Your search keyword '"Heggelund JE"' showing total 11 results

1. Autoantibody binding and unique enzyme-substrate intermediate conformation of human transglutaminase 3.

Author

Heggelund JE, Das S, Stamnaes J, Iversen R, and Sollid LM

Subjects

Humans, Autoantibodies, Transglutaminases, Immunoglobulin A metabolism, Glutens, Celiac Disease, Dermatitis Herpetiformis

Abstract

Transglutaminase 3 (TG3), the autoantigen of dermatitis herpetiformis (DH), is a calcium dependent enzyme that targets glutamine residues in polypeptides for either transamidation or deamidation modifications. To become catalytically active TG3 requires proteolytic cleavage between the core domain and two C-terminal β-barrels (C1C2). Here, we report four X-ray crystal structures representing inactive and active conformations of human TG3 in complex with a TG3-specific Fab fragment of a DH patient derived antibody. We demonstrate that cleaved TG3, upon binding of a substrate-mimicking inhibitor, undergoes a large conformational change as a β-sheet in the catalytic core domain moves and C1C2 detaches. The unique enzyme-substrate conformation of TG3 without C1C2 is recognized by DH autoantibodies. The findings support a model where B-cell receptors of TG3-specific B cells bind and internalize TG3-gluten enzyme-substrate complexes thereby facilitating gluten-antigen presentation, T-cell help and autoantibody production., (© 2023. Springer Nature Limited.)

Published

2023

2. Crystal structures of cholera toxin in complex with fucosylated receptors point to importance of secondary binding site.

Author

Heim JB, Hodnik V, Heggelund JE, Anderluh G, and Krengel U

Subjects

Binding Sites, Blood Group Antigens chemistry, Cholera microbiology, Cholera Toxin metabolism, G(M1) Ganglioside chemistry, G(M1) Ganglioside metabolism, Glycosylation, Humans, Protein Binding, Vibrio cholerae chemistry, Vibrio cholerae genetics, Blood Group Antigens metabolism, Cholera metabolism, Cholera Toxin chemistry, G(M1) Ganglioside analogs & derivatives, Vibrio cholerae metabolism

Abstract

Cholera is a life-threatening diarrhoeal disease caused by the human pathogen Vibrio cholerae. Infection occurs after ingestion of the bacteria, which colonize the human small intestine and secrete their major virulence factor - the cholera toxin (CT). The GM1 ganglioside is considered the primary receptor of the CT, but recent studies suggest that also fucosylated receptors such as histo-blood group antigens are important for cellular uptake and toxicity. Recently, a special focus has been on the histo-blood group antigen Lewis x (Le x ), however, where and how the CT binds to Le x remains unclear. Here we report the high-resolution crystal structure (1.5 Å) of the receptor-binding B-subunits of the CT bound to the Le x trisaccharide, and complementary quantitative binding data for CT holotoxins. Le x , and also L-fucose alone, bind to the secondary binding site of the toxin, distinct from the GM1 binding site. In contrast, fucosyl-GM1 mainly binds to the primary binding site due to high-affinity interactions of its GM1 core. Le x is the first histo-blood group antigen of non-secretor phenotype structurally investigated in complex with CT. Together with the quantitative binding data, this allows unique insight into why individuals with non-secretor phenotype are more prone to severe cholera than so-called 'secretors'.

Published

2019

3. Specificity of Escherichia coli Heat-Labile Enterotoxin Investigated by Single-Site Mutagenesis and Crystallography.

Author

Heggelund JE, Heim JB, Bajc G, Hodnik V, Anderluh G, and Krengel U

Subjects

Binding Sites, Carbohydrates chemistry, Crystallography, X-Ray, Humans, Molecular Conformation, Protein Binding, Structure-Activity Relationship, Surface Plasmon Resonance, Enterotoxigenic Escherichia coli genetics, Enterotoxins chemistry, Enterotoxins genetics, Models, Molecular, Mutagenesis, Site-Directed

Abstract

Diarrhea caused by enterotoxigenic Escherichia coli (ETEC) is one of the leading causes of mortality in children under five years of age and is a great burden on developing countries. The major virulence factor of the bacterium is the heat-labile enterotoxin (LT), a close homologue of the cholera toxin. The toxins bind to carbohydrate receptors in the gastrointestinal tract, leading to toxin uptake and, ultimately, to severe diarrhea. Previously, LT from human- and porcine-infecting ETEC (hLT and pLT, respectively) were shown to have different carbohydrate-binding specificities, in particular with respect to N -acetyllactosamine-terminating glycosphingolipids. Here, we probed 11 single-residue variants of the heat-labile enterotoxin with surface plasmon resonance spectroscopy and compared the data to the parent toxins. In addition we present a 1.45 Å crystal structure of pLTB in complex with branched lacto- N -neohexaose (Galβ4GlcNAcβ6[Galβ4GlcNAcβ3]Galβ4Glc). The largest difference in binding specificity is caused by mutation of residue 94, which links the primary and secondary binding sites of the toxins. Residue 95 (and to a smaller extent also residues 7 and 18) also contribute, whereas residue 4 shows no effect on monovalent binding of the ligand and may rather be important for multivalent binding and avidity.

Published

2019

4. Crystal structure of an L chain optimised 14F7 anti-ganglioside Fv suggests a unique tumour-specificity through an unusual H-chain CDR3 architecture.

Author

Bjerregaard-Andersen K, Johannesen H, Abdel-Rahman N, Heggelund JE, Hoås HM, Abraha F, Bousquet PA, Høydahl LS, Burschowsky D, Rojas G, Oscarson S, Løset GÅ, and Krengel U

Subjects

Antibodies, Monoclonal genetics, Antibodies, Monoclonal metabolism, Crystallography, X-Ray, Humans, Immunoglobulin Heavy Chains genetics, Immunoglobulin Heavy Chains metabolism, Immunoglobulin Light Chains genetics, Immunoglobulin Light Chains metabolism, Immunoglobulin Variable Region genetics, Immunoglobulin Variable Region metabolism, Protein Conformation, Single-Chain Antibodies genetics, Single-Chain Antibodies metabolism, Antibodies, Monoclonal chemistry, G(M3) Ganglioside chemistry, Immunoglobulin Heavy Chains chemistry, Immunoglobulin Light Chains chemistry, Immunoglobulin Variable Region chemistry, Neoplasms drug therapy, Single-Chain Antibodies chemistry

Abstract

Targeted cancer immunotherapy offers increased efficacy concomitantly with reduced side effects. One antibody with promising clinical potential is 14F7, which specifically recognises the NeuGc GM3 ganglioside. This antigen is found in the plasma membrane of a range of tumours, but is essentially absent from healthy human cells. 14F7 can discriminate NeuGc GM3 from the very similar NeuAc GM3, a common component of cell membranes. The molecular basis for this unique specificity is poorly understood. Here we designed and expressed 14F7-derived single-chain Fvs (scFvs), which retained the specificity of the parent antibody. Detailed expression and purification protocols are described as well as the synthesis of the NeuGc GM3 trisaccharide. The most successful scFv construct, which comprises an alternative variable light chain (V LA ), allowed structure determination to 2.2 Å resolution. The structure gives insights into the conformation of the important CDR H3 loop and the suspected antigen binding site. Furthermore, the presence of V LA instead of the original V L elucidates how this subdomain indirectly stabilises the CDR H3 loop. The current work may serve as a guideline for the efficient production of scFvs for structure determination.

Published

2018

5. Histo-blood group antigens as mediators of infections.

Author

Heggelund JE, Varrot A, Imberty A, and Krengel U

Subjects

Animals, Gastrointestinal Diseases blood, Gastrointestinal Diseases microbiology, Gastrointestinal Diseases virology, Humans, Infections microbiology, Infections virology, Polysaccharides metabolism, Respiratory Tract Infections blood, Blood Group Antigens metabolism, Infections blood

Abstract

The critical first step of a microbial infection is usually the attachment of pathogens to host cell glycans. Targets on host tissues are in particular the histo-blood group antigens (HBGAs), which are present in rich diversity in the mucus layer and on the underlying mucosa. Recent structural and functional studies have revealed significant new insight into the molecular mechanisms, explaining why individuals with certain blood groups are at increased risk of some infections. The most prominent example of blood-group-associated diseases is cholera, caused by infection with Vibrio cholerae. Many other microbial pathogens, for example Pseudomonas aeruginosa infecting the airways, and enterotoxigenic Escherichia coli (ETEC) causing traveler's diarrhea, also bind to histo-blood group antigens, but show a less clear correlation with blood group phenotype. Yet other pathogens, for example norovirus and Helicobacter pylori, recognize HBGAs differently depending on the strain. In all cases, milk oligosaccharides can aid the hosts' defenses, acting as natural receptor decoys, and anti-infectious therapy can be designed along similar strategies. In this review, we focus on important infections of humans, but the molecular mechanisms are of general relevance to a broad range of microbial infections of humans and animals., (Copyright © 2017 Elsevier Ltd. All rights reserved.)

Published

2017

6. Towards new cholera prophylactics and treatment: Crystal structures of bacterial enterotoxins in complex with GM1 mimics.

Author

Heggelund JE, Mackenzie A, Martinsen T, Heim JB, Cheshev P, Bernardi A, and Krengel U

Subjects

Bacterial Toxins chemistry, Binding Sites, Cholera microbiology, Crystallography, X-Ray, G(M1) Ganglioside chemistry, Glycosides, Humans, Models, Molecular, Monosaccharides antagonists & inhibitors, Protein Binding, Protein Conformation drug effects, Cholera drug therapy, Cholera Toxin chemistry, Enterotoxins chemistry, Monosaccharides chemistry

Abstract

Cholera is a life-threatening disease in many countries, and new drugs are clearly needed. C-glycosidic antagonists may serve such a purpose. Here we report atomic-resolution crystal structures of three such compounds in complexes with the cholera toxin. The structures give unprecedented atomic details of the molecular interactions and show how the inhibitors efficiently block the GM1 binding site. These molecules are well suited for development into low-cost prophylactic drugs, due to their relatively easy synthesis and their resistance to glycolytic enzymes. One of the compounds links two toxin B-pentamers in the crystal structure, which may yield improved inhibition through the formation of toxin aggregates. These structures can spark the improved design of GM1 mimics, either alone or as multivalent inhibitors connecting multiple GM1-binding sites. Future developments may further include compounds that link the primary and secondary binding sites. Serving as decoys, receptor mimics may lessen symptoms while avoiding the use of antibiotics.

Published

2017

7. 1 H, 13 C, 15 N backbone assignment of the human heat-labile enterotoxin B-pentamer and chemical shift mapping of neolactotetraose binding.

Author

Hatlem D, Heggelund JE, Burschowsky D, Krengel U, and Kristiansen PE

Subjects

Amino Acid Sequence, Humans, Models, Molecular, Protein Binding, Protein Structure, Quaternary, Enterotoxins chemistry, Enterotoxins metabolism, Hot Temperature, Nuclear Magnetic Resonance, Biomolecular, Oligosaccharides metabolism, Protein Multimerization

Abstract

The major virulence factor of enterotoxigenic Escherichia coli is the heat-labile enterotoxin (LT), an AB 5 toxin closely related to the cholera toxin. LT consists of six subunits, the catalytically active A-subunit and five B-subunits arranged as a pentameric ring (LTB), which enable the toxin to bind to the epithelial cells in the intestinal lumen. LTB has two recognized binding sites; the primary binding site is responsible for anchoring the toxin to its main receptor, the GM 1 -ganglioside, while the secondary binding site recognizes blood group antigens. Herein, we report the 1 H, 13 C, 15 N main chain assignment of LTB from human isolates (hLTB; 103 a.a. per subunit, with a total molecular mass of 58.5 kDa). The secondary structure was predicted based on 13 C', 13 C α, 13 C β, 1 H N and 15 N chemical shifts and compared to a published crystal structure of LTB. Neolactotetraose (NEO) was titrated to hLTB and chemical shift perturbations were measured. The chemical shift perturbations were mapped onto the crystal structure, confirming that NEO binds to the primary binding site of hLTB and competes with GM 1 -binding. Our new data further lend support to the hypothesis that binding at the primary binding site is transmitted to the secondary binding site of the toxin, where it may influence the binding to blood group antigens.

Published

2017

8. High-Resolution Crystal Structures Elucidate the Molecular Basis of Cholera Blood Group Dependence.

Author

Heggelund JE, Burschowsky D, Bjørnestad VA, Hodnik V, Anderluh G, and Krengel U

Subjects

Base Sequence, Crystallography, X-Ray, Humans, Molecular Sequence Data, Protein Conformation, Surface Plasmon Resonance, ABO Blood-Group System chemistry, ABO Blood-Group System metabolism, Cholera blood, Cholera Toxin chemistry, Cholera Toxin metabolism

Abstract

Cholera is the prime example of blood-group-dependent diseases, with individuals of blood group O experiencing the most severe symptoms. The cholera toxin is the main suspect to cause this relationship. We report the high-resolution crystal structures (1.1-1.6 Å) of the native cholera toxin B-pentamer for both classical and El Tor biotypes, in complexes with relevant blood group determinants and a fragment of its primary receptor, the GM1 ganglioside. The blood group A determinant binds in the opposite orientation compared to previously published structures of the cholera toxin, whereas the blood group H determinant, characteristic of blood group O, binds in both orientations. H-determinants bind with higher affinity than A-determinants, as shown by surface plasmon resonance. Together, these findings suggest why blood group O is a risk factor for severe cholera.

Published

2016

9. Comprehensive analysis of blood group antigen binding to classical and El Tor cholera toxin B-pentamers by NMR.

Author

Vasile F, Reina JJ, Potenza D, Heggelund JE, Mackenzie A, Krengel U, and Bernardi A

Subjects

Binding Sites, Blood Group Antigens chemistry, Carbohydrate Conformation, Cholera Toxin genetics, Humans, Magnetic Resonance Spectroscopy, Molecular Sequence Data, Blood Group Antigens analysis, Blood Group Antigens metabolism, Cholera Toxin chemistry, Cholera Toxin metabolism

Abstract

Cholera is a diarrheal disease responsible for the deaths of thousands, possibly even hundreds of thousands of people every year, and its impact is predicted to further increase with climate change. It has been known for decades that blood group O individuals suffer more severe symptoms of cholera compared with individuals with other blood groups (A, B and AB). The observed blood group dependence is likely to be caused by the major virulence factor of Vibrio cholerae, the cholera toxin (CT). Here, we investigate the binding of ABH blood group determinants to both classical and El Tor CTB-pentamers using saturation transfer difference NMR and show that all three blood group determinants bind to both toxin variants. Although the details of the interactions differ, we see no large differences between the two toxin genotypes and observe very similar binding constants. We also show that the blood group determinants bind to a site distinct from that of the primary receptor, GM1. Transferred NOESY data confirm that the conformations of the blood group determinants in complex with both toxin variants are similar to those of reported X-ray and solution structures. Taken together, this detailed analysis provides a framework for the interpretation of the epidemiological data linking the severity of cholera infection and an individual's blood group, and brings us one step closer to understanding the molecular basis of cholera blood group dependence., (© The Author 2014. Published by Oxford University Press. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com.)

Published

2014

10. Both El Tor and classical cholera toxin bind blood group determinants.

Author

Heggelund JE, Haugen E, Lygren B, Mackenzie A, Holmner Å, Vasile F, Reina JJ, Bernardi A, and Krengel U

Subjects

Binding Sites, Humans, Nuclear Magnetic Resonance, Biomolecular, Protein Conformation, Surface Plasmon Resonance, Blood Group Antigens chemistry, Cholera Toxin chemistry

Abstract

Cholera is a disease which shows a clear blood group profile, with blood group O individuals experiencing the most severe symptoms. For a long time, the cholera toxin has been suspected to be the main culprit of this blood group dependence. Here, we show that both El Tor and classical cholera toxin B-pentamers do indeed bind blood group determinants (with equal affinities), using Surface Plasmon Resonance and NMR spectroscopy. Together with previous structural data, this confirms our earlier hypothesis as to the molecular basis of cholera blood group dependence, with an interesting twist: the shorter blood group H-determinant characteristic of blood group O individuals binds with similar binding affinity compared to the A-determinant, however, with different kinetics., (Copyright © 2012 Elsevier Inc. All rights reserved.)

Published

2012

11. The human homolog of Escherichia coli endonuclease V is a nucleolar protein with affinity for branched DNA structures.

Author

Fladeby C, Vik ES, Laerdahl JK, Gran Neurauter C, Heggelund JE, Thorgaard E, Strøm-Andersen P, Bjørås M, Dalhus B, and Alseth I

Subjects

Alternative Splicing genetics, Cell Cycle genetics, Cell Line, Cell Nucleolus enzymology, Computational Biology, Deoxyribonuclease (Pyrimidine Dimer) genetics, Gene Expression Regulation, Neoplastic, Green Fluorescent Proteins metabolism, Humans, Models, Molecular, Mutant Proteins metabolism, Neoplasms enzymology, Neoplasms genetics, Nuclear Proteins genetics, Protein Binding genetics, Protein Transport, Substrate Specificity, Transcription, Genetic, Up-Regulation genetics, DNA chemistry, DNA metabolism, Deoxyribonuclease (Pyrimidine Dimer) metabolism, Escherichia coli Proteins chemistry, Nuclear Proteins metabolism, Nucleic Acid Conformation, Sequence Homology, Amino Acid

Abstract

Loss of amino groups from adenines in DNA results in the formation of hypoxanthine (Hx) bases with miscoding properties. The primary enzyme in Escherichia coli for DNA repair initiation at deaminated adenine is endonuclease V (endoV), encoded by the nfi gene, which cleaves the second phosphodiester bond 3' of an Hx lesion. Endonuclease V orthologs are widespread in nature and belong to a family of highly conserved proteins. Whereas prokaryotic endoV enzymes are well characterized, the function of the eukaryotic homologs remains obscure. Here we describe the human endoV ortholog and show with bioinformatics and experimental analysis that a large number of transcript variants exist for the human endonuclease V gene (ENDOV), many of which are unlikely to be translated into functional protein. Full-length ENDOV is encoded by 8 evolutionary conserved exons covering the core region of the enzyme, in addition to one or more 3'-exons encoding an unstructured and poorly conserved C-terminus. In contrast to the E. coli enzyme, we find recombinant ENDOV neither to incise nor bind Hx-containing DNA. While both enzymes have strong affinity for several branched DNA substrates, cleavage is observed only with E. coli endoV. We find that ENDOV is localized in the cytoplasm and nucleoli of human cells. As nucleoli harbor the rRNA genes, this may suggest a role for the protein in rRNA gene transactions such as DNA replication or RNA transcription.

Published

2012