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2. Técnicas básicas en un laboratorio de química orgánica: recristalización

Author

José Luis Jiménez Blanco, David Monge Fernández, María de Gracia Retamosa Hernández, María Isabel García Moreno, Elena Díez Martín, Fernando Ortega Caballero, Juan Vázquez Cabello, Ana Teresa Carmona Asenjo, Antonio José Moreno Vargas, and Francisco Javier Iglesias Sigüenza

Abstract

La función de estos videos didácticos consiste en proporcionar el apoyo necesario para la adquisición de habilidades prácticas dentro del laboratorio de cara al desarrollo profesional del alumnado. La producción de los mismos está dirigida al estudiantado que cursa asignaturas del área de química orgánica en diferentes grados universitarios. Recristalización: es el método más adecuado para purificar compuestos sólidos, siempre y cuando contengan una cantidad moderada de impurezas. La técnica se basa en dos factores: la diferente solubilidad del compuesto en un determinado disolvente a temperatura ambiente y en caliente, así como la diferencia de solubilidad de la sustancia problema y de las impurezas que la acompañan. La visualización de material didáctico en forma de videos explicativos que incluye las técnicas/operaciones básicas empleadas en un laboratorio de Química Orgánica, contribuirá a una mejor comprensión/asimilación de las mismas, resultando de gran apoyo para la correcta realización de las diferentes prácticas de laboratorio.

Published
2021
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3. Técnicas básicas en un laboratorio de química orgánica: destilación simple

Author

Ana Teresa Carmona Asenjo, José Luis Jiménez Blanco, María de Gracia Retamosa Hernández, María Isabel García Moreno, Fernando Ortega Caballero, Elena Díez Martín, Francisco Javier Iglesias Sigüenza, David Monge Fernández, Juan Vázquez Cabello, and Antonio José Moreno Vargas

Abstract

La función de estos videos didácticos consiste en proporcionar el apoyo necesario para la adquisición de habilidades prácticas dentro del laboratorio de cara al desarrollo profesional del alumnado. La producción de los mismos está dirigida al estudiantado que cursa asignaturas del área de química orgánica en diferentes grados universitarios. Destilación simple: se emplea fundamentalmente en dos casos, separar un sólido de un líquido, y separar dos líquidos cuyos puntos de ebullición difieren en, al menos, 70 grados Centígrados. La visualización de material didáctico en forma de videos explicativos que incluye las técnicas/operaciones básicas empleadas en un laboratorio de Química Orgánica, contribuirá a una mejor comprensión/asimilación de las mismas, resultando de gran apoyo para la correcta realización de las diferentes prácticas de laboratorio.

Published
2021
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4. Técnicas básicas en un laboratorio de química orgánica: cromatografía en columna de gel de sílice

Author

Antonio José Moreno Vargas, Fernando Ortega Caballero, Ana Teresa Carmona Asenjo, David Monge Fernández, Francisco Javier Iglesias Sigüenza, María Isabel García Moreno, Elena Díez Martín, José Luis Jiménez Blanco, María de Gracia Retamosa Hernández, and Juan Vázquez Cabello

Abstract

La función de estos videos didácticos consiste en proporcionar el apoyo necesario para la adquisición de habilidades prácticas dentro del laboratorio de cara al desarrollo profesional del alumnado. La producción de los mismos está dirigida al estudiantado que cursa asignaturas del área de química orgánica en diferentes grados universitarios. Cromatografía en Columna de Gel de Sílice: es el método más general para la separación y purificación de compuestos orgánicos, sólidos o líquidos, a escala preparativa. La visualización de material didáctico en forma de videos explicativos que incluye las técnicas/operaciones básicas empleadas en un laboratorio de Química Orgánica, contribuirá a una mejor comprensión/asimilación de las mismas, resultando de gran apoyo para la correcta realización de las diferentes prácticas de laboratorio.

Published
2021
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5. Técnicas básicas en un laboratorio de química orgánica: cromatografía en capa fina

Author

Fernando Ortega Caballero, Antonio José Moreno Vargas, José Luis Jiménez Blanco, Ana Teresa Carmona Asenjo, María de Gracia Retamosa Hernández, David Monge Fernández, Francisco Javier Iglesias Sigüenza, Juan Vázquez Cabello, María Isabel García Moreno, and Elena Díez Martín

Abstract

La función de estos videos didácticos consiste en proporcionar el apoyo necesario para la adquisición de habilidades prácticas dentro del laboratorio de cara al desarrollo profesional del alumnado. La producción de los mismos está dirigida al estudiantado que cursa asignaturas del área de química orgánica en diferentes grados universitarios. Cromatografía en Capa Fina: permite determinar el grado de pureza de un compuesto, comparar muestras, realizar el seguimiento de una reacción, así como controlar el contenido de las fracciones obtenidas. La visualización de material didáctico en forma de videos explicativos que incluye las técnicas/operaciones básicas empleadas en un laboratorio de Química Orgánica, contribuirá a una mejor comprensión/asimilación de las mismas, resultando de gran apoyo para la correcta realización de las diferentes prácticas de laboratorio.

Published
2021
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6. Técnicas básicas en un laboratorio de química orgánica: separación por extracción

Author

José Luis Jiménez Blanco, David Monge Fernández, Antonio José Moreno Vargas, Ana Teresa Carmona Asenjo, Juan Vázquez Cabello, Francisco Javier Iglesias Sigüenza, María de Gracia Retamosa Hernández, María Isabel García Moreno, Elena Díez Martín, and Fernando Ortega Caballero

Abstract

La función de estos videos didácticos consiste en proporcionar el apoyo necesario para la adquisición de habilidades prácticas dentro del laboratorio de cara al desarrollo profesional del alumnado. La producción de los mismos está dirigida al estudiantado que cursa asignaturas del área de química orgánica en diferentes grados universitarios. Separación por Extracción: es la técnica empleada para separar un producto de una mezcla de reacción o para aislarlo de sus fuentes naturales. Una de las separaciones por extracción más empleadas es la extracción líquido-líquido, en la que un compuesto se extrae de una fase acuosa por medio de un disolvente inmiscible con el agua. Las distintas sustancias presentes se distribuyen entre las fases acuosa y orgánica de acuerdo con sus solubilidades relativas. La visualización de material didáctico en forma de videos explicativos que incluye las técnicas/operaciones básicas empleadas en un laboratorio de Química Orgánica, contribuirá a una mejor comprensión/asimilación de las mismas, resultando de gran apoyo para la correcta realización de las diferentes prácticas de laboratorio.

Published
2021
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7. Técnicas básicas en un laboratorio de química orgánica: calentamiento a reflujo. Síntesis de acetanilida

Author

María Isabel García Moreno, Elena Díez Martín, David Monge Fernández, Antonio José Moreno Vargas, María de Gracia Retamosa Hernández, Fernando Ortega Caballero, Ana Teresa Carmona Asenjo, Francisco Javier Iglesias Sigüenza, Juan Vázquez Cabello, and José Luis Jiménez Blanco

Abstract

La función de estos videos didácticos consiste en proporcionar el apoyo necesario para la adquisición de habilidades prácticas dentro del laboratorio de cara al desarrollo profesional del alumnado. La producción de los mismos está dirigida al estudiantado que cursa asignaturas del área de química orgánica en diferentes grados universitarios. Calentamiento a Reflujo: permite mantener la reacción a temperatura constante, por ejemplo en el punto de ebullición del disolvente, el tiempo que sea necesario y sin que se produzca una pérdida del mismo. La visualización de material didáctico en forma de videos explicativos que incluye las técnicas/operaciones básicas empleadas en un laboratorio de Química Orgánica, contribuirá a una mejor comprensión/asimilación de las mismas, resultando de gran apoyo para la correcta realización de las diferentes prácticas de laboratorio.

Published
2021
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8. Pharmacological Chaperones for the Treatment of α-Mannosidosis

Author

Katsumi Higaki, Carmen Ortiz Mellet, Fernando Ortega-Caballero, Reimi Matsumoto, José M. García Fernández, Rocío Rísquez-Cuadro, Eiji Nanba, Universidad de Sevilla. Departamento de Química orgánica, Ministerio de Economía y Competitividad (MINECO). España, Junta de Andalucía, and Japan Society for the Promotion of Science

Subjects
Mutant, Amino Acid Motifs, 01 natural sciences, Cell Line, 03 medical and health sciences, Glycomimetic, alpha-Mannosidase, Lysosome, Drug Discovery, medicine, Humans, Glycosides, Enhancer, 030304 developmental biology, chemistry.chemical_classification, 0303 health sciences, biology, Chemistry, Transfection, Fibroblasts, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, medicine.anatomical_structure, Enzyme, Biochemistry, Chaperone (protein), Drug Design, alpha-Mannosidosis, biology.protein, Molecular Medicine, Protein folding, Imino Pyranoses
Abstract

α-Mannosidosis (AM) results from deficient lysosomal α-mannosidase (LAMAN) activity and subsequent substrate accumulation in the lysosome, leading to severe pathology. Many of the AM-causative mutations compromise enzyme folding and could be rescued with purpose-designed pharmacological chaperones (PCs). We found that PCs combining a LAMAN glycone-binding motif based on the 5N,6O-oxomethylidenemannojirimycin (OMJ) glycomimetic core and different aglycones, in either mono- or multivalent displays, elicit binding modes involving glycone and nonglycone enzyme regions that reinforce the protein folding and stabilization potential. Multivalent derivatives exhibited potent enzyme inhibition that generally prevailed over the chaperone effect. On the contrary, monovalent OMJ derivatives with LAMAN aglycone binding area-fitting substituents proved effective as activity enhancers for several mutant LAMAN forms in AM patient fibroblasts and/or transfected MAN2B1-KO cells. This translated into a significant improvement in endosomal/lysosomal function, reverting not only the primary LAMAN substrate accumulation but also the additional downstream consequences such as cholesterol accumulation. Ministerio de Economía y Competitividad SAF2016-76083-R, CTQ2015-64425-C2-1-R Junta de Andalucía FQM2012-1467 Japan Society for the Promotion of Science 17K10051

Published
2019

9. (Pseudo)amide-linked oligosaccharide mimetics: molecular recognition and supramolecular properties

Author

José L. Jiménez Blanco, Fernando Ortega-Caballero, Carmen Ortiz Mellet, and José M. García Fernández

Subjects
carbopeptoids, glycoclusters, glycomimetics, pseudooligosaccharides, spaced sugars, Science, Organic chemistry, QD241-441
Abstract

Oligosaccharides are currently recognised as having functions that influence the entire spectrum of cell activities. However, a distinct disadvantage of naturally occurring oligosaccharides is their metabolic instability in biological systems. Therefore, much effort has been spent in the past two decades on the development of feasible routes to carbohydrate mimetics which can compete with their O-glycosidic counterparts in cell surface adhesion, inhibit carbohydrate processing enzymes, and interfere in the biosynthesis of specific cell surface carbohydrates. Such oligosaccharide mimetics are potential therapeutic agents against HIV and other infections, against cancer, diabetes and other metabolic diseases. An efficient strategy to access this type of compounds is the replacement of the glycosidic linkage by amide or pseudoamide functions such as thiourea, urea and guanidine. In this review we summarise the advances over the last decade in the synthesis of oligosaccharide mimetics that possess amide and pseudoamide linkages, as well as studies focussing on their supramolecular and recognition properties.

Published
2010
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11. Screening sp-iminosugar N-glycosides as pharmacological chaperone candidates for α mannosidosis: The effect of aglycone nature and valency

Author

Eiji Nanba, Rocío Rísquez-Cuadro, Katsumi Higaki, Fernando Ortega-Caballero, José M. García Fernández, and Carmen Ortiz Mellet

Subjects
chemistry.chemical_classification, Chemistry, Stereochemistry, Endocrinology, Diabetes and Metabolism, α mannosidosis, Iminosugar, Valency, Glycoside, Biochemistry, Pharmacological chaperone, chemistry.chemical_compound, Endocrinology, Aglycone, Genetics, medicine, Molecular Biology, medicine.drug
Published
2019
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13. Trehalose-based Janus cyclooligosaccharides: the ‘‘Click’’ synthesis and DNA-directed assembly into pH-sensitive transfectious nanoparticles

Author

Laura Blanco-Fernandez, J. M. Garcia Fernandez, Emilio Aicart, Francisco Mendicuti, C. Tros de Ilarduya, María Martínez-Negro, Fernando Ortega-Caballero, Thais Carmona, Gema Marcelo, José L. Jiménez Blanco, Elena Junquera, C. Ortiz Mellet, CSIC - Unidad de Recursos de Información Científica para la Investigación (URICI), Ministerio de Economía y Competitividad (España), Junta de Andalucía, European Commission, Universidad Complutense de Madrid, Nafarroako Gobernua, Fundación Universitaria de Navarra, Universidad de Sevilla. Departamento de Química orgánica, Ministerio de Economia, Industria y Competitividad (MINECO). España, Gobierno de Navarra, Fundación Universidad de Navarra (FUN). España, European Commission (EC). Fondo Europeo de Desarrollo Regional (FEDER), and European Commission. Fondo Social Europeo (FSO)

Subjects
Stereochemistry, Oligosaccharides, Nanoparticle, 010402 general chemistry, 01 natural sciences, Catalysis, chemistry.chemical_compound, X-Ray Diffraction, Chlorocebus aethiops, Scattering, Small Angle, Materials Chemistry, Animals, Lamellar structure, Janus, 010405 organic chemistry, Small-angle X-ray scattering, Metals and Alloys, Cationic polymerization, Trehalose, DNA, General Chemistry, Transfection, Hydrogen-Ion Concentration, Combinatorial chemistry, 0104 chemical sciences, Surfaces, Coatings and Films, Electronic, Optical and Magnetic Materials, chemistry, COS Cells, Ceramics and Composites, Nanoparticles, Click Chemistry
Abstract

This article is licensed under a Creative Commons Attribution 3.0 Unported Licence.-- et al., The convergent preparation of Janus molecular nanoparticles by thiourea-‘‘clicking’’ of a,a0 -trehalose halves has been implemented; the strategy allows access to macrocyclic derivatives with seggregated cationic and lipophilic domains that in the presence of DNA undergo pH-dependent self-assembly into lamellar superstructures, as established by electrochemical, structural (SAXS), microscopical (TEM) and computational techniques, that mediate transfection in vitro and in vivo., We acknowledge support by the CSIC Open Access Publication Initiative through its Unit of Information Resources for Research (URICI)., The authors thank MINECO (contract numbers CTQ2012- 30821, SAF2013-44021-R, CTQ2015-64425-C2-1-R and CTQ2015-64425-C2-2-R), the Junta de Andalucía (contract number FQM2012-1467), University Complutense of Madrid (project no. UCMA05-33-010), the Government of Navarra (Department of Innovation and Industry, contract number IIQ14334.RI1), the University of Navarra Foundation (FUN), and the European Regional Development Funds (FEDER and FSE) for financial support.

Published
2016

14. Supramolecular Chemistry of Carbohydrate Clusters with Cores having Guest Binding Abilities

Author

Antonio Vargas-Berenguel, Juan M. Casas-Solvas, and Fernando Ortega-Caballero

Subjects
chemistry.chemical_classification, Molecular recognition, Cyclodextrin, Chemistry, Organic Chemistry, Drug delivery, Supramolecular chemistry, Carbohydrate, Combinatorial chemistry
Abstract

This review concentrates on both the protein receptor and guest binding abilities of carbohydrate clusters based on a cyclodextrin core. The combination of both complexation abilities is the basis of one of the pursued approaches for developing site-specific drug delivery systems. Influence on the molecular recognition properties of the number of appended saccharides, the type of carbohydrate clustering and the type of the spacer arms, among other factors, are discussed.

Published
2007
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15. Synthesis of Nitrogen-Functionalized β-Cycloaltrins

Author

Juan M. Casas-Solvas, Juan J. Giménez-Martínez, Fernando Ortega-Caballero, and Antonio Vargas-Berenguel

Subjects
Nitrogen, Chemistry, beta-Cyclodextrins, Organic Chemistry, chemistry.chemical_element, Stereoisomerism, Epoxy, chemistry.chemical_compound, Nucleophile, visual_art, visual_art.visual_art_medium, Epoxy Compounds, Organic chemistry, Surface modification, Organic synthesis, Azide
Abstract

We report the synthesis of functionalized beta-cycloaltrins having azido groups at C-3, C-6, and both C-3 and C-6 by nucleophilic epoxy ring-opening of per-2,3-anhidro-beta-cyclomannin derivatives. The value of these compounds as templates for further functionalization is exemplified by the conversion of heptakis(3,6-diazido-3,6-dideoxy)-beta-cycloaltrin into the per-3,6-diamino, per-3,6-diacetamido, per-3,6-dichloroacetamido, and per[3,6-bis(N'-ethylureido)] derivatives in good yields.

Published
2004
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16. Diverse Motifs of Mannoside Clustering on a β-Cyclodextrin Core

Author

Fernando Ortega-Caballero, Juan J. Giménez-Martínez, and Antonio Vargas-Berenguel

Subjects
chemistry.chemical_classification, Cyclodextrins, Mannosides, Cyclodextrin, Chemistry, Stereochemistry, Molecular Sequence Data, beta-Cyclodextrins, Organic Chemistry, Sonogashira coupling, General Medicine, Combinatorial chemistry, Biochemistry, Carbohydrate Sequence, Carbohydrate Conformation, Cluster (physics), Physical and Theoretical Chemistry, Cluster analysis
Abstract

[reaction: see text] A new method for the synthesis of beta-cyclodextrin-based cluster mannosides by application of the Sonogashira cross-coupling reaction is described. The method allows for the persubstitution of the beta-cyclodextrin at either 2- and 3-positions to give two types of heptavalent clusters, at both 2- and 6-positions to give clusters with 14 mannopyranoside units and at 2-, 3-, and 6-positions to obtain clusters with 21 mannopyranoside ligands.

Published
2003
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17. Dendritic Galactosides Based on aβ-Cyclodextrin Core for the Construction of Site-Specific Molecular Delivery Systems: Synthesis and Molecular Recognition Studies

Author

Francisco Santoyo-Gonzalez, Juan J. García-López, Antonio Vargas-Berenguel, Emilia Ortiz-Salmerón, Juan J. Giménez-Martínez, Luis García-Fuentes, and Fernando Ortega-Caballero

Subjects
Steric effects, chemistry.chemical_classification, Aqueous solution, Cyclodextrin, Stereochemistry, Organic Chemistry, General Chemistry, Binding constant, Catalysis, chemistry.chemical_compound, Monomer, Molecular recognition, chemistry, Galactosides, Dendrimer
Abstract

In order to evaluate the abil- ity of multivalent glycosides based on a -cyclodextrin core as site-specific mo- lecular carriers, a study on both the inclusion complexation behaviour and lectin binding affinity of branched and hyperbranched -cyclodextrins is pre- sented. A series of cluster galactosides constructed on -cyclodextrin scaffolds containing seven 1-thio--lactose or - lactosylamine bound to the macrocyclic core through different spacer arms were synthesised. In addition, the first syn- thesis of three first-order dendrimers based on a -cyclodextrin core contain- ing fourteen 1-thio---galactose, 1-thio--lactose and 1-thio--melibiose residues was performed. Calorimetric titrations performed at 25C in buffered aqueous solution (pH 7.4) gave the af- finity constants and the thermodynamic parameters for the complex formation of these -cyclodextrin derivatives with guests sodium 8-anilino-1-naphthalene- sulfonate (ANS) and 2-naphthalenesul- fonate, and lectin from peanut (Arachis hypogaea) (PNA). The persubstitution of the primary face of the -cyclodextrin with saccharides led to a slight increase of the binding constant values for the inclusion complexation with ANS rela- tive to the native -cyclodextrin. How- ever, the increase of the steric conges- tion due to the presence of the saccha- ride residues on the narrow rim of the - cyclodextrin may cause a decrease of the binding ability as shown for sodium 2-naphthalenesulfonate. The spacer arms are not passive elements and influence the host binding ability ac- cording to their chemical nature. PNA forms soluble cross-linked complexes with cluster galactosides and lactosides scaffolded on -cyclodextrin but not with cluster galactopyranosylamines or melibiose. Both, perbranched and hy- perbranched -cyclodextrins, form stronger complexes with PNA than the monomeric analogues. However, the use of hyperbranched CDs does not contrib- ute to the improvement of the complex stability relative to heptakis-glycocyclo- dextrin derivatives. Finally, a titration experiment with PNA and a complex formed by a heptakis lactose -cyclo- dextrin derivative with sodium 2-naph- thalenesulfonate showed the formation of a soluble cross-linked complex with stronger affinity constant and higher stoichiometry than those observed for the complex formation of PNA with the same heptakis-lactose -cyclodextrin derivative, suggesting the formation of a three component complex.

Published
2002
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18. Recent developments on synthetic tools towards structural and functional glycodiversity

Author

Fernando Ortega-Caballero and Juan M. Benito

Subjects
Pharmacology, Glycobiology, Computer science, media_common.quotation_subject, Research, Organic Chemistry, Chemical biology, Carbohydrates, Computational biology, Biochemistry, Living systems, Functional diversity, Drug Discovery, Molecular Medicine, Animals, Humans, Function (engineering), Glycoconjugates, Glycomics, media_common, Glycoproteins
Abstract

Despite being the most abundant type of biopolymers in Nature, the biological relevance of carbohydrates has systematically been underrated for decades, associating them far less sophisticated functions (structural or energy sourcing) than those unraveled for polynucleotides and proteins. The inherently large and complex diversity of carbohydrates and glycoconjugates, together with the lack of efficient technologies to either isolate them from natural sources or produce them synthetically in useful amounts, have burdened the appreciation of their utmost importance in the most fundamental biological processes. For these reasons, carbohydrate-mediated transmission of biological information was largely unexplored. However, over the decades, it became clear that the expression of complex carbohydrates is critical in the development of living systems. Nature uses this diverse repertoire of structures as codes in fundamental biological processes such as cellular differentiation, cellular signaling, fertilization or immune response, among many others. The urgency to elucidate the glycan code in terms of structure-function relationships has fuelled chemical biology approaches uncovering new frontiers in molecular biology, for which the term glycobiology had to be coined in the early 1980s'. Novel strategies for assembling oligosaccharides, glycoproteins, glycolipids and a range of glycoconjugates have flourished ever since providing access to glycomaterials for interrogating and interfering glycan function. This account focuses on the major breakthroughs made on the strategies during the last decades to synthetically reproduce the overwhelming glycodiversity, emphasizing on the dazzling array of concepts and techniques which development was required to cope with the task. In the first place, a succinct overview of the structural and functional diversity of biologically relevant saccharides and glycoconjugates will be given. Then, a selection of the most relevant strategies that composes the complex and diversity-oriented toolbox that modern carbohydrate synthesis consists on will be dissected. Finally, a selection of the most recent applications of this synthetic toolbox to chemical biology will be captured.

Published
2013

19. Symmetry complementarity-guided design of anthrax toxin inhibitors based on β-cyclodextrin: Synthesis and relative activities of face-selective functionalized polycationic clusters

Author

Adiamseged Yohannes, Vladimir A. Karginov, Alejandro Díaz-Moscoso, José M. García Fernández, Jacques Defaye, Juan M. Benito, Alejandro Méndez-Ardoy, Fernando Ortega-Caballero, Carmen Ortiz Mellet, and Tanisha M. Robinson

Subjects
Models, Molecular, Stereochemistry, Anthrax toxin, Chemistry, Pharmaceutical, Bacterial Toxins, Biochemistry, Cell Line, Cell membrane, Anthrax, Mice, Structure-Activity Relationship, Drug Discovery, medicine, Polyamines, Animals, Cluster Analysis, General Pharmacology, Toxicology and Pharmaceutics, Pharmacology, chemistry.chemical_classification, Cyclodextrins, Antigens, Bacterial, Cyclodextrin, Click chemistry, Organic Chemistry, beta-Cyclodextrins, Cationic polymerization, Polyelectrolytes, Symmetry complementary, Toxin inhibitors, Cytosol, medicine.anatomical_structure, chemistry, Protective antigen, Bacillus anthracis, Molecular Medicine, Computer-Aided Design, Amine gas treating
Abstract

12 páginas, 3 figuras, 1 tabla, 4 esquemas., Three new series of potential anthrax toxin inhibitors based on the β-cyclodextrin (βCD) scaffold were developed by exploiting face-selective CuI-catalyzed azide–alkyne 1,3-cycloadditions, amine–isothiocyanate coupling, and allyl group hydroboration–oxidation/hydroxy → amine replacement reactions. The molecular design follows the “symmetry–complementarity” concept between homogeneously functionalized polycationic βCD derivatives and protective antigen (PA), a component of anthrax toxin known to form C7-symmetric pores on the cell membrane used by lethal and edema factors to gain access to the cytosol. The synthesis and antitoxin activity of a collection of βCD derivatives differing in the number, arrangement, and face location of the cationic elements are reported herein. These results set the basis for a structure–activity relationship development program of new candidates to combat the anthrax threat., This work was supported by grant number 2R44AI052894-02 from the National Institute of Allergy and Infectious Diseases (USA), grants CTQ2007-61180/PPQ and CTQ2010-15848/BQU from the Spanish Ministry of Science and Education, the European Union (FEDER), and the Junta de Andalucía. A.D.-M. and A.M.-A. are grateful to the CSIC and the Spanish Ministry of Science and Education, respectively, for pre-doctoral fellowships.

Published
2010

20. ChemInform Abstract: (Pseudo)amide-Linked Oligosaccharide Mimetics: Molecular Recognition and Supramolecular Properties

Author

José M. García Fernández, Fernando Ortega-Caballero, Carmen Ortiz Mellet, and José L. Jiménez Blanco

Subjects
chemistry.chemical_classification, chemistry.chemical_compound, Molecular recognition, chemistry, Biochemistry, Biosynthesis, Amide, Supramolecular chemistry, Glycosidic bond, General Medicine, Oligosaccharide, Carbohydrate, Guanidine
Abstract

Oligosaccharides are currently recognised as having functions that influence the entire spectrum of cell activities. However, a distinct disadvantage of naturally occurring oligosaccharides is their metabolic instability in biological systems. Therefore, much effort has been spent in the past two decades on the development of feasible routes to carbohydrate mimetics which can compete with their O-glycosidic counterparts in cell surface adhesion, inhibit carbohydrate processing enzymes, and interfere in the biosynthesis of specific cell surface carbohydrates. Such oligosaccharide mimetics are potential therapeutic agents against HIV and other infections, against cancer, diabetes and other metabolic diseases. An efficient strategy to access this type of compounds is the replacement of the glycosidic linkage by amide or pseudoamide functions such as thiourea, urea and guanidine. In this review we summarise the advances over the last decade in the synthesis of oligosaccharide mimetics that possess amide and pseudoamide linkages, as well as studies focussing on their supramolecular and recognition properties.

Published
2010
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21. (Pseudo)amide-linked oligosaccharide mimetics: molecular recognition and supramolecular properties

Author

Fernando Ortega-Caballero, José L. Jiménez Blanco, Carmen Ortiz Mellet, José M. García Fernández, Universidad de Sevilla. Departamento de Química orgánica, and Ministerio de Ciencia e Innovación (MICIN). España

Subjects
Supramolecular chemistry, Glycoclusters, Review, glycoclusters, lcsh:QD241-441, chemistry.chemical_compound, Molecular recognition, Biosynthesis, lcsh:Organic chemistry, Amide, Guanidine, lcsh:Science, Pseudooligosaccharides, chemistry.chemical_classification, Organic Chemistry, Glycosidic bond, spaced sugars, Oligosaccharide, Carbohydrate, Combinatorial chemistry, Spaced sugars, Chemistry, Carbopeptoids, chemistry, Biochemistry, carbopeptoids, Glycomimetics, glycomimetics, pseudooligosaccharides, lcsh:Q
Abstract

18 páginas, 26 figuras, 5 esquemas, Oligosaccharides are currently recognised as having functions that influence the entire spectrum of cell activities. However, a distinct disadvantage of naturally occurring oligosaccharides is their metabolic instability in biological systems. Therefore, much effort has been spent in the past two decades on the development of feasible routes to carbohydrate mimetics which can compete with their O-glycosidic counterparts in cell surface adhesion, inhibit carbohydrate processing enzymes, and interfere in the biosynthesis of specific cell surface carbohydrates. Such oligosaccharide mimetics are potential therapeutic agents against HIV and other infections, against cancer, diabetes and other metabolic diseases. An efficient strategy to access this type of compounds is the replacement of the glycosidic linkage by amide or pseudoamide functions such as thiourea, urea and guanidine. In this review we summarise the advances over the last decade in the synthesis of oligosaccharide mimetics that possess amide and pseudoamide linkages, as well as studies focussing on their supramolecular and recognition properties., We thank the Spanish Ministerio de Ciencia e Innovación (MCINN, contract numbers CTQ2007-6118/PPQ and CTQ2009-14551-C02-01) and the Junta de Andalucía for the financial support.

Published
2010

22. Polycationic amphiphilic cyclodextrins for gene delivery: synthesis and effect of structural modifications on plasmid DNA complex stability, cytotoxicity, and gene expression

Author

Pierre Vierling, Carmen Ortiz Mellet, Patricia Balbuena, José M. García Fernández, Nicolas Guilloteau, Jacques Defaye, Fernando Ortega-Caballero, Christophe Di Giorgio, Juan M. Benito, Loïc Le Gourriérec, Marta Gómez-García, and Alejandro Díaz-Moscoso

Subjects
Stereochemistry, Polymers, Gene Expression, Gene delivery, Transfection, Catalysis, Cell Line, chemistry.chemical_compound, Gene expression, Amphiphile, Animals, Cytotoxicity, Gel electrophoresis, Cyclodextrins, Chemistry, Organic Chemistry, Cationic polymerization, Amphiphiles, Self-assembly, General Chemistry, DNA, Biophysics, Nanoparticles, Plasmids
Abstract

18 páginas, 11 figuras, 4 esquemas, A molecular-diversity-oriented approach for the preparation of well-defined polycationic amphiphilic cyclodextrins (paCDs) as gene-delivery systems is reported. The synthetic strategy takes advantage of the differential reactivity of primary versus secondary hydroxyl groups on the CD torus to regioselectively decorate each rim with cationic elements and lipophilic tails, respectively. Both the charge density and the hydrophobic–hydrophilic balance can be finely tuned in a highly symmetrical architecture that is reminiscent of both cationic lipids and cationic polymers, the two most prominent types of nonviral gene vectors. The monodisperse nature of paCDs and the modularity of the synthetic scheme are particularly well suited for structure–activity relationship studies. Gel electrophoresis revealed that paCDs self-assemble in the presence of plasmid DNA (pDNA) to provide homogeneous, stable nanoparticles (CDplexes) of 70–150 nm that fully protect pDNA from the environment. The transfection efficiency of the resulting CDplexes has been investigated in vitro on BNL-CL2 and COS-7 cell lines in the absence and presence of serum and found to be intimately dependent on architectural features. Facial amphiphilicity and the presence of a cluster of cationic and hydrogen-bonding centers for cooperative and reversible complexation of the polyanionic DNA chain is crucial to attain high transgene expression levels with very low toxicity profiles. Further enhancement of gene expression, eventually overcoming that of polyplexes from commercial polyethyleneimine (PEI) polymers (22 kDa), is achieved by building up space-oriented dendritic polycationic constructs., This work was supported by the Spanish Ministerio de Innovación y Ciencia (MICINN; contract numbers CTQ2006-15515-C02-01/BQU and CTQ2007-61180/PPQ), the Junta de Andalucía (P06-FQM-01601), the CSIC, the CNRS, and FUSINT (CNR project). A.D.M. and P.B.O. are grateful for predoctoral fellowships (CSIC and MICINN, respectively).

Published
2009

23. ChemInform Abstract: Supramolecular Chemistry of Carbohydrate Clusters with Cores Having Guest Binding Abilities

Author

Antonio Vargas-Berenguel, Fernando Ortega-Caballero, and Juan M. Casas-Solvas

Subjects
chemistry.chemical_classification, Molecular recognition, Cyclodextrin, chemistry, Drug delivery, Supramolecular chemistry, General Medicine, Carbohydrate, Combinatorial chemistry
Abstract

This review concentrates on both the protein receptor and guest binding abilities of carbohydrate clusters based on a cyclodextrin core. The combination of both complexation abilities is the basis of one of the pursued approaches for developing site-specific drug delivery systems. Influence on the molecular recognition properties of the number of appended saccharides, the type of carbohydrate clustering and the type of the spacer arms, among other factors, are discussed.

Published
2008
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24. ChemInform Abstract: High Dopamine Transporter Selectivity Can Be Displayed by Remarkably Simple Non-Nitrogen Containing Inhibitors

Author

Fernando Ortega-Caballero, Ove Wiborg, Henrik H. Jensen, Steffen Sinning, Søren V. Boye, and Mikael Bols

Subjects
chemistry.chemical_classification, chemistry, biology, Stereochemistry, Carboxylic acid, biology.protein, chemistry.chemical_element, General Medicine, Highly selective, Selectivity, Nitrogen, Dopamine transporter
Abstract

A series of 2-(3,4-dichlorophenyl)-cyclopent-1-enyl carboxylic acid esters and amides were prepared and tested for binding to the DAT, SERT, and NET. The achiral compounds were easily attained and found to inhibit DAT binding with K(i)-values ranging from 0.095 to 0.00003 mM. Among the compounds tested 2-(3,4-dichlorophenyl)-cyclopent-1-enyl carboxylic acid 2-methylphenyl ester was found to be highly selective with SERT/DAT>7000; NET/DAT>1700, K(i)=60 nM.

Published
2008
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25. Tailoring β-Cyclodextrin for DNA Complexation and Delivery by Homogeneous Functionalization at the Secondary Face

Author

Carmen Ortiz Mellet, José Manuel Garcia Fernandez, Jacques Defaye, Christophe Di Giorgio, Fernando Ortega-Caballero, Loïc Le Gourriérec, Pierre Vierling, Nicolas Guilloteau, Instituto de Investigaciones Químicas, Departamento de Química Orgánica, Facultad de Química, Laboratoire de Chimie des Molécules Bioactives et des Arômes (LCMBA), Université Nice Sophia Antipolis (... - 2019) (UNS), COMUE Université Côte d'Azur (2015-2019) (COMUE UCA)-COMUE Université Côte d'Azur (2015-2019) (COMUE UCA)-Centre National de la Recherche Scientifique (CNRS)-Université Côte d'Azur (UCA)-Institut de Chimie du CNRS (INC), Département de pharmacochimie moléculaire (DPM), and Institut de Chimie du CNRS (INC)-Centre National de la Recherche Scientifique (CNRS)-Université Joseph Fourier - Grenoble 1 (UJF)

Subjects
Beta-Cyclodextrins, Cell Survival, Betadex, Transfection, Biochemistry, Cell Line, chemistry.chemical_compound, Mice, Organic chemistry, Animals, Physical and Theoretical Chemistry, ComputingMilieux_MISCELLANEOUS, chemistry.chemical_classification, Cyclodextrin, Organic Chemistry, beta-Cyclodextrins, DNA, [SDV.SP]Life Sciences [q-bio]/Pharmaceutical sciences, Combinatorial chemistry, chemistry, Homogeneous, Surface modification, Cell line, Macromolecule
Abstract

4 páginas, 2 figuras, 3 esquemas, An efficient general strategy for the incorporation of functional elements onto the secondary hydroxyl rim of beta-cyclodextrin has been developed and applied to the synthesis of a novel series of C7-symmetric homogeneous macromolecular polycations with improved DNA complexing and delivery properties., This work was supported by the Spanish MEC (contract numbers CTQ2006-15515-C02-01/BQU and CTQ2007-61180/PPQ), the Junta de Andaluca (P06-FQM-01601), the CSIC, and the CNRS.

Published
2008

26. Synthesis and Biological Evaluation of Glycosidase Inhibitors: gem-Difluoromethylenated Nojirimycin Analogues

Author

Fernando Ortega-Caballero, Xiao-Long Qiu, Ruowen Wang, Feng-Ling Qing, and Mikael Bols

Subjects
chemistry.chemical_classification, Glucosamine, 1-Deoxynojirimycin, Glycoside Hydrolases, biology, Stereochemistry, Iminosugar, Biological activity, Hydrogen-Ion Concentration, Chemical synthesis, Nojirimycin, Structure-Activity Relationship, Enzyme, chemistry, Enzyme inhibitor, Drug Discovery, biology.protein, Molecular Medicine, Glycoside hydrolase, Amine gas treating, Imino Pyranoses
Abstract

In our ongoing program aimed at the design, synthesis, and biological evaluation of novel gem-difluoromethylenated glycosidase inhibitors, gem-4,4-difluoromethylenated iminosugars (5-9) were synthesized. The biological evaluation of these synthetic iminosugars showed that the gem-difluoromethylenyl group generally reduced the inhibition of glycosidases. However, this was not the case at pH 5.0, where the gem-difluoromethylenated iminosugar 6 was a stronger inhibitor than comparable iminosugars 1 and 36, suggesting that the influence of this group is mainly through its effect on the amine. It is proposed that the unprotonated iminosugar is the species preferably bound by beta-glucosidase, due to the lower pK(a) value of iminosugar 6 than of 1 or 36, leaving iminosugars 1 and 36 mostly protonated at pH 5.0, while iminosugar 6 is not. Iminosugar 6 also displayed good and selective inhibition of beta-glucosidase at pH 6.8.

Published
2006

27. Four orders of magnitude rate increase in artificial enzyme-catalyzed aryl glycoside hydrolysis

Author

Line Skall Laustsen, Fernando Ortega-Caballero, Mikael Bols, and Jeannette Bjerre

Subjects
chemistry.chemical_classification, Cyclodextrins, biology, Artificial enzyme, Aryl, Hydrolysis, Organic Chemistry, Molecular Conformation, Glycoside, Hydrogen-Ion Concentration, Aldehyde, Catalysis, chemistry.chemical_compound, chemistry, biology.protein, Phenol, Organic chemistry, Glycosides, Cyanohydrin
Abstract

[reaction: see text] (6AR,6DR)-6A,6D-Di-C-cyano-beta-cyclodextrin (1) and 6A,6D-di-C-cyano-alpha-cyclodextrin (2) were synthesized and shown to catalyze hydrolysis of aryl glycosides into glucose and phenol with a reaction following Michaelis-Menten kinetics. At pH 8.0 and 59 degrees C hydrolysis of 4-nitrophenyl alpha-glucopyranoside was catalyzed by 1 with KM = 10.5 +/- 1.5 mM, kcat = 1.42(+/-0.09) x 10(-4) s(-1), and kcat/kuncat = 7922. Catalysis was observed with a concentration of 1 as low as 10 microM. Hydrolysis of the other aryl glycosides containing stereochemical variation in the sugar-moiety and 4-nitro-, 2-nitro-, 2-aldehydo-, and 2,4-dinitro- were also catalyzed by 1 and 2 with kcat/kuncat ranging from 4 to 7100. Hydrolysis of a phenyl beta-d-glucoside or the thioglycoside tolylthio beta-D-glucoside was also catalyzed. From a series of prepared analogues of 1 it was found that the catalysis was associated with the hydroxyl groups alpha to the nitril groups. The monocyanohydrin 6-C-cyano-beta-cyclodextrin (3) was also found to catalyze the hydrolysis of 4-nitrophenyl beta-glucopyranoside with kcat/kuncat = 1356. It was proposed that the cyclodextrin cyanohydrins 1-3 catalyze the hydrolysis by general acid catalysis on the bound substrate.

Published
2005

28. Remarkable Supramolecular Catalysis of Glycoside Hydrolysis by a Cyclodextrin Cyanohydrin

Author

Fernando Ortega-Caballero, Torben E. Petersen, Brian Christensen, Mikaal Bols, and Cyril Rousseau

Subjects
chemistry.chemical_classification, Cyclodextrins, Cyclodextrin, Glycoside Hydrolases, Hydrolysis, Glycoside, Substrate (chemistry), General Chemistry, Biochemistry, Medicinal chemistry, Catalysis, chemistry.chemical_compound, Acid catalysis, Kinetics, Colloid and Surface Chemistry, chemistry, Biomimetic Materials, Nitriles, Organic chemistry, Glycosides, Supramolecular catalysis, Cyanohydrin
Abstract

(6AR,6DR)-6A,6D-di-C-cyano-beta-cyclodextrin (3) was synthesized and shown to catalyze hydrolysis of nitrophenyl glycosides with the reaction following Michaelis-Menten kinetics. At pH 7.4 and 25 degrees C, hydrolysis of 4-nitrophenyl-beta-glucopyranoside (2) was catalyzed with KM = 15 mM, kcat = 8.2 x 10-6 s-1, and kcat/kuncat = 1217. Catalysis was observed with concentration of 3 as low as 10 muM. Hydrolysis of the corresponding alpha-glucoside, alpha-galactoside, alpha-mannoside, and 2-nitrophenyl-beta-galactoside was also catalyzed by 3, with kcat/kuncat ranging from 283 to 2147. A series of analogues of 3 was prepared and investigated for catalysis of the hydrolysis of 2: (6AR,6DR)-6A,6D-di-C-propyl-beta-cyclodextrin (9) was not catalytic, while 6A,6D-di-C-cyano-6A,6D-dideoxy-beta-cyclodextrin (12) had a low catalytic activity (kcat/kuncat = 4). A kcat/kuncat = 48 was found for 6A,6D-dialdehydo-beta-cyclodextrin dihydrate (11). It was proposed that 3 acts by general acid catalysis on the bound substrate.

Published
2005

29. Artificial Glycosyl phosphorylases

Author

Fernando Ortega-Caballero, Mikael Bols, Torben E. Petersen, Lars Ulrik Rubæk Nordstrøm, Brian Christensen, and Cyril Rousseau

Subjects
Phosphorylases, Organic Chemistry, Kinetics, Substrate (chemistry), General Chemistry, Phosphate, Molecular sieve, Medicinal chemistry, Mass Spectrometry, Catalysis, Substrate Specificity, chemistry.chemical_compound, Hydrolysis, Sulfation, chemistry, Organic chemistry, Glycosyl, Nuclear Magnetic Resonance, Biomolecular
Abstract

alpha- and beta-Cyclodextrin 6(A),6(D)-diacids (1 and 2), beta-cyclodextrin-6-monoacid (14), beta-cyclodextrin 6(A),6(D)-di-O-sulfate (16) and beta-cyclodextrin-6-heptasulfate (19) were synthesised. Acids 1, 2 and 14 were made from perbenzylated alpha- or beta-cyclodextrin, by diisobutylaluminum hydride (DIBAL)-promoted debenzylation, oxidation and deprotection. Addition of molecular sieves was found to improve the debenzylation reaction. Sulfates 16 and 19 were made by sulfation of the appropriately partially protected derivatives and deprotection. Catalysis of 4-nitrophenyl glycoside cleavage by these cyclodextrin derivatives was studied. Compounds 1, 2 and 16 were found to catalyse the reaction, with the catalysis following Michaelis-Menten kinetics and depending first order on the phosphate concentration. In a phosphate buffer (0.5 M, 59 degrees C, pH 8.0), K(M) varied from 2-10 mM and the k(cat)/k(uncat) ratio from 80-1000 depending on the stereochemistry of the substrate and the catalyst, with 2 being the best catalyst and with the sulfated 16 also displaying catalytic ability. The monoacid 14 and the heptasulfate 19 were not catalytic.

Published
2005

31. Dendritic galactosides based on a beta-cyclodextrin core for the construction of site-specific molecular delivery systems: synthesis and molecular recognition studies

Author

Antonio, Vargas-Berenguel, Fernando, Ortega-Caballero, Francisco, Santoyo-González, Juan J, García-López, Juan J, Giménez-Martínez, Luis, García-Fuentes, and Emilia, Ortiz-Salmerón

Subjects
Cyclodextrins, Binding Sites, Arachis, beta-Cyclodextrins, Titrimetry, Galactosides, Calorimetry, Anilino Naphthalenesulfonates, Substrate Specificity, Structure-Activity Relationship, Drug Delivery Systems, Naphthalenesulfonates, Lectins, Thermodynamics
Abstract

In order to evaluate the ability of multivalent glycosides based on a beta-cyclodextrin core as site-specific molecular carriers, a study on both the inclusion complexation behaviour and lectin binding affinity of branched and hyperbranched beta-cyclodextrins is presented. A series of cluster galactosides constructed on beta-cyclodextrin scaffolds containing seven 1-thio-beta-lactose or beta-lactosylamine bound to the macrocyclic core through different spacer arms were synthesised. In addition, the first synthesis of three first-order dendrimers based on a beta-cyclodextrin core containing fourteen 1-thio-beta-D-galactose, 1-thio-beta-lactose and 1-thio-beta-melibiose residues was performed. Calorimetric titrations performed at 25 degrees C in buffered aqueous solution (pH 7.4) gave the affinity constants and the thermodynamic parameters for the complex formation of these beta-cyclodextrin derivatives with guests sodium 8-anilino-1-naphthalenesulfonate (ANS) and 2-naphthalenesulfonate, and lectin from peanut (Arachis hypogaea) (PNA). The persubstitution of the primary face of the beta-cyclodextrin with saccharides led to a slight increase of the binding constant values for the inclusion complexation with ANS relative to the native beta-cyclodextrin. However, the increase of the steric congestion due to the presence of the saccharide residues on the narrow rim of the beta-cyclodextrin may cause a decrease of the binding ability as shown for sodium 2-naphthalenesulfonate. The spacer arms are not passive elements and influence the host binding ability according to their chemical nature. PNA forms soluble cross-linked complexes with cluster galactosides and lactosides scaffolded on beta-cyclodextrin but not with cluster galactopyranosylamines or melibiose. Both, perbranched and hyperbranched beta-cyclodextrins, form stronger complexes with PNA than the monomeric analogues. However, the use of hyperbranched CDs does not contribute to the improvement of the complex stability relative to heptakis-glycocyclodextrin derivatives. Finally, a titration experiment with PNA and a complex formed by a heptakis lactose beta-cyclodextrin derivative with sodium 2-naphthalenesulfonate showed the formation of a soluble cross-linked complex with stronger affinity constant and higher stoichiometry than those observed for the complex formation of PNA with the same heptakis-lactose beta-cyclodextrin derivative, suggesting the formation of a three component complex.

Published
2002

34. High dopamine transporter selectivity can be displayed by remarkably simple non-nitrogen containing inhibitors

Author

Søren V. Boye, Fernando Ortega-Caballero, Steffen Sinning, Mikael Bols, Ove Wiborg, and Henrik H. Jensen

Subjects
chemistry.chemical_classification, Dopamine Plasma Membrane Transport Proteins, Spectrometry, Mass, Electrospray Ionization, Magnetic Resonance Spectroscopy, Monoamine transporter, biology, Chemistry, Stereochemistry, Carboxylic acid, Organic Chemistry, Clinical Biochemistry, Pharmaceutical Science, Nuclear magnetic resonance spectroscopy, Cyclopentanes, Biochemistry, Chemical synthesis, Biogenic amine, Drug Discovery, biology.protein, Molecular Medicine, Selectivity, Molecular Biology, Dopamine transporter
Abstract

A series of 2-(3,4-dichlorophenyl)-cyclopent-1-enyl carboxylic acid esters and amides were prepared and tested for binding to the DAT, SERT, and NET. The achiral compounds were easily attained and found to inhibit DAT binding with K(i)-values ranging from 0.095 to 0.00003 mM. Among the compounds tested 2-(3,4-dichlorophenyl)-cyclopent-1-enyl carboxylic acid 2-methylphenyl ester was found to be highly selective with SERT/DAT>7000; NET/DAT>1700, K(i)=60 nM.

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