Your search keyword '"Vivian A. Salazar"' showing total 17 results

1. Gold Nanoparticle Virus-like Particles Presenting SARS-CoV-2 Spike Protein: Synthesis, Biophysical Properties and Immunogenicity in BALB/c Mice

Author

Vivian A. Salazar, Joan Comenge, Rosa Suárez-López, Judith A. Burger, Rogier W. Sanders, Neus G. Bastús, Carlos Jaime, Joan Joseph-Munne, and Victor Puntes

Subjects

virus-like particles (VLPs), gold nanoparticles, spike protein SARS-CoV-2, SARS-CoV-2 vaccine, Medicine

Abstract

Gold nanoparticles (AuNPs) decorated with antigens have recently emerged as promising tools for vaccine development due to their innate ability to provide stability to antigens and modulate immune responses. In this study, we have engineered deactivated virus-like particles (VLPs) by precisely functionalizing gold cores with coronas comprising the full SARS-CoV-2 spike protein (S). Using BALB/c mice as a model, we investigated the immunogenicity of these S-AuNPs-VLPs. Our results demonstrate that S-AuNPs-VLPs consistently enhanced antigen-specific antibody responses compared to the S protein free in solution. This enhancement included higher binding antibody titers, higher neutralizing capacity of antibodies, and stronger T-cell responses. Compared to the mRNA COVID-19 vaccine, where the S protein is synthesized in situ, S-AuNPs-VLPs induced comparable binding and neutralizing antibody responses, but substantially superior T-cell responses. In conclusion, our study highlights the potential of conjugated AuNPs as an effective antigen-delivery system for protein-based vaccines targeting a broad spectrum of infectious diseases and other emergent viruses.

Published

2024

2. Exploiting endocytosis for transfection of mRNA for cytoplasmatic delivery using cationic gold nanoparticles

Author

Muriel F. Gustà, Michael J. Edel, Vivian A. Salazar, Belén Alvarez-Palomo, Manel Juan, Massimo Broggini, Giovanna Damia, Paolo Bigini, Alessandro Corbelli, Fabio Fiordaliso, Alexander Barbul, Rafi Korenstein, Neus G. Bastús, and Víctor Puntes

Subjects

gold nanoparticles, cationic, transfection, gene therapeutics, safety, Immunologic diseases. Allergy, RC581-607

Abstract

IntroductionGene therapy holds promise to cure various diseases at the fundamental level. For that, efficient carriers are needed for successful gene delivery. Synthetic ‘non-viral’ vectors, as cationic polymers, are quickly gaining popularity as efficient vectors for transmitting genes. However, they suffer from high toxicity associated with the permeation and poration of the cell membrane. This toxic aspect can be eliminated by nanoconjugation. Still, results suggest that optimising the oligonucleotide complexation, ultimately determined by the size and charge of the nanovector, is not the only barrier to efficient gene delivery.MethodsWe herein develop a comprehensive nanovector catalogue comprising different sizes of Au NPs functionalized with two different cationic molecules and further loaded with mRNA for its delivery inside the cell.Results and DiscussionTested nanovectors showed safe and sustained transfection efficiencies over 7 days, where 50 nm Au NPs displayed the highest transfection rates. Remarkably, protein expression was increased when nanovector transfection was performed combined with chloroquine. Cytotoxicity and risk assessment demonstrated that nanovectors are safe, ascribed to lesser cellular damage due to their internalization and delivery via endocytosis. Obtained results may pave the way to design advanced and efficient gene therapies for safely transferring oligonucleotides.

Published

2023

3. The development of highly dense highly protected surfactant ionizable lipid RNA loaded nanoparticles

Author

Ramon González-Rioja, Vivian A. Salazar, Neus G. Bastús, and Victor Puntes

Subjects

ionizable lipid nanoparticles, RNA-loading, drug delivery carriers, pharmacokinetics, biodistribution and clearance, Immunologic diseases. Allergy, RC581-607

Abstract

The long quest for efficient drug administration has been looking for a universal carrier that can precisely transport traditional drugs, new genomic and proteic therapeutic agents. Today, researchers have found conditions to overcome the two main drug delivery dilemmas. On the one side, the versatility of the vehicle to efficiently load, protect and transport the drug and then release it at the target place. On the other hand, the questions related to the degree of PEGylation which are needed to avoid nanoparticle (NP) aggregation and opsonization while preventing cellular uptake. The development of different kinds of lipidic drug delivery vehicles and particles has resulted in the development of ionizable lipid nanoparticles (iLNPs), which can overcome most of the typical drug delivery problems. Proof of their success is the late approval and massive administration as the prophylactic vaccine for SARS-CoV-2. These ILNPs are built by electrostatic aggregation of surfactants, the therapeutic agent, and lipids that self-segregate from an aqueous solution, forming nanoparticles stabilized with lipid polymers, such as PEG. These vehicles overcome previous limitations such as low loading and high toxicity, likely thanks to low charge at the working pH and reduced size, and their entry into the cells via endocytosis rather than membrane perforation or fusion, always associated with higher toxicity. We herein revise their primary features, synthetic methods to prepare and characterize them, pharmacokinetic (administration, distribution, metabolization and excretion) aspects, and biodistribution and fate. Owing to their advantages, iLNPs are potential drug delivery systems to improve the management of various diseases and widely available for clinical use.

Published

2023

4. Evolutionary Trends in RNA Base Selectivity Within the RNase A Superfamily

Author

Guillem Prats-Ejarque, Lu Lu, Vivian A. Salazar, Mohammed Moussaoui, and Ester Boix

Subjects

RNase, RNA, purine, catalysis, molecular dynamics, evolution, Therapeutics. Pharmacology, RM1-950

Abstract

There is a growing interest in the pharmaceutical industry to design novel tailored drugs for RNA targeting. The vertebrate-specific RNase A superfamily is nowadays one of the best characterized family of enzymes and comprises proteins involved in host defense with specific cytotoxic and immune-modulatory properties. We observe within the family a structural variability at the substrate-binding site associated to a diversification of biological properties. In this work, we have analyzed the enzyme specificity at the secondary base binding site. Towards this end, we have performed a kinetic characterization of the canonical RNase types together with a molecular dynamic simulation of selected representative family members. The RNases’ catalytic activity and binding interactions have been compared using UpA, UpG and UpI dinucleotides. Our results highlight an evolutionary trend from lower to higher order vertebrates towards an enhanced discrimination power of selectivity for adenine respect to guanine at the secondary base binding site (B2). Interestingly, the shift from guanine to adenine preference is achieved in all the studied family members by equivalent residues through distinct interaction modes. We can identify specific polar and charged side chains that selectively interact with donor or acceptor purine groups. Overall, we observe selective bidentate polar and electrostatic interactions: Asn to N1/N6 and N6/N7 adenine groups in mammals versus Glu/Asp and Arg to N1/N2, N1/O6 and O6/N7 guanine groups in non-mammals. In addition, kinetic and molecular dynamics comparative results on UpG versus UpI emphasize the main contribution of Glu/Asp interactions to N1/N2 group for guanine selectivity in lower order vertebrates. A close inspection at the B2 binding pocket also highlights the principal contribution of the protein ß6 and L4 loop regions. Significant differences in the orientation and extension of the L4 loop could explain how the same residues can participate in alternative binding modes. The analysis suggests that within the RNase A superfamily an evolution pressure has taken place at the B2 secondary binding site to provide novel substrate-recognition patterns. We are confident that a better knowledge of the enzymes’ nucleotide recognition pattern would contribute to identify their physiological substrate and eventually design applied therapies to modulate their biological functions.

Published

2019

5. Antioxidant and Neuroprotective Properties of Non-Centrifugal Cane Sugar and Other Sugarcane Derivatives in an In Vitro Induced Parkinson’s Model

Author

Javier Cifuentes, Vivian A. Salazar, Mónica Cuellar, María Claudia Castellanos, Jader Rodríguez, Juan C. Cruz, and Carolina Muñoz-Camargo

Subjects

sugarcane, antioxidant, Parkinson’s disease, neuroprotective, mitochondrial membrane potential, non-centrifugal cane sugar, Therapeutics. Pharmacology, RM1-950

Abstract

Non-centrifugal cane sugar (NCS) is a traditional sweetener in most sugarcane regions of the world. In Colombia, this product has a socio-economic importance due to the extensive cultivation area and the high consumption rate per capita. NCS traditional processing involves consecutive stages of thermal processing that begin with juice extraction, clarification, evaporation, and finish with syrup crystallization into a solid commercial product, identified as NCS. Sugarcane is known to have a natural content of polyphenols, amino acids, vitamins, minerals, and complex sugars, some of which are reported as antioxidant and antiproliferative agents thought to be responsible for the product’s bioactive profile. There is evidence to suggest that traditional thermal processing to obtain NCS leads to a considerable decrease in the contents of these bioactive compounds, mainly due to uncontrolled process variables such as temperature. Accordingly, the aim of this study was to assess and compare the bioactivity of sugarcane (SC) derivatives produced under controlled thermal conditions versus the traditional method. To achieve this goal, we evaluated the cytotoxic, antioxidant, and neuroprotective effects of varying concentrations of SC derivatives in an in vitro induced Parkinson’s model. Results demonstrate non-cytotoxic activity on the cellular model by 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide (MTT) and LDH assays, even at the highest tested concentration of 8 mg/mL, for all SC derivatives. The effect of SC derivatives on the induced oxidative stress model showed a biological reversion and recovering effect of the mitochondrial membrane potential and a halting of the progress into the early apoptosis phase. In conclusion, we demonstrated that the bioactive compounds present in SC derivatives obtained by a process under controlled temperature conditions are largely preserved, and even their biological activities are enhanced compared with SC derivatives obtained by the traditional thermal evaporation of SC-juice.

Published

2021

6. Magnetite Nanoparticles Functionalized with RNases against Intracellular Infection of Pseudomonas aeruginosa

Author

Nathaly Rangel-Muñoz, Alejandra Suarez-Arnedo, Raúl Anguita, Guillem Prats-Ejarque, Johann F. Osma, Carolina Muñoz-Camargo, Ester Boix, Juan C. Cruz, and Vivian A. Salazar

Subjects

Pseudomonas aeruginosa, ribonucleases, magnetite nanoparticles, antimicrobials, Pharmacy and materia medica, RS1-441

Abstract

Current treatments against bacterial infections have severe limitations, mainly due to the emergence of resistance to conventional antibiotics. In the specific case of Pseudomonas aeruginosa strains, they have shown a number of resistance mechanisms to counter most antibiotics. Human secretory RNases from the RNase A superfamily are proteins involved in a wide variety of biological functions, including antimicrobial activity. The objective of this work was to explore the intracellular antimicrobial action of an RNase 3/1 hybrid protein that combines RNase 1 high catalytic and RNase 3 bactericidal activities. To achieve this, we immobilized the RNase 3/1 hybrid on Polyetheramine (PEA)-modified magnetite nanoparticles (MNPs). The obtained nanobioconjugates were tested in macrophage-derived THP-1 cells infected with Pseudomonas aeruginosa PAO1. The obtained results show high antimicrobial activity of the functionalized hybrid protein (MNP-RNase 3/1) against the intracellular growth of P. aeruginosa of the functionalized hybrid protein. Moreover, the immobilization of RNase 3/1 enhances its antimicrobial and cell-penetrating activities without generating any significant cell damage. Considering the observed antibacterial activity, the immobilization of the RNase A superfamily and derived proteins represents an innovative approach for the development of new strategies using nanoparticles to deliver antimicrobials that counteract P. aeruginosa intracellular infection.

Published

2020

7. Essential role of enzymatic activity in the leishmanicidal mechanism of the eosinophil cationic protein (RNase 3)

Author

María Ángeles Abengózar, María Fernández-Reyes, Vivian A. Salazar, Marc Torrent, Beatriz G. de la Torre, David Andreu, Ester Boix, Luis Rivas, Ministerio de Ciencia e Innovación (España), Agencia Estatal de Investigación (España), Consejo Superior de Investigaciones Científicas (España), Generalitat de Catalunya, CSIC - Unidad de Recursos de Información Científica para la Investigación (URICI), Abengozar, M. A., Fernández-Reyes, María, Salazar, Vivian A., Torrent, Marc, García de la Torre, Beatriz, Andreu, David, Boix, Ester, Rivas, Luis, Abengozar, M. A. [0000-0002-2432-3512], Fernández-Reyes, María [0000-0002-6078-9475], Salazar, Vivian A. [0000-0002-8441-9217], Torrent, Marc [0000-0001-6567-3474], García de la Torre, Beatriz [0000-0001-8521-9172], Andreu, David [0000-0002-6317-6666], Boix, Ester [0000-0003-1790-2142], and Rivas, Luis [0000-0002-2958-3233]

Subjects

Membrane disruption, Infectious Diseases, Ribonucleases, Anti-Infective Agents, Eosinophil Cationic Protein, Cell-penetrating enzyme, Humans, RNase, Eosinophil Granule Proteins, Protozoa, Antimicrobial peptide, Leishmania donovani

Abstract

11p.-6 fig.-1 tab.-1 graph. abst., The recruitment of eosinophils into Leishmania lesions is frequently associated with a favorable evolution. A feasible effector for this process is eosinophil cationic protein (ECP, RNase 3), one of the main human eosinophil granule proteins, endowed with a broad spectrum of antimicrobial activity, including parasites. ECP was active on Leishmania promastigotes and axenic amastigotes (LC50’s = 3 and 16 μM, respectively) but, in contrast to the irreversible membrane damage caused on bacteria and reproduced by its N-terminal peptides, it only induced a mild and transient plasma membrane destabilization on Leishmania donovani promastigotes. To assess the contribution of RNase activity to the overall leishmanicidal activity of ECP, parasites were challenged in parallel with a single-mutant version, ECP-H15A, devoid of RNase activity, that fully preserves the conformation and liposome permeabilization ability. ECP-H15A showed a similar uptake to ECP on promastigotes, but with higher LC50’s (>25 μM) for both parasite stages. ECP-treated promastigotes showed a degraded RNA pattern, absent in ECP-H15A-treated samples. Moreover ECP, but not ECP-H15A, reduced more than 2-fold the parasite burden of infected macrophages. Altogether, our results suggest that ECP enters the Leishmania cytoplasm by an endocytic pathway, ultimately leading to RNA degradation as a key contribution to the leishmanicidal mechanism. Thus, ECP combines both membrane destabilization and enzymatic activities to effect parasite killing. Taken together, our data highlight the microbicidal versatility of ECP as an innate immunity component and support the development of cell-penetrating RNases as putative leishmanicidal agents., This work was supported by MCIN/AEI/ 10.13039/501100011033-FEDER grant numbers PID2019-108166GB-I00 (E.B.), SAF2011-24899 (D.A.), by MCIN Subdirección General de Redes y Centros de Investigación Cooperativa-FEDER RD16/0027/0010 (L.R.), by CSIC PIE 201620E038 (L.R.), and by Generalitat de Catalunya grant 2009SGR492 to D.A. V.A.S. was a recipient of a Francisco Caldas-Colciencias predoctoral fellowship. We acknowledge support of the publication fee by the CSIC Open Access Support Initiative through its Unit of Information Resources for Research (URICI).

Published

2022

8. Unveiling the multifaceted mechanisms of antibacterial activity of buforin II and frenatin 2.3S peptides from skin micro-organs of the orinoco lime treefrog (Sphaenorhynchus lacteus)

Author

Carolina Muñoz-Camargo, Laura Andrea Barrero-Guevara, Helena Groot, Angela Mosquera, Ester Boix, Vivian A. Salazar, and Sandra Liliana Camargo

Subjects

0301 basic medicine, Cell Membrane Permeability, Frenatin 2.3S, Bacterial cell structure, Monocytes, lcsh:Chemistry, antimicrobial peptides, antibacterial activity, frog skin secretions, Lipid bilayer, lcsh:QH301-705.5, Spectroscopy, Skin, biology, Chemistry, General Medicine, Bacterial agglutination, Antimicrobial, membrane leakage, Computer Science Applications, Anti-Bacterial Agents, Buforin II, Biochemistry, Pseudomonas aeruginosa, Antimicrobial peptides, Anura, Antibacterial activity, Staphylococcus aureus, Membrane leakage, buforin II, Cell Survival, 030106 microbiology, bacterial agglutination, frenatin 2.3S, Catalysis, Article, Amphibian Proteins, Frog skin secretions, Inorganic Chemistry, Lime treefrog, 03 medical and health sciences, membrane translocation, Escherichia coli, Animals, Immunologic Factors, Physical and Theoretical Chemistry, DNA binding, Molecular Biology, Sequence Homology, Amino Acid, Organic Chemistry, Proteins, Membrane translocation, biology.organism_classification, 030104 developmental biology, lcsh:Biology (General), lcsh:QD1-999, Frog Skin, Bacteria, Antimicrobial Cationic Peptides

Abstract

Amphibian skin is a rich source of natural compounds with diverse antimicrobial and immune defense properties. Our previous studies showed that the frog skin secretions obtained by skin micro-organs from various species of Colombian anurans have antimicrobial activities against bacteria and viruses. We purified for the first time two antimicrobial peptides from the skin micro-organs of the Orinoco lime treefrog (Sphaenorhynchus lacteus) that correspond to Buforin II (BF2) and Frenatin 2.3S (F2.3S). Here, we have synthesized the two peptides and tested them against Gram-negative and Gram-positive bacteria, observing an effective bactericidal activity at micromolar concentrations. Evaluation of BF2 and F2.3S membrane destabilization activity on bacterial cell cultures and synthetic lipid bilayers reveals a distinct membrane interaction mechanism. BF2 agglutinates E. coli cells and synthetic vesicles, whereas F2.3S shows a high depolarization and membrane destabilization activities. Interestingly, we found that F2.3S is able to internalize within bacterial cells and can bind nucleic acids, as previously reported for BF2. Moreover, bacterial exposure to both peptides alters the expression profile of genes related to stress and resistance response. Overall, these results show the multifaceted mechanism of action of both antimicrobial peptides that can provide alternative tools in the fight against bacterial resistance.

Published

2021

9. Exploring the mechanisms of action of human secretory RNase 3 and RNase 7 against Candida albicans

Author

Susanna Navarro, Vivian A. Salazar, Javier Arranz-Trullén, Ester Boix, Jose A. Blanco, Mohammed Moussaoui, and Daniel Barrientos Sánchez

Subjects

0301 basic medicine, Antifungal Agents, RNase P, Cytotoxicity, 030106 microbiology, Mutagenesis (molecular biology technique), Biology, infectious diseases, Microbiology, 03 medical and health sciences, Ribonucleases, Catalytic Domain, Candida albicans, Humans, Amino Acid Sequence, innate immunity, Peptide sequence, Original Research, chemistry.chemical_classification, Innate immunity, Microscopy, Confocal, Innate immune system, Host-pathogen interactions, Eosinophil Cationic Protein, RNA, RNA, Fungal, biology.organism_classification, Immunity, Innate, Yeast, 030104 developmental biology, Enzyme, chemistry, Biochemistry, Mutagenesis, Site-Directed, Infectious diseases, host–pathogen interactions

Abstract

Human antimicrobial RNases, which belong to the vertebrate RNase A superfamily and are secreted upon infection, display a wide spectrum of antipathogen activities. In this work, we examined the antifungal activity of the eosinophil RNase 3 and the skin‐derived RNase 7, two proteins expressed by innate cell types that are directly involved in the host defense against fungal infection. Candida albicans has been selected as a suitable working model for testing RNase activities toward a eukaryotic pathogen. We explored the distinct levels of action of both RNases on yeast by combining cell viability and membrane model assays together with protein labeling and confocal microscopy. Site‐directed mutagenesis was applied to ablate either the protein active site or the key anchoring region for cell binding. This is the first integrated study that highlights the RNases’ dual mechanism of action. Along with an overall membrane‐destabilization process, the RNases could internalize and target cellular RNA. The data support the contribution of the enzymatic activity for the antipathogen action of both antimicrobial proteins, which can be envisaged as suitable templates for the development of novel antifungal drugs. We suggest that both human RNases work as multitasking antimicrobial proteins that provide a first line immune barrier.

Published

2021

10. Insight into the Antifungal Mechanism of Action of Human RNase N-terminus Derived Peptides

Author

Vivian A. Salazar, Marc Torrent, David Andreu, Javier Arranz-Trullén, Guillem Prats-Ejarque, David Pulido, and Ester Boix

Subjects

0301 basic medicine, Antifungal Agents, RNase P, 030106 microbiology, Antimicrobial peptides, Drug resistance, RNaseA superfamily, Catalysis, Article, Microbiology, Inorganic Chemistry, lcsh:Chemistry, 03 medical and health sciences, antimicrobial peptides, Ribonucleases, Cell Wall, Candida albicans, medicine, Humans, Antifungal activity, Physical and Theoretical Chemistry, Mode of action, Molecular Biology, lcsh:QH301-705.5, Spectroscopy, biology, Organic Chemistry, antifungal activity, Cell Membrane, Eosinophil Cationic Protein, Biofilm, General Medicine, biology.organism_classification, Corpus albicans, Computer Science Applications, 030104 developmental biology, Mechanism of action, lcsh:Biology (General), lcsh:QD1-999, Biofilms, medicine.symptom, Peptides

Abstract

Candida albicans is a polymorphic fungus responsible for mucosal and skin infections. Candida cells establish themselves into biofilm communities resistant to most currently available antifungal agents. An increase of severe infections ensuing in fungal septic shock in elderly or immunosuppressed patients, along with the emergence of drug-resistant strains, urge the need for the development of alternative antifungal agents. In the search for novel antifungal drugs our laboratory demonstrated that two human ribonucleases from the vertebrate-specific RNaseA superfamily, hRNase3 and hRNase7, display a high anticandidal activity. In a previous work, we proved that the N-terminal region of the RNases was sufficient to reproduce most of the parental protein bactericidal activity. Next, we explored their potency against a fungal pathogen. Here, we have tested the N-terminal derived peptides that correspond to the eight human canonical RNases (RN1-8) against planktonic cells and biofilms of C. albicans. RN3 and RN7 peptides displayed the most potent inhibitory effect with a mechanism of action characterized by cell-wall binding, membrane permeabilization and biofilm eradication activities. Both peptides are able to eradicate planktonic and sessile cells, and to alter their gene expression, reinforcing its role as a lead candidate to develop novel antifungal and antibiofilm therapies. This research was funded by the Ministerio de Economía y Competitividad (SAF2017-82158-R and SAF2015-66007P, Fundació La Marató de TV3 (20180310) and Generalitat de Catalunya (2016-PROD-00060). M.T. would like to acknowledge support from the Programa Ramon y Cajal (RYC-2012-09999) and the European Society of Clinical Microbiology and Infectious Diseases though ans ESCMID-2016 grant.

Published

2019

11. Evolutionary trends in RNA base selectivity within the RNase A superfamily

Author

Mohammed Moussaoui, Vivian A. Salazar, Guillem Prats-Ejarque, Ester Boix, and Lu Lu

Subjects

0301 basic medicine, Purine, Stereochemistry, RNase P, Guanine, Evolution, Molecular dynamics, Catalysis, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, evolution, RNase, Pharmacology (medical), Nucleotide, Binding site, Original Research, chemistry.chemical_classification, Pharmacology, purine, catalysis, lcsh:RM1-950, RNA, molecular dynamics, RNase A superfamily, lcsh:Therapeutics. Pharmacology, 030104 developmental biology, Order (biology), Enzyme, chemistry, 030220 oncology & carcinogenesis

Abstract

Altres ajuts: Fundació La Marató de TV3 (Marató 20180310) There is a growing interest in the pharmaceutical industry to design novel tailored drugs for RNA targeting. The vertebrate-specific RNase A superfamily is nowadays one of the best characterized family of enzymes and comprises proteins involved in host defense with specific cytotoxic and immune-modulatory properties. We observe within the family a structural variability at the substrate-binding site associated to a diversification of biological properties. In this work, we have analyzed the enzyme specificity at the secondary base binding site. Towards this end, we have performed a kinetic characterization of the canonical RNase types together with a molecular dynamic simulation of selected representative family members. The RNases' catalytic activity and binding interactions have been compared using UpA, UpG and UpI dinucleotides. Our results highlight an evolutionary trend from lower to higher order vertebrates towards an enhanced discrimination power of selectivity for adenine respect to guanine at the secondary base binding site (B2). Interestingly, the shift from guanine to adenine preference is achieved in all the studied family members by equivalent residues through distinct interaction modes. We can identify specific polar and charged side chains that selectively interact with donor or acceptor purine groups. Overall, we observe selective bidentate polar and electrostatic interactions: Asn to N1/N6 and N6/N7 adenine groups in mammals versus Glu/Asp and Arg to N1/N2, N1/O6 and O6/N7 guanine groups in non-mammals. In addition, kinetic and molecular dynamics comparative results on UpG versus UpI emphasize the main contribution of Glu/Asp interactions to N1/N2 group for guanine selectivity in lower order vertebrates. A close inspection at the B2 binding pocket also highlights the principal contribution of the protein β6 and L4 loop regions. Significant differences in the orientation and extension of the L4 loop could explain how the same residues can participate in alternative binding modes. The analysis suggests that within the RNase A superfamily an evolution pressure has taken place at the B2 secondary binding site to provide novel substrate-recognition patterns. We are confident that a better knowledge of the enzymes' nucleotide recognition pattern would contribute to identify their physiological substrate and eventually design applied therapies to modulate their biological functions.

Published

2019

12. Antioxidant and Neuroprotective Properties of Non-Centrifugal Cane Sugar and Other Sugarcane Derivatives in an In Vitro Induced Parkinson’s Model

Author

Jader Rodríguez, Monica Cuellar, Javier Cifuentes, Vivian A. Salazar, Juan C. Cruz, Carolina Muñoz-Camargo, and Maria Claudia Castellanos

Subjects

0301 basic medicine, antioxidant, Antioxidant, Physiology, Parkinson's disease, medicine.medical_treatment, Clinical Biochemistry, RM1-950, medicine.disease_cause, Biochemistry, Article, 03 medical and health sciences, chemistry.chemical_compound, mitochondrial membrane potential, 0302 clinical medicine, Bromide, sugarcane, medicine, Food science, Sugar, Molecular Biology, chemistry.chemical_classification, Chemistry, Extraction (chemistry), neuroprotective, Cell Biology, Sugarcane, In vitro, Amino acid, Non-centrifugal cane sugar, 030104 developmental biology, Polyphenol, Parkinson’s disease, Therapeutics. Pharmacology, Mitochondrial membrane potential, non-centrifugal cane sugar, Neuroprotective, 030217 neurology & neurosurgery, Oxidative stress

Abstract

Non-centrifugal cane sugar (NCS) is a traditional sweetener in most sugarcane regions of the world. In Colombia, this product has a socio-economic importance due to the extensive cultivation area and the high consumption rate per capita. NCS traditional processing involves consecutive stages of thermal processing that begin with juice extraction, clarification, evaporation, and finish with syrup crystallization into a solid commercial product, identified as NCS. Sugarcane is known to have a natural content of polyphenols, amino acids, vitamins, minerals, and complex sugars, some of which are reported as antioxidant and antiproliferative agents thought to be responsible for the product’s bioactive profile. There is evidence to suggest that traditional thermal processing to obtain NCS leads to a considerable decrease in the contents of these bioactive compounds, mainly due to uncontrolled process variables such as temperature. Accordingly, the aim of this study was to assess and compare the bioactivity of sugarcane (SC) derivatives produced under controlled thermal conditions versus the traditional method. To achieve this goal, we evaluated the cytotoxic, antioxidant, and neuroprotective effects of varying concentrations of SC derivatives in an in vitro induced Parkinson’s model. Results demonstrate non-cytotoxic activity on the cellular model by 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide (MTT) and LDH assays, even at the highest tested concentration of 8 mg/mL, for all SC derivatives. The effect of SC derivatives on the induced oxidative stress model showed a biological reversion and recovering effect of the mitochondrial membrane potential and a halting of the progress into the early apoptosis phase. In conclusion, we demonstrated that the bioactive compounds present in SC derivatives obtained by a process under controlled temperature conditions are largely preserved, and even their biological activities are enhanced compared with SC derivatives obtained by the traditional thermal evaporation of SC-juice.

Published

2021

13. Characterization of an RNase with two catalytic centers. Human RNase6 catalytic and phosphate-binding site arrangement favors the endonuclease cleavage of polymeric substrates

Author

Victòria M. Nogués, Jose A. Blanco, Guillem Prats-Ejarque, Vivian A. Salazar, Ester Boix, and Mohammed Moussaoui

Subjects

0301 basic medicine, Exonucleases, Stereochemistry, RNase P, Polymers, Endoribonuclease, Biophysics, Cleavage (embryo), Crystallography, X-Ray, Biochemistry, Catalysis, Protein Structure, Secondary, Phosphates, Active center, 03 medical and health sciences, Ribonucleases, Catalytic Domain, Catalytic triad, Hydrolase, Humans, Histidine, Binding site, Molecular Biology, 030102 biochemistry & molecular biology, biology, Chemistry, Lysine, Active site, Ribonuclease, Pancreatic, Endonucleases, Kinetics, 030104 developmental biology, Mutation, biology.protein, Mutagenesis, Site-Directed

Abstract

Background Human RNase6 is a small cationic antimicrobial protein that belongs to the vertebrate RNaseA superfamily. All members share a common catalytic mechanism, which involves a conserved catalytic triad, constituted by two histidines and a lysine (His15/His122/Lys38 in RNase6 corresponding to His12/His119/Lys41 in RNaseA). Recently, our first crystal structure of human RNase6 identified an additional His pair (His36/His39) and suggested the presence of a secondary active site. Methods In this work we have explored RNase6 and RNaseA subsite architecture by X-ray crystallography, site-directed mutagenesis and kinetic characterization. Results The analysis of two novel crystal structures of RNase6 in complex with phosphate anions at atomic resolution locates a total of nine binding sites and reveals the contribution of Lys87 to phosphate-binding at the secondary active center. Contribution of the second catalytic triad residues to the enzyme activity is confirmed by mutagenesis. RNase6 catalytic site architecture has been compared with an RNaseA engineered variant where a phosphate-binding subsite is converted into a secondary catalytic center (RNaseA-K7H/R10H). Conclusions We have identified the residues that participate in RNase6 second catalytic triad (His36/His39/Lys87) and secondary phosphate-binding sites. To note, residues His39 and Lys87 are unique within higher primates. The RNaseA/RNase6 side-by-side comparison correlates the presence of a dual active site in RNase6 with a favored endonuclease-type cleavage pattern. General significance An RNase dual catalytic and extended binding site arrangement facilitates the cleavage of polymeric substrates. This is the first report of the presence of two catalytic centers in a single monomer within the RNaseA superfamily.

Published

2018

14. Protein post-translational modification in host defense: the antimicrobial mechanism of action of human eosinophil cationic protein native forms

Author

Ester Boix, David Pulido, Per Venge, M.V. Nogués, Jenny Rubin, Vivian A. Salazar, and Mohammed Moussaoui

Subjects

Eosinophil cationic protein, Glycosylation, Eosinophil Cationic Protein, Antimicrobial peptides, Microbial Sensitivity Tests, Cell Biology, Biology, medicine.disease_cause, medicine.disease, Antimicrobial, Biochemistry, Lipopolysaccharide binding, chemistry.chemical_compound, chemistry, Specific granule, Protein toxicity, Escherichia coli, medicine, Humans, Protein Processing, Post-Translational, Molecular Biology

Abstract

Knowledge on the contribution of protein glycosylation in host defense antimicrobial peptides is still scarce. We have studied here how the post-translational modification pattern modulates the antimicrobial activity of one of the best characterized leukocyte granule proteins. The human eosinophil cationic protein (ECP), an eosinophil specific granule protein secreted during inflammation and infection, can target a wide variety of pathogens. Previous work in human eosinophil extracts identified several ECP native forms and glycosylation heterogeneity was found to contribute to the protein biological properties. In this study we analyze for the first time the antimicrobial activity of the distinct native proteins purified from healthy donor blood. Low and heavy molecular weight forms were tested on Escherichia coli cell cultures and compared with the recombinant non-glycosylated protein. Further analysis on model membranes provided an insight towards an understanding of the protein behavior at the cytoplasmic membrane level. The results highlight the significant reduction in protein toxicity and bacteria agglutination activity for heavy glycosylated fractions. Notwithstanding, the lower glycosylated fraction mostly retains the lipopolysaccharide binding affinity together with the cytoplasmic membrane depolarization and membrane leakage activities. From structural analysis we propose that heavy glycosylation interferes with the protein self-aggregation, hindering the cell agglutination and membrane disruption processes. The results suggest the contribution of post-translational modifications to the antimicrobial role of ECP in host defense.

Published

2014

15. Frog skin cultures secrete anti-yellow fever compounds

Author

Margarita Correa Méndez, Franz Kaston Florez, Maria Mercedes Torres, Johanna Moscoso, Vivian A. Salazar, Carolina Muñoz-Camargo, Eduardo Mitrani, Diana Marcela Devia Narvaez, and Helena Groot

Subjects

0301 basic medicine, Ranidae, Antimicrobial peptides, CHO Cells, Pharmacology, Antiviral Agents, Virus, Amphibian Proteins, Microbiology, 03 medical and health sciences, Cricetulus, Drug Discovery, Chlorocebus aethiops, medicine, Animals, Amino Acid Sequence, Cloning, Molecular, Cytotoxicity, Vero Cells, Skin, biology, Base Sequence, Yellow fever, Sequence Analysis, DNA, biology.organism_classification, Antimicrobial, medicine.disease, Flavivirus, 030104 developmental biology, Vero cell, Yellow fever virus, Peptides, Frog Skin

Abstract

There is an urgent need to develop novel antimicrobial substances. Antimicrobial peptides (AMPs) are considered as promising candidates for future therapeutic use. Because of the re-emergence of the Flavivirus infection, and particularly the yellow fever virus (YFV), we have compared the antiviral activities from skin secretions of seven different frog species against YFV (strain 17D). Secretions from Sphaenorhynchus lacteus, Cryptobatrachus boulongeri and Leptodactylus fuscus displayed the more powerful activities. S. lacteus was found to inhibit viral lysis of Vero E6 cells even at the highest viral concentration evaluated of 10 LD50. We also report the identification of a novel frenatin-related peptide from S. lacteus and found that this peptide-on its own-can lead to 35% protection against YVF, while displaying no cytotoxicity against somatic cells even at fivefold higher concentrations. These results are attractive and support the need for continued exploration of new sources of AMPs from frog skin secretions such as those described here in the development of new compounds for the treatment of infectious diseases in general and specific viral infections in particular.

Published

2015

16. Structural determinants of the eosinophil cationic protein antimicrobial activity

Author

Marc Torrent, VIVIAN ANGELICA SALAZAR MONTOYA, Mohammed Moussaoui, Ester Boix, Vivian Angélica Salazar, M. Victoria Nogués, and David Pulido-Gomez

Subjects

Models, Molecular, RNase P, Proteolysis, Clinical Biochemistry, Molecular Sequence Data, Sequence alignment, Biology, Bacterial Physiological Phenomena, Biochemistry, medicine, Animals, Humans, Immunologic Factors, Amino Acid Sequence, Molecular Biology, Peptide sequence, Eosinophil cationic protein, medicine.diagnostic_test, Eosinophil Cationic Protein, Immunity, Innate, Anti-Bacterial Agents, Docking (molecular), Host-Pathogen Interactions, Nucleic acid, Bacterial outer membrane, Sequence Alignment

Abstract

Antimicrobial RNases are small cationic proteins belonging to the vertebrate RNase A superfamily and endowed with a wide range of antipathogen activities. Vertebrate RNases, while sharing the active site architecture, are found to display a variety of noncatalytical biological properties, providing an excellent example of multitask proteins. The antibacterial activity of distant related RNases suggested that the family evolved from an ancestral host-defence function. The review provides a structural insight into antimicrobial RNases, taking as a reference the human RNase 3, also named eosinophil cationic protein (ECP). A particular high binding affinity against bacterial wall structures mediates the protein action. In particular, the interaction with the lipopolysaccharides at the Gram-negative outer membrane correlates with the protein antimicrobial and specific cell agglutinating activity. Although a direct mechanical action at the bacteria wall seems to be sufficient to trigger bacterial death, a potential intracellular target cannot be discarded. Indeed, the cationic clusters at the protein surface may serve both to interact with nucleic acids and cell surface heterosaccharides. Sequence determinants for ECP activity were screened by prediction tools, proteolysis and peptide synthesis. Docking results are complementing the structural analysis to delineate the protein anchoring sites for anionic targets of biological significance.

Published

2012

17. Skin micro-organs from several frog species secrete a repertoire of powerful antimicrobials in culture

Author

Carolina Muñoz-Camargo, Vivian A. Salazar, Helena Groot, Franz Kaston Florez, Gina Riveros, Eduardo Mitrani, and Johanna Moscoso

Subjects

Pharmacology, Amphibian, Ranidae, Somatic cell, Cell Survival, Reverse Transcriptase Polymerase Chain Reaction, Repertoire, Microbial Sensitivity Tests, Biology, Colombia, Antimicrobial, In vitro, Amphibian Proteins, Microbiology, Cell Line, Organ Culture Techniques, biology.animal, Drug Discovery, Animals, RNA, Secretion, Antibacterial activity, Frog Skin, Antimicrobial Cationic Peptides, Skin

Abstract

This work is an attempt to take advantage of the rich biodiversity that exists in Colombia in order to start a systematic analysis of antimicrobial substances that have emerged through amphibian evolution. For this purpose we have developed a technique to grow intact frog skin derived micro-organs (SMOs) in vitro in the absence of serum. We show that in SMOs, the skin glands remain intact and continue to secrete into the medium substances with potent antibacterial activity, for several days in culture. Our strategy has been to create a bank of substances secreted by amphibian skin from different species. This bank contains at present around 50 species and is of particular importance as some of the species are in danger of disappearing. We show that some of the species tested displayed very strong antibacterial activity without being toxic to somatic cell lines, even at 10-fold higher concentration.

Published

2012