Your search keyword '"Esther Porras"' showing total 12 results

1. MymA Bioactivated Thioalkylbenzoxazole Prodrug Family Active against Mycobacterium tuberculosis

Author

Carine Sao Emani, Clement K. M. Tsui, Adama Bojang, Flavia Sorrentino, Yossef Av-Gay, María José Rebollo-López, Gagandeep Narula, Blanco Modesto J Remuinan, Eva Maria Lopez-Roman, Abraham L Moure, Beatriz Hernández Díaz, Esther Porras de Francisco, Patricia Casado Castro, Laura Guijarro López, Pedro Alfonso Torres-Gomez, Fátima Ortega, David Barros-Aguirre, Lluis Ballell, and Isabel Camino

Subjects

chemistry.chemical_classification, 0303 health sciences, biology, Intracellular parasite, Prodrug, biology.organism_classification, 01 natural sciences, In vitro, 0104 chemical sciences, 3. Good health, Mycobacterium tuberculosis, 010404 medicinal & biomolecular chemistry, 03 medical and health sciences, chemistry.chemical_compound, Enzyme, Biochemistry, chemistry, Drug Discovery, Molecular Medicine, Structure–activity relationship, Lead compound, Intracellular, 030304 developmental biology

Abstract

Screening of a GSK-proprietary library against intracellular Mycobacterium tuberculosis identified 1, a thioalkylbenzoxazole hit. Biological profiling and mutant analysis revealed that this compound is a prodrug that is bioactivated by the mycobacterial enzyme MymA. A hit-expansion program including design, synthesis, and profiling of a defined set of analogues with optimized drug-like properties led to the identification of an emerging lead compound, displaying potency against intracellular bacteria in the low micromolar range, high in vitro solubility and permeability, and excellent microsomal stability.

Published

2020

2. Dual-Pharmacophore Pyrithione-Containing Cephalosporins Kill Both Replicating and Nonreplicating

Author

Selin Somersan Karakaya, Landys Lopez Quezada, Kohta Saito, Cameron W Pharr, Sara Palomo Dı Az, Kelin Li, Quyen Nguyen, Hsin-Pin Ho Liang, Julia Roberts, Prisca Elis Javidnia, Manuel Marin Amieva, Véronique Dartois, Carl Nathan, Ben Gold, Stéphanie Sans, Matthew D. Zimmerman, Laurent Goullieux, Jeffrey Aubé, Alfonso Mendoza Losana, Esther Porras de Francisco, Christine Roubert, Andrew J. Perkowski, Kathrine McAulay, Stacey L. McDonald, Jun Zhang, and Sophie Lagrange

Subjects

0301 basic medicine, DNA Replication, Bacilli, Tuberculosis, medicine.drug_class, Pyridines, 030106 microbiology, Cephalosporin, Antitubercular Agents, Administration, Oral, Antimycobacterial, Article, Microbiology, Mycobacterium tuberculosis, 03 medical and health sciences, Mice, Drug Discovery, medicine, polycyclic compounds, Animals, Humans, biology, Chemistry, Thiones, Callithrix, Pyrithione, Hep G2 Cells, biology.organism_classification, medicine.disease, bacterial infections and mycoses, Cephalosporins, High-Throughput Screening Assays, 030104 developmental biology, Infectious Diseases, Female, Pharmacophore, Mycobacterium

Abstract

The historical view of β-lactams as ineffective antimycobacterials has given way to growing interest in the activity of this class against Mycobacterium tuberculosis (Mtb) in the presence of a β-lactamase inhibitor. However, most antimycobacterial β-lactams kill Mtb only or best when the bacilli are replicating. Here, a screen of 1904 β-lactams led to the identification of cephalosporins substituted with a pyrithione moiety at C3’ that are active against Mtb under both replicating and nonreplicating conditions, neither activity requiring a β-lactamase inhibitor. Studies showed that activity against nonreplicating Mtb required the in situ release of the pyrithione, independent of the known class A β-lactamase, BlaC. In contrast, replicating Mtb could be killed both by released pyrithione and by the parent β-lactam. Thus, the antimycobacterial activity of pyrithione-containing cephalosporins arises from two mechanisms that kill mycobacteria in different metabolic states.

Published

2019

3. Easy-To-Synthesize Spirocyclic Compounds Possess Remarkable in Vivo Activity against Mycobacterium tuberculosis

Author

Lourdes Encinas, Montserrat Ortega-Guerra, Ana Guardia, Joaquín Rullas, Esther Porras de Francisco, Juan Miguel-Siles, Cristina Rivero, Jorge Esquivias, Matthew H. Todd, Carlos Alemparte, Setshaba D. Khanye, Jessica Baiget, Raquel Vida Fernández, Winston Nxumalo, María Teresa Fraile-Gabaldón, Peter J. Rutledge, Esther Pérez-Herrán, Javier G. Osende, Modesto J. Remuiñán, Katrina A. Badiola, Marta León Alonso, Arancha Pérez, Ilaria Giordano, Elena Jimenez, Monica Cacho, and Fátima Ortega

Subjects

0301 basic medicine, ERG1 Potassium Channel, Maximum Tolerated Dose, 030106 microbiology, Antitubercular Agents, Drug Evaluation, Preclinical, Administration, Oral, Biological Availability, Computational biology, Mycobacterium tuberculosis, 03 medical and health sciences, Structure-Activity Relationship, In vivo, Drug Discovery, Animals, Humans, Tuberculosis, Spiro Compounds, biology, Low toxicity, Dose-Response Relationship, Drug, Chemistry, Heart, biology.organism_classification, Mice, Inbred C57BL, 030104 developmental biology, Open source, Molecular Medicine, Administration, Intravenous, Female, Rabbits

Abstract

Society urgently needs new, effective medicines for the treatment of tuberculosis. To kick-start the required hit-to-lead campaigns, the libraries of pharmaceutical companies have recently been evaluated for starting points. The GlaxoSmithKline (GSK) library yielded many high-quality hits, and the associated data were placed in the public domain to stimulate engagement by the wider community. One such series, the spiro compounds, are described here. The compounds were explored by a combination of traditional in-house research and open source methods. The series benefits from a particularly simple structure and a short associated synthetic chemistry route. Many members of the series displayed striking potency and low toxicity, and highly promising in vivo activity in a mouse model was confirmed with one of the analogues. Ultimately the series was discontinued due to concerns over safety, but the associated data remain public domain, empowering others to resume the series if the perceived deficiencies can be overcome.

Published

2018

4. An Invitation to Open Innovation in Malaria Drug Discovery: 47 Quality Starting Points from the TCAMS

Author

Pilar Manzano, Jose Luis Lavandera, Esther Porras, Francisco-Javier Gamo, Simon J. F. Macdonald, Jose M. Bueno, María Luisa León, Esther Fernández, Félix Calderón, David Barros, Julia Castro, Jose M. Coteron, Jose M. Fiandor, and Araceli Mallo

Subjects

Identification (information), Drug discovery, Computer science, media_common.quotation_subject, Organic Chemistry, Drug Discovery, Quality (business), Cluster analysis, Biochemistry, Data science, media_common, Open innovation, Hierarchical clustering

Abstract

In 2010, GlaxoSmithKline published the structures of 13533 chemical starting points for antimalarial lead identification. By using an agglomerative structural clustering technique followed by computational filters such as antimalarial activity, physicochemical properties, and dissimilarity to known antimalarial structures, we have identified 47 starting points for lead optimization. Their structures are provided. We invite potential collaborators to work with us to discover new clinical candidates.

Published

2011

5. Falcipain Inhibitors: Optimization Studies of the 2-Pyrimidinecarbonitrile Lead Series

Author

Mariola Gordo, Elena Sandoval, Jose M. Coteron, Jiri Gut, Beatriz Hernández Díaz, María J. Chaparro, Jennifer Legac, Santiago Ferrer, David Catterick, Julia Castro, Juan Miguel, Maria L. Marco, Pilar Ventosa, Philip J. Rosenthal, Vicente Muñoz, Jose M. Fiandor, José Ruiz, Juan C. de la Rosa, Francisco J. Gamo, Esther Porras, Esther Fernández, and Laura Fernández de las Heras

Subjects

chemistry.chemical_classification, Proteases, biology, Antiparasitic, medicine.drug_class, Plasmodium falciparum, Protozoan Proteins, Cysteine Proteinase Inhibitors, biology.organism_classification, Recombinant Proteins, Amino acid, Antimalarials, Cysteine Endopeptidases, Structure-Activity Relationship, Enzyme, chemistry, Drug development, Biochemistry, Drug Discovery, medicine, Hemoglobin hydrolysis, Molecular Medicine, Cysteine

Abstract

Falcipain-2 and falcipain-3 are papain-family cysteine proteases of the malaria parasite Plasmodium falciparum that are responsible for host hemoglobin hydrolysis to provide amino acids for parasite protein synthesis. Different heteroarylnitrile derivatives were studied as potential falcipain inhibitors and therefore potential antiparasitic lead compounds, with the 5-substituted-2-cyanopyrimidine chemical class emerging as the most potent and promising lead series. Through a sequential lead optimization process considering the different positions present in the initial scaffold, nanomolar and subnanomolar inhibitors at falcipains 2 and 3 were identified, with activity against cultured parasites in the micromolar range. Introduction of protonable amines within lead molecules led to marked improvements of up to 1000 times in activity against cultured parasites without noteworthy alterations in other SAR tendencies. Optimized compounds presented enzymatic activities in the picomolar to low nanomolar range and antiparasitic activities in the low nanomolar range.

Published

2010

6. Synthesis of New Serotonin 5-HT7 Receptor Ligands. Determinants of 5-HT7/5-HT1A Receptor Selectivity

Author

Bellinda Benhamú, Leonardo Pardo, Esther Porras, Mercedes Campillo, Rocío A Medina, Jessica Sallander, and María L. López-Rodríguez

Subjects

Models, Molecular, Indoles, Stereochemistry, Molecular Sequence Data, Serotonin 5-HT1 Receptor Antagonists, Ligands, Partial agonist, Chemical synthesis, Cell Line, 5-HT7 receptor, Radioligand Assay, Structure-Activity Relationship, chemistry.chemical_compound, Cricetulus, Cricetinae, Drug Discovery, Animals, Humans, Structure–activity relationship, Amino Acid Sequence, Receptor, Bicyclic molecule, Chemistry, Serotonin 5-HT1 Receptor Agonists, Isoquinolines, Serotonin Receptor Agonists, Drug Partial Agonism, Receptors, Serotonin, Receptor, Serotonin, 5-HT1A, Lactam, Molecular Medicine, Serotonin Antagonists, Selectivity

Abstract

We report the synthesis of a new set of compounds of general structure I (1-20) with structural modifications in the pharmacophoric elements of the previously reported lead UCM-5600. The new derivatives have been evaluated for binding affinity at 5-HT(7) and 5-HT(1A) receptors. The influence of the different structural features in terms of 5-HT(7)/5-HT(1A) receptor affinity and selectivity was analyzed by computational simulations of the complexes between compounds I and beta(2)-based 3-D models of these receptors. Compound 18 (HYD(1) = 1,3-dihydro-2H-indol-2-one; spacer = -(CH(2))(4)-; HYD(2) + HYD(3) = 3,4-dihydroisoquinolin-2(1H)-yl) exhibits high 5-HT(7)R affinity (K(i) = 7 nM) and selectivity over the 5-HT(1A)R (31-fold), and has been characterized as a partial agonist of the human 5-HT(7)R.

Published

2009

7. Synthesis and Structure−Activity Relationships of a New Model of Arylpiperazines. 5. Study of the Physicochemical Influence of the Pharmacophore on 5-HT1A/α1-Adrenergic Receptor Affinity: Synthesis of a New Derivative with Mixed 5-HT1A/D2 Antagonist Properties

Author

María L. López-Rodríguez, M. José Morcillo, Ma Eugenia Beneytez, Esther Fernandez, and Jorge Manzanares, L Orensanz, Esther Porras, and Jose Angel Fuentes

Subjects

chemistry.chemical_compound, Quantitative structure–activity relationship, chemistry, Bicyclic molecule, Stereochemistry, Amide, Drug Discovery, Substituent, Lactam, Molecular Medicine, Moiety, Pharmacophore, Chemical synthesis

Abstract

In this paper we have designed and synthesized a test series of 32 amide arylpiperazine derivatives VI in order to gain insight into the physicochemical influence of the pharmacophores of 5-HT1A and α1-adrenergic receptors. The training set was designed applying a fractional factorial design using six physicochemical descriptors. The amide moiety is a bicyclohydantoin or a diketopiperazine (X = −(CH2)3−, −(CH2)4−; m = 0, 1), the spacer length is 3 or 4 methylene units, which are the optimum values for both receptors, and the aromatic substituent R occupies the ortho- or meta-position and has been selected from a database of 387 substituents using the EDISFAR program. The 5-HT1A and α1-adrenergic receptor binding affinities of synthesized compounds VI (1−32) have been determined. This data set has been used to derive classical quantitative structure−activity relationships (QSAR) and neural networks models for both receptors (following paper). A comparison of these models gives information for the design of...

Published

2000

8. Synthesis and Structure−Activity Relationships of a New Model of Arylpiperazines. 3. 2-[ω-(4-Arylpiperazin-1-yl)alkyl]perhydropyrrolo- [1,2-c]imidazoles and -perhydroimidazo[1,5-a]pyridines: Study of the Influence of the Terminal Amide Fragment on 5-HT1A Affinity/Selectivity

Author

María L. López-Rodríguez, A M Sanz, M. J. Morcillo, M Murcia, Esther Porras, L Orensanz, and Esther Fernandez

Subjects

Imidazopyridine, Bicyclic molecule, Chemistry, Ligand, Stereochemistry, Chemical synthesis, chemistry.chemical_compound, nervous system, Amide, Drug Discovery, Molecular Medicine, Structure–activity relationship, Selectivity, Receptor

Abstract

A series of new arylpiperazine derivatives 2, which are devoid of the terminal amide fragment present in related 5-HT1A ligands, was prepared and evaluated for affinity at 5-HT1A and alpha 1 receptors. All the compounds 2 demonstrated high affinity for the 5-HT1A receptor and moderate affinity for alpha 1 receptor binding sites. Structure-activity relationship (SAR) studies suggest that there is influence of electronic factors on the no-pharmacophoric part of the alpha 1 receptor site. However there is no influence of electronic interactions on the stabilization of the 5-HT1A receptor-ligand complex.

Published

1997

9. Optimization of the pharmacophore model for 5-HT7R antagonism. Design and synthesis of new naphtholactam and naphthosultam derivatives

Author

Bellinda Benhamú, José A Ramos, Luis J Soto, Mireia Olivella, Leonardo Pardo, María L. López-Rodríguez, M. José Morcillo, José Luis Lavandera, Esther Porras, and Mercedes Campillo

Subjects

Male, Models, Molecular, Molecular model, Lactams, Stereochemistry, Hypothalamus, Molecular Conformation, In Vitro Techniques, Naphthalenes, Ligands, Chemical synthesis, Binding, Competitive, Rats, Sprague-Dawley, chemistry.chemical_compound, Radioligand Assay, Structure-Activity Relationship, Drug Discovery, Structure–activity relationship, Animals, Computer Simulation, Sulfonamides, Acceptor, Affinities, Rats, Transmembrane domain, Thiazoles, chemistry, Drug Design, Receptors, Serotonin, Lactam, Molecular Medicine, Serotonin Antagonists, Pharmacophore

Abstract

We present in this study an optimization of a preliminary pharmacophore model for 5-HT(7)R antagonism, with the incorporation of recently reported ligands and using an efficient procedure with the CATALYST program. The model consists of five features: a positive ionizable atom (PI), a H-bonding acceptor group (HBA), and three hydrophobic regions (HYD). This model has been supported by the design, synthesis, and biological evaluation of new naphtholactam and naphthosultam derivatives of general structure I (39-72). A systematic structure-affinity relationship (SAFIR) study on these analogues has allowed us to confirm that the model incorporates the essential structural features for 5-HT(7)R antagonism. In addition, computational simulation of the complex between compound 56 and a rhodopsin-based 3D model of the 5-HT(7)R transmembrane domain has permitted us to define the molecular details of the ligand-receptor interaction and gives additional support to the proposed pharmacophore model for 5-HT(7)R antagonism: (i) the HBA feature of the pharmacophore model binds Ser(5.42) and Thr(5.43), (ii) the HYD1 feature interacts with Phe(6.52), (iii) the PI feature forms an ionic interaction with Asp(3.32), and (iv) the HYD3 (AR) feature interacts with a set of aromatic residues (Phe(3.28), Tyr(7.43)). These results provide the tools for the design and synthesis of new ligands with predetermined affinities and pharmacological properties.

Published

2003

10. Corrections to Falcipain Inhibitors: Optimization Studies of the 2-Pyrimidinecarbonitrile Lead Series

Author

Beatriz Hernández Díaz, Esther Porras, Esther Fernández, José Ruiz, María J. Chaparro, Francisco J. Gamo, Julia Castro, Elena Sandoval, Juan C. de la Rosa, Jose M. Fiandor, Laura Fernández de las Heras, Jiri Gut, Jennifer Legac, David Catterick, Mariola Gordo, Jose M. Coteron, Santiago Ferrer, Philip J. Rosenthal, Maria L. Marco, Juan Miguel, Vicente Muñoz, and Pilar Ventosa

Subjects

Lead (geology), Series (mathematics), Computational chemistry, Chemistry, Drug Discovery, Molecular Medicine

Published

2010

11. First pharmacophoric hypothesis for 5-HT7 antagonism

Author

José Luis Lavandera, Bellinda Benhamú, José A. Ramos, Esther Porras, María L. López-Rodríguez, and M. José Morcillo

Subjects

Models, Molecular, Molecular model, Stereochemistry, Chemistry, Organic Chemistry, Clinical Biochemistry, Cell Membrane, Drug Evaluation, Preclinical, Hypothalamus, Pharmaceutical Science, Reproducibility of Results, Biochemistry, Rats, Structure-Activity Relationship, Drug Design, Receptors, Serotonin, Drug Discovery, Molecular Medicine, Animals, Serotonin Antagonists, Pharmacophore, Antagonism, Molecular Biology

Abstract

In order to make the first contribution to the elucidation of essential structural features for 5-HT7 antagonism, a set of thirty 5-HT7 antagonists were selected from the literature. A pharmacophore model was built using Molecular Modeling studies with Catalyst program. The information contained in this model was validated with new synthesized compounds.

Published

2000

12. Corrigendum to 'First pharmacophoric hypothesis for 5-HT7 antagonism'

Author

M. José Morcillo, Bellinda Benhamú, José Luis Lavandera, Esther Porras, María L. López-Rodríguez, and José A. Ramos

Subjects

Chemistry, Stereochemistry, Organic Chemistry, Clinical Biochemistry, Drug Discovery, Pharmaceutical Science, Molecular Medicine, Antagonism, Molecular Biology, Biochemistry

Published

2000