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Featured researches published by M.I. Torres.


Gut | 2011

Diversity in oat potential immunogenicity: basis for the selection of oat varieties with no toxicity in coeliac disease

Isabel Comino; Ana Real; Laura de Lorenzo; Hugh J. Cornell; Miguel Ángel López-Casado; Francisco Barro; Pedro Lorite; M.I. Torres; Angel Cebolla; Carolina Sousa

Background and aims Coeliac disease (CD) is triggered by an abnormal reaction to gluten. Peptides resulting from partially digested gluten of wheat, barley or rye cause inflammation of the small intestinal mucosa. Previous contradictory studies suggest that oats may trigger the abnormal immunological response in patients with CD. Monoclonal antibodies (moAbs) against the main immunotoxic 33-mer peptide (A1 and G12) react strongly against wheat, barley and rye but have less reactivity against oats. The stated aim of this study is to test whether this observed reactivity could be related to the potential toxicity of oats for patients with CD. Methods In the present study, different oat varieties, controlled for their purity and by their distinct protein pattern, were used to examine differences in moAb G12 recognition by ELISA and western blot. Immunogenicity of oat varieties was determined by 33-mer concentration, T cell proliferation and interferon γ production. Results Three groups of oat cultivars reacting differently against moAb G12 could be distinguished: a group with considerable affinity, a group showing slight reactivity and a third with no detectable reactivity. The immunogenicity of the three types of oats as well as that of a positive and negative control was determined with isolated peripheral blood mononuclear T cells from patients with CD by measurement of cell proliferation and interferon γ release. A direct correlation of the reactivity with G12 and the immunogenicity of the different prolamins was observed. Conclusions The results showed that the reactivity of the moAb G12 is proportional to the potential immunotoxicity of the cereal cultivar. These differences may explain the different clinical responses observed in patients suffering from CD and open up a means to identify immunologically safe oat cultivars, which could be used to enrich a gluten-free diet.


PLOS ONE | 2012

Molecular and Immunological Characterization of Gluten Proteins Isolated from Oat Cultivars That Differ in Toxicity for Celiac Disease

Ana Real; Isabel Comino; Laura de Lorenzo; Francisco Merchan; Javier Gil-Humanes; María J. Giménez; Miguel Ángel López-Casado; M.I. Torres; Angel Cebolla; Carolina Sousa; Francisco Barro; Fernando Pistón

A strict gluten-free diet (GFD) is the only currently available therapeutic treatment for patients with celiac disease (CD). Traditionally, treatment with a GFD has excluded wheat, barley and rye, while the presence of oats is a subject of debate. The most-recent research indicates that some cultivars of oats can be a safe part of a GFD. In order to elucidate the toxicity of the prolamins from oat varieties with low, medium, and high CD toxicity, the avenin genes of these varieties were cloned and sequenced, and their expression quantified throughout the grain development. At the protein level, we have accomplished an exhaustive characterization and quantification of avenins by RP-HPLC and an analysis of immunogenicity of peptides present in prolamins of different oat cultivars. Avenin sequences were classified into three different groups, which have homology with S-rich prolamins of Triticeae. Avenin proteins presented a lower proline content than that of wheat gliadin; this may contribute to the low toxicity shown by oat avenins. The expression of avenin genes throughout the development stages has shown a pattern similar to that of prolamins of wheat and barley. RP-HPLC chromatograms showed protein peaks in the alcohol-soluble and reduced-soluble fractions. Therefore, oat grains had both monomeric and polymeric avenins, termed in this paper gliadin- and glutenin-like avenins. We found a direct correlation between the immunogenicity of the different oat varieties and the presence of the specific peptides with a higher/lower potential immunotoxicity. The specific peptides from the oat variety with the highest toxicity have shown a higher potential immunotoxicity. These results suggest that there is wide range of variation of potential immunotoxicity of oat cultivars that could be due to differences in the degree of immunogenicity in their sequences.


Clinical and Experimental Immunology | 2007

Tryptophan metabolism and indoleamine 2,3-dioxygenase expression in coeliac disease

M.I. Torres; Miguel Ángel López-Casado; Pedro Lorite; A. Ríos

We have investigated the possible role of the metabolism of tryptophan and activity of the enzyme indoleamine 2,3‐dioxygenase (IDO) in the immune regulation of coeliac disease (CD). Serum concentrations of tryptophan and its metabolites kinurenines were determined by high performance liquid chromatography in 24 patients with CD, seven patients with Crohns disease and five healthy patients. We detected an increase of kynurenine (4·2 µmol/l ± 0·27 versus 2·6 µmol/l ± 0·54, P < 0002) and of the kynurenine/tryptophan ratio in supernatants of coeliac patients (11·5 µmol/l ± 1·01 versus 6·5 µmol/l ± 1·57, P < 0005) in comparison with healthy patients, respectively, and we found no differences with Crohns disease patients. Immunohistochemistry analysis of intestinal biopsies from CD patients showed an increased expression of IDO, interferon‐γ, interleukin‐10 and transforming growth factor‐β. Our data suggest that a mechanism(s) dependent on tryptophan catabolism might regulate the immune responses in CD.


Molecular Nutrition & Food Research | 2012

Significant differences in coeliac immunotoxicity of barley varieties.

Isabel Comino; Ana Real; Javier Gil-Humanes; Fernando Pistón; Laura de Lorenzo; Mª de Lourdes Moreno; Miguel Ángel López-Casado; Pedro Lorite; Angel Cebolla; M.I. Torres; Francisco Barro; Carolina Sousa

SCOPE The only treatment available for coeliac disease (CD) is a strict diet in which the intake of wheat, barley, rye, or oats is avoided. Barley is a major cereal crop, grown mainly for its use in brewing, and it has high nutritional value. The identification of varieties with a reduced toxicity profile may contribute to improve the diet, the quality of life and health of CD patients. METHODS AND RESULTS Searching for harmless barleys, we investigated accessions of malting and wild barley, used for developing new cultivated cereals. The CD toxicity profile of barleys was screened using G12 antibody and cell proliferation and IFN-γ release from peripheral blood mononuclear cells and intestinal biopsies from CD patients. We found a direct correlation between the reactivity with G12 and the immunogenicity of the different barleys. CONCLUSION The malting barleys were less immunogenic, with reduced levels of toxic gluten, and were possibly less harmful to CD patients. Our findings could raise the prospect of breeding barley species with low levels of harmful gluten, and the attractive goal of developing nontoxic barley cultivars, always taking into account the Codex standard for foods for special dietary use for persons intolerant to gluten.


Human Immunology | 2009

14–Base pair polymorphism of human leukocyte antigen–G as genetic determinant in heart transplantation and cyclosporine therapy monitoring

M.I. Torres; J. Luque; Pedro Lorite; B. Isla-Tejera; Teresa Palomeque; M.D. Aumente; J.M. Arizón; J. Peña

The 14-base pair (bp) polymorphism within the HLA-G gene has been investigated in heart transplant patients for the first time. The 14-bp polymorphism is associated with HLA-G mRNA stability and the patterns of alternative isoforms splicing, and therefore may influence the functionality of the HLA-G molecule. In heart transplantation, the highest production of soluble HLA-G was related to the -14/-14-bp genotype in the pre- and post-transplantation periods. Our study findings showed that the 14-bp polymorphism of the HLA-G gene influenced the expression of soluble HLA-G in heart transplantation and accordingly resulted in low rejection rates, being a possible marker of genetic variability associated with heart transplantation. In addition, the 14-bp polymorphism of the HLA-G gene is related to the absorber status of cyclosporine of each individual patient, and is useful for determining the oral dose of cyclosporine to manage patients (to adjust immunosuppressive protocols) so as to minimize the risk of a low or high immunosuppression and the side effects in the early stages of heart transplantation.


PLOS ONE | 2014

Identification and in vitro reactivity of celiac immunoactive peptides in an apparent gluten-free beer.

Ana Real; Isabel Comino; Mª de Lourdes Moreno; Miguel Ángel López-Casado; Pedro Lorite; M.I. Torres; Angel Cebolla; Carolina Sousa

Gluten content from barley, rye, wheat and in certain oat varieties, must be avoid in individuals with celiac disease. In most of the Western countries, the level of gluten content in food to be considered as gluten-free products is below 20 parts per million measured by ELISA based on specific anti-gluten peptide antibody. However, in beverages or food suffering complex hydrolytic processes as beers, the relative proportion of reactive peptides for celiac patients and the analytical techniques may differ, because of the diversity of the resulting peptide populations after fermentations. A beer below 20 parts per million of gluten but yet detectable levels of gluten peptides by anti-gliadin 33-mer antibodies (G12 and A1) was analyzed. We identified and characterized the relevant peptides for either antibody recognition or immunoactivity in celiac patients. The beer was fractionated by HPLC. The relative reactivity of the different HPLC fractions to the G12/A1 antibodies correlated to the reactivity of peripheral blood mononuclear cells isolated from 14 celiac individuals. Peptides from representative fractions classified according to the relative reactivity to G12/A1 antibodies were identified by mass spectrometry. The beer peptides containing sequences with similarity to those of previously described G12 and A1 epitopes were synthesized and confirmed significant reactivity for the antibodies. The most reactive peptides for G12/A1 also confirmed the highest immunogenicity by peripheral blood mononuclear cell activation and interferon γ production from celiac patients. We concluded that preparative HPLC combined with anti-gliadin 33-mer G12/A1 antibodies were very sensitive and specific methods to analyze the relevant immunogenic peptides in hydrolyzed gluten.


International Immunology | 2004

Expression of HLA-G in inflammatory bowel disease provides a potential way to distinguish between ulcerative colitis and Crohn's disease

M.I. Torres; M. Le Discorde; Pedro Lorite; A. Ríos; M. A. Gassull; A. Gil; J. Maldonado; Jean Dausset; Edgardo D. Carosella


Human Immunology | 2006

Soluble HLA-G in heart transplantation: their relationship to rejection episodes and immunosuppressive therapy.

J. Luque; M.I. Torres; M.D. Aumente; J. Marı́n; G. García-Jurado; R. González; D. Pascual; N. Guerra; F. López-Rubio; M.R. Álvarez-López; J.M. Arizón; J. Peña


International Immunology | 2006

New advances in coeliac disease: serum and intestinal expression of HLA-G

M.I. Torres; M A López-Casado; J Luque; J Peña; A. Ríos


Transplant Immunology | 2006

sHLA-G levels in the monitoring of immunosuppressive therapy and rejection following heart transplantation.

J. Luque; M.I. Torres; M.D. Aumente; J.M. Lozano; G. García-Jurado; R. González; M.R. Álvarez-López; J.M. Arizón; J. Peña

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A. Ríos

University of Granada

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Ana Real

University of Seville

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Angel Cebolla

Centre national de la recherche scientifique

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Francisco Barro

Spanish National Research Council

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Laura de Lorenzo

Spanish National Research Council

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