Miguel Soriano
University of Granada
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Featured researches published by Miguel Soriano.
Chemosphere | 2000
M.A. Rivadeneyra; G. Delgado; Miguel Soriano; A. Ramos-Cormenzana; R. Delgado
We investigated the precipitation of carbonates by Nesterenkonia halobia in a liquid medium at different concentrations of salts and incubation times. N. halobia only produced crystals at salt concentrations of 2.5%, 7.5% and 15%. At 20% salt concentration no crystal formation was observed. Calcite, aragonite and dolomite were precipitated in different quantities, depending on the salinity of the medium and incubation time. Scanning and transmission electron microscopy, microanalysis and electron diffraction were all used to study in detail the morphology, composition and internal structure of the bioliths. We propose a mechanism for biolith formation involving both biological and inorganic processes.
Current Microbiology | 1999
María-Angustias Rivadeneyra; G. Delgado; Miguel Soriano; A. Ramos-Cormenzana; R. Delgado
Abstract. We studied the precipitation of carbonates in 17 strains of moderately halophilic, Gram-positive cocci belonging to two species: Marinococcus halophilus and Marinococcus albus, isolated from the Salar de Atacama (Chile). They were cultivated in solid and liquid laboratory media for 42 days at salt concentrations (wt/vol) of 3%, 7.5%, 15%, and 20%. The bioliths precipitated were studied by X-ray diffraction and scanning electron microscopy. M. halophilus formed crystals at each of the salt concentrations, with a maximum number of strains capable of precipitating carbonates at 7.5% and 15% salt concentrations. M. albus did not precipitate at 20% and showed a maximum at 7.5%. This behavior is similar to that of other Gram-positive bacteria and differs from that found in Gram-negative bacteria. The bioliths precipitated were spherical, generally isolated, with a size of 10–100 μm, varying with salinity. They were of magnesium calcite (CO3 Ca1-x Mgx) with Mg content increasing with increasing salinity and Mg/Ca molar ratio of the culture medium. These results demonstrate the active role played by M. halophilus and M. albus in the precipitation of carbonates.
Journal of Controlled Release | 2015
José L. Arias; Juan Diego Unciti-Broceta; José Maceira; Teresa Fajardo del Castillo; José Hernández-Quero; Stefan Magez; Miguel Soriano; Jose A. Garcia-Salcedo
Targeted delivery of therapeutics is an alternative approach for the selective treatment of infectious diseases. The surface of African trypanosomes, the causative agents of African trypanosomiasis, is covered by a surface coat consisting of a single variant surface glycoprotein, termed VSG. This coat is recycled by endocytosis at a very high speed, making the trypanosome surface an excellent target for the delivery of trypanocidal drugs. Here, we report the design of a drug nanocarrier based on poly ethylen glycol (PEG) covalently attached (PEGylated) to poly(D,L-lactide-co-glycolide acid) (PLGA) to generate PEGylated PLGA nanoparticles. This nanocarrier was coupled to a single domain heavy chain antibody fragment (nanobody) that specifically recognizes the surface of the protozoan pathogen Trypanosoma brucei. Nanoparticles were loaded with pentamidine, the first-line drug for T. b. gambiense acute infection. An in vitro effectiveness assay showed a 7-fold decrease in the half-inhibitory concentration (IC50) of the formulation relative to free drug. Furthermore, in vivo therapy using a murine model of African trypanosomiasis demonstrated that the formulation cured all infected mice at a 10-fold lower dose than the minimal full curative dose of free pentamidine and 60% of mice at a 100-fold lower dose. This nanocarrier has been designed with components approved for use in humans and loaded with a drug that is currently in use to treat the disease. Moreover, this flexible nanobody-based system can be adapted to load any compound, opening a range of new potential therapies with application to other diseases.
Therapeutic Delivery | 2013
Juan Diego Unciti-Broceta; Teresa del Castillo; Miguel Soriano; Stefan Magez; Jose A. Garcia-Salcedo
Nanobodies (Nbs) are small antibody fragments derived from camelid heavy chain antibodies through recombinant gene technology. Their exceptional physicochemical properties, possibility of humanization and unique antigen recognition properties make them excellent candidates for targeted delivery of biologically active components. Several different therapeutic approaches based on the novel camelid Nbs have been developed to treat a wide range of diseases ranging from immune, bone, blood and neurological disorders; infectious diseases and cancer. This review provides a comprehensive overview of the current state of the use of camelid-derived Nbs as novel therapeutic agents against multiple diseases.
PLOS Pathogens | 2015
Juan Diego Unciti-Broceta; José L. Arias; José Maceira; Miguel Soriano; Matilde Ortiz-González; José Hernández-Quero; Manuel Muñoz-Torres; Harry P. de Koning; Stefan Magez; Jose A. Garcia-Salcedo
African trypanosomiasis is a deadly neglected disease caused by the extracellular parasite Trypanosoma brucei. Current therapies are characterized by high drug toxicity and increasing drug resistance mainly associated with loss-of-function mutations in the transporters involved in drug import. The introduction of new antiparasitic drugs into therapeutic use is a slow and expensive process. In contrast, specific targeting of existing drugs could represent a more rapid and cost-effective approach for neglected disease treatment, impacting through reduced systemic toxicity and circumventing resistance acquired through impaired compound uptake. We have generated nanoparticles of chitosan loaded with the trypanocidal drug pentamidine and coated by a single domain nanobody that specifically targets the surface of African trypanosomes. Once loaded into this nanocarrier, pentamidine enters trypanosomes through endocytosis instead of via classical cell surface transporters. The curative dose of pentamidine-loaded nanobody-chitosan nanoparticles was 100-fold lower than pentamidine alone in a murine model of acute African trypanosomiasis. Crucially, this new formulation displayed undiminished in vitro and in vivo activity against a trypanosome cell line resistant to pentamidine as a result of mutations in the surface transporter aquaglyceroporin 2. We conclude that this new drug delivery system increases drug efficacy and has the ability to overcome resistance to some anti-protozoal drugs.
Reactive & Functional Polymers | 1998
Jesús Párraga; M.A. Rivadeneyra; R. Delgado; J. Iñiguez; Miguel Soriano; G. Delgado
Abstract The role of bacteria in mineral neoformation in a saline soil was studied. In this soil, authigenic precipitation of gypsum and calcite takes place. Bacteria isolated from the soil were cultivated ‘in vitro’ in solid and liquid media prepared from soil solutions (1: 1 extract). Precipitation of calcite spherulites of between 20 and 50 μm diameter and of other bioliths was observed. From soil solutions (1 : 1 extract and saturation extract) activity coefficients and the states of reaction for 18 minerals were calculated using the SOLMINEQ 88 program. Calcite, dolomite, gypsum and aragonite were in equilibrium with the saturation extract while in the 1:1 extract no mineral phases in equilibrium were present. Therefore, bacteria must play an active role in calcite precipitation in this saline soil.
Frontiers in Pharmacology | 2016
Jose A. Garcia-Salcedo; Juan Diego Unciti-Broceta; Javier Valverde-Pozo; Miguel Soriano
Leishmania and Trypanosoma are members of the Trypanosomatidae family that cause severe human infections such as leishmaniasis, Chagas disease, and sleeping sickness affecting millions of people worldwide. Despite efforts to eradicate them, migrations are expanding these infections to developing countries. There are no vaccines available and current treatments depend only on chemotherapy. Drug resistance is a major obstacle for the treatment of these diseases given that existing drugs are old and limited, with some having severe side effects. Most resistance mechanisms developed by these parasites are related with a decreased uptake or increased efflux of the drug due to mutations or altered expression of membrane transporters. Different new approaches have been elaborated that can overcome these mechanisms of resistance including the use of inhibitors of efflux pumps and drug carriers for both active and passive targeting. Here we review new formulations that have been successfully applied to circumvent resistance related to drug transporters, opening alternative ways to solve drug resistance in protozoan parasitic diseases.
Scientific Reports | 2017
Manuel Sánchez-Marañón; Isabel Miralles; José Félix Aguirre-Garrido; Manuel Anguita-Maeso; Vicenta Millán; Raúl Ortega; Jose A. Garcia-Salcedo; Francisco Martínez-Abarca; Miguel Soriano
Current research on the influence of environmental and physicochemical factors in shaping the soil bacterial structure has seldom been approached from a pedological perspective. We studied the bacterial communities of eight soils selected along a pedogenic gradient at the local scale in a Mediterranean calcareous mountain (Sierra de María, SE Spain). The results showed that the relative abundance of Acidobacteria, Canditate division WPS-1, and Armatimonadetes decreased whereas that of Actinobacteria, Bacteroidetes, and Proteobacteria increased from the less-developed soils (Leptosol) to more-developed soils (Luvisol). This bacterial distribution pattern was also positively correlated with soil-quality parameters such as organic C, water-stable aggregates, porosity, moisture, and acidity. In addition, at a lower taxonomic level, the abundance of Acidobacteria Gp4, Armatimonadetes_gp4, Solirubrobacter, Microvirga, Terrimonas, and Nocardioides paralleled soil development and quality. Therefore, our work indicates that the composition of bacterial populations changes with pedogenesis, which could be considered a factor influencing the communities according to the environmental and physicochemical conditions during the soil formation.
Nanomedicine: Nanotechnology, Biology and Medicine | 2015
Jose A. Garcia-Salcedo; Juan Diego Unciti-Broceta; Miguel Soriano
Archive | 2011
Isabel Miralles; Raúl Ortega; Vicenta Millán-Casamayor; Ma Carmen Leirós; Carmen Trasar-Cepeda; Miguel Soriano; Francisco Martínez-Abarca; F. Gil-Sotres