Your search keyword '"G, Ronzoni"' showing total 66 results

1. Synthetic glycol-split heparin tri- and tetrasaccharides provide new insights into structural peculiarities for antiheparanase activity.

Author

Ni M, Parafioriti M, Esposito E, Danzi M, Cano O, Muzi L, Kayal Y, Ferro V, Vlodavsky I, Elli S, Naggi A, Petitou M, and Guerrini M

Subjects

Humans, Oligosaccharides chemistry, Oligosaccharides chemical synthesis, Oligosaccharides pharmacology, Enzyme Inhibitors chemistry, Enzyme Inhibitors pharmacology, Enzyme Inhibitors chemical synthesis, Structure-Activity Relationship, Trisaccharides chemistry, Trisaccharides pharmacology, Trisaccharides chemical synthesis, Glycols chemistry, Glycols pharmacology, Glycols chemical synthesis, Molecular Structure, Glucuronidase antagonists & inhibitors, Glucuronidase metabolism, Heparin chemistry, Heparin pharmacology, Heparin chemical synthesis, Molecular Docking Simulation

Abstract

Heparanase is the only known endo-β-glucuronidase able to cleave heparan sulfate, participating in degradation and remodelling of the extracellular matrix. Heparanase upregulation promotes tumor growth and metastasis, therefore, its inhibition is a target for anticancer therapies. Heparan sulfate mimetics bearing glycol-split (gs) units are one of the most promising class of heparanase inhibitors. Herein we describe a total synthesis of two trisaccharides (MeO-GlcNS6S-IdoA/GlcA-GlcNS6S-OMe) differing in epimeric uronic acid residues and one tetrasaccharide (MeO-IdoA-GlcNS6S-IdoA-GlcNS6S-OMe), together with their corresponding glycol-split versions, prepared by periodate oxidation and further modified either via reduction or Pinnick oxidation to obtain gs or tricarboxylated saccharides. An intermediate imine was observed during periodate oxidation, which causes formation of byproducts. Evaluation of the heparanase inhibitory activity showed that the glycol-split trisaccharides were more potent than their intact uronic acid congeners. The binding interactions of the glycol-split trisaccharides with heparanase were investigated by a combined STD NMR and molecular docking approach, with good agreement obtained between the STD NMR experimental data, docking calculations and the in vitro activity results, helping to rationalize the observed inhibition data., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 Elsevier Ltd. All rights reserved.)

Published

2025

2. Differential Solvent DEEP-STD NMR and MD Simulations Enable the Determinants of the Molecular Recognition of Heparin Oligosaccharides by Antithrombin to Be Disentangled.

Author

Parafioriti M, Elli S, Muñoz-García JC, Ramírez-Cárdenas J, Yates EA, Angulo J, and Guerrini M

Subjects

Humans, Binding Sites, Epitope Mapping methods, Magnetic Resonance Spectroscopy methods, Molecular Dynamics Simulation, Protein Binding, Solvents chemistry, Antithrombins chemistry, Antithrombins metabolism, Heparin chemistry, Heparin metabolism, Oligosaccharides chemistry, Oligosaccharides metabolism

Abstract

The interaction of heparin with antithrombin (AT) involves a specific sequence corresponding to the pentasaccharide GlcNAc/NS6S-GlcA-GlcNS3S6S-IdoA2S-GlcNS6S (AGA*IA). Recent studies have revealed that two AGA*IA-containing hexasaccharides, which differ in the sulfation degree of the iduronic acid unit, exhibit similar binding to AT, albeit with different affinities. However, the lack of experimental data concerning the molecular contacts between these ligands and the amino acids within the protein-binding site prevents a detailed description of the complexes. Differential epitope mapping (DEEP)-STD NMR, in combination with MD simulations, enables the experimental observation and comparison of two heparin pentasaccharides interacting with AT, revealing slightly different bound orientations and distinct affinities of both glycans for AT. We demonstrate the effectiveness of the differential solvent DEEP-STD NMR approach in determining the presence of polar residues in the recognition sites of glycosaminoglycan-binding proteins.

Published

2024

3. Heparins are potent inhibitors of ectonucleotide pyrophosphatase/phospho-diesterase-1 (NPP1) - a promising target for the immunotherapy of cancer.

Author

Lopez V, Schuh HJM, Mirza S, Vaaßen VJ, Schmidt MS, Sylvester K, Idris RM, Renn C, Schäkel L, Pelletier J, Sévigny J, Naggi A, Scheffler B, Lee SY, Bendas G, and Müller CE

Subjects

Humans, Immunotherapy, Anticoagulants, Heparin, Low-Molecular-Weight pharmacology, Heparin, Low-Molecular-Weight therapeutic use, Heparin pharmacology, Glioma

Abstract

Introduction: Heparins, naturally occurring glycosaminoglycans, are widely used for thrombosis prevention. Upon application as anticoagulants in cancer patients, heparins were found to possess additional antitumor activities. Ectonucleotidases have recently been proposed as novel targets for cancer immunotherapy., Methods and Results: In the present study, we discovered that heparin and its derivatives act as potent, selective, allosteric inhibitors of the poorly investigated ectonucleotidase NPP1 (nucleotide pyrophosphatase/phosphodiesterase-1, CD203a). Structure-activity relationships indicated that NPP1 inhibition could be separated from the compounds' antithrombotic effect. Moreover, unfractionated heparin (UFH) and different low molecular weight heparins (LMWHs) inhibited extracellular adenosine production by the NPP1-expressing glioma cell line U87 at therapeutically relevant concentrations. As a consequence, heparins inhibited the ability of U87 cell supernatants to induce CD4+ T cell differentiation into immunosuppressive Treg cells., Discussion: NPP1 inhibition likely contributes to the anti-cancer effects of heparins, and their specific optimization may lead to improved therapeutics for the immunotherapy of cancer., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2023 Lopez, Schuh, Mirza, Vaaßen, Schmidt, Sylvester, Idris, Renn, Schäkel, Pelletier, Sévigny, Naggi, Scheffler, Lee, Bendas and Müller.)

Published

2023

4. Blended Heparin: A new Perspective to Guarantee the Supply of a Life-Saving Drug?

Author

Guerrini M

Subjects

Animals, Sheep, Cattle, Swine, Europe, Heparin, Low-Molecular-Weight, Heparin pharmacology, Heparin therapeutic use, Anticoagulants pharmacology, Anticoagulants therapeutic use

Abstract

The risk of heparin shortage opens up the possibility of diversifying the sources of heparin by introducing products of other animal/organ origins. In addition to bovine heparin, already used in the past in the United States and Europe, ovine heparin can become another alternative to the widely used pig source. It is therefore appropriate to compare the anticoagulant activity of pig heparin with that of products of different animal origin and to verify whether blended heparin obtained from different sources can give rise to anticoagulant effects comparable to those of heparin of a single origin.

Published

2023

5. NMR spectroscopy and chemometric models to detect a specific non-porcine ruminant contaminant in pharmaceutical heparin.

Author

Colombo E, Mauri L, Marinozzi M, Rudd TR, Yates EA, Ballabio D, and Guerrini M

Subjects

Animals, Discriminant Analysis, Least-Squares Analysis, Magnetic Resonance Spectroscopy methods, Pharmaceutical Preparations, Swine, Heparin analysis, Ruminants

Abstract

Heparin has been used successfully as a clinical antithrombotic for almost one century. Its isolation from animal sources (mostly porcine intestinal mucosa) involves multistep purification processes starting from the slaughterhouse (as mucosa) to the pharmaceutical plant (as the API). This complex supply chain increases the risk of contamination and adulteration, mainly with non-porcine ruminant material. The structural similarity of heparins from different origins, the natural variability of the heparin within samples from each source as well as the structural changes induced by manufacturing processes, require increasingly sophisticated methods capable of detecting low levels of contamination. The application of suitable multivariate classification approaches on API 1 H NMRspectra serve as rapid and reliable tools for product authentication and the detection of contaminants. Soft Independent Modeling of Class Analogies (SIMCA), Discriminant Analysis (DA), Partial Least Square Discriminant Analysis (PLS-DA) and local classification methods (kNN, BNN and N3) were tested on about one hundred certified heparin samples produced by 14 different manufacturers revealing that Partial Least Squares Discriminant Analysis (PLS-DA) provided the best discrimination of contaminated batches, with a balanced accuracy of 97%., (Copyright © 2022 Elsevier B.V. All rights reserved.)

Published

2022

6. Structural variation in the linkage region of pharmaceutical heparin arising from oxidative treatments during manufacture.

Author

Urso E, Mantione G, Sala F, Yates EA, Guerrini M, and Naggi A

Subjects

Animals, Carbohydrate Sequence, Heparin Lyase, Oxidative Stress, Pharmaceutical Preparations chemical synthesis, Swine, Heparin chemical synthesis, Heparin chemistry, Oligosaccharides chemistry

Abstract

During the manufacture of pharmaceutical heparin, a range of treatments are applied to sanitize, decolourise and reduce the pyrogenic properties of the samples. The structural effects of bleaching, an oxidative process, are examined. Among 1 H and 13 C NMR signals ascribable to the tetrasaccharide linkage region of heparin, samples of porcine mucosal heparin frequently display characteristic signals at chemical shift values of 4.5 and 106 ppm respectively, which have not been explained previously. Fractions enriched with material reporting this signal were isolated from heparinase digested porcine mucosal heparin samples and subjected to analysis using mass spectrometry and NMR spectroscopy. A novel structure, ΔU-Gal-Gal-Xyl-CH 2 -CONH 2 , was identified by mass fragmentation experiments and further interesting structural motifs emerged following evaluation by mass spectrometry of longer oligosaccharide chains biosynthesized away from the linker tetrasaccharide, GlcA-Gal-Gal-Xyl. The carbohydrate-protein linkage region is thus affected by the bleaching step involved in the manufacturing process of heparin. The discovery of specific modifications that reflect the extent of the oxidation treatment adopted is relevant to the monitoring of inadvertent damage to the heparin structure during manufacture that contributes to sample variation and which could also lead to reduced drug quality., (Copyright © 2022 Elsevier Ltd. All rights reserved.)

Published

2022

7. Saturated tetrasaccharide profile of enoxaparin. An additional piece to the heparin biosynthesis puzzle.

Author

Gardini C, Bisio A, Mazzini G, Guerrini M, Naggi A, and Alekseeva A

Subjects

Chromatography, High Pressure Liquid methods, Enoxaparin metabolism, Fibrinolytic Agents chemistry, Glucosamine metabolism, Glucuronic Acid chemistry, Heparin Lyase metabolism, Humans, Iduronic Acid chemistry, Magnetic Resonance Spectroscopy methods, Mass Spectrometry methods, Oligosaccharides metabolism, Enoxaparin chemistry, Heparin biosynthesis, Oligosaccharides chemistry

Abstract

Enoxaparin, widely used antithrombotic drug, is a polydisperse glycosaminoglycan with highly microheterogeneous structure dictated by both parent heparin heterogeneity and depolymerization conditions. While the process-related modifications of internal and terminal sequences of enoxaparin have been extensively studied, very little is known about the authentic non-reducing ends (NRE). In the present study a multi-step isolation and thorough structural elucidation by NMR and LC/MS allowed to identify 16 saturated tetramers along with 23 unsaturated ones in the complex enoxaparin tetrasaccharide fraction. Altogether the elucidated structures represent a unique enoxaparin signature, whereas the composition of saturated tetramers provides a structural readout strictly related to the biosynthesis of parent heparin NRE. In particular, both glucuronic and iduronic acids were detected at the NRE of macromolecular heparin. The tetrasaccharides bearing glucosamine at the NRE are most likely associated with the heparanase hydrolytic action. High sulfation degree and 3-O-sulfation are characteristic for both types of NRE., (Copyright © 2021 Elsevier Ltd. All rights reserved.)

Published

2021

8. BMP6 binding to heparin and heparan sulfate is mediated by N-terminal and C-terminal clustered basic residues.

Author

Denardo A, Elli S, Federici S, Asperti M, Gryzik M, Ruzzenenti P, Carmona F, Bergese P, Naggi A, Arosio P, and Poli M

Subjects

Animals, Binding Sites, Bone Morphogenetic Protein 6 chemistry, CHO Cells, Cricetulus, Hep G2 Cells, Hepcidins metabolism, Humans, Models, Molecular, Protein Binding, Protein Interaction Domains and Motifs, Bone Morphogenetic Protein 6 metabolism, Heparin metabolism, Heparitin Sulfate metabolism

Abstract

Background: The bone morphogenetic protein 6 (BMP6) is a crucial inducer of hepcidin, the peptide hormone that regulates the iron availability in our body. Hepcidin expression is influenced by hepatic heparan sulfate (HS) and by heparin administration, suggesting BMP6 interaction with heparin/HS. The BMP2/4 subfamily has been deeply characterized to have a N-terminal heparin/HS binding domain (HBD), whose basic residues contact the sulfate groups on heparin and HS. Such detailed characterization is still required for other, structurally different BMPs, including BMP6., Methods: BMP6 peptides encompassing potential HBDs were analysed on heparin-functionalized plates and microcantilevers, and on membrane HS expressing CHO-K1 cells. Monomeric wild-type BMP6 and mutants were produced, substituting the basic residues with non-charged ones, and their affinity to the heparin-column was measured. The BMP6-heparin interaction was also predicted at atomic level by in silico molecular dynamics., Results: N-terminal and C-terminal BMP6 peptides showed high heparin affinity in solid-phase assays. The mutation of the two sites (R5L, R6S, R7L and K126N, K127N, R129S) abolished the heparin-binding activity of the recombinant monomeric BMP6. Monomeric BMP6 and peptides specifically bound to membrane HS of CHO-K1 cells through the same domains. Molecular dynamic studies supported the role of the two HBDs, suggesting a cooperative behaviour., Conclusions: In BMP6, N-terminal (R5, R6, R7) and C-terminal (K126, K127, R129) domains mediate the interaction with heparin and HS., General Significance: This study provides the molecular mechanism supporting the use of heparin to sequester BMP6 and inhibit hepcidin expression, a novel clinical approach for high-hepcidin iron disorders., (Copyright © 2020 Elsevier B.V. All rights reserved.)

Published

2021

9. Heparin Inhibits Cellular Invasion by SARS-CoV-2: Structural Dependence of the Interaction of the Spike S1 Receptor-Binding Domain with Heparin.

Author

Mycroft-West CJ, Su D, Pagani I, Rudd TR, Elli S, Gandhi NS, Guimond SE, Miller GJ, Meneghetti MCZ, Nader HB, Li Y, Nunes QM, Procter P, Mancini N, Clementi M, Bisio A, Forsyth NR, Ferro V, Turnbull JE, Guerrini M, Fernig DG, Vicenzi E, Yates EA, Lima MA, and Skidmore MA

Subjects

Animals, Anticoagulants therapeutic use, Antiviral Agents therapeutic use, Chlorocebus aethiops, Enoxaparin therapeutic use, Heparin therapeutic use, Humans, Molecular Dynamics Simulation, Nebulizers and Vaporizers, Protein Binding, Protein Conformation, Protein Domains genetics, Spike Glycoprotein, Coronavirus chemistry, Spike Glycoprotein, Coronavirus genetics, Structure-Activity Relationship, Vero Cells, Virus Internalization, Anticoagulants pharmacology, Antiviral Agents pharmacology, Enoxaparin pharmacology, Heparin pharmacology, SARS-CoV-2 physiology, Spike Glycoprotein, Coronavirus metabolism, COVID-19 Drug Treatment

Abstract

The dependence of development and homeostasis in animals on the interaction of hundreds of extracellular regulatory proteins with the peri- and extracellular glycosaminoglycan heparan sulfate (HS) is exploited by many microbial pathogens as a means of adherence and invasion. Heparin, a widely used anticoagulant drug, is structurally similar to HS and is a common experimental proxy. Exogenous heparin prevents infection by a range of viruses, including S-associated coronavirus isolate HSR1. Here, we show that heparin inhibits severe acute respiratory syndrome coronavirus-2 (SARS-CoV-2) invasion of Vero cells by up to 80% at doses achievable through prophylaxis and, particularly relevant, within the range deliverable by nebulisation. Surface plasmon resonance and circular dichroism spectroscopy demonstrate that heparin and enoxaparin, a low-molecular-weight heparin which is a clinical anticoagulant, bind and induce a conformational change in the spike (S1) protein receptor-binding domain (S1 RBD) of SARS-CoV-2. A library of heparin derivatives and size-defined fragments were used to probe the structural basis of this interaction. Binding to the RBD is more strongly dependent on the presence of 2- O or 6- O sulfate groups than on N -sulfation and a hexasaccharide is the minimum size required for secondary structural changes to be induced in the RBD. It is likely that inhibition of viral infection arises from an overlap between the binding sites of heparin/HS on S1 RBD and that of the angiotensin-converting enzyme 2. The results suggest a route for the rapid development of a first-line therapeutic by repurposing heparin and its derivatives as antiviral agents against SARS-CoV-2 and other members of the Coronaviridae ., Competing Interests: None declared., (Thieme. All rights reserved.)

Published

2020

10. Degeneracy of the Antithrombin Binding Sequence in Heparin: 2-O-Sulfated Iduronic Acid Can Replace the Critical Glucuronic Acid.

Author

Elli S, Stancanelli E, Wang Z, Petitou M, Liu J, and Guerrini M

Subjects

Anticoagulants pharmacology, Antithrombins metabolism, Magnetic Resonance Spectroscopy, Molecular Conformation, Sulfates chemistry, Anticoagulants chemistry, Antithrombins chemistry, Glucuronic Acid chemistry, Heparin chemistry, Iduronic Acid chemistry, Oligosaccharides chemistry, Polysaccharides chemistry

Abstract

Heparin binds to and activates antithrombin (AT) through a specific pentasaccharide sequence, in which a trisaccharide subsite, containing glucuronic acid (GlcA), has been considered as the initiator in the recognition of the polysaccharide by the protein. Recently it was suggested that sulfated iduronic acid (IdoA2S) could replace this "canonical" GlcA. Indeed, a heparin octasaccharidic sequence obtained by chemoenzymatic synthesis, in which GlcA is replaced with IdoA2S, has been found to similarly bind to and activate antithrombin. By using saturation-transfer-difference (STD) NMR, NOEs, transferred NOEs (tr-NOEs) NMR and molecular dynamics, we show that, upon binding to AT, this IdoA2S unit develops comparable interactions with AT as GlcA. Interestingly, two IdoA2S units, both present in a 1 C 4 - 2 S 0 equilibrium in the unbound saccharide, shift to full 2 S 0 and full 1 C 4 upon binding to antithrombin, providing the best illustration of the critical role of iduronic acid conformational flexibility in biological systems., (© 2020 Wiley-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2020

11. Novel N-acetyl-Glycol-split heparin biotin-conjugates endowed with anti-heparanase activity.

Author

Esposito E, Vlodavsky I, Barash U, Roscilli G, Milazzo FM, Giannini G, and Naggi A

Subjects

Animals, Antineoplastic Agents chemical synthesis, Antineoplastic Agents chemistry, Cell Proliferation drug effects, Dose-Response Relationship, Drug, Drug Screening Assays, Antitumor, Female, Glucuronidase metabolism, Glycols chemical synthesis, Glycols chemistry, Glycoside Hydrolase Inhibitors chemical synthesis, Glycoside Hydrolase Inhibitors chemistry, Melanoma, Experimental drug therapy, Melanoma, Experimental metabolism, Melanoma, Experimental pathology, Mice, Mice, Inbred C57BL, Molecular Structure, Optical Imaging, Structure-Activity Relationship, Antineoplastic Agents pharmacology, Biotin chemistry, Glucuronidase antagonists & inhibitors, Glycols pharmacology, Glycoside Hydrolase Inhibitors pharmacology, Heparin chemistry

Abstract

Heparanase is regarded as a promising target for anticancer drugs and Ronepastat is one of the most promising heparanase inhibitors insert in clinical study for Multiple Myeloma Therapy. To improve its pharmacokinetic/pharmacodynamic profile, as well to have an antidote able to neutralize its activity in case of over dosages or intolerance, a new class of its derivatives was obtained inserting non-carbohydrate moieties of different length between the polysaccharide chain and biotin or its derivatives. In vitro these novel derivatives maintain the anti-heparanase activity without induced toxicity. The newly synthesized compounds retained the ability to attenuate the growth of CAG myeloma tumors in mice with potency similar, or in one case even higher than that of the reference compound Roneparstat as well as inhibited metastatic dissemination (lung colonization) of murine B16-F10 melanoma cells in vivo., (Copyright © 2019 Elsevier Masson SAS. All rights reserved.)

Published

2020

12. Non-Anticoagulant Heparins as Heparanase Inhibitors.

Author

Cassinelli G, Torri G, and Naggi A

Subjects

Animals, Glucuronidase metabolism, Heparin chemistry, Heparitin Sulfate metabolism, Humans, Neoplasms drug therapy, Glucuronidase antagonists & inhibitors, Heparin analogs & derivatives, Heparin pharmacology

Abstract

The chapter will review early and more recent seminal contributions to the discovery and characterization of heparanase and non-anticoagulant heparins inhibiting its peculiar enzymatic activity. Indeed, heparanase displays a unique versatility in degrading heparan sulfate chains of several proteoglycans expressed in all mammalian cells. This endo-β-D-glucuronidase is overexpressed in cancer, inflammation, diabetes, atherosclerosis, nephropathies and other pathologies. Starting from known low- or non-anticoagulant heparins, the search for heparanase inhibitors evolved focusing on structure-activity relationship studies and taking advantage of new chemical-physical analytical methods which have allowed characterization and sequencing of polysaccharide chains. New methods to screen heparanase inhibitors and to evaluate their mechanism of action and in vivo activity in experimental models prompted their development. New non-anticoagulant heparin derivatives endowed with anti-heparanase activity are reported. Some leads are under clinical evaluation in the oncology field (e.g., acute myeloid leukemia, multiple myeloma, pancreatic carcinoma) and in other pathological conditions (e.g., sickle cell disease, malaria, labor arrest).

Published

2020

13. Molecular Aspects of Heparanase Interaction with Heparan Sulfate, Heparin and Glycol Split Heparin.

Author

Elli S and Guerrini M

Subjects

Humans, Hydrolysis, Substrate Specificity, Glucuronidase antagonists & inhibitors, Glucuronidase chemistry, Glucuronidase metabolism, Glycols chemistry, Glycols metabolism, Heparin chemistry, Heparin metabolism, Heparitin Sulfate chemistry, Heparitin Sulfate metabolism

Abstract

Heparanase is the principal enzyme that degrades heparan sulfate (HS) in both physiological (HS turnover) and pathological (tumor metastasis, inflammation) cell conditions, catalysing the hydrolysis of the β-1-4 glycosidic bond in -GlcUA-β(1-4)-GlcNX-. Despite efforts to define the minimum trisaccharide sequence that allows glycans to be recognized by heparanase, a rigorous "molecular code" by which the enzyme reads and degrades HS chains has not been identified. The X-ray diffraction model of heparanase, resolved by Wu et al (2015), revealed a complex between the trisaccharide GlcNS6S-GlcUA-GlcNS6S and heparanase. Efforts are ongoing to better understand how HS mimetics longer than three residues are recognized by heparanase before being hydrolyzed or inhibit the enzyme. It is also important to consider the flexibility of the enzyme active site, a feature that opens up the development of heparanase inhibitors with structures significantly different from HS or heparin. This chapter reviews the state-of-the-art knowledge about structural aspects of heparanase activities in terms of substrate recognition, mechanism of hydrolysis, and inhibition.

Published

2020

14. Heparanase as an Additional Tool for Detecting Structural Peculiarities of Heparin Oligosaccharides.

Author

Alekseeva A, Urso E, Mazzini G, and Naggi A

Subjects

Animals, Antithrombins chemistry, Binding Sites, Cattle, Chromatography, High Pressure Liquid, Heparin, Low-Molecular-Weight chemistry, Molecular Structure, Polymerization, Protein Binding, Spectrometry, Mass, Electrospray Ionization, Tandem Mass Spectrometry, Glucuronidase chemistry, Heparin chemistry, Oligosaccharides chemistry

Abstract

Due to the biological properties of heparin and low-molecular-weight heparin (LMWH), continuous advances in elucidation of their microheterogeneous structure and discovery of novel structural peculiarities are crucial. Effective strategies for monitoring manufacturing processes and assessment of more restrictive specifications, as imposed by the current regulatory agencies, need to be developed. Hereby, we apply an efficient heparanase-based strategy to assert the structure of two major isomeric octasaccharides of dalteparin and investigate the tetrasaccharides arising from antithrombin binding region (ATBR) of bovine mucosal heparin. Heparanase, especially when combined with other sample preparation methods (e.g., size exclusion, affinity chromatography, heparinase depolymerization), was shown to be a powerful tool providing relevant information about heparin structural peculiarities. The applied approach provided direct evidence that oligomers bearing glucuronic acid-glucosamine-3- O -sulfate at their nonreducing end represent an important structural signature of dalteparin. When extended to ATBR-related tetramers of bovine heparin, the heparanase-based approach allowed for elucidation of the structure of minor sequences that have not been reported yet. The obtained results are of high importance in the view of the growing interest of regulatory agencies and manufacturers in the development of low-molecular-weight heparin generics as well as bovine heparin as alternative source.

Published

2019

15. Fine structural characterization of sulodexide.

Author

Veraldi N, Guerrini M, Urso E, Risi G, Bertini S, Bensi D, and Bisio A

Subjects

Chemical Fractionation, Chromatography, High Pressure Liquid, Dermatan Sulfate chemistry, Glycosaminoglycans chemistry, Heparin chemistry, Magnetic Resonance Spectroscopy, Mass Spectrometry, Molecular Structure, Molecular Weight, Oligosaccharides, Dermatan Sulfate analysis, Glycosaminoglycans analysis, Heparin analysis

Abstract

Sulodexide is a heparinoid which combines the properties of its components heparin and dermatan sulfate and is used not only for the prophylaxis and treatment of thromboembolic diseases but also for the treatment of diabetic nephropathy. Despite many clinical studies have been conducted to investigate its activity and safety, no data are available on the fine chemical characterization of its components. In this work, the in-depth investigation on the structural features of both the whole mixture and the isolated components was accomplished, involving the analysis of molecular weight distribution and of their mono, di and oligosaccharide composition by HP-SEC/TDA, 2D-NMR and HPLC-MS techniques. Moreover, also the separation of fractions endowed of graded affinity to antithrombin was achieved followed again by detailed structural analysis. The combination of different techniques permits to profile in depth the structural features of such a drug and offers a useful tool for possible analysis of batch production., (Copyright © 2018 Elsevier B.V. All rights reserved.)

Published

2018

16. The effect of increasing the sulfation level of chondroitin sulfate on anticoagulant specific activity and activation of the kinin system.

Author

Hogwood J, Naggi A, Torri G, Page C, Rigsby P, Mulloy B, and Gray E

Subjects

Animals, Anticoagulants chemistry, Anticoagulants pharmacology, Chondroitin Sulfates chemistry, Chondroitin Sulfates pharmacology, Dose-Response Relationship, Drug, Drug Contamination, Enzyme Activation drug effects, Heparin Cofactor II metabolism, Humans, Structure-Activity Relationship, Anticoagulants chemical synthesis, Bradykinin metabolism, Chondroitin Sulfates chemical synthesis, Heparin chemistry, Kallikreins metabolism

Abstract

Oversulfated chondroitin sulfate (OSCS) was identified as a contaminant in certain heparin preparations as the cause of adverse reactions in patients. OSCS was found to possess both plasma anticoagulant activity and the ability to activate prekallikrein to kallikrein. Differentially sulfated chondroitin sulfates were prepared by synthetic modification of chondroitin sulfate and were compared to the activity of OSCS purified from contaminated heparin. Whilst chondroitin sulfate was found to have minimal anticoagulant activity, increasing sulfation levels produced an anticoagulant response which we directly show for the first time is mediated through heparin cofactor II. However, the tetra-sulfated preparations did not possess any higher anticoagulant activity than several tri-sulfated variants, and also had lower heparin cofactor II mediated activity. Activation of prekallikrein was concentration dependent for all samples, and broadly increased with the degree of sulfation, though the di-sulfated preparation was able to form more kallikrein than some of the tri-sulfated preparations. The ability of the samples to activate the kinin system, as measured by bradykinin, was observed to be through kallikrein generation. These results show that whilst an increase in sulfation of chondroitin sulfate did cause an increase in anticoagulant activity and activation of the kinin system, there may be subtler structural interactions other than sulfation at play given the different responses observed.

Published

2018

17. Looking Forward to the Future of Heparin: New Sources, Developments and Applications.

Author

Torri G and Cassinelli G

Subjects

Animals, Humans, Heparin chemistry, Heparin therapeutic use

Abstract

The seven reviews and the eleven articles in this special issue provide an updated survey of recent research and developments in the ever-growing field of heparin, along with low molecular weight heparins (LMWHs) and glycosaminoglycans (GAGs)., Competing Interests: The authors declare no conflict of interest.

Published

2018

18. Remembering Professor Benito Casu (1927-2016).

Author

Torri G and Cassinelli G

Subjects

History, 20th Century, History, 21st Century, Humans, Drug Discovery history, Heparin history

Abstract

Heparin and related drugs have contributed in so many different ways to the drug discovery process, and have provided a platform to understand the pathophysiology of vascular and inflammatory diseases for nearly 100 years., Competing Interests: The authors declare no conflict of interest.

Published

2018

19. Characterization of PF4-Heparin Complexes by Photon Correlation Spectroscopy and Zeta Potential.

Author

Bertini S, Fareed J, Madaschi L, Risi G, Torri G, and Naggi A

Subjects

Animals, Cattle, Heparin chemistry, Heparin, Low-Molecular-Weight, Humans, Macromolecular Substances immunology, Platelet Factor 4 chemistry, Sheep, Spectrum Analysis, Swine, Heparin immunology, Macromolecular Substances chemistry, Platelet Factor 4 immunology

Abstract

Heparin-induced thrombocytopenia (HIT) is associated with antibodies to complexes between heparin and platelet factor 4 (PF4), a basic protein usually found in platelet alpha granules. Heparin-induced thrombocytopenia antibodies preferentially recognize macromolecular complexes formed between positively charged PF4 and polyanionic heparins over a narrow range of molar ratios. The aim of this work was to study the complexes that human PF4 forms with heparins from various species, such as porcine, bovine, and ovine; heparins from various organs, such as mucosa and lung; and different low-molecular-weight heparins (LMWHs) at several stoichiometric ratios to evaluate their sizes and charges by photo correlation spectroscopy and zeta potential measurements. The resulting data of the PF4 complexes with unfractionated heparins (UFHs), LMWHs and their fractions, and oligosaccharide components suggest that the size of aggregates is not only a simple function of average molecular weight but also of the molecular weight distribution of the sample. Moreover, it was found that lower concentrations of the tested ovine-derived mucosal heparin are required to form the large PF4/heparin complexes as compared to mucosal porcine and bovine heparin.

Published

2017

20. Molecular Weights of Bovine and Porcine Heparin Samples: Comparison of Chromatographic Methods and Results of a Collaborative Survey.

Author

Bertini S, Risi G, Guerrini M, Carrick K, Szajek AY, and Mulloy B

Subjects

Animals, Anticoagulants chemistry, Cattle, Chromatography methods, Europe, India, Intestinal Mucosa metabolism, Molecular Weight, Surveys and Questionnaires, Swine, Heparin chemistry

Abstract

In a collaborative study involving six laboratories in the USA, Europe, and India the molecular weight distributions of a panel of heparin sodium samples were determined, in order to compare heparin sodium of bovine intestinal origin with that of bovine lung and porcine intestinal origin. Porcine samples met the current criteria as laid out in the USP Heparin Sodium monograph. Bovine lung heparin samples had consistently lower average molecular weights. Bovine intestinal heparin was variable in molecular weight; some samples fell below the USP limits, some fell within these limits and others fell above the upper limits. These data will inform the establishment of pharmacopeial acceptance criteria for heparin sodium derived from bovine intestinal mucosa. The method for MW determination as described in the USP monograph uses a single, broad standard calibrant to characterize the chromatographic profile of heparin sodium on high-resolution silica-based GPC columns. These columns may be short-lived in some laboratories. Using the panel of samples described above, methods based on the use of robust polymer-based columns have been developed. In addition to the use of the USP's broad standard calibrant for heparin sodium with these columns, a set of conditions have been devised that allow light-scattering detected molecular weight characterization of heparin sodium, giving results that agree well with the monograph method. These findings may facilitate the validation of variant chromatographic methods with some practical advantages over the USP monograph method.

Published

2017

21. Combining NMR Spectroscopy and Chemometrics to Monitor Structural Features of Crude Hep-arin.

Author

Mauri L, Marinozzi M, Mazzini G, Kolinski RE, Karfunkle M, Keire DA, and Guerrini M

Subjects

Animals, Chromatography, High Pressure Liquid, Dermatan Sulfate isolation & purification, Drug Contamination, Glycosaminoglycans isolation & purification, Heparin isolation & purification, Heparin standards, Humans, Magnetic Resonance Spectroscopy, Quality Control, Dermatan Sulfate chemistry, Glycosaminoglycans chemistry, Heparin chemistry

Abstract

Because of the complexity and global nature of the heparin supply chain, the control of heparin quality during manufacturing steps is essential to ensure the safety of the final active pharmaceutical ingredient (API). For this reason, there is a need to develop consistent analytical methods able to assess the quality of heparin early in production (i.e., as the crude heparin before it is purified to API under cGMP conditions). Although a number of analytical techniques have been applied to characterize heparin APIs, few of them have been applied for crude heparin structure and composition analyses. Here, to address this issue, NMR spectroscopy and chemometrics were applied to characterize 88 crude heparin samples. The samples were also analyzed by strong anion exchange HPLC (SAX-HPLC) as an orthogonal check of the purity levels of the crudes analyzed by NMR. The HPLC data showed that the chemometric analysis of the NMR data differentiated the samples based on their purity. These orthogonal approaches differentiated samples according their glycosaminoglycan (GAG) composition and their mono and disaccharide composition and structure for each GAG family (e.g., heparin/heparan, dermatan sulfate, and chondroitin sulfate A). Moreover, quantitative HSQC and multivariate analysis (PCA) were used to distinguish between crude heparin of different animal and tissue sources., Competing Interests: The authors declare no conflict of interest. FDA Disclaimer: This publication reflects the views of the author and should not be construed to represent the FDA’s views or policies.

Published

2017

22. Non-Anticoagulant Heparins Are Hepcidin Antagonists for the Treatment of Anemia.

Author

Poli M, Asperti M, Ruzzenenti P, Naggi A, and Arosio P

Subjects

Anemia etiology, Animals, Bone Morphogenetic Protein 6 metabolism, Bone Morphogenetic Proteins metabolism, Gene Expression, Heparitin Sulfate metabolism, Hepcidins genetics, Hepcidins metabolism, Homeostasis, Humans, Iron metabolism, Liver metabolism, Protein Binding, Anemia drug therapy, Anemia metabolism, Heparin pharmacology, Heparin therapeutic use, Hepcidins antagonists & inhibitors

Abstract

The peptide hormone hepcidin is a key controller of systemic iron homeostasis, and its expression in the liver is mainly regulated by bone morphogenetic proteins (BMPs), which are heparin binding proteins. In fact, heparins are strong suppressors of hepcidin expression in hepatic cell lines that act by inhibiting the phosphorylation of SMAD1/5/8 proteins elicited by the BMPs. The inhibitory effect of heparins has been demonstrated in cells and in mice, where subcutaneous injections of non-anticoagulant heparins inhibited liver hepcidin expression and increased iron bioavailability. The chemical characteristics for high anti-hepcidin activity in vitro and in vivo include the 2O-and 6O-sulfation and a molecular weight above 7 kDa. The most potent heparins have been found to be the super-sulfated ones, active in hepcidin suppression with a molecular weight as low as 4 kDa. Moreover, the alteration of endogenous heparan sulfates has been found to cause a reduction in hepcidin expression in vitro and in vivo, indicating that heparins act by interfering with the interaction between BMPs and components of the complex involved in the activation of the BMP/SMAD1/5/8 pathway. This review summarizes recent findings on the anti-hepcidin activity of heparins and their possible use for the treatment of anemia caused by hepcidin excess, including the anemia of chronic diseases.

Published

2017

23. Qualification of HSQC methods for quantitative composition of heparin and low molecular weight heparins.

Author

Mauri L, Boccardi G, Torri G, Karfunkle M, Macchi E, Muzi L, Keire D, and Guerrini M

Subjects

Limit of Detection, Molecular Structure, Molecular Weight, Reproducibility of Results, Disaccharides analysis, Heparin analysis, Heparin, Low-Molecular-Weight analysis, Monosaccharides analysis, Nuclear Magnetic Resonance, Biomolecular methods

Abstract

An NMR HSQC method has recently been proposed for the quantitative determination of the mono- and disaccharide subunits of heparin and low molecular weight heparins (LMWH). The focus of the current study was the validation of this procedure to make the 2D-NMR method suitable for pharmaceutical quality control applications. Pre-validation work investigated the effects of several experimental parameters to assess robustness and to optimize critical factors. Important experimental parameters were pulse sequence selection, equilibration interval between pulse trains and temperature. These observations were needed so that the NMR method was sufficiently understood to enable continuous improvement. A standard validation study on heparin then examined linearity, repeatability, intermediate precision and limits of detection and quantitation; selected validation parameters were also determined for LMWH., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2017

24. Structural features of heparanase-inhibiting non-anticoagulant heparin derivative Roneparstat.

Author

Alekseeva A, Mazzini G, Giannini G, and Naggi A

Subjects

Enzyme Inhibitors chemistry, Enzyme Inhibitors pharmacology, Molecular Structure, Oxidation-Reduction, Glucuronidase antagonists & inhibitors, Heparin chemistry, Heparin pharmacology

Abstract

Owing to their anti-tumor and anti-inflammatory properties, non-anticoagulant glycol-split (gs) heparins, obtained by periodate oxidation/borohydride reduction, are of growing interest. The present study was focused on the structural characterization of N-acetylated gs-heparin Roneparstat, a promising anti-cancer heparanase-inhibiting drug currently being investigated in clinical trials. The major and minor structural features of structurally complex Roneparstat have been characterized for the first time using conductimetric titration, size-exclusion chromatography with triple detector array, NMR and LC/MS. It has been shown that gs-uronic acids are mainly interspersed by unmodified disaccharide building blocks, but can also be present within sequences with consequent gs-residues. Peculiar gs-sequences, such as those derived from antithrombin binding regions and those containing I 2S -A NS3S6S , as well as a variety of unnatural terminal groups, markers of preparation processes, have also been identified in Roneparstat. Structural features of Roneparstat that may play an important role in interactions with proteins have been summarized., (Copyright © 2016 Elsevier Ltd. All rights reserved.)

Published

2017

25. Investigating Glycol-Split-Heparin-Derived Inhibitors of Heparanase: A Study of Synthetic Trisaccharides.

Author

Ni M, Elli S, Naggi A, Guerrini M, Torri G, and Petitou M

Subjects

Carbohydrate Sequence, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors chemistry, Enzyme Inhibitors pharmacology, Models, Molecular, Structure-Activity Relationship, Trisaccharides chemistry, Glucuronidase antagonists & inhibitors, Glycols chemistry, Heparin chemistry, Trisaccharides chemical synthesis, Trisaccharides pharmacology

Abstract

Heparanase is the only known endoglycosidase able to cleave heparan sulfate. Roneparstat and necuparanib, heparanase inhibitors obtained from heparin and currently being tested in man as a potential drugs against cancer, contain in their structure glycol-split uronic acid moieties probably responsible for their strong inhibitory activity. We describe here the total chemical synthesis of the trisaccharide GlcNS6S-GlcA-1,6anGlcNS ( 1 ) and its glycol-split (gs) counterpart GlcNS6S-gsGlcA-1,6anGlcNS ( 2 ) from glucose. As expected, in a heparanase inhibition assay, compound 2 is one order of magnitude more potent than 1 . Using molecular modeling techniques we have created a 3D model of 1 and 2 that has been validated by NOESY NMR experiments. The pure synthetic oligosaccharides have allowed the first in depth study of the conformation of a glycol-split glucuronic acid. Introducing a glycol-split unit in the structure of 1 increases the conformational flexibility and shortens the distance between the two glucosamine motives, thus promoting interaction with heparanase. However, comparing the relative activities of 2 and roneparstat, we can conclude that the glycol-split motive is not the only determinant of the strong inhibitory effect of roneparstat.

Published

2016

26. Old and new applications of non-anticoagulant heparin.

Author

Cassinelli G and Naggi A

Subjects

Anti-Inflammatory Agents pharmacology, Anti-Inflammatory Agents therapeutic use, Antimalarials pharmacology, Antimalarials therapeutic use, Antineoplastic Agents pharmacology, Antineoplastic Agents therapeutic use, Clinical Trials as Topic, Drug Repositioning, Heparin chemistry, Heparin, Low-Molecular-Weight pharmacology, Heparin, Low-Molecular-Weight therapeutic use, Humans, Signal Transduction drug effects, Heparin pharmacology, Heparin therapeutic use

Abstract

The aim of this chapter is to provide an overview of non-anticoagulant effects of heparins and their potential use in new therapeutic applications. Heparin and heparin derivatives have been tested in inflammatory, pulmonary and reproductive diseases, in cardiovascular, nephro- and neuro-tissue protection and repair, but also as agents against angiogenesis, atheroschlerosis, metastasis, protozoa and viruses. Targeting and inhibition of specific mediators involved in the inflammatory process, promoting some of the above mentioned pathologies, are reported along with recent studies of heparin conjugates and oral delivery systems. Some reports from the institute of the authors, such as those devoted to glycol-split heparins are also included. Among the members and derivatives of this class, several are undergoing clinical trials as antimetastatic and antimalarial agents and for the treatment of labour pain and severe hereditary anaemia. Other heparins, whose therapeutic targets are non-anticoagulant such as nephropathies, retinopathies and cystic fibrosis are also under investigation., (© 2016 Elsevier Ireland Ltd.)

Published

2016

27. Structural peculiarity and antithrombin binding region profile of mucosal bovine and porcine heparins.

Author

Naggi A, Gardini C, Pedrinola G, Mauri L, Urso E, Alekseeva A, Casu B, Cassinelli G, Guerrini M, Iacomini M, Baigorria V, and Torri G

Subjects

Animals, Binding Sites physiology, Cattle, Chromatography, High Pressure Liquid methods, Magnetic Resonance Spectroscopy methods, Swine, Antithrombins chemistry, Antithrombins metabolism, Heparin chemistry, Heparin metabolism, Intestinal Mucosa metabolism

Abstract

The major compositional differences between bovine mucosal heparin (BMH) and the currently employed porcine mucosal heparin (PMH) have been reported to essentially consist of reduced 6-O-sulfation of the glucosamine residues in BMH and somewhat lower 2-O-sulfation of the iduronate residues in PMH. The present work is based on direct comparison of several BMH and PMH commercial preparations. A combined study by 2D (heteronuclear single quantum coherence, HSQC) NMR and ion-pair reversed-phase high performance liquid chromatography (IPRP-HPLC) coupled with electrospray ionization mass spectrometry (ESI-MS) on the heparins, extended to the analysis of their heparinases digests and fractions separated by affinity chromatography on antithrombin (AT), confirmed the previously reported lower degree of 6-O-sulfation and showed lower 3-O-sulfated glucosamine content in BMH. More detailed studies allowed the identification of structural variants of AT-binding region (ATBR) structural variants, showing higher content of the N-sulfated components in BMH than in PMH., (Copyright © 2015 Elsevier B.V. All rights reserved.)

Published

2016

28. Determination of the molecular weight of low-molecular-weight heparins by using high-pressure size exclusion chromatography on line with a triple detector array and conventional methods.

Author

Bisio A, Mantegazza A, Vecchietti D, Bensi D, Coppa A, Torri G, and Bertini S

Subjects

Chromatography, Gel standards, Dynamic Light Scattering, Heparin, Low-Molecular-Weight chemistry, Molecular Weight, Refractometry, Scattering, Radiation, Chromatography, Gel methods, Heparin chemistry

Abstract

The evaluation of weight average molecular weight (Mw) and molecular weight distribution represents one of the most controversial aspects concerning the characterization of low molecular weight heparins (LMWHs). As the most commonly used method for the measurement of such parameters is high performance size exclusion chromatography (HP-SEC), the soundness of results mainly depends on the appropriate calibration of the chromatographic columns used. With the aim of meeting the requirement of proper Mw standards for LMWHs, in the present work the determination of molecular weight parameters (Mw and Mn) by HP-SEC combined with a triple detector array (TDA) was performed. The HP-SEC/TDA technique permits the evaluation of polymeric samples by exploiting the combined and simultaneous action of three on-line detectors: light scattering detectors (LALLS/RALLS); refractometer and viscometer. Three commercial LMWH samples, enoxaparin, tinzaparin and dalteparin, a γ-ray depolymerized heparin (γ-Hep) and its chromatographic fractions, and a synthetic pentasaccharide were analysed by HP-SEC/TDA. The same samples were analysed also with a conventional HP-SEC method employing refractive index (RI) and UV detectors and two different chromatographic column set, silica gel and polymeric gel columns. In both chromatographic systems, two different calibration curves were built up by using (i) γ-Hep chromatographic fractions and the corresponding Mw parameters obtained via HP-SEC/TDA; (ii) the whole γ-Hep preparation with broad Mw dispersion and the corresponding cumulative distribution function calculated via HP-SEC/TDA. In addition, also a chromatographic column calibration according to European Pharmacopoeia indication was built up. By comparing all the obtained results, some important differences among Mw and size distribution values of the three LMWHs were found with the five different calibration methods and with HP-SEC/TDA method. In particular, the detection of the lower molecular weight components turned out to be the most critical aspect. Whereas HP-SEC/TDA may underestimate species under 2 KDa when present in low concentration, other methods appeared to emphasize their content.

Published

2015

29. Heparin derivatives for the targeting of multiple activities in the inflammatory response.

Author

Veraldi N, Hughes AJ, Rudd TR, Thomas HB, Edwards SW, Hadfield L, Skidmore MA, Siligardi G, Cosentino C, Shute JK, Naggi A, and Yates EA

Subjects

Anticoagulants chemical synthesis, Anticoagulants chemistry, Dose-Response Relationship, Drug, Enzyme-Linked Immunosorbent Assay, Heparin chemical synthesis, Heparin chemistry, Humans, Inflammation metabolism, Interleukin-8 analysis, Leukocyte Elastase antagonists & inhibitors, Leukocyte Elastase metabolism, Proteinase Inhibitory Proteins, Secretory chemical synthesis, Proteinase Inhibitory Proteins, Secretory chemistry, Structure-Activity Relationship, Anticoagulants pharmacology, Heparin analogs & derivatives, Heparin pharmacology, Inflammation drug therapy, Proteinase Inhibitory Proteins, Secretory pharmacology

Abstract

An attractive strategy for ameliorating symptoms arising from the multi-faceted processes of excessive and/or continual inflammation would be to identify compounds able to interfere with multiple effectors of inflammation. The well-tolerated pharmaceutical, heparin, is capable of acting through several proteins in the inflammatory cascade, but its use is prevented by strong anticoagulant activity. Derivatives of heparin involving the periodate cleavage of 2,3 vicinal diols in non-sulfated uronate residues (glycol-split) and replacement of N-sulphamido- with N-acetamido- groups in glucosamine residues, capable of inhibiting neutrophil elastase activity in vitro, while exhibiting attenuated anticoagulant properties, have been identified and characterised. These also interact with two other important modulators of the inflammatory response, IL-8 and TNF-alpha. It is therefore feasible in principle to modulate several activities, while minimising anticoagulant side effects, providing a platform from which improved anti-inflammatory agents might be developed., (Copyright © 2014 Elsevier Ltd. All rights reserved.)

Published

2015

30. Re-visiting the structure of heparin.

Author

Casu B, Naggi A, and Torri G

Subjects

Animals, Antithrombins metabolism, Biotechnology, Carbohydrate Conformation, Heparin chemical synthesis, Heparin metabolism, Heparin pharmacology, Humans, Iduronic Acid chemistry, Molecular Weight, Heparin chemistry

Abstract

The sulfated polysaccharide heparin has been used as a life-saving anticoagulant in clinics well before its detailed structure was known. This mini-review is a survey of the evolution in the discovery of the primary and secondary structure of heparin. Highlights in this history include elucidation and synthesis of the specific sequence that binds to antithrombin, the development of low-molecular-weight heparins currently used as antithrombotic drugs, and the most promising start of chemo-enzymatic synthesis. Special emphasis is given to peculiar conformational properties contributing to interaction with proteins that modulate different biological properties., (Copyright © 2014 Elsevier Ltd. All rights reserved.)

Published

2015

31. Oversulfated heparins with low anticoagulant activity are strong and fast inhibitors of hepcidin expression in vitro and in vivo.

Author

Poli M, Asperti M, Ruzzenenti P, Mandelli L, Campostrini N, Martini G, Di Somma M, Maccarinelli F, Girelli D, Naggi A, and Arosio P

Subjects

Animals, Anticoagulants chemistry, Factor Xa metabolism, Factor Xa Inhibitors pharmacology, Hep G2 Cells drug effects, Heparin, Low-Molecular-Weight chemistry, Heparin, Low-Molecular-Weight pharmacology, Hepcidins metabolism, Humans, Liver drug effects, Liver metabolism, Mice, Inbred C57BL, Prothrombin metabolism, Structure-Activity Relationship, Sulfates chemistry, Triglycerides metabolism, Anticoagulants pharmacology, Heparin chemistry, Heparin pharmacology, Hepcidins antagonists & inhibitors

Abstract

Hepcidin is a peptide hormone that controls systemic iron availability and is upregulated by iron and inflammation. Heparins have been shown to be efficient hepcidin inhibitors both in vitro and in vivo, even when their anticoagulant activity has been abolished by chemical reactions of oxidation/reduction (glycol-split). We analyzed a modified heparin type, characterized by a high, almost saturated, sulfation degree and low molecular weight. It inhibited hepcidin expression in hepatic HepG2 cells, and when used in mice, it readily suppressed liver hepcidin mRNA and serum hepcidin, with a significant decrease of spleen iron. This occurred also in inflammation-model, LPS-treated animals, and after heparin chronic 10-day treatments. The heparin had low/absent anticoagulant activity, as tested for factor-Xa and -IIA, APTT and anti Xa. It reduced triglyceride levels in the mice. This heparin acts faster and is more potent than the glycol split-heparins, probably because of its smaller molecular weight and higher sulfation degree. This modified heparin has potential applications for the treatment of diseases with high hepcidin levels., (Copyright © 2014 Elsevier Inc. All rights reserved.)

Published

2014

32. A heparin-like glycosaminoglycan from shrimp containing high levels of 3-O-sulfated D-glucosamine groups in an unusual trisaccharide sequence.

Author

Chavante SF, Brito AS, Lima M, Yates E, Nader H, Guerrini M, Torri G, and Bisio A

Subjects

Animals, Antithrombins isolation & purification, Carbohydrate Conformation, Carbohydrate Sequence, Glucosamine, Heparin isolation & purification, Humans, Molecular Sequence Data, Molecular Weight, Trisaccharides isolation & purification, Antithrombins chemistry, Heparin chemistry, Penaeidae chemistry, Trisaccharides chemistry

Abstract

The detailed characterization of a novel heparin-like glycosaminoglycan purified from the viscera (heads) of the shrimp Litopenaeus vannamei is reported. Structural analysis performed by mono- and two-dimensional nuclear magnetic resonance (NMR) spectroscopy revealed it to be rich in both glucuronic acid and N,6-sulfated glucosamine residues. The key peculiarities were its high 3-O-sulfated glucosamine content compared to mammalian heparins; a residue which is usually associated with the antithrombin (AT) binding site, and the location of these residues within 2-O-sulfated iduronate and glucuronate-containing sequences (I2S-A(∗)-G), a situation not found in mammalian heparin. It also exhibited higher molecular weight (∼36kDa) than conventional heparin (∼16kDa) but, negligible anticoagulant activity (∼5IU/mg compared to heparin ∼190IU/mg) and stabilization of AT, which has been linked directly to anticoagulation activity. A high affinity fraction, eluting at a similar salt concentration (0.75-1.5M NaCl) from an antithrombin affinity column, to the high affinity fraction of heparin, also showed only weak thermal stabilization of AT (+∼2°C). These structural peculiarities may help elucidate more clearly the relationship between structure and function of sulfated polysaccharides, and provide useful model compounds with which to better understand interactions of biological significance., (Copyright © 2014. Published by Elsevier Ltd.)

Published

2014

33. An unusual antithrombin-binding heparin octasaccharide with an additional 3-O-sulfated glucosamine in the active pentasaccharide sequence.

Author

Guerrini M, Elli S, Mourier P, Rudd TR, Gaudesi D, Casu B, Boudier C, Torri G, and Viskov C

Subjects

Antithrombins metabolism, Carbohydrate Sequence, Glucosamine metabolism, Heparin metabolism, Kinetics, Magnetic Resonance Spectroscopy, Models, Molecular, Molecular Conformation, Molecular Sequence Data, Molecular Structure, Oligosaccharides metabolism, Protein Binding, Protein Conformation, Sulfates chemistry, Sulfates metabolism, Temperature, Antithrombins chemistry, Glucosamine chemistry, Heparin chemistry, Oligosaccharides chemistry

Abstract

The 3-O-sulfation of N-sulfated glucosamine is the last event in the biosynthesis of heparin/heparan sulfate, giving rise to the antithrombin-binding pentasaccharide sequence AGA*IA, which is largely associated with the antithrombotic activity of these molecules. The aim of the present study was the structural and biochemical characterization of a previously unreported AGA*IA*-containing octasaccharide isolated from the very-low-molecular-mass heparin semuloparin, in which both glucosamine residues of the pentasaccharide moiety located at the non-reducing end bear 3-O-sulfate groups. Two-dimensional and STD (saturation transfer difference) NMR experiments clearly confirmed its structure and identified its ligand epitope binding to antithrombin. The molecular conformation of the octasaccharide-antithrombin complex has been determined by NMR experiments and docking/energy minimization. The presence of the second 3-O-sulfated glucosamine in the octasaccharide induced more than one order of magnitude increase in affinity to antithrombin compared to the pentasaccharide AGA*IA.

Published

2013

34. How to find a needle (or anything else) in a haystack: two-dimensional correlation spectroscopy-filtering with iterative random sampling applied to pharmaceutical heparin.

Author

Rudd TR, Macchi E, Gardini C, Muzi L, Guerrini M, Yates EA, and Torri G

Subjects

Animals, Biosimilar Pharmaceuticals chemistry, Cattle, Drug Contamination, Mucous Membrane metabolism, Swine, Heparin chemistry, Nuclear Magnetic Resonance, Biomolecular

Abstract

Risks of contamination of the major clinical anticoagulant heparin can arise from deliberate adulteration with unnatural or natural polysaccharides, including heparin from other animal sources, other natural products, or artifacts of manufacture, and these can escape detection by conventional means. Currently, there is no generally applicable, objective test recommended by regulators that can detect these in pharmaceutical heparin, and this continues to leave heparin exposed to contamination risks. Two-dimensional correlation spectroscopic-filtering with iterative random sampling (2D-COS-firs) is reported. It employs a difference covariance matrix with iterative random sampling, and is capable of revealing contamination in pharmaceutical heparin to a high level of sensitivity irrespective of the nature of those features. The technique is suitable to any situation in which a comparison of a single entity to a family of heterogeneous entities, particularly natural products and biosimilars, needs to be made, and will find application in pharmaceutical monitoring, manufacturing quality control, materials science, biotechnology, and metabolomic investigations.

Published

2012

35. High-sensitivity visualisation of contaminants in heparin samples by spectral filtering of 1H NMR spectra.

Author

Rudd TR, Gaudesi D, Lima MA, Skidmore MA, Mulloy B, Torri G, Nader HB, Guerrini M, and Yates EA

Subjects

Chondroitin Sulfates chemistry, Dermatan Sulfate chemistry, Magnetic Resonance Spectroscopy instrumentation, Heparin chemistry, Magnetic Resonance Spectroscopy methods

Abstract

A novel application of two-dimensional correlation analysis has been employed to filter (1)H NMR heparin spectra distinguishing acceptable natural variation and the presence of foreign species. Analysis of contaminated heparin samples, compared to a dataset of accepted heparin samples using two-dimensional correlation spectroscopic analysis of their 1-dimensional (1)H NMR spectra, allowed the spectral features of contaminants to be recovered with high sensitivity, without having to resort to more complicated NMR experiments. Contaminants, which exhibited features distinct from those of heparin and those with features normally hidden within the spectral mass of heparin could be distinguished readily. A heparin sample which had been pre-mixed with a known contaminant, oversulfated chondroitin sulfate (OSCS), was tested against the heparin reference library. It was possible to recover the (1)H NMR spectrum of the OSCS component through difference 2D-COS power spectrum analysis of as little as 0.25% (w/w) with ease, and of 2% (w/w) for more challenging contaminants, whose NMR signals fell under those of heparin. The approach shows great promise for the quality control of heparin and provides the basis for greatly improved regulatory control for the analysis of heparin, as well as other intrinsically heterogeneous and varied products., (© The Royal Society of Chemistry 2011)

Published

2011

36. Construction and use of a library of bona fide heparins employing 1H NMR and multivariate analysis.

Author

Rudd TR, Gaudesi D, Skidmore MA, Ferro M, Guerrini M, Mulloy B, Torri G, and Yates EA

Subjects

Chondroitin Sulfates chemistry, Multivariate Analysis, Oxidation-Reduction, Principal Component Analysis, Small Molecule Libraries chemistry, Heparin chemistry, Magnetic Resonance Spectroscopy methods

Abstract

In contrast to most pharmaceutical agents, the major anticoagulant agent, heparin, lacks a uniquely defined chemical structure. It is an inherently structurally varying, poly-disperse polymer, rendering quality control problematic. Structural modifications introduced during manufacture and the presence of possible contaminants are dangers. The comparison of any heparin test sample to a library of bona fide, but intrinsically variable heparins, is limited fundamentally to measuring the degree of similarity between them. A general approach for constructing a suitable illustrative heparin library employing (1)H NMR and multivariate analysis, is proposed and examples shown. Heparin samples contaminated with non-N-acetylated, persulfated, non-glycosaminoglycan carbohydrates (10%) were detected, some of which would not be easily detected under current regulatory guidelines. The ability to identify contaminated heparin is fundamentally dependent on the contents of the library, which should contain all the 'normal' variability within 'heparin'. Oversulfated chondroitin sulfate can be detected (∼5%) (using components 1 and 2, but is detectable at 3% using additional components, e.g. 1 and 5) analysing the full spectrum and at <1% if only the N-acetyl region is used. Signals arising from oxidation during the manufacturing processes can also be found. The design, properties and limitations of this approach are discussed. Assembly of such a library of market heparin can be termed the 'Current Statistical Definition of Heparin' (CSDH) and will form the basis of future quantitative methods., (© The Royal Society of Chemistry 2011)

Published

2011

37. Heparin-derived heparan sulfate mimics to modulate heparan sulfate-protein interaction in inflammation and cancer.

Author

Casu B, Naggi A, and Torri G

Subjects

Animals, Anticoagulants metabolism, Antimicrobial Cationic Peptides metabolism, Blood Proteins metabolism, Carrier Proteins metabolism, Extracellular Matrix metabolism, Fibroblast Growth Factor 1 metabolism, Fibroblast Growth Factor 2 metabolism, Glucuronidase metabolism, Heparan Sulfate Proteoglycans metabolism, Heparin chemistry, Heparitin Sulfate chemistry, Humans, Interleukin-8 metabolism, Models, Molecular, Oligosaccharides metabolism, Polysaccharides metabolism, Heparin metabolism, Heparitin Sulfate metabolism, Inflammation metabolism, Neoplasms metabolism, Proteins metabolism

Abstract

The heparan sulfate (HS) chains of heparan sulfate proteoglycans (HSPG) are "ubiquitous" components of the cell surface and the extracellular matrix (EC) and play important roles in the physiopathology of developmental and homeostatic processes. Most biological properties of HS are mediated by interactions with "heparin-binding proteins" and can be modulated by exogenous heparin species (unmodified heparin, low molecular weight heparins, shorter heparin oligosaccharides and various non-anticoagulant derivatives of different sizes). Heparin species can promote or inhibit HS activities to different extents depending, among other factors, on how closely their structure mimics the biologically active HS sequences. Heparin shares structural similarities with HS, but is richer in "fully sulfated" sequences (S domains) that are usually the strongest binders to heparin/HS-binding proteins. On the other hand, HS is usually richer in less sulfated, N-acetylated sequences (NA domains). Some of the functions of HS chains, such as that of activating proteins by favoring their dimerization, often require short S sequences separated by rather long NA sequences. The biological activities of these species cannot be simulated by heparin, unless this polysaccharide is appropriately chemically/enzymatically modified or biotechnologically engineered. This mini review covers some information and concepts concerning the interactions of HS chains with heparin-binding proteins and some of the approaches for modulating HS interactions relevant to inflammation and cancer. This is approached through a few illustrative examples, including the interaction of HS and heparin-derived species with the chemokine IL-8, the growth factors FGF1 and FGF2, and the modulation of the activity of the enzyme heparanase by these species. Progresses in sequencing HS chains and reproducing them either by chemical synthesis or semi-synthesis, and in the elucidation of the 3D structure of oligosaccharide-protein complexes, are paving the way for rational approaches to the development of HS-inspired drugs in the field of inflammation and cancer, as well in other therapeutic fields., (Copyright © 2010 International Society of Matrix Biology. Published by Elsevier B.V. All rights reserved.)

Published

2010

38. Orthogonal analytical approaches to detect potential contaminants in heparin.

Author

Guerrini M, Zhang Z, Shriver Z, Naggi A, Masuko S, Langer R, Casu B, Linhardt RJ, Torri G, and Sasisekharan R

Subjects

Animals, Anticoagulants chemistry, Cattle, Chondroitin Sulfates chemistry, Drug Contamination prevention & control, Humans, Reproducibility of Results, Swine, Chondroitin Sulfates isolation & purification, Electrophoresis, Capillary methods, Heparin chemistry, Magnetic Resonance Spectroscopy methods

Abstract

Heparin is a widely used anticoagulant and antithrombotic agent. Recently, a contaminant, oversulfated chondroitin sulfate (OSCS), was discovered within heparin preparations. The presence of OSCS within heparin likely led to clinical manifestations, most prevalently, hypotension and abdominal pain leading to the deaths of several dozens of patients. Given the biological effects of OSCS, one continuing item of concern is the ability for existing methods to identify other persulfonated polysaccharide compounds that would also have anticoagulant activity and would likely elicit a similar activation of the contact system. To complete a more extensive analysis of the ability for NMR and capillary electrophoresis (CE) to capture a broader array of potential contaminants within heparin, we completed a systematic study of NMR, both mono- and bidimensional, and CE to detect both various components of sidestream heparin and their persulfonated derivatives. We show that given the complexity of heparin samples, and the requirement to ensure their purity and safety, use of orthogonal analytical techniques is effective at detecting an array of potential contaminants that could be present.

Published

2009

39. Minimum FGF2 binding structural requirements of heparin and heparan sulfate oligosaccharides as determined by NMR spectroscopy.

Author

Guglier S, Hricovíni M, Raman R, Polito L, Torri G, Casu B, Sasisekharan R, and Guerrini M

Subjects

Fibroblast Growth Factor 2 metabolism, Heparin metabolism, Heparitin Sulfate metabolism, Magnetic Resonance Spectroscopy, Molecular Structure, Oligosaccharides metabolism, Protein Binding, Structure-Activity Relationship, Fibroblast Growth Factor 2 chemistry, Heparin chemistry, Heparitin Sulfate chemistry, Oligosaccharides chemistry

Abstract

Heparin and heparan sulfate (HS) glycosaminoglycans (HSGAGs) are sulfated polysaccharidesthat play important roles in fundamental biological processes by binding to proteins. The prototypic exampleof HSGAG-protein interactions is that with the fibroblast growth factors (FGFs), specifically FGF1 andFGF2. Structural and biochemical studies have shown that the chain length, sulfation pattern, andconformation of HSGAGs play a critical role in FGF binding and activity. Previously, we showed that atetrasaccharide of the form ANS,6X-I2S-ANS,6X-I2S-OPr (where X is OH or O-sulfate and Pr is propyl) withat least one of the ANS,6X residues having a 6-O sulfate group was the minimum binding motif for FGF1[Guerrini, M., Agulles, T., Bisio, A., Hricovini, M., Lay, L., Naggi, A., Poletti, L., Sturiale, L., Torri, G.,and Casu, B. (2002) Biochem. Biophys. Res. Commun. 292, 222-230]. We report NMR structural analysisusing two-dimensional NOE spectroscopy (2D-NOESY) and transferred NOESY (trNOESY) on a non-6-O-sulfated synthetic tetrasaccharide TETRA (ANS-I2S-ANS-I2S-OPr) both in its free state and bound toFGF2. This tetrasaccharide comprises both the structural trisaccharide motif ANS-I2S-ANS that forms "kinks"in longer heparin chains induced by FGF binding [Raman, R., Venkataraman, G., Ernst, S., Sasisekharan,V., and Sasisekharan, R. (2003) Proc. Natl. Acad. Sci. U.S.A. 100, 2357-2362] and the common bindingmotif I2S-ANS-I2S present in octasaccharides that exhibited strong FGF2 binding [Kreuger, J., Salmivirta,M., Sturiale, L., Gimenez-Gallego, G., and Lindahl, U. (2001) J. Biol. Chem. 276, 30744-30752]. Thesedata suggest that TETRA could be the shortest HSGAG oligosaccharide that binds to FGF2. Furthermore,our study confirms that both the IdoA residues in TETRA adopt the chair 1C4 conformation upon FGF2binding to provide the best molecular fit in contrast to an analogous 6-O-sulfated tetrasaccharide motifobserved in the FGF2-HSGAG cocrystal structure where one of the IdoAs adopts skew-boat 2SOconformation. Thus, our study highlights the fact that the conformational plurality of IdoA is able toaccommodate the changes in the sulfation pattern to provide the necessary specificity for protein binding.

Published

2008

40. Oversulfated chondroitin sulfate is a contaminant in heparin associated with adverse clinical events.

Author

Guerrini M, Beccati D, Shriver Z, Naggi A, Viswanathan K, Bisio A, Capila I, Lansing JC, Guglieri S, Fraser B, Al-Hakim A, Gunay NS, Zhang Z, Robinson L, Buhse L, Nasr M, Woodcock J, Langer R, Venkataraman G, Linhardt RJ, Casu B, Torri G, and Sasisekharan R

Subjects

Drug Evaluation, Preclinical, Humans, Chondroitin Sulfates analysis, Chondroitin Sulfates chemistry, Drug Contamination prevention & control, Drug-Related Side Effects and Adverse Reactions, Heparin analysis, Heparin chemistry

Abstract

Recently, certain lots of heparin have been associated with an acute, rapid onset of serious side effects indicative of an allergic-type reaction. To identify potential causes for this sudden rise in side effects, we examined lots of heparin that correlated with adverse events using orthogonal high-resolution analytical techniques. Through detailed structural analysis, the contaminant was found to contain a disaccharide repeat unit of glucuronic acid linked beta1-->3 to a beta-N-acetylgalactosamine. The disaccharide unit has an unusual sulfation pattern and is sulfated at the 2-O and 3-O positions of the glucuronic acid as well as at the 4-O and 6-O positions of the galactosamine. Given the nature of this contaminant, traditional screening tests cannot differentiate between affected and unaffected lots. Our analysis suggests effective screening methods that can be used to determine whether or not heparin lots contain the contaminant reported here.

Published

2008

41. High-performance liquid chromatographic/mass spectrometric studies on the susceptibility of heparin species to cleavage by heparanase.

Author

Bisio A, Mantegazza A, Urso E, Naggi A, Torri G, Viskov C, and Casu B

Subjects

Binding Sites, Carbohydrate Sequence, Chromatography, High Pressure Liquid standards, Reference Standards, Antithrombins chemistry, Glucuronidase chemistry, Heparin chemistry, Heparitin Sulfate chemistry, Oligosaccharides chemistry, Spectrometry, Mass, Electrospray Ionization standards

Abstract

Heparanase is an endo-beta-D-glucuronidase that cleaves the heparan sulfate chains of heparan sulfate proteoglycans and is implicated in angiogenesis and metastasis. With the aim of establishing a simple and reliable method for studying the susceptibility of heparin/heparan sulfate oligosaccharides to be cleaved by heparanase, an on-line ion pair reversed-phase high-performance liquid chromatographic/electrospray ionization mass spectrometric method was set up. The method works in the micromolar range of concentration and does not require derivatization of the substrate or of the products. It is based on mass identification of oligosaccharide fragments generated by heparanase and their quantification with reference to an internal heparin disaccharide standard. Substrates were (1) the synthetic pentasaccharides GlcN (NS,6S) - GlcA - GlcN (NS,3S,6S) - IdoA (2S) - GlcN (NS,6S) - OMe (AGA*IA (M)) and GlcN (NS,6S) - GlcA - GlcN (NS,6S) - IdoA (2S) - GlcN (NS,6S) - OMe (AGAIA (M)), corresponding to the heparin/heparan sulfate active site for antithrombin, and to the same sequence devoid of the 3- O-sulfate group in the central glucosamine, respectively; and (2) two natural heparin octasaccharides containing the AGA*IA sequence in different locations along the chain. The two pentasaccharides exhibited a higher susceptibility to heparanase cleavage with respect to the octasaccharides. The commercial availability of AGA*IA (M) makes it an ideal substrate to determine the specific activity of heparanase preparations. The present method could also be used for rapid screening of potential heparanase inhibitors.

Published

2007

42. Interaction of heparins with fibroblast growth factors: conformational aspects.

Author

Guerrini M, Hricovíni M, and Torri G

Subjects

Angiogenesis Inhibitors pharmacology, Animals, Carbohydrate Conformation, Heparin metabolism, Heparin pharmacology, Heparitin Sulfate metabolism, Heparitin Sulfate pharmacology, Humans, Magnetic Resonance Spectroscopy, Fibroblast Growth Factors metabolism, Heparin chemistry, Heparitin Sulfate chemistry

Abstract

Heparin and heparin-like oligo- and polysaccharides bind to fibroblast growth factors (FGFs) and modulate their ability to form active ternary complexes with FGF receptors (FGFRs). Considerable efforts have been made in recent years to identify the minimal heparin and heparan sulfate (HS) sequences that bind and activate individual FGFs. Heparin sequences involved in interaction with FGFs invariably contain at least one residue of 2-O-sulfated iduronic acid (IdoA2S), which adopts either the (1)(4) chair conformation or the equi-energetic skew-boat (2)S(0). In solution and in the absence of a binding protein, both these conformations are present in a dynamic equilibrium. In oligosaccharide-protein co-crystals, the protein selects those conformers that provide optimal contacts. The crystalline structure of a heparin hexasaccharide/FGF complex exhibits one of the two IdoA2S residues in the active site of the growth factor in (1)C(4) conformation and the other (outside the active site) in (2)S(0) conformation. NMR studies suggest that active conformations of heparin/HS oligosaccharides in solution could be distinct from those adopted in crystals. Heparin tetrasaccharides in the presence of FGF1 and FGF2 have both their IdoA2S residues prevalently in the (1)C(4) form. Current NMR and molecular modelling studies are being extended to longer heparin oligosaccharides as well as to heparins with "glycol-split" residues along their chains.

Published

2007

43. Conformational transitions induced in heparin octasaccharides by binding with antithrombin III.

Author

Guerrini M, Guglieri S, Beccati D, Torri G, Viskov C, and Mourier P

Subjects

Antithrombin III analysis, Antithrombin III chemistry, Carbohydrate Conformation, Heparin analysis, Humans, Iduronic Acid chemistry, Models, Molecular, Nuclear Magnetic Resonance, Biomolecular, Oligosaccharides analysis, Protein Binding, Antithrombin III metabolism, Heparin chemistry, Heparin metabolism, Oligosaccharides chemistry, Oligosaccharides metabolism

Abstract

The present study deals with the conformation in solution of two heparin octasaccharides containing the pentasaccharide sequence GlcN(NAc,6S)-GlcA-GlcN(NS,3,6S)-IdoA(2S)-GlcN(NS,6S) [AGA*IA; where GlcN(NAc,6S) is N-acetylated, 6-O-sulfated alpha-D-glucosamine, GlcN(NS,3,6S) is N,3,6-O-trisulfated alpha-D-glucosamine and IdoA(2S) is 2-O-sulfated IdoA (alpha-L-iduronic acid)] located at different positions in the heparin chain and focuses on establishing geometries of IdoA residues (IdoA(2S) and IdoA) both inside and outside the AGA*IA sequence. AGA*IA constitutes the active site for AT (antithrombin) and is essential for the expression of high anticoagulant and antithrombotic activities. Analysis of NMR parameters [NOEs (nuclear Overhauser effects), transferred NOEs and coupling constants] for the two octasaccharides indicated that between the 1C4 and 2S0 conformations present in dynamic equilibrium in the free state for the IdoA(2S) residue within AGA*IA, AT selects the 2S0 form, as previously shown [Hricovini, Guerrini, Bisio, Torri, Petitou and Casu (2001) Biochem. J. 359, 265-272]. Notably, the 2S0 conformation is also adopted by the non-sulfated IdoA residue preceding AGA*IA that, in the absence of AT, adopts predominantly the 1C4 form. These results further support the concept that heparin-binding proteins influence the conformational equilibrium of iduronic acid residues that are directly or indirectly involved in binding and select one of their equi-energetic conformations for best fitting in the complex. The complete reversal of an iduronic acid conformation preferred in the free state is also demonstrated for the first time. Preliminary docking studies provided information on the octasaccharide binding location agreeing most closely with the experimental data. These results suggest a possible biological role for the non-sulfated IdoA residue preceding AGA*IA, previously thought not to influence the AT-binding properties of the pentasaccharide. Thus, for each AT binding sequence longer than AGA*IA, the interactions with the protein could differ and give to each heparin fragment a specific biological response.

Published

2006

44. Modulation of the heparanase-inhibiting activity of heparin through selective desulfation, graded N-acetylation, and glycol splitting.

Author

Naggi A, Casu B, Perez M, Torri G, Cassinelli G, Penco S, Pisano C, Giannini G, Ishai-Michaeli R, and Vlodavsky I

Subjects

Acetylation, Animals, CHO Cells, Carbohydrate Sequence, Cattle, Cells, Cultured, Cornea cytology, Cricetinae, Disaccharides chemistry, Dose-Response Relationship, Drug, Endothelium, Vascular cytology, Fibroblast Growth Factor 2 metabolism, Glucuronic Acid chemistry, Glucuronidase chemistry, Heparin chemistry, Humans, Inhibitory Concentration 50, Kinetics, Magnetic Resonance Spectroscopy, Molecular Sequence Data, Protein Structure, Tertiary, Recombinant Proteins chemistry, Uronic Acids chemistry, Glucuronidase antagonists & inhibitors, Glucuronidase metabolism, Glycols chemistry, Heparin metabolism

Abstract

Heparanase is an endo-beta-glucuronidase that cleaves heparan sulfate (HS) chains of heparan sulfate proteoglycans on cell surfaces and in the extracellular matrix (ECM). Heparanase, overexpressed by most cancer cells, facilitates extravasation of blood-borne tumor cells and causes release of growth factors sequestered by HS chains, thus accelerating tumor growth and metastasis. Inhibition of heparanase with HS mimics is a promising target for a novel strategy in cancer therapy. In this study, in vitro inhibition of recombinant heparanase was determined for heparin derivatives differing in degrees of 2-O- and 6-O-sulfation, N-acetylation, and glycol splitting of nonsulfated uronic acid residues. The contemporaneous presence of sulfate groups at O-2 of IdoA and at O-6 of GlcN was found to be non-essential for effective inhibition of heparanase activity provided that one of the two positions retains a high degree of sulfation. N-Desulfation/ N-acetylation involved a marked decrease in the inhibitory activity for degrees of N-acetylation higher than 50%, suggesting that at least one NSO3 group per disaccharide unit is involved in interaction with the enzyme. On the other hand, glycol splitting of preexisting or of both preexisting and chemically generated nonsulfated uronic acids dramatically increased the heparanase-inhibiting activity irrespective of the degree of N-acetylation. Indeed N-acetylated heparins in their glycol-split forms inhibited heparanase as effectively as the corresponding N-sulfated derivatives. Whereas heparin and N-acetylheparins containing unmodified D-glucuronic acid residues inhibited heparanase by acting, at least in part, as substrates, their glycol-split derivatives were no more susceptible to cleavage by heparanase. Glycol-split N-acetylheparins did not release basic fibroblast growth factor from ECM and failed to stimulate its mitogenic activity. The combination of high inhibition of heparanase and low release/potentiation of ECM-bound growth factor indicates that N-acetylated, glycol-split heparins are potential antiangiogenic and antimetastatic agents that are more effective than their counterparts with unmodified backbones.

Published

2005

45. Molecular weight determination of heparin and dermatan sulfate by size exclusion chromatography with a triple detector array.

Author

Bertini S, Bisio A, Torri G, Bensi D, and Terbojevich M

Subjects

Chromatography, Gel instrumentation, Molecular Weight, Sensitivity and Specificity, Chromatography, Gel methods, Dermatan Sulfate chemistry, Heparin chemistry

Abstract

The determination of molecular weight (M) and molecular weight distribution (MD) of heparins by a novel approach, consisting of a high performance size exclusion chromatography (HP-SEC) combined with a triple detector array (TDA) is described. HP-SEC/TDA permits the evaluation of MD of polymeric samples through a combined and simultaneous action of three on-line detectors, right-angle laser light scattering (RALLS), refractometer (RI), and viscometer. The method does not require any chromatographic column calibration, thus overcoming also the difficulty to obtain adequate reference standards. It permits the size determination also of small molecules, even when scattering dissimmetry is not observable. Unfractionated heparins, eight fractions of a size fractionated heparin, and dermatan sulfates were analyzed by HP-SEC/TDA. The M values found for the heparin fractions were used to build up a calibration curve of a conventional HP-SEC system: the results obtained analyzing unfractionated heparin samples with both HP-SEC/TDA and HP-SEC were in excellent agreement, suggesting the possibility to use the TDA data to generate standard samples with known MD and intrinsic viscosity [eta]. Moreover, HP-SEC/TDA can successfully be employed also for the determination of the Mark-Houwink a and k parameters.

Published

2005

46. Undersulfated and glycol-split heparins endowed with antiangiogenic activity.

Author

Casu B, Guerrini M, Guglieri S, Naggi A, Perez M, Torri G, Cassinelli G, Ribatti D, Carminati P, Giannini G, Penco S, Pisano C, Belleri M, Rusnati M, and Presta M

Subjects

Allantois blood supply, Angiogenesis Inhibitors pharmacology, Animals, Cattle, Cell Adhesion drug effects, Cell Division drug effects, Chick Embryo, Chorion blood supply, Endothelium, Vascular cytology, Endothelium, Vascular drug effects, Fibroblast Growth Factor 2 metabolism, Heparin pharmacology, In Vitro Techniques, Models, Molecular, Proteoglycans metabolism, Receptors, Fibroblast Growth Factor metabolism, Structure-Activity Relationship, Uronic Acids chemistry, Angiogenesis Inhibitors chemical synthesis, Fibroblast Growth Factor 2 antagonists & inhibitors, Glycols chemistry, Heparin analogs & derivatives, Heparin chemical synthesis, Sulfonic Acids chemistry

Abstract

Tumor neovascularization (angiogenesis) is regarded as a promising target for anticancer drugs. Heparin binds to fibroblast growth factor-2 (FGF2) and promotes the formation of ternary complexes with endothelial cell surface receptors, inducing an angiogenic response. As a novel strategy to generate antiangiogenic substances exploiting binding to FGF2 while preventing FGF receptor (FGFR) activation, sulfation gaps were generated along the heparin chains by controlled alkali-catalyzed removal of sulfate groups of iduronic acid 2-O-sulfate residues, giving rise to the corresponding epoxide derivatives. A new class of heparin derivatives was then obtained by opening the epoxide rings followed by oxidative glycol-splitting of the newly formed (and the preexisting) nonsulfated uronic acid residues. In vitro these heparin derivatives prevent the formation of FGFR/FGF2/heparan sulfate proteoglycan ternary complexes and inhibit FGF2-stimulated endothelial cell proliferation. They exert an antiangiogenic activity in the chick embryo chorioallantoic membrane assay, where the parent heparin is inactive. Low and very low molecular weight derivatives of a prototype compound, as well as its glycine and taurine derivatives obtained by reductive amination of glycol-split residues, retained the angiostatic activity. A significant relationship was found between the extent of glycol-splitting and the FGF2-antagonist/angiostatic activities of these heparin derivatives. Molecular dynamics calculations support the assumption that glycol-split residues act as flexible joints that, while favoring 1:1 binding to FGF2, disrupt the linearity of heparin chains necessary for formation of active complexes with FGFRs.

Published

2004

47. A novel computational approach to integrate NMR spectroscopy and capillary electrophoresis for structure assignment of heparin and heparan sulfate oligosaccharides.

Author

Guerrini M, Raman R, Venkataraman G, Torri G, Sasisekharan R, and Casu B

Subjects

Carbohydrate Conformation, Carbohydrate Sequence, Electrophoresis, Capillary methods, Heparin chemistry, Heparitin Sulfate chemistry, Magnetic Resonance Spectroscopy methods

Abstract

Heparin and heparan sulfate (HS) glycosaminoglycans (GAGs) are cell surface polysaccharides that bind to a multitude of signaling molecules, enzymes, and pathogens and modulate critical biological processes ranging from cell growth and development to anticoagulation and viral invasion. Heparin has been widely used as an anticoagulant in a variety of clinical applications for several decades. The heterogeneity and complexity of HS GAGs pose significant challenges to their purification and characterization of structure-function relationships. Nuclear magnetic resonance (NMR) spectroscopy is a promising tool that provides abundant sequence and structure information for characterization of HS GAGs. However, complex NMR spectra and low sensitivity often make analysis of HS GAGs a daunting task. We report the development of a novel methodology that incorporates distinct linkage information between adjacent monosaccharides obtained from NMR and capillary electrophoresis (CE) data using a property encoded nomenclature (PEN) computational framework to facilitate a rapid and unbiased procedure for sequencing HS GAG oligosaccharides. We demonstrate that the integration of NMR and CE data sets with the help of the PEN framework dramatically reduces the number of experimental constraints required to arrive at an HS GAG oligosaccharide sequence.

Published

2002

48. Short heparin sequences spaced by glycol-split uronate residues are antagonists of fibroblast growth factor 2 and angiogenesis inhibitors.

Author

Casu B, Guerrini M, Naggi A, Perez M, Torri G, Ribatti D, Carminati P, Giannini G, Penco S, Pisano C, Belleri M, Rusnati M, and Presta M

Subjects

Allantois blood supply, Allantois physiology, Angiogenesis Inhibitors physiology, Animals, CHO Cells, Carbohydrate Conformation, Carbohydrate Sequence, Cattle, Cell Line, Chick Embryo, Chorion blood supply, Chorion physiology, Cricetinae, Endothelium, Vascular cytology, Endothelium, Vascular physiology, Fetus, Fibroblast Growth Factor 2 physiology, Glycosaminoglycans chemistry, Growth Inhibitors physiology, Humans, Molecular Sequence Data, Nuclear Magnetic Resonance, Biomolecular, Swine, Trisaccharides chemistry, Angiogenesis Inhibitors chemistry, Ethylene Glycol chemistry, Fibroblast Growth Factor 2 antagonists & inhibitors, Heparin analogs & derivatives, Heparin chemistry, Iduronic Acid chemistry

Abstract

Fibroblast Growth Factor-2 (FGF2) is a major inducer of neovascularization (angiogenesis). Heparin activates FGF2 by favoring formation of ternary complexes with its cellular receptors (FGFRs). Controlled 2-O-desulfation followed by exhaustive periodate oxidation/borohydride reduction has been used to generate sulfation gaps within the prevalent heparin sequences, building-up arrays of pentasulfated trisaccharides (PST, consisting of a 2-O-sulfated iduronic acid flanked by two N,6-disulfated glucosamines) spaced by reduced, glycol-split uronic acid (sU) residues. The structure of the prevalent sequences of the novel heparin derivative has been confirmed by mono- and two-dimensional NMR analysis. NMR spin-lattice relaxation times (T2) and nuclear Overhauser effects suggest that the sU residues act as flexible joints between the PST sequences and cause a marked distortion of the chain conformation of heparin required for formation of ternary complexes. Since the splitting reaction also occurs at the level of the essential glucuronic acid residue of the active site for antithrombin, the heparin derivative has no anticoagulant activity. However, it fully retains the FGF2-binding ability of the original heparin, as shown by its capacity to protect FGF2 from trypsin cleavage and to prevent the formation of heparan sulfate proteoglycan (HSPG)/FGF2/FGFR1 ternary complexes. However, when compared to heparin it showed a reduced capacity to induce FGF2 dimerization and to favor the interaction of [125I]FGF2 with FGFR1 in HSPG-deficient, FGFR1-transfected CHO cells. Accordingly, it was more effective than heparin in inhibiting the mitogenic activity exerted by FGF2 in cultured endothelial cells. Finally, it inhibited angiogenesis in a chick embrio chorioallantoic membrane (CAM) assay in which heparin is inactive.

Published

2002

49. Minimal heparin/heparan sulfate sequences for binding to fibroblast growth factor-1.

Author

Guerrini M, Agulles T, Bisio A, Hricovini M, Lay L, Naggi A, Poletti L, Sturiale L, Torri G, and Casu B

Subjects

Binding, Competitive, Carbohydrate Sequence, Dimerization, Fibroblast Growth Factor 1 chemistry, Humans, Magnetic Resonance Spectroscopy, Models, Molecular, Molecular Sequence Data, Oligosaccharides chemistry, Oligosaccharides metabolism, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, Surface Plasmon Resonance, Fibroblast Growth Factor 1 metabolism, Heparin chemistry, Heparin metabolism, Heparitin Sulfate chemistry, Heparitin Sulfate metabolism

Abstract

The glycosaminoglycans heparin and heparan sulfate (HS) bind to fibroblast growth factor FGF1 and promote its dimerization, a proposed prerequisite for binding to a cellular receptor and triggering mitogenic signals. The problem of minimal structural requirements for heparin/HS sequences to bind FGF1 was approached by surface plasmon resonance (SPR), NMR spectroscopy, and MALDI mass spectrometry studies using the three synthetic tetrasaccharides GlcNSO(3)6OR-IdoA2SO(3)-GlcNSO(3)6OR'-IdoA2SO(3)OPr (AA, R = R' = SO(3); BA, R = H, R' = SO(3); BB, R = R' = H; Pr, propyl). AA and BA significantly interact with the protein, whereas BB is practically inactive. The NMR spectra show that, whereas the interaction of AA primarily involves the GlcNSO(3)6SO(3)IdoA2SO(3) disaccharide moiety at its nonreducing end, residues at both the nonreducing (NR) and reducing side (R) appear to be involved in the weaker complex of BA. Furthermore, MALDI experiments show that, in addition to 1:1 protein:tetrasaccharide complexes, AA and BA are able to form 2:1 complexes, indicating that heparin/HS-induced dimerization of FGF1 requires only one 6-OSO(3) group per tetrasaccharide., ((C)2002 Elsevier Science (USA).)

Published

2002

50. Generation of anti-factor Xa active, 3-O-sulfated glucosamine-rich sequences by controlled desulfation of oversulfated heparins.

Author

Naggi A, De Cristofano B, Bisio A, Torri G, and Casu B

Subjects

Animals, Anticoagulants chemistry, Anticoagulants pharmacology, Glucosamine chemistry, Heparin pharmacology, Humans, Kinetics, Magnetic Resonance Spectroscopy, Structure-Activity Relationship, Sulfates chemistry, Sulfates pharmacology, Anticoagulants chemical synthesis, Factor Xa Inhibitors, Glucosamine analogs & derivatives, Glucosamine chemical synthesis, Heparin chemistry

Abstract

In the framework of a project aimed at generating heparin-like sulfation patterns and biological activities in biotechnological glycosaminoglycans, different approaches have been considered for simulating the alpha(1-->4)-linked 2-O-sulfated L-iduronic acid (IdoA2SO(3))-->N,6-O-sulfated D-glucosamine (GlcNSO(3)6SO(3)) disaccharide sequences prevalent in mammalian heparins. Since the direct approach of sulfating totally O-desulfated heparins, taken as model compounds for C-5-epimerized sulfaminoheparosan (N-deacetylated, N-sulfated Escherichia coli K5 polysaccharide), preferentially afforded heparins O-sulfated at C-3 instead than at C-2 of the iduronate residues, leading to products with low anticoagulant activities, the problem of re-generating a substantial proportion of the original IdoA2SO(3) residues was circumvented by performing controlled solvolytic desulfation (with 9:1 v/v DMSO-MeOH) of extensively sulfated heparins. The order of desulfation of major residues of heparin GlcN and IdoA and of the minor one D-glucuronic acid was: GlcNSO(3)>GlcN6SO(3)>IdoA3SO(3) congruent with GlcA2SO(3) congruent with GlcN3SO(3)>IdoA2SO(3) congruent with GlcA3SO(3). Starting from a 'supersulfated' low-molecular weight heparin, we obtained products with up to 40% of iduronate residues O-sulfated exclusively at C-2 and up to 40% of their glucosamine residues O-sulfated at both C-6 and C-3. Upon re-N-sulfation, these products displayed an in vitro antithrombotic activity (expressed as anti-factor Xa units) comparable with those of current low-molecular weight heparins.

Published

2001