Your search keyword '"Louis Maes"' showing total 12 results

1. N

Author

Cai, Lin, Denise da Gama, Jaén Batista, Ana Lia, Mazzeti, Roberson, Donola Girão, Gabriel Melo, de Oliveira, Izet, Karalic, Fabian, Hulpia, Maria de Nazaré C, Soeiro, Louis, Maes, Guy, Caljon, and Serge, Van Calenbergh

Subjects

Leishmania, Mice, Structure-Activity Relationship, Purines, Trypanosoma cruzi, Animals, Chagas Disease, Nucleosides, Trypanocidal Agents

Abstract

Chagas disease and leishmaniasis are two poverty-related neglected tropical diseases that cause high mortality and morbidity. Current treatments suffer from severe limitations and novel, safer and more effective drugs are urgently needed. Both Trypanosoma cruzi and Leishmania are auxotrophic for purines and absolutely depend on uptake and assimilation of host purines. This led us to successfully explore purine nucleoside analogues as chemotherapeutic agents against these and other kinetoplastid infections. This study extensively explored the modification of the 6-amino group of tubercidin, a natural product with trypanocidal activity but unacceptable toxicity for clinical use. We found that mono-substitution of the amine with short alkyls elicits potent and selective antitrypanosomal and antileishmanial activity. The methyl analogue 15 displayed the best in vitro activity against both T. cruzi and L. infantum and high selectivity versus host cells. Oral administration for five consecutive days in an acute Chagas disease mouse model resulted in significantly reduced peak parasitemia levels (75, 89 and 96% with 12.5, 25 and 50 mg/kg/day, respectively). as well as increased animal survival rates with the lower doses (83 and 67% for 12.5 and 25 mg/kg/day, respectively).

Published

2021

2. Exploration of 6-methyl-7-(Hetero)Aryl-7-Deazapurine ribonucleosides as antileishmanial agents

Author

Cai Lin, Izet Karalic, An Matheeussen, Pim-Bart Feijens, Fabian Hulpia, Louis Maes, Guy Caljon, and Serge Van Calenbergh

Subjects

Leishmania, Pharmacology, NUCLEOSIDE, ANALOGS, Pharmacology. Therapy, Organic Chemistry, Antiprotozoal Agents, LEISHMANIA-DONOVANI, Biology and Life Sciences, Nucleosides, Purine Nucleosides, General Medicine, MECHANISMS, CYTOSTATIC ACTIVITY, Mice, Chemistry, Purines, Cricetinae, PURINE SALVAGE PATHWAY, Drug Discovery, Animals, Ribonucleosides, Leishmaniasis

Abstract

Leishmaniasis causes high mortality and morbidity in tropical and subtropical regions of Africa, Asia, the Americas and southern Europe, and is characterized by diverse clinical manifestations. As a neglected tropical disease, limited resources are allocated for antileishmanial drug discovery. The Leishmania parasite is deficient in de novo purine synthesis, and therefore acquires purines from the host and processes these using a purine salvage pathway. By making use of purine transport systems and interfering with this salvage pathway, purine (nucleoside) analogues might exert a selective detrimental impact on its growth and survival. In vitro screening of an in-house purine nucleoside library and analogue synthesis afforded the 6-methyl-7-(2-pyridyl)-7-deazapurine ribonucleoside analogue 18 as a promising hit. Optimization of the 7-substituent afforded 31 and 32 which displayed potent activity against wild-type and resistant L. infantum, intracellular amastigote and extracellular promastigote forms, and favorable selectivity versus primary mouse macrophages (M phi) and MRC-5 cells. Encouraged by the favorable in vitro metabolic stability of 32, an in vivo study was performed using an early curative L. infantum hamster model. When orally administrated at 50 mg/kg once daily (s.i.d) for 10 days, 32 was devoid of side effects, however, it only poorly reduced amastigote burdens in the major target organs.

Published

2022

3. Synthesis and evaluation of a collection of purine-like C-nucleosides as antikinetoplastid agents

Author

Serge Van Calenbergh, Guy Caljon, Jakob Bouton, Louis Maes, and Izet Karalic

Subjects

Antiparasitic, Purine, Trypanosoma, Trypanosoma cruzi, Trypanosoma brucei brucei, Antiprotozoal Agents, Trypanosoma brucei, 01 natural sciences, Structure-Activity Relationship, 03 medical and health sciences, chemistry.chemical_compound, Parasitic Sensitivity Tests, Drug Discovery, parasitic diseases, Medicine and Health Sciences, medicine, Leishmania infantum, Inosine, Purine metabolism, 030304 developmental biology, Leishmania, Pharmacology, 0303 health sciences, Dose-Response Relationship, Drug, Molecular Structure, biology, 010405 organic chemistry, Drug discovery, Pharmacology. Therapy, Organic Chemistry, Nucleosides, General Medicine, biology.organism_classification, 0104 chemical sciences, Chemistry, Biochemistry, chemistry, C-nucleosides, medicine.drug

Abstract

The kinetoplastid parasites Trypanosoma brucei, Trypanosoma cruzi and Leishmania spp. are the causative agents of neglected tropical diseases with a serious burden in several parts of the world. These parasites are incapable of synthesizing purines de novo, and therefore rely on ingenious purine salvage pathways to acquire and process purines from their host. Purine nucleoside analogs that may interfere with these pathways therefore constitute a privileged source of new antikinetoplastid agents. In this study, we synthetized a collection of C-nucleosides employing five different heterocyclic nucleobase surrogates. C-nucleosides are chemically and enzymatically stable and allow for extensive structural modification. Inspired by earlier 7-deazaadenosine nucleosides and known antileishmanial C-nucleosides, we introduced different modifications tailored towards antikinetoplastid activity. Both adenosine and inosine analogs were synthesized with the aim of discovering new antikinetoplastid hits and expanding knowledge of structure-activity relationships. Several promising hits with potent activity against Trypanosoma brucei, Trypanosoma cruzi and Leishmania infantum were discovered, and the nature of the nucleobase surrogate was found to have a profound influence on the selectivity profile of the compounds. (C) 2020 Elsevier Masson SAS. All rights reserved.

Published

2021

4. N-modification of 7-Deazapurine nucleoside analogues as Anti-Trypanosoma cruzi and anti-Leishmania agents: Structure-activity relationship exploration and In vivo evaluation

Author

Cai Lin, Denise da Gama Jaén Batista, Ana Lia Mazzeti, Roberson Donola Girão, Gabriel Melo de Oliveira, Izet Karalic, Fabian Hulpia, Maria de Nazaré C. Soeiro, Louis Maes, Guy Caljon, and Serge Van Calenbergh

Subjects

Pharmacology, Chemistry, Pharmacology. Therapy, parasitic diseases, Organic Chemistry, Drug Discovery, Human medicine, General Medicine, Biology

Abstract

Chagas disease and leishmaniasis are two poverty-related neglected tropical diseases that cause high mortality and morbidity. Current treatments suffer from severe limitations and novel, safer and more effective drugs are urgently needed. Both Trypanosoma cruzi and Leishmania are auxotrophic for purines and absolutely depend on uptake and assimilation of host purines. This led us to successfully explore purine nucleoside analogues as chemotherapeutic agents against these and other kinetoplastid infections. This study extensively explored the modification of the 6-amino group of tubercidin, a natural product with trypanocidal activity but unacceptable toxicity for clinical use. We found that mono-substitution of the amine with short alkyls elicits potent and selective antitrypanosomal and antileishmanial activity. The methyl analogue 15 displayed the best in vitro activity against both T. cruzi and L. infantum and high selectivity versus host cells. Oral administration for five consecutive days in an acute Chagas disease mouse model resulted in significantly reduced peak parasitemia levels (75, 89 and 96% with 12.5, 25 and 50 mg/kg/day, respectively). as well as increased animal survival rates with the lower doses (83 and 67% for 12.5 and 25 mg/kg/day, respectively).

Published

2022

5. Heteroaryl ether analogues of an antileishmanial 7-substituted 2-nitroimidazooxazine lead afford attenuated hERG risk: In vitro and in vivo appraisal

Author

William A. Denny, Zhenkun Ma, Eric Chatelain, Scott G. Franzblau, Andrew J. Marshall, Stéphanie Braillard, Andrew M. Thompson, Delphine Launay, Christopher B. Cooper, Patrick D. O'Connor, Louis Maes, Vanessa Yardley, Baojie Wan, and Suman Gupta

Subjects

Male, Pyridines, hERG, Leishmania donovani, Antiprotozoal Agents, Ether, Oxazines, Pharmacology, 01 natural sciences, Hydrocarbons, Aromatic, 03 medical and health sciences, chemistry.chemical_compound, Mice, Structure-Activity Relationship, Parasitic Sensitivity Tests, In vivo, Cricetinae, Drug Discovery, Animals, Humans, Biology, 030304 developmental biology, chemistry.chemical_classification, 0303 health sciences, biology, Dose-Response Relationship, Drug, 010405 organic chemistry, Pharmacology. Therapy, Organic Chemistry, General Medicine, biology.organism_classification, 0104 chemical sciences, Bioavailability, Disease Models, Animal, chemistry, Solubility, Pretomanid, biology.protein, Leishmaniasis, Visceral, Female, Human medicine, Enantiomer

Abstract

Previous investigation of the potent antileishmanial properties of antitubercular 7-substituted 2-nitroimidazo[2,1-b][1,3]oxazines with biaryl side chains led to our development of a new clinical candidate for visceral leishmaniasis (DNDI-0690). Within a collaborative backup program, a racemic monoaryl lead (3) possessing comparable activity in mice but a greater hERG liability formed the starting point for our pursuit of efficacious second generation analogues having good solubility and safety. Asymmetric synthesis and appraisal of its enantiomers first established that chiral preferences for in vivo efficacy were species dependent and that neither form afforded a reduced hERG risk. However, in line with our findings in a structurally related series, less lipophilic heteroaryl ethers provided significant solubility enhancements (up to 16-fold) and concomitantly attenuated hERG inhibition. One promising pyridine derivative (49) displayed 100% oral bioavailability in mice and delivered a 96% parasite burden reduction when dosed at 50 mg/kg in a Leishmania donovani mouse model of visceral leishmaniasis.

Published

2020

6. C6-O-alkylated 7-deazainosine nucleoside analogues : discovery of potent and selective anti-sleeping sickness agents

Author

Serge Van Calenbergh, Guy Caljon, Ibrahim A. Alfayez, Dorien Mabille, Gustavo D. Campagnaro, Jakob Bouton, Harry P. de Koning, Fabian Hulpia, and Louis Maes

Subjects

Purine, Alkylation, Inosine nucleoside analogues, 01 natural sciences, chemistry.chemical_compound, SUBSTRATE RECOGNITION MOTIFS, Parasitic Sensitivity Tests, PURINE, Drug Discovery, TUBERCIDIN, Medicine and Health Sciences, Parasite nucleoside transporter, Trypanosoma brucei, Cytotoxicity, Purine metabolism, 0303 health sciences, Molecular Structure, biology, Chemistry, Pharmacology. Therapy, Nucleosides, Biological activity, General Medicine, ADENOSINE, Trypanocidal Agents, Biochemistry, TRYPANOSOMA-BRUCEI, Cell Survival, Trypanosoma brucei brucei, Tubercidin, Cell Line, Structure-Activity Relationship, 03 medical and health sciences, Humans, 030304 developmental biology, Pharmacology, Dose-Response Relationship, Drug, INOSINE ANALOGS, 010405 organic chemistry, GLYCOSYLATION, Organic Chemistry, biology.organism_classification, Inosine, 0104 chemical sciences, ACID RELATED-COMPOUNDS, Nucleoside, BIOLOGICAL-ACTIVITY, RESISTANCE

Abstract

African trypanosomiasis, a deadly infectious disease caused by the protozoan Trypanosoma brucei spp., is spread to new hosts by bites of infected tsetse flies. Currently approved therapies all have their specific drawbacks, prompting a search for novel therapeutic agents. T. brucei lacks the enzymes necessary to forge the purine ring from amino acid precursors, rendering them dependent on the uptake and interconversion of host purines. This dependency renders analogues of purines and corresponding nucleosides an interesting source of potential anti-T. brucei agents. In this study, we synthesized and evaluated a series of 7-substituted 7-deazainosine derivatives and found that 6-O-alkylated analogues in particular showed highly promising in vitro activity with EC50 values in the mid-nanomolar range. SAR investigation of the O-alkyl chain showed that antitrypanosomal activity increased, and also cytotoxicity, with alkyl chain length, at least in the linear alkyl chain series. However, this could be attenuated by introducing a terminal branch point, resulting in the highly potent and selective analogues, 36, 37 and 38. No resistance related to transporter-mediated uptake could be identified, earmarking several of these analogues for further in vivo follow-up studies. (C) 2020 Elsevier Masson SAS. All rights reserved.

Published

2020

7. Optimization of the pharmacokinetic properties of potent anti-trypanosomal triazine derivatives

Author

Irene G. Salado, Tomas Verdeyen, Adrienn Baán, Louis Maes, Pieter Van der Veken, An Matheeussen, Koen Augustyns, Guy Caljon, and Filip Kiekens

Subjects

0301 basic medicine, Phenotypic screening, Trypanosoma brucei brucei, 030106 microbiology, Pharmacology, Trypanosoma brucei, Tropolone, Mice, Structure-Activity Relationship, 03 medical and health sciences, chemistry.chemical_compound, Pharmacokinetics, parasitic diseases, Drug Discovery, medicine, Animals, Humans, African trypanosomiasis, Cytotoxicity, Trypanosoma cruzi, Triazine, biology, Triazines, Pharmacology. Therapy, Organic Chemistry, Plasmodium falciparum, General Medicine, biology.organism_classification, medicine.disease, Trypanocidal Agents, Disease Models, Animal, Trypanosomiasis, African, 030104 developmental biology, chemistry

Abstract

Human African trypanosomiasis is causing thousands of deaths every year in the rural areas of sub-saharan Africa. There is a high unmet medical need since the approved drugs are poorly efficacious, show considerable toxicity and are not easy to administer. This work describes the optimization of the pharmacokinetic properties of a previously published family of triazine lead compounds. One compound (35 (UAMC-03011)) with potent anti-trypanosomal activity and no cytotoxicity was selected for further study because of its good microsomal stability and high selectivity for Trypanosoma brucei over a panel including Trypanosoma cruzi, L.eishmania infantum, and Plasmodium falciparum. In vivo pharmacokinetic parameters were determined and the compound was studied in an acute in vivo mouse disease model. One of the important learnings of this study was that the rate of trypanocidal activity is an important parameter during the lead optimization process.

Published

2018

8. Revisiting tubercidin against kinetoplastid parasites : aromatic substitutions at position 7 improve activity and reduce toxicity

Author

Serge Van Calenbergh, Gustavo D. Campagnaro, Kristof Van Hecke, Harry P. de Koning, Louis Maes, Mirko Scortichini, Fabian Hulpia, and Guy Caljon

Subjects

Purine, Trypanosoma brucei brucei, Adenosine kinase, Nucleoside Transport Proteins, Trypanosoma brucei, Nucleoside transporter, 01 natural sciences, Tubercidin, 03 medical and health sciences, chemistry.chemical_compound, Mice, Structure-Activity Relationship, Drug Discovery, parasitic diseases, Animals, Kinetoplastida, Cytotoxicity, Biology, 030304 developmental biology, Pharmacology, 0303 health sciences, biology, 010405 organic chemistry, Chemistry, Pharmacology. Therapy, Organic Chemistry, Transporter, Biological Transport, General Medicine, biology.organism_classification, Trypanocidal Agents, 0104 chemical sciences, Biochemistry, biology.protein, Human medicine, Nucleoside

Abstract

The nucleoside antibiotic tubercidin displays strong activity against different target organisms, but it is notoriously toxic to mammalian cells. However, the effects of tubercidin against T. brucei parasites inspired us to synthesize several C7 substituted analogs for in vitro evaluation, in order to find suitable hit compounds. C7 Deazaadenosines substituted with electron-poor phenyl groups were found to have micromolar activity against T. brucei in vitro. Replacement of the phenyl for a pyridine ring gave compound 13 with submicromolar potency and much-attenuated cytotoxicity compared to tubercidin. The veterinary pathogen T. congolense was equally affected by 13in vitro. Transporter studies in T. b. brucei indicated that 13 is taken up efficiently by both the P1 and P2 adenosine transporters, making the occurrence of transporter-related resistance and cross-resistance with diamidine drugs such as diminazene aceturate and pentamidine as well as with melaminophenyl arsenicals unlikely. Evaluation of the in vitro metabolic stability of analog 13 indicated that this analog was significantly metabolized in mouse microsomal fractions, precluding further in vivo evaluation in mouse models of HAT.

Published

2019

9. The synthesis and in vitro biological evaluation of novel fluorinated tetrahydrobenzo[j]phenanthridine-7,12-diones against Mycobacterium tuberculosis

Author

Tatiana Piller, Louis Maes, Pieter Claes, Elena Semina, Davie Cappoen, Paul Cos, Peter Delputte, Freya Cools, Olivier Neyrolles, Francis Holvoet, An Matheeussen, Kevin Van Calster, Norbert De Kimpe, Sven Mangelinckx, Tamara Meiresonne, Guy Caljon, Maíra Bidart de Macedo, and Eveline Torfs

Subjects

Hydrocarbons, Fluorinated, Stereochemistry, Antitubercular Agents, Microbial Sensitivity Tests, medicine.disease_cause, Cell Line, Mycobacterium tuberculosis, chemistry.chemical_compound, Mice, Structure-Activity Relationship, Drug Discovery, medicine, Extracellular, Animals, Humans, Mycothione reductase, Pharmacology, chemistry.chemical_classification, Benzophenanthridines, Reactive oxygen species, Phenanthridine, biology, Dose-Response Relationship, Drug, Molecular Structure, Pharmacology. Therapy, Macrophages, Organic Chemistry, General Medicine, biology.organism_classification, In vitro, chemistry, Microsome, Genotoxicity

Abstract

Tuberculosis (TB) still has a major impact on public health. In order to efficiently eradicate this life-threatening disease, the exploration of novel anti-TB drugs is of paramount importance. As part of our program to design new 2-azaanthraquinones with anti-mycobacterial activity, various “out-of-plane” tetrahydro- and octahydrobenzo[j]phenanthridinediones were synthesized. In this study, the scaffold of the most promising hits was further optimized in an attempt to improve the bioactivity and to decrease enzymatic degradation. The rudiment bio-evaluation of a small library of fluorinated tetrahydrobenzo[j]phenanthridine-7,12-dione derivatives indicated no significant improvement of the bio-activity against intracellular and extracellular Mycobacterium tuberculosis (Mtb). Though, the derivatives showed an acceptable toxicity against J774A.1 macrophages and early signs of genotoxicity were absent. All derivatives showed to be metabolic stabile in the presence of both phase I and phase II murine or human microsomes. Finally, the onset of reactive oxygen species within Mtb after exposure to the derivatives was measured by electron paramagnetic resonance (EPR). Results showed that the most promising fluorinated derivative is still a possible candidate for the subversive inhibition of mycothione reductase.

Published

2018

10. Novel triazine dimers with potent antitrypanosomal activity

Author

Muthusamy Venkatraj, Pieter Van der Veken, Jan Heeres, Guy Caljon, Koen Augustyns, Jurgen Joossens, Louis Maes, Paul J. Lewi, and Irene G. Salado

Subjects

0301 basic medicine, Male, Trypanosoma brucei rhodesiense, Cell Survival, Phenotypic screening, Trypanosoma cruzi, Trypanosoma brucei brucei, Antiprotozoal Agents, Pharmacology, Trypanosoma brucei, 01 natural sciences, 03 medical and health sciences, chemistry.chemical_compound, Mice, Structure-Activity Relationship, Usually fatal, Drug Discovery, medicine, Animals, Humans, African trypanosomiasis, Leishmania infantum, Biology, Triazine, Cell Proliferation, biology, Dose-Response Relationship, Drug, Molecular Structure, 010405 organic chemistry, Triazines, Pharmacology. Therapy, Organic Chemistry, Tsetse fly, General Medicine, Fibroblasts, medicine.disease, biology.organism_classification, Reverse transcriptase, 3. Good health, 0104 chemical sciences, 030104 developmental biology, chemistry, Reverse Transcriptase Inhibitors, Human medicine, %22">Glossina , Dimerization

Abstract

Human African trypanosomiasis (HAT), also known as sleeping sickness is a parasitic disease transmitted by the bite of the 'Glossina' insect, commonly known as the tsetse fly. This disease affects mostly poor populations living in remote rural areas of Africa. Untreated, it is usually fatal. Currently, safe and effective treatments against this disease are lacking. Phenotypic screening of triazine non-nucleoside HIV-1 reverse transcriptase inhibitors (monomers) resulted in potent and selective antitrypanosomal compounds. This serendipitous discovery and the presence of dimers in many compounds active against these neglected tropical diseases prompted us to investigate antitrypanosomal activity of triazine dimers. Optimization of the triazine dimers resulted in 3,3'-(((ethane-1,2-diylbis(azanediyl))bis(4-(mesityloxy)-1,3,5-triazine-6,2-diyl))bis(azanediyl))dibenzonitrile (compound 38), a compound with very potent in vitro and moderate in vivo antitrypanosomal activity.

Published

2017

11. Synthesis and antimalarial activity of new analogues of amodiaquine

Author

Louis Maes, Sandrine Delarue-Cochin, Elisabeth Mouray, Christian Sergheraert, Emilia Păunescu, Philippe Grellier, Patricia Melnyk, Molécules de Communication et Adaptation des Micro-organismes (MCAM), and Muséum national d'Histoire naturelle (MNHN)-Centre National de la Recherche Scientifique (CNRS)

Subjects

Magnetic Resonance Spectroscopy, Plasmodium berghei, Stereochemistry, [SDV]Life Sciences [q-bio], Amodiaquine, 01 natural sciences, Chemical synthesis, Cell Line, Antimalarials, Mice, Drug Discovery, medicine, Animals, Humans, [CHIM]Chemical Sciences, Cytotoxicity, Chromatography, High Pressure Liquid, ComputingMilieux_MISCELLANEOUS, Pharmacology, chemistry.chemical_classification, biology, 010405 organic chemistry, Organic Chemistry, Aromatic amine, Hydrogen Bonding, Plasmodium falciparum, Biological activity, General Medicine, biology.organism_classification, 0104 chemical sciences, 3. Good health, 010404 medicinal & biomolecular chemistry, [SDV.MP]Life Sciences [q-bio]/Microbiology and Parasitology, chemistry, Female, Amine gas treating, medicine.drug

Abstract

In order to determine the real significance of the 4'-phenolic group in the antimalarial activity and/or cytotoxicity of amodiaquine (AQ), analogues for which this functionality was shifted or modified were synthesized. Good in vitro antimalarial activity was obtained for compounds unable to form intramolecular hydrogen bond. Among the compounds synthesized, new amino derivative 5 displayed the greatest selectivity index towards the most CQ-resistant strain tested and was active in mice infected by Plasmodium berghei.

Published

2008

12. Novel inhibitors of Trypanosoma cruzi dihydrofolate reductase

Author

Fabio Zuccotto, Dolores Gonzalez Pacanowska, Raffaella Di Lucrezia, Reto Brun, Luis M. Ruiz-Pérez, Louis Maes, Ian H. Gilbert, Shafinaz F. Chowdhury, Marketa Zvelebil, and Isabel Leal

Subjects

Trypanosoma brucei rhodesiense, Chagas disease, Trypanosoma cruzi, Drug Evaluation, Preclinical, Trypanosoma brucei, Cell Line, Inhibitory Concentration 50, Mice, parasitic diseases, Drug Discovery, Dihydrofolate reductase, medicine, Animals, Chagas Disease, Enzyme Inhibitors, Pharmacology, biology, Muscles, Organic Chemistry, Kinetoplastida, General Medicine, biology.organism_classification, medicine.disease, Virology, Rats, Disease Models, Animal, Tetrahydrofolate Dehydrogenase, Databases as Topic, Biochemistry, Enzyme inhibitor, Drug Design, biology.protein, Trypanosoma, Folic Acid Antagonists

Abstract

There is an urgent need for the development of new drugs to treat Chagas' disease, which is caused by the protozoan parasite Trypanosoma cruzi . The enzyme dihydrofolate reductase (DHFR) has been a very successful drug target in a number of diseases and we decided to investigate it as a potential drug target for Chagas' disease. A homology model of the enzyme was used to search the Cambridge Structural Database using the program dock 3.5. Compounds were then tested against the enzyme and the whole parasite. Compounds were also screened against the related parasite, Trypanosoma brucei .

Published

2001