Your search keyword '"Alterio V"' showing total 115 results

101. Hypoxia-targeting carbonic anhydrase IX inhibitors by a new series of nitroimidazole-sulfonamides/sulfamides/sulfamates.

Author

Rami M, Dubois L, Parvathaneni NK, Alterio V, van Kuijk SJ, Monti SM, Lambin P, De Simone G, Supuran CT, and Winum JY

Subjects

Carbonic Anhydrase IX, Dose-Response Relationship, Drug, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors chemistry, HT29 Cells, HeLa Cells, Humans, Hypoxia, Models, Molecular, Molecular Structure, Structure-Activity Relationship, Amides chemistry, Antigens, Neoplasm metabolism, Carbonic Anhydrases metabolism, Enzyme Inhibitors pharmacology, Nitroimidazoles chemistry, Sulfonamides chemistry, Sulfonic Acids chemistry

Abstract

A series of nitroimidazoles incorporating sulfonamide/sulfamide/sulfamate moieties were designed and synthesized as radio/chemosensitizing agent targeting the tumor-associated carbonic anhydrase (CA) isoforms IX and XII. Most of the new compounds were nanomolar inhibitors of these isoforms. Crystallographic studies on the complex of hCA II with the lead sulfamide derivative of this series clarified the binding mode of this type of inhibitors in the enzyme active site cavity. Some of the best nitroimidazole CA IX inhibitors showed significant activity in vitro by reducing hypoxia-induced extracellular acidosis in HT-29 and HeLa cell lines. In vivo testing of the lead molecule in the sulfamide series, in cotreatment with doxorubicin, demonstrated a chemosensitization of CA IX containing tumors. Such CA inhibitors, specifically targeting the tumor-associated isoforms, are candidates for novel treatment strategies against hypoxic tumors overexpressing extracellular CA isozymes.

Published

2013

102. Exploiting the hydrophobic and hydrophilic binding sites for designing carbonic anhydrase inhibitors.

Author

De Simone G, Alterio V, and Supuran CT

Subjects

Binding Sites, Crystallography, X-Ray, Humans, Models, Molecular, Structure-Activity Relationship, Carbonic Anhydrase Inhibitors chemistry, Carbonic Anhydrase Inhibitors pharmacology, Drug Design, Hydrophobic and Hydrophilic Interactions drug effects

Abstract

Introduction: Carbonic anhydrases (CAs, EC 4.2.1.1) exist as five genetically distinct families (α, β, γ, δ and ζ) in organisms all over the phylogenetic tree. Due to the ubiquity of such enzymes, the selective inhibition and polypharmacology of inhibitors is an important aspect of all drug design campaigns. There are several classes of CA inhibitors (CAIs): i) metal ion binders (sulfonamides and their isosteres [sulfamates/sulfamides], dithiocarbamates, mercaptans and hydroxamates); ii) compounds anchoring to the zinc-coordinated water molecule/hydroxide ion (phenols, carboxylates, polyamines, esters and sulfocoumarins) and iii) coumarins and related compounds which apparently bind even further away from the metal ion., Areas Covered: The authors rationalize the drug design strategies of inhibitors belonging to the first two classes, based on recent X-ray crystallographic data. More precisely, this is achieved by analyzing how the hydrophobic and hydrophilic halves of the enzyme active site interact with inhibitors. This task has been eased by the recent report of β-CA-like enzymes possessing carbon disulfide and carbonyl sulfide hydrolase activities, respectively, allowing the authors to propose a general approach of structure-based drug design of CAIs., Expert Opinion: Although amazing progress has been made in the structure-based drug design of CAIs, this field is still in progress, with many constantly emerging new findings. Indeed, several new such enzymes were discovered and characterized recently and novel chemotypes were explored for finding compounds with a better inhibition profile. It is anticipated that this will continue to be one of the main frontiers in the search of pharmacologically relevant enzyme inhibitors.

Published

2013

103. Multiple binding modes of inhibitors to carbonic anhydrases: how to design specific drugs targeting 15 different isoforms?

Author

Alterio V, Di Fiore A, D'Ambrosio K, Supuran CT, and De Simone G

Subjects

Amino Acid Sequence, Animals, Carbonic Anhydrase Inhibitors chemistry, Carbonic Anhydrases chemistry, Humans, Isoenzymes antagonists & inhibitors, Isoenzymes chemistry, Isoenzymes metabolism, Molecular Sequence Data, Protein Binding, Zinc metabolism, Carbonic Anhydrase Inhibitors metabolism, Carbonic Anhydrase Inhibitors pharmacology, Carbonic Anhydrases metabolism, Drug Design

Published

2012

104. Structural and inhibition insights into carbonic anhydrase CDCA1 from the marine diatom Thalassiosira weissflogii.

Author

Alterio V, Langella E, Viparelli F, Vullo D, Ascione G, Dathan NA, Morel FM, Supuran CT, De Simone G, and Monti SM

Subjects

Amino Acid Sequence, Crystallography, X-Ray, Molecular Sequence Data, Protein Structure, Secondary, Sequence Homology, Amino Acid, Carbonic Anhydrases chemistry, Carbonic Anhydrases metabolism, Diatoms enzymology

Abstract

Carbonic anhydrases (CAs) catalyze with high efficiency the reversible hydration of carbon dioxide, an essential reaction for many biological processes, such as photosynthesis, respiration, renal tubular acidification, and bone resorption. Diatoms, which are one of the most common types of phytoplankton and are widespread in oceans, possess CAs fundamental for acquisition of inorganic carbon. Recently, in the marine diatom Thalassiosira weissflogii a novel enzyme, CDCA1, naturally using Cd in its active site, has been isolated and categorized in a new CA class, namely zeta-CA. This enzyme, which consists of three repeats (R1, R2 and R3), is a cambialistic carbonic anhydrase that can spontaneously exchange Zn or Cd at its active centre, presumably an adaptative advantage for diatoms that grow fast in the metal-poor environment of the surface ocean. In this paper we completed the characterization of this enzyme, reporting the X-ray structure of the last repeat, CDCA1-R3 in its cadmium-bound form, and presenting a model of the full length protein obtained by docking approaches. Results show that CDCA1 has a quite compact not symmetric structure, characterized by two covalently linked R1-R2 and R2-R3 interfaces and a small non-covalent R1-R3 interface. The three dimensional arrangement shows that most of the non-conserved aminoacids of the three repeats are located at the interface regions and that the active sites are far from each other and completely accessible to the substrate. Finally, a detailed inhibition study of CDCA1-R3 repeat in both cadmium- and zinc- bound form has been performed with sulfonamides and sulfamates derivatives. The results have been compared with those previously reported for other CA classes, namely alpha- and beta-classes, and correlated with the structural features of these enzymes., (Copyright © 2012 Elsevier Masson SAS. All rights reserved.)

Published

2012

105. Carbonic anhydrase VII is S-glutathionylated without loss of catalytic activity and affinity for sulfonamide inhibitors.

Author

Truppo E, Supuran CT, Sandomenico A, Vullo D, Innocenti A, Di Fiore A, Alterio V, De Simone G, and Monti SM

Subjects

Amino Acid Sequence, Carbonic Anhydrase Inhibitors pharmacology, Carbonic Anhydrases genetics, Cytosol enzymology, Enzyme Activation drug effects, Humans, Inhibitory Concentration 50, Molecular Sequence Data, Protein Isoforms genetics, S-Nitrosoglutathione chemistry, Sequence Alignment, Spectrometry, Mass, Electrospray Ionization, Sulfonamides pharmacology, Carbonic Anhydrase Inhibitors chemistry, Carbonic Anhydrases metabolism, Sulfonamides chemistry

Abstract

Human carbonic anhydrase (CA, EC 4.2.1.1) VII is a cytosolic enzyme with high carbon dioxide hydration activity. Here we report an unexpected S-glutathionylation of hCA VII which has also been observed earlier in vivo for hCA III, another cytosolic isoform. Cys183 and Cys217 were found to be the residues involved in reaction with glutathione for hCA VII. The two reactive cysteines were then mutated and the corresponding variant (C183S/C217S) expressed. The native enzyme, the variant and the S-glutathionylated adduct (sgCA VII) as well as hCA III were fully characterized for their CO(2) hydration, esterase/phosphatase activities, and inhibition with sulfonamides. Our findings suggest that hCA VII could use the in vivo S-glutathionylation to function as an oxygen radical scavenger for protecting cells from oxidative damage, as the activity and affinity for inhibitors of the modified enzyme are similar to those of the wild type., (Copyright © 2012 Elsevier Ltd. All rights reserved.)

Published

2012

106. Carbonic anhydrase inhibitors: X-ray crystallographic studies for the binding of N-substituted benzenesulfonamides to human isoform II.

Author

Di Fiore A, Maresca A, Alterio V, Supuran CT, and De Simone G

Subjects

Crystallography, X-Ray, Models, Molecular, Protein Binding, Sulfonamides chemistry, Carbonic Anhydrase II metabolism, Carbonic Anhydrase Inhibitors chemistry, Sulfonamides metabolism

Abstract

N-substituted benzenesulfonamides, incorporating the N-amino-, N-hydroxy- and N-methoxy-moieties at the sulfonamide zinc binding group, have been investigated as CAIs by means of inhibition and structural studies, unraveling interesting aspects related to their inhibition mechanism., (This journal is © The Royal Society of Chemistry 2011)

Published

2011

107. Molecular organization of the cullin E3 ligase adaptor KCTD11.

Author

Correale S, Pirone L, Di Marcotullio L, De Smaele E, Greco A, Mazzà D, Moretti M, Alterio V, Vitagliano L, Di Gaetano S, Gulino A, and Pedone EM

Subjects

Amino Acid Sequence, Base Sequence, Cell Cycle Proteins, Cullin Proteins chemistry, Cullin Proteins genetics, HEK293 Cells, Humans, Models, Molecular, Molecular Sequence Data, Mutagenesis, Site-Directed methods, Protein Binding genetics, Protein Isoforms chemistry, Protein Isoforms genetics, Protein Structure, Tertiary, Recombinant Proteins chemistry, Recombinant Proteins genetics, Transferases, Ubiquitin chemistry, Potassium Channels chemistry, Potassium Channels genetics, Ubiquitin-Protein Ligases chemistry

Abstract

The family of human proteins containing a potassium channel tetramerization domain (KCTD) includes 21 members whose function is largely unknown. Recent reports have however suggested that these proteins are implicated in very important biological processes. KCTD11/REN, the best-characterized member of the family to date, plays a crucial role in the ubiquitination of HDAC1 by acting, in complex with Cullin3, as an E3 ubiquitin ligase. By combining bioinformatics and mutagenesis analyses, here we show that the protein is expressed in two alternative variants: a short previously characterized form (sKCTD11) composed by 232 amino acids and a longer variant (lKCTD11) which contains an N-terminal extension of 39 residues. Interestingly, we demonstrate that lKCTD11 starts with a non-canonical AUU codon. Although both sKCTD11 and lKCTD11 bear a POZ/BTB domain in their N-terminal region, this domain is complete only in the long form. Indeed, sKCTD11 presents an incomplete POZ/BTB domain. Nonetheless, sKCTD11 is still able to bind Cul3, although to much lesser extent than lKCTD11, and to perform its biological activity. The heterologous expression of sKCTD11 and lKCTD11 and their individual domains in Escherichia coli yielded soluble products as fusion proteins only for the longer form. In contrast to the closely related KCTD5 which is pentameric, the characterization of both lKCTD11 and its POZ/BTB domain by gel filtration and light scattering indicates that the protein likely forms stable tetramers. In line with this result, experiments conducted in cells show that the active protein is not monomeric. Based on these findings, homology-based models were built for lKCTD11 BTB and for its complex with Cul3. These analyses indicate that a stable lKCTD11 BTB-Cul3 three-dimensional model with a 4:4 stoichiometry can be generated. Moreover, these models provide insights into the determinants of the tetramer stability and into the regions involved in lKCTD11-Cul3 recognition., (Copyright © 2011 Elsevier Masson SAS. All rights reserved.)

Published

2011

108. Crystal structure of the C183S/C217S mutant of human CA VII in complex with acetazolamide.

Author

Di Fiore A, Truppo E, Supuran CT, Alterio V, Dathan N, Bootorabi F, Parkkila S, Monti SM, and De Simone G

Subjects

Amino Acid Sequence, Carbonic Anhydrases genetics, Crystallography, X-Ray, Humans, Models, Molecular, Molecular Sequence Data, Protein Structure, Secondary, Sequence Homology, Amino Acid, Acetazolamide chemistry, Carbonic Anhydrases chemistry, Mutation

Abstract

Human carbonic anhydrase VII (hCA VII) is a cytosolic member of the alpha-CA family. This enzyme is mainly localized in a number of brain tissues such as the cortex, hippocampus and thalamus and has been noted for its contribution in generating neuronal excitation and seizures. Recently, it has been also proposed that hCA VII may be involved in the control of neuropathic pain, thus its inhibition may offer a new approach in designing pain killers useful for combating neuropathic pain. We report here the X-ray crystallographic structure of a mutated form of human CA VII in complex with acetazolamide, a classical sulfonamide inhibitor. These crystallographic studies provide important implications for the rational drug design of selective CA inhibitors with clinical applications., (Copyright 2010 Elsevier Ltd. All rights reserved.)

Published

2010

109. The first example of a significant active site conformational rearrangement in a carbonic anhydrase-inhibitor adduct: the carbonic anhydrase I-topiramate complex.

Author

Alterio V, Monti SM, Truppo E, Pedone C, Supuran CT, and De Simone G

Subjects

Amino Acid Sequence, Carbonic Anhydrase I antagonists & inhibitors, Carbonic Anhydrase Inhibitors chemistry, Crystallography, X-Ray, Fructose chemistry, Fructose metabolism, Fructose pharmacology, Humans, Isoenzymes antagonists & inhibitors, Isoenzymes chemistry, Isoenzymes metabolism, Models, Molecular, Molecular Sequence Data, Protein Binding, Topiramate, Carbonic Anhydrase I chemistry, Carbonic Anhydrase I metabolism, Carbonic Anhydrase Inhibitors metabolism, Carbonic Anhydrase Inhibitors pharmacology, Catalytic Domain, Fructose analogs & derivatives

Abstract

Topiramate is a widely used antiepileptic drug, which has been demonstrated to act as an efficient weight loss agent. Since several studies have pointed out that is a potent in vitro inhibitor of several Carbonic anhydrase (CA) isozymes, it has been hypothesized that its anti-obesity properties could be ascribed to the inhibition of the CAs involved in de novo lipogenesis. Consequently, the study of the interactions of with all human CA isoforms represents an important step for the rational drug design of selective CA inhibitors to be used as anti-obesity drugs. In this paper we report the crystallographic structure of the adduct that forms with hCA I, showing for the first time a profound reorganization of the CA active site upon binding of the inhibitor. Moreover, a structural comparison with hCA II- and hCA VA- adducts, previously investigated, has been performed showing that a different H-bond network together with the movement of some amino acid residues in the active site may account for the different inhibition constants of toward these three CA isozymes.

Published

2010

110. Recent advances in structural studies of the carbonic anhydrase family: the crystal structure of human CA IX and CA XIII.

Author

Supuran CT, Di Fiore A, Alterio V, Monti SM, and De Simone G

Subjects

Antigens, Neoplasm drug effects, Antigens, Neoplasm metabolism, Carbonic Anhydrase IX, Carbonic Anhydrase Inhibitors pharmacology, Carbonic Anhydrases drug effects, Carbonic Anhydrases metabolism, Drug Design, Humans, Isoenzymes antagonists & inhibitors, Isoenzymes chemistry, Isoenzymes drug effects, Models, Molecular, Antigens, Neoplasm chemistry, Carbonic Anhydrases chemistry, Crystallography, X-Ray methods, Protein Structure, Quaternary

Abstract

The carbonic anhydrase (CA) family has recently become an important target for the drug design of inhibitors with potential use as diagnostic and therapeutic tools. However, given the high degree of sequence and structure similarity among the different CA isoforms, no CA-directed drug developed so far has displayed selectivity for a specific isozyme. Since X-Ray crystallography is a very useful tool for the rational drug design of selective enzyme inhibitors, in recent years extensive research efforts have been devoted to the structural studies of all catalytically active α-CA isoforms, with the consequent resolution of the crystallographic structures of nearly all such enzyme isoforms. In this paper we review the progress that has recently been made in this field. In particular, we summarize the main structural features of hCA XIII and hCA IX, the most recently characterized human CA isoforms, and recapitulate how 3D structures of these enzymes, together with kinetic experiments, have been used either to deepen our knowledge on the structural features responsible of the catalytic properties of this protein family or to obtain important information for the rational drug design of inhibitors with better selectivity properties.

Published

2010

111. Carbonic anhydrase inhibitors. Comparison of aliphatic sulfamate/bis-sulfamate adducts with isozymes II and IX as a platform for designing tight-binding, more isoform-selective inhibitors.

Author

Vitale RM, Alterio V, Innocenti A, Winum JY, Monti SM, De Simone G, and Supuran CT

Subjects

Carbonic Anhydrase IX, Carbonic Anhydrase Inhibitors pharmacology, Catalytic Domain, Drug Design, Humans, Models, Molecular, Protein Binding, Structure-Activity Relationship, Sulfonic Acids pharmacology, Antigens, Neoplasm drug effects, Carbonic Anhydrase II antagonists & inhibitors, Carbonic Anhydrase Inhibitors chemistry, Carbonic Anhydrases drug effects, Sulfonic Acids chemistry

Abstract

Two approaches were used to design inhibitors of the metalloenzyme carbonic anhydrase (CA, EC 4.2.1.1): the tail and the ring approaches. Aliphatic sulfamates constitute a class of CA inhibitors (CAIs) that cannot be classified in either one of these categories. We report here the detailed inhibition profile of four such compounds against isoforms CAs I-XIV, the first crystallographic structures of these compounds in adduct with isoform II, and molecular modeling studies for their interaction with hCA IX. Aliphatic monosulfamates/bis-sulfamates were nanomolar inhibitors of hCAs II, IX, and XII, unlike aromatic/heterocyclic sulfonamides that promiscuously inhibit most CA isozymes with low nanomolar affinity. The bis-sulfamates incorporating 8 or 10 carbon atoms showed higher affinity for the tumor-associated hCA IX compared to hCA II, whereas the opposite was true for the monosulfamates. The explanation for their interaction with CA active site furnishes insights for obtaining compounds with increased affinity/selectivity for various isozymes.

Published

2009

112. Carbonic anhydrase inhibitors: inhibition of human, bacterial, and archaeal isozymes with benzene-1,3-disulfonamides--solution and crystallographic studies.

Author

Alterio V, De Simone G, Monti SM, Scozzafava A, and Supuran CT

Subjects

Carbonic Anhydrase Inhibitors chemistry, Crystallography, X-Ray, Hydrogen Bonding, Models, Molecular, Sulfonamides chemistry, Carbonic Anhydrase Inhibitors pharmacology, Carbonic Anhydrases drug effects, Isoenzymes antagonists & inhibitors, Sulfonamides pharmacology

Abstract

Three benzene-1,3-disulfonamide derivatives were investigated for their interaction with 12 mammalian alpha-carbonic anhydrases (CAs, EC 4.2.1.1), and three bacterial/archaeal CAs belonging to the alpha-, beta-, and gamma-CA class, respectively. X-ray crystal structure of the three inhibitors in complex with the dominant human isozyme CA II revealed a particular binding mode within the cavity. The sulfonamide group in meta-position to the Zn(2+)-coordinated SO(2)NH(2) moiety was oriented toward the hydrophilic side of the active site cleft, establishing hydrogen bonds with His64, Asn67, Gln92, and Thr200. The plane of the phenyl moiety of the inhibitors was rotated by 45 degrees and tilted by 10 degrees with respect to its most recurrent orientation in other CA II-sulfonamide complexes.

Published

2007

113. Carbonic anhydrase inhibitors: X-ray and molecular modeling study for the interaction of a fluorescent antitumor sulfonamide with isozyme II and IX.

Author

Alterio V, Vitale RM, Monti SM, Pedone C, Scozzafava A, Cecchi A, De Simone G, and Supuran CT

Subjects

Amino Acid Sequence, Antigens, Neoplasm drug effects, Antineoplastic Agents pharmacology, Binding Sites, Carbonic Anhydrase II antagonists & inhibitors, Carbonic Anhydrase IX, Carbonic Anhydrase Inhibitors pharmacology, Carbonic Anhydrases drug effects, Computer Simulation, Crystallography, X-Ray, Fluoresceins pharmacology, Fluorescence, Isoenzymes chemistry, Models, Molecular, Molecular Sequence Data, Sequence Alignment, Spectrometry, Fluorescence, Sulfonamides pharmacology, Thiourea chemistry, Thiourea pharmacology, Antigens, Neoplasm chemistry, Antineoplastic Agents chemistry, Carbonic Anhydrase II chemistry, Carbonic Anhydrase Inhibitors chemistry, Carbonic Anhydrases chemistry, Fluoresceins chemistry, Isoenzymes antagonists & inhibitors, Sulfonamides chemistry, Thiourea analogs & derivatives

Abstract

The X-ray crystal structure of the fluorescent antitumor sulfonamide carbonic anhydrase (CA, EC, 4.2.1.1) inhibitor (4-sulfamoylphenylethyl)thioureido fluorescein (1) in complex with the cytosolic isoform hCA II is reported, together with a modeling study of the adduct of 1 with the tumor-associated isoform hCA IX. Its binding to hCA II is similar to that of other benzesulfonamides, with the ionized sulfonamide coordinated to the Zn2+ ion within the enzyme active site, and also participating in a network of hydrogen bonds with residues Thr199 and Glu106. The scaffold of 1 did not establish polar interactions within the enzyme active site but made hydrophobic contacts (<4.5 A) with Gln92, Val121, Phe131, Val135, Leu198, Thr199, Thr200, and Pro202. The substituted 3-carboxy-amino-phenyl functionality was at van der Waals distance from Phe131, Gly132, and Val135. The bulky tricyclic fluorescein moiety was located at the rim of the active site, on the protein surface, and strongly interacted with the alpha-helix formed by residues Asp130-Val135. All these interactions were preserved in the hCA IX-1 adduct, but the carbonyl moiety of the fluorescein tail of 1 participates in a strong hydrogen bond with the guanidine moiety of Arg130, an amino acid characteristic of the hCA IX active site. This may account for the roughly 2 times higher affinity of 1 for hCA IX over hCA II and may explain why in vivo the compound specifically accumulates only in hypoxic tumors overexpressing CA IX and not in the normal tissues. The compound is in clinical studies as an imaging tool for acute hypoxic tumors.

Published

2006

114. Metal ion substitution in the catalytic site greatly affects the binding of sulfhydryl-containing compounds to leucyl aminopeptidase.

Author

Cappiello M, Alterio V, Amodeo P, Del Corso A, Scaloni A, Pedone C, Moschini R, De Donatis GM, De Simone G, and Mura U

Subjects

Binding Sites, Catalytic Domain, Crystallography, X-Ray, Enzyme Inhibitors metabolism, Enzyme Inhibitors pharmacology, Hydrolases metabolism, Kinetics, Leucyl Aminopeptidase chemistry, Manganese metabolism, Manganese pharmacology, Models, Molecular, Structure-Activity Relationship, Substrate Specificity, Sulfhydryl Compounds chemistry, Zinc metabolism, Zinc pharmacology, Cations, Divalent metabolism, Leucyl Aminopeptidase metabolism, Manganese chemistry, Sulfhydryl Compounds metabolism, Zinc chemistry

Abstract

Bovine lens leucyl aminopeptidase (blLAP), a homohexameric metallopeptidase preferring bulky and hydrophobic amino acids at the N-terminus of (di)peptides, contains two Zn(2+) ions per subunit that are essential for catalytic activity. They may be replaced by other divalent cations with different exchange kinetics. The protein readily exchangeable site (site 1) can be occupied by Zn(2+), Mn(2+), Mg(2+), or Co(2+), while the tight binding site (site 2) can be occupied by Zn(2+) or Co(2+). We recently reported that introduction of Mn(2+) into site 1 generates a novel activity of blLAP toward CysGly [Cappiello, M., et al. (2004) Biochem. J. 378, 35-44], which in contrast is not hydrolyzed by the (Zn/Zn) enzyme. This finding, while disclosing a potential specific role for blLAP in glutathione metabolism, raised a question about the features required for molecules to be a substrate for the enzyme. To clarify the interaction of the enzyme with sulfhydryl-containing derivatives, (Zn/Zn)- and (Mn/Zn)blLAP forms were prepared and functional-structural studies were undertaken. Thus, a kinetic analysis of various compounds with both enzyme forms was performed; the crystal structure of (Zn/Zn)blLAP in complex with the peptidomimetic derivative Zofenoprilat was determined, and a modeling study on the CysGly-(Zn/Zn)blLAP complex was carried out. This combined approach provided insight into the interaction of blLAP with sulfhydryl-containing derivatives, showing that the metal exchange in site 1 modulates binding to these molecules that may result in enzyme substrates or inhibitors, depending on the nature of the metal.

Published

2006

115. Henoch-Schonlein purpura with antiphospholipid antibodies after influenza vaccination: how fearful is it in children?

Author

Mormile R, D'Alterio V, Treccagnoli G, and Sorrentino P

Subjects

Child, Preschool, Female, Humans, Antibodies, Antiphospholipid blood, IgA Vasculitis etiology, Influenza Vaccines adverse effects

Published

2004