Your search keyword '"Hemopexin chemistry"' showing total 137 results

1. Free heme and hemopexin in acute kidney injury after cardiopulmonary bypass and transient renal ischemia.

Author

Greite R, Schott S, Wang L, Gohlke L, Kreimann K, Derlin K, Gutberlet M, Schmidbauer M, Leffler A, Tudorache I, Salman J, Ius F, Natanov R, Fegbeutel C, Haverich A, Lichtinghagen R, Hüsing AM, von Vietinghoff S, Schmitt R, Shushakova N, Rong S, Haller H, Schmidt-Ott KM, Gram M, Vijayan V, Scheffner I, Gwinner W, and Immenschuh S

Subjects

Animals, Humans, Mice, Cardiopulmonary Bypass adverse effects, Heme, Hemoglobins metabolism, Hemolysis, Ischemia complications, Kidney metabolism, Mice, Inbred C57BL, Acute Kidney Injury diagnosis, Acute Kidney Injury etiology, Hemopexin chemistry, Hemopexin metabolism, Reperfusion Injury etiology

Abstract

Free heme is released from hemoproteins during hemolysis or ischemia reperfusion injury and can be pro-inflammatory. Most studies on nephrotoxicity of hemolysis-derived proteins focus on free hemoglobin (fHb) with heme as a prosthetic group. Measurement of heme in its free, non-protein bound, form is challenging and not commonly used in clinical routine diagnostics. In contrast to fHb, the role of free heme in acute kidney injury (AKI) after cardiopulmonary bypass (CPB) surgery is unknown. Using an apo-horseradish peroxidase-based assay, we identified free heme during CPB surgery as predictor of AKI in patients undergoing cardiac valve replacement (n = 37). Free heme levels during CPB surgery correlated with depletion of hemopexin (Hx), a heme scavenger-protein. In mice, the impact of high levels of circulating free heme on the development of AKI following transient renal ischemia and the therapeutic potential of Hx were investigated. C57BL/6 mice were subjected to bilateral renal ischemia/reperfusion injury for 15 min which did not cause AKI. However, additional administration of free heme in this model promoted overt AKI with reduced renal function, increased renal inflammation, and reduced renal perfusion on functional magnetic resonance imaging. Hx treatment attenuated AKI. Free heme administration to sham operated control mice did not cause AKI. In conclusion, free heme is a predictor of AKI in CPB surgery patients and promotes AKI in transient renal ischemia. Depletion of Hx in CPB surgery patients and attenuation of AKI by Hx in the in vivo model encourage further research on Hx therapy in patients with increased free heme levels during CPB surgery., (© 2023 The Authors. Clinical and Translational Science published by Wiley Periodicals LLC on behalf of American Society for Clinical Pharmacology and Therapeutics.)

Published

2023

2. Detecting the PEX Like Domain of Matrix Metalloproteinase-14 (MMP-14) with Therapeutic Conjugated CNTs.

Author

Vieira D, Barralet J, Harvey EJ, and Merle G

Subjects

Hemopexin chemistry, Hemopexin metabolism, Hemopexin pharmacology, Matrix Metalloproteinase 1 metabolism, Protein Structure, Tertiary, Matrix Metalloproteinase 14 chemistry, Matrix Metalloproteinase 14 metabolism, Nanotubes, Carbon

Abstract

Matrix metalloproteinases (MMPs) are essential proteins acting directly in the breakdown of the extra cellular matrix and so in cancer invasion and metastasis. Given its impact on tumor angiogenesis, monitoring MMP-14 provides strategic insights on cancer severity and treatment. In this work, we report a new approach to improve the electrochemical interaction of the MMP-14 with the electrode surface while preserving high specificity. This is based on the detection of the hemopexin (PEX) domain of MMP-14, which has a greater availability with a stable and low-cost commercial molecule, as a recognition element. This molecule, called NSC-405020, is specific of the PEX domain of MMP-14 within the binding pocket. Through the covalent grafting of the NSC-405020 molecule on carbon nanotubes (CNTs), we were able to detect and quantify MMP-14 using electrochemical impedance spectroscopy with a linear range of detection of 10 ng⋅mL -1 to 100 ng⋅mL -1 , and LOD of 7.5 ng⋅mL -1 . The specificity of the inhibitory small molecule was validated against the PEX domain of MMP-1. The inhibitor loaded CNTs system showed as a desirable candidate to become an alternative to the conventional recognition bioelements for the detection of MMP-14.

Published

2022

3. Identification and characterization of warm temperature acclimation proteins (Wap65s) in rainbow trout (Oncorhynchus mykiss).

Author

Roh H, Park J, Park J, Kim BS, Park CI, and Kim DH

Subjects

Acclimatization, Amino Acid Sequence, Animals, Dextrans, Fish Proteins metabolism, Hemopexin chemistry, Hemopexin genetics, Hemopexin metabolism, Iron, Lipopolysaccharides, Mammals, Phylogeny, Temperature, Fish Diseases, Oncorhynchus mykiss

Abstract

Hemopexin is a vital glycoprotein for processing excessive iron in blood and functions as an iron scavenger in mammals. Teleosts however, unlike mammals, have two known hemopexin paralogs called warm temperature acclimation-related 65 kDa protein (Wap65-1 and Wap65-2, collectively termed Wap65s). Although Wap65s in rainbow trout have been considered notable biomarkers with significantly higher and/or lower expression under conditions of stress or disease, the individual roles, similarities and differences between the two paralogs are not well known. The aim of this study was to gain an understanding of the characteristics and functions of trout Wap65s from the perspective of iron-metabolism, physiological roles, and relevant immunological responses. The expression of Wap65-1 and -2 in this study was determined in the face of challenges by Aeromonas salmonicida, infectious hematopoietic necrosis virus (IHNV), and iron-dextran. Immuno-histochemistry (IHC) was employed to localize the major cell types for Wap65-2 expression, and trout leukocytes were isolated and incubated with LPS and OxLDL for comprehending the immunological characteristics of Wap65-2. We demonstrate that Wap65-1 is expressed only in the liver but Wap65-2 is systemically expressed in most organs and tissues. Interestingly, Wap65-1 expression was not significantly changed under A. salmonicida and iron-dextran administration, but was significantly decreased under IHNV. In contrast, Wap65-2 was up-regulated in all challenged groups, however with different expression patterns in the blood and liver. These results suggested that the two paralogs may participate in different biological roles. IHC showed that Wap65-2 antibody had high affinity for leukocyte-like cells, and macrophages but not lymphocytes significantly increased expression under LPS and OxLDL stimulation. These results support the conclusion that trout Wap65-2, not Wap65-1 may have conventional hemopexin functions such as reported in mammals including effects on iron metabolism, inflammation, and acute-phase protein., (Copyright © 2022 Elsevier Ltd. All rights reserved.)

Published

2022

4. Modular Platform for the Development of Recombinant Hemoglobin Scavenger Biotherapeutics.

Author

Buzzi RM, Owczarek CM, Akeret K, Tester A, Pereira N, Butcher R, Brügger-Verdon V, Hardy MP, Illi M, Wassmer A, Vallelian F, Humar R, Hugelshofer M, Buehler PW, Gentinetta T, and Schaer DJ

Subjects

Animals, Antigens, CD metabolism, Antigens, Differentiation, Myelomonocytic metabolism, Basilar Artery drug effects, Biological Products chemistry, Biological Products pharmacology, HEK293 Cells, Haptoglobins chemistry, Haptoglobins genetics, Heme metabolism, Hemoglobins chemistry, Hemolysis, Hemopexin chemistry, Hemopexin genetics, Humans, Protein Binding, Receptors, Cell Surface metabolism, Receptors, Scavenger metabolism, Recombinant Fusion Proteins genetics, Serum Albumin, Human chemistry, Serum Albumin, Human genetics, Serum Albumin, Human metabolism, Swine, Transfection, Vasodilation drug effects, Biological Products metabolism, Drug Design methods, Haptoglobins metabolism, Hemoglobins metabolism, Hemopexin metabolism, Recombinant Fusion Proteins metabolism, Recombinant Fusion Proteins pharmacology

Abstract

Cell-free hemoglobin (Hb) is a driver of disease progression in conditions with intravascular or localized hemolysis. Genetic and acquired anemias or emergency medical conditions such as aneurysmal subarachnoid hemorrhage involve tissue Hb exposure. Haptoglobin (Hp) captures Hb in an irreversible protein complex and prevents its pathophysiological contributions to vascular nitric oxide depletion and tissue oxidation. Preclinical proof-of-concept studies suggest that human plasma-derived Hp is a promising therapeutic candidate for several Hb-driven diseases. Optimizing the efficacy and safety of Hb-targeting biotherapeutics may require structural and functional modifications for specific indications. Improved Hp variants could be designed to achieve the desired tissue distribution, metabolism, and elimination to target hemolytic disease states effectively. However, it is critical to ensure that these modifications maintain the function of Hp. Using transient mammalian gene expression of Hp combined with co-transfection of the pro-haptoglobin processing protease C1r-LP, we established a platform for generating recombinant Hp-variants. We designed an Hpβ-scaffold, which was expressed in this system at high levels as a monomeric unit (mini-Hp) while maintaining the key protective functions of Hp. We then used this Hpβ-scaffold as the basis to develop an initial proof-of-concept Hp fusion protein using human serum albumin as the fusion partner. Next, a hemopexin-Hp fusion protein with bispecific heme and Hb detoxification capacity was generated. Further, we developed a Hb scavenger devoid of CD163 scavenger receptor binding. The functions of these proteins were then characterized for Hb and heme-binding, binding of the Hp-Hb complexes with the clearance receptor CD163, antioxidant properties, and vascular nitric oxide sparing capacity. Our platform is designed to support the generation of innovative Hb scavenger biotherapeutics with novel modes of action and potentially improved formulation characteristics, function, and pharmacokinetics.

Published

2021

5. Revisiting the interaction of heme with hemopexin.

Author

Detzel MS, Schmalohr BF, Steinbock F, Hopp MT, Ramoji A, Paul George AA, Neugebauer U, and Imhof D

Subjects

Humans, Models, Molecular, Spectrophotometry, Ultraviolet, Surface Plasmon Resonance, Heme chemistry, Hemopexin chemistry

Abstract

In hemolytic disorders, erythrocyte lysis results in massive release of hemoglobin and, subsequently, toxic heme. Hemopexin is the major protective factor against heme toxicity in human blood and currently considered for therapeutic use. It has been widely accepted that hemopexin binds heme with extraordinarily high affinity of <1 pM in a 1:1 ratio. However, several lines of evidence point to a higher stoichiometry and lower affinity than determined 50 years ago. Here, we re-analyzed these data. SPR and UV/Vis spectroscopy were used to monitor the interaction of heme with the human protein. The heme-binding sites of hemopexin were characterized using hemopexin-derived peptide models and competitive displacement assays. We obtained a K D value of 0.32 ± 0.04 nM and the ratio for the interaction was determined to be 1:1 at low heme concentrations and at least 2:1 (heme:hemopexin) at high concentrations. We were able to identify two yet unknown potential heme-binding sites on hemopexin. Furthermore, molecular modelling with a newly created homology model of human hemopexin suggested a possible recruiting mechanism by which heme could consecutively bind several histidine residues on its way into the binding pocket. Our findings have direct implications for the potential administration of hemopexin in hemolytic disorders., (© 2021 Walter de Gruyter GmbH, Berlin/Boston.)

Published

2021

6. Human Plasma and Recombinant Hemopexins: Heme Binding Revisited.

Author

Karnaukhova E, Owczarek C, Schmidt P, Schaer DJ, and Buehler PW

Subjects

Biological Transport, Circular Dichroism, Heme chemistry, Hemopexin chemistry, Humans, Hydrogen Peroxide metabolism, Methemalbumin, Nitric Oxide metabolism, Photoelectron Spectroscopy, Protein Binding, Temperature, Heme metabolism, Hemopexin metabolism, Recombinant Proteins

Abstract

Plasma hemopexin (HPX) is the key antioxidant protein of the endogenous clearance pathway that limits the deleterious effects of heme released from hemoglobin and myoglobin (the term "heme" is used in this article to denote both the ferrous and ferric forms). During intra-vascular hemolysis, heme partitioning to protein and lipid increases as the plasma concentration of HPX declines. Therefore, the development of HPX as a replacement therapy during high heme stress could be a relevant intervention for hemolytic disorders. A logical approach to enhance HPX yield involves recombinant production strategies from human cell lines. The present study focuses on a biophysical assessment of heme binding to recombinant human HPX (rhHPX) produced in the Expi293F TM (HEK293) cell system. In this report, we examine rhHPX in comparison with plasma HPX using a systematic analysis of protein structural and functional characteristics related to heme binding. Analysis of rhHPX by UV/Vis absorption spectroscopy, circular dichroism (CD), size-exclusion chromatography (SEC)-HPLC, and catalase-like activity demonstrated a similarity to HPX fractionated from plasma. In particular, the titration of HPX apo-protein(s) with heme was performed for the first time using a wide range of heme concentrations to model HPX-heme interactions to approximate physiological conditions (from extremely low to more than two-fold heme molar excess over the protein). The CD titration data showed an induced bisignate CD Soret band pattern typical for plasma and rhHPX versions at low heme-to-protein molar ratios and demonstrated that further titration is dependent on the amount of protein-bound heme to the extent that the arising opposite CD couplet results in a complete inversion of the observed CD pattern. The data generated in this study suggest more than one binding site in both plasma and rhHPX. Furthermore, our study provides a useful analytical platform for the detailed characterization of HPX-heme interactions and potentially novel HPX fusion constructs.

Published

2021

7. Comparison of Different HILIC Stationary Phases in the Separation of Hemopexin and Immunoglobulin G Glycopeptides and Their Isomers.

Author

Molnarova K and Kozlík P

Subjects

Amides chemistry, Chromatography, Liquid instrumentation, Glycopeptides chemistry, Glycopeptides isolation & purification, Glycopeptides metabolism, Glycosylation, Hemopexin chemistry, Humans, Hydrophobic and Hydrophilic Interactions, Immunoglobulin G chemistry, Isomerism, Polysaccharides chemistry, Temperature, Trypsin chemistry, Chromatography, Liquid methods, Hemopexin isolation & purification, Immunoglobulin G isolation & purification

Abstract

Protein glycosylation analysis is challenging due to the structural variety of complex conjugates. However, chromatographically separating glycans attached to tryptic peptides enables their site-specific characterization. For this purpose, we have shown the importance of selecting a suitable hydrophilic interaction liquid chromatography (HILIC) stationary phase in the separation of glycopeptides and their isomers. Three different HILIC stationary phases, i.e., HALO ® penta-HILIC, Glycan ethylene bridged hybrid (BEH) Amide, and ZIC-HILIC, were compared in the separation of complex N -glycopeptides of hemopexin and Immunoglobulin G glycoproteins. The retention time increased with the polarity of the glycans attached to the same peptide backbone in all HILIC columns tested in this study, except for the ZIC-HILIC column when adding sialic acid to the glycan moiety, which caused electrostatic repulsion with the negatively charged sulfobetaine functional group, thereby decreasing retention. The HALO ® penta-HILIC column provided the best separation results, and the ZIC-HILIC column the worst. Moreover, we showed the potential of these HILIC columns for the isomeric separation of fucosylated and sialylated glycoforms. Therefore, HILIC is a useful tool for the comprehensive characterization of glycoproteins and their isomers.

Published

2020

8. The Diversity of Mammalian Hemoproteins and Microbial Heme Scavengers Is Shaped by an Arms Race for Iron Piracy.

Author

Mozzi A, Forni D, Clerici M, Cagliani R, and Sironi M

Subjects

Animals, Bacterial Proteins metabolism, Cation Transport Proteins metabolism, Haemophilus influenzae chemistry, Haemophilus influenzae metabolism, Haptoglobins metabolism, Hemopexin metabolism, Humans, Iron metabolism, Neisseria meningitidis chemistry, Neisseria meningitidis metabolism, Protozoan Proteins metabolism, Receptors, Cell Surface metabolism, Staphylococcus aureus chemistry, Staphylococcus aureus metabolism, Trypanosoma brucei brucei chemistry, Trypanosoma brucei brucei metabolism, Bacterial Proteins chemistry, Cation Transport Proteins chemistry, Haptoglobins chemistry, Hemopexin chemistry, Iron chemistry, Protozoan Proteins chemistry, Receptors, Cell Surface chemistry

Abstract

Iron is an essential micronutrient for most living species. In mammals, hemoglobin (Hb) stores more than two thirds of the body's iron content. In the bloodstream, haptoglobin (Hp) and hemopexin (Hpx) sequester free Hb or heme. Pathogenic microorganisms usually acquire iron from their hosts and have evolved complex systems of iron piracy to circumvent nutritional immunity. Herein, we performed an evolutionary analysis of genes coding for mammalian heme-binding proteins and heme-scavengers in pathogen species. The underlying hypothesis is that these molecules are engaged in a molecular arms race. We show that positive selection drove the evolution of mammalian Hb and Hpx. Positively selected sites in Hb are located at the interaction surface with Neisseria meningitidis heme scavenger HpuA and with Staphylococcus aureus iron-regulated surface determinant B (IsdB). In turn, positively selected sites in HpuA and IsdB are located in the flexible protein regions that contact Hb. A residue in Hb (S45H) was also selected on the Caprinae branch. This site stabilizes the interaction with Trypanosoma brucei hemoglobin-haptoglobin (HbHp) receptor ( Tb HpHbR), a molecule that also mediates trypanosome lytic factor (TLF) entry. In Tb HpHbR, positive selection drove the evolution of a variant (L210S) which allows evasion from TLF but reduces affinity for HbHp. Finally, selected sites in Hpx are located at the interaction surface with the Haemophilus influenzae hemophore HxuA, which in turn displays fast evolving sites at the Hpx-binding interface. These results shed light into host-pathogens conflicts and establish the importance of nutritional immunity as an evolutionary force.

Published

2018

9. Proteomic Characterization of the Heart and Skeletal Muscle Reveals Widespread Arginine ADP-Ribosylation by the ARTC1 Ectoenzyme.

Author

Leutert M, Menzel S, Braren R, Rissiek B, Hopp AK, Nowak K, Bisceglie L, Gehrig P, Li H, Zolkiewska A, Koch-Nolte F, and Hottiger MO

Subjects

ADP Ribose Transferases chemistry, ADP Ribose Transferases genetics, ADP-Ribosylation, Animals, Arginine metabolism, Carrier Proteins classification, Carrier Proteins genetics, Carrier Proteins metabolism, Cell Line, Gene Ontology, Heme chemistry, Heme metabolism, Hemopexin chemistry, Hemopexin genetics, Isoenzymes chemistry, Isoenzymes genetics, Isoenzymes metabolism, Male, Membrane Proteins classification, Membrane Proteins genetics, Membrane Proteins metabolism, Mice, Mice, Knockout, Molecular Sequence Annotation, Muscle Fibers, Skeletal metabolism, Muscle Fibers, Skeletal pathology, Muscle Proteins classification, Muscle Proteins metabolism, Muscle Weakness metabolism, Muscle Weakness pathology, Muscle, Skeletal pathology, Myocardium pathology, Protein Binding, Proteome genetics, Proteome metabolism, Proteomics methods, Signal Transduction, ADP Ribose Transferases metabolism, Hemopexin metabolism, Muscle Proteins genetics, Muscle Weakness genetics, Muscle, Skeletal metabolism, Myocardium metabolism, Protein Processing, Post-Translational

Abstract

The clostridium-like ecto-ADP-ribosyltransferase ARTC1 is expressed in a highly restricted manner in skeletal muscle and heart tissue. Although ARTC1 is well studied, the identification of ARTC1 targets in vivo and subsequent characterization of ARTC1-regulated cellular processes on the proteome level have been challenging and only a few ARTC1-ADP-ribosylated targets are known. Applying our recently developed mass spectrometry-based workflow to C2C12 myotubes and to skeletal muscle and heart tissues from wild-type mice, we identify hundreds of ARTC1-ADP-ribosylated proteins whose modifications are absent in the ADP-ribosylome of ARTC1-deficient mice. These proteins are ADP-ribosylated on arginine residues and mainly located on the cell surface or in the extracellular space. They are associated with signal transduction, transmembrane transport, and muscle function. Validation of hemopexin (HPX) as a ARTC1-target protein confirmed the functional importance of ARTC1-mediated extracellular arginine ADP-ribosylation at the systems level., (Copyright © 2018 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2018

10. Hydrophilic interaction liquid chromatography in the separation of glycopeptides and their isomers.

Author

Kozlik P, Goldman R, and Sanda M

Subjects

Amino Acid Sequence, Glycopeptides isolation & purification, Humans, Hydrophobic and Hydrophilic Interactions, Isomerism, Proteomics methods, Chromatography, Liquid methods, Glycopeptides analysis, Hemopexin chemistry, Tandem Mass Spectrometry methods

Abstract

The analysis of intact glycopeptides is a challenge because of the structural variety of the complex conjugates. In this work, we used separation involving hydrophilic interaction liquid chromatography using a superficially porous particle HALO® penta-HILIC column with tandem mass spectrometric detection for the analysis of N-glycopeptides of hemopexin. We tested the effect of the mobile phase composition on retention and separation of the glycopeptides. The results indicated that the retention of the glycopeptides was the combination of partitioning and adsorption processes. Under the optimized conditions, our HILIC method showed the ability to efficiently separate the glycoforms of the same peptide backbone including separation of the isobaric glycoforms. We achieved efficient separation of core and outer arm linked fucose of bi-antennary and tri-antennary glycoforms of the SWPAVGNCSSALR peptide and bi-antennary glycoform of the ALPQPQNVTSLLGCTH peptide, respectively. Moreover, we demonstrated the separation of antennary position of sialic acid linked via α2-6 linkage of the monosialylated glycopeptides. Glycopeptide isomers are often differentially associated with various biological processes. Therefore, chromatographic separation of the species without the need for an extensive sample preparation appears attractive for their identification, characterization, and reliable quantification.

Published

2018

11. Prospective plasma proteome changes in preterm infants with different gestational ages.

Author

Suski M, Bokiniec R, Szwarc-Duma M, Madej J, Bujak-Giżycka B, Kwinta P, Borszewska-Kornacka MK, Revhaug C, Baumbusch LO, Saugstad OD, and Pietrzyk JJ

Subjects

Female, Hemopexin chemistry, Homeostasis, Humans, Infant, Newborn, Inflammation, Male, Obstetric Labor, Premature, Pregnancy, Prospective Studies, Spectrometry, Mass, Electrospray Ionization, Tandem Mass Spectrometry, Blood Proteins chemistry, Gestational Age, Infant, Premature blood, Proteome chemistry

Abstract

Background: In this study, we aimed to analyze time-resolved plasma proteome changes in preterm neonates stratified by their gestational age to detect malfunctioning pathways that derive from the systemic immaturity of the neonate and to highlight those that are differentially regulated during the early development., Methods: Preterm newborns were enrolled in three subgroups with different gestational ages: before 26 weeks of gestation (group 1), between 27 and 28 weeks of gestation (group 2), and between 29 and 30 (group 3) weeks of gestation. Plasma protein abundances were assessed at two time points (at preterm delivery and at the 36th week of post-menstrual age) by quantitative proteomics., Result: The quantitative analysis of plasma proteome in preterm infants revealed a multitude of time-related differences in protein abundances between the studied groups. We report protein changes in several functional domains, including inflammatory domains, immunomodulatory factors, and coagulation regulators as key features, with important gestational age-dependent hemopexin induction., Conclusion: The global trend emerging from our data, which can collectively be interpreted as a progression toward recovery from the perinatal perturbations, highlights the profound impact of gestation duration on the ability to bridge the gap in systemic homeostasis after preterm labor.

Published

2018

12. Co-precipitation molecules hemopexin and transferrin may be key molecules for fibrillogenesis in TTR V30M amyloidogenesis.

Author

Ohta M, Sugano A, Hatano N, Sato H, Shimada H, Niwa H, Sakaeda T, Tei H, Sakaki Y, Yamamura KI, and Takaoka Y

Subjects

Amyloid metabolism, Amyloid Neuropathies, Familial genetics, Animals, Blood Proteins analysis, Blood Proteins metabolism, Computer Simulation, Disease Models, Animal, Electrophoresis, Polyacrylamide Gel, Hemopexin chemistry, Hemopexin genetics, Humans, Intestine, Small metabolism, Intestine, Small pathology, Mice, Transgenic, Molecular Dynamics Simulation, Prealbumin metabolism, Transferrin chemistry, Transferrin genetics, Amyloid genetics, Amyloid Neuropathies, Familial etiology, Hemopexin metabolism, Prealbumin genetics, Transferrin metabolism

Abstract

The disease model of familial amyloidotic polyneuropathy-7.2-hMet30 mice-manifests amyloid deposition that consists of a human amyloidogenic mutant transthyretin (TTR) (TTR V30M). Our previous study found amyloid deposits in 14 of 27 7.2-hMet30 mice at 21-24 months of age. In addition, non-fibrillar TTR deposits were found in amyloid-negative 7.2hMet30 mice. These results suggested that TTR amyloidogenesis required not only mutant TTR but also an additional factor (or factors) as an etiologic molecule. To determine the differences in serum proteome in amyloid-positive and amyloid-negative mice in the 7.2-hMet30 model, we used proteomic analyses and studied serum samples obtained from these mice. Hemopexin (HPX) and transferrin (Tf) were detected in the serum samples from amyloid-positive mice and were also found in amyloid deposits via immunohistochemistry, but serum samples from amyloid-negative mice did not contain HPX and Tf. These two proteins were also not detected in non-fibrillar TTR deposits. In addition, in silico analyses suggested that HPX and Tf facilitate destabilization of TTR secondary structures and misfolding of TTR. These results suggest that HPX and Tf may be associated with TTR amyloidogenesis after fibrillogenesis in vivo.

Published

2018

13. Targeting the Hemopexin-like Domain of Latent Matrix Metalloproteinase-9 (proMMP-9) with a Small Molecule Inhibitor Prevents the Formation of Focal Adhesion Junctions.

Author

Alford VM, Kamath A, Ren X, Kumar K, Gan Q, Awwa M, Tong M, Seeliger MA, Cao J, Ojima I, and Sampson NS

Subjects

Animals, COS Cells, Cell Line, Tumor, Cell Movement drug effects, Chickens, Chlorocebus aethiops, Enzyme Precursors chemistry, Focal Adhesions metabolism, Hemopexin chemistry, Humans, Hyaluronan Receptors metabolism, Integrin alpha4beta1 metabolism, Matrix Metalloproteinase 9 chemistry, Models, Molecular, Neoplasms drug therapy, Neoplasms metabolism, Small Molecule Libraries chemistry, Small Molecule Libraries pharmacology, Enzyme Precursors antagonists & inhibitors, Enzyme Precursors metabolism, Focal Adhesions drug effects, Matrix Metalloproteinase 9 metabolism, Matrix Metalloproteinase Inhibitors chemistry, Matrix Metalloproteinase Inhibitors pharmacology, Protein Domains drug effects

Abstract

A lack of target specificity has greatly hindered the success of inhibitor development against matrix metalloproteinases (MMPs) for the treatment of various cancers. The MMP catalytic domains are highly conserved, whereas the hemopexin-like domains of MMPs are unique to each family member. The hemopexin-like domain of MMP-9 enhances cancer cell migration through self-interaction and heterointeractions with cell surface proteins including CD44 and α4β1 integrin. These interactions activate EGFR-MAP kinase dependent signaling that leads to cell migration. In this work, we generated a library of compounds, based on hit molecule N-[4-(difluoromethoxy)phenyl]-2-[(4-oxo-6-propyl-1H-pyrimidin-2-yl)sulfanyl]-acetamide, that target the hemopexin-like domain of MMP-9. We identify N-(4-fluorophenyl)-4-(4-oxo-3,4,5,6,7,8-hexahydroquinazolin-2-ylthio)butanamide, 3c, as a potent lead (K d = 320 nM) that is specific for binding to the proMMP-9 hemopexin-like domain. We demonstrate that 3c disruption of MMP-9 homodimerization prevents association of proMMP-9 with both α4β1 integrin and CD44 and results in the dissociation of EGFR. This disruption results in decreased phosphorylation of Src and its downstream target proteins focal adhesion kinase (FAK) and paxillin (PAX), which are implicated in promoting tumor cell growth, migration, and invasion. Using a chicken chorioallantoic membrane in vivo assay, we demonstrate that 500 nM 3c blocks cancer cell invasion of the basement membrane and reduces angiogenesis. In conclusion, we present a mechanism of action for 3c whereby targeting the hemopexin domain results in decreased cancer cell migration through simultaneous disruption of α4β1 integrin and EGFR signaling pathways, thereby preventing signaling bypass. Targeting through the hemopexin-like domain is a powerful approach to antimetastatic drug development.

Published

2017

14. A novel function of N-linked glycoproteins, alpha-2-HS-glycoprotein and hemopexin: Implications for small molecule compound-mediated neuroprotection.

Author

Kanno T, Yasutake K, Tanaka K, Hadano S, and Ikeda JE

Subjects

Animals, Cattle, Cell Death drug effects, Central Nervous System pathology, Hemopexin chemistry, Humans, Mice, Neurons drug effects, Neurons pathology, Neuroprotective Agents administration & dosage, Neuroprotective Agents chemistry, Oxidative Stress drug effects, Small Molecule Libraries chemistry, alpha-2-HS-Glycoprotein chemistry, Acetamides administration & dosage, Central Nervous System drug effects, Culture Media chemistry, Hemopexin metabolism, Imidazoles administration & dosage, Small Molecule Libraries administration & dosage, alpha-2-HS-Glycoprotein metabolism

Abstract

Therapeutic agents to the central nervous system (CNS) need to be efficiently delivered to the target site of action at appropriate therapeutic levels. However, a limited number of effective drugs for the treatment of neurological diseases has been developed thus far. Further, the pharmacological mechanisms by which such therapeutic agents can protect neurons from cell death have not been fully understood. We have previously reported the novel small-molecule compound, 2-[mesityl(methyl)amino]-N-[4-(pyridin-2-yl)-1H-imidazol-2-yl] acetamide trihydrochloride (WN1316), as a unique neuroprotectant against oxidative injury and a highly promising remedy for the treatment of amyotrophic lateral sclerosis (ALS). One of the remarkable characteristics of WN1316 is that its efficacious doses in ALS mouse models are much less than those against oxidative injury in cultured human neuronal cells. It is also noted that the WN1316 cytoprotective activity observed in cultured cells is totally dependent upon the addition of fetal bovine serum in culture medium. These findings led us to postulate some serum factors being tightly linked to the WN1316 efficacy. In this study, we sieved through fetal bovine serum proteins and identified two N-linked glycoproteins, alpha-2-HS-glycoprotein (AHSG) and hemopexin (HPX), requisites to exert the WN1316 cytoprotective activity against oxidative injury in neuronal cells in vitro. Notably, the removal of glycan chains from these molecules did not affect the WN1316 cytoprotective activity. Thus, two glycoproteins, AHSG and HPX, represent a pivotal glycoprotein of the cytoprotective activity for WN1316, showing a concrete evidence for the novel glycan-independent function of serum glycoproteins in neuroprotective drug efficacy.

Published

2017

15. Identification of oxidative modifications of hemopexin and their predicted physiological relevance.

Author

Hahl P, Hunt R, Bjes ES, Skaff A, Keightley A, and Smith A

Subjects

Amino Acid Sequence, Animals, Apoproteins chemistry, Apoproteins isolation & purification, Apoproteins metabolism, Binding Sites, Chromatography, High Pressure Liquid, Conserved Sequence, Heme chemistry, Heme metabolism, Hemopexin chemistry, Hemopexin isolation & purification, Humans, Kinetics, Ligands, Molecular Structure, Oxidation-Reduction, Protein Conformation, Rabbits, Rats, Reactive Oxygen Species chemistry, Reactive Oxygen Species metabolism, Species Specificity, Tandem Mass Spectrometry, Tryptophan chemistry, Tyrosine chemistry, Hemopexin metabolism, Models, Molecular

Abstract

Hemopexin protects against heme toxicity in hemolytic diseases and conditions, sepsis, and sickle cell disease. This protection is sustained by heme-hemopexin complexes in biological fluids that resist oxidative damage during heme-driven inflammation. However, apo-hemopexin is vulnerable to inactivation by reactive nitrogen (RNS) and oxygen species (ROS) that covalently modify amino acids. The resultant nitration of amino acids is considered a specific effect reflecting biological events. Using LC-MS, we discovered low endogenous levels of tyrosine nitration in the peptide YYCFQGNQFLR in the heme-binding site of human hemopexin, which was similarly nitrated in rabbit and rat hemopexins. Immunoblotting and selective reaction monitoring were used to quantify tyrosine nitration of in vivo samples and when hemopexin was incubated in vitro with nitrating nitrite/myeloperoxidase/glucose oxidase. Significantly, heme binding by hemopexin declined as tyrosine nitration proceeded in vitro Three nitrated tyrosines reside in the heme-binding site of hemopexin, and we found that one, Tyr-199, interacts directly with the heme ring D propionate. Investigating the oxidative modifications of amino acids after incubation with tert -butyl hydroperoxide and hypochlorous acid in vitro , we identified additional covalent oxidative modifications on four tyrosine residues and one tryptophan residue of hemopexin. Importantly, three of the four modified tyrosines, some of which have more than one modification, cluster in the heme-binding site, supporting a hierarchy of vulnerable amino acids. We propose that during inflammation, apo-hemopexin is nitrated and oxidated in niches of the body containing activated RNS- and ROS-generating immune and endothelial cells, potentially impairing hemopexin's protective extracellular antioxidant function., (© 2017 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2017

16. Ensnaring membrane type 1-matrix metalloproteinase (MT1-MMP) with tissue inhibitor of metalloproteinase (TIMP)-2 using the haemopexin domain of the protease as a carrier: a targeted approach in cancer inhibition.

Author

Jiang B, Zhang Y, Liu J, Tsigkou A, Rapti M, and Lee MH

Subjects

Amino Acid Sequence, Apoptosis drug effects, Biomarkers, Tumor metabolism, Cell Movement drug effects, Cell Proliferation drug effects, Extracellular Matrix metabolism, Fibrosarcoma metabolism, Fibrosarcoma pathology, HeLa Cells, Humans, Matrix Metalloproteinase 14 metabolism, Tumor Cells, Cultured, Fibrosarcoma drug therapy, Hemopexin chemistry, Matrix Metalloproteinase 14 chemistry, Matrix Metalloproteinase Inhibitors pharmacology, Tissue Inhibitor of Metalloproteinase-2 pharmacology

Abstract

Metastatic cancer cells express Membrane Type 1-Matrix Metalloproteinase (MT1-MMP) to degrade the extracellular matrix in order to facilitate migration and proliferation. Tissue Inhibitor of Metalloproteinase (TIMP)-2 is the endogenous inhibitor of the MMP. Here, we describe a novel and highly effective fusion strategy to enhance the delivery of TIMP-2 to MT1-MMP. We can reveal that TIMP-2 fused to the haemopexin +/- transmembrane domains of MT1-MMP (two chimeras named T2PEX+TM and T2PEX) are able to interact with MT1-MMP on the cell surface as well as intracellularly. In the case of T2PEX+TM, there is even a clear sign of MT1-MMP:T2PEX+TM aggregation by the side of the nucleus to form aggresomes. In vitro, T2PEX+TM and T2PEX suppress the gelatinolytic and invasive abilities of cervical carcinoma (HeLa) and HT1080 fibrosarcoma cancer cells significantly better than wild type TIMP-2. In mouse xenograft, we further demonstrate that T2PEX diminishes cervical carcinoma growth by 85% relative to the control. Collectively, our findings indicate the effectiveness of the fusion strategy as a potential targeted approach in cancer inhibition.

Published

2017

17. Nano-LC-MS/MS for the identification of proteins trapped in sorbent cartridges used for coupled plasma filtration-adsorption treatments of healthy pigs.

Author

Nardiello D, Prattichizzo C, Rocchetti MT, Gesualdo L, and Centonze D

Subjects

Acute-Phase Reaction, Animals, Cattle, Computational Biology, Cytochromes c chemistry, Electrophoresis, Gel, Two-Dimensional, Electrophoresis, Polyacrylamide Gel, Filtration, Haptoglobins chemistry, Hemopexin chemistry, Inflammation, Orosomucoid chemistry, Proteolysis, Sepsis blood, Sepsis therapy, Software, Sorption Detoxification methods, Swine, alpha-2-HS-Glycoprotein chemistry, Chromatography, Liquid methods, Proteins chemistry, Tandem Mass Spectrometry methods

Abstract

A dedicated proteomic approach based on nano-Liquid Chromatography coupled with tandem mass spectrometry in ion trap is proposed for the analysis of proteins trapped in sorbent resin cartridges used to remove inflammatory mediators from blood by coupled plasma filtration adsorption (CPFA). The final purpose of the proposed proteomic approach was to obtain a reference map of plasma proteins trapped in CPFA sorbents used for the extracorporeal blood purification of healthy pigs, with the potential impact to design new bio-filters able to control the inflammatory imbalance under pathological conditions, such as severe sepsis. The five main steps of the proteomics analysis, (i) protein extraction from resin cartridges, (ii) two-dimensional gel electrophoresis (2D-PAGE) for protein separation and profiling, (iii) in-gel proteolytic digestion, (iv) tandem mass analysis of peptides resulting from enzymatic cleavage and (v) bioinformatics, for protein identification and post-processing validation of MS/MS data sets, have been carefully evaluated. Prior to electrophoresis, the efficiency of different extraction solutions and procedures to recovery plasma proteins trapped into the sorbents were tested. Then, a rapid one-step procedure for protein extraction was optimized. Protein bands corresponding to the main plasma proteins, namely porcine serum albumin, serotransferrin and immunoglobulins, were identified. In addition, the presence of haptoglobin, hemopexin, α-1 acid glycoprotein and fetuin-A, that are known as acute-phase reaction proteins, was observed, suggesting that CPFA resins led to a non-specifically protein depletion from plasma, rather than targeting specific molecules., (Copyright © 2016 Elsevier B.V. All rights reserved.)

Published

2017

18. Bilayer Membrane Modulation of Membrane Type 1 Matrix Metalloproteinase (MT1-MMP) Structure and Proteolytic Activity.

Author

Cerofolini L, Amar S, Lauer JL, Martelli T, Fragai M, Luchinat C, and Fields GB

Subjects

Cell Membrane metabolism, Collagen chemistry, Enzyme Activation, HEK293 Cells, Hemopexin chemistry, Humans, Hydrolysis, Magnetic Resonance Spectroscopy, Mutation, Myocardium metabolism, Protein Domains, Proteolysis, Lipid Bilayers chemistry, Matrix Metalloproteinase 14 chemistry, Matrix Metalloproteinase 14 metabolism

Abstract

Cell surface proteolysis is an integral yet poorly understood physiological process. The present study has examined how the pericellular collagenase membrane-type 1 matrix metalloproteinase (MT1-MMP) and membrane-mimicking environments interplay in substrate binding and processing. NMR derived structural models indicate that MT1-MMP transiently associates with bicelles and cells through distinct residues in blades III and IV of its hemopexin-like domain, while binding of collagen-like triple-helices occurs within blades I and II of this domain. Examination of simultaneous membrane interaction and triple-helix binding revealed a possible regulation of proteolysis due to steric effects of the membrane. At bicelle concentrations of 1%, enzymatic activity towards triple-helices was increased 1.5-fold. A single mutation in the putative membrane interaction region of MT1-MMP (Ser466Pro) resulted in lower enzyme activation by bicelles. An initial structural framework has thus been developed to define the role(s) of cell membranes in modulating proteolysis.

Published

2016

19. Signatures of positive selection at hemopexin (PEX) domain of matrix metalloproteinase-9 (MMP-9) gene.

Author

Liu Y, Zhao Y, Lu C, Fu M, Dou T, and Tan X

Subjects

Amino Acid Sequence, Animals, Exons, Hemopexin chemistry, Hemopexin metabolism, Humans, Matrix Metalloproteinase 9 chemistry, Matrix Metalloproteinase 9 genetics, Molecular Sequence Data, Protein Structure, Tertiary, Selection, Genetic, Vertebrates, Evolution, Molecular, Matrix Metalloproteinase 9 metabolism, Phylogeny

Abstract

Matrix metalloproteinases-9 (MMP-9) is an important cancer-associated, zinc-dependent endopeptidase. To investigate the natural selection hypothesis of MMP-9, the orthologous sequences from 12 vertebrates were compared and a molecular evolution analysis was performed. Results suggest that amino acid residues present in the middle region of the protein are more selectively constrained, whereas amino acid residues in the C-terminal region of the MMP-9 protein including exon 13 showed lowest conservation level in non-primate species, suggesting that it is an exon with fast evolving rate compared to the others analyzed. InterProScan analysis shows that exon 13 was located in hemopexin (PEX) domain of MMP-9. Positive selection was detected in PEX domain of MMP-9 protein between human and other species, which indicates that selective pressure may play a role in shaping the function of MMP-9 in the course of evolution.

Published

2015

20. Crystal Structure of Mg(2+) Containing Hemopexin-Fold Protein from Kabuli Chana (Chickpea-White, CW-25) at 2.45 Å Resolution Reveals Its Metal Ion Transport Property.

Author

Kumar S, Singh A, Yamini S, Dey S, and Singh TP

Subjects

Amino Acid Sequence, Crystallography, X-Ray, Magnesium chemistry, Models, Molecular, Molecular Sequence Data, Protein Conformation, Sequence Alignment, Cicer chemistry, Hemopexin chemistry, Hemopexin metabolism, Magnesium metabolism, Plant Proteins chemistry, Plant Proteins metabolism

Abstract

Plant seeds contain a number of proteins which play important roles in the protection and the process of germination of seeds. We have isolated and purified a 25 kDa protein from Kabuli Chana (Cicer arietinum L., Chickpea-white, CW-25). The CW-25 protein was crystallized using 0.5 M magnesium acetate, 0.1 M sodium cacodylate and 20 % (w/v) polyethylene glycol 8000, pH 6.5. The crystals of CW-25 belonged to space group P3 with unit cell dimensions, a = b = 80.5 Å, and c = 69.2 Å. The structure of CW-25 was determined using molecular replacement method and refined to an R factor of 0.152. The buried surface area between two molecules was found to be approximately 653 Å(2) indicating the formation of a weak homodimer. The polypeptide chain of CW-25 adopted a hemopexin-fold with four-bladed β-propellers. The structure formed a central tunnel-like architecture. A magnesium ion was observed in the centre of the tunnel. It was located at distances varying between 2.3 and 2.7 Å from five oxygen atoms of which four were backbone oxygen atoms belonging to residues, Asn7, Asp65, Asp121 and Asp174 while the fifth oxygen atom, O(δ1) was from the side chain of Asn7. The approximate length of the tunnel was 30 Å. Furthermore, a series of carbonyl oxygen atoms were present along the internal face of the tunnel. The diameter of the tunnel varied from 4.6 to 6.2 Å. The diameter and chemical environment of the tunnel clearly indicated that it might be used for the transport of various metal ions across the molecule.

Published

2015

21. Crystal structure of a plant albumin from Cicer arietinum (chickpea) possessing hemopexin fold and hemagglutination activity.

Author

Sharma U, Katre UV, and Suresh CG

Subjects

Amino Acid Sequence, Crystallography, X-Ray, Molecular Sequence Data, Protein Folding, Sequence Homology, Amino Acid, Albumins chemistry, Cicer chemistry, Hemagglutination, Hemopexin chemistry

Abstract

Main Conclusion: Crystal structure of a reported PA2 albumin from Cicer arietinum shows that it belongs to hemopexin fold family, has four beta-propeller motifs and possesses hemagglutination activity, making it different from known legume lectins. A plant albumin (PA2) from Cicer arietinum, presumably a lectin (CAL) owing to its hemagglutination activity which is inhibited by complex sugars as well as glycoproteins such as fetuin, desialylated fetuin and fibrinogen. The three-dimensional structure of this homodimeric protein has been determined using X-ray crystallography at 2.2 Å in two crystal forms: orthorhombic (P21212) and trigonal (P3). The structure determined using molecular replacement method and refined in orthorhombic crystal form reached R-factors R free 22.6 % and R work 18.2 % and in trigonal form had 22.3 and 17.9 % in the resolution range of 20.0-2.2 and 35.3-2.2 Å, respectively. Interestingly, unlike the known legume lectin fold, the structure of this homodimeric hemagglutinin belonged to hemopexin fold that consisted of four-bladed β-propeller architecture. Each subunit has a central cavity forming a channel, inside of which is lined with hydrophobic residues. The channel also bears binding sites for ligands such as calcium, sodium and chloride ions, iodine atom in the case of iodine derivative and water molecules. However, none of these ligands seem important for the sugar recognition. No monosaccharide sugar specificity could be detected using hemagglutination inhibition. Chemical modification studies identified a potential sugar-binding site per subunit molecule. Comparison of C-alpha atom positions in subunit structures showed that the deviations between the two crystal forms were more with respect to blades I and IV. Differences also existed between subunits in two forms in terms of type and site of ligand binding.

Published

2015

22. Quantification of fucosylated hemopexin and complement factor H in plasma of patients with liver disease.

Author

Benicky J, Sanda M, Pompach P, Wu J, and Goldman R

Subjects

Amino Acid Sequence, Complement Factor H chemistry, Female, Hemopexin chemistry, Humans, Male, Middle Aged, Complement Factor H metabolism, Fucose chemistry, Hemopexin metabolism, Liver Diseases blood

Abstract

Enhanced fucosylation has been suggested as a marker for serologic monitoring of liver disease and hepatocellular carcinoma (HCC). We present a workflow for quantitative site-specific analysis of fucosylation and apply it to a comparison of hemopexin (HPX) and complement factor H (CFH), two liver-secreted glycoproteins, in healthy individuals and patients with liver cirrhosis and HCC. Label-free LC-MS quantification of glycopeptides derived from these purified glycoproteins was performed on pooled samples (2 pools/group, 5 samples/pool) and complemented by glycosidase assisted analysis using sialidase and endoglycosidase F2/F3, respectively, to improve resolution of glycoforms. Our analysis, presented as relative abundance of individual fucosylated glycoforms normalized to the level of their nonfucosylated counterparts, revealed a consistent increase in fucosylation in liver disease with significant site- and protein-specific differences. We have observed the highest microheterogeneity of glycoforms at the N187 site of HPX, absence of core fucosylation at N882 and N911 sites of CFH, or a higher degree of core fucosylation in CFH compared to HPX, but we did not identify changes differentiating HCC from matched cirrhosis samples. Glycosidase assisted LC-MS-MRM analysis of individual patient samples prepared by a simplified protocol confirmed the quantitative differences. Transitions specific to outer arm fucose document a disease-associated increase in outer arm fucose on both bi- and triantennary glycans at the N187 site of HPX. Further verification is needed to confirm that enhanced fucosylation of HPX and CFH may serve as an indicator of premalignant liver disease. The analytical strategy can be readily adapted to analysis of other proteins in the appropriate disease context.

Published

2014

23. A novel CD44-binding peptide from the pro-matrix metalloproteinase-9 hemopexin domain impairs adhesion and migration of chronic lymphocytic leukemia (CLL) cells.

Author

Ugarte-Berzal E, Bailón E, Amigo-Jiménez I, Albar JP, García-Marco JA, and García-Pardo A

Subjects

Aged, Amino Acid Sequence, Disease Progression, Drug Design, Enzyme Precursors chemistry, Enzyme Precursors metabolism, Female, Hemopexin chemistry, Hemopexin metabolism, Humans, Leukemia, Lymphocytic, Chronic, B-Cell drug therapy, Leukemia, Lymphocytic, Chronic, B-Cell pathology, Male, Matrix Metalloproteinase 9 chemistry, Middle Aged, Molecular Sequence Data, Peptides chemical synthesis, Peptides metabolism, Protein Binding physiology, Protein Structure, Tertiary, Cell Adhesion physiology, Cell Movement physiology, Hyaluronan Receptors metabolism, Leukemia, Lymphocytic, Chronic, B-Cell metabolism, Matrix Metalloproteinase 9 metabolism

Abstract

(pro)MMP-9 binds to CLL cells through the PEX9 domain and contributes to CLL progression. To biochemically characterize this interaction and identify potential therapeutic targets, we prepared GST-PEX9 forms containing structural blades B1B2 or B3B4. We recently described a sequence in blade B4 (P3 sequence) that bound α4β1 integrin and partially impaired cell adhesion and migration. We have now studied the possible contribution of the B1B2 region to cell interaction with PEX9. CLL cells bound to GST-B1B2 and CD44 was the primary receptor. GST-B1B2 inhibited CLL cell migration as effectively as GST-B3B4. Overlapping synthetic peptides spanning the B1B2 region identified the sequence FDAIAEIGNQLYLFKDGKYW, present in B1 and contained in peptide P6, as the most effective site. P6 inhibited cell adhesion to PEX9 in a dose-dependent manner and with an IC50 value of 90 μM. P6 also inhibited cell adhesion to hyaluronan but had no effect on adhesion to VCAM-1 (α4β1 integrin ligand), confirming its specific interaction with CD44. Spatial localization analyses mapped P6 to the central cavity of PEX9, in close proximity to the previously identified P3 sequence. Both P6 and P3 equally impaired cell adhesion to (pro)MMP-9. Moreover, P6 synergistically cooperated with P3, resulting in complete inhibition of CLL cell binding to PEX9, chemotaxis, and transendothelial migration. Thus, P6 is a novel sequence in PEX9 involved in cell-PEX9/(pro)MMP-9 binding by interacting with CD44. Targeting both sites, P6 and P3, should efficiently prevent (pro)MMP-9 binding to CLL cells and its pathological consequences., (© 2014 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2014

24. Adaptive functional divergence of the warm temperature acclimation-related protein (WAP65) in fishes and the ortholog hemopexin (HPX) in mammals.

Author

Machado JP, Vasconcelos V, and Antunes A

Subjects

Animals, Evolution, Molecular, Fish Proteins genetics, Gene Duplication, Phylogeny, Protein Conformation, Selection, Genetic, Acclimatization genetics, Fishes genetics, Hemopexin chemistry, Hemopexin genetics, Mammals genetics, Temperature

Abstract

Gene duplication is an important mechanism that leads to genetic novelty. Different, nonexclusive processes are likely involved, and many adaptive and nonadaptive events may contribute to the maintenance of duplicated genes. In some teleosts, a duplicate copy of the mammalian ortholog Hemopexin (HPX) is present, known as the warm temperature acclimation-related protein (WAP65). Both WAP65 and HPX have been associated with iron homeostasis due to the affinity to bind the toxic-free heme circulating in the blood stream. We have assessed the evolutionary dynamics of WAP65 and HPX genes to understand the adaptive role of positive selection at both nucleotide and amino acid level. Our results showed an asymmetrical evolution between the paralogs WAP65-1 and WAP65-2 after duplication with a slight acceleration of the evolutionary rate in WAP65-1, but not in WAP65-2, and few sites contributing to the functional distinction between the paralogs, whereas the majority of the protein remained under negative selection or relaxed negative selection. WAP65-1 is functionally more distinct from the ancestral protein function than WAP65-2. HPX is phylogenetically closer to WAP65-2 but even so functional divergence was detected between both proteins. In addition, HPX showed a fast rate of evolution when compared with both WAP65-1 and WAP65-2 genes. The assessed 3-dimensional (3-D) structure of WAP65-1 and WAP65-2 suggests that the functional differences detected are not causing noticeable structural changes in these proteins. However, such subtle changes between WAP65 paralogs may be important to understand the differential gene retention of both copies in 20 out of 30 teleosts species studied.

Published

2014

25. Structure of the secretion domain of HxuA from Haemophilus influenzae.

Author

Baelen S, Dewitte F, Clantin B, and Villeret V

Subjects

Amino Acid Sequence, Bacterial Outer Membrane Proteins genetics, Bacterial Outer Membrane Proteins metabolism, Bacterial Secretion Systems genetics, Carrier Proteins genetics, Carrier Proteins metabolism, Crystallography, X-Ray, Escherichia coli genetics, Escherichia coli metabolism, Gene Expression, Haemophilus influenzae metabolism, Heme metabolism, Hemopexin metabolism, Molecular Sequence Data, Protein Binding, Protein Interaction Domains and Motifs, Protein Structure, Secondary, Recombinant Proteins chemistry, Recombinant Proteins genetics, Recombinant Proteins metabolism, Sequence Alignment, Structural Homology, Protein, Bacterial Outer Membrane Proteins chemistry, Carrier Proteins chemistry, Haemophilus influenzae chemistry, Heme chemistry, Hemopexin chemistry, Models, Molecular

Abstract

Haemophilus influenzae HxuA is a cell-surface protein with haem-haemopexin binding activity which is key to haem acquisition from haemopexin and thus is one of the potential sources of haem for this microorganism. HxuA is secreted by its specific transporter HxuB. HxuA/HxuB belongs to the so-called two-partner secretion systems (TPSs) that are characterized by a conserved N-terminal domain in the secreted protein which is essential for secretion. Here, the 1.5 Å resolution structure of the secretion domain of HxuA, HxuA301, is reported. The structure reveals that HxuA301 folds into a β-helix domain with two extra-helical motifs, a four-stranded β-sheet and an N-terminal cap. Comparisons with other structures of TpsA secretion domains are reported. They reveal that despite limited sequence identity, strong structural similarities are found between the β-helix motifs, consistent with the idea that the TPS domain plays a role not only in the interaction with the specific TpsB partners but also as the scaffold initiating progressive folding of the TpsA proteins at the bacterial surface.

Published

2013

26. Glycosylation of closely spaced acceptor sites in human glycoproteins.

Author

Shrimal S and Gilmore R

Subjects

Amino Acid Motifs, Animals, Endoplasmic Reticulum metabolism, Gene Expression, Glycoproteins chemistry, Glycoproteins genetics, Glycosylation, Haptoglobins chemistry, Haptoglobins genetics, HeLa Cells, Hemopexin chemistry, Hemopexin genetics, Hexosyltransferases genetics, Humans, Membrane Proteins genetics, Mice, Molecular Sequence Data, Glycoproteins metabolism, Haptoglobins metabolism, Hemopexin metabolism, Hexosyltransferases metabolism, Membrane Proteins metabolism, Protein Processing, Post-Translational

Abstract

Asparagine-linked glycosylation of proteins by the oligosaccharyltransferase (OST) occurs when acceptor sites or sequons (N-x≠P-T/S) on nascent polypeptides enter the lumen of the rough endoplasmic reticulum. Metazoan organisms assemble two isoforms of the OST that have different catalytic subunits (STT3A or STT3B) and partially non-overlapping cellular roles. Potential glycosylation sites move past the STT3A complex, which is associated with the translocation channel, at the protein synthesis elongation rate. Here, we investigated whether close spacing between acceptor sites in a nascent protein promotes site skipping by the STT3A complex. Biosynthetic analysis of four human glycoproteins revealed that closely spaced sites are efficiently glycosylated by an STT3B-independent process unless the sequons contain non-optimal sequence features, including extreme close spacing between sequons (e.g. NxTNxT) or the presence of paired NxS sequons (e.g. NxSANxS). Many, but not all, glycosylation sites that are skipped by the STT3A complex can be glycosylated by the STT3B complex. Analysis of a murine glycoprotein database revealed that closely spaced sequons are surprisingly common, and are enriched for paired NxT sites when the gap between sequons is less than three residues.

Published

2013

27. Ostreopexin: a hemopexin fold protein from the oyster mushroom, Pleurotus ostreatus.

Author

Ota K, Mikelj M, Papler T, Leonardi A, Križaj I, and Maček P

Subjects

Albumins metabolism, Chromatography, Liquid, Fabaceae metabolism, Fungal Proteins chemistry, Hemopexin metabolism, Nitrilotriacetic Acid metabolism, Oryza metabolism, Plant Proteins metabolism, Pleurotus growth & development, Protein Conformation, Seeds metabolism, Spectrometry, Mass, Electrospray Ionization, Tandem Mass Spectrometry, Fungal Proteins metabolism, Hemin metabolism, Hemopexin chemistry, Nitrilotriacetic Acid analogs & derivatives, Organometallic Compounds metabolism, Pleurotus metabolism, Polyamines metabolism, Recombinant Proteins metabolism

Abstract

Proteins with hemopexin repeats are widespread in viruses, prokaryotes and eukaryotes. We report here for the first time the existence of a protein in fungi with the four-bladed β-propeller fold that is typical for hemopexin-like proteins. This protein was isolated from the edible basidiomycetous fungus Pleurotus ostreatus and is named ostreopexin. It binds to Ni(2+)-NTA-agarose, and is structurally and functionally very similar to PA2 albumins isolated from legume seeds and the hemopexin fold protein from rice. Like these plant proteins, ostreopexin shows reversible binding to hemin with moderate affinity, but does not bind to polyamines. We suggest that ostreopexin participates in intracellular management of metal (II or III)-chelates., (Copyright © 2013 Elsevier B.V. All rights reserved.)

Published

2013

28. LC-MS3 quantification of O-glycopeptides in human serum.

Author

Sanda M, Pompach P, Benicky J, and Goldman R

Subjects

Amino Acid Sequence, Carbohydrate Sequence, Hemopexin chemistry, Hemopexin isolation & purification, Humans, Limit of Detection, Linear Models, Models, Chemical, Molecular Sequence Data, Reproducibility of Results, Sensitivity and Specificity, Sex Hormone-Binding Globulin, Chromatography, Liquid methods, Glycopeptides blood, Glycopeptides chemistry, Tandem Mass Spectrometry methods

Abstract

Quantitative analysis of site-specific glycosylation of proteins is a challenging part of glycoproteomic research. Multiple enrichment steps are typically required in the analytical workflows to achieve adequate characterization of the site-specific glycoforms. In spite of recent advances, quantitative workflows need further development. Here, we report a selective and sensitive MS2 followed by further fragmentation in the linear IT-MS analyzer (MS3) multiple reaction monitoring workflow mass spectrometric method for direct analysis of O-glycopeptides in difficult matrix such as serum. Method optimization was performed using two serum glycoproteins, hemopexin (HPX) and sex hormone binding globulin. With the optimized MS3 workflow, we were able to analyze major glycoforms of HPX directly in human serum. Quantification of the minor glycoforms of HPX and glycoforms of sex hormone binding globulin required enrichment of the protein because these analytes were below the sensitivity of the 4000 quadrupole ion trap hybrid mass spectrometer in the complex serum background. In conclusion, we present a quantitative method for site-specific analysis of O-glycosylation with general applicability to mucin-type glycoproteins. Our results document reliable application of the optimized MS3 multiple reaction monitoring workflow to the relative quantification of O-glycosylation microheterogeneity of HPX in human serum. Introduction of isotopically labeled standards would be desirable to achieve absolute quantification of the analytes. The possibility to analyze serum samples directly represents a significant improvement of the quantitative glycopeptide workflows with the potential for use in clinical applications., (© 2013 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2013

29. [Progress in biochemical characteristics of hemopexin and its clinical application].

Author

Dong BB, Zhu FY, Wei HD, Dong HL, and Xiong LZ

Subjects

Humans, Heme, Heme Oxygenase (Decyclizing), Hemopexin chemistry, Hemopexin metabolism

Abstract

Hemopexin (HPX) is a plasma protein with the strongest binding capacity to heme and widely involved in modulation of a variety of physiological and pathological processes. The main physiological function of HPX is to bind and transport free toxic heme. Recent studies indicate that HPX also plays roles of anti-oxidant, anti-apoptosis, immune regulation and organic protection. In addition, HPX participates in regulation of cell differentiation and extracellular matrix reconstruction. In recent years, a great deal of progress has been made in studies of the mechanisms of HPX protective effects and on possible clinical application. In the past few years, especially, a number of proteomic studies have demonstrated that HPX could be served as positive molecular biomarkers for cancers of lung, liver, kidney, colon, and uterine myoma as well as osteoarthritis. In this review, recent progress in the biochemical characteristics and function of HPX and its possible clinical applications are summarized.

Published

2013

30. LC-MS/MS characterization of O-glycosylation sites and glycan structures of human cerebrospinal fluid glycoproteins.

Author

Halim A, Rüetschi U, Larson G, and Nilsson J

Subjects

Amino Acid Sequence, Apolipoproteins E chemistry, Chromatography, Liquid, Glycomics, Glycosylation, Hemopexin chemistry, Humans, Membrane Proteins chemistry, Molecular Conformation, Molecular Sequence Data, Peptide-N4-(N-acetyl-beta-glucosaminyl) Asparagine Amidase chemistry, Receptor Protein-Tyrosine Kinases chemistry, Receptors, G-Protein-Coupled, Spectrometry, Mass, Electrospray Ionization, Trypsin chemistry, Cerebrospinal Fluid chemistry, Glycoproteins chemistry, Polysaccharides chemistry, Serine chemistry, Threonine chemistry

Abstract

The GalNAc O-glycosylation on Ser/Thr residues of extracellular proteins has not been well characterized from a proteomics perspective. We previously reported a sialic acid capture-and-release protocol to enrich tryptic N- and O-glycopeptides from human cerebrospinal fluid glycoproteins using nano-LC-ESI-MS/MS with collision-induced dissociation (CID) for glycopeptide characterization. Here, we have introduced peptide N-glycosidase F (PNGase F) pretreatment of CSF samples to remove the N-glycans facilitating the selective characterization of O-glycopeptides and enabling the use of an automated CID-MS(2)/MS(3) search protocol for glycopeptide identification. We used electron-capture and -transfer dissociation (ECD/ETD) to pinpoint the glycosylation site(s) of the glycopeptides, identified as predominantly core-1-like HexHexNAc-O- structure attached to one to four Ser/Thr residues. We characterized 106 O-glycosylations and found Pro residues preferentially in the n - 1, n + 1, and/or n + 3 positions in relation to the Ser/Thr attachment site (n). The characterization of glycans and glycosylation sites in glycoproteins from human clinical samples provides a basis for future studies addressing the biological and diagnostic importance of specific protein glycosylations in relation to human disease.

Published

2013

31. Cyanide binding to human plasma heme-hemopexin: a comparative study.

Author

Ascenzi P, Leboffe L, and Polticelli F

Subjects

Humans, Thermodynamics, Cyanides chemistry, Heme chemistry, Hemopexin chemistry

Abstract

Hemopexin (HPX) displays a pivotal role in heme scavenging and delivery to the liver. In turn, heme-Fe-hemopexin (HPX-heme-Fe) displays heme-based spectroscopic and reactivity properties. Here, kinetics and thermodynamics of cyanide binding to ferric and ferrous hexa-coordinate human plasma HPX-heme-Fe (HHPX-heme-Fe(III) and HHPX-heme-Fe(II), respectively), and for the dithionite-mediated reduction of the HHPX-heme-Fe(III)-cyanide complex, at pH 7.4 and 20.0°C, are reported. Values of thermodynamic and kinetic parameters for cyanide binding to HHPX-heme-Fe(III) and HHPX-heme-Fe(II) are K = (4.1 ± 0.4) × 10(-6) M, k(on) = (6.9 ± 0.5) × 10(1) M(-1) s(-1), and k(off) = 2.8 × 10(-4) s(-1); and H = (6 ± 1) × 10(-1) M, h(on) = 1.2 × 10(-1) M(-1) s(-1), and h(off) = (7.1 ± 0.8) × 10(-2) s(-1), respectively. The value of the rate constant for the dithionite-mediated reduction of the HHPX-heme-Fe(III)-cyanide complex is l = 8.9 ± 0.8 M(-1/2) s(-1). HHPX-heme-Fe reactivity is modulated by proton acceptor/donor amino acid residue(s) (e.g., His236) assisting the deprotonation and protonation of the incoming and outgoing ligand, respectively., (Copyright © 2012 Elsevier Inc. All rights reserved.)

Published

2012

32. [Cloning, physical and chemical property analysis of the Japanese sea bass Wap65-2 gene and its expression following Vibrio harveyi infection].

Author

Shi YH, Chen J, Gao SS, Shen GQ, Lu XJ, and Li MY

Subjects

Animals, Bass classification, Bass metabolism, Bass microbiology, Cloning, Molecular, Fish Diseases genetics, Fish Diseases metabolism, Fish Proteins chemistry, Fish Proteins metabolism, Hemopexin chemistry, Hemopexin metabolism, Molecular Sequence Data, Phylogeny, Vibrio Infections genetics, Vibrio Infections metabolism, Vibrio Infections microbiology, Bass genetics, Fish Diseases microbiology, Fish Proteins genetics, Hemopexin genetics, Vibrio physiology, Vibrio Infections veterinary

Abstract

The warm temperature acclimation related 65 kDa protein-2 (Wap65-2), a teleost plasma glycoprotein, plays an important role in immune regulation against bacterial infection. Here, for the first time we determined the full length cDNA sequence of the Japanese sea bass Wap65-2 gene (1 601 bp in length excluding the 3'-polyA tail). The sequence contains an open reading frame that encodes a protein of 436 amino acids with a molecular weight of 4.87×10(4). The predicted protein had a signal peptide in the N-terminal domain containing 19 residues. Sequence comparison and phylogenetic tree analysis showed that the Japanese sea bass Wap65-2 has a relatively high similarity to the Dicentrarchus labrax Wap65-2. In the healthy Japanese sea bass, Wap65-2 mRNA was expressed mainly in the liver and weakly in the heart and muscle. qRT-PCR results revealed that liver Wap65-2 transcripts were significantly increased after a Vibrio harveyi infection, and peaked 24 hour post injection (6.89 fold increase). The Japanese sea bass Wap65-2 protein was expressed in Escherichia coli and subsequently used for antiserum preparation. Western blot analysis showed that Wap65-2 was significantly increased in V. harveyi infected Japanese sea bass and reached a maximum of 5.33-fold increase at 36 h. In conclusion, the alteration of Japanese sea bass Wap65-2 expression was tightly associated with the progression of the V. harveyi bacterial infection.

Published

2012

33. Alendronate promotes plasmin-mediated MMP-9 inactivation by exposing cryptic plasmin degradation sites within the MMP-9 catalytic domain.

Author

Farina AR, Cappabianca L, Di Ianni N, Ruggeri P, Ragone M, Merolle S, Gulino A, and Mackay AR

Subjects

Catalysis, Catalytic Domain, Cations, Cell Line, Tumor, Chelating Agents pharmacology, Dose-Response Relationship, Drug, Edetic Acid chemistry, Hemopexin chemistry, Humans, Plasminogen chemistry, Protein Structure, Tertiary, Recombinant Proteins chemistry, Alendronate pharmacology, Fibrinolysin metabolism, Matrix Metalloproteinase 9 metabolism

Abstract

Irreversible MMP-9 inhibition is considered a significant therapeutic goal in inflammatory, vascular and tumour pathology. We report that divalent cation chelators Alendronate and EDTA not only directly inhibited MMP-9 but also promoted irreversible plasmin-mediated MMP-9 inactivation by exposing cryptic plasmin-degradation sites within the MMP-9 catalytic-domain and producing an inhibitory hemopexin-domain fragment. This effect was also observed using MDA-MB-231 breast cancer cells, which activated exogenous plasminogen to degrade endogenous proMMP-9 in the presence of Alendronate or EDTA. Degradation-mediated inactivation of proMMP-9 occurred in the absence of transient activation, attesting to the incapacity of plasmin to directly activate proMMP-9 and direct MMP-9 inhibition by Alendronate and EDTA. Our study provides a novel rational for therapeutic Alendronate use in MMP-9-dependent pathology characterised by plasminogen activation., (Copyright © 2012 Federation of European Biochemical Societies. Published by Elsevier B.V. All rights reserved.)

Published

2012

34. Modulation of warm-temperature-acclimation-associated 65-kDa protein genes (Wap65-1 and Wap65-2) in mud loach (Misgurnus mizolepis, Cypriniformes) liver in response to different stimulatory treatments.

Author

Cho YS, Kim BS, Kim DS, and Nam YK

Subjects

Acclimatization, Amino Acid Sequence, Animals, Cypriniformes metabolism, DNA, Complementary chemistry, DNA, Complementary genetics, DNA, Complementary metabolism, Fish Proteins chemistry, Fish Proteins genetics, Hemopexin chemistry, Hemopexin genetics, Hot Temperature, Molecular Sequence Data, Protein Isoforms chemistry, Protein Isoforms genetics, Protein Isoforms metabolism, Real-Time Polymerase Chain Reaction veterinary, Cypriniformes genetics, Fish Proteins metabolism, Hemopexin analogs & derivatives, Hemopexin metabolism, Liver metabolism

Abstract

Two paralogous isoform cDNAs of warm-temperature-acclimation-associated 65-kDa protein (Wap65-1 and Wap65-2) were isolated from the cypriniform species, mud loach (Misgurnus mizolepis), and characterized. The deduced amino acid sequences of the two mud loach Wap65 isoforms (mlWap65-1 and mlWap65-2) share moderate levels of sequence homology with their corresponding orthologues from teleosts and with human hemopexin, a possible mammalian homologue. Both isoforms display conserved features, including essential motifs and/or residues that are important for the protein structure of hemopexin. In overall, mlWap65-2 is more homologous to human hemopexin than is mlWap65-1. Both mud loach Wap65 transcripts are predominantly expressed in liver, although the transcripts are ubiquitously detectable in most tissues with variable basal expression. Both mlWap65 isoforms are differentially regulated during embryonic development, and the changes in transcript levels during embryogenesis are greater for mlWap65-2 than for mlWap65-1. The transcription of the mlWap65 genes is differentially modulated by various stimuli, including thermal changes, immune challenge (lipopolysaccharide injection or bacterial infection), and heavy metal exposure (cadmium, copper, or nickel). The isoform mlWap65-1 is more responsive to warm temperature treatments than mlWap65-2, whereas mlWap65-2 is much more strongly stimulated by immune and heavy metal challenges than is mlWap65-1. Taken together, the results of this study suggest that mud loach Wap65 isoforms are potentially involved in multiple cellular pathways and that the two mud loach Wap65 isoforms undergo functional partitioning or subfunctionalization., (Copyright © 2012 Elsevier Ltd. All rights reserved.)

Published

2012

35. Novel MT1-MMP small-molecule inhibitors based on insights into hemopexin domain function in tumor growth.

Author

Remacle AG, Golubkov VS, Shiryaev SA, Dahl R, Stebbins JL, Chernov AV, Cheltsov AV, Pellecchia M, and Strongin AY

Subjects

Animals, Breast Neoplasms drug therapy, Breast Neoplasms enzymology, Breast Neoplasms pathology, Cell Growth Processes drug effects, Cell Growth Processes physiology, Female, Humans, Matrix Metalloproteinase 14 biosynthesis, Matrix Metalloproteinase 14 chemistry, Matrix Metalloproteinase 14 genetics, Mice, Mice, Inbred BALB C, Mice, Nude, Models, Molecular, Protein Structure, Tertiary, Xenograft Model Antitumor Assays, Hemopexin chemistry, Matrix Metalloproteinase Inhibitors, Protease Inhibitors pharmacology

Abstract

Membrane type-1 matrix metalloproteinase (MT1-MMP) is a promising drug target in malignancy. The structure of MT1-MMP includes the hemopexin domain (PEX) that is distinct from and additional to the catalytic domain. Current MMP inhibitors target the conserved active site in the catalytic domain and, as a result, repress the proteolytic activity of multiple MMPs instead of MT1-MMP alone. In our search for noncatalytic inhibitors of MT1-MMP, we compared the protumorigenic activity of wild-type MT1-MMP with an MT1-MMP mutant lacking PEX (ΔPEX). In contrast to MT1-MMP, ΔPEX did not support tumor growth in vivo, and its expression resulted in small fibrotic tumors that contained increased levels of collagen. Because these findings suggested an important role for PEX in tumor growth, we carried out an inhibitor screen to identify small molecules targeting the PEX domain of MT1-MMP. Using the Developmental Therapeutics Program (National Cancer Institute/NIH), virtual ligand screening compound library as a source and the X-ray crystal structure of PEX as a target, we identified and validated a novel PEX inhibitor. Low dosage, intratumoral injections of PEX inhibitor repressed tumor growth and caused a fibrotic, ΔPEX-like tumor phenotype in vivo. Together, our findings provide a preclinical proof of principle rationale for the development of novel and selective MT1-MMP inhibitors that specifically target the PEX domain., (©2012 AACR)

Published

2012

36. A structurally novel hemopexin fold protein of rice plays role in chlorophyll degradation.

Author

Chattopadhyay T, Bhattacharyya S, Das AK, and Maiti MK

Subjects

Models, Chemical, Protein Conformation, Protein Folding, Chlorophyll metabolism, Hemopexin chemistry, Hemopexin physiology, Oryza metabolism, Plant Proteins chemistry, Plant Proteins physiology

Abstract

Proteins containing hemopexin fold domain are suggested to have diverse functions in various living organisms. In order to investigate the structure and function of this type of protein in rice plant (Oryza sativa), the gene encoding a hemopexin fold protein (OsHFP) was cloned, analyzed in silico and characterized. Molecular modeling revealed that the OsHFP is closely related to other hemopexin fold proteins, but is unique with a cylindrical central tunnel as well as extended N- and C-terminal domains. The recombinant OsHFP was found to bind hemin, the oxidized form of heme in vitro. The expression of the single copy OsHFP gene was detected in rice flower buds. Heterologous expression of OsHFP in green leaf tissues resulted in chlorophyll degradation; however, stable expression of OsHFP was observed in transgenic hairy roots, a non-green tissue. The possible role of OsHFP in regulating programmed cell death in anther green tissues of rice is proposed., (Copyright © 2012 Elsevier Inc. All rights reserved.)

Published

2012

37. Semi-automated identification of N-Glycopeptides by hydrophilic interaction chromatography, nano-reverse-phase LC-MS/MS, and glycan database search.

Author

Pompach P, Chandler KB, Lan R, Edwards N, and Goldman R

Subjects

Amino Acid Sequence, Carbohydrate Sequence, Databases, Protein, Glycoproteins chemistry, Haptoglobins chemistry, Haptoglobins isolation & purification, Hemopexin chemistry, Hemopexin isolation & purification, Humans, Hydrophobic and Hydrophilic Interactions, Molecular Sequence Data, Peptide Fragments chemistry, Peptide Fragments isolation & purification, Peptide Mapping methods, Polysaccharides chemistry, Protein Isoforms chemistry, Protein Isoforms isolation & purification, Proteolysis, Tandem Mass Spectrometry, Chromatography, Reverse-Phase methods, Glycoproteins isolation & purification, Polysaccharides isolation & purification, Software

Abstract

Glycoproteins fulfill many indispensable biological functions, and changes in protein glycosylation have been observed in various diseases. Improved analytical methods are needed to allow a complete characterization of this complex and common post-translational modification. In this study, we present a workflow for the analysis of the microheterogeneity of N-glycoproteins that couples hydrophilic interaction and nanoreverse-phase C18 chromatography to tandem QTOF mass spectrometric analysis. A glycan database search program, GlycoPeptideSearch, was developed to match N-glycopeptide MS/MS spectra with the glycopeptides comprised of a glycan drawn from the GlycomeDB glycan structure database and a peptide from a user-specified set of potentially glycosylated peptides. Application of the workflow to human haptoglobin and hemopexin, two microheterogeneous N-glycoproteins, identified a total of 57 distinct site-specific glycoforms in the case of haptoglobin and 14 site-specific glycoforms of hemopexin. Using glycan oxonium ions and peptide-characteristic glycopeptide fragment ions and by collapsing topologically redundant glycans, the search software was able to make unique N-glycopeptide assignments for 51% of assigned spectra, with the remaining assignments primarily representing isobaric topological rearrangements. The optimized workflow, coupled with GlycoPeptideSearch, is expected to make high-throughput semiautomated glycopeptide identification feasible for a wide range of users.

Published

2012

38. Inhibition of MT1-MMP activity using functional antibody fragments selected against its hemopexin domain.

Author

Basu B, Correa de Sampaio P, Mohammed H, Fogarasi M, Corrie P, Watkins NA, Smethurst PA, English WR, Ouwehand WH, and Murphy G

Subjects

Cell Line, Tumor, Collagen chemistry, Collagen metabolism, Hemopexin chemistry, Humans, Matrix Metalloproteinase 14 chemistry, Protein Structure, Tertiary, Single-Chain Antibodies chemistry, Single-Chain Antibodies isolation & purification, Hemopexin immunology, Matrix Metalloproteinase 14 immunology, Matrix Metalloproteinase Inhibitors, Single-Chain Antibodies pharmacology

Abstract

The membrane associated MMP, MT1-MMP, is a critical pericellular protease involved in tumour cell invasion and angiogenesis and is highly up-regulated in numerous human cancers. It therefore represents an exciting new therapeutic cancer-specific target. We have generated recombinant human scFv antibodies against the non-catalytic, hemopexin domain of MT1-MMP that modulate its interactions with collagen. One of these is an effective inhibitor of the invasive capacity of cancer cells and of angiogenesis in model systems. This demonstrates that targeting sites outside the catalytic domain presents a potential novel approach to proteinase inhibition that could have applications in cancer therapeutics., (Copyright © 2011 Elsevier Ltd. All rights reserved.)

Published

2012

39. Molecular evolution of matrix metalloproteinase 20.

Author

Kawasaki K and Suzuki T

Subjects

Ameloblasts enzymology, Amelogenesis, Animals, Chromosomes, Human, Pair 11 genetics, Dental Enamel Proteins genetics, Hemopexin chemistry, Humans, Multigene Family genetics, Phylogeny, Vertebrates genetics, Dental Enamel enzymology, Evolution, Molecular, Matrix Metalloproteinase 20 chemistry, Matrix Metalloproteinase 20 genetics, Takifugu genetics

Abstract

Dental enamel is a hypermineralized tissue, containing only trace amounts of organic components. During enamel formation, matrix metalloproteinase 20 (MMP20) processes proteins comprising enamel matrix and facilitates hypermineralization. In the human genome, 24 distinct MMP genes have been identified. Among these genes, MMP20 is clustered with eight other genes, including MMP13, and all these clustered genes show phylogenetically close relationships. In this study, we investigated MMP20 and closely related MMP genes in various tetrapods and in a teleost fish, fugu. In the genome of the chicken, a toothless tetrapod, we identified degraded exons of MMP20, which supports the previous proposition that MMP20 is important specifically for enamel formation. Nevertheless, for unknown reasons, we failed to identify MMP20 in the platypus genome. In the opossum, lizard, and frog genomes, MMP20 was found clustered with MMP13. Furthermore, in the fugu genome, we identified an MMP20-like gene located adjacent to MMP13, suggesting that MMP20 arose before the divergence of ray-finned fish and lobe-finned fish. The teleost tooth surface is covered with enameloid, a hypermineralized tissue different from enamel. Thus, we hypothesize that MMP20 could have been used in an ancient hypermineralized tissue, which evolved into enameloid in teleosts and into enamel in tetrapods., (© 2011 Eur J Oral Sci.)

Published

2011

40. Biochemical and functional characterization of an albumin protein belonging to the hemopexin superfamily from Lens culinaris seeds.

Author

Scarafoni A, Gualtieri E, Barbiroli A, Carpen A, Negri A, and Duranti M

Subjects

Albumins immunology, Albumins metabolism, Allergens, Amino Acid Sequence, Drug Stability, Hot Temperature, Molecular Sequence Data, Plant Proteins metabolism, Protein Conformation, Thiamine metabolism, Albumins chemistry, Hemopexin chemistry, Lens Plant chemistry, Plant Proteins chemistry, Seeds chemistry

Abstract

The present paper reports the purification and biochemical characterization of an albumin identified in mature lentil seeds with high sequence similarity to pea PA2. These proteins are found in many edible seeds and are considered potentially detrimental for human health due to the potential allergenicity and lectin-like activity. Thus, the description of their possible presence in food and the assessment of the molecular properties are relevant. The M(r), pI, and N-terminal sequence of this protein have been determined. The work included the study of (i) the binding properties to hemine to assess the presence of hemopexin structural domains and (ii) the binding properties of the protein to thiamin. In addition, the structural changes induced by heating have been evaluated by means of spectroscopic techniques. Denaturation temperature has also been determined. The present work provides new insights about the structural molecular features and the ligand-binding properties and dynamics of this kind of seed albumin.

Published

2011

41. Proteolytic action of kallikrein-related peptidase 7 produces unique active matrix metalloproteinase-9 lacking the C-terminal hemopexin domains.

Author

Ramani VC, Kaushal GP, and Haun RS

Subjects

Breast Neoplasms metabolism, Cell Line, Tumor, Enzyme Activation, Enzyme Precursors chemistry, Enzyme Precursors metabolism, Female, Gelatinases chemistry, Gelatinases metabolism, Hemopexin chemistry, Hemopexin metabolism, Humans, Matrix Metalloproteinase 2 chemistry, Matrix Metalloproteinase 2 metabolism, Matrix Metalloproteinase 9 chemistry, Peptide Fragments chemistry, Peptide Fragments metabolism, Protein Structure, Tertiary, Substrate Specificity, Kallikreins metabolism, Matrix Metalloproteinase 9 metabolism

Abstract

The gelatinases, matrix metalloproteinase (MMP)-9 and -2, are produced as latent, inactive enzymes that can be proteolytically activated by a number of proteases. In many normal and pathological conditions, where the expression of MMPs is deregulated, changes in the expression of other proteases have also been reported. Human kallikrein-related peptidase 7 (KLK7), a chymotryptic-like serine protease, is overexpressed in many different types of neoplastic conditions, which have also been shown to express high levels of both MMP-9 and -2. Since the activation of MMPs by KLK7 has never been examined, we sought to determine whether KLK7 can activate these MMPs. To test this hypothesis KLK7 was incubated with the recombinant MMPs and the products of the reaction were analyzed for their activity. Incubation of proMMP-9 with KLK7 resulted in the production of a novel truncated, active MMP-9 lacking the C-terminal hemopexin domains. In contrast, KLK7 degraded, but did not activate, proMMP-2. The novel activation of proMMP-9 by KLK7 was further confirmed using conditioned medium prepared from an MMP-9-expressing cell line, MDA-MMP-9. Our results clearly establish that KLK7 activates proMMP-9 to produce a novel truncated, active MMP-9 product not generated by other proteases. These findings suggest that KLK7 may play an important role in the activation of MMP-9 in tumors that express high levels of both these proteases and the resulting truncated MMP may possess altered substrate specificities compared with full-length MMP-9 activated by other proteases., (2011 Elsevier B.V. All rights reserved.)

Published

2011

42. Small-molecule anticancer compounds selectively target the hemopexin domain of matrix metalloproteinase-9.

Author

Dufour A, Sampson NS, Li J, Kuscu C, Rizzo RC, Deleon JL, Zhi J, Jaber N, Liu E, Zucker S, and Cao J

Subjects

Animals, Antineoplastic Agents chemistry, Binding Sites, Breast Neoplasms drug therapy, Breast Neoplasms enzymology, Breast Neoplasms pathology, COS Cells, Cell Growth Processes drug effects, Cell Line, Tumor, Cell Movement drug effects, Chlorocebus aethiops, Hemopexin chemistry, Hemopexin metabolism, Humans, Lung Neoplasms prevention & control, Lung Neoplasms secondary, Matrix Metalloproteinase 9 biosynthesis, Matrix Metalloproteinase 9 chemistry, Matrix Metalloproteinase 9 metabolism, Mice, Mice, Nude, Models, Molecular, Protease Inhibitors chemistry, Protein Structure, Tertiary, Substrate Specificity, Transfection, Xenograft Model Antitumor Assays, Antineoplastic Agents pharmacology, Hemopexin antagonists & inhibitors, Matrix Metalloproteinase Inhibitors, Protease Inhibitors pharmacology

Abstract

Lack of target specificity by existing matrix metalloproteinase (MMP) inhibitors has hindered antimetastatic cancer drug discovery. Inhibitors that bind to noncatalytic sites of MMPs and disrupt protease signaling function have the potential to be more specific and selective. In this work, compounds that target the hemopexin (PEX) domain of MMP-9 were identified using an in silico docking approach and evaluated using biochemical and biological approaches. Two of the selected compounds interfere with MMP-9-mediated cancer cell migration and proliferation in cells expressing exogenous or endogenous MMP-9. Furthermore, these inhibitors do not modulate MMP-9 catalytic activity. The lead compound, N-[4-(difluoromethoxy)phenyl]-2-[(4-oxo-6-propyl-1H-pyrimidin-2-yl)sulfanyl]-acetamide, specifically binds to the PEX domain of MMP-9, but not other MMPs. This interaction between the compound and the PEX domain results in the abrogation of MMP-9 homodimerization and leads to blockage of a downstream signaling pathway required for MMP-9-mediated cell migration. In a tumor xenograft model, this pyrimidinone retarded MDA-MB-435 tumor growth and inhibited lung metastasis. Thus, we have shown for the first time that a novel small-molecule interacts specifically with the PEX domain of MMP-9 and inhibits tumor growth and metastasis by reducing cell migration and proliferation., (©2011 AACR.)

Published

2011

43. An alternative view of the proposed alternative activities of hemopexin.

Author

Mauk MR, Smith A, and Mauk AG

Subjects

Amino Acid Sequence, Heme chemistry, Heme metabolism, Hemopexin genetics, Humans, Models, Molecular, Oligopeptides chemistry, Oligopeptides genetics, Oligopeptides metabolism, Protein Binding, Recombinant Proteins chemistry, Recombinant Proteins isolation & purification, Recombinant Proteins metabolism, Serine Proteases chemistry, Serine Proteases genetics, Serine Proteases metabolism, Hemopexin chemistry, Hemopexin metabolism, Protein Conformation, Protein Structure, Secondary

Abstract

Hemopexin is a plasma protein that plays a well-established biological role in sequestering heme that is released into the plasma from hemoglobin and myoglobin as the result of intravascular or extravascular hemolysis as well as from skeletal muscle trauma or neuromuscular disease. In recent years, a variety of additional biological activities have been attributed to hemopexin, for example, hyaluronidase activity, serine protease activity, pro-inflammatory and anti-inflammatory activity as well as suppression of lymphocyte necrosis, inhibition of cellular adhesion, and binding of divalent metal ions. This review examines the challenges involved in the purification of hemopexin from plasma and in the recombinant expression of hemopexin and evaluates the questions that these challenges and the characteristics of hemopexin raise concerning the validity of many of the new activities proposed for this protein. As well, an homology model of the three-dimensional structure of human hemopexin is used to reveal that the protein lacks the catalytic triad that is characteristic of many serine proteases but that hemopexin possesses two highly exposed Arg-Gly-Glu sequences that may promote interaction with cell surfaces., (Copyright © 2011 The Protein Society.)

Published

2011

44. A comparative evaluation of Golgi protein-73, fucosylated hemopexin, α-fetoprotein, and PIVKA-II in the serum of patients with chronic hepatitis, cirrhosis, and hepatocellular carcinoma.

Author

Morota K, Nakagawa M, Sekiya R, Hemken PM, Sokoll LJ, Elliott D, Chan DW, and Dowell BL

Subjects

Animals, Biomarkers blood, Blood Chemical Analysis standards, Carcinoma, Hepatocellular diagnosis, Enzyme-Linked Immunosorbent Assay standards, Fibrosis, Hemopexin analysis, Hemopexin chemistry, Hepatitis, Chronic diagnosis, Humans, Liver Neoplasms diagnosis, Luminescent Measurements, Protein Precursors blood, Prothrombin, ROC Curve, Reference Standards, alpha-Fetoproteins analysis, Blood Chemical Analysis methods, Carcinoma, Hepatocellular blood, Enzyme-Linked Immunosorbent Assay methods, Hepatitis, Chronic blood, Liver Neoplasms blood, Membrane Proteins blood

Abstract

Background: Golgi protein-73 (GP73) and fucosylated proteins have been proposed as potential serum markers for liver disease and/or hepatocellular carcinoma (HCC). The purpose of this study was to compare the sensitivity and specificity of serum GP73 and fucosylated hemopexin (Fuc-HPX) with α-fetoprotein (AFP) and with protein induced by the absence of vitamin K or antagonist-II (PIVKA-II) for diagnosing chronic hepatitis, cirrhosis, and HCC., Methods: The concentration of GP73 in human sera was determined using an enzyme-linked immunosorbent assay employing mouse monoclonal and rabbit polyclonal GP73 antibodies. Fuc-HPX was detected using a lectin chemiluminescence-linked immunosorbent assay using a mouse monoclonal anti-hemopexin antibody and Aleuria aurantia lectin. A total of 229 serum samples from patients with chronic hepatitis, cirrhosis, and HCC, as well as from normal individuals were evaluated using these four markers., Results: GP73 and Fuc-HPX showed significantly higher values in samples from patients with cirrhosis and HCC than in samples from patients with hepatitis and from normal individuals. The areas under the curves (AUCs) for GP73, Fuc-HPX, AFP, and PIVKA-II were 0.90, 0.77, 0.74, and 0.88, respectively, for liver cirrhosis and HCC samples vs. hepatitis and normal samples. The AUCs of GP73, Fuc-HPX, AFP, and PIVKA-II were 0.78, 0.72, 0.81, and 0.90, respectively, for HCC samples vs. all other samples., Conclusions: PIVKA-II showed superior sensitivity and specificity for HCC compared with the other three markers. GP73 may be useful for detecting cirrhosis as a risk factor for HCC. Fuc-HPX showed inferior sensitivity and specificity compared to the other markers.

Published

2011

45. The dimer interface of the membrane type 1 matrix metalloproteinase hemopexin domain: crystal structure and biological functions.

Author

Tochowicz A, Goettig P, Evans R, Visse R, Shitomi Y, Palmisano R, Ito N, Richter K, Maskos K, Franke D, Svergun D, Nagase H, Bode W, and Itoh Y

Subjects

Animals, COS Cells, Chlorocebus aethiops, Crystallography, Dimerization, Enzyme Activation physiology, HeLa Cells, Hemopexin genetics, Humans, Matrix Metalloproteinase 14 genetics, Membrane Proteins chemistry, Membrane Proteins genetics, Membrane Proteins metabolism, Mutagenesis, Protein Structure, Tertiary, Solubility, Structure-Activity Relationship, Extracellular Matrix enzymology, Hemopexin chemistry, Hemopexin metabolism, Matrix Metalloproteinase 14 chemistry, Matrix Metalloproteinase 14 metabolism

Abstract

Homodimerization is an essential step for membrane type 1 matrix metalloproteinase (MT1-MMP) to activate proMMP-2 and to degrade collagen on the cell surface. To uncover the molecular basis of the hemopexin (Hpx) domain-driven dimerization of MT1-MMP, a crystal structure of the Hpx domain was solved at 1.7 Å resolution. Two interactions were identified as potential biological dimer interfaces in the crystal structure, and mutagenesis studies revealed that the biological dimer possesses a symmetrical interaction where blades II and III of molecule A interact with blades III and II of molecule B. The mutations of amino acids involved in the interaction weakened the dimer interaction of Hpx domains in solution, and incorporation of these mutations into the full-length enzyme significantly inhibited dimer-dependent functions on the cell surface, including proMMP-2 activation, collagen degradation, and invasion into the three-dimensional collagen matrix, whereas dimer-independent functions, including gelatin film degradation and two-dimensional cell migration, were not affected. These results shed light on the structural basis of MT1-MMP dimerization that is crucial to promote cellular invasion.

Published

2011

46. The structure of a haemopexin-fold protein from cow pea (Vigna unguiculata) suggests functional diversity of haemopexins in plants.

Author

Gaur V, Chanana V, Jain A, and Salunke DM

Subjects

Amino Acid Motifs, Amino Acid Sequence, Base Sequence, Calibration, Conserved Sequence, Crystallization, Crystallography, X-Ray methods, Dimerization, Heme metabolism, Hemopexin metabolism, Hydrolysis, Hydrophobic and Hydrophilic Interactions, Lathyrus metabolism, Macromolecular Substances chemistry, Macromolecular Substances metabolism, Models, Molecular, Molecular Sequence Data, Molecular Weight, Plant Proteins isolation & purification, Plant Proteins metabolism, Protein Structure, Secondary, Protein Structure, Tertiary, Protein Subunits chemistry, Proteome analysis, Reference Standards, Seeds chemistry, Sequence Analysis, Protein, Sequence Homology, Amino Acid, Spermine metabolism, Fabaceae metabolism, Hemopexin chemistry, Pisum sativum metabolism, Plant Proteins chemistry, Plants metabolism

Abstract

The haemopexin fold is present in almost all life forms and is utilized for carrying out diverse physiological functions. The structure of CP4, a haemopexin-fold protein from cow pea (Vigna unguiculata), was determined at 2.1 Å resolution. The protein exists as a monomer both in solution and in the crystal. The structure revealed a typical four-bladed β-propeller topology. The protein exhibits 42% sequence similarity to LS-24 from Lathyrus sativus, with substantial differences in the surface-charge distribution and in the oligomeric state. A structure-based sequence analysis of haemopexin-fold proteins of plant and mammalian origin established a sequence signature associated with the haemopexin motif. This signature sequence enabled the identification of other proteins with possible haemopexin-like topology of both plant and animal origin. Although CP4 shares a structural fold with LS-24 and other haemopexins, biochemical studies indicated possible functional differences between CP4 and LS-24. While both of these proteins exhibit spermine-binding potential, CP4 does not bind to haem, unlike LS-24.

Published

2011

47. Thrombin-dependent MMP-2 activity is regulated by heparan sulfate.

Author

Koo BH, Han JH, Yeom YI, and Kim DS

Subjects

Animals, Binding Sites, Brain cytology, COS Cells, Cell Line, Tumor, Chlorocebus aethiops, Hemopexin chemistry, Humans, K562 Cells, Mutation, Protein Conformation, Protein Structure, Tertiary, Heparitin Sulfate chemistry, Matrix Metalloproteinase 2 metabolism, Thrombin chemistry

Abstract

Like most metalloproteases, matrix metalloprotease 2 (MMP-2) is synthesized as a zymogen. MMP-2 propeptide plays a role in inhibition of catalytic activity through a cysteine-zinc ion pairing, disruption of which results in full enzyme activation. A variety of proteases have been shown to be involved in the activation of pro-MMP-2, including metalloproteases and serine proteases. In the previous study we showed that MMP-2 activation occurred via specific cleavages of the propeptide by thrombin followed by intermolecular autoproteolytic processing for full enzymatic activity. Thrombin also degraded MMP-2, but this degradation was reduced greatly under cell-associated conditions with a concomitant increase in activation, prompting us to elucidate the molecular mechanisms underlying thrombin-mediated MMP-2 activation. In the present study we demonstrate that heparan sulfate is essential for thrombin-mediated activation of pro-MMP-2. Binding of heparan sulfate to thrombin is primarily responsible for this activation process, presumably through conformational changes at the active site. Furthermore, interaction of MMP-2 with exosites 1 and 2 of thrombin is crucial for thrombin-mediated MMP-2 degradation, and inhibition of this interaction by heparan sulfate or hirudin fragment results in a decrease in MMP-2 degradation. Finally, we demonstrated interaction between exosite 1 and hemopexin-like domain of MMP-2, suggesting a regulatory role of hemopexin-like domain in MMP-2 degradation. Taken together, our experimental data suggest a novel regulatory mechanism of thrombin-dependent MMP-2 enzymatic activity by heparan sulfate proteoglycans.

Published

2010

48. Molecular interactions of MMP-13 C-terminal domain with chondrocyte proteins.

Author

Zhang L, Yang M, Yang D, Cavey G, Davidson P, and Gibson G

Subjects

Cartilage, Articular metabolism, Cartilage, Articular pathology, Cells, Cultured, Chondrocytes pathology, Chromatography, Affinity, Cloning, Molecular, Conserved Sequence, Hemopexin chemistry, Hemopexin metabolism, Kidney, Mass Spectrometry, Matrix Metalloproteinase 13 chemistry, Osteoarthritis pathology, Peptide Mapping, Protein Binding, Proteoglycans metabolism, Vesicular Transport Proteins metabolism, Catalytic Domain, Chondrocytes metabolism, Matrix Metalloproteinase 13 metabolism

Abstract

Matrix metalloproteinases (MMP)-13 activity is necessary for normal skeletal development and plays a central role in cartilage degeneration associated with osteoarthritis (OA). The studies we described here examine the interactions of the hemopexin domain of MMP-13 with proteins secreted by human chondrocytes in culture. The hemopexin domain of the MMPs and many other proteins in which this structure is found mediates protein function by forming the primary site of interaction with other proteins. We have modified a tandem affinity expression tag (hTAP) to enable efficient expression of the tagged bait protein. In this case the MMP-13 C-terminal domain (CTD) comprises hinge and hemopexin domain, and we immobilized the fusion construct on a column of agarose bound immunoglobin G. The MMP-13 CTD affinity column so generated enabled the efficient and gentle isolation of interacting proteins from the culture medium of human articular chondrocytes. TIMP1 and alpha2-macroglobulin previously shown to interact with MMP-13 as well as several proteins, fibronectin, type VI collagen and xylosyltransferase 1 and several proteoglycans, decorin, syndecan 4 and serglycin not previously recognized as interacting with MMP-13 were identified by mass spectrometry. The interaction between isolated proteins and MMP-13 CTD was verified by yeast two hybrid analysis. We also demonstrated serglycin expression by chondrocytes for the first time and its co localization with MMP-13 in a cytoplasmic granular morphology. The consequence of these interactions remains to be demonstrated, however; binding to MMP-13 suggests a role in the regulation of cartilage degradation.

Published

2010

49. Crystal structure and functional insights of hemopexin fold protein from grass pea.

Author

Gaur V, Qureshi IA, Singh A, Chanana V, and Salunke DM

Subjects

Amino Acid Sequence, Crystallography, X-Ray, Models, Molecular, Molecular Sequence Data, Protein Conformation, Protein Folding, Hemopexin chemistry, Pisum sativum chemistry

Abstract

A regulatory protein from grass pea (Lathyrus sativus), LS-24, a close homolog of albumin 2 from garden pea (Pisum sativum) that is associated with polyamine biosynthesis, was characterized and the structure of a hemopexin-type fold among plant proteins illustrated. Crystal structure of LS-24 determined at 2.2 A resolution by multiple isomorphous replacement phasing showed four-bladed beta-propeller structure having a pseudo 4-fold molecular symmetry along a metal ion-binding central channel. The structure represents typical mammalian hemopexin fold with discernible features correlated with the possible functional variations. The protein was found to exist in the dimeric state. While LS-24 dimer binds to spermine in the crystal structure as well as in solution, binding of heme in solution resulted in the dissociation of the dimer into monomers with concomitant release of bound spermine. Interactions of heme and spermine with LS-24 bear physiological implications. While binding of spermine to LS-24 can be linked with polyamine biosynthesis that of heme correlates with oxidative stress. Mutually exclusive binding of heme and spermine in different oligomeric states suggest a role for LS-24 in sensing oxidative stress through a ligand-regulated monomer-dimer transition switch.

Published

2010

50. Quantitation of saccharide compositions of O-glycans by mass spectrometry of glycopeptides and its application to rheumatoid arthritis.

Author

Wada Y, Tajiri M, and Ohshima S

Subjects

Acetylgalactosamine chemistry, Hemopexin chemistry, Humans, Immunoglobulin A chemistry, Mucins chemistry, Arthritis, Rheumatoid metabolism, Glycopeptides chemistry, Mass Spectrometry methods, Oligosaccharides analysis, Polysaccharides analysis

Abstract

Profiling of oligosaccharide structures is widely utilized for both identification and evaluation of glycobiomarkers, and site-specific profiling of N-linked glycans of glycoproteins is conducted by mass spectrometry of glycopeptides. However, our knowledge of mucin-type O-glycans including site occupancy and profile variance, as well as attachment sites, is quite limited. Saccharide compositions and site-occupancy of O-glycans were calculated from the signal intensity of glycopeptide ions in the mass spectra and tandem mass spectra from electron transfer dissociation. The results for two major plasma glycoproteins, IgA1 and hemopexin, representing clustered and scattered O-glycan attachments, respectively, indicated that the variability in modifications among individuals is so small as to justify rigorous standards enabling reliable detection of disease-related alterations. Indeed, this method revealed a novel abnormality associated with rheumatoid arthritis: a significant decrease in the N-acetylgalactosamine content of IgA1 O-glycans, indicating that the glycosylation abnormality is not limited to hypogalactosylation of IgG N-glycans in chronic inflammatory conditions.

Published

2010