Your search keyword '"Lien, Moreels"' showing total 11 results

1. Cross-Reactive SARS-CoV-2 Neutralizing Antibodies From Deep Mining of Early Patient Responses

Author

Georgia Bullen, Jacob D. Galson, Gareth Hall, Pedro Villar, Lien Moreels, Line Ledsgaard, Giada Mattiuzzo, Emma M. Bentley, Edward W. Masters, David Tang, Sophie Millett, Danielle Tongue, Richard Brown, Ioannis Diamantopoulos, Kothai Parthiban, Claire Tebbutt, Rachael Leah, Krishna Chaitanya, Sandra Ergueta-Carballo, Deividas Pazeraitis, Sachin B. Surade, Omodele Ashiru, Lucia Crippa, Richard Cowan, Matthew W. Bowler, Jamie I. Campbell, Wing-Yiu Jason Lee, Mark D. Carr, David Matthews, Paul Pfeffer, Simon E. Hufton, Kovilen Sawmynaden, Jane Osbourn, John McCafferty, and Aneesh Karatt-Vellatt

Subjects

COVID-19, antibodies, convergence, phage display, SARS-CoV-2 variants, Immunologic diseases. Allergy, RC581-607

Abstract

Passive immunization using monoclonal antibodies will play a vital role in the fight against COVID-19. The recent emergence of viral variants with reduced sensitivity to some current antibodies and vaccines highlights the importance of broad cross-reactivity. This study describes deep-mining of the antibody repertoires of hospitalized COVID-19 patients using phage display technology and B cell receptor (BCR) repertoire sequencing to isolate neutralizing antibodies and gain insights into the early antibody response. This comprehensive discovery approach has yielded a panel of potent neutralizing antibodies which bind distinct viral epitopes including epitopes conserved in SARS-CoV-1. Structural determination of a non-ACE2 receptor blocking antibody reveals a previously undescribed binding epitope, which is unlikely to be affected by the mutations in any of the recently reported major viral variants including B.1.1.7 (from the UK), B.1.351 (from South Africa) and B.1.1.28 (from Brazil). Finally, by combining sequences of the RBD binding and neutralizing antibodies with the B cell receptor repertoire sequencing, we also describe a highly convergent early antibody response. Similar IgM-derived sequences occur within this study group and also within patient responses described by multiple independent studies published previously.

Published

2021

2. Synthesis of novel purpurealidin analogs and evaluation of their effect on the cancer-relevant potassium channel KV10.1.

Author

Lien Moreels, Chinmay Bhat, Manuela Voráčová, Steve Peigneur, Hannah Goovaerts, Eero Mäki-Lohiluoma, Farrah Zahed, Luis A Pardo, Jari Yli-Kauhaluoma, Paula Kiuru, and Jan Tytgat

Subjects

Medicine, Science

Abstract

In the search for novel anticancer drugs, the potassium channel KV10.1 has emerged as an interesting cancer target. Here, we report a new group of KV10.1 inhibitors, namely the purpurealidin analogs. These alkaloids are produced by the Verongida sponges and are known for their wide variety of bioactivities. In this study, we describe the synthesis and characterization of 27 purpurealidin analogs. Structurally, bromine substituents at the central phenyl ring and a methoxy group at the distal phenyl ring seem to enhance the activity on KV10.1. The mechanism of action of the most potent analog 5 was investigated. A shift of the activation curve to more negative potentials and an apparent inactivation was observed. Since KV10.1 inhibitors can be interesting anticancer drug lead compounds, the effect of 5 was evaluated on cancerous and non-cancerous cell lines. Compound 5 showed to be cytotoxic and appeared to induce apoptosis in all the evaluated cell lines.

Published

2017

3. APETx4, a Novel Sea Anemone Toxin and a Modulator of the Cancer-Relevant Potassium Channel KV10.1

Author

Lien Moreels, Steve Peigneur, Diogo T. Galan, Edwin De Pauw, Lászlo Béress, Etienne Waelkens, Luis A. Pardo, Loïc Quinton, and Jan Tytgat

Subjects

sea anemone peptide, APETx, potassium channel, KV10.1, cancer, Biology (General), QH301-705.5

Abstract

The human ether-à-go-go channel (hEag1 or KV10.1) is a cancer-relevant voltage-gated potassium channel that is overexpressed in a majority of human tumors. Peptides that are able to selectively inhibit this channel can be lead compounds in the search for new anticancer drugs. Here, we report the activity-guided purification and electrophysiological characterization of a novel KV10.1 inhibitor from the sea anemone Anthopleura elegantissima. Purified sea anemone fractions were screened for inhibitory activity on KV10.1 by measuring whole-cell currents as expressed in Xenopus laevis oocytes using the two-microelectrode voltage clamp technique. Fractions that showed activity on Kv10.1 were further purified by RP-HPLC. The amino acid sequence of the peptide was determined by a combination of MALDI- LIFT-TOF/TOF MS/MS and CID-ESI-FT-ICR MS/MS and showed a high similarity with APETx1 and APETx3 and was therefore named APETx4. Subsequently, the peptide was electrophysiologically characterized on KV10.1. The selectivity of the toxin was investigated on an array of voltage-gated ion channels, including the cardiac human ether-à-go-go-related gene potassium channel (hERG or Kv11.1). The toxin inhibits KV10.1 with an IC50 value of 1.1 μM. In the presence of a similar toxin concentration, a shift of the activation curve towards more positive potentials was observed. Similar to the effect of the gating modifier toxin APETx1 on hERG, the inhibition of Kv10.1 by the isolated toxin is reduced at more positive voltages and the peptide seems to keep the channel in a closed state. Although the peptide also induces inhibitory effects on other KV and NaV channels, it exhibits no significant effect on hERG. Moreover, APETx4 induces a concentration-dependent cytotoxic and proapoptotic effect in various cancerous and noncancerous cell lines. This newly identified KV10.1 inhibitor can be used as a tool to further characterize the oncogenic channel KV10.1 or as a scaffold for the design and synthesis of more potent and safer anticancer drugs.

Published

2017

4. Astemizole analogues with reduced hERG inhibition as potent antimalarial compounds

Author

Steve Peigneur, Jan Tytgat, Steven De Jonghe, Jef Rozenski, Philippe E. Van den Steen, Leen Vandermosten, Piet Herdewijn, Lien Moreels, and Junjun Tian

Subjects

0301 basic medicine, congenital, hereditary, and neonatal diseases and abnormalities, Plasmodium falciparum, Clinical Biochemistry, hERG, Pharmaceutical Science, Pharmacology, Biochemistry, Antimalarials, Structure-Activity Relationship, 03 medical and health sciences, 0302 clinical medicine, Parasitic Sensitivity Tests, Transcriptional Regulator ERG, Drug Discovery, medicine, Humans, cardiovascular diseases, Molecular Biology, Dose-Response Relationship, Drug, Molecular Structure, biology, Chemistry, Organic Chemistry, Antagonist, Plasmodium parasite, Astemizole, 030104 developmental biology, 030220 oncology & carcinogenesis, biology.protein, Molecular Medicine, medicine.drug

Abstract

Astemizole is a H 1 -antagonist endowed with antimalarial activity, but has hERG liabilities. Systematic structural modifications of astemizole led to the discovery of analogues that display very potent activity as inhibitors of the growth of the Plasmodium parasite, but show a decreased hERG inhibition, when compared to astemizole. These compounds can be used as starting point for the development of a new class of antimalarials.

Published

2017

5. Expanding the pharmacological profile of κ-hefutoxin 1 and analogues: A focus on the inhibitory effect on the oncogenic channel Kv10.1

Author

Kim Vriens, Yoko Yamaguchi, Karin Thevissen, Bruno P. A. Cammue, Shunyi Zhu, Steve Peigneur, Etienne Waelkens, Jan Tytgat, Kazuki Sato, and Lien Moreels

Subjects

0301 basic medicine, chemistry.chemical_classification, biology, Physiology, Stereochemistry, Toxin, Voltage clamp, Peptide, biology.organism_classification, medicine.disease_cause, Biochemistry, Hefutoxin, Potassium channel, Yeast, 03 medical and health sciences, Cellular and Molecular Neuroscience, 030104 developmental biology, Endocrinology, chemistry, Fusarium culmorum, medicine, Pathogen

Abstract

Peptide toxins, such as scorpion peptides, are interesting lead compounds in the search for novel drugs. In this paper, the focus is on the scorpion peptide κ-hefutoxin 1. This peptide displays a cysteine-stabilized helix-loop-helix fold (CSα/α) and is known to be a weak Kv1.x inhibitor. Due to the low affinity of κ-hefutoxin 1 for these channels, it is assumed that the main target(s) of κ-hefutoxin 1 remain(s) unknown. In order to identify novel targets, electrophysiological measurements and antifungal assays were performed. The effect of κ-hefutoxin 1 was previously evaluated on a panel of 11 different voltage-gated potassium channels. Here, we extended this target screening with the oncogenic potassium channel Kv10.1. κ-Hefutoxin 1 was able to inhibit this channel in a dose-dependent manner (IC50 ∼ 26 μM). Although the affinity is rather low, this is the first peptide toxin ever described to be a Kv10.1 inhibitor. The structure-activity relationship of κ-hefutoxin 1 on Kv10.1 was investigated by testing eight κ-hefutoxin 1 variants using the two-electrode voltage clamp technique. Several important amino acid residues were identified; the functional dyad residues (Tyr5 and Lys19), N-terminal residues (Gly1 and His2) and the amidated C-terminal residue (Cys22). Since the CSα/α fold is also found in a class of antifungal plant peptides, the α-hairpinines, we investigated the antifungal activity of κ-hefutoxin 1. κ-Hefutoxin 1 showed low activity against the plant pathogen Fusarium culmorum and no activity against three other yeast and fungal species, even at high concentrations (∼100 μM).

Published

2017

6. Cross-reactive SARS-CoV-2 neutralizing antibodies from deep mining of early patient responses

Author

Kothai Parthiban, Sandra Ergueta-Carballo, Aneesh Karatt-Vellatt, Omodele Ashiru, Jacob D. Galson, David A. Matthews, Simon E. Hufton, Deividas Pazeraitis, Edward W. Masters, Claire Tebbutt, Richard Cowan, Mark D. Carr, Wing-Yiu Jason Lee, Sachin Surade, Paul E Pfeffer, Lucia Crippa, Line Ledsgaard, Sophie Millett, Richard J. C. Brown, Danielle Tongue, Emma M. Bentley, Lien Moreels, John McCafferty, Georgia Bullen, Ioannis Diamantopoulos, Krishna Chaitanya, David Tang, Matthew W. Bowler, Pedro Villar, Giada Mattiuzzo, Jane K. Osbourn, Kovilen Sawmynaden, Jamie Campbell, Rachael A. Leah, and Gareth Hall

Subjects

0301 basic medicine, Phage display, medicine.drug_class, Immunology, B-cell receptor, Biology, Antibodies, Viral, Monoclonal antibody, Epitope, Epitopes, 03 medical and health sciences, 0302 clinical medicine, Blocking antibody, medicine, Data Mining, Humans, antibodies, Immunology and Allergy, COVID-19 Serotherapy, Original Research, SARS-CoV-2 variants, convergence, SARS-CoV-2, Immunization, Passive, breakpoint cluster region, Antibodies, Monoclonal, COVID-19, RC581-607, Antibodies, Neutralizing, Virology, 030104 developmental biology, Immunization, Spike Glycoprotein, Coronavirus, biology.protein, Immunologic diseases. Allergy, phage display, Antibody, Cell Surface Display Techniques, 030217 neurology & neurosurgery

Abstract

Passive immunization using monoclonal antibodies will play a vital role in the fight against COVID-19. The recent emergence of viral variants with reduced sensitivity to some current antibodies and vaccines highlights the importance of broad cross-reactivity. This study describes deep-mining of the antibody repertoires of hospitalized COVID-19 patients using phage display technology and B cell receptor (BCR) repertoire sequencing to isolate neutralizing antibodies and gain insights into the early antibody response. This comprehensive discovery approach has yielded a panel of potent neutralizing antibodies which bind distinct viral epitopes including epitopes conserved in SARS-CoV-1. Structural determination of a non-ACE2 receptor blocking antibody reveals a previously undescribed binding epitope, which is unlikely to be affected by the mutations in any of the recently reported major viral variants including B.1.1.7 (from the UK), B.1.351 (from South Africa) and B.1.1.28 (from Brazil). Finally, by combining sequences of the RBD binding and neutralizing antibodies with the B cell receptor repertoire sequencing, we also describe a highly convergent early antibody response. Similar IgM-derived sequences occur within this study group and also within patient responses described by multiple independent studies published previously.

Published

2021

7. Evaluation of the suitability of ionic liquid-based liquid-liquid microextractions for blood protein removal

Author

Wim Dehaen, Marieke De Boeck, Eva Cuypers, Lien Moreels, and Jan Tytgat

Subjects

Liquid Phase Microextraction, Clinical Biochemistry, Serum albumin, Pharmaceutical Science, Ionic Liquids, Ion suppression in liquid chromatography–mass spectrometry, Analytical Chemistry, Xenobiotics, Benzodiazepines, Limit of Detection, Drug Discovery, Protein purification, Protein precipitation, Humans, Sample preparation, Spectroscopy, Chromatography, High Pressure Liquid, Whole blood, Chromatography, biology, Chemistry, Solid Phase Extraction, Albumin, Blood Proteins, Blood proteins, biology.protein

Abstract

The analysis of biological samples, such as whole blood, comes with several sample preparation challenges. Biological matrices often contain a variety of endogenous components that can interfere with the determination of xenobiotics. Especially blood plasma proteins (e.g. serum albumin) are known to interfere with electrospray ionization and result in analyte ion suppression. Sample preparation techniques should guarantee adequate removal of these biomolecules. The current study aims to determine to which extent proteins are removed from whole blood samples, using ionic liquid-based dispersive liquid-liquid microextraction (IL-DLLME). A qualitative comparison of the protein presence in extracts of IL-DLLME, solid-phase extraction (SPE) and protein precipitation (PP) was performed, using sodium dodecyl sulfate polyacrylamide gel electrophoresis (SDS-PAGE). Additionally, UV/VIS spectrophotometry was used to determine the protein content of a whole blood sample and IL-DLLME, SPE and PP extracts of the same sample. Finally, a quantitative comparison of matrix effects of benzodiazepines present in both whole blood and water samples. SDS-PAGE results showed that IL-DLLME extracts still contained proteins (i.e. albumin, hemoglobin); however, band intensities were comparable to SPE extracts. Spectrophotometric tests showed a total protein content of approximately 2 mg/mL in the final extracts. PP showed the highest protein extraction rate (19 mg/mL). Quantitative ME results showed no significant differences (α = 0.05) between blood and water IL-DLLME extracts. Overall, this is the first study to conclude that IL-DLLME is able to sufficiently remove blood proteins from whole blood samples, in order to avoid significant ion suppression. ispartof: Journal of Pharmaceutical and Biomedical Analysis vol:164 pages:57-61 ispartof: location:England status: published

Published

2018

8. APETx4, a Novel Sea Anemone Toxin and a Modulator of the Cancer-Relevant Potassium Channel Kv10.1

Author

Edwin De Pauw, Lászlo Béress, Luis A. Pardo, Diogo T. Galan, Loïc Quinton, Steve Peigneur, Lien Moreels, Jan Tytgat, and Etienne Waelkens

Subjects

0301 basic medicine, Voltage clamp, hERG, Xenopus, Pharmaceutical Science, Peptide, Biology, medicine.disease_cause, sea anemone peptide, 03 medical and health sciences, 0302 clinical medicine, APETx, Drug Discovery, medicine, cancer, potassium channel, KV10.1, lcsh:QH301-705.5, Pharmacology, Toxicology and Pharmaceutics (miscellaneous), Peptide sequence, Ion channel, chemistry.chemical_classification, Toxin, biology.organism_classification, Potassium channel, 030104 developmental biology, lcsh:Biology (General), chemistry, Biochemistry, 030220 oncology & carcinogenesis, biology.protein

Abstract

The human ether-à-go-go channel (hEag1 or KV10.1) is a cancer-relevant voltage-gated potassium channel that is overexpressed in a majority of human tumors. Peptides that are able to selectively inhibit this channel can be lead compounds in the search for new anticancer drugs. Here, we report the activity-guided purification and electrophysiological characterization of a novel KV10.1 inhibitor from the sea anemone Anthopleura elegantissima. Purified sea anemone fractions were screened for inhibitory activity on KV10.1 by measuring whole-cell currents as expressed in Xenopus laevis oocytes using the two-microelectrode voltage clamp technique. Fractions that showed activity on Kv10.1 were further purified by RP-HPLC. The amino acid sequence of the peptide was determined by a combination of MALDI- LIFT-TOF/TOF MS/MS and CID-ESI-FT-ICR MS/MS and showed a high similarity with APETx1 and APETx3 and was therefore named APETx4. Subsequently, the peptide was electrophysiologically characterized on KV10.1. The selectivity of the toxin was investigated on an array of voltage-gated ion channels, including the cardiac human ether-à-go-go-related gene potassium channel (hERG or Kv11.1). The toxin inhibits KV10.1 with an IC50 value of 1.1 μM. In the presence of a similar toxin concentration, a shift of the activation curve towards more positive potentials was observed. Similar to the effect of the gating modifier toxin APETx1 on hERG, the inhibition of Kv10.1 by the isolated toxin is reduced at more positive voltages and the peptide seems to keep the channel in a closed state. Although the peptide also induces inhibitory effects on other KV and NaV channels, it exhibits no significant effect on hERG. Moreover, APETx4 induces a concentration-dependent cytotoxic and proapoptotic effect in various cancerous and noncancerous cell lines. This newly identified KV10.1 inhibitor can be used as a tool to further characterize the oncogenic channel KV10.1 or as a scaffold for the design and synthesis of more potent and safer anticancer drugs. ispartof: Marine Drugs vol:15 issue:9 ispartof: location:Switzerland status: published

Published

2017

9. Identification of potential anticancer toxins: A focus on KV10.1 inhibitors

Author

Chinmaya Bhat, Edwin De Pauw, Lázlo Béress, Paula Kiuru, Diogo T. Galan, Jan Tytgat, Eero Mäki-Lohiluoma, Etienne Waelkens, Manuela Voráčová, Lien Moreels, Steve Peigneur, Luis A. Pardo, Loïc Quinton, and Jari Yli-Kauhaluoma

Subjects

Focus (computing), Computer science, Identification (biology), Computational biology, Toxicology

Published

2019

10. Expanding the pharmacological profile of κ-hefutoxin 1 and analogues: A focus on the inhibitory effect on the oncogenic channel K

Author

Lien, Moreels, Steve, Peigneur, Yoko, Yamaguchi, Kim, Vriens, Etienne, Waelkens, Shunyi, Zhu, Karin, Thevissen, Bruno P A, Cammue, Kazuki, Sato, and Jan, Tytgat

Subjects

Antifungal Agents, Helix-Loop-Helix Motifs, Scorpion Venoms, Antineoplastic Agents, Spores, Fungal, Ether-A-Go-Go Potassium Channels, Structure-Activity Relationship, Xenopus laevis, Potassium Channels, Voltage-Gated, Yeasts, Oocytes, Potassium Channel Blockers, Animals, Cysteine

Abstract

Peptide toxins, such as scorpion peptides, are interesting lead compounds in the search for novel drugs. In this paper, the focus is on the scorpion peptide κ-hefutoxin 1. This peptide displays a cysteine-stabilized helix-loop-helix fold (CSα/α) and is known to be a weak K

Published

2016

11. Synthesis of novel purpurealidin analogs and evaluation of their effect on the cancer-relevant potassium channel KV10.1

Author

Hannah Goovaerts, Farrah Zahed, Chinmaya Bhat, Steve Peigneur, Paula Kiuru, Luis A. Pardo, Manuela Voráčová, Lien Moreels, Jan Tytgat, Eero Mäki-Lohiluoma, Jari Yli-Kauhaluoma, Faculty of Pharmacy, Jari Yli-Kauhaluoma / Principal Investigator, Division of Pharmaceutical Chemistry and Technology, Pharmaceutical Design and Discovery group, and Drug Research Program

Subjects

0301 basic medicine, Xenopus, Cytotoxicity, Cancer Treatment, lcsh:Medicine, Apoptosis, Toxicology, Pathology and Laboratory Medicine, METABOLITES, 01 natural sciences, Chemical synthesis, Mice, 4-Butyrolactone, Neoplasms, Medicine and Health Sciences, Amines, lcsh:Science, DU145 cells, Multidisciplinary, Cell Death, Organic Compounds, Chemistry, SPONGE PSAMMAPLYSILLA-PURPU REA, Eukaryota, Animal Models, 3T3 Cells, CANCER, Potassium channel, APOPTOSIS, 3. Good health, Multidisciplinary Sciences, medicine.anatomical_structure, Experimental Organism Systems, Oncology, 317 Pharmacy, Cell Processes, Ether-A-Go-Go Potassium Channels, Xenopus Oocytes, Vertebrates, Physical Sciences, Science & Technology - Other Topics, Cell lines, Frogs, MARINE SPONGE, medicine.symptom, Biological cultures, Research Article, medicine.drug, BROMOTYROSINE ALKALOIDS, Stereochemistry, 3T3 cells, Amphibians, 03 medical and health sciences, Model Organisms, NIH 3T3 cells, Cell Line, Tumor, Potassium Channel Blockers, medicine, Animals, Humans, SPONGE PSAMMAPLYSILLA-PURPUREA, Science & Technology, Dose-Response Relationship, Drug, 010405 organic chemistry, lcsh:R, Organic Chemistry, Organisms, Chemical Compounds, Biology and Life Sciences, Potassium channel blocker, Cell Biology, 0104 chemical sciences, Research and analysis methods, HEK293 Cells, 030104 developmental biology, Mechanism of action, Cell culture, CELLS, lcsh:Q, Cultured Fibroblasts, Drug Screening Assays, Antitumor

Abstract

In the search for novel anticancer drugs, the potassium channel KV10.1 has emerged as an interesting cancer target. Here, we report a new group of KV10.1 inhibitors, namely the purpurealidin analogs. These alkaloids are produced by the Verongida sponges and are known for their wide variety of bioactivities. In this study, we describe the synthesis and characterization of 27 purpurealidin analogs. Structurally, bromine substituents at the central phenyl ring and a methoxy group at the distal phenyl ring seem to enhance the activity on KV10.1. The mechanism of action of the most potent analog 5 was investigated. A shift of the activation curve to more negative potentials and an apparent inactivation was observed. Since KV10.1 inhibitors can be interesting anticancer drug lead compounds, the effect of 5 was evaluated on cancerous and non-cancerous cell lines. Compound 5 showed to be cytotoxic and appeared to induce apoptosis in all the evaluated cell lines. ispartof: PLoS One vol:12 issue:12 ispartof: location:United States status: published

Published

2017