Your search keyword '"Heparitin Sulfate immunology"' showing total 242 results

1. Immunogenic Sulfated l-Idose Homo Oligosaccharides Elicit Neutralizing Antibody against Native Heparan Sulfate with Biomarker and Therapeutic Possibilities.

Author

Vishweshwara SS, Bhoge PR, Anand S, Raigawali R, Chandra A, Saladi SV, and Kikkeri R

Subjects

Animals, Female, Humans, Mice, Biomarkers, Cell Line, Tumor, Mice, Inbred BALB C, Oligosaccharides chemistry, Oligosaccharides pharmacology, Oligosaccharides immunology, Antibodies, Neutralizing immunology, Heparitin Sulfate chemistry, Heparitin Sulfate immunology

Abstract

Heparan sulfate (HS) is a non-immunogenic antigen, and developing antibodies against specific sulfated patterns in HS poses significant challenges. Herein, we employed an innovative immunization strategy that exploits the molecular mimicry of HS to generate antibodies against HS sequences. Mice were immunized with synthetic sulfated oligo-l-idose ( ID49 ) that mimics optimum 67% of the conserved structure of HS ligands. This immunization of ID49@CRM 197 with alum and Freund's adjuvant resulted in the production of robust IgG antibody responses targeting ID49 and cross-reactivity with the N -sulfated HS ligands compared to N -unsubstituted and N -acetate domain synthetic HS ligands. Such a pharmacological agent exhibited distinct staining of tissue sections and cell lines and induced complement-dependent cell cytotoxicity against SK-BR-3 cancer cells. Moreover, these antibodies inhibited heparin-mediated anticoagulation activity similar to that of protamine. These findings highlight the biomarker and possible therapeutic capability of the antibodies.

Published

2024

2. Identification of heparin-binding amino acid residues in antibody HS4C3 with the potential to design antibodies against heparan sulfate domains.

Author

Damen LAA, Bui TP, van Wessel T, Li Y, Straten BF, Pampiermole R, Daamen WF, Fernig DG, and van Kuppevelt TH

Subjects

Molecular Docking Simulation, Single-Chain Antibodies chemistry, Single-Chain Antibodies immunology, Single-Chain Antibodies genetics, Humans, Animals, Mutagenesis, Site-Directed, Binding Sites, Amino Acid Sequence, Heparitin Sulfate chemistry, Heparitin Sulfate immunology, Heparitin Sulfate metabolism, Heparin chemistry, Heparin metabolism

Abstract

Heparan sulfate (HS) is a linear polysaccharide with high structural and functional diversity. Detection and localization of HS in tissues can be performed using single chain variable fragment (scFv) antibodies. Although several anti-HS antibodies recognizing different sulfation motifs have been identified, little is known about their interaction with HS. In this study the interaction between the scFv antibody HS4C3 and heparin was investigated. Heparin-binding lysine and arginine residues were identified using a protect and label methodology. Site-directed mutagenesis was applied to further identify critical heparin-binding lysine/arginine residues using immunohistochemical and biochemical assays. In addition, computational docking of a heparin tetrasaccharide towards a 3-D homology model of HS4C3 was applied to identify potential heparin-binding sites. Of the 12 lysine and 15 arginine residues within the HS4C3 antibody, 6 and 9, respectively, were identified as heparin-binding. Most of these residues are located within one of the complementarity determining regions (CDR) or in their proximity. All basic amino acid residues in the CDR3 region of the heavy chain were involved in binding. Computational docking showed a heparin tetrasaccharide close to these regions. Mutagenesis of heparin-binding residues reduced or altered reactivity towards HS and heparin. Identification of heparin-binding arginine and lysine residues in HS4C3 allows for better understanding of the interaction with HS and creates a framework to rationally design antibodies targeting specific HS motifs., (© The Author(s) 2024. Published by Oxford University Press.)

Published

2024

3. Therapeutic plasma exchange for peripheral neuropathy associated with trisulfated heparan disaccharide IgM antibodies: A case series of 17 patients.

Author

Olsen GM, Tormey CA, Tseng B, Hendrickson JE, and Sostin N

Subjects

Adult, Aged, Aged, 80 and over, Disaccharides immunology, Female, Humans, Male, Middle Aged, Retrospective Studies, Heparitin Sulfate immunology, Immunoglobulin M, Plasma Exchange, Small Fiber Neuropathy immunology, Small Fiber Neuropathy therapy

Abstract

Background: Small fiber neuropathy (SFN) can be associated with autoantibodies, including those of IgM class with specificity for the trisulfated heparan disaccharide (TS-HDS) antigen. We hypothesized that, as an IgM autoantibody-mediated disorder, TS-HDS-associated SFN symptoms may be reduced with therapeutic plasma exchange (TPE)., Study Methods: This was an observational analysis of all patients referred for TPE from 2018 to 2020 following laboratory confirmation of SFN with TS-HDS autoantibodies; a loading course of 3 to 5 procedures over 2 weeks was completed, with some patients returning for monthly procedures. The following data were collected: demographics, symptoms and duration, TS-HDS levels, skin biopsy results, reported responses to TPE, and TPE-associated adverse events., Results: Of the 17 subjects, 12 (71%) were female and the mean age was 57.5 years (range 27-94). The most common reported symptom was lower extremity paresthesia (88% of subjects). The mean number of TPE procedures completed per subject was 9 (range 3-18), with 71% (12/17) reporting symptomatic improvement or slowed disease progression. About 15% of procedures were associated with an adverse event, with vasovagal reactions being the most common; 53% of patients had at least one adverse event., Conclusions: Given a reported symptomatic response rate of more than 70%, TPE may be a treatment option for individuals with autoimmune-mediated SFN associated with increased titers of TS-HDS IgM autoantibodies. Since TPE-associated adverse events appear common in this population, close monitoring during procedures is warranted., (© 2021 Wiley Periodicals LLC.)

Published

2022

4. Glycosaminoglycan binding by arboviruses: a cautionary tale.

Author

Alcorn MDH and Klimstra WB

Subjects

Animals, Humans, Arbovirus Infections virology, Arboviruses immunology, Heparitin Sulfate immunology

Abstract

Arboviruses are medically important arthropod-borne viruses that cause a range of diseases in humans from febrile illness to arthritis, encephalitis and hemorrhagic fever. Given their transmission cycles, these viruses face the challenge of replicating in evolutionarily divergent organisms that can include ticks, flies, mosquitoes, birds, rodents, reptiles and primates. Furthermore, their cell attachment receptor utilization may be affected by the opposing needs for generating high and sustained serum viremia in vertebrates such that virus particles are efficiently collected during a hematophagous arthropod blood meal but they must also bind sufficiently to cellular structures on divergent organisms such that productive infection can be initiated and viremia generated. Sulfated polysaccharides of the glycosaminoglycan (GAG) groups, primarily heparan sulfate (HS), have been identified as cell attachment moieties for many arboviruses. Original identification of GAG binding as a phenotype of arboviruses appeared to involve this attribute arising solely as a consequence of adaptation of virus isolates to growth in cell culture. However, more recently, naturally circulating strains of at least one arbovirus, eastern equine encephalitis, have been shown to bind HS efficiently and the GAG binding phenotype continues to be associated with arbovirus infection in published studies. If GAGs are attachment receptors for many naturally circulating arboviruses, this could lead to development of broad-spectrum antiviral therapies through blocking of the virus-GAG interaction. This review summarizes the available data for GAG/HS binding as a phenotype of naturally circulating arbovirus strains emphasizing the importance of avoiding tissue culture amplification and artifactual phenotypes during their isolation.

Published

2022

5. Morphological cell profiling of SARS-CoV-2 infection identifies drug repurposing candidates for COVID-19.

Author

Mirabelli C, Wotring JW, Zhang CJ, McCarty SM, Fursmidt R, Pretto CD, Qiao Y, Zhang Y, Frum T, Kadambi NS, Amin AT, O'Meara TR, Spence JR, Huang J, Alysandratos KD, Kotton DN, Handelman SK, Wobus CE, Weatherwax KJ, Mashour GA, O'Meara MJ, Chinnaiyan AM, and Sexton JZ

Subjects

Animals, COVID-19 immunology, COVID-19 prevention & control, COVID-19 virology, Caco-2 Cells, Cell Line, Tumor, Chlorocebus aethiops, Dose-Response Relationship, Drug, Drug Discovery, Drug Repositioning methods, Epithelial Cells, Heparitin Sulfate antagonists & inhibitors, Heparitin Sulfate immunology, Heparitin Sulfate metabolism, Hepatocytes, High-Throughput Screening Assays, Humans, SARS-CoV-2 growth & development, SARS-CoV-2 pathogenicity, Vero Cells, COVID-19 Drug Treatment, Antiviral Agents pharmacology, Immunologic Factors pharmacology, Lactoferrin pharmacology, SARS-CoV-2 drug effects, Virus Internalization drug effects, Virus Replication drug effects

Abstract

The global spread of the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), and the associated disease COVID-19, requires therapeutic interventions that can be rapidly identified and translated to clinical care. Traditional drug discovery methods have a >90% failure rate and can take 10 to 15 y from target identification to clinical use. In contrast, drug repurposing can significantly accelerate translation. We developed a quantitative high-throughput screen to identify efficacious agents against SARS-CoV-2. From a library of 1,425 US Food and Drug Administration (FDA)-approved compounds and clinical candidates, we identified 17 hits that inhibited SARS-CoV-2 infection and analyzed their antiviral activity across multiple cell lines, including lymph node carcinoma of the prostate (LNCaP) cells and a physiologically relevant model of alveolar epithelial type 2 cells (iAEC2s). Additionally, we found that inhibitors of the Ras/Raf/MEK/ERK signaling pathway exacerbate SARS-CoV-2 infection in vitro. Notably, we discovered that lactoferrin, a glycoprotein found in secretory fluids including mammalian milk, inhibits SARS-CoV-2 infection in the nanomolar range in all cell models with multiple modes of action, including blockage of virus attachment to cellular heparan sulfate and enhancement of interferon responses. Given its safety profile, lactoferrin is a readily translatable therapeutic option for the management of COVID-19., Competing Interests: The authors declare no competing interest., (Copyright © 2021 the Author(s). Published by PNAS.)

Published

2021

6. Identification of cell-surface glycans that mediate motility-dependent binding and internalization of Pseudomonas aeruginosa by phagocytes.

Author

Sanchez H, Hopkins D, Demirdjian S, Gutierrez C, O'Toole GA, Neelamegham S, and Berwin B

Subjects

Cell Line, Tumor, Cells, Cultured, HL-60 Cells, Heparitin Sulfate immunology, Humans, Immunity, Innate immunology, Interleukin-1beta immunology, Monocytes immunology, Phagocytosis immunology, THP-1 Cells, Phagocytes immunology, Polysaccharides immunology, Pseudomonas Infections immunology, Pseudomonas aeruginosa immunology

Abstract

Phagocytic cells are critical to host defense against Pseudomonas aeruginosa, a Gram-negative bacterium that is an opportunistic pathogen. Accordingly, susceptible individuals frequently have impaired innate immune responses, including those with cystic fibrosis or neutropenia. Previous studies identified that the downregulation, or loss, of bacterial flagellar motility enables bacteria to evade interactions with phagocytic cells that result in phagocytic uptake of the bacteria. However, the mechanistic bases for motility-dependent interactions between P. aeruginosa and host cell surfaces that lead to phagocytic uptake of the bacteria are poorly understood. A recent insight is that exogenous addition of a negatively charged phospholipid, phosphatidylinositol-(3,4,5)-triphosphate (PIP 3 ), promotes the engagement of non-motile strains of P. aeruginosa with phagocytes leading to uptake of the bacteria. Thus, we hypothesized that the engagement of P. aeruginosa by phagocytic cells is mediated by motility-dependent interactions with cell-surface polyanions. Here we report that endogenous polyanionic N-linked glycans and heparan sulfate mediate bacterial binding of P. aeruginosa by human monocytic cells. These specific interactions resulted in P. aeruginosa phagocytosis, bacterial type 3 secretion system (T3SS)-mediated cellular intoxication and the IL-1β response of host innate immune cells. Importantly, the bacterial interactions with the glycans were motility-dependent and could be recapitulated with purified, immobilized glycans. Therefore, this work describes novel interactions of P. aeruginosa with specific phagocyte cell-surface glycans that modulate relevant host innate immune responses to the bacteria, including phagocytosis, inflammation and cytotoxicity., (Copyright © 2020 Elsevier Ltd. All rights reserved.)

Published

2021

7. Construction and evaluation of an antibody phage display library targeting heparan sulfate.

Author

Damen LAA, van de Westerlo EMA, Versteeg EMM, van Wessel T, Daamen WF, and van Kuppevelt TH

Subjects

Animals, Binding Sites, Bioprospecting, Enzyme-Linked Immunosorbent Assay, Epitopes chemistry, Epitopes immunology, Heparin metabolism, Heparitin Sulfate metabolism, Kidney immunology, Kidney metabolism, Male, Rats, Wistar, Single-Chain Antibodies chemistry, Single-Chain Antibodies metabolism, Single-Domain Antibodies genetics, Single-Domain Antibodies metabolism, Heparitin Sulfate immunology, Peptide Library, Single-Chain Antibodies immunology, Single-Domain Antibodies chemistry

Abstract

Heparan sulfate (HS) is a linear polysaccharide with high structural diversity. Different HS epitopes have been detected and localized using single chain variable fragment (scFv) antibodies from a 'single pot' phage display library containing a randomized complementarity determining region of the heavy chain (CDR3). In this study, we created a new library containing anti-HS scFvs that all harbor a dp-38 heavy chain segment where the CDR3 region was engineered to contain the XBBXBX heparin binding consensus site (X = any amino acid, B = R, K or H). The library contained ~1.73 × 10 6 unique antibodies and was biopanned against HS from several sources. The selected antibodies were sequenced and chemically/immunohistologically characterized. A number of 67 anti-HS scFv antibodies were selected, of which 31 contained a XBBXBX CDR3 sequence. There was a clear preference for glycine at the first and proline at the fourth position of the CDR3. The sequence GZZP(R/K)X (Z = R, K or H, but may also contain N, S, or Q) was unusually overrepresented. Selected antibodies reacted with HS/heparin, but not with other glycosaminoglycans. Antibodies reacted differentially with respect to N-, 2-O, or 6-O-desulfated heparin preparations, and showed distinct topologies of HS epitopes in rat kidney sections. The library may be instrumental in the selection of a large pool of HS epitope-specific antibodies, and - since all antibodies differ only in their 6 amino acid CDR region - may be a tool for a rational design of antibodies recognizing specific HS sulfation patterns.

Published

2020

8. Immunomodulatory Activities of the Heparan Sulfate Mimetic PG545.

Author

Bendersky V, Yang Y, and Brennan TV

Subjects

Humans, Neoplasms enzymology, Neoplasms immunology, Neoplasms pathology, Glucuronidase antagonists & inhibitors, Heparitin Sulfate immunology, Heparitin Sulfate pharmacology, Neoplasms drug therapy, Saponins immunology, Saponins pharmacology

Abstract

Heparanase regulates multiple biological activities that enhance tumor growth and metastatic spread. Heparanase cleaves and degrades heparan sulfate (HS), a key structural component of the extracellular matrix that serves as a barrier to cell invasion and also as a reservoir for cytokines and growth factors critical for tumor growth and metastasis. For this reason, heparanase is an attractive target for the development of novel anti-cancer therapies. Pixatimod (PG545), a heparanase inhibitor, has shown promising results in the treatment of multiple tumor types. PG545 offers a diversity of mechanisms of action in tumor therapy that include angiogenic inhibition, inhibition of growth factor release, inhibition of tumor cell migration, tumor cell apoptosis, activation of ER stress response, dysregulation of autophagy, and NK cell activation. Further investigation into the role that heparanase and its inhibitors play in tumor therapy can lead to the development of effective tumor therapies.

Published

2020

9. ROP9, MIC3, and SAG2 are heparin-binding proteins in Toxoplasma gondii and involved in host cell attachment and invasion.

Author

Zhang D, Jiang N, and Chen Q

Subjects

Animals, Antibodies, Protozoan, Antimicrobial Cationic Peptides, Blood Proteins, Carrier Proteins, Female, Membrane Glycoproteins pharmacology, Membrane Proteins pharmacology, Mice, Mice, Inbred BALB C, Protozoan Proteins pharmacology, Recombinant Proteins, Vaccines, DNA, Antigens, Protozoan pharmacology, Heparitin Sulfate immunology, Immunization methods, Protozoan Vaccines pharmacology, Toxoplasma immunology

Abstract

Toxoplasma gondii (T. gondii) is an obligatory intracellular parasite that can infect varieties of warm-blooded animals, including humans and birds. Heparan sulfate (HS) is widely distributed on the eukaryotic cell surface of vertebrates and can inhibit T. gondii invasion. In this study, we investigated the transcription and expression of the level of TgROP9, TgMIC3, and TgSAG2 in T. gondii RH strain, and found that the expression levels of these three proteins in invading parasites were higher compared to those free ranging parasites. The recombinant proteins showed specific binding activity to both heparin and host cell surface. Incubation of these proteins with the host cells could block T. gondiiinvasion. Furthermore, protein-specific antibodies also blocked parasite invasion. Antibodies in the sera of T. gondii infected individuals recognized the recombinant TgROP9, TgMIC3, and TgSAG2, which suggested the exposure of these proteins to human immune system. Mice immunized with the three proteins exhibited protective immunity against lethal challenge. The data collectively suggested that these parasitic proteins may be used as candidate antigens for development of anti-toxoplasmosis vaccine., (Copyright © 2019 Elsevier B.V. All rights reserved.)

Published

2019

10. A mutant-cell library for systematic analysis of heparan sulfate structure-function relationships.

Author

Qiu H, Shi S, Yue J, Xin M, Nairn AV, Lin L, Liu X, Li G, Archer-Hartmann SA, Dela Rosa M, Galizzi M, Wang S, Zhang F, Azadi P, van Kuppevelt TH, Cardoso WV, Kimata K, Ai X, Moremen KW, Esko JD, Linhardt RJ, and Wang L

Subjects

Animals, Antibody Specificity, Cells, Cultured, Endothelium, Vascular cytology, Endothelium, Vascular immunology, Heparitin Sulfate genetics, Heparitin Sulfate metabolism, Lung cytology, Lung immunology, Mice, Inbred C57BL, Peptide Library, Signal Transduction, Structure-Activity Relationship, Sulfur chemistry, Antibodies immunology, Endothelium, Vascular metabolism, Epitopes immunology, Heparitin Sulfate chemistry, Heparitin Sulfate immunology, Lung metabolism, Mutation

Abstract

Heparan sulfate (HS) is a complex linear polysaccharide that modulates a wide range of biological functions. Elucidating the structure-function relationship of HS has been challenging. Here we report the generation of an HS-mutant mouse lung endothelial cell library by systematic deletion of HS genes expressed in the cell. We used this library to (1) determine that the strictly defined fine structure of HS, not its overall degree of sulfation, is more important for FGF2-FGFR1 signaling; (2) define the epitope features of commonly used anti-HS phage display antibodies; and (3) delineate the fine inter-regulation networks by which HS genes modify HS and chain length in mammalian cells at a cell-type-specific level. Our mutant-cell library will allow robust and systematic interrogation of the roles and related structures of HS in a cellular context.

Published

2018

11. Isolation of Antibodies to Heparan Sulfate on Glypicans by Phage Display.

Author

Kim H and Ho M

Subjects

Heparitin Sulfate chemistry, Heparitin Sulfate immunology, Peptide Library, Single-Chain Antibodies chemistry, Single-Chain Antibodies genetics, Single-Chain Antibodies immunology

Abstract

Heparan sulfate (HS) plays an important role in development and disease. It interacts with many growth factors, chemokines, and other ligands known to be important for cell growth, motility, and differentiation. However, isolating an antibody to HS in mice, rabbits, or humans is difficult due to the poor immunogenicity of HS. Phage display is a major antibody engineering technology that allows the selection of antibodies for poorly immunogenic or highly conserved antigens. This protocol contains detailed procedures for HS antigen preparation and isolation of a phage displayed human single-chain Fv (HS20) that binds HS on glypican-3 (GPC3), and analysis of the selected phage antibody. It is conceivable that the procedures described in this protocol may be applicable to the isolation of antibodies for a variety of HS molecules. © 2018 by John Wiley & Sons, Inc., (© 2018 John Wiley & Sons, Inc.)

Published

2018

12. Heparan Sulfate Proteoglycans as Relays of Neuroinflammation.

Author

O'Callaghan P, Zhang X, and Li JP

Subjects

Alzheimer Disease pathology, Animals, Brain pathology, Cytokines immunology, Glucuronidase immunology, Heparitin Sulfate immunology, Humans, Inflammation pathology, Neuroglia pathology, Neuroimmunomodulation, Toll-Like Receptor 4 immunology, Alzheimer Disease immunology, Brain immunology, Heparan Sulfate Proteoglycans immunology, Immunity, Innate, Inflammation immunology, Neuroglia immunology

Abstract

Heparan sulfate proteoglycans (HSPGs) are implicated as inflammatory mediators in a variety of settings, including chemokine activation, which is required to recruit circulating leukocytes to infection sites. Heparan sulfate (HS) polysaccharide chains are highly interactive and serve co-receptor roles in multiple ligand:receptor interactions. HS may also serve as a storage depot, sequestering ligands such as cytokines and restricting their access to binding partners. Heparanase, through its ability to fragment HS chains, is a key regulator of HS function and has featured prominently in studies of HS's involvement in inflammatory processes. This review focuses on recent discoveries regarding the role of HSPGs, HS, and heparanase during inflammation, with particular focus on the brain. HS chains emerge as critical go-betweens in multiple aspects of the inflammatory response-relaying signals between receptors and cells. The molecular interactions proposed to occur between HSPGs and the pathogen receptor toll-like receptor 4 (TLR4) are discussed, and we summarize some of the contrasting roles that HS and heparanase have been assigned in diseases associated with chronic inflammatory states, including Alzheimer's disease (AD). We conclude by briefly discussing how current knowledge could potentially be applied to augment HS-mediated events during sustained neuroinflammation, which contributes to neurodegeneration in AD.

Published

2018

13. The Role of Heparan Sulfate in Inflammation, and the Development of Biomimetics as Anti-Inflammatory Strategies.

Author

Farrugia BL, Lord MS, Melrose J, and Whitelock JM

Subjects

Animals, Anti-Inflammatory Agents chemistry, Biomimetics methods, Chemokines immunology, Glucuronidase antagonists & inhibitors, Glucuronidase immunology, Heparitin Sulfate chemistry, Humans, Inflammation drug therapy, Anti-Inflammatory Agents immunology, Anti-Inflammatory Agents pharmacology, Drug Discovery methods, Heparitin Sulfate immunology, Heparitin Sulfate pharmacology, Immunity, Innate drug effects, Inflammation immunology

Abstract

Key events that occur during inflammation include the recruitment, adhesion, and transmigration of leukocytes from the circulation to the site of inflammation. These events are modulated by chemokines, integrins, and selectins and the interaction of these molecules with glycosaminoglycans, predominantly heparan sulfate (HS). The development of HS/heparin mimetics that interfere or inhibit the interactions that occur between glycosaminoglycans and modulators of inflammation holds great potential for use as anti-inflammatory therapeutics. This review will detail the role of HS in the events that occur during inflammation, their interaction and modulation of inflammatory mediators, and the current advances in the development of HS/heparin mimetics as anti-inflammatory biotherapeutics.

Published

2018

14. Protein array autoantibody profiles to determine diagnostic markers for neuropsychiatric systemic lupus erythematosus.

Author

van der Meulen PM, Barendregt AM, Cuadrado E, Magro-Checa C, Steup-Beekman GM, Schonenberg-Meinema D, Van den Berg JM, Li QZ, Baars PA, Wouters D, Voskuyl AE, Ten Berge IRJM, Huizinga TWJ, and Kuijpers TW

Subjects

Adult, Autoantibodies immunology, Biomarkers blood, Case-Control Studies, Female, Heparitin Sulfate immunology, Histones immunology, Humans, Immunoglobulin G immunology, Lupus Vasculitis, Central Nervous System immunology, Male, Middle Aged, Protein Array Analysis, Vimentin immunology, Autoantibodies blood, Lupus Vasculitis, Central Nervous System diagnosis

Abstract

Objective: The aim was to investigate the association between autoantibodies (autoAbs) and neuropsychiatric (NP) involvement in patients with SLE and to evaluate whether any autoAb or a combination of these autoAbs could indicate the underlying pathogenic process., Methods: Using a multiplexed protein array for 94 antigens, we compared the serum autoAb profiles of 69 NPSLE patients, 203 SLE patients without NP involvement (non-NPSLE) and 51 healthy controls. Furthermore, we compared the profiles of NPSLE patients with clinical inflammatory (n = 38) and ischaemic (n = 31) NP involvement., Results: In total, 75 IgG and 47 IgM autoAbs were associated with SLE patients in comparison with healthy controls. Comparing NPSLE with non-NPSLE and healthy control sera, 9 IgG (amyloid, cardiolipin, glycoprotein 2, glycoprotein 210, heparin, heparan sulphate, histone H2A, prothrombin protein and vimentin) and 12 IgM (amyloid, cardiolipin, centromere protein A, collagen II, histones H2A and H2B, heparan sulphate, heparin, mitochondrial 2, nuclear Mi-2, nucleoporin 62 and vimentin) autoAbs were present at significantly different levels in NPSLE. The combination of IgG autoAbs against heparan sulphate, histone H2B and vimentin could differentiate NPSLE from non-NPSLE (area under the curve 0.845, 99.97% CI: 0.756, 0.933; P < 0.0001). Compared with non-NPSLE, four IgG and seven IgM autoAbs were significantly associated with inflammatory NPSLE. In ischaemic NPSLE, three IgG and three IgM autoAbs were significantly different from non-NPSLE patients., Conclusion: In our cohort, the presence of high levels of anti-heparan sulphate and anti-histone H2B combined with low levels of anti-vimentin IgG autoAbs is highly suggestive of NPSLE. These results need to be validated in external cohorts., (© The Author 2017. Published by Oxford University Press on behalf of the British Society for Rheumatology. All rights reserved. For Permissions, please email: journals.permissions@oup.com)

Published

2017

15. Anti-heparan sulfate antibody and functional loss of glomerular heparan sulfate proteoglycans in lupus nephritis.

Author

Kim HJ, Hong YH, Kim YJ, Kim HS, Park JW, Do JY, Kim KJ, Bae SW, Kim CW, and Lee CK

Subjects

Adult, Basement Membrane metabolism, Case-Control Studies, Enzyme-Linked Immunosorbent Assay, Female, Glomerular Filtration Rate, Glomerulonephritis, Membranous immunology, Humans, Kidney Glomerulus immunology, Kidney Glomerulus metabolism, Lupus Erythematosus, Systemic complications, Lupus Erythematosus, Systemic immunology, Lupus Nephritis physiopathology, Male, Middle Aged, Nephritis immunology, Proteinuria etiology, Proteinuria immunology, Young Adult, Heparan Sulfate Proteoglycans metabolism, Heparitin Sulfate immunology, Immunoglobulin G immunology, Lupus Nephritis immunology

Abstract

Background The purpose of this study was to evaluate the features of heparan sulfate proteoglycans (HSPGs) as agrins of the glomerular basement membrane (GBM) and circulating anti-heparan sulfate (HS) antibodies in lupus nephritis, comparing titers among the following groups: lupus nephritis (LN), non-renal lupus, non-lupus nephritis, and healthy controls. Methods The stage of nephritis was determined based on the kidney biopsy. Alcian blue staining and immunohistochemical (IHC) staining for agrin were performed for histological evaluation of GBM HSPGs in normal glomeruli, non-lupus membranous glomerulonephritis (MGN), and lupus MGN. The results were used for measurement of the serum anti-HS antibody titers using an enzyme-linked immunosorbent assay (ELISA) in the following groups: 38 healthy controls, 38 non-lupus nephritis, 37 non-renal lupus, and 38 LN. Results Glomerulus HSPGs were stained bluish-green along the GBM with Alcian blue. However, IHC staining against agrin was almost completely negative in the lupus MGN group compared with the normal and non-lupus MGN groups, which showed brown staining of GBM. A higher level of anti-HS IgG was detected in LN compared with other groups, respectively. Higher titers were associated with the presence of SLE and nephritis. A higher degree of proteinuria normalized to glomerular filtration rate (eGFR) was observed in association with higher anti-HS antibody titers in LN. Conclusion This study demonstrated a functional loss of GBM HSPGs and higher levels of circulating anti-HS antibodies as a characteristic feature of lupus nephritis, suggesting their involvement in the pathogenesis of lupus nephritis and proteinuria.

Published

2017

16. Glomerular basement membrane heparan sulfate in health and disease: A regulator of local complement activation.

Author

Borza DB

Subjects

Agrin genetics, Agrin immunology, Animals, Collagen Type IV genetics, Collagen Type IV immunology, Complement C3b genetics, Complement C3b metabolism, Complement Factor H genetics, Complement Factor H metabolism, Glomerular Basement Membrane metabolism, Glomerulonephritis, Membranous genetics, Glomerulonephritis, Membranous pathology, Heparitin Sulfate metabolism, Humans, Laminin genetics, Laminin immunology, Lupus Nephritis genetics, Lupus Nephritis pathology, Membrane Glycoproteins genetics, Membrane Glycoproteins immunology, Signal Transduction, Static Electricity, Complement Activation, Gene Expression Regulation immunology, Glomerular Basement Membrane immunology, Glomerulonephritis, Membranous immunology, Heparitin Sulfate immunology, Lupus Nephritis immunology

Abstract

The glomerular basement membrane (GBM) is an essential component of the glomerular filtration barrier. Heparan sulfate proteoglycans such as agrin are major components of the GBM, along with α345(IV) collagen, laminin-521 and nidogen. A loss of GBM heparan sulfate chains is associated with proteinuria in several glomerular diseases and may contribute to the underlying pathology. As the major determinants of the anionic charge of the GBM, heparan sulfate chains have been thought to impart charge selectivity to the glomerular filtration, a view challenged by the negligible albuminuria in mice that lack heparan sulfate in the GBM. Recent studies provide increasing evidence that heparan sulfate chains modulate local complement activation by recruiting complement regulatory protein factor H, the major inhibitor of the alternative pathway in plasma. Factor H selectively inactivates C3b bound to surfaces bearing host-specific polyanions such as heparan sulfate, thus limiting complement activation on self surfaces such as the GBM, which are not protected by cell-bound complement regulators. We discuss mechanisms whereby the acquired loss of GBM heparan sulfate can impair the local regulation of the alternative pathway, exacerbating complement activation and glomerular injury in immune-mediated kidney diseases such as membranous nephropathy and lupus nephritis., (Copyright © 2016 Elsevier B.V. All rights reserved.)

Published

2017

17. Cross-Reactivity Between Heparin and Danaparoid Antibodies in Cardiac Surgery.

Author

Ronchard T, Salaun E, Theron A, Grisoli D, Jaussaud N, Collart F, Habib G, and Camoin-Jau L

Subjects

Anticoagulants immunology, Anticoagulants therapeutic use, Chondroitin Sulfates therapeutic use, Cross Reactions, Dermatan Sulfate therapeutic use, Heparin adverse effects, Heparitin Sulfate therapeutic use, Humans, Male, Middle Aged, Thrombocytopenia immunology, Cardiac Surgical Procedures, Chondroitin Sulfates immunology, Dermatan Sulfate immunology, Heart Valve Diseases surgery, Heparin immunology, Heparitin Sulfate immunology, Thrombocytopenia complications

Abstract

Management of heparin-induced thrombocytopenia (HIT) entails cessation of heparin and initiation of a nonheparin parenteral anticoagulant such as danaparoid. Danaparoid cross-reactivity with HIT antibodies is an uncommon complication of treatment of HIT. We report the case of confirmed HIT and in vivo cross-reactivity with danaparoid, complicating severe sepsis due to an infectious endocarditis treated by cardiac surgery., (Copyright © 2017 The Society of Thoracic Surgeons. Published by Elsevier Inc. All rights reserved.)

Published

2017

18. Epitope mapping by a Wnt-blocking antibody: evidence of the Wnt binding domain in heparan sulfate.

Author

Gao W, Xu Y, Liu J, and Ho M

Subjects

Animals, Antibodies, Monoclonal metabolism, Antibody Specificity, Binding Sites, CHO Cells, Carbohydrate Sequence, Cell Line, Cricetulus, Glypicans chemistry, Glypicans immunology, Glypicans metabolism, Heparitin Sulfate metabolism, Humans, L Cells, Mice, Oligosaccharides chemistry, Oligosaccharides immunology, Oligosaccharides metabolism, Protein Binding, Protein Domains, Signal Transduction, Wnt Proteins metabolism, Antibodies, Blocking metabolism, Epitope Mapping methods, Heparitin Sulfate chemistry, Heparitin Sulfate immunology, Wnt Proteins antagonists & inhibitors, Wnt Proteins immunology

Abstract

Heparan sulfate (HS) is a polysaccharide known to modulate many important biological processes, including Wnt signaling. However, the biochemical interaction between HS and Wnt molecules is not well characterized largely due to the lack of suitable methods. To determine the Wnt binding domain in HS, we used a Wnt signaling-inhibitory antibody (HS20) and a panel of synthetic HS oligosaccharides with distinct lengths and sulfation modifications. We found that the binding of HS20 to heparan sulfate required sulfation at both the C2 position (2-O-sulfation) and C6 position (6-O-sulfation). The oligosaccharides with the greatest competitive effect for HS20 binding were between six and eight saccharide residues in length. Additionally, a four residue-long oligosaccharide could also be recognized by HS20 if an additional 3-O-sulfation modification was present. Furthermore, similar oligosaccharides with 2-O, 6-O and 3-O-sulfations showed inhibition for Wnt activation. These results have revealed that HS20 and Wnt recognize a HS structure containing IdoA2S and GlcNS6S, and that the 3-O-sulfation in GlcNS6S3S significantly enhances the binding of both HS20 and Wnt. This study provides the evidence for identifying the Wnt binding domain in HS and suggests a therapeutic approach to target the interaction of Wnt and HS in cancer and other diseases.

Published

2016

19. Heparanase augments inflammatory chemokine production from colorectal carcinoma cell lines.

Author

Tsunekawa N, Higashi N, Kogane Y, Waki M, Shida H, Nishimura Y, Adachi H, Nakajima M, and Irimura T

Subjects

Catalysis, Cell Line, Tumor, Enzyme Activation, Humans, Chemokines immunology, Colorectal Neoplasms enzymology, Colorectal Neoplasms immunology, Glucuronidase immunology, Heparitin Sulfate immunology, Inflammasomes immunology

Abstract

To explore possible roles of heparanase in cancer-host crosstalk, we examined whether heparanase influences expression of inflammatory chemokines in colorectal cancer cells. Murine colorectal carcinoma cells incubated with heparanase upregulated MCP-1, KC, and RANTES genes and released MCP-1 and KC proteins. Heparanase-dependent production of IL-8 was detected in two human colorectal carcinoma cell lines. Addition of a heparanase inhibitor Heparastatin (SF4) did not influence MCP-1 production, while both latent and mature forms of heparanase augmented MCP-1 release, suggesting that heparanase catalytic activity was dispensable for MCP-1 production. In contrast, addition of heparin to the medium suppressed MCP-1 release in a dose-dependent manner. Similarly, targeted suppression of Ext1 by RNAi significantly suppressed cell surface expression of heparan sulfate and MCP-1 production in colon 26 cells. Taken together, it is concluded that colon 26 cells transduce the heparanase-mediated signal through heparan sulfate binding. We propose a novel function for heparanase independent of its endoglycosidase activity, namely as a stimulant for chemokine production., (Copyright © 2015 Elsevier Inc. All rights reserved.)

Published

2016

20. Heparan sulfate phage display antibodies recognise epitopes defined by a combination of sugar sequence and cation binding.

Author

Solari V, Rudd TR, Guimond SE, Powell AK, Turnbull JE, and Yates EA

Subjects

Animals, Carbohydrate Conformation, Carbohydrate Sequence, Cations immunology, Cell Line, Enzyme-Linked Immunosorbent Assay, Epitopes chemistry, Heparitin Sulfate chemistry, Humans, Mice, Peptide Library, Antibodies immunology, Epitopes immunology, Heparitin Sulfate immunology

Abstract

Phage display antibodies are widely used to follow heparan sulfate (HS) expression in tissues and cells. We demonstrate by ELISA, that cations alter phage display antibody binding profiles to HS and this is mediated by changes in polysaccharide conformation, demonstrated by circular dichroism spectroscopy. Native HS structures, expressed on the cell surfaces of neuroblastoma and fibroblast cells, also exhibited altered antibody binding profiles following exposure to low mM concentrations of these cations. Phage display antibodies recognise conformationally-defined HS epitopes, rather than sequence alone, as has been assumed, and resemble proteins in being sensitive to changes in both charge distribution and conformation following binding of cations to HS polysaccharides.

Published

2015

21. The role of heparan sulfate as determining pathogenic factor in complement factor H-associated diseases.

Author

Loeven MA, Rops AL, Berden JH, Daha MR, Rabelink TJ, and van der Vlag J

Subjects

Complement Factor H chemistry, Complement Factor H metabolism, Heparitin Sulfate chemistry, Heparitin Sulfate metabolism, Humans, Organ Specificity, Complement Factor H immunology, Heparitin Sulfate immunology, Kidney Diseases immunology

Abstract

Complement factor H (FH) systemically inhibits excessive complement activation in the microenvironment of host cells, but for instance not on microbes. This self-recognition is mediated by two binding sites that recognize distinctly sulfated heparan sulfate (HS) domains. The interaction with HS not only concentrates FH on host cells, but directly affects its activity, evoking novel models of conformational activation. Genetic aberrations in the HS-binding domains systemically disturb the protective function of FH, yet the resulting loss of complement control affects mainly ocular and renal tissues. Recent results suggest that the specific expression of HS domains in these tissues restricts the interaction of HS to a single binding site within FH. This lack of redundancy could predispose eyes and kidneys to complement-mediated damage, making HS a central determinant for FH-associated diseases., (Copyright © 2014 Elsevier Ltd. All rights reserved.)

Published

2015

22. Use of flow cytometry for characterization and fractionation of cell populations based on their expression of heparan sulfate epitopes.

Author

Holley RJ, Smith RA, van de Westerlo EM, Pickford CE, Merry CL, and van Kuppevelt TH

Subjects

Animals, Antibody Specificity, Cell Separation, Mice, Staining and Labeling, Cell Fractionation methods, Epitopes immunology, Flow Cytometry methods, Heparitin Sulfate immunology

Abstract

The ability to characterize alterations in heparan sulfate (HS) structure during development or as a result of loss or mutation of one or more components of the HS biosynthetic pathway is essential for broad understanding of the effects these changes may have on cell/tissue function. The use of anti-HS antibodies provides an opportunity to study HS chain composition in situ, with a multitude of different antibodies having been generated that recognize subtle differences in HS patterning, with the number and positioning of sulfate groups influencing antibody binding affinity. Flow cytometry is a valuable technique to enable the rapid characterization of the changes in HS-specific antibody binding in situ, allowing multiple cell types to be directly compared. Additionally fluorescent-activated cell sorting (FACS) allows fractionation of cells based on their HS-epitope expression.

Published

2015

23. Heparan Sulfate Proteoglycan Metabolism and the Fate of Grafted Tissues.

Author

Platt JL, Wrenshall LE, Johnson GB, and Cascalho M

Subjects

Complement Activation drug effects, Complement System Proteins drug effects, Complement System Proteins genetics, Dendritic Cells drug effects, Dendritic Cells immunology, Dendritic Cells pathology, Endothelial Cells drug effects, Endothelial Cells immunology, Endothelial Cells pathology, Extracellular Matrix drug effects, Extracellular Matrix metabolism, Gene Expression Regulation, Graft Rejection genetics, Graft Rejection immunology, Graft Rejection pathology, Heparan Sulfate Proteoglycans immunology, Heparitin Sulfate immunology, Heparitin Sulfate pharmacology, Humans, Leukocytes drug effects, Leukocytes immunology, Leukocytes pathology, Signal Transduction, Systemic Inflammatory Response Syndrome genetics, Systemic Inflammatory Response Syndrome immunology, Systemic Inflammatory Response Syndrome pathology, Toll-Like Receptor 4 genetics, Toll-Like Receptor 4 immunology, Graft Rejection metabolism, Heparan Sulfate Proteoglycans metabolism, Heparitin Sulfate metabolism, Systemic Inflammatory Response Syndrome metabolism, Tissue Transplantation

Abstract

Tissue and organ transplants between genetically distinct individuals are always or nearly always rejected. The universality and speed of transplant rejection distinguishes this immune response from all others. Although this distinction is incompletely understood, some efforts to shed light on transplant rejection have revealed broader insights, including a relationship between activation of complement in grafted tissues, the metabolism of heparan sulfate proteoglycan and the nature of immune and inflammatory responses that ensue. Complement activation on cell surfaces, especially on endothelial cell surfaces, causes the shedding heparan sulfate, an acidic saccharide, from the cell surface and neighboring extracellular matrix. Solubilized in this way, heparan sulfate can activate leukocytes via toll like receptor-4, triggering inflammatory responses and activating dendritic cells, which migrate to regional lymphoid organs where they spark and to some extent govern cellular immune responses. In this way local ischemia, tissue injury and infection, exert systemic impact on immunity. Whether or in what circumstances this series of events explains the distinct characteristics of the immune response to transplants is still unclear but the events offer insight into the inception of immunity under the sub-optimal conditions accompanying infection and mechanisms by which infection and tissue injury engender systemic inflammation.

Published

2015

24. Identification of factor H-like protein 1 as the predominant complement regulator in Bruch's membrane: implications for age-related macular degeneration.

Author

Clark SJ, Schmidt CQ, White AM, Hakobyan S, Morgan BP, and Bishop PN

Subjects

Bruch Membrane immunology, Bruch Membrane pathology, Complement Activation, Complement C3b Inactivator Proteins genetics, Complement C3b Inactivator Proteins immunology, Complement Factor H genetics, Complement Factor H immunology, Extracellular Matrix immunology, Extracellular Matrix metabolism, Extracellular Matrix pathology, Gene Expression Regulation, Glycosylation, Heparitin Sulfate immunology, Heparitin Sulfate metabolism, Homeostasis, Humans, Immunity, Innate, Macular Degeneration genetics, Macular Degeneration immunology, Macular Degeneration pathology, Protein Binding, Protein Transport, Retina immunology, Retina pathology, Retinal Drusen genetics, Retinal Drusen immunology, Retinal Drusen pathology, Signal Transduction, Bruch Membrane metabolism, Complement C3b Inactivator Proteins metabolism, Complement Factor H metabolism, Macular Degeneration metabolism, Retina metabolism, Retinal Drusen metabolism

Abstract

The tight regulation of innate immunity on extracellular matrix (ECM) is a vital part of immune homeostasis throughout the human body, and disruption to this regulation in the eye is thought to contribute directly to the progression of age-related macular degeneration (AMD). The plasma complement regulator factor H (FH) is thought to be the main regulator that protects ECM against damaging complement activation. However, in the present study we demonstrate that a truncated form of FH, called FH-like protein 1 (FHL-1), is the main regulatory protein in the layer of ECM under human retina, called Bruch's membrane. Bruch's membrane is a major site of AMD disease pathogenesis and where drusen, the hallmark lesions of AMD, form. We show that FHL-1 can passively diffuse through Bruch's membrane, whereas the full sized, glycosylated, FH cannot. FHL-1 is largely bound to Bruch's membrane through interactions with heparan sulfate, and we show that the common Y402H polymorphism in the CFH gene, associated with an increased risk of AMD, reduces the binding of FHL-1 to this heparan sulfate. We also show that FHL-1 is retained in drusen whereas FH coats the periphery of the lesions, perhaps inhibiting their clearance. Our results identify a novel mechanism of complement regulation in the human eye, which highlights potential new avenues for therapeutic strategies., (Copyright © 2014 by The American Association of Immunologists, Inc.)

Published

2014

25. Inhibiting stromal cell heparan sulfate synthesis improves stem cell mobilization and enables engraftment without cytotoxic conditioning.

Author

Saez B, Ferraro F, Yusuf RZ, Cook CM, Yu VW, Pardo-Saganta A, Sykes SM, Palchaudhuri R, Schajnovitz A, Lotinun S, Lymperi S, Mendez-Ferrer S, Toro RD, Day R, Vasic R, Acharya SS, Baron R, Lin CP, Yamaguchi Y, Wagers AJ, and Scadden DT

Subjects

Animals, Anticoagulants pharmacology, Binding, Competitive immunology, Diabetes Mellitus, Experimental immunology, Diabetes Mellitus, Experimental metabolism, Granulocyte Colony-Stimulating Factor pharmacology, Green Fluorescent Proteins genetics, Heparin pharmacology, Heparitin Sulfate immunology, Male, Mice, Inbred C57BL, Mice, Transgenic, N-Acetylglucosaminyltransferases immunology, Signal Transduction drug effects, Signal Transduction immunology, Stromal Cells immunology, Vascular Cell Adhesion Molecule-1 immunology, Vascular Cell Adhesion Molecule-1 metabolism, Hematopoietic Stem Cell Mobilization methods, Hematopoietic Stem Cell Transplantation methods, Heparitin Sulfate biosynthesis, N-Acetylglucosaminyltransferases metabolism, Stromal Cells metabolism, Transplantation Conditioning

Abstract

The glycosyltransferase gene, Ext1, is essential for heparan sulfate production. Induced deletion of Ext1 selectively in Mx1-expressing bone marrow (BM) stromal cells, a known population of skeletal stem/progenitor cells, in adult mice resulted in marked changes in hematopoietic stem and progenitor cell (HSPC) localization. HSPC egressed from BM to spleen after Ext1 deletion. This was associated with altered signaling in the stromal cells and with reduced vascular cell adhesion molecule 1 production by them. Further, pharmacologic inhibition of heparan sulfate mobilized qualitatively more potent and quantitatively more HSPC from the BM than granulocyte colony-stimulating factor alone, including in a setting of granulocyte colony-stimulating factor resistance. The reduced presence of endogenous HSPC after Ext1 deletion was associated with engraftment of transfused HSPC without any toxic conditioning of the host. Therefore, inhibiting heparan sulfate production may provide a means for avoiding the toxicities of radiation or chemotherapy in HSPC transplantation for nonmalignant conditions., (© 2014 by The American Society of Hematology.)

Published

2014

26. WNT/β-catenin signaling and hepatocellular carcinoma.

Author

Wands JR and Kim M

Subjects

Animals, Female, Humans, Antibodies, Monoclonal immunology, Carcinoma, Hepatocellular immunology, Glypicans immunology, Heparitin Sulfate immunology, Liver Neoplasms immunology, Wnt Signaling Pathway immunology

Published

2014

27. Inactivation of Wnt signaling by a human antibody that recognizes the heparan sulfate chains of glypican-3 for liver cancer therapy.

Author

Gao W, Kim H, Feng M, Phung Y, Xavier CP, Rubin JS, and Ho M

Subjects

Animals, Antibodies, Monoclonal pharmacology, Carcinoma, Hepatocellular drug therapy, Cell Surface Display Techniques, Female, Hep G2 Cells, Humans, Liver Neoplasms drug therapy, Mice, Mice, Inbred BALB C, Mice, Nude, Wnt Signaling Pathway drug effects, Xenograft Model Antitumor Assays, beta Catenin immunology, Antibodies, Monoclonal immunology, Carcinoma, Hepatocellular immunology, Glypicans immunology, Heparitin Sulfate immunology, Liver Neoplasms immunology, Wnt Signaling Pathway immunology

Abstract

Unlabelled: Wnt signaling is important for cancer pathogenesis and is often up-regulated in hepatocellular carcinoma (HCC). Heparan sulfate proteoglycans (HSPGs) function as coreceptors or modulators of Wnt activation. Glypican-3 (GPC3) is an HSPG that is highly expressed in HCC, where it can attract Wnt proteins to the cell surface and promote cell proliferation. Thus, GPC3 has emerged as a candidate therapeutic target in liver cancer. While monoclonal antibodies to GPC3 are currently being evaluated in preclinical and clinical studies, none have shown an effect on Wnt signaling. Here, we first document the expression of Wnt3a, multiple Wnt receptors, and GPC3 in several HCC cell lines, and demonstrate that GPC3 enhanced the activity of Wnt3a/β-catenin signaling in these cells. Then we report the identification of HS20, a human monoclonal antibody against GPC3, which preferentially recognized the heparan sulfate chains of GPC3, both the sulfated and nonsulfated portions. HS20 disrupted the interaction of Wnt3a and GPC3 and blocked Wnt3a/β-catenin signaling. Moreover, HS20 inhibited Wnt3a-dependent cell proliferation in vitro and HCC xenograft growth in nude mice. In addition, HS20 had no detectable undesired toxicity in mice. Taken together, our results show that a monoclonal antibody primarily targeting the heparin sulfate chains of GPC3 inhibited Wnt/β-catenin signaling in HCC cells and had potent antitumor activity in vivo., Conclusion: An antibody directed against the heparan sulfate of a proteoglycan shows efficacy in blocking Wnt signaling and HCC growth, suggesting a novel strategy for liver cancer therapy., (Published 2014. This article is a U.S. Government work and is in the public domain in the USA.)

Published

2014

28. Synthetic di-sulfated iduronic acid attenuates asthmatic response by blocking T-cell recruitment to inflammatory sites.

Author

Nonaka M, Bao X, Matsumura F, Götze S, Kandasamy J, Kononov A, Broide DH, Nakayama J, Seeberger PH, and Fukuda M

Subjects

Animals, Asthma immunology, Bronchoalveolar Lavage Fluid immunology, Carbohydrate Sequence, Chemokine CCL20 immunology, Chemokine CCL20 metabolism, Chemotaxis immunology, Disease Models, Animal, Eosinophils cytology, Eosinophils drug effects, Eosinophils immunology, Heparitin Sulfate immunology, Heparitin Sulfate metabolism, Iduronic Acid chemical synthesis, Lung immunology, Mice, Mice, Knockout, N-Acetylglucosaminyltransferases genetics, Ovalbumin immunology, Ovalbumin pharmacology, Polysaccharides immunology, Polysaccharides metabolism, Receptor, TIE-2 genetics, Sulfates chemical synthesis, T-Lymphocytes cytology, T-Lymphocytes immunology, Asthma drug therapy, Iduronic Acid pharmacology, Sulfates pharmacology, T-Lymphocytes drug effects

Abstract

Identification of carbohydrate sequences that determine affinity to specific chemokines is a critical step for strategies to interfere with chemokine-mediated leukocyte trafficking. Here, we first characterized the development of allergic asthma in Tie2-dependent and inducible Ext1-knockout (Tie2-Ext1(iKO)) mice. We showed that heparan sulfate is essential for leukocyte recruitment in the peribronchial region and bronchoalveolar lavage fluid (BALF), and is crucial for induction of airway hyperresponsiveness. Our glycan microarray showed a unique affinity profile of chemokine CCL20 to substructures of heparin and heparin-like oligo/di/monosaccharides. Among them, we identified a synthetic and not naturally occurring monosaccharide, 2,4-O-di-sulfated iduronic acid (Di-S-IdoA), as a potential inhibitor for CCL20-heparan sulfate interaction. Mice injected with Di-S-IdoA via tail vain or nasal inhalation showed attenuated leukocyte recruitment into inflammatory sites and BALF. These results demonstrate a critical role of chemokine-heparan sulfate interaction in the asthma development and Di-S-IdoA as a potential drug for asthma treatment.

Published

2014

29. Lymphatic specific disruption in the fine structure of heparan sulfate inhibits dendritic cell traffic and functional T cell responses in the lymph node.

Author

Yin X, Johns SC, Kim D, Mikulski Z, Salanga CL, Handel TM, Macal M, Zúñiga EI, and Fuster MM

Subjects

Animals, CD8-Positive T-Lymphocytes cytology, Cell Movement genetics, Chemokines genetics, Chemokines immunology, Dendritic Cells cytology, Endothelium, Lymphatic cytology, Heparitin Sulfate genetics, Humans, Lymph Nodes cytology, Mice, Mice, Transgenic, CD8-Positive T-Lymphocytes immunology, Cell Movement immunology, Dendritic Cells immunology, Endothelium, Lymphatic immunology, Heparitin Sulfate immunology, Lymph Nodes immunology

Abstract

Dendritic cells (DCs) are potent APCs essential for initiating adaptive immunity. Following pathogen exposure, trafficking of DCs to lymph nodes (LNs) through afferent lymphatic vessels constitutes a crucial step in the execution of their functions. The mechanisms regulating this process are poorly understood, although the involvement of certain chemokines in this process has recently been reported. In this study, we demonstrate that genetically altering the fine structure (N-sulfation) of heparan sulfate (HS) specifically in mouse lymphatic endothelium significantly reduces DC trafficking to regional LNs in vivo. Moreover, this alteration had the unique functional consequence of reducing CD8(+) T cell proliferative responses in draining LNs in an ovalbumin immunization model. Mechanistic studies suggested that lymphatic endothelial HS regulates multiple steps during DC trafficking, including optimal presentation of chemokines on the surface of DCs, thus acting as a co-receptor that may function "in trans" to mediate chemokine receptor binding. This study not only identifies novel glycan-mediated mechanisms that regulate lymphatic DC trafficking, but it also validates the fine structure of lymphatic vascular-specific HS as a novel molecular target for strategies aiming to modulate DC behavior and/or alter pathologic T cell responses in lymph nodes.

Published

2014

30. Heparin-dependent regulation of fibronectin matrix conformation.

Author

Hubbard B, Buczek-Thomas JA, Nugent MA, and Smith ML

Subjects

Binding Sites, Cell Adhesion genetics, Extracellular Matrix chemistry, Extracellular Matrix immunology, Fibronectins chemistry, Fibronectins immunology, Heparin chemistry, Heparitin Sulfate immunology, Heparitin Sulfate metabolism, Humans, Protein Binding, Protein Conformation, Protein Structure, Tertiary, Antibodies immunology, Extracellular Matrix metabolism, Fibronectins metabolism, Heparin metabolism

Abstract

Extracellular matrix (ECM) conformation is regulated by a variety of stimuli in vivo, including mechanical forces and allosteric binding partners, and these conformational changes contribute to the regulation of cell behavior. Heparin and heparan sulfate, for example, have been shown to regulate the sequestration and presentation of numerous growth factors, including vascular endothelial growth factor, on the heparin 2 binding domain in fibronectin (Fn). However, mechanical force also alters Fn conformation, indicating that the growth factor binding region may be co-regulated by both heparin and mechanical force. Herein, we describe a simple antibody-based method for evaluating the conformation of the heparin 2 binding domain in Fn, and use it to determine the relative contributions of heparin and mechanical strain to the regulation of Fn conformation. We achieved specificity in quantifying conformational changes in this region of Fn by measuring the ratio of two fluorescent monoclonal antibodies, one that is insensitive to Fn conformational changes and a second whose binding is reduced or enhanced by non-equilibrium conformational changes. Importantly, this technique is shown to work on Fn adsorbed on surfaces, single Fn fibers, and Fn matrix fibers in cell culture. Using our dual antibody approach, we show that heparin and mechanical strain co-regulate Fn conformation in matrix fibrils, which is the first demonstration of heparin-dependent regulation of Fn in its physiologically-relevant fibrillar state. Furthermore, the dual antibody approach utilizes commercially available antibodies and simple immunohistochemistry, thus making it accessible to a wide range of scientists interested in Fn mechanobiology., (© 2013.)

Published

2014

31. Unexpected new roles for heparanase in Type 1 diabetes and immune gene regulation.

Author

Parish CR, Freeman C, Ziolkowski AF, He YQ, Sutcliffe EL, Zafar A, Rao S, and Simeonovic CJ

Subjects

Animals, Cell Proliferation, Diabetes Mellitus, Type 1 drug therapy, Diabetes Mellitus, Type 1 immunology, Diabetes Mellitus, Type 1 pathology, Enzyme Inhibitors pharmacology, Extracellular Matrix chemistry, Extracellular Matrix immunology, Extracellular Matrix metabolism, Free Radicals antagonists & inhibitors, Free Radicals metabolism, Gene Expression Regulation immunology, Glucuronidase genetics, Heparitin Sulfate immunology, Humans, Islets of Langerhans drug effects, Islets of Langerhans immunology, Islets of Langerhans pathology, Mice, Oligosaccharides pharmacology, Signal Transduction, T-Lymphocytes drug effects, T-Lymphocytes immunology, T-Lymphocytes pathology, Diabetes Mellitus, Type 1 enzymology, Glucuronidase metabolism, Heparitin Sulfate biosynthesis, Islets of Langerhans enzymology

Abstract

Heparanase (Hpse) is an endo-β-d-glucuronidase that degrades the glycosaminoglycan heparan sulfate (HS) in basement membranes (BMs) to facilitate leukocyte migration into tissues. Heparanase activity also releases HS-bound growth factors from the extracellular matrix (ECM), a function that aids wound healing and angiogenesis. In disease states, the degradation of HS in BMs by heparanase is well recognized as an invasive property of metastatic cancer cells. Recent studies by our group, however, have identified unexpected new roles for heparanase and HS. First, we discovered that in Type 1 diabetes (T1D) (i) HS in the pancreatic islet BM acts as a barrier to invading cells and (ii) high levels of HS within the insulin-producing islet beta cells themselves are critical for beta cell survival, protecting the cells from free radical-mediated damage. Furthermore, catalytically active heparanase produced by autoreactive T cells and other insulitis mononuclear cells was shown to degrade intra-islet HS, increasing the susceptibility of islet beta cells to free radical damage and death. This totally novel molecular explanation for the onset of T1D diabetes opens up new therapeutic approaches for preventing disease progression. Indeed, administration of the heparanase inhibitor, PI-88, dramatically reduced T1D incidence in diabetes-prone NOD mice, preserved islet beta cell HS and reduced islet inflammation. Second, in parallel studies it has been shown that heparanase and HS can be transported to the nucleus of cells where they impact directly or indirectly on gene transcription. Based on ChIP-on-chip studies heparanase was found to interact with the promoters and transcribed regions of several hundred genes and micro-RNAs in activated Jurkat T cells and up-regulate transcription, with many of the target genes/micro-RNAs being involved in T cell differentiation. At the molecular level, nuclear heparanase appears to regulate histone 3 lysine 4 (H3K4) methylation by influencing the recruitment of demethylases to transcriptionally active genes. These studies have unveiled new functions for heparanase produced by T lymphocytes, with the enzyme mediating unexpected intracellular effects on T cell differentiation and insulin-producing beta cell survival in T cell-dependent autoimmune T1D., (Crown Copyright © 2013. Published by Elsevier B.V. All rights reserved.)

Published

2013

32. A sulfated glycosaminoglycan array for molecular interactions between glycosaminoglycans and growth factors or anti-glycosaminoglycan antibodies.

Author

Takada W, Fukushima M, Pothacharoen P, Kongtawelert P, and Sugahara K

Subjects

Chondroitin Sulfates analysis, Chondroitin Sulfates immunology, Chondroitin Sulfates metabolism, Glycosaminoglycans immunology, Glycosaminoglycans metabolism, Heparitin Sulfate analysis, Heparitin Sulfate immunology, Heparitin Sulfate metabolism, High-Throughput Screening Assays, Humans, Polymethacrylic Acids chemistry, Protein Binding, Spectrometry, Fluorescence, Antibodies immunology, Glycosaminoglycans analysis, Intercellular Signaling Peptides and Proteins metabolism, Microarray Analysis

Abstract

Glycosaminoglycans (GAGs) take part in numerous biological processes by binding to protein molecules and functionally regulating protein-ligand interactions; therefore, molecular interactions of GAGs have been studied by several methods, including surface plasmon resonance, enzyme-linked immunosorbent assays (ELISAs), and GAG microarrays. To achieve rapid, sensitive, and high-throughput screening of GAG interactions, we have developed a novel microarray in which GAGs, including chondroitin sulfate, heparan sulfate, and heparin, were immobilized. The microarray is made from cyclic polyolefin substrate coated with metacrylate polymers, which have phospholipid groups as side chains. The polymer also has aminooxy groups that react specifically with aldehyde groups at the reducing termini of GAG chains, whereas the phospholipid groups prevent nonspecific adsorption of proteins. Thus, minute amounts of GAGs can be chemically immobilized on the surface with low nonspecific binding of proteins. Using this array, interactions between GAGs and antibodies against chondroitin or heparan sulfate and heparin-binding growth factors were examined. The results were in agreement with previously reported specificities, suggesting that the GAG array is useful for high-throughput interaction analyses between GAGs and functional proteins in miniscule amounts and can be applied to both basic studies of GAGs and the development of diagnostic methods for metabolic diseases involving GAGs., (Copyright © 2013 Elsevier Inc. All rights reserved.)

Published

2013

33. Kidney transplantation: analysis of the expression and T cell-mediated activation of latent TGF-β.

Author

Willet JD, Pichitsiri W, Jenkinson SE, Brain JG, Wood K, Alhasan AA, Spielhofer J, Robertson H, Ali S, and Kirby JA

Subjects

Adult, Aged, Antigens, CD genetics, Antigens, CD immunology, Basic Helix-Loop-Helix Leucine Zipper Transcription Factors genetics, Basic Helix-Loop-Helix Leucine Zipper Transcription Factors immunology, Cell Communication drug effects, Cell Differentiation, Cell Line, Transformed, Female, Gene Expression Regulation drug effects, Graft Rejection immunology, Graft Rejection metabolism, Graft Rejection pathology, Heparitin Sulfate immunology, Heparitin Sulfate metabolism, Humans, Integrin alpha Chains genetics, Integrin alpha Chains immunology, Kidney Transplantation immunology, Kidney Tubules immunology, Kidney Tubules metabolism, Lymphocyte Activation drug effects, Male, Middle Aged, Protein Binding, Signal Transduction drug effects, Smad3 Protein genetics, Smad3 Protein immunology, T-Lymphocytes immunology, T-Lymphocytes metabolism, Transforming Growth Factor beta immunology, Transforming Growth Factor beta pharmacology, Transplantation, Homologous, Graft Rejection genetics, Kidney Transplantation pathology, Kidney Tubules pathology, T-Lymphocytes pathology, Transforming Growth Factor beta genetics

Abstract

Activated T cells infiltrate a renal allograft during rejection and can respond to TGF-β within the tubules, causing local differentiation and expression of the αE(CD103)β7 integrin. This study was performed to examine the expression of latent TGF-β within renal allograft tissues and to define a mechanism by which T cells can activate and respond to this latent factor. Rejecting renal allograft biopsy tissues showed increased expression of the latent TGF-β complex, which was localized around the tubules by a mechanism that might involve interaction with heparan sulfate in the basement membrane. A cultured renal TEC line also expressed the latent complex, but these cells did not respond to this form of TGF-β by pSmad 3. However, coculture of these cells with activated T cells induced the expression of CD103, suggesting that T cells can activate and respond to the latent TGF-β associated with TEC. Although activated T cells expressed little cell-surface TSP-1, this was increased by culture with fibronectin or fibronectin-expressing renal TEC. Blockade of TSP-1 using LSKL peptides reduced the potential of activated T cells to differentiate in response to latent TGF-β. This study suggests that penetration of renal tubules by activated T cells leads to increased expression of T cell-surface TSP-1, allowing activation of latent TGF-β sequestered on heparan sulfate within the microenvironment. This mechanism may be important for localized phenotypic maturation of T cells that have infiltrated the kidney during allograft rejection.

Published

2013

34. Inactivation of heparan sulfate 2-O-sulfotransferase accentuates neutrophil infiltration during acute inflammation in mice.

Author

Axelsson J, Xu D, Kang BN, Nussbacher JK, Handel TM, Ley K, Sriramarao P, and Esko JD

Subjects

Animals, Cells, Cultured, Chemokines immunology, Endothelial Cells immunology, Endothelial Cells metabolism, Heparitin Sulfate chemistry, Heparitin Sulfate immunology, Inflammation chemically induced, Inflammation genetics, Inflammation immunology, L-Selectin immunology, Male, Mice, Mice, Inbred C57BL, Neutrophils cytology, Peritonitis chemically induced, Peritonitis genetics, Thioglycolates, Gene Silencing, Neutrophil Infiltration, Neutrophils immunology, Peritonitis immunology, Sulfotransferases genetics, Sulfotransferases immunology

Abstract

Neutrophil recruitment and extravasation at sites of inflammation provide a mechanism for host defense. We showed previously that heparan sulfate, a type of sulfated glycosaminoglycan, facilitates neutrophil recruitment based on the reduction of neutrophil infiltration in mice in which the overall sulfation of the chains was reduced by selective inactivation of N-acetylglucosamine N-deacetylase-N-sulfotransferase (Ndst1) in endothelial cells. Here we show that inactivation of uronyl 2-O-sulfotransferase in endothelial cells (Hs2st), an enzyme that acts downstream from Ndst1, results in enhanced neutrophil recruitment in several models of acute inflammation. Enhanced neutrophil infiltration resulted in part from reduced rolling velocity under flow both in vivo and in vitro, which correlated with stronger binding of neutrophil L-selectin to mutant endothelial cells. Hs2st-deficient endothelial cells also displayed a striking increase in binding of IL-8 and macrophage inflammatory protein-2. The enhanced binding of these mediators of neutrophil recruitment resulted from a change in heparan sulfate structure caused by increased N-sulfation and 6-O-sulfation of glucosamine units in response to the decrease in 2-O-sulfation of uronic acid residues. This gain-of-function phenotype provides formidable evidence demonstrating the importance of endothelial heparan sulfate in inflammation and suggests a novel enzyme target for enhancing the innate immune response.

Published

2012

35. Heparin inhibits the interaction of DNA topoisomerase I/anti-topoisomerase I immune complexes with heparan sulfate on dermal fibroblasts.

Author

Arcand J, Robitaille G, Koenig M, Senécal JL, and Raymond Y

Subjects

Antigen-Antibody Complex immunology, Antigens, Surface immunology, Autoantibodies immunology, Autoantibodies pharmacology, Cells, Cultured, Dermis pathology, Fibroblasts immunology, Fibroblasts pathology, Humans, Protein Binding, Scleroderma, Systemic immunology, Antigen-Antibody Complex drug effects, DNA Topoisomerases, Type I immunology, Fibrinolytic Agents pharmacology, Fibroblasts drug effects, Heparin pharmacology, Heparitin Sulfate immunology

Abstract

Objective: Previous studies have demonstrated that the systemic sclerosis (SSc)-associated autoantigen DNA topoisomerase I (topo I) binds specifically to the surface of fibroblasts when released in the extracellular environment and recruits anti-topo I autoantibodies, which subsequently leads to the adhesion and activation of monocytes. This study aimed to characterize the molecular interactions of topo I with fibroblast surfaces in order to elucidate the pathogenic role of topo I/anti-topo I immune complexes (ICs) in SSc., Methods: Topo I directly coupled to fluorochromes was used to follow its binding to fibroblast surfaces by flow cytometry and fluorescence microscopy. Purified IgG from normal subjects or SSc patients was added with topo I to the cells; unfractionated heparin (UFH) and low molecular weight heparin (LMWH) were used to determine their effects on the binding of topo I and topo I/anti-topo I IC to fibroblast surfaces., Results: Heparan sulfate (HS) proteoglycans on fibroblast surfaces were found to act as coreceptors for topo I binding. The addition of anti-topo I autoantibodies from SSc sera led to the amplification of topo I binding to HS chains. UFH and LMWH were shown to inhibit topo I and topo I/anti-topo I IC binding to HS chains., Conclusion: This study is the first to show that topo I binds specifically to HS proteoglycans on fibroblast surfaces and that anti-topo I autoantibodies from SSc patients amplify topo I binding to HS chains. The accumulation of topo I on cell surfaces by anti-topo I autoantibodies could contribute to the initiation of an inflammatory cascade stimulating the fibrosis. UFH and LMWH inhibited the binding of topo I/anti-topo I IC to fibroblasts, suggesting a potential therapeutic role in SSc-associated fibrosis., (Copyright © 2012 by the American College of Rheumatology.)

Published

2012

36. Hitting the sweet spot.

Author

Kulkarni G and Wadsworth WG

Subjects

Animals, Animals, Genetically Modified, Caenorhabditis elegans genetics, Epitopes genetics, Epitopes immunology, Green Fluorescent Proteins analysis, Green Fluorescent Proteins chemistry, Heparitin Sulfate genetics, Heparitin Sulfate immunology, Single-Chain Antibodies genetics, Single-Chain Antibodies immunology, Caenorhabditis elegans immunology, Epitopes analysis, Green Fluorescent Proteins genetics, Heparitin Sulfate chemistry, Single-Chain Antibodies analysis

Published

2012

37. Genistein reduces heparan sulfate accumulation in human mucolipidosis II skin fibroblasts.

Author

Otomo T, Hossain MA, Ozono K, and Sakai N

Subjects

Antibodies, Anti-Idiotypic immunology, Cells, Cultured, Dose-Response Relationship, Drug, Extracellular Space drug effects, Fibroblasts drug effects, Heparitin Sulfate immunology, Heparitin Sulfate isolation & purification, Humans, Inclusion Bodies drug effects, Inclusion Bodies metabolism, Skin metabolism, Extracellular Space metabolism, Fibroblasts metabolism, Genistein pharmacology, Heparitin Sulfate metabolism, Mucolipidoses metabolism

Abstract

Genistein, a soy isoflavone, reduces glycosaminoglycan synthesis and its effect on mucopolysaccharidoses has been tested. In this report, we examined the effect of genistein in human mucolipidosis II skin fibroblasts in vitro. Heparan sulfate was accumulated within both cells and in extracellular spaces in mucolipidosis II. Genistein reduced the amount of heparan sulfate in cultured cells dose dependently and also inhibited cell growth dose dependently., (Copyright © 2011. Published by Elsevier Inc.)

Published

2012

38. Dissociation between mature phenotype and impaired transmigration in dendritic cells from heparanase-deficient mice.

Author

Benhamron S, Reiner I, Zcharia E, Atallah M, Grau A, Vlodavsky I, and Mevorach D

Subjects

Animals, Bone Marrow Cells enzymology, Dendritic Cells enzymology, Extracellular Matrix genetics, Extracellular Matrix immunology, Extracellular Matrix metabolism, Glucuronidase genetics, Glucuronidase metabolism, Heparitin Sulfate genetics, Heparitin Sulfate immunology, Heparitin Sulfate metabolism, Matrix Metalloproteinase 14 biosynthesis, Matrix Metalloproteinase 14 genetics, Matrix Metalloproteinase 14 immunology, Mice, Mice, Knockout, Receptors, CCR7 biosynthesis, Receptors, CCR7 genetics, Receptors, CCR7 immunology, Transendothelial and Transepithelial Migration genetics, Up-Regulation genetics, Up-Regulation immunology, Bone Marrow Cells immunology, Dendritic Cells immunology, Glucuronidase immunology, Transendothelial and Transepithelial Migration immunology

Abstract

To reach the lymphatics, migrating dendritic cells (DCs) need to interact with the extracellular matrix (ECM). Heparanase, a mammalian endo-β-D-glucuronidase, specifically degrades heparan sulfate proteoglycans ubiquitously associated with the cell surface and ECM. The role of heparanase in the physiology of bone marrow-derived DCs was studied in mutant heparanase knock-out (Hpse-KO) mice. Immature DCs from Hpse-KO mice exhibited a more mature phenotype; however their transmigration was significantly delayed, but not completely abolished, most probably due to the observed upregulation of MMP-14 and CCR7. Despite their mature phenotype, uptake of beads was comparable and uptake of apoptotic cells was more efficient in DCs from Hpse-KO mice. Heparanase is an important enzyme for DC transmigration. Together with CCR7 and its ligands, and probably MMP-14, heparanase controls DC trafficking.

Published

2012

39. Detection and characterization of syndecan-1-associated heparan sulfate 6-O-sulfated motifs overexpressed in multiple myeloma cells using single chain antibody variable fragments.

Author

Delcommenne M and Klingemann HG

Subjects

Antibody Specificity, Antigens, Neoplasm, Cell Line, Tumor, HL-60 Cells, Humans, Plasma Cells metabolism, Cell Surface Display Techniques methods, Heparitin Sulfate chemistry, Heparitin Sulfate immunology, Multiple Myeloma immunology, Single-Chain Antibodies biosynthesis, Single-Chain Antibodies immunology, Syndecan-1 immunology

Abstract

This study was undertaken to generate human single chain variable antibody fragments (scFvs) reacting specifically against multiple myeloma (MM) cells using the phage display technique. To isolate myeloma-specific scFvs, we used a simple subtractive strategy by adsorbing the Griffin #1 antibody phage library against myeloma cells in the presence of excess decoy biotinylated HL60 cells, and then removing the unwanted decoy cells using streptavidin coated plates. From eleven scFvs that were isolated, two antibodies, D4A4 and D6B10 stained MM cell lines and patient MM cells with higher intensity than normal plasma cells. Both D4A4 and D6B10 scFvs immunoprecipitated syndecan-1 from myeloma cells and recognized sulfated motifs on syndecan-1-associated heparan sulfate (HS) chains. ScFv D4A4 competed with D6B10 for binding to MM cells. However, they differed in their fine specificities. ScFv D6B10 recognized HS 2,6-O-, N-sulfated motifs and, in contrast, binding of scFv D4A4 required N-sulfation combined with either 2-O- or 6-O-sulfation. Increased D6B10 binding on MM cells suggests that their HS chains contain a greater number of 2,6-O-, N-sulfated motifs than normal plasma cells. Since these highly sulfated motifs bind various angiogenic and growth factors and present them to their respective receptors, they could be instrumental for MM cell survival, proliferation and metastasis. Therefore, scFvs D4A4 and D6B10 provide a means to easily monitor changes in sulfation patterns of heparan sulfate during myeloma tumor progression.

Published

2012

40. Virally-induced upregulation of heparan sulfate on B cells via the action of type I IFN.

Author

Jarousse N, Trujillo DL, Wilcox-Adelman S, and Coscoy L

Subjects

Animals, B-Lymphocytes immunology, Blotting, Western, Cell Separation, Flow Cytometry, Gammaherpesvirinae immunology, Heparitin Sulfate immunology, Immunoprecipitation, Interferon Type I immunology, Mice, Mice, Inbred C57BL, Mice, Knockout, Muromegalovirus immunology, Spleen cytology, Spleen immunology, Up-Regulation, B-Lymphocytes metabolism, Heparitin Sulfate biosynthesis, Herpesviridae Infections immunology, Interferon Type I metabolism

Abstract

Cell surface heparan sulfate (HS) is an important coreceptor for many cytokines, chemokines, and growth factors. In this study, we report that splenic murine B cells express very little HS and that upon infection with either gammaherpesvirus (murine gammaherpesvirus 68) or betaherpesvirus (murine cytomegalovirus), HS is rapidly upregulated at the surface of B cells. HS upregulation was not observed in mice deficient for the type I IFN (IFN-I) receptor. Additionally, treatment of wild-type mice with the IFN-I inducer polyinosine polycytidylic acid triggered HS expression at the B cell surface. Similarly, incubation of purified splenic B cells with IFN-I, TLR ligands, or BCR stimulators ex vivo resulted in a drastic increase in HS surface expression. We found that IFN-I induced an increase in the surface expression of HS-modified syndecan 4 as well as that of an unidentified heparan sulfate proteoglycan. Finally, IFN-I treatment increased B cell responsiveness to APRIL, a cytokine involved in B cell survival and T cell-independent B cell responses. Enzymatic removal of HS from IFN-I-treated B cells inhibited APRIL. Altogether, our results indicate that upon herpesvirus infection in mice, HS is rapidly upregulated at the surface of B cells due to the action of IFN-I, potentially increasing B cell responsiveness to cytokines. Induction of HS expression at the B cell surface by stimulators of the innate immune response likely plays a key role in the development of a robust immune response.

Published

2011

41. Glycotranscriptome study reveals an enzymatic switch modulating glycosaminoglycan synthesis during B-cell development and activation.

Author

Duchez S, Pascal V, Cogné N, Jayat-Vignoles C, Julien R, and Cogné M

Subjects

Animals, B-Lymphocytes immunology, Cell Differentiation genetics, Cell Differentiation immunology, Cell Line, Cell Line, Tumor, Chondroitin Sulfates biosynthesis, Chondroitin Sulfates immunology, Genetic Variation, Glycosaminoglycans genetics, Heparitin Sulfate biosynthesis, Heparitin Sulfate immunology, Immunoglobulins biosynthesis, Immunoglobulins immunology, Lymphocyte Activation genetics, Lymphocyte Activation immunology, Mice, Mice, Inbred C57BL, Mice, Transgenic, N-Acetylgalactosaminyltransferases genetics, N-Acetylgalactosaminyltransferases immunology, N-Acetylglucosaminyltransferases genetics, N-Acetylglucosaminyltransferases immunology, Tumor Suppressor Proteins genetics, Tumor Suppressor Proteins immunology, B-Lymphocytes cytology, B-Lymphocytes metabolism, Glycosaminoglycans biosynthesis

Abstract

B-cell fate and responses are modulated by soluble mediators and direct cellular interactions. Migration properties also vary during differentiation, commitment and activation. In many cells, modulation of responses to stimuli involves cell surface glycans, whose architecture depends on the simultaneous expression of multiple enzymes. By looking at the glycosylation-related gene expression patterns among B-cell populations, we determined in this study that the strongest variations were observed for CSGalNAcT-1 and EXTL1. These are enzymes involved in the biosynthesis of alternative forms of glycosaminoglycans (GAGs), namely chondroitin sulfate and heparan sulfate, respectively. These two enzymes showed inverse fluctuations in progenitors, resting B cells and activated B cells, suggesting a developmentally regulated switch between chondroitin and heparan sulfate synthesis. To explore whether these variations contributed to optimal B-cell differentiation, we overexpressed EXTL1 in the B-cell lineage of transgenic mice, yielding a partial differentiation blockade at the pro-B to pre-B transition. In the periphery, this defect was almost fully compensated for in vivo, with normal-size B-cell compartments and normal serum immunoglobulin levels in the transgenic EXTL1 mice. The peripheral B cells from EXTL1 transgenics were only affected with regard to their in vitro responses to polyclonal activation, showing reduced proliferation. Together the data suggest that despite their low amounts in lymphocytes, the heparan sulfate chains decorating the endogenous GAGs appear to be regulators of B-cell physiology., (Copyright © 2011 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2011

42. RB4CD12 epitope expression and heparan sulfate disaccharide composition in brain vasculature.

Author

Hosono-Fukao T, Ohtake-Niimi S, Nishitsuji K, Hossain MM, van Kuppevelt TH, Michikawa M, and Uchimura K

Subjects

Animals, Disaccharides immunology, Mice, Cerebral Cortex immunology, Cerebrovascular Circulation immunology, Epitopes immunology, Heparitin Sulfate immunology

Abstract

RB4CD12 is a phage display antibody that recognizes a heparan sulfate (HS) glycosaminoglycan epitope. The epitope structure is proposed to contain a trisulfated disaccharide, [-IdoA(2-OSO(3))-GlcNSO(3) (6-OSO(3))-], which supports HS binding to various macromolecules such as growth factors and cytokines in central nervous tissues. Chemically modified heparins that lack the trisulfated disaccharides failed to inhibit the RB4CD12 recognition of HS chains. To determine the localization of the RB4CD12 anti-HS epitope in the brain, we performed an immunohistochemical analysis for cryocut sections of mouse brain. The RB4CD12 staining signals were colocalized with laminin and were detected abundantly in the vascular basement membrane. Bacterial heparinases eliminated the RB4CD12 staining signals. The RB4CD12 epitope localization was confirmed by immunoelectron microscopy. Western blotting analysis revealed that the size of a major RB4CD12-positive molecule is ∼460 kDa in a vessel-enriched fraction of the mouse brain. Disaccharide analysis with reversed-phase ion-pair HPLC showed that [-IdoA(2-OSO(3))-GlcNSO(3) (6-OSO(3))-] trisulfated disaccharide residues are present in HS purified from the vessel-enriched brain fraction. These results indicated that the RB4CD12 anti-HS epitope exists in large quantities in the brain vascular basement membrane., (Copyright © 2011 Wiley-Liss, Inc.)

Published

2011

43. Suppression of amyloid beta A11 antibody immunoreactivity by vitamin C: possible role of heparan sulfate oligosaccharides derived from glypican-1 by ascorbate-induced, nitric oxide (NO)-catalyzed degradation.

Author

Cheng F, Cappai R, Ciccotosto GD, Svensson G, Multhaup G, Fransson LÅ, and Mani K

Subjects

Animals, Catalysis, Flow Cytometry, Humans, Hydrolysis, Mice, Mice, Transgenic, Microscopy, Fluorescence, Amyloid beta-Peptides immunology, Ascorbic Acid pharmacology, Glypicans chemistry, Heparitin Sulfate immunology, Nitric Oxide chemistry

Abstract

Amyloid β (Aβ) is generated from the copper- and heparan sulfate (HS)-binding amyloid precursor protein (APP) by proteolytic processing. APP supports S-nitrosylation of the HS proteoglycan glypican-1 (Gpc-1). In the presence of ascorbate, there is NO-catalyzed release of anhydromannose (anMan)-containing oligosaccharides from Gpc-1-nitrosothiol. We investigated whether these oligosaccharides interact with Aβ during APP processing and plaque formation. anMan immunoreactivity was detected in amyloid plaques of Alzheimer (AD) and APP transgenic (Tg2576) mouse brains by immunofluorescence microscopy. APP/APP degradation products detected by antibodies to the C terminus of APP, but not Aβ oligomers detected by the anti-Aβ A11 antibody, colocalized with anMan immunoreactivity in Tg2576 fibroblasts. A 50-55-kDa anionic, sodium dodecyl sulfate-stable, anMan- and Aβ-immunoreactive species was obtained from Tg2576 fibroblasts using immunoprecipitation with anti-APP (C terminus). anMan-containing HS oligo- and disaccharide preparations modulated or suppressed A11 immunoreactivity and oligomerization of Aβ42 peptide in an in vitro assay. A11 immunoreactivity increased in Tg2576 fibroblasts when Gpc-1 autoprocessing was inhibited by 3-β[2(diethylamino)ethoxy]androst-5-en-17-one (U18666A) and decreased when Gpc-1 autoprocessing was stimulated by ascorbate. Neither overexpression of Gpc-1 in Tg2576 fibroblasts nor addition of copper ion and NO donor to hippocampal slices from 3xTg-AD mice affected A11 immunoreactivity levels. However, A11 immunoreactivity was greatly suppressed by the subsequent addition of ascorbate. We speculate that temporary interaction between the Aβ domain and small, anMan-containing oligosaccharides may preclude formation of toxic Aβ oligomers. A portion of the oligosaccharides are co-secreted with the Aβ peptides and deposited in plaques. These results support the notion that an inadequate supply of vitamin C could contribute to late onset AD in humans.

Published

2011

44. HIV-1 p17 matrix protein interacts with heparan sulfate side chain of CD44v3, syndecan-2, and syndecan-4 proteoglycans expressed on human activated CD4+ T cells affecting tumor necrosis factor alpha and interleukin 2 production.

Author

De Francesco MA, Baronio M, and Poiesi C

Subjects

CD4-Positive T-Lymphocytes immunology, Female, HIV Antigens genetics, HIV Antigens immunology, HIV-1 genetics, HIV-1 immunology, HeLa Cells, Heparitin Sulfate genetics, Heparitin Sulfate immunology, Humans, Hyaluronan Receptors genetics, Hyaluronan Receptors immunology, Interleukin-2 genetics, Interleukin-2 immunology, Lymphocyte Activation, Male, Protein Binding, Syndecan-2 genetics, Syndecan-2 immunology, Syndecan-4 genetics, Syndecan-4 immunology, Tumor Necrosis Factor-alpha genetics, Tumor Necrosis Factor-alpha immunology, gag Gene Products, Human Immunodeficiency Virus genetics, gag Gene Products, Human Immunodeficiency Virus immunology, CD4-Positive T-Lymphocytes metabolism, HIV Antigens metabolism, HIV-1 metabolism, Heparitin Sulfate metabolism, Hyaluronan Receptors metabolism, Interleukin-2 biosynthesis, Syndecan-2 metabolism, Syndecan-4 metabolism, Tumor Necrosis Factor-alpha biosynthesis, gag Gene Products, Human Immunodeficiency Virus metabolism

Abstract

HIV-1 p17 contains C- and N-terminal sequences with positively charged residues and a consensus cluster for heparin binding. We have previously demonstrated by affinity chromatography that HIV-1 p17 binds strongly to heparin-agarose at physiological pH and to human activated CD4(+) T cells. In this study we demonstrated that the viral protein binds to heparan sulfate side chains of syndecan-2, syndecan-4, and CD44v3 purified from HeLa cells and that these heparan sulfate proteoglycans (HSPGs) co-localize with HIV-1 p17 on activated human CD4(+) T cells by confocal fluorescence analysis. Moreover, we observed a stimulatory or inhibitory activity when CD4(+) T cells were activated with mitogens together with nanomolar or micromolar concentrations of the matrix protein.

Published

2011

45. Sézary syndrome cells overexpress syndecan-4 bearing distinct heparan sulfate moieties that suppress T-cell activation by binding DC-HIL and trapping TGF-beta on the cell surface.

Author

Chung JS, Shiue LH, Duvic M, Pandya A, Cruz PD Jr, and Ariizumi K

Subjects

Aged, Aged, 80 and over, Cell Membrane metabolism, Female, Heparitin Sulfate chemistry, Heparitin Sulfate immunology, Heparitin Sulfate metabolism, Humans, Lymphoma, T-Cell, Cutaneous immunology, Lymphoma, T-Cell, Cutaneous metabolism, Lymphoma, T-Cell, Cutaneous pathology, Male, Membrane Glycoproteins physiology, Middle Aged, Protein Binding immunology, Protein Binding physiology, Protein Transport, Receptors, Immunologic immunology, Sezary Syndrome genetics, Sezary Syndrome metabolism, Sezary Syndrome pathology, Syndecan-4 chemistry, Syndecan-4 metabolism, T-Lymphocytes metabolism, T-Lymphocytes pathology, Heparitin Sulfate physiology, Lymphocyte Activation immunology, Membrane Glycoproteins metabolism, Receptors, Immunologic metabolism, Sezary Syndrome immunology, Syndecan-4 genetics, T-Lymphocytes immunology, Transforming Growth Factor beta metabolism

Abstract

Because syndecan-4 (SD-4) on effector and memory T cells inhibits T-cell activation by binding dendritic cell-associated heparan sulfate proteoglycan-integrin ligand (DC-HIL) on antigen presenting cells and because malignant cells of the cutaneous T-cell lymphoma (CTCL) subset, Sézary syndrome (SS), exhibit memory T-cell phenotype, we posited SS cells to express SD-4. Indeed, malignant T cells from patients with SS and from CTCL cell lines constitutively expressed SD-4 at high levels, in contrast to T cells from healthy volunteers and patients with other inflammatory skin diseases and to non-CTCL cell lines that did not. SS cells also bound to DC-HIL at a level higher than normal T cells activated in vitro, resulting in their inhibited proliferation to anti-CD3 antibody. SD-4 on SS cells also trapped transforming growth factor-β1 to their cell surface, enhancing their ability to inhibit activation of syngeneic and allogeneic normal T cells. All of these inhibitory properties were dependent on overexpression of distinct heparan sulfate (HS) moieties by SD-4 on SS cells. Finally, we showed toxin-conjugated DC-HIL to abrogate the ability of SS cells to proliferate in vitro. These findings indicate that SD-4 bearing distinct HS moieties plays a pathogenic role in SS and may be targeted for treatment.

Published

2011

46. The heparan sulfate motif (GlcNS6S-IdoA2S)3, common in heparin, has a strict topography and is involved in cell behavior and disease.

Author

Smits NC, Kurup S, Rops AL, ten Dam GB, Massuger LF, Hafmans T, Turnbull JE, Spillmann D, Li JP, Kennel SJ, Wall JS, Shworak NW, Dekhuijzen PN, van der Vlag J, and van Kuppevelt TH

Subjects

Amyloidogenic Proteins immunology, Amyloidogenic Proteins metabolism, Amyloidosis immunology, Animals, Antibodies, Monoclonal immunology, Biomarkers metabolism, CHO Cells, Carbohydrate Sequence, Cell Proliferation drug effects, Cricetinae, Cricetulus, Disease Models, Animal, Endothelial Cells immunology, Female, Heparitin Sulfate antagonists & inhibitors, Heparitin Sulfate immunology, Humans, Male, Mice, Neoplasms immunology, Rats, Rats, Wistar, Single-Chain Antibodies immunology, Tumor Necrosis Factor-alpha pharmacology, Amyloidosis metabolism, Antibodies, Monoclonal pharmacology, Endothelial Cells metabolism, Heparitin Sulfate metabolism, Neoplasms metabolism, Single-Chain Antibodies pharmacology

Abstract

Heparan sulfate (HS) is a structurally complex polysaccharide that interacts with a broad spectrum of extracellular effector ligands and thereby is thought to regulate a diverse array of biologic processes. The specificity of HS-ligand interactions is determined by the arrangement of sulfate groups on HS, which creates distinct binding motifs. Biologically important HS motifs are expected to exhibit regulated expression, yet there is a profound lack of tools to identify such motifs; consequently, little is known of their structures and functions. We have identified a novel phage display-derived antibody (NS4F5) that recognizes a highly regulated HS motif (HS(NS4F5)), which we have rigorously identified as (GlcNS6S-IdoA2S)(3). HS(NS4F5) exhibits a restricted expression in healthy adult tissues. Blocking HS(NS4F5) on cells in culture resulted in reduced proliferation and enhanced sensitivity to apoptosis. HS(NS4F5) is up-regulated in tumor endothelial cells, consistent with a role in endothelial cell activation. Indeed, TNF-α stimulated endothelial expression of HS(NS4F5), which contributed to leukocyte adhesion. In a mouse model of severe systemic amyloid protein A amyloidosis, HS(NS4F5) was expressed within amyloid deposits, which were successfully detected by microSPECT imaging using NS4F5 as a molecularly targeted probe. Combined, our results demonstrate that NS4F5 is a powerful tool for elucidating the biological function of HS(NS4F5) and can be exploited as a probe to detect novel polysaccharide biomarkers of disease processes.

Published

2010

47. Cobra CRISP functions as an inflammatory modulator via a novel Zn2+- and heparan sulfate-dependent transcriptional regulation of endothelial cell adhesion molecules.

Author

Wang YL, Kuo JH, Lee SC, Liu JS, Hsieh YC, Shih YT, Chen CJ, Chiu JJ, and Wu WG

Subjects

Animals, Binding Sites, Cell Adhesion, Cell Adhesion Molecules immunology, Cell Line, Cells, Cultured, Elapid Venoms chemistry, Elapid Venoms immunology, Endothelial Cells drug effects, Gene Expression drug effects, Humans, Inflammation Mediators chemistry, Inflammation Mediators immunology, Molecular Conformation, Protein Binding, Protein Structure, Tertiary, X-Ray Diffraction, Cell Adhesion Molecules genetics, Elapid Venoms pharmacology, Elapidae, Endothelial Cells immunology, Heparitin Sulfate immunology, Inflammation Mediators pharmacology, Transcription, Genetic drug effects, Zinc immunology

Abstract

Cysteine-rich secretory proteins (CRISPs) have been identified as a toxin family in most animal venoms with biological functions mainly associated with the ion channel activity of cysteine-rich domain (CRD). CRISPs also bind to Zn(2+) at their N-terminal pathogenesis-related (PR-1) domain, but their function remains unknown. Interestingly, similar the Zn(2+)-binding site exists in all CRISP family, including those identified in a wide range of organisms. Here, we report that the CRISP from Naja atra (natrin) could induce expression of vascular endothelial cell adhesion molecules, i.e. intercellular adhesion molecule-1, vascular adhesion molecule-1, and E-selectin, to promote monocytic cell adhesion in a heparan sulfate (HS)- and Zn(2+)-dependent manner. Using specific inhibitors and small interfering RNAs, the activation mechanisms are shown to involve both mitogen-activated protein kinases and nuclear factor-κB. Biophysical characterization of natrin by using fluorescence, circular dichroism, and x-ray crystallographic methods further reveals the presence of two Zn(2+)-binding sites for natrin. The strong binding site is located near the putative Ser-His-Glu catalytic triad of the N-terminal domain. The weak binding site remains to be characterized, but it may modulate HS binding by enhancing its interaction with long chain HS. Our results strongly suggest that natrin may serve as an inflammatory modulator that could perturb the wound-healing process of the bitten victim by regulating adhesion molecule expression in endothelial cells. Our finding uncovers a new aspect of the biological role of CRISP family in immune response and is expected to facilitate future development of new therapeutic strategy for the envenomed victims.

Published

2010

48. Endothelial heparan sulfate controls chemokine presentation in recruitment of lymphocytes and dendritic cells to lymph nodes.

Author

Bao X, Moseman EA, Saito H, Petryniak B, Thiriot A, Hatakeyama S, Ito Y, Kawashima H, Yamaguchi Y, Lowe JB, von Andrian UH, and Fukuda M

Subjects

Animals, Cell Adhesion immunology, Chemokines metabolism, Dendritic Cells metabolism, Endothelium, Vascular immunology, Heparitin Sulfate metabolism, Integrins immunology, Lymph Nodes metabolism, Lymphocytes metabolism, Mice, Mice, Inbred C57BL, N-Acetylglucosaminyltransferases deficiency, Venules immunology, Venules metabolism, Chemokines immunology, Dendritic Cells immunology, Heparitin Sulfate immunology, Lymph Nodes immunology, Lymphocytes immunology

Abstract

Heparan sulfate can bind several adhesion molecules involved in lymphocyte trafficking. However, the in vivo function of endothelial heparan sulfate in lymphocyte homing and stimulation of the immune response has not been elucidated. Here, we generated mutant mice deficient in the enzyme Ext1, which is required for heparan sulfate synthesis, in a Tek-dependent and inducible manner. Chemokine presentation was diminished in the mutant mice, causing the lack of appropriate integrin-mediated adhesion, and resulted in a marked decrease in lymphocyte sticking to high endothelial venules and in recruitment of resident dendritic cells through lymphatic vessels to the lymph nodes. As a consequence, mutant mice displayed a severe impairment in lymphocyte homing and a compromised contact hypersensitivity response. By contrast, lymphocyte rolling was increased because of loss of electrostatic repulsion by heparan sulfate. These results demonstrate critical roles of endothelial heparan sulfate in immune surveillance and immune response generation., (Copyright © 2010 Elsevier Inc. All rights reserved.)

Published

2010

49. Heparan sulfate, including that in Bruch's membrane, inhibits the complement alternative pathway: implications for age-related macular degeneration.

Author

Kelly U, Yu L, Kumar P, Ding JD, Jiang H, Hageman GS, Arshavsky VY, Frank MM, Hauser MA, and Rickman CB

Subjects

Adult, Aged, Aged, 80 and over, Bruch Membrane chemistry, Bruch Membrane metabolism, Complement C3b immunology, Complement C3b metabolism, Complement Factor H genetics, Complement Factor H immunology, Complement Factor H metabolism, Female, Heparitin Sulfate metabolism, Humans, Macular Degeneration metabolism, Macular Degeneration pathology, Male, Microscopy, Electron, Transmission, Middle Aged, Protein Isoforms genetics, Protein Isoforms immunology, Protein Isoforms metabolism, Bruch Membrane immunology, Complement Pathway, Alternative immunology, Heparitin Sulfate immunology, Macular Degeneration immunology

Abstract

An imbalance between activation and inhibition of the complement system has been implicated in the etiologies of numerous common diseases. Allotypic variants of a key complement fluid-phase regulatory protein, complement factor H (CFH), are strongly associated with age-related macular degeneration (AMD), a leading cause of worldwide visual dysfunction, although its specific role in AMD pathogenesis is still not clear. CFH was isolated from individuals carrying combinations of two of the nonsynonymous coding variants most strongly associated with AMD risk, V62/H402 (risk haplotype variants), I62/Y402 (nonrisk haplotype variants), and V62/Y402. These proteins were used in two functional assays (cell surface- and fluid-phase-based) measuring cofactor activity of CFH in the factor I-mediated cleavage of C3b. Although no variant-specific differences in the cofactor activity were detected, when heparan sulfate (HS) was added to these assays, it accelerated the rate of C3b cleavage, and this effect could be modulated by degree of HS sulfation. Bruch's membrane/choroid, a site of tissue damage in AMD, contains high concentrations of glycosaminoglycans, including HS. Addition of human Bruch's membrane/choroid to the fluid-phase assay accelerated the C3b cleavage, and this effect was lost posttreatment of the tissue with heparinase III. Binding of CFH variants to Bruch's membrane/choroid isolated from elderly, non-AMD donor eyes, was similar, as was the functional activity of bound CFH. These findings refine our understanding of interactions of HS and complement and support the hypothesis that these interactions play a role in the transition between normal aging and AMD in Bruch's membrane/choroid.

Published

2010

50. Peroxynitrite modifies the structure and function of the extracellular matrix proteoglycan perlecan by reaction with both the protein core and the heparan sulfate chains.

Author

Kennett EC, Rees MD, Malle E, Hammer A, Whitelock JM, and Davies MJ

Subjects

Cell Line, Cell Proliferation, Coronary Artery Disease pathology, Coronary Artery Disease physiopathology, Coronary Vessels pathology, Epithelial Cells pathology, Heparan Sulfate Proteoglycans immunology, Heparitin Sulfate immunology, Humans, Immunohistochemistry, Oxidative Stress, Peroxynitrous Acid metabolism, Protein Binding, Protein Multimerization, Tunica Intima pathology, Coronary Artery Disease metabolism, Epithelial Cells metabolism, Extracellular Matrix metabolism, Heparan Sulfate Proteoglycans metabolism, Heparitin Sulfate metabolism, Tunica Intima metabolism

Abstract

The heparan sulfate (HS) proteoglycan perlecan is a major component of basement membranes, plays a key role in extracellular matrix (ECM) structure, interacts with growth factors and adhesion molecules, and regulates the adhesion, differentiation and proliferation of vascular cells. Atherosclerosis is characterized by chronic inflammation and the presence of oxidized materials within lesions, with the majority of protein damage present on ECM, rather than cell, proteins. Weakening of ECM structure plays a key role in lesion rupture, the major cause of heart attacks and strokes. In this study peroxynitrite, a putative lesion oxidant, is shown to damage perlecan structurally and functionally. Exposure of human perlecan to peroxynitrite decreases recognition by antibodies raised against both the core protein and heparan sulfate chains; dose-dependent formation of 3-nitrotyrosine was also detected. These effects were modulated by bicarbonate and reaction pH. Oxidant exposure resulted in aggregate formation, consistent with oxidative protein crosslinking. Peroxynitrite treatment modified functional properties of perlecan that are dependent on both the protein core (decreased binding of human coronary artery endothelial cells), and the HS chains (diminished fibroblast growth factor-2 (FGF-2) receptor-mediated proliferation of Baf-32 cells). The latter is consistent with a decrease in FGF-2 binding to the HS chains of modified perlecan. Immunofluorescence of advanced human atherosclerotic lesions provided evidence for the presence of perlecan and extensive formation of 3-nitrotyrosine epitopes within the intimal region; these materials showing marked co-localization. These data indicate that peroxynitrite induces major structural and functional changes to perlecan and that damage to this material occurs within human atherosclerotic lesions., (Copyright 2010 Elsevier Inc. All rights reserved.)

Published

2010