

Published

2021

39. Antioxidant Potential of Fucose Isolated from the Marine Macroalgae Padina gymnospora

Author

R. Swaminathan

Subjects

chemistry.chemical_compound, Biochemistry, Chemistry, General Medicine, Antioxidant potential, Fucose, Padina gymnospora

Published

2021

40. Efficient Production of 2′-Fucosyllactose from <scp>l</scp>-Fucose via Self-Assembling Multienzyme Complexes in Engineered Escherichia coli

Author

Geng Chen, Guocong Luo, Li Wan, Wenli Zhang, Wanmeng Mu, and Yingying Zhu

Subjects

chemistry.chemical_classification, biology, Biomedical Engineering, General Medicine, medicine.disease_cause, Biochemistry, Genetics and Molecular Biology (miscellaneous), Cofactor, Fucose, Metabolic engineering, chemistry.chemical_compound, 2'-Fucosyllactose, Enzyme, Biosynthesis, chemistry, Biochemistry, medicine, biology.protein, Fermentation, Escherichia coli

Abstract

2'-Fucosyllactose (2'-FL) has been widely used as a nutritional additive in infant formula due to its multifarious nutraceutical and pharmaceutical functions in neonate health. As such, it is essential to develop an efficient and extensive microbial fermentation platform to cater to the needs of the 2'-FL market. In this study, a spatial synthetic biology strategy was employed to promote 2'-FL biosynthesis in recombinant Escherichia coli. First, the salvage pathway for 2'-FL production from l-fucose and lactose was constructed by introducing a bifunctional enzyme l-fucokinase/GDP-l-fucose pyrophosphorylase (Fkp) derived from Bacteroides fragilis and an α-1,2-fucosyltransferase (FutC) derived from Helicobacter pylori into engineered E. coli BL21(DE3). Next, the endogenous genes involved in the degradation and shunting of the substrate and key intermediate were inactivated to improve the availability of precursors for 2'-FL biosynthesis. Moreover, to further improve the yield and titer of 2'-FL, a short peptide pair (RIAD-RIDD) was used to form self-assembling multienzyme complexes in vivo. The spatial localization of peptides and stoichiometry of enzyme assemblies were subsequently optimized to further improve 2'-FL production. Finally, cofactor regeneration was also considered to alleviate the potential cofactor deficiency and redox flux imbalance in the biocatalysis process. Fed-batch fermentation of the final WLS20 strain accumulated 30.5 g/L extracellular 2'-FL with the yield and productivity of 0.661 mol/mol fucose and 0.48 g/L/h, respectively. This research has demonstrated that the application of spatial synthetic biology and metabolic engineering strategies can dramatically enlarge the titer and yield of 2'-FL biosynthesis in engineered E. coli.

Published

2021

41. The effect of substance P on blood serum glycoproteins under technogenic rotating electric fields in animals with different stress resistance profiles

Author

T S Vorontsova, L S Isakova, and N N Vasileva

Subjects

chemistry.chemical_classification, medicine.medical_specialty, Mucoproteins, business.industry, Substance P, General Medicine, Metabolism, Open field, Fucose, chemistry.chemical_compound, Endocrinology, Blood serum, chemistry, Internal medicine, Electric field, medicine, Glycoprotein, business

Abstract

Aim. To study the effect of substance P on the blood serum glycoproteins in experimental animals with different stress-resistance profiles under technogenic rotating electric field. Methods. The level of sialic acids, mucoproteins, fucose, and -L-fucosidase was determined in the blood serum of 72 noninbred white male rats before (control) and on the 10th and 20th day of exposure to a technogenic rotating electric field (REF), as well as under the combination of technogenic rotating electric field and substance P injection at the same time. To determine the stress resistance, the animals were tested using the open field method. Animals were divided into groups based on the tests data obtained: stress-resistant, not stress-resistant and ambivalent. Results. On the 10th day of technogenic rotating electric field action, the level of sialic acids, fucose, and -L-fucosidase activity increased in all animals. The concentration of mucoproteins tended to decrease. On the 20th day, the sialic acids content remained elevated compared with the control in all groups. The content of mucoproteins decreased in stress-resistant, not stress-resistant and restored to the control level in ambivalent compared with those on the 10th day. On the 20th day, fucose concentration reached control values in stress-resistant and ambivalent animals and decreased in not stress-resistant. On the 10th day of the combined exposure, the concentration of sialic acids, mucoproteins, fucose, -L-fucosidase was reduced in all animals compared with the 10th day of technogenic rotating electric field action. On the 20th day of the combined exposure, the values of the studied parameters remained reduced in all groups of animals compared with those on the 20th day of isolated technogenic rotating electric field action. Conclusion. The substance P injection limits the effects of technogenic rotating electric field on the metabolism of carbohydrate-containing biopolymers in blood serum in all groups of animals, as can be seen by a decrease in the level of sialic acids, fucose, and low enzymatic activity of -L-fucosidase under combined exposure.

Published

2021

42. Klebsiella pneumoniae <scp>l-</scp> Fucose Metabolism Promotes Gastrointestinal Colonization and Modulates Its Virulence Determinants

Author

Andrew W. Hudson, Andrew J. Barnes, Andrew S. Bray, David A. Ornelles, and M. Ammar Zafar

Subjects

Virulence, Virulence Factors, Immunology, Mucins, Molecular Pathogenesis, Microbiology, Carbon, Klebsiella Infections, Mice, Klebsiella pneumoniae, Infectious Diseases, Escherichia coli, Animals, Parasitology, Fucose

Abstract

Colonization of the gastrointestinal (GI) tract by Klebsiella pneumoniae is generally considered asymptomatic. However, gut colonization allows K. pneumoniae to either translocate to sterile site within the same host or transmit through the fecal-oral route to another host. K. pneumoniae gut colonization is poorly understood, but knowledge of this first step toward infection and spread is critical for combatting its disease manifestations. K. pneumoniae must overcome colonization resistance (CR) provided by the host microbiota to establish itself within the gut. One such mechanism of CR is through nutrient competition. Pathogens that metabolize a broad range of substrates have the ability to bypass nutrient competition and overcome CR. Herein, we demonstrate that in response to mucin-derived fucose, the conserved fucose metabolism operon (fuc) of K. pneumoniae is upregulated in the murine gut, and we subsequently show that fucose metabolism promotes robust gut colonization. Growth studies using cecal filtrate as a proxy for the gut lumen illustrate the growth advantage that the fuc operon provides K. pneumoniae. We further show that fucose metabolism allows K. pneumoniae to be competitive with a commensal Escherichia coli isolate (Nissle). However, Nissle is eventually able to outcompete K. pneumoniae, suggesting that it can be utilized to enhance CR. Finally, we observed that fucose metabolism positively modulates hypermucoviscosity, autoaggregation, and biofilm formation but not capsule biogenesis. Together, these insights enhance our understanding of the role of alternative carbon sources in K. pneumoniae gut colonization and the complex relationship between metabolism and virulence in this species.

Published

2022

43. Synthesis of O-Linked Glycoconjugates in the Nervous System

Author

Jin-ichi Inokuchi, Yoshio Hirabayashi, and Shinji Go

Subjects

chemistry.chemical_classification, chemistry.chemical_compound, Ceramide, chemistry, Biochemistry, Glycoconjugate, Mannose, lipids (amino acids, peptides, and proteins), Glycosphingolipid, Phosphatidic acid, Membrane transport, Glycoprotein, Fucose

Abstract

Glycoproteins carrying O-linked N-acetylgalactosamine, N-acetylgluco-samine, mannose, fucose, glucose, and xylose are found in the nervous system. Lipids can be glycosylated as well. Membrane lipid, ceramide, is modified by the addition of either glucose or galactose to form glycosphingolipid, galactosylceramide, or glucosylceramide. Recent analyses have identified glucosylated lipids of cholesterol and phosphatidic acid. These O-linked carbohydrate residues are found primarily on the outer surface of the plasma membrane or in the extracellular space. Their expression is cell or tissue specific and developmentally regulated. Due to their structural diversity, they play important roles in a variety of biological processes such as membrane transport and cell–cell interactions.

Published

2022

44. Synthesis, Processing, and Function of N-Glycans in N-Glycoproteins

Author

Erhard Bieberich

Subjects

Glycan, Endoplasmic-reticulum-associated protein degradation, Fucose, Article, Acetylglucosamine, chemistry.chemical_compound, symbols.namesake, Polysaccharides, Glycosyltransferase, Humans, Asparagine, Glycoproteins, biology, Endoplasmic reticulum, Galactose, COVID-19, Golgi apparatus, Lipids, N-Acetylneuraminic Acid, Sialic acid, carbohydrates (lipids), chemistry, Biochemistry, biology.protein, symbols

Abstract

Many membrane-resident and secrected proteins, including growth factors and their receptors are N-glycosylated. The initial N-glycan structure consists of 14 sugar residues (Glc3Man9GlcNAc2) that are first synthesized in the endoplasmic reticulum (ER) as a branched structure on a lipid anchor (dolicholpyrophosphate) and then co-translationally, “en bloc” transferred and linked via N-acetylglucosamine (GlcNAc) to asparagine within a specific N-glycosylation acceptor sequence (Asn-X-Ser/Thr) of the nascent recipient protein. In the ER and then the Golgi apparatus, the N-linked glycan structure is modified by hydrolytic removal of sugar residues (“trimming”) followed by re-glycosylation with additional sugar residues (“processing”) such as galactose, fucose or sialic acid in complex N-glycoproteins. While the sequence of the reactions leading to biosynthesis, “en bloc” transfer and processing of N-glycans is well investigated, it is still not completely understood how N-glycans affect the biological fate and function of N-glycoproteins. Initially, N-glycans have been found to be critical for proper protein folding and quality control by chaperones in the ER, a process now known as the “calnexin/calreticulin cycle” in the unfolded protein response and ER-assisted degradation (ERAD). More recently, N-glycans have been shown to modulate the function of many cell surface proteins involved in migration and adhesion, including those regulating myelination. Currently, the Golgi has emerged as an organelle that is intimately linked to editing the function of N-glycans in N-glycoprotein transport and sorting. For one, it has been shown that mutations in Golgi glycosyltransferases and transport proteins lead to defects in N-glycan processing that cause severe congenital disorders of glycosylation (CDG). On the other hand, it has been found that N-glycans affect transport of glycosylated proteins in the Golgi, including sorting of secreted proteins such as prions and amyloid. Our group has shown that N-glycan-dependent enzyme complex formation may entangle processing of N-glycosylated glycosyltransferases with glycosphingolipid metabolism, which appears to be important for ganglioside class switches during embryonic brain development. This review will discuss the biology of N-glycoprotein synthesis, processing and function with specific reference to the physiology and pathophysiology of the nervous system.

Published

2022

45. Human FSH Glycoform α-Subunit Asparagine52 Glycans: Major Glycan Structural Consistency, Minor Glycan Variation in Abundance

Author

Viktor Y. Butnev, Jeffrey V. May, Alan R. Brown, Tarak Sharma, Vladimir Y. Butnev, William K. White, David J. Harvey, and George R. Bousfield

Subjects

Polysaccharides, Endocrinology, Diabetes and Metabolism, Humans, Receptors, FSH, Follicle Stimulating Hormone, Human, Asparagine, Follicle Stimulating Hormone, Fucose

Abstract

Follicle-stimulating hormone (FSH), an α/β heterodimeric glycoprotein hormone, consists of functionally significant variants resulting from the presence or absence of either one of two FSHβ subunit N-glycans. The two most abundant variants are fully-glycosylated FSH24 (based on 24 kDa FSHβ band in Western blots) and hypo-glycosylated FSH21 (21 kDa band, lacks βAsn24 glycans). Due to its ability to bind more rapidly to the FSH receptor and occupy more FSH binding sites than FSH24, hypo-glycosylated FSH21 exhibits greater biological activity. Endoglycosidase F1-deglycosylated FSH bound to the complete extracellular domain of the FSH receptor crystallized as a trimeric complex. It was noted that a single biantennary glycan attached to FSHα Asn52 might preemptively fill the central pocket in this complex and prevent the other two FSH ligands from binding the remaining ligand-binding sites. As the most active FSH21 preparations possessed more rapidly migrating α-subunit bands in Western blots, we hypothesized that Asn52 glycans in these preparations were small enough to enable greater FSH21 receptor occupancy in the putative FSHR trimer model. Highly purified hFSH oligosaccharides derived from each FSH subunit, were characterized by electrospray ionization-ion mobility-collision-induced dissociation (ESI-IM-CID) mass spectrometry. FSHβ glycans typically possessed core-linked fucose and were roughly one third bi-antennary, one third tri-antennary and one third tetra-antennary. FSHα oligosaccharides largely lacked core fucose and were bi- or tri-antennary. Those αAsn52 glycans exhibiting tetra-antennary glycan m/z values were found to be tri-antennary, with lactosamine repeats accounting for the additional mass. Selective αAsn52 deglycosylation of representative pituitary hFSH glycoform Superdex 75 gel filtration fractions followed by ESI-IM-CID mass spectrometry revealed tri-antennary glycans predominated even in the lowest molecular weight FSH glycoforms. Accordingly, the differences in binding capacity of the same receptor preparation to different FSH glycoforms are likely the organization of the FSH receptor in cell membranes, rather than the αAsn52 oligosaccharide.

Published

2022

46. Strain engineering and metabolic flux analysis of a probiotic yeast Saccharomyces boulardii for metabolizing l-fucose, a mammalian mucin component

Author

Jungyeon Kim, Yu Eun Cheong, Sora Yu, Yong-Su Jin, and Kyoung Heon Kim

Subjects

Mammals, Probiotics, Mucins, Bioengineering, Saccharomyces cerevisiae, Propylene Glycol, Applied Microbiology and Biotechnology, Metabolic Flux Analysis, Oxygen, Saccharomyces boulardii, Escherichia coli, Lactates, Animals, Pyruvates, Fucose, Biotechnology

Abstract

Background Saccharomyces boulardii is a probiotic yeast that exhibits antimicrobial and anti-toxin activities. Although S. boulardii has been clinically used for decades to treat gastrointestinal disorders, several studies have reported weak or no beneficial effects of S. boulardii administration in some cases. These conflicting results of S. boulardii efficacity may be due to nutrient deficiencies in the intestine that make it difficult for S. boulardii to maintain its metabolic activity. Results To enable S. boulardii to overcome any nutritional deficiencies in the intestine, we constructed a S. boulardii strain that could metabolize l-fucose, a major component of mucin in the gut epithelium. The fucU, fucI, fucK, and fucA from Escherichia coli and HXT4 from S. cerevisiae were overexpressed in S. boulardii. The engineered S. boulardii metabolized l-fucose and produced 1,2-propanediol under aerobic and anaerobic conditions. It also produced large amounts of 1,2-propanediol under strict anaerobic conditions. An in silico genome-scale metabolic model analysis was performed to simulate the growth of S. boulardii on l-fucose, and elementary flux modes were calculated to identify critical metabolic reactions for assimilating l-fucose. As a result, we found that the engineered S. boulardii consumes l-fucose via (S)-lactaldehyde-(S)-lactate-pyruvate pathway, which is highly oxygen dependent. Conclusion To the best of our knowledge, this is the first study in which S. cerevisiae and S. boulardii strains capable of metabolizing l-fucose have been constructed. This strategy could be used to enhance the metabolic activity of S. boulardii and other probiotic microorganisms in the gut.

Published

2022

47. Cryo-EM structures of human fucosidase FucA1 reveal insight into substrate recognition and catalysis

Author

Zachary Armstrong, Richard W. Meek, Liang Wu, James N. Blaza, and Gideon J. Davies

Subjects

alpha-L-Fucosidase, Aspartic Acid, Glutamates, Structural Biology, Cryoelectron Microscopy, Humans, Glycoconjugates, Molecular Biology, Catalysis, Fucose

Abstract

Enzymatic hydrolysis of α-L-fucose from fucosylated glycoconjugates is consequential in bacterial infections and the neurodegenerative lysosomal storage disorder fucosidosis. Understanding human α-L-fucosidase catalysis, in an effort toward drug design, has been hindered by the absence of three-dimensional structural data for any animal fucosidase. Here, we have used cryoelectron microscopy (cryo-EM) to determine the structure of human lysosomal α-L-fucosidase (FucA1) in both an unliganded state and in complex with the inhibitor deoxyfuconojirimycin. These structures, determined at 2.49 Å resolution, reveal the homotetrameric structure of FucA1, the architecture of the catalytic center, and the location of both natural population variations and disease-causing mutations. Furthermore, this work has conclusively identified the hitherto contentious identity of the catalytic acid/base as aspartate-276, representing a shift from both the canonical glutamate acid/base residue and a previously proposed glutamate residue. These findings have furthered our understanding of how FucA1 functions in both health and disease.

Published

2022

48. Origin of cytoplasmic GDP-fucose determines its contribution to glycosylation reactions

Author

Paulina Sosicka, Bobby G. Ng, Lauren E. Pepi, Asif Shajahan, Maurice Wong, David A. Scott, Kenjiroo Matsumoto, Zhi-Jie Xia, Carlito B. Lebrilla, Robert S. Haltiwanger, Parastoo Azadi, and Hudson H. Freeze

Subjects

Glycosylation, Polysaccharides, Guanosine Diphosphate Fucose, Cell Biology, Generic health relevance, Biological Sciences, Medical and Health Sciences, Fucose, Developmental Biology

Abstract

Biosynthesis of macromolecules requires precursors such as sugars or amino acids, originating from exogenous/dietary sources, reutilization/salvage of degraded molecules, or de novo synthesis. Since these sources are assumed to contribute to one homogenous pool, their individual contributions are often overlooked. Protein glycosylation uses monosaccharides from all the above sources to produce nucleotide sugars required to assemble hundreds of distinct glycans. Here, we demonstrate that cells identify the origin/heritage of the monosaccharide, fucose, for glycosylation. We measured the contribution of GDP-fucose from each of these sources for glycan synthesis and found that different fucosyltransferases, individual glycoproteins, and linkage-specific fucose residues identify and select different GDP-fucose pools dependent on their heritage. This supports the hypothesis that GDP-fucose exists in multiple, distinct pools, not as a single homogenous pool. The selection is tightly regulated since the overall pool size remains constant. We present novel perspectives on monosaccharide metabolism, which may have a general applicability.

Published

2022

49. Branched Chondroitin Sulfate Oligosaccharides Derived from the Sea Cucumber

Author

Weili, Wang, Hui, Mao, Sujuan, Li, Longlong, Zhang, Lian, Yang, Ronghua, Yin, and Jinhua, Zhao

Subjects

Sulfates, Sea Cucumbers, Chondroitin Sulfates, Neuronal Outgrowth, Animals, Oligosaccharides, Disaccharides, Fucose

Abstract

Fucosylated chondroitin sulfate (FCS) from the sea cucumber

Published

2022

50. Targeting a Multidrug-Resistant Pathogen: First Generation Antagonists of

Author

Rafael, Bermeo, Kanhaya, Lal, Davide, Ruggeri, Daniele, Lanaro, Sarah, Mazzotta, Francesca, Vasile, Anne, Imberty, Laura, Belvisi, Annabelle, Varrot, and Anna, Bernardi

Subjects

Models, Molecular, Burkholderia, Burkholderia cenocepacia, Lectins, Humans, Oligosaccharides, Fucose

Abstract

Multidrug-resistant pathogens such as

Published

2022