Your search keyword '"Bogdan I. Florea"' showing total 194 results

1. The proteasome modulates endocytosis specifically in glomerular cells to promote kidney filtration

Author

Wiebke Sachs, Lukas Blume, Desiree Loreth, Lisa Schebsdat, Favian Hatje, Sybille Koehler, Uta Wedekind, Marlies Sachs, Stephanie Zieliniski, Johannes Brand, Christian Conze, Bogdan I. Florea, Frank Heppner, Elke Krüger, Markus M. Rinschen, Oliver Kretz, Roland Thünauer, and Catherine Meyer-Schwesinger

Subjects

Science

Abstract

Abstract Kidney filtration is ensured by the interaction of podocytes, endothelial and mesangial cells. Immunoglobulin accumulation at the filtration barrier is pathognomonic for glomerular injury. The mechanisms that regulate filter permeability are unknown. Here, we identify a pivotal role for the proteasome in a specific cell type. Combining genetic and inhibitor-based human, pig, mouse, and Drosophila models we demonstrate that the proteasome maintains filtration barrier integrity, with podocytes requiring the constitutive and glomerular endothelial cells the immunoproteasomal activity. Endothelial immunoproteasome deficiency as well as proteasome inhibition disrupt the filtration barrier in mice, resulting in pathologic immunoglobulin deposition. Mechanistically, we observe reduced endocytic activity, which leads to altered membrane recycling and endocytic receptor turnover. This work expands the concept of the (immuno)proteasome as a control protease orchestrating protein degradation and antigen presentation and endocytosis, providing new therapeutic targets to treat disease-associated glomerular protein accumulations.

Published

2024

2. A monoacylglycerol lipase inhibitor showing therapeutic efficacy in mice without central side effects or dependence

Author

Ming Jiang, Mirjam C. W. Huizenga, Jonah L. Wirt, Janos Paloczi, Avand Amedi, Richard J. B. H. N. van den Berg, Joerg Benz, Ludovic Collin, Hui Deng, Xinyu Di, Wouter F. Driever, Bogdan I. Florea, Uwe Grether, Antonius P. A. Janssen, Thomas Hankemeier, Laura H. Heitman, Tsang-Wai Lam, Florian Mohr, Anto Pavlovic, Iris Ruf, Helma van den Hurk, Anna F. Stevens, Daan van der Vliet, Tom van der Wel, Matthias B. Wittwer, Constant A. A. van Boeckel, Pal Pacher, Andrea G. Hohmann, and Mario van der Stelt

Subjects

Science

Abstract

Abstract Monoacylglycerol lipase (MAGL) regulates endocannabinoid 2-arachidonoylglycerol (2-AG) and eicosanoid signalling. MAGL inhibition provides therapeutic opportunities but clinical potential is limited by central nervous system (CNS)-mediated side effects. Here, we report the discovery of LEI-515, a peripherally restricted, reversible MAGL inhibitor, using high throughput screening and a medicinal chemistry programme. LEI-515 increased 2-AG levels in peripheral organs, but not mouse brain. LEI-515 attenuated liver necrosis, oxidative stress and inflammation in a CCl4-induced acute liver injury model. LEI-515 suppressed chemotherapy-induced neuropathic nociception in mice without inducing cardinal signs of CB1 activation. Antinociceptive efficacy of LEI-515 was blocked by CB2, but not CB1, antagonists. The CB1 antagonist rimonabant precipitated signs of physical dependence in mice treated chronically with a global MAGL inhibitor (JZL184), and an orthosteric cannabinoid agonist (WIN55,212-2), but not with LEI-515. Our data support targeting peripheral MAGL as a promising therapeutic strategy for developing safe and effective anti-inflammatory and analgesic agents.

Published

2023

3. Genetic ablation of Lmp2 increases the susceptibility for impaired cardiac function

Author

Felix A. Trogisch, Franziska Koser, Synje Michel, David A. Liem, Bogdan I. Florea, Markus Hecker, and Oliver Drews

Subjects

proteostasis, ubiquitin-proteasome system, cardiac remodeling, heart failure, proteasome intervention, adverse cardiac effects, Biology (General), QH301-705.5

Abstract

Proteasome degradation is an integral part of cellular growth and function. Proteasomal intervention may mitigate adverse myocardial remodeling, but is associated with the onset of heart failure. Previously, we have demonstrated that increasing abundance of cardiac Lmp2 and its incorporation into proteasome complexes is an endogenous mechanism for proteasome regulation during hypertrophic remodeling of the heart induced by chronic ß-adrenoreceptor stimulation. Here, we investigated whether Lmp2 is required for myocardial remodeling not driven by inflammation and show that Lmp2 is a tipping element for growth and function in the heart but not for proteasome insufficiency. While it has no apparent impact under unchallenged conditions, myocardial remodeling without Lmp2 exacerbates hypertrophy and restricts cardiac function. Under chronic ß-adrenoreceptor stimulation, as seen in the development of cardiovascular disease and the manifestation of heart failure, genetic ablation of Lmp2 in mice caused augmented concentric hypertrophy of the left ventricle. While the heart rate was similarly elevated as in wildtype, myocardial contractility was not maintained without Lmp2, and apparently uncoupled of the ß-adrenergic response. Normalized to the exacerbated myocardial mass, contractility was reduced by 41% of the pretreatment level, but would appear preserved at absolute level. The lack of Lmp2 interfered with elevated 26S proteasome activities during early cardiac remodeling reported previously, but did not cause bulk proteasome insufficiency, suggesting the Lmp2 containing proteasome subpopulation is required for a selected group of proteins to be degraded. In the myocardial interstitium, augmented collagen deposition suggested matrix stiffening in the absence of Lmp2. Indeed, echocardiography of left ventricular peak relaxation velocity (circumferential strain rate) was reduced in this treatment group. Overall, targeting Lmp2 in a condition mimicking chronic ß-adrenoreceptor stimulation exhibited the onset of heart failure. Anticancer therapy inhibiting proteasome activity, including Lmp2, is associated with adverse cardiac events, in particular heart failure. Sparing Lmp2 may be an avenue to reduce adverse cardiac events when chronic sympathetic nervous system activation cannot be excluded.

Published

2024

4. Non-functional ubiquitin C-terminal hydrolase L1 drives podocyte injury through impairing proteasomes in autoimmune glomerulonephritis

Author

Julia Reichelt, Wiebke Sachs, Sarah Frömbling, Julia Fehlert, Maja Studencka-Turski, Anna Betz, Desiree Loreth, Lukas Blume, Susanne Witt, Sandra Pohl, Johannes Brand, Maire Czesla, Jan Knop, Bogdan I. Florea, Stephanie Zielinski, Marlies Sachs, Elion Hoxha, Irm Hermans-Borgmeyer, Gunther Zahner, Thorsten Wiech, Elke Krüger, and Catherine Meyer-Schwesinger

Subjects

Science

Abstract

Abstract Little is known about the mechanistic significance of the ubiquitin proteasome system (UPS) in a kidney autoimmune environment. In membranous nephropathy (MN), autoantibodies target podocytes of the glomerular filter resulting in proteinuria. Converging biochemical, structural, mouse pathomechanistic, and clinical information we report that the deubiquitinase Ubiquitin C-terminal hydrolase L1 (UCH-L1) is induced by oxidative stress in podocytes and is directly involved in proteasome substrate accumulation. Mechanistically, this toxic gain-of-function is mediated by non-functional UCH-L1, which interacts with and thereby impairs proteasomes. In experimental MN, UCH-L1 becomes non-functional and MN patients with poor outcome exhibit autoantibodies with preferential reactivity to non-functional UCH-L1. Podocyte-specific deletion of UCH-L1 protects from experimental MN, whereas overexpression of non-functional UCH-L1 impairs podocyte proteostasis and drives injury in mice. In conclusion, the UPS is pathomechanistically linked to podocyte disease by aberrant proteasomal interactions of non-functional UCH-L1.

Published

2023

5. Publisher Correction: Non-functional ubiquitin C-terminal hydrolase L1 drives podocyte injury through impairing proteasomes in autoimmune glomerulonephritis

Author

Julia Reichelt, Wiebke Sachs, Sarah Frömbling, Julia Fehlert, Maja Studencka-Turski, Anna Betz, Desiree Loreth, Lukas Blume, Susanne Witt, Sandra Pohl, Johannes Brand, Maire Czesla, Jan Knop, Bogdan I. Florea, Stephanie Zielinski, Marlies Sachs, Elion Hoxha, Irm Hermans-Borgmeyer, Gunther Zahner, Thorsten Wiech, Elke Krüger, and Catherine Meyer-Schwesinger

Subjects

Science

Published

2023

6. Chemical genetics strategy to profile kinase target engagement reveals role of FES in neutrophil phagocytosis

Author

Tom van der Wel, Riet Hilhorst, Hans den Dulk, Tim van den Hooven, Nienke M. Prins, Joost A. P. M. Wijnakker, Bogdan I. Florea, Eelke B. Lenselink, Gerard J. P. van Westen, Rob Ruijtenbeek, Herman S. Overkleeft, Allard Kaptein, Tjeerd Barf, and Mario van der Stelt

Subjects

Science

Abstract

Chemical tools to monitor drug-target engagement of endogenous enzymes are essential for preclinical target validation. Here, the authors present a chemical genetics strategy to study target engagement of endogenous kinases, achieving specific labeling and inactivation of FES kinase to provide insights into FES’ role in neutrophil phagocytosis.

Published

2020

7. Unbiased Identification of the Liposome Protein Corona using Photoaffinity-based Chemoproteomics

Author

Roy Pattipeiluhu, Stefan Crielaard, Iris Klein-Schiphorst, Bogdan I. Florea, Alexander Kros, and Frederick Campbell

Subjects

Chemistry, QD1-999

Published

2020

8. Development of a Retinal-Based Probe for the Profiling of Retinaldehyde Dehydrogenases in Cancer Cells

Author

Sebastiaan T. A. Koenders, Lukas S. Wijaya, Martje N. Erkelens, Alexander T. Bakker, Vera E. van der Noord, Eva J. van Rooden, Lindsey Burggraaff, Pasquale C. Putter, Else Botter, Kim Wals, Hans van den Elst, Hans den Dulk, Bogdan I. Florea, Bob van de Water, Gerard J. P. van Westen, Reina E. Mebius, Herman S. Overkleeft, Sylvia E. Le Dévédec, and Mario van der Stelt

Subjects

Chemistry, QD1-999

Published

2019

9. Dynamic and Functional Profiling of Xylan-Degrading Enzymes in Aspergillus Secretomes Using Activity-Based Probes

Author

Sybrin P. Schröder, Casper de Boer, Nicholas G. S. McGregor, Rhianna J. Rowland, Olga Moroz, Elena Blagova, Jos Reijngoud, Mark Arentshorst, David Osborn, Marc D. Morant, Eric Abbate, Mary A. Stringer, Kristian B. R. M. Krogh, Lluís Raich, Carme Rovira, Jean-Guy Berrin, Gilles P. van Wezel, Arthur F. J. Ram, Bogdan I. Florea, Gijsbert A. van der Marel, Jeroen D. C. Codée, Keith S. Wilson, Liang Wu, Gideon J. Davies, and Herman S. Overkleeft

Subjects

Chemistry, QD1-999

Published

2019

10. Identification of α,β-Hydrolase Domain Containing Protein 6 as a Diacylglycerol Lipase in Neuro-2a Cells

Author

Annelot C. M. van Esbroeck, Vasudev Kantae, Xinyu Di, Tom van der Wel, Hans den Dulk, Anna F. Stevens, Simar Singh, Alexander T. Bakker, Bogdan I. Florea, Nephi Stella, Herman S. Overkleeft, Thomas Hankemeier, and Mario van der Stelt

Subjects

α, β-hydrolase domain containing protein 6, diacylglycerol lipase, 2-AG, endocannabinoids, lipidomics, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

The endocannabinoid 2-arachidonoylglycerol (2-AG) is involved in neuronal differentiation. This study aimed to identify the biosynthetic enzymes responsible for 2-AG production during retinoic acid (RA)-induced neurite outgrowth of Neuro-2a cells. First, we confirmed that RA stimulation of Neuro-2a cells increases 2-AG production and neurite outgrowth. The diacylglycerol lipase (DAGL) inhibitor DH376 blocked 2-AG production and reduced neuronal differentiation. Surprisingly, CRISPR/Cas9-mediated knockdown of DAGLα and DAGLβ in Neuro-2a cells did not reduce 2-AG levels, suggesting another enzyme capable of producing 2-AG in this cell line. Chemical proteomics revealed DAGLβ and α,β-hydrolase domain containing protein (ABHD6) as the only targets of DH376 in Neuro-2a cells. Biochemical, genetic and lipidomic studies demonstrated that ABHD6 possesses DAGL activity in conjunction with its previously reported monoacylglycerol lipase activity. RA treatment of Neuro-2a cells increased by three-fold the amount of active ABHD6. Our study shows that ABHD6 exhibits significant DAG lipase activity in Neuro-2a cells in addition to its known MAG lipase activity and suggest it is involved in neuronal differentiation.

Published

2019

11. Visualizing Proteasome Activity and Intracellular Localization Using Fluorescent Proteins and Activity-Based Probes

Author

Sabine Schipper-Krom, Alicia Sanz Sanz, Emma J. van Bodegraven, Dave Speijer, Bogdan I. Florea, Huib Ovaa, and Eric A. Reits

Subjects

proteasome, dynamics, fluorescence, activity probes, living cells, Biology (General), QH301-705.5

Abstract

The proteasome is a multi-catalytic molecular machine that plays a key role in the degradation of many cytoplasmic and nuclear proteins. The proteasome is essential and proteasome malfunction is associated with various disease pathologies. Proteasome activity depends on its catalytic subunits which are interchangeable and also on the interaction with the associated regulatory cap complexes. Here, we describe and compare various methods that allow the study of proteasome function in living cells. Methods include the use of fluorescently tagged proteasome subunits and the use of activity-based proteasome probes. These probes can be used in both biochemical assays and in microscopy-based experiments. Together with tagged proteasomes, they can be used to study proteasome localization, dynamics, and activity.

Published

2019

12. Detection of Active Mammalian GH31 α‑Glucosidases in Health and Disease Using In-Class, Broad-Spectrum Activity-Based Probes

Author

Jianbing Jiang, Chi-Lin Kuo, Liang Wu, Christian Franke, Wouter W. Kallemeijn, Bogdan I. Florea, Eline van Meel, Gijsbert A. van der Marel, Jeroen D. C. Codée, Rolf G. Boot, Gideon J. Davies, Herman S. Overkleeft, and Johannes M. F. G. Aerts

Subjects

Chemistry, QD1-999

Published

2016

13. C-Terminal Extensions of Ku70 and Ku80 Differentially Influence DNA End Binding Properties

Author

Takabumi Inagawa, Thomas Wennink, Joyce H. G. Lebbink, Guido Keijzers, Bogdan I. Florea, Nicole S. Verkaik, and Dik C. van Gent

Subjects

DNA repair, non-homologous end-joining, DNA-PK, DNA binding, surface plasmon resonance (SPR), Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

The Ku70/80 heterodimer binds to DNA ends and attracts other proteins involved in the non-homologous end-joining (NHEJ) pathway of DNA double-strand break repair. We developed a novel assay to measure DNA binding and release kinetics using differences in Förster resonance energy transfer (FRET) of the ECFP-Ku70/EYFP-Ku80 heterodimer in soluble and DNA end bound states. We confirmed that the relative binding efficiencies of various DNA substrates (blunt, 3 nucleotide 5′ extension, and DNA hairpin) measured in the FRET assay reflected affinities obtained from direct measurements using surface plasmon resonance. The FRET assay was subsequently used to investigate Ku70/80 behavior in the context of a DNA-dependent kinase (DNA-PK) holocomplex. As expected, this complex was much more stable than Ku70/80 alone, and its stability was influenced by DNA-PK phosphorylation status. Interestingly, the Ku80 C-terminal extension contributed to DNA-PK complex stability but was not absolutely required for its formation. The Ku70 C-terminal SAP domain, on the other hand, was required for the stable association of Ku70/80 to DNA ends, but this effect was abrogated in DNA-PK holocomplexes. We conclude that FRET measurements can be used to determine Ku70/80 binding kinetics. The ability to do this in complex mixtures makes this assay particularly useful to study larger NHEJ protein complexes on DNA ends.

Published

2020

14. Chemical Proteomic Analysis of Serine Hydrolase Activity in Niemann-Pick Type C Mouse Brain

Author

Eva J. van Rooden, Annelot C. M. van Esbroeck, Marc P. Baggelaar, Hui Deng, Bogdan I. Florea, André R. A. Marques, Roelof Ottenhoff, Rolf G. Boot, Herman S. Overkleeft, Johannes M. F. G. Aerts, and Mario van der Stelt

Subjects

chemical proteomics, activity-based protein profiling, endocannabinoid system, hydrolases, Niemann-Pick type C, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

The endocannabinoid system (ECS) is considered to be an endogenous protective system in various neurodegenerative diseases. Niemann-Pick type C (NPC) is a neurodegenerative disease in which the role of the ECS has not been studied yet. Most of the endocannabinoid enzymes are serine hydrolases, which can be studied using activity-based protein profiling (ABPP). Here, we report the serine hydrolase activity in brain proteomes of a NPC mouse model as measured by ABPP. Two ABPP methods are used: a gel-based method and a chemical proteomics method. The activities of the following endocannabinoid enzymes were quantified: diacylglycerol lipase (DAGL) α, α/β-hydrolase domain-containing protein 4, α/β-hydrolase domain-containing protein 6, α/β-hydrolase domain-containing protein 12, fatty acid amide hydrolase, and monoacylglycerol lipase. Using the gel-based method, two bands were observed for DAGL α. Only the upper band corresponding to this enzyme was significantly decreased in the NPC mouse model. Chemical proteomics showed that three lysosomal serine hydrolase activities (retinoid-inducible serine carboxypeptidase, cathepsin A, and palmitoyl-protein thioesterase 1) were increased in Niemann-Pick C1 protein knockout mouse brain compared to wild-type brain, whereas no difference in endocannabinoid hydrolase activity was observed. We conclude that these targets might be interesting therapeutic targets for future validation studies.

Published

2018

15. Correction to 'Detection of Active Mammalian GH31 α‑Glucosidases in Health and Disease Using In-Class, Broad-Spectrum Activity-Based Probes'

Author

Jianbing Jiang, Chi-Lin Kuo, Liang Wu, Christian Franke, Wouter W. Kallemeijn, Bogdan I. Florea, Eline van Meel, Gijsbert A. van der Marel, Jeroen D. C. Codée, Rolf G. Boot, Gideon J. Davies, Herman S. Overkleeft, and Johannes M. F. G. Aerts

Subjects

Chemistry, QD1-999

Published

2017

16. Chemical Proteomics Reveals Antibiotic Targets of Oxadiazolones in MRSA

Author

Alexander T. Bakker, Ioli Kotsogianni, Liza Mirenda, Verena M. Straub, Mariana Avalos, Richard J. B. H. N. van den Berg, Bogdan I. Florea, Gilles P. van Wezel, Antonius P. A. Janssen, Nathaniel I. Martin, and Mario van der Stelt

Subjects

Colloid and Surface Chemistry, General Chemistry, Biochemistry, Catalysis

Abstract

Phenotypic screening is a powerful approach to identify novel antibiotics, but elucidation of the targets responsible for the antimicrobial activity is often challenging in the case of compounds with a polypharmacological mode of action. Here, we show that activity-based protein profiling maps the target interaction landscape of a series of 1,3,4-oxadiazole-3-ones identified in a phenotypic screen to have high antibacterial potency against multidrug-resistant

Published

2022

17. Supplementary Movie S1C from Treatment with HIV-Protease Inhibitor Nelfinavir Identifies Membrane Lipid Composition and Fluidity as a Therapeutic Target in Advanced Multiple Myeloma

Author

Christoph Driessen, Herman S. Overkleeft, Christopher D. Vulpe, Hesso Farhan, Marc Pilon, Celia R. Berkers, Bart Everts, Alex Loguinov, J. Thomas Hannich, Heinz Ludwig, Arnold Bolomsky, Julia Huber, Marcus Ståhlman, Jan Borén, Bogdan I. Florea, Marc Sathianathan, Lorina Büchler, Santosh Phuyal, Mario Ruiz, Alwin J. van der Ham, Esther A. Zaal, Amin Sobh, Sara C. Stolze, Andrej Besse, and Lenka Besse

Abstract

Cells pre-treated for 3h with 10 µM brefeldin A

Published

2023

18. Supplementary Data from Treatment with HIV-Protease Inhibitor Nelfinavir Identifies Membrane Lipid Composition and Fluidity as a Therapeutic Target in Advanced Multiple Myeloma

Author

Christoph Driessen, Herman S. Overkleeft, Christopher D. Vulpe, Hesso Farhan, Marc Pilon, Celia R. Berkers, Bart Everts, Alex Loguinov, J. Thomas Hannich, Heinz Ludwig, Arnold Bolomsky, Julia Huber, Marcus Ståhlman, Jan Borén, Bogdan I. Florea, Marc Sathianathan, Lorina Büchler, Santosh Phuyal, Mario Ruiz, Alwin J. van der Ham, Esther A. Zaal, Amin Sobh, Sara C. Stolze, Andrej Besse, and Lenka Besse

Abstract

Supplementary Methods, figures and tables

Published

2023

19. Data from Treatment with HIV-Protease Inhibitor Nelfinavir Identifies Membrane Lipid Composition and Fluidity as a Therapeutic Target in Advanced Multiple Myeloma

Author

Christoph Driessen, Herman S. Overkleeft, Christopher D. Vulpe, Hesso Farhan, Marc Pilon, Celia R. Berkers, Bart Everts, Alex Loguinov, J. Thomas Hannich, Heinz Ludwig, Arnold Bolomsky, Julia Huber, Marcus Ståhlman, Jan Borén, Bogdan I. Florea, Marc Sathianathan, Lorina Büchler, Santosh Phuyal, Mario Ruiz, Alwin J. van der Ham, Esther A. Zaal, Amin Sobh, Sara C. Stolze, Andrej Besse, and Lenka Besse

Abstract

The HIV-protease inhibitor nelfinavir has shown broad anticancer activity in various preclinical and clinical contexts. In patients with advanced, proteasome inhibitor (PI)–refractory multiple myeloma, nelfinavir-based therapy resulted in 65% partial response or better, suggesting that this may be a highly active chemotherapeutic option in this setting. The broad anticancer mechanism of action of nelfinavir implies that it interferes with fundamental aspects of cancer cell biology. We combined proteome-wide affinity-purification of nelfinavir-interacting proteins with genome-wide CRISPR/Cas9–based screening to identify protein partners that interact with nelfinavir in an activity-dependent manner alongside candidate genetic contributors affecting nelfinavir cytotoxicity. Nelfinavir had multiple activity-specific binding partners embedded in lipid bilayers of mitochondria and the endoplasmic reticulum. Nelfinavir affected the fluidity and composition of lipid-rich membranes, disrupted mitochondrial respiration, blocked vesicular transport, and affected the function of membrane-embedded drug efflux transporter ABCB1, triggering the integrated stress response. Sensitivity to nelfinavir was dependent on ADIPOR2, which maintains membrane fluidity by promoting fatty acid desaturation and incorporation into phospholipids. Supplementation with fatty acids prevented the nelfinavir-induced effect on mitochondrial metabolism, drug-efflux transporters, and stress-response activation. Conversely, depletion of fatty acids/cholesterol pools by the FDA-approved drug ezetimibe showed a synergistic anticancer activity with nelfinavir in vitro. These results identify the modification of lipid-rich membranes by nelfinavir as a novel mechanism of action to achieve broad anticancer activity, which may be suitable for the treatment of PI–refractory multiple myeloma.Significance:Nelfinavir induces lipid bilayer stress in cellular organelles that disrupts mitochondrial respiration and transmembrane protein transport, resulting in broad anticancer activity via metabolic rewiring and activation of the unfolded protein response.

Published

2023

20. Synthesis of broad-specificity activity-based probes for exo-β-mannosidases

Author

Nicholas G. S. McGregor, Chi-Lin Kuo, Thomas J. M. Beenakker, Chun-Sing Wong, Wendy A. Offen, Zachary Armstrong, Bogdan I. Florea, Jeroen D. C. Codée, Herman S. Overkleeft, Johannes M. F. G. Aerts, and Gideon J. Davies

Subjects

Organic Chemistry, Physical and Theoretical Chemistry, Biochemistry

Abstract

Exo-beta-mannosidases are a broad class of stereochemically retaining hydrolases that are essential for the breakdown of complex carbohydrate substrates found in all kingdoms of life. Yet the detection of exo-beta-mannosidases in complex biological samples remains challenging, necessitating the development of new methodologies. Cyclophellitol and its analogues selectively label the catalytic nucleophiles of retaining glycoside hydrolases, making them valuable tool compounds. Furthermore, cyclophellitol can be readily redesigned to enable the incorporation of a detection tag, generating activity-based probes (ABPs) that can be used to detect and identify specific glycosidases in complex biological samples. Towards the development of ABPs for exo-beta-mannosidases, we present a concise synthesis of beta-manno-configured cyclophellitol, cyclophellitol aziridine, and N-alkyl cyclophellitol aziridines. We show that these probes covalently label exo-beta-mannosidases from GH families 2, 5, and 164. Structural studies of the resulting complexes support a canonical mechanism-based mode of action in which the active site nucleophile attacks the pseudoanomeric centre to form a stable ester linkage, mimicking the glycosyl enzyme intermediate. Furthermore, we demonstrate activity-based protein profiling using an N-alkyl aziridine derivative by specifically labelling MANBA in mouse kidney tissue. Together, these results show that synthetic manno-configured cyclophellitol analogues hold promise for detecting exo-beta-mannosidases in biological and biomedical research.

Published

2022

21. Material Consuption Reduction and the Influence on the Mechanical Properties of the 3D Printed Parts for ABS Silver

Author

Irinel Radomir, Tibor Bedo, Virgil Geamăn, Mihai Alin Pop, Brandusa Ghiban, Bogdan I. Florea, and Augustin Semenescu

Subjects

Reduction (complexity), 3d printed, Materials science, Polymers and Plastics, Mechanics of Materials, Materials Chemistry, General Chemistry, Composite material

Abstract

The main objective was to reduce the consumption of material when obtaining 3D printed parts (different empty shapes inside) and the secondary one was to maintain the mechanical properties closer to the full printed version. In order to achieve these objectives, two internal configurations were designed - a configuration with hexagonal gaps (material reduction was 30%) and a configuration with sinuous gaps (material reduction was 15%). The specimens thus obtained were tested for traction, three-point bending and shock (resilience). Hexagonal hollow configuration has a resistance values close to those of solid specimens but with the advantage of consuming with 30% less material.

Published

2021

22. A Chemical Biological Approach to Study G Protein-Coupled Receptors: Labeling the Adenosine A

Author

Bert L H, Beerkens, Çağla, Koç, Rongfang, Liu, Bogdan I, Florea, Sylvia E, Le Dévédec, Laura H, Heitman, Adriaan P, IJzerman, and Daan, van der Es

Subjects

Adenosine, Ligands, Receptors, G-Protein-Coupled, Signal Transduction

Abstract

G protein-coupled receptors (GPCRs) have been known for decades as attractive drug targets. This has led to the development and approval of many ligands targeting GPCRs. Although ligand binding effects have been studied thoroughly for many GPCRs, there are multiple aspects of GPCR signaling that remain poorly understood. The reasons for this are the difficulties that are encountered upon studying GPCRs, for example, a poor solubility and low expression levels. In this work, we have managed to overcome some of these issues by developing an affinity-based probe for a prototypic GPCR, the adenosine A

Published

2022

23. Comparative photoaffinity profiling of omega-3 signaling lipid probes reveals prostaglandin reductase 1 as a metabolic hub in human macrophages

Author

Berend Gagestein, Johannes H. von Hegedus, Joanneke C. Kwekkeboom, Marieke Heijink, Niek Blomberg, Tom van der Wel, Bogdan I. Florea, Hans van den Elst, Kim Wals, Herman S. Overkleeft, Martin Giera, René E. M. Toes, Andreea Ioan-Facsinay, and Mario van der Stelt

Subjects

Azides, Docosahexaenoic Acids, Macrophages, Anti-Inflammatory Agents, Biotin, General Chemistry, Leukotriene B4, Biochemistry, Catalysis, Fish Oils, Colloid and Surface Chemistry, Alkynes, Fatty Acids, Omega-3, Prostaglandins, Humans, Oxidoreductases, Copper

Abstract

The fish oil constituent docosahexaenoic acid (DHA, 22:6 n-3) is a signaling lipid with anti-inflammatory properties. The molecular mechanisms underlying the biological effect of DHA are poorly understood. Here, we report the design, synthesis, and application of a complementary pair of bio-orthogonal, photoreactive probes based on the polyunsaturated scaffold DHA and its oxidative metabolite 17-hydroxydocosahexaenoic acid (17-HDHA). In these probes, an alkyne serves as a handle to introduce a fluorescent reporter group or a biotin-affinity tag via copper(I)-catalyzed azide-alkyne cycloaddition. This pair of chemical probes was used to map specific targets of the omega-3 signaling lipids in primary human macrophages. Prostaglandin reductase 1 (PTGR1) was identified as an interaction partner that metabolizes 17-oxo-DHA, an oxidative metabolite of 17-HDHA. 17-oxo-DHA reduced the formation of pro-inflammatory lipids 5-HETE and LTB4 in human macrophages and neutrophils. Our results demonstrate the potential of comparative photoaffinity protein profiling for the discovery of metabolic enzymes of bioactive lipids and highlight the power of chemical proteomics to uncover new biological insights.

Published

2022

24. The Influence of Thermal Behaviour to Composites Based on Cotton Tissue and Unsaturated Polyester Resin

Author

Oana Roxana Chivu, Irinel Radomir, Virgil Geamăn, Augustin Semenescu, Mihai Alin Pop, and Bogdan I. Florea

Subjects

Materials science, Polymers and Plastics, Mechanics of Materials, Thermal, Materials Chemistry, Unsaturated polyester, General Chemistry, Composite material

Abstract

The work focuses some experimental aspects concerning the weight gain, differential scanning calorimetric (DSC), dilatometer analysis (DIL) and thermo - gravimetric analysis (TG/DTA) for a composite material, based on cotton tissue and unsaturated polyester resin noted MCTDBN and immersed in salt water with 5% NaCl for 90 days. Following these analyzes are emphasized the thermal expansion, temperature glass transition and thermal decomposition. Before of thermal analysis, the treated specimens were dried in an oven at temperature of 30�C for several days. The paper presents also the effect of salt solution treatment and comparative analysis between untreated and treated composites.

Published

2020

25. Development of a Retinal-Based Probe for the Profiling of Retinaldehyde Dehydrogenases in Cancer Cells

Author

Hans den Dulk, Reina E Mebius, Eva J. van Rooden, Hans van den Elst, Pasquale C Putter, Bob van de Water, Else Botter, Gerard J. P. van Westen, Alexander T Bakker, Vera E. van der Noord, Bogdan I. Florea, Mario van der Stelt, Kim Wals, Sylvia E. Le Dévédec, Sebastiaan T A Koenders, Herman S. Overkleeft, Lukas S Wijaya, Martje N. Erkelens, Lindsey Burggraaff, Molecular cell biology and Immunology, AII - Cancer immunology, CCA - Cancer biology and immunology, and AGEM - Digestive immunity

Subjects

biology, 010405 organic chemistry, Drug discovery, General Chemical Engineering, Cellular differentiation, Retinoic acid, Aldehyde dehydrogenase, Retinal, General Chemistry, 010402 general chemistry, Proteomics, 01 natural sciences, 0104 chemical sciences, ALDH1A1, chemistry.chemical_compound, Chemistry, chemistry, Biochemistry, Cancer cell, biology.protein, QD1-999, Research Article

Abstract

Retinaldehyde dehydrogenases belong to a superfamily of enzymes that regulate cell differentiation and are responsible for detoxification of anticancer drugs. Chemical tools and methods are of great utility to visualize and quantify aldehyde dehydrogenase (ALDH) activity in health and disease. Here, we present the discovery of a first-in-class chemical probe based on retinal, the endogenous substrate of retinal ALDHs. We unveil the utility of this probe in quantitating ALDH isozyme activity in a panel of cancer cells via both fluorescence and chemical proteomic approaches. We demonstrate that our probe is superior to the widely used ALDEFLUOR assay to explain the ability of breast cancer (stem) cells to produce all-trans retinoic acid. Furthermore, our probe revealed the cellular selectivity profile of an advanced ALDH1A1 inhibitor, thereby prompting us to investigate the nature of its cytotoxicity. Our results showcase the application of substrate-based probes in interrogating pathologically relevant enzyme activities. They also highlight the general power of chemical proteomics in driving the discovery of new biological insights and its utility to guide drug discovery efforts., LEI-945 is a first-in-class retinal-based probe that enables profiling aldehyde dehydrogenase activity in living cancer cells and maps the selectivity profile of ALDH inhibitors.

Published

2019

26. Platelet EVs contain an active proteasome involved in protein processing for antigen presentation via MHC-I molecules

Author

Genevieve Marcoux, Audrée Laroche, Stephan Hasse, Marie Bellio, Maroua Mbarik, Marie Tamagne, Isabelle Allaeys, Anne Zufferey, Tania Lévesque, Johan Rebetz, Annie Karakeussian-Rimbaud, Julie Turgeon, Sylvain G. Bourgoin, Hind Hamzeh-Cognasse, Fabrice Cognasse, Rick Kapur, John W. Semple, Marie-Josée Hébert, France Pirenne, Herman S. Overkleeft, Bogdan I. Florea, Mélanie Dieude, Benoît Vingert, Eric Boilard, and Landsteiner Laboratory

Subjects

Blood Platelets, Proteasome Endopeptidase Complex, Lymphocyte, Immunology, Antigen presentation, Inbred C57BL, Biochemistry, Extracellular Vesicles, Mice, Immune system, Antigen, MHC class I, medicine, Animals, Humans, Platelet activation, Antigen Presentation, biology, Chemistry, Histocompatibility Antigens Class I/analysis, Histocompatibility Antigens Class I, fungi, Proteasome Endopeptidase Complex/analysis, Cell Biology, Hematology, Acquired immune system, Immune complex, Cell biology, Blood Platelets/chemistry, Mice, Inbred C57BL, medicine.anatomical_structure, Extracellular Vesicles/chemistry, biology.protein

Abstract

In addition to their hemostatic role, platelets play a significant role in immunity. Once activated, platelets release extracellular vesicles (EVs) formed by the budding of their cytoplasmic membranes. Because of their heterogeneity, platelet EVs (PEVs) are thought to perform diverse functions. It is unknown, however, whether the proteasome is transferred from platelets to PEVs or whether its function is retained. We hypothesized that functional protein processing and antigen presentation machinery are transferred to PEVs by activated platelets. Using molecular and functional assays, we found that the active 20S proteasome was enriched in PEVs, along with major histocompatibility complex class I (MHC-I) and lymphocyte costimulatory molecules (CD40L and OX40L). Proteasome-containing PEVs were identified in healthy donor blood, but did not increase in platelet concentrates that caused adverse transfusion reactions. They were augmented, however, after immune complex injections in mice. The complete biodistribution of murine PEVs after injection into mice revealed that they principally reached lymphoid organs, such as spleen and lymph nodes, in addition to the bone marrow, and to a lesser extent, liver and lungs. The PEV proteasome processed exogenous ovalbumin (OVA) and loaded its antigenic peptide onto MHC-I molecules, which promoted OVA-specific CD8+ T-lymphocyte proliferation. These results suggest that PEVs contribute to adaptive immunity through cross-presentation of antigens and have privileged access to immune cells through the lymphatic system, a tissue location that is inaccessible to platelets.

Published

2021

27. Non‐lethal proteasome inhibition activates pro‐tumorigenic pathways in multiple myeloma cells

Author

Leonidas G. Alexopoulos, Bogdan I. Florea, Efstathios Kastritis, Herman S. Overkleeft, Ioannis P. Trougakos, Theodore Sakellaropoulos, Ourania E. Tsitsilonis, Despoina D. Gianniou, Aikaterini Skorda, Meletios A. Dimopoulos, Evangelos Terpos, and Aimilia D. Sklirou

Subjects

Proteomics, 0301 basic medicine, Carcinogenesis, medicine.medical_treatment, Plasma cell, Bortezomib, chemistry.chemical_compound, 0302 clinical medicine, Bone Marrow, Recurrence, immune system diseases, Tumor Microenvironment, Multiple myeloma, 3. Good health, multiple myeloma, kinases, medicine.anatomical_structure, Cytokine, 030220 oncology & carcinogenesis, Molecular Medicine, Original Article, Oligopeptides, Signal Transduction, medicine.drug, STAT3 Transcription Factor, Proteasome Endopeptidase Complex, Cell Survival, T cell, proteasome inhibitors, Antineoplastic Agents, 03 medical and health sciences, Epoxomicin, Cell Line, Tumor, medicine, Humans, CXCL10, Interleukin-6, business.industry, Interleukin-8, Original Articles, Cell Biology, medicine.disease, cytokines, Chemokine CXCL10, proteasome, 030104 developmental biology, chemistry, Cancer research, Bone marrow, STAT6 Transcription Factor, business

Abstract

Multiple myeloma (MM) is a haematological malignancy being characterized by clonal plasma cell proliferation in the bone marrow. Targeting the proteasome with specific inhibitors (PIs) has been proven a promising therapeutic strategy and PIs have been approved for the treatment of MM and mantle‐cell lymphoma; yet, while outcome has improved, most patients inevitably relapse. As relapse refers to MM cells that survive therapy, we sought to identify the molecular responses induced in MM cells after non‐lethal proteasome inhibition. By using bortezomib (BTZ), epoxomicin (EPOX; a carfilzomib‐like PI) and three PIs, namely Rub999, PR671A and Rub1024 that target each of the three proteasome peptidases, we found that only BTZ and EPOX are toxic in MM cells at low concentrations. Phosphoproteomic profiling after treatment of MM cells with non‐lethal (IC10) doses of the PIs revealed inhibitor‐ and cell type‐specific readouts, being marked by the activation of tumorigenic STAT3 and STAT6. Consistently, cytokine/chemokine profiling revealed the increased secretion of immunosuppressive pro‐tumorigenic cytokines (IL6 and IL8), along with the inhibition of potent T cell chemoattractant chemokines (CXCL10). These findings indicate that MM cells that survive treatment with therapeutic PIs shape a pro‐tumorigenic immunosuppressive cellular and secretory bone marrow microenvironment that enables malignancy to relapse.

Published

2019

28. Experimental and Finite Element Analysis of the Open-Cells Porous Materials Subjected to Compression Mechanical Loading

Author

Bogdan I. Florea, Augustin Semenescu, Lucia-Antoneta Chicos, Camil Lancea, Sebastian Marian Zaharia, Pop, Oana Roxana Chivu, and Ian Campbell

Subjects

Fabrication, Materials science, Polymers and Plastics, Experimental data, General Chemistry, Compression (physics), Indentation hardness, Finite element method, Improved performance, Mechanics of Materials, Materials Chemistry, Composite material, Manufacturing methods, Porous medium

Abstract

Progress in Additive Manufacturing (AM) technology enables the fabrication of complex structures that could not be obtained with traditional manufacturing methods. One AM research area is the development and use of lightweight products with cellular structures, containing complex lattices and pores, which give improved performance and functionality. It is well known that there is a strong link between mechanical properties and architecture of samples with cellular structures. This paper presents a comparison and validation of Finite Element Analysis (FEA) simulations of cellular structures with experimental data obtained from compression tests, and degradation behaviour under load compression. The specimens, with spherical open-cells, were produced in VeroClear RGD810 photopolymer resin. Mechanical compression tests were performed to investigate the compressive behaviour and the mechanical response was registered in the form of compressive stress-strain curves. Also, using the specimens� CAD data and compression test parameters, a Finite Element Analysis (FEA) was performed. A macroscopic analysis of the specimens� structure and microhardness tests before and after compression tests were also carried out.

Published

2019

29. Fluorescent Probes from Aromatic Polycyclic Nitrile Oxides: Isoxazoles versus Dihydro‐1λ3,3,2λ4‐Oxazaborinines

Author

Bogdan I. Florea, Misal Giuseppe Memeo, Herman S. Overkleeft, Paolo Quadrelli, Mattia Moiola, Mariella Mella, Stefano Crespi, and Antonio Bova

Subjects

Anthracene, Full Paper, Nitrile, 010405 organic chemistry, General Chemistry, Full Papers, 010402 general chemistry, Triple bond, 01 natural sciences, Combinatorial chemistry, Cycloaddition, 0104 chemical sciences, lcsh:Chemistry, chemistry.chemical_compound, chemistry, Suzuki reaction, lcsh:QD1-999, fluorescent probes, boron complexes, Moiety, isoxazoles, enamino-ketones, Propargyl bromide, Isoxazole, photophysical studies

Abstract

Anthracenenitrile oxide undergoes 1,3‐dipolar cycloaddition reaction with propargyl bromide affording the expected isoxazole as single regioisomer, suitably synthetically elaborated and functionalized with a protected triple bond. The introduction of a bromine atom at the position C10 of the anthracene moiety allows for inserting a variety of aromatic and heterocyclic substituents through Suzuki coupling. A two‐way synthetic route can lead to simple isoxazole derivatives or, after N−O bond reductive cleavage and BF3 complexation, enamino ketone boron complexes. The photophysical properties of both the substituted isoxazoles and the corresponding boron complexes were investigated to show the potentialities for the employment as fluorescent tags in imaging techniques. The quite good quantum yield values confirm the suitability of these compounds in the cellular environment. Scope and limitations of the methodology are discussed.

Published

2019

30. Heat Treatment of Steel 1.1730 with Concentrated Solar Energy

Author

Ioan Milosan, Bogdan I. Florea, Ioan Giacomelli, Oana Roxana Chivu, Maria Stoicanescu, Augustin Semenescu, Martinez I. Canadas, Mihai Alin Pop, Aurel Crisan, Garcia J. Rodriguez, and Tibor Bedo

Subjects

Range (particle radiation), 1.1730 Steel, Polymers and Plastics, Solar furnace, business.industry, 020209 energy, Nuclear engineering, Heattreatment, Vertical axis, 02 engineering and technology, General Chemistry, Radiation, 021001 nanoscience & nanotechnology, Solar energy, Hardness, Mechanics of Materials, 0202 electrical engineering, electronic engineering, information engineering, Materials Chemistry, Environmental science, 0210 nano-technology, Plataforma Solar de Almería, business, Methane gas, Energy (signal processing)

Abstract

This paper presents and discusses research conducted with the purpose of developing the use of solar energy in the heat treatment of steels. For this, a vertical axis solar furnace called at Plataforma Solar de Almeria was adapted such as to allow control of the heating and cooling processes of samples made from 1.1730 steel. Thus temperature variation in pre-set points of the heated samples could be monitored in correlation with the working parameters: the level of solar radiation and implicitly the energy used the conditions of sample exposed to solar radiation, and the various protections and cooling mediums.The recorded data allowed establishing the types of treatments applied for certain working conditions. The distribution of hardness, as the representative feature resulting from heat treatment, was analysed on all sides of the treated samples. In correlation with the time-temperature-transformation diagram of 1.1730 steel, the measured values confirmed the possibility of using solar energy in all types of heat treatment applied to this steel. In parallel the efficiency of using solar energy was analysed in comparison to the energy obtained by burning methane gas for the heat treatment for the same set of samples. The analysis considered energy consumption, productivity and the impact on the environment. Thanks to various data obtained through developed experiences, which cover a wide range of thermic treatments applied steels 1.1730 model, we can certainly state that this can be a solid base in using solar energy in applications of thermic treatment at a high industrial level.

Published

2019

31. Structure-Based Design of Inhibitors Selective for Human Proteasome β2c or β2i Subunits

Author

Bogdan I. Florea, Emily S. Weyburne, Bo-Tao Xin, Marissa Janssens, Wolfgang Heinemeyer, Eva M. Huber, Gerjan de Bruin, Michael Groll, Christoph Driessen, Gijsbert A. van der Marel, Alexei F. Kisselev, Christofer Espinal, Yimeng Du, Elmer Maurits, and Herman S. Overkleeft

Subjects

Proteasome Endopeptidase Complex, Saccharomyces cerevisiae Proteins, Structural similarity, Protein subunit, Recombinant Fusion Proteins, Mutagenesis (molecular biology technique), Plasma protein binding, Saccharomyces cerevisiae, Crystallography, X-Ray, Protein Engineering, 01 natural sciences, Article, Small Molecule Libraries, 03 medical and health sciences, Mice, Peptide Library, Catalytic Domain, Cell Line, Tumor, Drug Discovery, Animals, Humans, Peptide library, 030304 developmental biology, 0303 health sciences, Chemistry, Stereoisomerism, Protein engineering, ddc, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, Protein Subunits, Proteasome, Structural biology, Biochemistry, Drug Design, Mutation, Molecular Medicine, Oligopeptides, Proteasome Inhibitors, Protein Binding

Abstract

Subunit-selective proteasome inhibitors are valuable tools to assess the biological and medicinal relevance of individual proteasome active sites. Whereas the inhibitors for the beta 1c, beta 1i, beta 5c, and beta 5i subunits exploit the differences in the substrate-binding channels identified by X-ray crystallography, compounds selectively targeting beta 2c or beta 2i could not yet be rationally designed because of the high structural similarity of these two subunits. Here, we report the development, chemical synthesis, and biological screening of a compound library that led to the identification of the beta 2c- and beta 2i-selective-compounds LU-002c (4; IC50 beta 2c: 8 nM, IC50 beta 2i/beta 2c: 40-fold) and LU-002i (5; IC50 beta 2i: 220 nM, IC50 beta 2c/beta 2i: 45-fold), respectively. Co-crystal structures with beta 2 humanized yeast proteasomes visualize protein-ligand interactions crucial for subunit specificity. Altogether, organic syntheses, activity-based protein profiling, yeast mutagenesis, and structural biology allowed us to decipher significant differences of beta 2 substrate-binding channels and to complete the set of subunit-selective proteasome inhibitors.

Published

2019

32. Development of Non-Hydrolysable Oligosaccharide Activity-Based Inactivators for Endoglycanases: A Case Study on alpha-1,6 Mannanases

Author

Gideon J. Davies, Casper de Boer, Herman S. Overkleeft, Wendy A. Offen, Jacopo Enotarpi, Gijsbert A. van der Marel, Jeroen D. C. Codée, Sybrin P. Schröder, Laura Marino, Bogdan I. Florea, Alexandra Males, and Yi Jin

Subjects

Glycoside Hydrolases, Stereochemistry, polysaccharides, Oligosaccharides, 010402 general chemistry, 01 natural sciences, Catalysis, Endoglycosidase, chemistry.chemical_compound, Trisaccharide, endoglycosidase, chemistry.chemical_classification, biology, 010405 organic chemistry, Communication, Organic Chemistry, Regioselectivity, Glycosidic bond, General Chemistry, Carbasugars, Aziridine, Oligosaccharide, Communications, 0104 chemical sciences, Carbasugar, mechanism-based inhibitor, Enzyme, chemistry, Covalent bond, cyclophellitol, biology.protein, Epoxy Compounds

Abstract

There is a vast genomic resource for enzymes active on carbohydrates. Lagging far behind, however, are functional chemical tools for the rapid characterization of carbohydrate‐active enzymes. Activity‐based probes (ABPs) offer one chemical solution to these issues with ABPs based upon cyclophellitol epoxide and aziridine covalent and irreversible inhibitors representing a potent and widespread approach. Such inhibitors for enzymes active on polysaccharides are potentially limited by the requirement for several glycosidic bonds, themselves substrates for the enzyme targets. Here, it is shown that non‐hydrolysable trisaccharide can be synthesized and applied even to enzymes with challenging subsite requirements. It was found that incorporation of carbasugar moieties, which was accomplished by cuprate‐assisted regioselective trans‐diaxial epoxide opening of carba‐mannal synthesised for this purpose, yields inactivators that act as powerful activity‐based inhibitors for α‐1,6 endo‐mannanases. 3‐D structures at 1.35–1.47 Å resolutions confirm the design rationale and binding to the enzymatic nucleophile. Carbasugar oligosaccharide cyclophellitols offer a powerful new approach for the design of robust endoglycosidase inhibitors, while the synthesis procedures presented here should allow adaptation towards activity‐based endoglycosidase probes as well as configurational isosteres targeting other endoglycosidase families., Carba‐trisaccharide cyclophellitols are potent GH76 α‐1,6 endo‐mannanase inactivators and resistant to endoglycosidic bond cleavage.

Published

2021

33. Immunoediting role for major vault protein in apoptotic signaling induced by bacterial N-acyl homoserine lactones

Author

Bastiaan P. Krom, Nicholas T. Jacob, Kim D. Janda, Josep Rayo, Gunnar F. Kaufmann, Benjamin F. Cravatt, Herman S. Overkleeft, Alexander Aranovich, Michael M. Meijler, Erik A.C. Wiemer, Bogdan I. Florea, Valerie A. Kickhoefer, Manikandan Thangaraj, Rambabu Dandela, Tsaffrir Zor, John C. Mathison, Richard J. Ulevitch, Rachel Gregor, Orna Ernst, Sergey Malitsky, Luba Dubinsky, Vladimir V. Kravchenko, Eran Barash, Leonard H. Rome, Alex Yashkin, Medical Oncology, and Preventive Dentistry

Subjects

Proteomics, 1.1 Normal biological development and functioning, Homoserine, Apoptosis, immunosurveillance, Acyl-Butyrolactones, Bacterial Physiological Phenomena, Mass Spectrometry, Immunomodulation, immunoediting, 03 medical and health sciences, chemistry.chemical_compound, Rare Diseases, SDG 3 - Good Health and Well-being, Underpinning research, Major vault protein, Humans, Protein kinase A, Lipid raft, Immunologic Surveillance, Lung, 030304 developmental biology, Vault Ribonucleoprotein Particles, Cancer, 0303 health sciences, Chromatography, Liquid, Multidisciplinary, Acyl-Homoserine Lactones, biology, Bacteria, 030302 biochemistry & molecular biology, bacterial signaling, 3. Good health, Cell biology, Immunosurveillance, Quorum sensing, Immunoediting, chemistry, biology.protein, cross-kingdom communication, Signal Transduction

Abstract

© 2021 National Academy of Sciences. All rights reserved.The major vault protein (MVP) mediates diverse cellular responses, including cancer cell resistance to chemotherapy and protection against inflammatory responses to Pseudomonas aeruginosa. Here, we report the use of photoactive probes to identify MVP as a target of the N-(3-oxo-dodecanoyl) homoserine lactone (C12), a quorum sensing signal of certain proteobacteria including P. aeruginosa. A treatment of normal and cancer cells with C12 or other N-acyl homoserine lactones (AHLs) results in rapid translocation of MVP into lipid raft (LR) membrane fractions. Like AHLs, inflammatory stimuli also induce LR-localization of MVP, but the C12 stimulation reprograms (functionalizes) bioactivity of the plasma membrane by recruiting death receptors, their apoptotic adaptors, and caspase-8 into LR. These functionalized membranes control AHL-induced signaling processes, in that MVP adjusts the protein kinase p38 pathway to attenuate programmed cell death. Since MVP is the structural core of large particles termed vaults, our findings suggest a mechanism in which MVP vaults act as sentinels that fine-tune inflammation-activated processes such as apoptotic signaling mediated by immunosurveillance cytokines including tumor necrosis factor-related apoptosis inducing ligand (TRAIL).

Published

2021

34. Immunoediting role for major vault protein in apoptotic signaling induced by bacterial

Author

Josep, Rayo, Rachel, Gregor, Nicholas T, Jacob, Rambabu, Dandela, Luba, Dubinsky, Alex, Yashkin, Alexander, Aranovich, Manikandan, Thangaraj, Orna, Ernst, Eran, Barash, Sergey, Malitsky, Bogdan I, Florea, Bastiaan P, Krom, Erik A C, Wiemer, Valerie A, Kickhoefer, Leonard H, Rome, John C, Mathison, Gunnar F, Kaufmann, Herman S, Overkleeft, Benjamin F, Cravatt, Tsaffrir, Zor, Kim D, Janda, Richard J, Ulevitch, Vladimir V, Kravchenko, and Michael M, Meijler

Subjects

Proteomics, Bacteria, bacterial signaling, Apoptosis, immunosurveillance, Acyl-Butyrolactones, Biological Sciences, Bacterial Physiological Phenomena, Microbiology, Mass Spectrometry, Immunomodulation, immunoediting, Chemistry, Physical Sciences, Humans, cross-kingdom communication, Immunologic Surveillance, Chromatography, Liquid, Signal Transduction, Vault Ribonucleoprotein Particles

Abstract

Significance It has become clear that our immune system can significantly inhibit the growth of cancer cells, in a process that has been coined “cancer immunoediting.” Based on this model, if the programmed cell death (apoptosis) mediated through immunosurveillance processes is not successful, the tumor cells may enter an equilibrium phase where they are either maintained or “edited” immunologically, leading to populations of tumor variants in the escape phase. Microbial factors have been found to affect cancer immunoediting. In this study we have identified a central player in these processes, called the major vault protein (MVP). Binding of certain bacterial signaling molecules to MVP strongly modulates apoptotic signaling, provoking new ideas and avenues to understand human-bacterial relationships and fight cancer., The major vault protein (MVP) mediates diverse cellular responses, including cancer cell resistance to chemotherapy and protection against inflammatory responses to Pseudomonas aeruginosa. Here, we report the use of photoactive probes to identify MVP as a target of the N-(3-oxo-dodecanoyl) homoserine lactone (C12), a quorum sensing signal of certain proteobacteria including P. aeruginosa. A treatment of normal and cancer cells with C12 or other N-acyl homoserine lactones (AHLs) results in rapid translocation of MVP into lipid raft (LR) membrane fractions. Like AHLs, inflammatory stimuli also induce LR-localization of MVP, but the C12 stimulation reprograms (functionalizes) bioactivity of the plasma membrane by recruiting death receptors, their apoptotic adaptors, and caspase-8 into LR. These functionalized membranes control AHL-induced signaling processes, in that MVP adjusts the protein kinase p38 pathway to attenuate programmed cell death. Since MVP is the structural core of large particles termed vaults, our findings suggest a mechanism in which MVP vaults act as sentinels that fine-tune inflammation-activated processes such as apoptotic signaling mediated by immunosurveillance cytokines including tumor necrosis factor-related apoptosis inducing ligand (TRAIL).

Published

2021

35. Bioorthogonal protein labelling enables the study of antigen processing of citrullinated and carbamylated auto-antigens

Author

Can Araman, Mikkel H. S. Marqvorsen, René E. M. Toes, Marcel Camps, George M.C. Janssen, Ferry Ossendorp, Clarissa R. Nascimento, Gerard J. P. van Westen, Willemijn van der Wulp, G. J. Mirjam Groenewold, Arieke S. B. Kampstra, Thomas Bakkum, Tyrza van Leeuwen, Antonius P A Janssen, Herman S. Overkleeft, Peter A. van Veelen, Sander I. van Kasteren, Bogdan I. Florea, and Linda Pieper Pournara

Subjects

Proteolysis, 010402 general chemistry, 01 natural sciences, Biochemistry, Genetics and Molecular Biology (miscellaneous), Biochemistry, 03 medical and health sciences, Immune system, Antigen, medicine, Molecular Biology, 030304 developmental biology, 0303 health sciences, medicine.diagnostic_test, biology, Chemistry, Antigen processing, Citrullination, Acquired immune system, 3. Good health, 0104 chemical sciences, Cell biology, Ovalbumin, Chemistry (miscellaneous), biology.protein, Bioorthogonal chemistry

Abstract

Proteolysis is fundamental to many biological processes. In the immune system, it underpins the activation of the adaptive immune response: degradation of antigenic material into short peptides and presentation thereof on major histocompatibility complexes, leads to activation of T-cells. This initiates the adaptive immune response against many pathogens. Studying proteolysis is difficult, as the oft-used polypeptide reporters are susceptible to proteolytic sequestration themselves. Here we present a new approach that allows the imaging of antigen proteolysis throughout the processing pathway in an unbiased manner. By incorporating bioorthogonal functionalities into the protein in place of methionines, antigens can be followed during degradation, whilst leaving reactive sidechains open to templated and non-templated post-translational modifications, such as citrullination and carbamylation. Using this approach, we followed and imaged the post-uptake fate of the commonly used antigen ovalbumin, as well as the post-translationally citrullinated and/or carbamylated auto-antigen vinculin in rheumatoid arthritis, revealing differences in antigen processing and presentation., Click handle-containing antigens can be used to study uptake, processing and presentation by immune cells.

Published

2021

36. Activity-Based Protein Profiling of Retaining α-Amylases in Complex Biological Samples

Author

Casper de Boer, Marta Artola, Johannes M. F. G. Aerts, Yurong Chen, Maher Abou Hachem, Chi-Lin Kuo, Mikkel S Rasmussen, Herman S. Overkleeft, Bogdan I. Florea, Zachary Armstrong, Gideon J. Davies, Gijsbert A. van der Marel, and Jeroen D. C. Codée

Subjects

Starch, Industrial biotechnology, 010402 general chemistry, 01 natural sciences, Biochemistry, Catalysis, Article, chemistry.chemical_compound, Mice, Colloid and Surface Chemistry, SDG 3 - Good Health and Well-being, Animals, Humans, Amylase, Saliva, Enzyme Assays, chemistry.chemical_classification, biology, Activity-based proteomics, Assimilation (biology), General Chemistry, 0104 chemical sciences, Protein profiling, Enzyme, chemistry, biology.protein, alpha-Amylases, Digestion

Abstract

Amylases are key enzymes in the processing of starch in many kingdoms of life. They are important catalysts in industrial biotechnology where they are applied in, among others, food processing and the production of detergents. In man amylases are the first enzymes in the digestion of starch to glucose and arguably also the preferred target in therapeutic strategies aimed at the treatment of type 2 diabetes patients through down-tuning glucose assimilation. Efficient and sensitive assays that report selectively on retaining amylase activities irrespective of the nature and complexity of the biomaterial studied are of great value both in finding new and effective human amylase inhibitors and in the discovery of new microbial amylases with potentially advantageous features for biotechnological application. Activity-based protein profiling (ABPP) of retaining glycosidases is inherently suited for the development of such an assay format. We here report on the design and synthesis of 1,6-epi-cyclophellitol-based pseudodisaccharides equipped with a suite of reporter entities and their use in ABPP of retaining amylases from human saliva, murine tissue as well as secretomes from fungi grown on starch. The activity and efficiency of the inhibitors and probes are substantiated by extensive biochemical analysis, and the selectivity for amylases over related retaining endoglycosidases is validated by structural studies.

Published

2021

37. Manno-epi-cyclophellitols enable activity-based protein profiling of human α-mannosidases and discovery of new Golgi mannosidase II inhibitors

Author

Zachary Armstrong, Gideon J. Davies, Chi-Lin Kuo, Erwin R. van Rijssel, Thomas J. M. Beenakker, Bogdan I. Florea, Mario van der Stelt, Gijsbert M. van der Marel, Rachel Johnson, D. Lahav, Bing Liu, Colin Hissink, Marjoke F. Debets, Jeroen D. C. Codée, C.S. Wong, Johannes M. F. G. Aerts, Paul P. Geurink, Casper de Boer, Huib Ovaa, Rolf G. Boot, Liang Wu, and Herman S. Overkleeft

Subjects

chemistry.chemical_classification, Lysis, Activity-based proteomics, Epoxide, General Chemistry, Aziridine, Golgi apparatus, 010402 general chemistry, 01 natural sciences, Biochemistry, Catalysis, 0104 chemical sciences, 3. Good health, carbohydrates (lipids), chemistry.chemical_compound, symbols.namesake, Colloid and Surface Chemistry, Enzyme, chemistry, symbols, Mannosidases, Fluorescence anisotropy

Abstract

Golgi mannosidase II (GMII) catalyzes the sequential hydrolysis of two mannosyl residues from GIcNAc-Man(5)GlcNAc(2) to produce GlcNAcMan(3) GlcNAc(2), the precursor for all complex N-glycans, including the branched N-glycans associated with cancer. Inhibitors of GMII are potential cancer therapeutics, but their usefulness is limited by off-target effects, which produce alpha-mannosidosis-like symptoms. Despite many structural and mechanistic studies of GMII, we still lack a potent and selective inhibitor of this enzyme. Here, we synthesized manno-epi-cyclophellitol epoxide and aziridines and demonstrate their covalent modification and time-dependent inhibition of GMII. Application of fluorescent manno-epi-cyclophellitol aziridine derivatives enabled activity-based protein profiling of alpha-mannosidases from both human cell lysate and mouse tissue extracts. Synthesized probes also facilitated a fluorescence polarization-based screen for dGMII inhibitors. We identified seven previously unknown inhibitors of GMII from a library of over 350 iminosugars and investigated their binding modalities through X-ray crystallography. Our results reveal previously unobserved inhibitor binding modes and promising scaffolds for the generation of selective GMII inhibitors.

Published

2020

38. Manno

Author

Zachary, Armstrong, Chi-Lin, Kuo, Daniël, Lahav, Bing, Liu, Rachel, Johnson, Thomas J M, Beenakker, Casper, de Boer, Chung-Sing, Wong, Erwin R, van Rijssel, Marjoke F, Debets, Bogdan I, Florea, Colin, Hissink, Rolf G, Boot, Paul P, Geurink, Huib, Ovaa, Mario, van der Stelt, Gijsbert M, van der Marel, Jeroen D C, Codée, Johannes M F G, Aerts, Liang, Wu, Herman S, Overkleeft, and Gideon J, Davies

Subjects

Molecular Structure, Drug Discovery, Mannosidases, Humans, Enzyme Inhibitors, Cyclohexanols

Abstract

Golgi mannosidase II (GMII) catalyzes the sequential hydrolysis of two mannosyl residues from GlcNAcMan

Published

2020

39. Chemical genetics strategy to profile kinase target engagement reveals role of FES in neutrophil phagocytosis

Author

Tim van den Hooven, Joost A. P. M. Wijnakker, Tjeerd Barf, Herman S. Overkleeft, Hans den Dulk, Rob Ruijtenbeek, Tom van der Wel, Eelke B. Lenselink, Allard Kaptein, Gerard J. P. van Westen, Bogdan I. Florea, Nienke M. Prins, Mario van der Stelt, and Riet Hilhorst

Subjects

0301 basic medicine, Neutrophils, Science, Cellular differentiation, General Physics and Astronomy, Kinases, Article, Chemical genetics, General Biochemistry, Genetics and Molecular Biology, Cell Line, 03 medical and health sciences, 0302 clinical medicine, Phagocytosis, Fluorescence Resonance Energy Transfer, Humans, Syk Kinase, CRISPR, lcsh:Science, Sensors and probes, Fluorescent Dyes, Gene Editing, Multidisciplinary, Drug discovery, Chemistry, Kinase, Cas9, Macrophages, Cell Differentiation, General Chemistry, Protein-Tyrosine Kinases, Cell biology, 030104 developmental biology, Proto-Oncogene Proteins c-fes, 030220 oncology & carcinogenesis, Mutation, lcsh:Q, ATP-Binding Cassette Transporters, CRISPR-Cas Systems, Signal transduction, Chemical tools, Tyrosine kinase, Signal Transduction

Abstract

Chemical tools to monitor drug-target engagement of endogenously expressed protein kinases are highly desirable for preclinical target validation in drug discovery. Here, we describe a chemical genetics strategy to selectively study target engagement of endogenous kinases. By substituting a serine residue into cysteine at the DFG-1 position in the ATP-binding pocket, we sensitize the non-receptor tyrosine kinase FES towards covalent labeling by a complementary fluorescent chemical probe. This mutation is introduced in the endogenous FES gene of HL-60 cells using CRISPR/Cas9 gene editing. Leveraging the temporal and acute control offered by our strategy, we show that FES activity is dispensable for differentiation of HL-60 cells towards macrophages. Instead, FES plays a key role in neutrophil phagocytosis via SYK kinase activation. This chemical genetics strategy holds promise as a target validation method for kinases., Chemical tools to monitor drug-target engagement of endogenous enzymes are essential for preclinical target validation. Here, the authors present a chemical genetics strategy to study target engagement of endogenous kinases, achieving specific labeling and inactivation of FES kinase to provide insights into FES’ role in neutrophil phagocytosis.

Published

2020

40. Structure-Based Design of Fluorogenic Substrates Selective for Human Proteasome Subunits

Author

Alexei F. Kisselev, Elmer Maurits, Christian G. Degeling, Herman S. Overkleeft, and Bogdan I. Florea

Subjects

Proteasome Endopeptidase Complex, 010402 general chemistry, Human b cell, 01 natural sciences, Biochemistry, 20s proteasome, Substrate Specificity, immunoproteasome, fluorogenic substrates, Humans, Molecular Biology, Michaelis-Menten kinetics, Fluorescent Dyes, Oligopeptide, Molecular Structure, 010405 organic chemistry, Chemistry, Hydrolysis, Communication, Organic Chemistry, Low activity, Leaving group, Communications, 0104 chemical sciences, Protein Subunits, proteasome, Proteasome, kinetics, Electrophile, Molecular Medicine, Structure based, Proteasome Inhibitors

Abstract

Proteasomes are established therapeutic targets for hematological cancers and promising targets for autoimmune diseases. In the past, we have designed and synthesized mechanism‐based proteasome inhibitors that are selective for the individual catalytic activities of human constitutive proteasomes and immunoproteasomes: β1c, β1i, β2c, β2i, β5c and β5i. We show here that by taking the oligopeptide recognition element and substituting the electrophile for a fluorogenic leaving group, fluorogenic substrates are obtained that report on the proteasome catalytic activity also targeted by the parent inhibitor. Though not generally applicable (β5c and β2i substrates showing low activity), effective fluorogenic substrates reporting on the individual activity of β1c, β1i, β2c and β5i subunits in Raji (human B cell) lysates and purified 20S proteasome were identified in this manner. Our work thus adds to the expanding proteasome research toolbox through the identification of new and/or more effective subunit‐selective fluorogenic substrates., Selective reporting: A set of fluorogenic substrates for each of the human proteasome subunits was reverse designed based on selective proteasome inhibitors. Assays on both cell lysates and purified proteasome were conducted and revealed high selectivity could be maintained.

Published

2020

41. Spatiotemporal proteomics uncovers cathepsin-dependent macrophage cell death during Salmonella infection

Author

André Mateus, Mikhail M. Savitski, Haruna Imamura, Bogdan I. Florea, Wolf-Dietrich Hardt, Anna Sueki, Matthew Mangan, Boris Turk, Jeroen Krijgsveld, Eicke Latz, Nataša Kopitar-Jerala, Annika Hausmann, Jacob Bobonis, Gianluca Sigismondo, Matylda Zietek, Joel Selkrig, Athanasios Typas, Bachir El Debs, Pedro Beltrao, Nan Li, and Herman S. Overkleeft

Subjects

Salmonella typhimurium, Proteomics, Lipopolysaccharides, Proteome, Inflammasomes, metabolism [Phosphate-Binding Proteins], metabolism [Peptide Hydrolases], physiology [Cell Death], medicine.disease_cause, Applied Microbiology and Biotechnology, metabolism [Salmonella Infections], metabolism [Lysosomes], Mice, Protein targeting, 0303 health sciences, Cell Death, Chemistry, Intracellular Signaling Peptides and Proteins, metabolism [Lipopolysaccharides], Inflammasome, Cell biology, Salmonella Infections, metabolism [Intracellular Signaling Peptides and Proteins], Intracellular, medicine.drug, Microbiology (medical), Programmed cell death, Immunology, Microbiology, Article, 03 medical and health sciences, metabolism [Cathepsins], ddc:570, Genetics, Extracellular, medicine, Animals, Cystatin B, Gsdmd protein, mouse, 030304 developmental biology, Cathepsin, 030306 microbiology, Macrophages, microbiology [Salmonella Infections], drug effects [Cell Death], antagonists & inhibitors [Cystatin B], Cell Biology, Phosphate-Binding Proteins, Cathepsins, microbiology [Macrophages], drug effects [Cathepsins], RAW 264.7 Cells, Cytoplasm, metabolism [Macrophages], metabolism [Salmonella typhimurium], Lysosomes, metabolism [Inflammasomes], Peptide Hydrolases

Abstract

The interplay between host and pathogen relies heavily on rapid protein synthesis and accurate protein targeting to ensure pathogen destruction. To gain insight into this dynamic interface, we combined Click chemistry with pulsed stable isotope labelling of amino acids in cell culture to quantify the host proteome response during macrophage infection with the intracellular bacterial pathogen Salmonella enterica Typhimurium. We monitored newly synthesized proteins across different host cell compartments and infection stages. Within this rich resource, we detected aberrant trafficking of lysosomal proteases to the extracellular space and the nucleus. We verified that active cathepsins re-traffic to the nucleus and that these are linked to cell death. Pharmacological cathepsin inhibition and nuclear targeting of a cellular cathepsin inhibitor (stefin B) suppressed S. enterica Typhimurium-induced cell death. We demonstrate that cathepsin activity is required for pyroptotic cell death via the non-canonical inflammasome, and that lipopolysaccharide transfection into the host cytoplasm is sufficient to trigger active cathepsin accumulation in the host nucleus and cathepsin-dependent cell death. Finally, cathepsin inhibition reduced gasdermin D expression, thus revealing an unexpected role for cathepsin activity in non-canonical inflammasome regulation. Overall, our study illustrates how resolution of host proteome dynamics during infection can drive the discovery of biological mechanisms at the host-microbe interface.

Published

2020

42. Olaparib-Based Photoaffinity Probes for PARP-1 Detection in Living Cells

Author

Thomas Bakkum, Berend Gagestein, Herman S. Overkleeft, Sander I. van Kasteren, Dmitri V. Filippov, Jim Voorneveld, Rafal J Mendowicz, Miriam S van der Veer, Bogdan I. Florea, and Mario van der Stelt

Subjects

DNA repair, DNA damage, Ultraviolet Rays, Poly ADP ribose polymerase, Poly (ADP-Ribose) Polymerase-1, Context (language use), PARP-1, Photoaffinity Labels, Poly(ADP-ribose) Polymerase Inhibitors, 010402 general chemistry, 01 natural sciences, Biochemistry, olaparib, Piperazines, Olaparib, chemistry.chemical_compound, chemical proteomics, Ribose, Humans, Molecular Biology, Polymerase, Cells, Cultured, biology, Molecular Structure, 010405 organic chemistry, Communication, Organic Chemistry, Photochemical Processes, bioorthogonal chemistry, Communications, 0104 chemical sciences, Blot, photoaffinity probes, chemistry, biology.protein, Molecular Medicine, Phthalazines

Abstract

The poly‐ADP‐ribose polymerase (PARP) is a protein from the family of ADP‐ribosyltransferases that catalyzes polyadenosine diphosphate ribose (ADPR) formation in order to attract the DNA repair machinery to sites of DNA damage. The inhibition of PARP activity by olaparib can cause cell death, which is of clinical relevance in some tumor types. This demonstrates that quantification of PARP activity in the context of living cells is of great importance. In this work, we present the design, synthesis and biological evaluation of photo‐activatable affinity probes inspired by the olaparib molecule that are equipped with a diazirine for covalent attachment upon activation by UV light and a ligation handle for the addition of a reporter group of choice. SDS‐PAGE, western blotting and label‐free LC‐MS/MS quantification analysis show that the probes target the PARP‐1 protein and are selectively outcompeted by olaparib; this suggests that they bind in the same enzymatic pocket. Proteomics data are available via ProteomeXchange with identifier PXD018661., Impair the repair: Olaparib is a PARP inhibitor (PARPi) of clinical relevance because it causes cell death in certain tumor types. By using a substructure of olaparib and adding a photo‐activatable linker, a proteomics assay is presented for visualizing PARP1 with in‐gel fluorescence and MS/MS analysis.

Published

2020

43. Discovery of a NAPE-PLD inhibitor that modulates emotional behavior in mice

Author

Ozge Gunduz-Cinar, Laura I. Castillo, Antonius P A Janssen, Helma van den Hurk, Marjolein Soethoudt, Andrew Holmes, Resat Cinar, Cristina Miliano, Annelot C. M. van Esbroeck, Colleen M Donovan, Pal Pacher, Elliot D. Mock, Aron H. Lichtman, Alexander T Bakker, Jesse Wat, Matthew W. Buczynski, Anouk M F van der Gracht, Tom van der Wel, Ioli Kotsogianni, Vasudev Kantae, Tiemen J Wendel, Xinyu Di, Thomas Hankemeier, Matthias B. Wittwer, Matthew N. Hill, János Pálóczi, Gavin N. Petrie, Uwe Grether, Joshua K. Park, Andrea Martella, Zoltán Varga, Ming Jiang, Daisuke Ogasawara, Giulia Donvito, Benjamin F. Cravatt, Constant A. A. van Boeckel, Bogdan I. Florea, Mario van der Stelt, and Mohammed A. Mustafa

Subjects

Male, Cannabinoid receptor, Nape, medicine.medical_treatment, Drug Evaluation, Preclinical, Article, Amidohydrolases, 03 medical and health sciences, chemistry.chemical_compound, Mice, Fatty acid amide hydrolase, Cell Line, Tumor, Lipidomics, medicine, Phospholipase D, Animals, Humans, Enzyme Inhibitors, Receptors, Cannabinoid, Molecular Biology, Cannabinoid Receptor Antagonists, 030304 developmental biology, 0303 health sciences, Behavior, Animal, Molecular Structure, Chemistry, Phosphatidylethanolamines, 030302 biochemistry & molecular biology, Brain, Cell Biology, Anandamide, Blood Proteins, Fear, Lipid Metabolism, Endocannabinoid system, Cell biology, Mice, Inbred C57BL, medicine.anatomical_structure, lipids (amino acids, peptides, and proteins), Cannabinoid, Signal Transduction

Abstract

N-acylethanolamines (NAEs), which include the endocannabinoid anandamide, represent an important family of signaling lipids in the brain. The lack of chemical probes that modulate NAE biosynthesis in living systems hamper the understanding of the biological role of these lipids. Using a high-throughput screen, chemical proteomics and targeted lipidomics, we report here the discovery and characterization of LEI-401 as a CNS-active N-acylphosphatidylethanolamine phospholipase D (NAPE-PLD) inhibitor. LEI-401 reduced NAE levels in neuroblastoma cells and in the brain of freely moving mice, but not in NAPE-PLD KO cells and mice, respectively. LEI-401 activated the hypothalamus–pituitary–adrenal axis and impaired fear extinction, thereby emulating the effect of a cannabinoid CB1 receptor antagonist, which could be reversed by a fatty acid amide hydrolase inhibitor. Our findings highlight the distinctive role of NAPE-PLD in NAE biosynthesis in the brain and suggest the presence of an endogenous NAE tone controlling emotional behavior.

Published

2020

44. Immunoproteasome inhibitor-doxorubicin conjugates target multiple myeloma cells and release doxorubicin upon low-dose photon irradiation

Author

Santina Maiorana, Elmer Maurits, Bogdan I. Florea, Patrick M Dekker, Herman S. Overkleeft, Dennis P A Wander, Sander I. van Kasteren, Sabina Y van der Zanden, Michel J. van de Graaff, and Jacques Neefjes

Subjects

Drug, Models, Molecular, Optics and Photonics, media_common.quotation_subject, Peptide, 010402 general chemistry, 01 natural sciences, Biochemistry, Catalysis, Colloid and Surface Chemistry, medicine, Humans, Doxorubicin, Cytotoxicity, media_common, chemistry.chemical_classification, Antibiotics, Antineoplastic, biology, Communication, General Chemistry, Prodrug, 3. Good health, 0104 chemical sciences, chemistry, Proteasome, Targeted drug delivery, Enzyme inhibitor, Cancer research, biology.protein, Multiple Myeloma, Proteasome Inhibitors, medicine.drug

Abstract

Proteasome inhibitors are established therapeutic agents for the treatment of hematological cancers, as are anthracyclines such as doxorubicin. We here present a new drug targeting approach that combines both drug classes into a single molecule. Doxorubicin was conjugated to an immunoproteasome-selective inhibitor via light-cleavable linkers, yielding peptide epoxyketone-doxorubicin prodrugs that remained selective and active toward immunoproteasomes. Upon cellular uptake and immunoproteasome inhibition, doxorubicin is released from the immunoproteasome inhibitor through photoirradiation. Multiple myeloma cells in this way take a double hit: immunoproteasome inhibition and doxorubicin-induced toxicity. Our strategy, which entails targeting of a cytotoxic agent, through a covalent enzyme inhibitor that is detrimental to tumor tissue in its own right, may find use in the search for improved anticancer drugs.

Published

2020

45. Unbiased identification of the liposome protein corona using photoaffinity-based chemoproteomics

Author

Stefan Crielaard, Iris Klein-Schiphorst, Frederick Campbell, Bogdan I. Florea, Alexander Kros, and Roy Pattipeiluhu

Subjects

0303 health sciences, Liposome, Chemistry, General Chemical Engineering, Protein Corona, 02 engineering and technology, General Chemistry, 021001 nanoscience & nanotechnology, Blood proteins, 03 medical and health sciences, In vivo, Native state, Biophysics, Chemoproteomics, Identification (biology), 0210 nano-technology, QD1-999, Research Article, 030304 developmental biology, Protein adsorption

Abstract

Protein adsorption to the surface of a nanoparticle can fundamentally alter the character, behavior, and fate of a nanoparticle in vivo. Current methods to capture the protein corona rely on physical separation techniques and are unable to resolve key, individual protein–nanoparticle interactions. As a result, the precise link between the “synthetic” and the “biological” identity of a nanoparticle remains unclear. Herein, we report an unbiased photoaffinity-based approach to capture, characterize, and quantify the protein corona of liposomes in their native state. Compared to conventional methods, our photoaffinity approach reveals markedly different interacting proteins as well as reduced total protein binding to liposome surfaces. Identified proteins do not follow protein abundancy patterns of human serum, as has been generally reported, but are instead dominated by soluble apolipoproteins–endogenous serum proteins that have evolved to recognize the lipidic surface of circulating lipoproteins. We believe our findings are the most accurate characterization of a liposome’s biological identity but, more fundamentally, reveal liposome–protein binding is, in many cases, significantly less complex than previously thought., Serum protein adsorption can drastically affect the in vivo performance of a liposome. A method to capture, characterize, and quantify the protein corona of a liposome in its native state is presented.

Published

2020

46. New Irreversible α‐<scp>l</scp>‐Iduronidase Inhibitors and Activity‐Based Probes

Author

Chi-Lin Kuo, Jeroen D. C. Codée, Allison R. Kermode, Bogdan I. Florea, Johannes M. F. G. Aerts, Xu He, Marta Artola, Herman S. Overkleeft, Stephen A. McMahon, Verena Oehler, Tracey M. Gloster, Gijsbert A. van der Marel, Hans van den Elst, Martijn J.C. van der Lienden, Thomas Hansen, The Wellcome Trust, University of St Andrews. School of Biology, University of St Andrews. Biomedical Sciences Research Complex, Chemistry and Pharmaceutical Sciences, Medical Biochemistry, ACS - Amsterdam Cardiovascular Sciences, and AGEM - Amsterdam Gastroenterology Endocrinology Metabolism

Subjects

Models, Molecular, 0301 basic medicine, cyclophellitol aziridines, QH301 Biology, Aziridines, law.invention, Iduronidase, chemistry.chemical_compound, Tandem Mass Spectrometry, law, QD, Glycoside hydrolase, Enzyme Inhibitors, Cyclophellitol aziridines, Trifluoromethyl, Full Paper, Chemistry, conformational analysis, Activity-based proteomics, Full Papers, Recombinant Proteins, Covalent bond, glycosidase, Recombinant DNA, Stereochemistry, NDAS, irreversible inhibitors, Cyclohexene, Activity‐Based Probes | Hot Paper, Catalysis, QH301, 03 medical and health sciences, Hydrolase, Humans, Enzyme Assays, Fluorescent Dyes, activity-based protein profiling, Staining and Labeling, Organic Chemistry, General Chemistry, QD Chemistry, Cyclohexanols, Glycosidase, Conformational analysis, Irrevesible inhibitors, 030104 developmental biology, Microscopy, Fluorescence, Activity-based protein profiling, Chromatography, Liquid

Abstract

We thank The Netherlands Organization for Scientific Research (NWO-CW, ChemThem grant to J.M.F.G.A. and H.S.O.), the European Research Council (ERC-2011-AdG290836 “Chembiosphing”, to H.S.O.) and Sanofi Genzyme (research grant to J.M.F.G.A. and H.S.O. and postdoctoral contract to M.A.). We acknowledge ChemAxon for kindly providing the Instant JChem software to manage our compound library. T.M.G., V.O. and S.A.M. are supported by a Wellcome Trust Research Career Development Fellowship and Institutional Strategic Support Funding. Cyclophellitol aziridines are potent irreversible inhibitors of retaining glycosidases and versatile intermediates in the synthesis of activity‐based glycosidase probes (ABPs). Direct 3‐amino‐2‐(trifluoromethyl)quinazolin‐4(3H)‐one‐mediated aziridination of ʟ‐ido‐configured cyclohexene has enabled the synthesis of new covalent inhibitors and ABPs of α‐ʟ‐iduronidase, deficiency of which underlies the lysosomal storage disorder mucopolysaccharidosis type I (MPS I). The iduronidase ABPs react covalently and irreversibly in an activity‐based manner with human recombinant α‐ʟ‐iduronidase (rIDUA, Aldurazyme®). The structures of IDUA when complexed with the inhibitors in a non‐covalent transition state mimicking form and a covalent enzyme‐bound form provide insights into its conformational itinerary. Inhibitors 1–3 adopt a half‐chair conformation in solution (4H3 and 3H4), as predicted by DFT calculations, which is different from the conformation of the Michaelis complex observed by crystallographic studies. Consequently, 1–3 may need to overcome an energy barrier in order to switch from the 4H3 conformation to the transition state (2, 5B) binding conformation before reacting and adopting a covalent 5S1 conformation. rIDUA can be labeled with fluorescent Cy5 ABP 2 , which allows monitoring of the delivery of therapeutic recombinant enzyme to lysosomes, as is intended in enzyme replacement therapy for the treatment of MPS I patients. Publisher PDF

Published

2018

47. An inhibitor of proteasome β2 sites sensitizes myeloma cells to immunoproteasome inhibitors

Author

Christoph Driessen, Ananta Bhatt, Constantine S. Mitsiades, Paul G. Richardson, Herman S. Overkleeft, Sondra L. Downey-Kopyscinski, Alexei F. Kisselev, Ellen W. Daily, Bogdan I. Florea, and Marc Gautier

Subjects

Male, 0301 basic medicine, Proteasome Endopeptidase Complex, Cell Survival, Antineoplastic Agents, Ixazomib, Bortezomib, Mice, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, immune system diseases, In vivo, Interferon, hemic and lymphatic diseases, medicine, Animals, Humans, cardiovascular diseases, Cytotoxicity, neoplasms, Multiple myeloma, Lymphoid Neoplasia, Dose-Response Relationship, Drug, Drug Synergism, Hematology, medicine.disease, Carfilzomib, 030104 developmental biology, chemistry, Proteasome, 030220 oncology & carcinogenesis, Cancer research, Multiple Myeloma, Oligopeptides, Proteasome Inhibitors, Biomarkers, medicine.drug

Abstract

Proteasome inhibitors bortezomib, carfilzomib and ixazomib (approved by the US Food and Drug Administration [FDA]) induce remissions in patients with multiple myeloma (MM), but most patients eventually become resistant. MM and other hematologic malignancies express ubiquitous constitutive proteasomes and lymphoid tissue–specific immunoproteasomes; immunoproteasome expression is increased in resistant patients. Immunoproteasomes contain 3 distinct pairs of active sites, β5i, β1i, and β2i, which are different from their constitutive β5c, β1c, and β2c counterparts. Bortezomib and carfilzomib block β5c and β5i sites. We report here that pharmacologically relevant concentrations of β5i-specific inhibitor ONX-0914 show cytotoxicity in MM cell lines similar to that of carfilzomib and bortezomib. In addition, increasing immunoproteasome expression by interferon-γ increases sensitivity to ONX-0914 but not to carfilzomib. LU-102, an inhibitor of β2 sites, dramatically sensitizes MM cell lines and primary cells to ONX-0914. ONX-0914 synergizes with all FDA-approved proteasome inhibitors in MM in vitro and in vivo. Thus, immunoproteasome inhibitors, currently in clinical trials for the treatment of autoimmune diseases, should also be considered for the treatment of MM.

Published

2018

48. Chl a fluorescence and proteomics reveal protection of the photosynthetic apparatus to dehydration in tolerant but not in susceptible wheat cultivars

Author

J. Debski, Bogdan I. Florea, Małgorzata Nykiel, K. Rybka, and P. Lisik

Subjects

Photosystem II, Spots, Drought tolerance, fungi, food and beverages, Plant Science, drought, Horticulture, Biology, Photosynthesis, medicine.disease, Water saturation, polyphasic fluorescence transient, medicine, Kautsky effect, Cultivar, Dehydration, OJIP, 2D electrophoresis

Abstract

Seedlings of spring wheat (Triticum aestivum L.) cultivars, Ethos and Zebra, differing in drought tolerance were dehydrated to reach a water saturation deficit (WSD) in leaves ~15, 30, and 50 %. Ethos, the drought tolerant cultivar, dried slower in comparison with Zebra and regrew in 70 % upon rehydration. The effect of dehydration on photosystem Seedlings of spring wheat (Triticum aestivum L.) cultivars, Ethos and Zebra, differing in drought tolerance were dehydrated to reach a water saturation deficit (WSD) in leaves ~15, 30, and 50 %. Ethos, the drought tolerant cultivar, dried slower in comparison with Zebra and regrew in 70 % upon rehydration. The effect of dehydration on photosystem II was evaluated by Chl a fluorescence (OJIP transients). The inflection point of double normalized curves (ΔWOJ) calculated for Ethos was negative for seedlings with 15 % WSD, nearly zero for those with 30 % WSD, and about +0.05 for those with 50 % WSD. In case of Zebra, the 15 % WSD already induced a positive ΔWOJ (+0.05) and 50 % WSD maximized it to +0.10, which is a sign of drought susceptibility. The proteomic studies revealed, that among identified 850 spots, 80 protein spots were differentially expressed during dehydration. The differentially expressed proteins of the drought tolerant cultivar indicated the protection of the photosynthetic apparatus and proteome rebuilding in response to drought. In the drought susceptible cultivar, protection of proteins and membranes and partial scavenging reactive oxygen species appeared.

Published

2019

49. STA-55, an Easily Accessible, Broad-Spectrum, Activity-Based Aldehyde Dehydrogenase Probe

Author

Sebastiaan T A Koenders, Bogdan I. Florea, Mario van der Stelt, Hans van den Elst, Herman S. Overkleeft, and Eva J. van Rooden

Subjects

Proteomics, Aldehyde dehydrogenase, 010402 general chemistry, 01 natural sciences, Biochemistry, Downregulation and upregulation, Cell Line, Tumor, medicine, Humans, Chemoproteomics, Enzyme Inhibitors, Molecular Biology, Fluorescent Dyes, chemistry.chemical_classification, biology, 010405 organic chemistry, Chemistry, Organic Chemistry, Target engagement, Activity-based proteomics, Cancer, Aldehyde Dehydrogenase, medicine.disease, 0104 chemical sciences, Enzyme, Drug Design, biology.protein, Molecular Medicine, Click Chemistry

Abstract

Aldehyde dehydrogenases (ALDHs) convert aldehydes into carboxylic acids and are often upregulated in cancer. They have been linked to therapy resistance and are therefore potential therapeutic targets. However, only a few selective and potent inhibitors are currently available for this group of enzymes. Competitive activity-based protein profiling (ABPP) would aid the development and validation of new selective inhibitors. Herein, a broad-spectrum activity-based probe that reports on several ALDHs is presented. This probe was used in a competitive ABPP protocol against three ALDH inhibitors in lung cancer cells to determine their selectivity profiles and establish their target engagement.

Published

2019

50. Accelerated Corrosion Analysis of AlSi10Mg Alloy Manufactured by Selective Laser Melting (SLM)

Author

Mihai Alin Pop, Augustin Semenescu, Bogdan I. Florea, Oana Roxana Chivu, Lucia-Antoneta Chicos, Sebastian Marian Zaharia, and Camil Lancea

Subjects

010302 applied physics, Materials science, Materials Science (miscellaneous), Process Chemistry and Technology, Metallurgy, Alloy, General Engineering, 02 engineering and technology, General Chemistry, General Medicine, engineering.material, 021001 nanoscience & nanotechnology, 01 natural sciences, General Biochemistry, Genetics and Molecular Biology, Corrosion, 0103 physical sciences, Materials Chemistry, engineering, General Pharmacology, Toxicology and Pharmaceutics, Selective laser melting, 0210 nano-technology

Abstract

The Selective Laser Melting (SLM) technology uses metal powders as building material which is melted and welded together using a high-power laser in order to obtain quick configuration of complex parts, most often for testing them. Another advantage of this method is the fact that allows obtaining any 3D geometry of the parts, even parts that cannot be processed through conventional manufacturing procedures. In this work were performed a number of tests for accelerated corrosion of AlSi10Mg alloy specimens in order to determine their mean life in the conditions of their use in a high salinity environment. For specimens, optical analysis was used the SEM microscope which has the advantage of obtaining an enlarged image of the investigated objects without processing. Following these analyses, it has been determined the mass loss of specimens due to corrosion.

Published

2018