Search

Your search keyword '"Andrade-Pavón, Dulce"' showing total 28 results
Start Over Author "Andrade-Pavón, Dulce"
28 results on '"Andrade-Pavón, Dulce"'

6. Review and Current Perspectives on DNA Topoisomerase I and II Enzymes of Fungi as Study Models for the Development of New Antifungal Drugs.

Author

Andrade-Pavón, Dulce, Gómez-García, Omar, and Villa-Tanaca, Lourdes

Subjects
*DNA topoisomerase II, *FUNGAL enzymes, *BINDING sites, *DNA topoisomerases, *AMINO acid residues, *DNA topoisomerase I
Abstract

Fungal infections represent a growing public health problem, mainly stemming from two phenomena. Firstly, certain diseases (e.g., AIDS and COVID-19) have emerged that weaken the immune system, leaving patients susceptible to opportunistic pathogens. Secondly, an increasing number of pathogenic fungi are developing multi-drug resistance. Consequently, there is a need for new antifungal drugs with novel therapeutic targets, such as type I and II DNA topoisomerase enzymes of fungal organisms. This contribution summarizes the available information in the literature on the biology, topology, structural characteristics, and genes of topoisomerase (Topo) I and II enzymes in humans, two other mammals, and 29 fungi (including Basidiomycetes and Ascomycetes). The evidence of these enzymes as alternative targets for antifungal therapy is presented, as is a broad spectrum of Topo I and II inhibitors. Research has revealed the genes responsible for encoding the Topo I and II enzymes of fungal organisms and the amino acid residues and nucleotide residues at the active sites of the enzymes that are involved in the binding mode of topoisomerase inhibitors. Such residues are highly conserved. According to molecular docking studies, antifungal Topo I and II inhibitors have good affinity for the active site of the respective enzymes. The evidence presented in the current review supports the proposal of the suitability of Topo I and II enzymes as molecular targets for new antifungal drugs, which may be used in the future in combined therapies for the treatment of infections caused by fungal organisms. [ABSTRACT FROM AUTHOR]

Published
2024
Full Text
View/download PDF

7. Synthesis, In Silico Study, and In Vitro Antifungal Activity of New 5-(1,3-Diphenyl-1H-Pyrazol-4-yl)-4-Tosyl-4,5-Dihydrooxazoles

Author

Tlapale-Lara, Neively, primary, López, Julio, additional, Gómez, Elizabeth, additional, Villa-Tanaca, Lourdes, additional, Barrera, Edson, additional, Escalante, Carlos H., additional, Tamariz, Joaquín, additional, Delgado, Francisco, additional, Andrade-Pavón, Dulce, additional, and Gómez-García, Omar, additional

Published
2024
Full Text
View/download PDF

11. Synthesis, In Silico Study, and In Vitro Antifungal Activity of New 5-(1,3-Diphenyl-1 H -Pyrazol-4-yl)-4-Tosyl-4,5-Dihydrooxazoles.

Author

Tlapale-Lara, Neively, López, Julio, Gómez, Elizabeth, Villa-Tanaca, Lourdes, Barrera, Edson, Escalante, Carlos H., Tamariz, Joaquín, Delgado, Francisco, Andrade-Pavón, Dulce, and Gómez-García, Omar

Subjects
BINDING sites, ERGOSTEROL, MOLECULAR docking, ANTIFUNGAL agents, MYCOSES, IMMUNOCOMPROMISED patients, PROTEIN models
Abstract

The increase in multi-drug resistant Candida strains has caused a sharp rise in life-threatening fungal infections in immunosuppressed patients, including those with SARS-CoV-2. Novel antifungal drugs are needed to combat multi-drug-resistant yeasts. This study aimed to synthesize a new series of 2-oxazolines and evaluate the ligands in vitro for the inhibition of six Candida species and in silico for affinity to the CYP51 enzymes (obtained with molecular modeling and protein homology) of the same species. The 5-(1,3-diphenyl-1H-pyrazol-4-yl)-4-tosyl-4,5-dihydrooxazoles 6a-j were synthesized using the Van Leusen reaction between 1,3-diphenyl-4-formylpyrazoles 4a-j and TosMIC 5 in the presence of K2CO3 or KOH without heating, resulting in short reaction times, high compound purity, and high yields. The docking studies revealed good affinity for the active site of the CYP51 enzymes of the Candida species in the following order: 6a-j > 4a-j > fluconazole (the reference drug). The in vitro testing of the compounds against the Candida species showed lower MIC values for 6a-j than 4a-j, and for 4a-j than fluconazole, thus correlating well with the in silico findings. According to growth rescue assays, 6a-j and 4a-j (like fluconazole) inhibit ergosterol synthesis. The in silico toxicity assessment evidenced the safety of compounds 6a-j, which merit further research as possible antifungal drugs. [ABSTRACT FROM AUTHOR]

Published
2024
Full Text
View/download PDF

12. Synthesis and Molecular Docking Studies of Alkoxy- and Imidazole-Substituted Xanthones as α-Amylase and α-Glucosidase Inhibitors

Author

Aguila-Muñoz, Dolores G., primary, Vázquez-Lira, Gabriel, additional, Sarmiento-Tlale, Erika, additional, Cruz-López, María C., additional, Jiménez-Montejo, Fabiola E., additional, López y López, Víctor E., additional, Escalante, Carlos H., additional, Andrade-Pavón, Dulce, additional, Gómez-García, Omar, additional, Tamariz, Joaquín, additional, and Mendieta-Moctezuma, Aarón, additional

Published
2023
Full Text
View/download PDF

15. New Organotin (IV) Compounds Derived from Dehydroacetic Acid and Thiosemicarbazides: Synthesis, Rational Design, Cytotoxic Evaluation, and Molecular Docking Simulation.

Author

Gómez, Elizabeth, Galván-Hidalgo, José Miguel, Pérez-Cuéllar, Guillermo, Huerta-Landa, Karoline Alondra, González-Hernández, Arturo, Gómez-García, Omar, Andrade-Pavón, Dulce, Ramírez-Apan, Teresa, Rodríguez Hernández, Karla Daniela, Hernández, Simón, Cano-Sánchez, Patricia, and Gómez-Velasco, Homero

Subjects
THIOSEMICARBAZONES, MOLECULAR docking, ISOTHERMAL titration calorimetry, CERCOPITHECUS aethiops, CARBON-hydrogen bonds, NUCLEAR magnetic resonance, PYRAN
Abstract

Organotin complexes were prepared through a one-pot reaction with three components by reacting thiosemicarbazide or 4-methyl-3-thiosemicarbazide or 4-phenylthiosemicarbazide, dehydroacetic acid (DHA) and dibutyl, diphenyl, dicyclohexyl, and bis[(trimethylsilyl)methyl]tin(IV) oxides; all complexes were characterized by infrared (IR), ultraviolet-visible (UV-vis), mass spectrometry (MS), and nuclear magnetic resonance (NMR) spectroscopy. The 119Sn NMR revealed chemical shifts corresponding to a pentacoordinated environment in solution. The X-ray crystallography of the two complexes evidenced the formation of monomeric complexes with a pentacoordinated geometry around tin via three donor atoms from the ligand, the sulfur of the thiol, the nitrogen of the imine group, and the oxygen of the pyran ring. The geometries of the five-coordinated complexes 3a (Bu2SnL3), 3c (Ph2SnL3), and 3d (Cy2SnL3) acid were intermediate between square pyramidal and trigonal bipyramidal, and complex 1a (Bu2SnL1) adopted a bipyramidal trigonal geometry (BPT). The sulforhodamine B assay assessed the cytotoxicity of organotin(IV) complexes against the MDA-MB-231 and MCF-7 (human mammary adenocarcinoma) cell lines and one normal COS-7 (African green monkey kidney fibroblast). The IC50 values evidenced a significant antiproliferative effect on cancer cells; the complexes were more potent than the positive cisplatin control and the corresponding ligands, dehydroacetic acid thiosemicarbazone (L1), dehydroacetic acid-N(4)-methylthiosemicarbazone (L2), and dehydroacetic acid-N(4)-phenylthiosemicarbazone (L3). The IC50 values also indicated that the organotin(IV) complexes were more cytotoxic against the triple-negative breast cell line MDA-MB-231 than MCF-7, inducing significant morphological alterations. The interactions of organotin(IV) 1c (Ph2SnL1), 1d (Cy2SnL1), and 1e (((CH3)3SiCH2)2SnL1) were evaluated with ss-DNA by fluorescence; intensity changes of the fluorescence were indicative of the displacement of ethidium bromide (EB), confirming the interaction of the organotin(IV) complexes with ss-DNA; the results showed a DNA binding affinity. The thermodynamic parameters obtained through isothermal titration calorimetry showed that the interaction of 1c (Ph2SnL1), with ss-ADN, was exothermic. Molecular docking studies also demonstrated that the organotin(IV) complexes were intercalated in DNA by conventional hydrogen bonds, carbon-hydrogen bonds, and π-alkyl interactions. These complexes furthermore showed a greater affinity towards DNA than cisplatin. [ABSTRACT FROM AUTHOR]

Published
2023
Full Text
View/download PDF

16. Pyrrole-Based Enaminones as Building Blocks for the Synthesis of Indolizines and Pyrrolo[1,2- a ]pyrazines Showing Potent Antifungal Activity.

Author

Miranda-Sánchez, Diter, Escalante, Carlos H., Andrade-Pavón, Dulce, Gómez-García, Omar, Barrera, Edson, Villa-Tanaca, Lourdes, Delgado, Francisco, and Tamariz, Joaquín

Subjects
PYRAZINES, AMMONIUM acetate, LEWIS acids, PYRROLES, ACRYLATES, ACETOPHENONE, ACETATES
Abstract

As a new approach, pyrrolo[1,2-a]pyrazines were synthesized through the cyclization of 2-formylpyrrole-based enaminones in the presence of ammonium acetate. The enaminones were prepared with a straightforward method, reacting the corresponding alkyl 2-(2-formyl-1H-pyrrol-1-yl)acetates, 2-(2-formyl-1H-pyrrol-1-yl)acetonitrile, and 2-(2-formyl-1H-pyrrol-1-yl)acetophenones with DMFDMA. Analogous enaminones elaborated from alkyl (E)-3-(1H-pyrrol-2-yl)acrylates were treated with a Lewis acid to afford indolizines. The antifungal activity of the series of substituted pyrroles, pyrrole-based enaminones, pyrrolo[1,2-a]pyrazines, and indolizines was evaluated on six Candida spp., including two multidrug-resistant ones. Compared to the reference drugs, most test compounds produced a more robust antifungal effect. Docking analysis suggests that the inhibition of yeast growth was probably mediated by the interaction of the compounds with the catalytic site of HMGR of the Candida species. [ABSTRACT FROM AUTHOR]

Published
2023
Full Text
View/download PDF

17. Vacuolar proteases and autophagy in phytopathogenic fungi: A review

Author

Juárez-Montiel, Margarita, Clark-Flores, Daniel, Tesillo-Moreno, Pedro, de la Vega-Camarillo, Esaú, Andrade-Pavón, Dulce, Hernández-García, Juan Alfredo, Hernández-Rodríguez, César, and Villa-Tanaca, Lourdes

Subjects
General Medicine
Abstract

Autophagy (macroautophagy) is a survival and virulence mechanism of different eukaryotic pathogens. Autophagosomes sequester cytosolic material and organelles, then fuse with or enter into the vacuole or lysosome (the lytic compartment of most fungal/plant cells and many animal cells, respectively). Subsequent degradation of cargoes delivered to the vacuole via autophagy and endocytosis maintains cellular homeostasis and survival in conditions of stress, cellular differentiation, and development. PrA and PrB are vacuolar aspartyl and serine endoproteases, respectively, that participate in the autophagy of fungi and contribute to the pathogenicity of phytopathogens. Whereas the levels of vacuolar proteases are regulated by the expression of the genes encoding them (e.g., PEP4 for PrA and PRB1 for PrB), their activity is governed by endogenous inhibitors. The aim of the current contribution is to review the main characteristics, regulation, and role of vacuolar soluble endoproteases and Atg proteins in the process of autophagy and the pathogenesis of three fungal phytopathogens: Ustilago maydis, Magnaporthe oryzae, and Alternaria alternata. Aspartyl and serine proteases are known to participate in autophagy in these fungi by degrading autophagic bodies. However, the gene responsible for encoding the vacuolar serine protease of U. maydis has yet to be identified. Based on in silico analysis, this U. maydis gene is proposed to be orthologous to the Saccharomyces cerevisiae genes PRB1 and PBI2, known to encode the principal protease involved in the degradation of autophagic bodies and its inhibitor, respectively. In fungi that interact with plants, whether phytopathogenic or mycorrhizal, autophagy is a conserved cellular degradation process regulated through the TOR, PKA, and SNF1 pathways by ATG proteins and vacuolar proteases. Autophagy plays a preponderant role in the recycling of cell components as well as in the fungus-plant interaction.

Published
2022
Full Text
View/download PDF

18. Síntesis de (E)-1-(imidazo[1,2-a]piridin-3-il)-2-fenilprop-2-en-1-onas y Evaluación in Sílico e in Vitro de su Actividad Antifúngica.

Author

Gómez García, Jorge Omar, Andrade Pavón, Dulce María, Delgado, Francisco, Tlapale Lara, Neively, Moran Chamorro, Carlos David, Reyes Sánchez, Brian Raúl, and López Martínez, Julio César

Abstract

Copyright of Congreso Internacional de Investigación Academia Journals is the property of PDHTech, LLC and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published
2022

19. Three-Component Synthesis of 2-Amino-3-cyano-4H-chromenes, In Silico Analysis of Their Pharmacological Profile, and In Vitro Anticancer and Antifungal Testing

Author

Feliciano, Alberto, primary, Gómez-García, Omar, additional, Escalante, Carlos H., additional, Rodríguez-Hernández, Mario A., additional, Vargas-Fuentes, Mariana, additional, Andrade-Pavón, Dulce, additional, Villa-Tanaca, Lourdes, additional, Álvarez-Toledano, Cecilio, additional, Ramírez-Apan, María Teresa, additional, Vázquez, Miguel A., additional, Tamariz, Joaquín, additional, and Delgado, Francisco, additional

Published
2021
Full Text
View/download PDF

22. Inhibitors of DNA topoisomerases I and II applied to Candida dubliniensis reduce growth, viability, the generation of petite mutants and toxicity, while acting synergistically with fluconazole

Author

Tagle-Olmedo, Tania, primary, Andrade-Pavón, Dulce, additional, Martínez-Gamboa, Areli, additional, Gómez-García, Omar, additional, García-Sierra, Francisco, additional, Hernández-Rodríguez, César, additional, and Villa-Tanaca, Lourdes, additional

Published
2021
Full Text
View/download PDF

23. Evaluación del Efecto Antitumoral de los Flavonoides Naringina, Naringenina y Catequina en un Modelo de Cáncer de Colon en Ratones de la Cepa BALB/c.

Author

Gómez García, Jorge Omar and Andrade Pavón, Dulce María

Abstract

Copyright of Congreso Internacional de Investigación Academia Journals is the property of PDHTech, LLC and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published
2022

27. The 3-hydroxy-3-methylglutaryl coenzyme-A reductases from fungi: A proposal as a therapeutic target and as a study model

Author

Andrade Pavón, Dulce, Sánchez Sandoval, Eugenia, Rosales Acosta, Blanca, Ibarra, José Antonio, Tamariz, Joaquín, Hernández Rodríguez, César, Villa Tanaca, Lourdes, Andrade Pavón, Dulce, Sánchez Sandoval, Eugenia, Rosales Acosta, Blanca, Ibarra, José Antonio, Tamariz, Joaquín, Hernández Rodríguez, César, and Villa Tanaca, Lourdes

Abstract

The enzyme 3-hydroxy-3-methylglutaryl coenzyme-A reductase (HMGR) catalyzes the conversion of HMG-Co-Aintomevalonate.Thisstepisthelimitingpointfor thesynthesisofcholesterolinmammalsand ergosterolinfungi.Wedescribe inthis article the genome organizationofHMGRcoding genes andthose deduced from different fungi, recount the evidence showing statins as HMGR inhibitors for ergosterol synthesis and its effectin yeast viability, and propose fungal HMGR(HMGRf) as amodelto study the use ofpharmaceutical compounds to inhibit cholesterol andergosterol synthesis.Bibliographical searchand bioinformaticanalyseswereperformedanddiscussed.HMGRfsbelongtotheclass Iwithahighhomology in the catalytic region. The sterol biosynthetic pathway in humans and fungi sharemany enzymes in the initial steps (such as the HMGR enzyme), but in the last steps enzymes are different rendering the two ?nalproducts: cholesterolinmammals andergosterolinfungi.Withregards to inhibitors suchas statins and other compounds, these affect also fungal viability. Since HMGR from Schizosaccharomyces pombe and Ustilago maydis are very similar to thehuman HMGRinthe catalytic regions, we propose thatfungal enzymes can be used to testinhibitors for a potential use in humans.We consider that HMGRf is a good therapeutic targetto design and test new antifungal compounds

Published
2014

28. Three-Component Synthesis of 2-Amino-3-cyano-4 H -chromenes, In Silico Analysis of Their Pharmacological Profile, and In Vitro Anticancer and Antifungal Testing.

Author

Feliciano, Alberto, Gómez-García, Omar, Escalante, Carlos H., Rodríguez-Hernández, Mario A., Vargas-Fuentes, Mariana, Andrade-Pavón, Dulce, Villa-Tanaca, Lourdes, Álvarez-Toledano, Cecilio, Ramírez-Apan, María Teresa, Vázquez, Miguel A., Tamariz, Joaquín, and Delgado, Francisco

Subjects
ANTIFUNGAL agents, CANCER cell growth, MOLECULAR docking, ANTINEOPLASTIC agents, BINDING energy, CISPLATIN
Abstract

Chromenes are compounds that may be useful for inhibiting topoisomerase and cytochrome, enzymes involved in the growth of cancer and fungal cells, respectively. The aim of this study was to synthesize a series of some novel 2-amino-3-cyano-4-aryl-6,7-methylendioxy-4H-chromenes 4a–o and 2-amino-3-cyano-5,7-dimethoxy-4-aryl-4H-chromenes 6a–h by a three-component reaction, and test these derivatives for anticancer and antifungal activity. Compounds 4a and 4b were more active than cisplatin (9) and topotecan (7) in SK-LU-1 cells, and more active than 9 in PC-3 cells. An evaluation was also made of the series of compounds 4 and 6 as potential antifungal agents against six Candida strains, finding their MIC50 to be less than or equal to that of fluconazole (8). Molecular docking studies are herein reported, for the interaction of 4 and 6 with topoisomerase IB and the active site of CYP51 of Candida spp. Compounds 4a–o and 6a–h interacted in a similar way as 7 with key amino acids of the active site of topoisomerase IB and showed better binding energy than 8 at the active site of CYP51. Hence, 4a–o and 6a–h are good candidates for further research, having demonstrated their dual inhibition of enzymes that participate in the growth of cancer and fungal cells. [ABSTRACT FROM AUTHOR]

Published
2021
Full Text
View/download PDF

Catalog

Books, media, physical & digital resources
See catalog results