Your search keyword '"Kiappes JL"' showing total 20 results

1. Inhibition of endoplasmic reticulum glucosidases is required for in vitro and in vivo dengue antiviral activity by the iminosugar UV-4

Author

Warfield, Kelly L, Plummer, Emily M, Sayce, Andrew C, Alonzi, Dominic S, Tang, William, Tyrrell, Beatrice E, Hill, Michelle L, Caputo, Alessandro T, Killingbeck, Sarah S, Beatty, P Robert, Harris, Eva, Iwaki, Ren, Kinami, Kyoko, Ide, Daisuke, Kiappes, JL, Kato, Atsushi, Buck, Michael D, King, Kevin, Eddy, William, Khaliq, Mansoora, Sampath, Aruna, Treston, Anthony M, Dwek, Raymond A, Enterlein, Sven G, Miller, Joanna L, Zitzmann, Nicole, Ramstedt, Urban, and Shresta, Sujan

Subjects

Rare Diseases, Vaccine Related, Infectious Diseases, Prevention, Biodefense, Emerging Infectious Diseases, Biotechnology, Vector-Borne Diseases, Orphan Drug, Infection, Good Health and Well Being, 1-Deoxynojirimycin, Animals, Antibodies, Viral, Antibody-Dependent Enhancement, Antiviral Agents, Cells, Cultured, Chlorocebus aethiops, Clinical Trials as Topic, Dengue Virus, Disease Models, Animal, Drugs, Investigational, Endoplasmic Reticulum, Glycoside Hydrolase Inhibitors, Humans, Inhibitory Concentration 50, Mice, Monocytes, Receptors, Interferon, Serogroup, Severe Dengue, Vero Cells, alpha-Glucosidases, Iminosugar, UV-4B, Dengue, Antibody-dependent enhancement, Antiviral, Glucosidase, Microbiology, Medical Microbiology, Pharmacology and Pharmaceutical Sciences, Virology

Abstract

The antiviral activity of UV-4 was previously demonstrated against dengue virus serotype 2 (DENV2) in multiple mouse models. Herein, step-wise minimal effective dose and therapeutic window of efficacy studies of UV-4B (UV-4 hydrochloride salt) were conducted in an antibody-dependent enhancement (ADE) mouse model of severe DENV2 infection in AG129 mice lacking types I and II interferon receptors. Significant survival benefit was demonstrated with 10-20 mg/kg of UV-4B administered thrice daily (TID) for seven days with initiation of treatment up to 48 h after infection. UV-4B also reduced infectious virus production in in vitro antiviral activity assays against all four DENV serotypes, including clinical isolates. A set of purified enzyme, in vitro, and in vivo studies demonstrated that inhibition of endoplasmic reticulum (ER) α-glucosidases and not the glycosphingolipid pathway appears to be responsible for the antiviral activity of UV-4B against DENV. Along with a comprehensive safety package, these and previously published data provided support for an Investigational New Drug (IND) filing and Phases 1 and 2 clinical trials for UV-4B with an indication of acute dengue disease.

Published

2016

2. A Quinolin-8-Ol Sub-Millimolar Inhibitor of UGGT, the ER Glycoprotein Folding Quality Control Checkpoint

Author

Guay, Kevin P., primary, Ibba, Roberta, additional, Kiappes, JL, additional, De Benedictis, Maria, additional, Zeni, Ilaria, additional, Le Cornu, James David, additional, Hensen, Mario, additional, Chandran, Anu V., additional, Kantsadi, Anastassia L., additional, Caputo, Alessandro T., additional, Blanco Capurro, Juan Ignacio, additional, Bayo, Yusupha, additional, Hill, Johan Christopher, additional, Hudson, Kieran, additional, Lia, Andrea, additional, Vasiljevic, Snezana, additional, Modenutti, Carlos Pablo, additional, Withers, Stephen G., additional, Martí, Marcelo, additional, Biasini, Emiliano, additional, Santino, Angelo, additional, Hebert, Daniel N., additional, Zitzmann, Nicole, additional, and Roversi, Pietro, additional

Published

2022

3. Targeting ER α-glucosidase I with a single-dose iminosugar treatment protects against lethal influenza and dengue virus infections

Author

Warfield, K, Alonzi, DS, Hill, JC, Caputo, AT, Roversi, P, Kiappes, JL, Sheets, N, Duchars, M, Dwek, RA, Biggins, J, Barnard, D, Shresta, S, Treston, A, and Zitzmann, N

Abstract

Influenza and dengue viruses present a growing global threat to public health. Both viruses depend on the host endoplasmic reticulum (ER) glycoprotein folding pathway. In 2014, Sadat et al. reported two siblings with a rare genetic defect in ER alpha-glucosidase I (ER Glu I) who showed resistance to viral infections, identifying ER Glu I as a key antiviral target. Here we show that a single dose of UV-4B (the hydrochloride salt form of N-(9′-methoxynonyl)-1- deoxynojirimycin; MON-DNJ) capable of inhibiting Glu I in vivo is sufficient to prevent death in mice infected with lethal viral doses, even when treatment is started as late as 48 hours post-infection. The first crystal structure of mammalian ER Glu I will constitute the basis for the development of potent and selective inhibitors. Targeting ER Glu I with UV-4B derived compounds may alter treatment paradigms for acute viral disease through development of a single-dose therapeutic regime.

Published

2020

4. Structural Insights into the Broad-Spectrum Antiviral Target Endoplasmic Reticulum Alpha-Glucosidase II

Author

Caputo, AT, Alonzi, DS, Kiappes, JL, Struwe, WB, Cross, A, Basu, S, Darlot, B, Roversi, P, Zitzmann, N, Hilgenfeld, R, and Vasudevan, S

Subjects

0301 basic medicine, chemistry.chemical_classification, 030102 biochemistry & molecular biology, Endoplasmic reticulum, Iminosugar, 03 medical and health sciences, Broad spectrum, 030104 developmental biology, Enzyme, chemistry, Catalytic cycle, Biochemistry, Glycoprotein, Estrogen receptor alpha, Alpha-glucosidase II

Abstract

Targeting the host-cell endoplasmic reticulum quality control (ERQC) pathway is an effective broad-spectrum antiviral strategy. The two ER resident α-glucosidases whose sequential action permits entry in this pathway are the targets of glucomimetic inhibitors. Knowledge of the molecular details of the ER α-glucosidase II (α-Glu II) structure was limited. We determined crystal structures of a trypsinolytic fragment of murine α-Glu II, alone and in complex with key catalytic cycle ligands, and four different broad-spectrum antiviral iminosugar inhibitors, two of which are currently in clinical trials against dengue fever. The structures highlight novel portions of the enzyme outside its catalytic pocket which contribute to its activity and substrate specificity. These crystal structures and hydrogen-deuterium exchange mass spectrometry of the murine ER alpha glucosidase II heterodimer uncover the quaternary arrangement of the enzyme’s α- and β-subunits, and suggest a conformational rearrangement of ER α-Glu II upon association of the enzyme with client glycoproteins.

Published

2018

5. Structural studies of Endoplasmic Reticulum Glucosidase II

Author

Caputo, AT, Alonzi, D, Cross, A, Kiappes, JL, Roversi, P, and Zitzmann, N

Published

2016

6. Iminosugars Inhibit Dengue Virus Production via Inhibition of ER Alpha-Glucosidases—Not Glycolipid Processing Enzymes

Author

Sayce, AC, Alonzi, DS, Killingbeck, SS, Tyrrell, BE, Hill, ML, Caputo, AT, Iwaki, R, Kinami, K, Ide, D, Kiappes, JL, Beatty, PR, Kato, A, Harris, E, Dwek, RA, Miller, JL, and Zitzmann, N

Subjects

Models, Molecular, lcsh:Arctic medicine. Tropical medicine, lcsh:RC955-962, Glycobiology, Mouse Models, Endoplasmic Reticulum, Research and Analysis Methods, Biochemistry, Microbiology, Antiviral Agents, Model Organisms, Stereochemistry, Animals, Humans, Animal Models of Disease, Enzyme Inhibitors, Cells, Cultured, Virus Release, Glycoproteins, Secretory Pathway, Molecular Structure, lcsh:Public aspects of medicine, Macrophages, Indolizines, Biology and Life Sciences, lcsh:RA1-1270, alpha-Glucosidases, Cell Biology, Animal Models, Cell Cultures, Dengue Virus, Imino Sugars, Animal Models of Infection, Chemistry, Cell Processes, Physical Sciences, Enzymology, Animal Studies, Biological Cultures, Glycolipids, Cellular Structures and Organelles, Research Article

Abstract

It has long been thought that iminosugar antiviral activity is a function of inhibition of endoplasmic reticulum-resident α-glucosidases, and on this basis, many iminosugars have been investigated as therapeutic agents for treatment of infection by a diverse spectrum of viruses, including dengue virus (DENV). However, iminosugars are glycomimetics possessing a nitrogen atom in place of the endocyclic oxygen atom, and the ubiquity of glycans in host metabolism suggests that multiple pathways can be targeted via iminosugar treatment. Successful treatment of patients with glycolipid processing defects using iminosugars highlights the clinical exploitation of iminosugar inhibition of enzymes other than ER α-glucosidases. Evidence correlating antiviral activity with successful inhibition of ER glucosidases together with the exclusion of alternative mechanisms of action of iminosugars in the context of DENV infection is limited. Celgosivir, a bicyclic iminosugar evaluated in phase Ib clinical trials as a therapeutic for the treatment of DENV infection, was confirmed to be antiviral in a lethal mouse model of antibody-enhanced DENV infection. In this study we provide the first evidence of the antiviral activity of celgosivir in primary human macrophages in vitro, in which it inhibits DENV secretion with an EC50 of 5 μM. We further demonstrate that monocyclic glucose-mimicking iminosugars inhibit isolated glycoprotein and glycolipid processing enzymes and that this inhibition also occurs in primary cells treated with these drugs. By comparison to bicyclic glucose-mimicking iminosugars which inhibit glycoprotein processing but do not inhibit glycolipid processing and galactose-mimicking iminosugars which do not inhibit glycoprotein processing but do inhibit glycolipid processing, we demonstrate that inhibition of endoplasmic reticulum-resident α-glucosidases, not glycolipid processing, is responsible for iminosugar antiviral activity against DENV. Our data suggest that inhibition of ER α-glucosidases prevents release of virus and is the primary antiviral mechanism of action of iminosugars against DENV., Author Summary Current treatment of dengue virus infection is supportive; however, iminosugars have been widely investigated as an antiviral strategy. The means by which these molecules are thought to exert their antiviral effects is through inhibition of host-resident glycoprotein processing enzymes, the endoplasmic reticulum-resident α-glucosidases, but many iminosugars are also capable of inhibiting host glycolipid processing and are utilized clinically for the treatment of lysosomal storage disorders such as Gaucher’s and Niemann-Pick type C diseases. The work presented here is the first to conclusively differentiate the antiviral properties of these two major mechanisms of action of iminosugars, and our data support the long-standing hypothesis that inhibition of glycoprotein processing is the essential antiviral property of iminosugars in the case of dengue virus infection. These results indicate that further development of iminosugars as dengue antivirals should focus on optimization of glycoprotein inhibition efficacy with reduction or elimination of glycolipid modulating properties to minimize off-target effects. These results are supported by the in vitro and in vivo efficacy of the bicyclic iminosugar, celgosivir, which we demonstrate to lack capacity for inhibition of glycosphingolipid processing.

Published

2016

7. Assessment of repurposed compounds against coronaviruses highlights the antiviral broad-spectrum activity of host-targeting iminosugars and confirms the activity of potent directly acting antivirals.

Author

Brun J, Arman BY, Hill ML, Kiappes JL, Alonzi DS, Makower LL, Witt KD, Gileadi C, Rangel V, Dwek RA, von Delft A, and Zitzmann N

Abstract

The COVID-19 pandemic highlights the need for novel antiviral drug discovery approaches that could dramatically shorten timelines from compound discovery to clinical development. At the beginning of the pandemic, repurposing approaches were at the forefront of early research efforts to screen for antiviral activity against SARS-CoV-2 in over 2500 compounds. Here, we report cellular screening results of 100 FDA-approved and experimental compounds against SARS-CoV-2 in the human Calu-3 cell line. We observed 13 compounds showing antiviral activity against SARS-CoV-2, including seven FDA-approved compounds (remdesivir, boceprevir, amiloride, nafamostat, cisplatin, silmitasertib, and miglustat), and six compounds in pre-clinical and clinical development (tarloxotinib, lucerastat (NB-DGJ), MON-DNJ, NAP-DNJ, NN-DGJ and NN-DNJ). Further, we observed that our screening hits include several host-targeting antivirals, namely iminosugars, that are largely non-toxic and offer a large therapeutic window. The most-developed iminosugar MON-DNJ (UV-4B), which has been evaluated in a Phase 1 clinical trial, shows antiviral activity against SARS-CoV-2 wild type as well as alpha, beta, gamma, delta, and Omicron variants. Its activity also extended to another betacoronavirus HCoV OC43, but not alphacoronavirus HCoV 229E. Our cellular screening results add to the body of knowledge on antivirals against coronaviruses and confirm the antiviral efficacy of iminosugars in cellular assays using the human lung-cell line Calu-3., 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 © 2025 The Authors. Published by Elsevier B.V. All rights reserved.)

Published

2025

8. Open science discovery of potent noncovalent SARS-CoV-2 main protease inhibitors.

Author

Boby ML, Fearon D, Ferla M, Filep M, Koekemoer L, Robinson MC, Chodera JD, Lee AA, London N, von Delft A, von Delft F, Achdout H, Aimon A, Alonzi DS, Arbon R, Aschenbrenner JC, Balcomb BH, Bar-David E, Barr H, Ben-Shmuel A, Bennett J, Bilenko VA, Borden B, Boulet P, Bowman GR, Brewitz L, Brun J, Bvnbs S, Calmiano M, Carbery A, Carney DW, Cattermole E, Chang E, Chernyshenko E, Clyde A, Coffland JE, Cohen G, Cole JC, Contini A, Cox L, Croll TI, Cvitkovic M, De Jonghe S, Dias A, Donckers K, Dotson DL, Douangamath A, Duberstein S, Dudgeon T, Dunnett LE, Eastman P, Erez N, Eyermann CJ, Fairhead M, Fate G, Fedorov O, Fernandes RS, Ferrins L, Foster R, Foster H, Fraisse L, Gabizon R, García-Sastre A, Gawriljuk VO, Gehrtz P, Gileadi C, Giroud C, Glass WG, Glen RC, Glinert I, Godoy AS, Gorichko M, Gorrie-Stone T, Griffen EJ, Haneef A, Hassell Hart S, Heer J, Henry M, Hill M, Horrell S, Huang QYJ, Huliak VD, Hurley MFD, Israely T, Jajack A, Jansen J, Jnoff E, Jochmans D, John T, Kaminow B, Kang L, Kantsadi AL, Kenny PW, Kiappes JL, Kinakh SO, Kovar B, Krojer T, La VNT, Laghnimi-Hahn S, Lefker BA, Levy H, Lithgo RM, Logvinenko IG, Lukacik P, Macdonald HB, MacLean EM, Makower LL, Malla TR, Marples PG, Matviiuk T, McCorkindale W, McGovern BL, Melamed S, Melnykov KP, Michurin O, Miesen P, Mikolajek H, Milne BF, Minh D, Morris A, Morris GM, Morwitzer MJ, Moustakas D, Mowbray CE, Nakamura AM, Neto JB, Neyts J, Nguyen L, Noske GD, Oleinikovas V, Oliva G, Overheul GJ, Owen CD, Pai R, Pan J, Paran N, Payne AM, Perry B, Pingle M, Pinjari J, Politi B, Powell A, Pšenák V, Pulido I, Puni R, Rangel VL, Reddi RN, Rees P, Reid SP, Reid L, Resnick E, Ripka EG, Robinson RP, Rodriguez-Guerra J, Rosales R, Rufa DA, Saar K, Saikatendu KS, Salah E, Schaller D, Scheen J, Schiffer CA, Schofield CJ, Shafeev M, Shaikh A, Shaqra AM, Shi J, Shurrush K, Singh S, Sittner A, Sjö P, Skyner R, Smalley A, Smeets B, Smilova MD, Solmesky LJ, Spencer J, Strain-Damerell C, Swamy V, Tamir H, Taylor JC, Tennant RE, Thompson W, Thompson A, Tomásio S, Tomlinson CWE, Tsurupa IS, Tumber A, Vakonakis I, van Rij RP, Vangeel L, Varghese FS, Vaschetto M, Vitner EB, Voelz V, Volkamer A, Walsh MA, Ward W, Weatherall C, Weiss S, White KM, Wild CF, Witt KD, Wittmann M, Wright N, Yahalom-Ronen Y, Yilmaz NK, Zaidmann D, Zhang I, Zidane H, Zitzmann N, and Zvornicanin SN

Subjects

Humans, Molecular Docking Simulation, Structure-Activity Relationship, Crystallography, X-Ray, Coronavirus 3C Proteases antagonists & inhibitors, Coronavirus 3C Proteases chemistry, SARS-CoV-2, Drug Discovery, Coronavirus Protease Inhibitors chemical synthesis, Coronavirus Protease Inhibitors chemistry, Coronavirus Protease Inhibitors pharmacology, COVID-19 Drug Treatment

Abstract

We report the results of the COVID Moonshot, a fully open-science, crowdsourced, and structure-enabled drug discovery campaign targeting the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) main protease. We discovered a noncovalent, nonpeptidic inhibitor scaffold with lead-like properties that is differentiated from current main protease inhibitors. Our approach leveraged crowdsourcing, machine learning, exascale molecular simulations, and high-throughput structural biology and chemistry. We generated a detailed map of the structural plasticity of the SARS-CoV-2 main protease, extensive structure-activity relationships for multiple chemotypes, and a wealth of biochemical activity data. All compound designs (>18,000 designs), crystallographic data (>490 ligand-bound x-ray structures), assay data (>10,000 measurements), and synthesized molecules (>2400 compounds) for this campaign were shared rapidly and openly, creating a rich, open, and intellectual property-free knowledge base for future anticoronavirus drug discovery.

Published

2023

9. A quinolin-8-ol sub-millimolar inhibitor of UGGT, the ER glycoprotein folding quality control checkpoint.

Author

Guay KP, Ibba R, Kiappes JL, Vasiljević S, Bonì F, De Benedictis M, Zeni I, Le Cornu JD, Hensen M, Chandran AV, Kantsadi AL, Caputo AT, Blanco Capurro JI, Bayo Y, Hill JC, Hudson K, Lia A, Brun J, Withers SG, Martí M, Biasini E, Santino A, De Rosa M, Milani M, Modenutti CP, Hebert DN, Zitzmann N, and Roversi P

Abstract

Misfolded glycoprotein recognition and endoplasmic reticulum (ER) retention are mediated by the ER glycoprotein folding quality control (ERQC) checkpoint enzyme, UDP-glucose glycoprotein glucosyltransferase (UGGT). UGGT modulation is a promising strategy for broad-spectrum antivirals, rescue-of-secretion therapy in rare disease caused by responsive mutations in glycoprotein genes, and many cancers, but to date no selective UGGT inhibitors are known. The small molecule 5-[(morpholin-4-yl)methyl]quinolin-8-ol (5M-8OH-Q) binds a Ct UGGT GT24 "WY" conserved surface motif conserved across UGGTs but not present in other GT24 family glycosyltransferases. 5M-8OH-Q has a 47 μM binding affinity for Ct UGGT GT24 in vitro as measured by ligand-enhanced fluorescence. In cellula , 5M-8OH-Q inhibits both human UGGT isoforms at concentrations higher than 750 μM. 5M-8OH-Q binding to Ct UGGT GT24 appears to be mutually exclusive to M5-9 glycan binding in an in vitro competition experiment. A medicinal program based on 5M-8OH-Q will yield the next generation of UGGT inhibitors., Competing Interests: The authors declare no competing interests., (© 2023 The Author(s).)

Published

2023

10. N-Substituted Valiolamine Derivatives as Potent Inhibitors of Endoplasmic Reticulum α-Glucosidases I and II with Antiviral Activity.

Author

Karade SS, Hill ML, Kiappes JL, Manne R, Aakula B, Zitzmann N, Warfield KL, Treston AM, and Mariuzza RA

Subjects

Animals, Antiviral Agents chemical synthesis, Antiviral Agents metabolism, Binding Sites, Chlorocebus aethiops, Crystallography, X-Ray, Dengue Virus drug effects, Endoplasmic Reticulum enzymology, Glycoside Hydrolase Inhibitors chemical synthesis, Glycoside Hydrolase Inhibitors metabolism, Humans, Imino Sugars chemical synthesis, Imino Sugars metabolism, Inositol chemical synthesis, Inositol metabolism, Inositol pharmacology, Mice, Microbial Sensitivity Tests, Molecular Docking Simulation, Protein Binding, SARS-CoV-2 drug effects, Vero Cells, alpha-Glucosidases chemistry, Antiviral Agents pharmacology, Glycoside Hydrolase Inhibitors pharmacology, Imino Sugars pharmacology, Inositol analogs & derivatives, alpha-Glucosidases metabolism

Abstract

Most enveloped viruses rely on the host cell endoplasmic reticulum (ER) quality control (QC) machinery for proper folding of glycoproteins. The key ER α-glucosidases (α-Glu) I and II of the ERQC machinery are attractive targets for developing broad-spectrum antivirals. Iminosugars based on deoxynojirimycin have been extensively studied as ER α-glucosidase inhibitors; however, other glycomimetic compounds are less established. Accordingly, we synthesized a series of N-substituted derivatives of valiolamine, the iminosugar scaffold of type 2 diabetes drug voglibose. To understand the basis for up to 100,000-fold improved inhibitory potency, we determined high-resolution crystal structures of mouse ER α-GluII in complex with valiolamine and 10 derivatives. The structures revealed extensive interactions with all four α-GluII subsites. We further showed that N-substituted valiolamines were active against dengue virus and SARS-CoV-2 in vitro . This study introduces valiolamine-based inhibitors of the ERQC machinery as candidates for developing potential broad-spectrum therapeutics against the existing and emerging viruses.

Published

2021

11. Assessing Antigen Structural Integrity through Glycosylation Analysis of the SARS-CoV-2 Viral Spike.

Author

Brun J, Vasiljevic S, Gangadharan B, Hensen M, V Chandran A, Hill ML, Kiappes JL, Dwek RA, Alonzi DS, Struwe WB, and Zitzmann N

Abstract

Severe acute respiratory syndrome coronavirus 2 is the causative pathogen of the COVID-19 pandemic which as of March 29, 2021, has claimed 2 776 175 lives worldwide. Vaccine development efforts focus on the viral trimeric spike glycoprotein as the main target of the humoral immune response. Viral spikes carry glycans that facilitate immune evasion by shielding specific protein epitopes from antibody neutralization, and antigen efficacy is influenced by spike glycoprotein production in vivo. Therefore, immunogen integrity is important for glycoprotein-based vaccine candidates. Here, we show how site-specific glycosylation differs between virus-derived spikes, wild-type, non-stabilized spikes expressed from a plasmid with a CMV promoter and tPA signal sequence, and commonly used recombinant, engineered spike glycoproteins. Furthermore, we show that their distinctive cellular secretion pathways result in different protein glycosylation and secretion patterns, including shedding of spike monomeric subunits for the non-stabilized wild-type spike tested, which may have implications for the resulting immune response and vaccine design., Competing Interests: The authors declare the following competing financial interest(s): W.B.S. is a shareholder and consultant to Refeyn Ltd. All other authors declare no conflict of interest., (© 2021 The Authors. Published by American Chemical Society.)

Published

2021

12. ToP-DNJ, a Selective Inhibitor of Endoplasmic Reticulum α-Glucosidase II Exhibiting Antiflaviviral Activity.

Author

Kiappes JL, Hill ML, Alonzi DS, Miller JL, Iwaki R, Sayce AC, Caputo AT, Kato A, and Zitzmann N

Subjects

1-Deoxynojirimycin chemistry, Administration, Oral, Animals, Antiviral Agents chemical synthesis, Dengue Virus drug effects, Glycoside Hydrolase Inhibitors administration & dosage, Glycoside Hydrolase Inhibitors chemistry, HL-60 Cells, Hepacivirus drug effects, Humans, Inhibitory Concentration 50, Liver drug effects, Male, Mice, Inbred BALB C, Rats, Tissue Distribution, Tocopherols chemistry, alpha-Glucosidases metabolism, Antiviral Agents chemistry, Antiviral Agents pharmacology, Endoplasmic Reticulum enzymology, Glycoside Hydrolase Inhibitors pharmacology

Abstract

Iminosugars have therapeutic potential against a range of diseases, due to their efficacy as glycosidase inhibitors. A major challenge in the development of iminosugar drugs lies in making a compound that is selective for the glycosidase associated with a given disease. We report the synthesis of ToP-DNJ, an antiviral iminosugar-tocopherol conjugate. Tocopherol was incorporated into the design of the iminosugar in order to direct the drug to the liver and immune cells, specific tissues of interest for antiviral therapy. ToP-DNJ inhibits ER α-glucosidase II at low micromolar concentrations and selectively accumulates in the liver in vivo. In cellular assays, the drug showed efficacy exclusively in immune cells of the myeloid lineage. Taken together, these data demonstrate that inclusion of a native metabolite into an iminosugar provides selectivity with respect to target enzyme, target cell, and target tissue.

Published

2018

13. Structural Insights into the Broad-Spectrum Antiviral Target Endoplasmic Reticulum Alpha-Glucosidase II.

Author

Caputo AT, Alonzi DS, Kiappes JL, Struwe WB, Cross A, Basu S, Darlot B, Roversi P, and Zitzmann N

Subjects

Animals, Endoplasmic Reticulum genetics, Endoplasmic Reticulum immunology, Endoplasmic Reticulum virology, Host-Pathogen Interactions, Humans, Virus Diseases genetics, Virus Diseases virology, Viruses genetics, alpha-Glucosidases genetics, Endoplasmic Reticulum enzymology, Virus Diseases enzymology, Virus Diseases immunology, Virus Physiological Phenomena, alpha-Glucosidases chemistry, alpha-Glucosidases immunology

Abstract

Targeting the host-cell endoplasmic reticulum quality control (ERQC) pathway is an effective broad-spectrum antiviral strategy. The two ER resident α-glucosidases whose sequential action permits entry in this pathway are the targets of glucomimetic inhibitors. Knowledge of the molecular details of the ER α-glucosidase II (α-Glu II) structure was limited. We determined crystal structures of a trypsinolytic fragment of murine α-Glu II, alone and in complex with key catalytic cycle ligands, and four different broad-spectrum antiviral iminosugar inhibitors, two of which are currently in clinical trials against dengue fever. The structures highlight novel portions of the enzyme outside its catalytic pocket which contribute to its activity and substrate specificity. These crystal structures and hydrogen-deuterium exchange mass spectrometry of the murine ER alpha glucosidase II heterodimer uncover the quaternary arrangement of the enzyme's α- and β-subunits, and suggest a conformational rearrangement of ER α-Glu II upon association of the enzyme with client glycoproteins.

Published

2018

14. Essential chemistry for biochemists.

Author

Jonsson AL, Roberts MAJ, Kiappes JL, and Scott KA

Subjects

Animals, Biochemistry education, Humans, Organic Chemicals metabolism, Biochemistry methods, Metabolome, Organic Chemicals chemistry, Organic Chemistry Phenomena

Abstract

Within every living organism, countless reactions occur every second. These reactions typically occur more rapidly and with greater efficiency than would be possible under the same conditions in the chemical laboratory, and while using only the subset of elements that are readily available in nature. Despite these apparent differences between life and the laboratory, biological reactions are governed by the same rules as any other chemical reaction. Thus, a firm understanding of the fundamentals of chemistry is invaluable in biochemistry. There are entire textbooks devoted to the application of chemical principles in biological systems and so it is not possible to cover all of the relevant topics in depth in this short article. The aim is instead to provide a brief overview of those areas in chemistry that are most relevant to biochemistry. We summarize the basic principles, give examples of how these principles are applied in biological systems and suggest further reading on individual topics., (© 2017 The Author(s).)

Published

2017

15. Structures of mammalian ER α-glucosidase II capture the binding modes of broad-spectrum iminosugar antivirals.

Author

Caputo AT, Alonzi DS, Marti L, Reca IB, Kiappes JL, Struwe WB, Cross A, Basu S, Lowe ED, Darlot B, Santino A, Roversi P, and Zitzmann N

Subjects

Animals, Catalysis, Crystallography, X-Ray, Mice, Protein Conformation, Protein Subunits, Scattering, Small Angle, Substrate Specificity, Antiviral Agents pharmacology, Endoplasmic Reticulum enzymology, Glycoside Hydrolase Inhibitors pharmacology, alpha-Glucosidases chemistry

Abstract

The biosynthesis of enveloped viruses depends heavily on the host cell endoplasmic reticulum (ER) glycoprotein quality control (QC) machinery. This dependency exceeds the dependency of host glycoproteins, offering a window for the targeting of ERQC for the development of broad-spectrum antivirals. We determined small-angle X-ray scattering (SAXS) and crystal structures of the main ERQC enzyme, ER α-glucosidase II (α-GluII; from mouse), alone and in complex with key ligands of its catalytic cycle and antiviral iminosugars, including two that are in clinical trials for the treatment of dengue fever. The SAXS data capture the enzyme's quaternary structure and suggest a conformational rearrangement is needed for the simultaneous binding of a monoglucosylated glycan to both subunits. The X-ray structures with key catalytic cycle intermediates highlight that an insertion between the +1 and +2 subsites contributes to the enzyme's activity and substrate specificity, and reveal that the presence of d-mannose at the +1 subsite renders the acid catalyst less efficient during the cleavage of the monoglucosylated substrate. The complexes with iminosugar antivirals suggest that inhibitors targeting a conserved ring of aromatic residues between the α-GluII +1 and +2 subsites would have increased potency and selectivity, thus providing a template for further rational drug design.

Published

2016

16. Inhibition of endoplasmic reticulum glucosidases is required for in vitro and in vivo dengue antiviral activity by the iminosugar UV-4.

Author

Warfield KL, Plummer EM, Sayce AC, Alonzi DS, Tang W, Tyrrell BE, Hill ML, Caputo AT, Killingbeck SS, Beatty PR, Harris E, Iwaki R, Kinami K, Ide D, Kiappes JL, Kato A, Buck MD, King K, Eddy W, Khaliq M, Sampath A, Treston AM, Dwek RA, Enterlein SG, Miller JL, Zitzmann N, Ramstedt U, and Shresta S

Subjects

1-Deoxynojirimycin administration & dosage, 1-Deoxynojirimycin pharmacology, 1-Deoxynojirimycin therapeutic use, Animals, Antibodies, Viral blood, Antibody-Dependent Enhancement drug effects, Antiviral Agents administration & dosage, Antiviral Agents therapeutic use, Cells, Cultured, Chlorocebus aethiops, Clinical Trials as Topic, Disease Models, Animal, Drugs, Investigational, Endoplasmic Reticulum drug effects, Endoplasmic Reticulum enzymology, Glycoside Hydrolase Inhibitors administration & dosage, Glycoside Hydrolase Inhibitors chemistry, Glycoside Hydrolase Inhibitors therapeutic use, Humans, Inhibitory Concentration 50, Mice, Monocytes virology, Receptors, Interferon deficiency, Serogroup, Severe Dengue virology, Vero Cells, 1-Deoxynojirimycin analogs & derivatives, Antiviral Agents pharmacology, Dengue Virus drug effects, Glycoside Hydrolase Inhibitors pharmacology, Severe Dengue drug therapy, alpha-Glucosidases metabolism

Abstract

The antiviral activity of UV-4 was previously demonstrated against dengue virus serotype 2 (DENV2) in multiple mouse models. Herein, step-wise minimal effective dose and therapeutic window of efficacy studies of UV-4B (UV-4 hydrochloride salt) were conducted in an antibody-dependent enhancement (ADE) mouse model of severe DENV2 infection in AG129 mice lacking types I and II interferon receptors. Significant survival benefit was demonstrated with 10-20 mg/kg of UV-4B administered thrice daily (TID) for seven days with initiation of treatment up to 48 h after infection. UV-4B also reduced infectious virus production in in vitro antiviral activity assays against all four DENV serotypes, including clinical isolates. A set of purified enzyme, in vitro, and in vivo studies demonstrated that inhibition of endoplasmic reticulum (ER) α-glucosidases and not the glycosphingolipid pathway appears to be responsible for the antiviral activity of UV-4B against DENV. Along with a comprehensive safety package, these and previously published data provided support for an Investigational New Drug (IND) filing and Phases 1 and 2 clinical trials for UV-4B with an indication of acute dengue disease., (Copyright © 2016 The Authors. Published by Elsevier B.V. All rights reserved.)

Published

2016

17. Isolation and SAR studies of bicyclic iminosugars from Castanospermum australe as glycosidase inhibitors.

Author

Kato A, Hirokami Y, Kinami K, Tsuji Y, Miyawaki S, Adachi I, Hollinshead J, Nash RJ, Kiappes JL, Zitzmann N, Cha JK, Molyneux RJ, Fleet GW, and Asano N

Subjects

1-Deoxynojirimycin analogs & derivatives, 1-Deoxynojirimycin chemistry, 1-Deoxynojirimycin pharmacology, Alkaloids chemistry, Enzyme Inhibitors chemistry, Glucosamine analogs & derivatives, Glucosamine chemistry, Hypoglycemic Agents chemistry, Hypoglycemic Agents pharmacology, Imino Sugars chemistry, Indolizines chemistry, Piperidines pharmacology, Stereoisomerism, Structure-Activity Relationship, Alkaloids isolation & purification, Alkaloids pharmacology, Castanospermum chemistry, Enzyme Inhibitors isolation & purification, Enzyme Inhibitors pharmacology, Glycoside Hydrolases antagonists & inhibitors, Imino Sugars isolation & purification, Imino Sugars pharmacology, Indolizines isolation & purification, Indolizines pharmacology

Abstract

We report the isolation and structural determination of fourteen iminosugars, containing five pyrrolizidines and five indolizidines, from Castanospermum australe. The structure of a new alkaloid was elucidated by spectroscopic methods as 6,8-diepi-castanospermine (13). Our side-by-side comparison between bicyclic and corresponding monocyclic iminosugars revealed that inhibition potency and spectrum against each enzyme are clearly changed by their core structures. Castanospermine (10) and 1-deoxynojirimycin (DNJ) have a common d-gluco configuration, and they showed the expected similar inhibition potency and spectrum. In sharp contrast, 6-epi-castanospermine (12) and 1-deoxymannojirimycin (manno-DNJ) both have the d-manno configuration but the α-mannosidase inhibition of 6-epi-castanospermine (12) was much better than that of manno-DNJ. 6,8-Diepi-castanospermine (13) could be regarded as a bicyclic derivative of talo-DNJ, but it showed a complete loss of α-galactosidase A inhibition. This behavior against α-galactosidase A is similar to that observed for 1-epi-australine (6) and altro-DMDP., (Copyright © 2014 Elsevier Ltd. All rights reserved.)

Published

2015

18. Synthesis of the carboline disaccharide domain of shishijimicin A.

Author

Nicolaou KC, Kiappes JL, Tian W, Gondi VB, and Becker J

Subjects

Disaccharides chemistry, Fluorides chemistry, Molecular Structure, Carbolines chemistry, Disaccharides chemical synthesis, Enediynes chemistry

Abstract

A synthetic route to the carboline disaccharide domain (2) of shishijimicin A (1) has been developed. The convergent synthesis relies on a novel application of the Reetz-Müller-Starke reaction to form the central, sulfur-bearing quaternary carbon center and addition of the carboline structural motif as a dianion to a disaccharide aldehyde fragment., (© 2011 American Chemical Society)

Published

2011

19. Synthesis of fluorescent dye-tagged nanomachines for single-molecule fluorescence spectroscopy.

Author

Vives G, Guerrero JM, Godoy J, Khatua S, Wang YP, Kiappes JL, Link S, and Tour JM

Subjects

Fluorescent Dyes chemistry, Molecular Structure, Rhodamines chemistry, Spectrometry, Fluorescence, Stereoisomerism, Fluorescent Dyes chemical synthesis, Nanostructures chemistry

Abstract

In an effort to elucidate the mechanism of movement of nanovehicles on nonconducting surfaces, the synthesis and optical properties of five fluorescently tagged nanocars are reported. The nanocars were specifically designed for studies by single-molecule fluorescence spectroscopy and bear a tetramethylrhodamine isothiocyanate fluorescent tag for excitation at 532 nm. The molecules were designed such that the arrangement of their molecular axles and p-carborane wheels relative to the chassis would be conducive to the control of directionality in the motion of these nanovehicles.

Published

2010

20. Synthesis of a porphyrin-fullerene pinwheel.

Author

Sasaki T, Osgood AJ, Kiappes JL, Kelly KF, and Tour JM

Abstract

We disclose the synthesis of a porphyrin-fullerene pinwheel that was subsequently observed by scanning tunneling microscopy. The molecule was designed to further our understanding of fullerene-surface interactions, directional control, and surface-rolling versus pivoting capabilities of this class of nanomachines. The inner porphyrin provides the square planar configuration that might lead to realization of the pinwheel spiraling motion on surfaces.

Published

2008