Your search keyword '"Comini MA"' showing total 12 results

1. Selenosugars targeting the infective stage of Trypanosoma brucei with high selectivity.

Author

Dibello E, Oddone N, Franco J, Illyés TZ, Medeiros A, Kiss A, Hőgye F, Kövér KE, Szilágyi L, and Comini MA

Subjects

Animals, Mice, Humans, Homeostasis, Oxidation-Reduction, Trypanosoma brucei brucei, Trypanosoma, Trypanosomiasis, African drug therapy, Trypanocidal Agents pharmacology, Trypanocidal Agents therapeutic use

Abstract

Earlier evidences showed that diglycosyl diselenides are active against the infective stage of African trypanosomes (top hits IC 50 0.5 and 1.5 μM) but poorly selective (selectivity index <10). Here we extended the study to 33 new seleno-glycoconjugates with the aim to improve potency and selectivity. Three selenoglycosides and three glycosyl selenenylsulfides displayed IC 50 against bloodstream Trypanosoma brucei in the sub-μM range (IC 50 0.35-0.77 μM) and four of them showed an improved selectivity (selectivity index >38-folds vs. murine and human macrohages). For the glycosyl selenylsulfides, the anti-trypanosomal activity was not significantly influenced by the nature of the moiety attached to the sulfur atom. Except for a quinoline-, and to a minor extent a nitro-derivative, the most selective hits induced a rapid (within 60 min) and marked perturbation of the LMWT-redox homeostasis. The formation of selenenylsulfide glycoconjugates with free thiols has been identified as a potential mechanism involved in this process., Competing Interests: Declaration of competing interest The authors declare no competing financial interest., (Copyright © 2024 The Authors. Published by Elsevier Ltd.. All rights reserved.)

Published

2024

2. Drugging the Undruggable Trypanosoma brucei Monothiol Glutaredoxin 1.

Author

Favaro A, Bolcato G, Comini MA, Moro S, Bellanda M, and Sturlese M

Subjects

Humans, Female, Animals, Cattle, Horses, Glutaredoxins chemistry, Glutathione metabolism, Trypanosoma brucei brucei metabolism, Trypanosoma metabolism, Trypanosomiasis, African drug therapy

Abstract

Trypanosoma brucei is a species of kinetoplastid causing sleeping sickness in humans and nagana in cows and horses. One of the peculiarities of this species of parasites is represented by their redox metabolism. One of the proteins involved in this redox machinery is the monothiol glutaredoxin 1 (1CGrx1) which is characterized by a unique disordered N-terminal extension exclusively conserved in trypanosomatids and other organisms. This region modulates the binding profile of the glutathione/trypanothione binding site, one of the functional regions of 1CGrx1. No endogenous ligands are known to bind this protein which does not present well-shaped binding sites, making it target particularly challenging to target. With the aim of targeting this peculiar system, we carried out two different screenings: (i) a fragment-based lead discovery campaign directed to the N-terminal as well as to the canonical binding site of 1CGrx1; (ii) a structure-based virtual screening directed to the 1CGrx1 canonical binding site. Here we report a small molecule that binds at the glutathione binding site in which the binding mode of the molecule was deeply investigated by Nuclear Magnetic Resonance (NMR). This compound represents an important step in the attempt to develop a novel strategy to interfere with the peculiar Trypanosoma Brucei redox system, making it possible to shed light on the perturbation of this biochemical machinery and eventually to novel therapeutic possibilities.

Published

2023

3. Novel distamycin analogues that block the cell cycle of African trypanosomes with high selectivity and potency.

Author

Franco J, Scarone L, and Comini MA

Subjects

Animals, Female, Macrophages parasitology, Mice, Mice, Inbred BALB C, Thiazoles chemistry, Trypanocidal Agents chemistry, Trypanosoma parasitology, Trypanosomiasis, African parasitology, Cell Cycle drug effects, Distamycins chemistry, Macrophages drug effects, Thiazoles pharmacology, Trypanocidal Agents pharmacology, Trypanosoma drug effects, Trypanosoma brucei brucei drug effects, Trypanosomiasis, African drug therapy

Abstract

Polyamides-based compounds related to the Streptomycetal distamycin and netropsin are potent cytostatic molecules that bind to AT-rich regions of the minor groove of the DNA, hence interfering with DNA replication and transcription. Recently, derivatives belonging to this scaffold have been reported to halt the proliferation of deadly African trypanosomes by different and unrelated mechanisms. Here we describe the synthesis and preliminary characterization of the anti-trypanosomal mode of action of new potent and selective distamycin analogues. Two tri-heterocyclic derivatives containing a central N-methyl pyrrole ring (16 and 17) displayed high activity (EC 50  < 20 nM) and selectivity (selectivity index >5000 with respect to mammalian macrophages) against the infective form of T. brucei. Both compounds caused cell cycle arrest by blocking the replication of the mitochondrial DNA but without affecting its integrity. This mode of action clearly differs from that reported for classical minor groove binder (MGB) drugs, which induce the degradation of the mitochondrial DNA. In line with this, in vitro assays suggest that 16 and 17 have a comparatively lower affinity for different template DNAs than the MGB drug diminazene. Therapeutic efficacy studies and stability assays suggest that the pharmacological properties of the hits should be optimized. The compounds can be rated as excellent scaffolds for the design of highly potent and selective anti-T. brucei agents., (Copyright © 2020 Elsevier Masson SAS. All rights reserved.)

Published

2020

4. Kinetic studies reveal a key role of a redox-active glutaredoxin in the evolution of the thiol-redox metabolism of trypanosomatid parasites.

Author

Manta B, Möller MN, Bonilla M, Deambrosi M, Grunberg K, Bellanda M, Comini MA, and Ferrer-Sueta G

Subjects

Animals, Catalytic Domain, Glutaredoxins chemistry, Humans, Kinetics, Oxidation-Reduction, Biological Evolution, Glutaredoxins metabolism, Sulfhydryl Compounds metabolism, Trypanosoma metabolism

Abstract

Trypanosomes are flagellated protozoan parasites (kinetoplastids) that have a unique redox metabolism based on the small dithiol trypanothione (T(SH) 2 ). Although GSH may still play a biological role in trypanosomatid parasites beyond being a building block of T(SH) 2 , most of its functions are replaced by T(SH) 2 in these organisms. Consequently, trypanosomes have several enzymes adapted to using T(SH) 2 instead of GSH, including the glutaredoxins (Grxs). However, the mechanistic basis of Grx specificity for T(SH) 2 is unknown. Here, we combined fast-kinetic and biophysical approaches, including NMR, MS, and fluorescent tagging, to study the redox function of Grx1, the only cytosolic redox-active Grx in trypanosomes. We observed that Grx1 reduces GSH-containing disulfides (including oxidized trypanothione) in very fast reactions ( k > 5 × 10 5 m -1 s -1 ). We also noted that disulfides without a GSH are much slower oxidants, suggesting a strongly selective binding of the GSH molecule. Not surprisingly, oxidized Grx1 was also reduced very fast by T(SH) 2 (4.8 × 10 6 m -1 s -1 ); however, GSH-mediated reduction was extremely slow (39 m -1 s -1 ). This kinetic selectivity in the reduction step of the catalytic cycle suggests that Grx1 uses preferentially a dithiol mechanism, forming a disulfide on the active site during the oxidative half of the catalytic cycle and then being rapidly reduced by T(SH) 2 in the reductive half. Thus, the reduction of glutathionylated substrates avoids GSSG accumulation in an organism lacking GSH reductase. These findings suggest that Grx1 has played an important adaptive role during the rewiring of the thiol-redox metabolism of kinetoplastids., (© 2019 Manta et al.)

Published

2019

5. The lineage-specific, intrinsically disordered N-terminal extension of monothiol glutaredoxin 1 from trypanosomes contains a regulatory region.

Author

Sturlese M, Manta B, Bertarello A, Bonilla M, Lelli M, Zambelli B, Grunberg K, Mammi S, Comini MA, and Bellanda M

Subjects

Amino Acid Sequence, Catalytic Domain physiology, Glutaredoxins metabolism, Glutathione metabolism, Oxidation-Reduction, Protein Conformation, Protein Multimerization physiology, Iron-Sulfur Proteins metabolism, Regulatory Sequences, Nucleic Acid physiology, Sulfur metabolism, Trypanosoma metabolism, Trypanosoma brucei brucei metabolism

Abstract

Glutaredoxins (Grx) are small proteins conserved throughout all the kingdoms of life that are engaged in a wide variety of biological processes and share a common thioredoxin-fold. Among them, class II Grx are redox-inactive proteins involved in iron-sulfur (FeS) metabolism. They contain a single thiol group in their active site and use low molecular mass thiols such as glutathione as ligand for binding FeS-clusters. In this study, we investigated molecular aspects of 1CGrx1 from the pathogenic parasite Trypanosoma brucei brucei, a mitochondrial class II Grx that fulfills an indispensable role in vivo. Mitochondrial 1CGrx1 from trypanosomes differs from orthologues in several features including the presence of a parasite-specific N-terminal extension (NTE) whose role has yet to be elucidated. Previously we have solved the structure of a truncated form of 1CGrx1 containing only the conserved glutaredoxin domain but lacking the NTE. Our aim here is to investigate the effect of the NTE on the conformation of the protein. We therefore solved the NMR structure of the full-length protein, which reveals subtle but significant differences with the structure of the NTE-less form. By means of different experimental approaches, the NTE proved to be intrinsically disordered and not involved in the non-redox dependent protein dimerization, as previously suggested. Interestingly, the portion comprising residues 65-76 of the NTE modulates the conformational dynamics of the glutathione-binding pocket, which may play a role in iron-sulfur cluster assembly and delivery. Furthermore, we disclosed that the class II-strictly conserved loop that precedes the active site is critical for stabilizing the protein structure. So far, this represents the first communication of a Grx containing an intrinsically disordered region that defines a new protein subgroup within class II Grx.

Published

2018

6. Diglycosyl diselenides alter redox homeostasis and glucose consumption of infective African trypanosomes.

Author

Franco J, Sardi F, Szilágyi L, Kövér KE, Fehér K, and Comini MA

Subjects

Animals, Glycosylation, Homeostasis physiology, Macrophages drug effects, Macrophages parasitology, Metabolic Networks and Pathways drug effects, Mice, Oxidation-Reduction drug effects, Selenium chemistry, Selenium pharmacology, Antiprotozoal Agents pharmacology, Glucose metabolism, Homeostasis drug effects, Trypanosoma drug effects, Trypanosoma metabolism

Abstract

With the aim to develop compounds able to target multiple metabolic pathways and, thus, to lower the chances of drug resistance, we investigated the anti-trypanosomal activity and selectivity of a series of symmetric diglycosyl diselenides and disulfides. Of 18 compounds tested the fully acetylated forms of di-β-D-glucopyranosyl and di-β-D-galactopyranosyl diselenides (13 and 15, respectively) displayed strong growth inhibition against the bloodstream stage of African trypanosomes (EC 50 0.54 μM for 13 and 1.49 μM for 15) although with rather low selectivity (SI < 10 assayed with murine macrophages). Nonacetylated versions of the same sugar diselenides proved to be, however, much less efficient or completely inactive to suppress trypanosome growth. Significantly, the galactosyl (15), and to a minor extent the glucosyl (13), derivative inhibited glucose catabolism but not its uptake. Both compounds induced redox unbalance in the pathogen. In vitro NMR analysis indicated that diglycosyl diselenides react with glutathione, under physiological conditions, via formation of selenenylsulfide bonds. Our results suggest that non-specific cellular targets as well as actors of the glucose and the redox metabolism of the parasite may be affected. These molecules are therefore promising leads for the development of novel multitarget antitrypanosomal agents., (Copyright © 2017 The Authors. Published by Elsevier Ltd.. All rights reserved.)

Published

2017

7. In vitro activity and mode of action of distamycin analogues against African trypanosomes.

Author

Franco J, Medeiros A, Benítez D, Perelmuter K, Serra G, Comini MA, and Scarone L

Subjects

Africa, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, Cell Membrane drug effects, Lysosomes drug effects, Oxidation-Reduction drug effects, Thiazoles chemical synthesis, Trypanocidal Agents pharmacology, Trypanosoma brucei brucei drug effects, Distamycins pharmacology, Trypanocidal Agents chemistry, Trypanosoma drug effects

Abstract

Distamycin, a natural polyamide containing three heterocycle rings with a polar end, has inspired several groups to prepare synthetic analogues, which proved to have anti-trypanosomal and anti-tumoral activity. We describe the synthesis of bi and tri thiazoles amides that harbor different substitutions at their ends and the evaluation of their anti-Trypanosoma brucei activity. The most active compound 10b showed better biological activity (EC 50 310 nM and selectivity index 16) than the control drug nifurtimox (EC 50 15 μM and selectivity index 10). Studies on the mode of action show that the parasiticidal activity of 10b originates from disruption of lysosomal homeostasis, which is followed by release of redox active iron, an increase in oxidizing species and collapse of cell membrane integrity. In this respect, our study suggests that non-charged lipophylic distamycins destabilize cell membranes., (Copyright © 2017 Elsevier Masson SAS. All rights reserved.)

Published

2017

8. Mono- and dithiol glutaredoxins in the trypanothione-based redox metabolism of pathogenic trypanosomes.

Author

Comini MA, Krauth-Siegel RL, and Bellanda M

Subjects

Amino Acid Sequence, Animals, Conserved Sequence, Glutaredoxins chemistry, Glutathione metabolism, Humans, Models, Molecular, Molecular Sequence Data, Oxidation-Reduction, Protein Conformation, Protozoan Proteins chemistry, Spermidine metabolism, Trypanosomiasis parasitology, Glutaredoxins physiology, Glutathione analogs & derivatives, Protozoan Proteins physiology, Spermidine analogs & derivatives, Trypanosoma enzymology

Abstract

Significance: Glutaredoxins are ubiquitous small thiol proteins of the thioredoxin-fold superfamily. Two major groups are distinguished based on their active sites: the dithiol (2-C-Grxs) and the monothiol (1-C-Grxs) glutaredoxins with a CXXC and a CXXS active site motif, respectively. Glutaredoxins are involved in cellular redox and/or iron sulfur metabolism. Usually their functions are closely linked to the glutathione system. Trypanosomatids, the causative agents of several tropical diseases, rely on trypanothione as principal low molecular mass thiol, and their glutaredoxins readily react with the unique bis(glutathionyl) spermidine conjugate., Recent Advances: Two 2-C-Grxs and three 1-C-Grxs have been identified in pathogenic trypanosomatids. The 2-C-Grxs catalyze the reduction of glutathione disulfide by trypanothione and display reductase activity towards protein disulfides, as well as protein-glutathione mixed disulfides. In vitro, all three 1-C-Grxs as well as the cytosolic 2-C-Grx of Trypanosoma brucei can complex an iron-sulfur cluster. Recently the structure of the 1-C-Grx1 has been solved by NMR spectroscopy. The structure is very similar to those of other 1-C-Grxs, with some differences in the loop containing the conserved cis-Pro and the surface charge distribution., Critical Issues: Although four of the five trypanosomal glutaredoxins proved to coordinate an iron-sulfur cluster in vitro, the physiological role of the mitochondrial and cytosolic proteins, respectively, has only started to be unraveled., Future Directions: The use of trypanothione by the glutaredoxins has established a novel role for this parasite-specific dithiol. Future work should reveal if these differences can be exploited for the development of novel antiparasitic drugs.

Published

2013

9. Preparative enzymatic synthesis of trypanothione and trypanothione analogues.

Author

Comini MA, Dirdjaja N, Kaschel M, and Krauth-Siegel RL

Subjects

Disulfides metabolism, Drug Design, Glutathione biosynthesis, Molecular Sequence Data, Spermidine biosynthesis, Substrate Specificity, Amide Synthases genetics, Crithidia fasciculata enzymology, Glutathione analogs & derivatives, Spermidine analogs & derivatives, Trypanocidal Agents metabolism, Trypanosoma enzymology

Abstract

Trypanosomatids, the causative agents of several tropical diseases, have a unique thiol metabolism based on trypanothione [bis(glutathionyl)spermidine]. Enzymes of the pathway are attractive drug target molecules but the availability of trypanothione remains an obstacle. Here, we present a convenient method for the production of trypanothione and trypanothione disulfide in >200mg quantities using a mutant of Crithidia fasciculata trypanothione synthetase in which Cys59 has been replaced by an alanine residue. The reagent costs less than 1% of the commercial price of trypanothione disulfide. The protocol also allows the synthesis of related glutathione conjugates. It will greatly facilitate the thorough analysis of this parasite's metabolism and drug screening approaches against trypanothione-dependent enzymes.

Published

2009

10. Redox control in trypanosomatids, parasitic protozoa with trypanothione-based thiol metabolism.

Author

Krauth-Siegel RL and Comini MA

Subjects

Animals, DNA, Kinetoplast biosynthesis, Glutathione chemistry, Glutathione metabolism, Oxidation-Reduction, Spermidine chemistry, Spermidine metabolism, Glutathione analogs & derivatives, Parasites metabolism, Spermidine analogs & derivatives, Sulfhydryl Compounds metabolism, Trypanosoma metabolism

Abstract

Trypanosomes and leishmania, the causative agents of several tropical diseases, possess a unique redox metabolism which is based on trypanothione. The bis(glutathionyl)spermidine is the central thiol that delivers electrons for the synthesis of DNA precursors, the detoxification of hydroperoxides and other trypanothione-dependent pathways. Many of the reactions are mediated by tryparedoxin, a distant member of the thioredoxin protein family. Trypanothione is kept reduced by the parasite-specific flavoenzyme trypanothione reductase. Since glutathione reductases and thioredoxin reductases are missing, the reaction catalyzed by trypanothione reductase represents the only connection between the NADPH- and the thiol-based redox metabolisms. Thus, cellular thiol redox homeostasis is maintained by the biosynthesis and reduction of trypanothione. Nearly all proteins of the parasite-specific trypanothione metabolism have proved to be essential.

Published

2008

11. Cytotoxic interactions of methylene blue with trypanosomatid-specific disulfide reductases and their dithiol products.

Author

Buchholz K, Comini MA, Wissenbach D, Schirmer RH, Krauth-Siegel RL, and Gromer S

Subjects

Animals, Antioxidants metabolism, Catalysis, Dihydrolipoamide Dehydrogenase antagonists & inhibitors, Glutathione analogs & derivatives, Glutathione metabolism, NADH, NADPH Oxidoreductases antagonists & inhibitors, Oxidation-Reduction, Reactive Oxygen Species metabolism, Spermidine analogs & derivatives, Spermidine metabolism, Methylene Blue pharmacokinetics, Sulfhydryl Compounds metabolism, Trypanocidal Agents pharmacokinetics, Trypanosoma enzymology

Abstract

Methylene blue (MB) is known to have trypanocidal activity. We tested the interactions of MB with a number of trypanosomatid-specific molecules of the antioxidant metabolism. At pH 7, trypanothione and other (di)thiols were oxidized to disulfides by the phenothiazine drug. MB inhibited Trypanosoma cruzi trypanothione reductase (TR) (K(i)=1.9 microM), and served as a significant subversive substrate of this enzyme (K(M)=30 microM, k(cat)=4.9s(-1)). With lipoamide dehydrogenase, the second thiol-generating flavoenzyme of T. cruzi, the catalytic efficiency for MB reduction was found to be almost 10(6)M(-1)s(-1). When the system MB-enzyme-molecular oxygen acts as a NAD(P)H-driven redox cycler, a reactive oxygen species, H(2)O(2) or superoxide, is produced in each cycle. Since MB is an affordable, available, and accessible drug it might be tested--alone or in drug combinations--against trypanosomatid-caused diseases of animal and man.

Published

2008

12. The lineage-specific, intrinsically disordered N-terminal extension of monothiol glutaredoxin 1 from trypanosomes contains a regulatory region

Author

Moreno Lelli, Mattia Sturlese, Karin Grunberg, Barbara Zambelli, Marcelo A. Comini, Mariana Bonilla, Bruno Manta, Massimo Bellanda, Stefano Mammi, Andrea Bertarello, Sturlese M, Manta B, Bertarello A, Bonilla M, Lelli M, Zambelli B, Grunberg K, Mammi S, Comini MA, Bellanda M., Manta, Bruno. Universidad de la República (Uruguay). Facultad de Ciencias. Instituto de Química Biológica, Bonilla Chao, Mariana Magdalena. Instituto Pasteur (Montevideo), Grunberg, Karin. Instituto Pasteur (Montevideo), and Comini, Marcelo A. Instituto Pasteur (Montevideo)

Subjects

0301 basic medicine, Iron-Sulfur Proteins, Protein Conformation, INTRINSICALLY DISORDERED PROTEIN, Glutaredoxin, Plasma protein binding, Regulatory Sequences, Nucleic Acid, Protein structure, Intrinsically Disordered Regions, INTRINSICALLY DISORDERED PROTEIN, AFRICAN TRYPANOSOMES, MONOTHIOL GLUTAREDOXINS, NMR-SPECTROSCOPY, Catalytic Domain, Trypanosoma brucei, Protein Dimerization, Peptide sequence, AFRICAN TRYPANOSOMES, Multidisciplinary, biology, Chemistry, Molecular mass, glutaredoxin, trypanosomes, NMR, iron-sulfur, Ligand (biochemistry), Glutathione, Cell biology, NMR-SPECTROSCOPY, Grx C1, Medicine, 1CGrx1, Oxidation-Reduction, MONOTHIOL GLUTAREDOXINS, Trypanosoma, Trypanosoma Brucei Brucei, Science, Trypanosoma brucei brucei, Limited Proteolysis Assays, Residual Dipolar Couplings (RDCs), Intrinsically disordered proteins, Article, 03 medical and health sciences, Amino Acid Sequence, Glutaredoxins, Active site, Proteins, biology.organism_classification, NMR, 030104 developmental biology, intrinsically disordered proteins, Protein Multimerization, Sulfur, Multiangle Light Scattering (MALS)

Abstract

Glutaredoxins (Grx) are small proteins conserved throughout all the kingdoms of life that are engaged in a wide variety of biological processes and share a common thioredoxin-fold. Among them, class II Grx are redox-inactive proteins involved in iron-sulfur (FeS) metabolism. They contain a single thiol group in their active site and use low molecular mass thiols such as glutathione as ligand for binding FeS-clusters. In this study, we investigated molecular aspects of 1CGrx1 from the pathogenic parasite Trypanosoma brucei brucei, a mitochondrial class II Grx that fulfills an indispensable role in vivo. Mitochondrial 1CGrx1 from trypanosomes differs from orthologues in several features including the presence of a parasite-specific N-terminal extension (NTE) whose role has yet to be elucidated. Previously we have solved the structure of a truncated form of 1CGrx1 containing only the conserved glutaredoxin domain but lacking the NTE. Our aim here is to investigate the effect of the NTE on the conformation of the protein. We therefore solved the NMR structure of the full-length protein, which reveals subtle but significant differences with the structure of the NTE-less form. By means of different experimental approaches, the NTE proved to be intrinsically disordered and not involved in the non-redox dependent protein dimerization, as previously suggested. Interestingly, the portion comprising residues 65–76 of the NTE modulates the conformational dynamics of the glutathione-binding pocket, which may play a role in iron-sulfur cluster assembly and delivery. Furthermore, we disclosed that the class II-strictly conserved loop that precedes the active site is critical for stabilizing the protein structure. So far, this represents the first communication of a Grx containing an intrinsically disordered region that defines a new protein subgroup within class II Grx.

Published

2018