Immune Presentation and Regulation

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Content with Investigacion Infección Viral e Inmunidad .

Infección Viral e Inmunidad

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Guasp, P., E. Lorente, A. Martín-Esteban, E. Barnea, P. Romania, D. Fruci, J. J. W. Kuiper, A. Admon, and J. A. López de Castro. 2019. Redundancy and Complementarity between ERAP1 and ERAP2 Revealed by their Effects on the Behcet's Disease-Associated HLA-B*51 Peptidome. Mol.Cell Proteomics.

Guasp, P., E. Lorente, A. Martín-Esteban, E. Barnea, P. Romania, D. Fruci, J. J. W. Kuiper, A. Admon, and J. A. López de Castro. 2019. Redundancy and Complementarity between ERAP1 and ERAP2 Revealed by their Effects on the Behcet's Disease-Associated HLA-B*51 Peptidome. Mol.Cell Proteomics.

PUBMED DOI

CD69 targeting enhances anti-Vaccinia virus immunity

Notario L., Redondo-Antón J., Alari-Pahissa E., Albentosa A., Leiva M., López D., Sabio G., and Lauzurica P. (2019) CD69 targeting enhances anti-Vaccinia virus immunity. Journal of Virology 12;93(19). pii: e00553-19.

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Proteomics analysis reveals that structural proteins of the virion core and involved in gene expression are the main source for HLA class II ligands in vaccinia virus-infected cells.

Lorente, E., Martin-Galiano, A. J., Barnea, E., Barriga, A., Palomo, C., Garcia-Arriaza, J., Mir, C., Lauzurica, P., Esteban, M., Admon, A., and Lopez, D. (2019) Proteomics analysis reveals that structural proteins of the virion core and involved in gene expression are the main source for HLA class II ligands in vaccinia virus-infected cells. J.Proteome.Res. 18(9):3512-3520

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Computational characterization of the peptidome in transporter associated with antigen processing (TAP)-deficient cells.

Martin-Galiano, A. J. and Lopez, D. (2019) Computational characterization of the peptidome in transporter associated with antigen processing (TAP)-deficient cells. PLoS.ONE. 14, e0210583.

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Content with Investigacion Infección Viral e Inmunidad .

Ana Virseda Berdices

Investigador Predoctoral “CIBER”

ORCID code: 0000-0002-9549-567X
Amanda Fernández Rodríguez

Investigador Distinguido de OPIs

ORCID code: 0000-0002-5110-2213
Salvador Resino García

Investigador Científico de OPIs

ORCID code: 0000-0001-8783-0450
Daniel Sepúlveda Crespo

Investigador Postdoctoral “Sara Borrel”

ORCID code: 0000-0002-8053-6045
Rubén Martin Escolano

Investigador Postdoctoral “Juan de la Cierva”

ORCID code: 0000-0002-6262-9344
Raquel Behar Lagares

Investigador Predoctoral “Rio Hortega”

ORCID code: 0000-0003-1799-2723
Rafael Amigot Sánchez

Investigador Predoctoral “PFIS”

ORCID code: 0000-0001-9253-1631
Carlos Pita Martínez

Investigador Predoctoral “FPU”

ORCID code: 0000-0001-9253-1631
Mª José Muñoz Gómez

Investigador Predoctoral “CIBER”

ORCID code: 0000-0002-9244-4500
María Ángeles Jiménez Sousa

Científico Titular de OPIs

ORCID code: 0000-0002-1945-6169
Isidoro Martínez González

Científico Titular de OPIs

ORCID code: 0000-0002-9949-9264
Ignacio Rodríguez Izquierdo

Investigador Postdoctoral “Sara Borrel”

ORCID code: 0000-0002-6130-3545
Óscar Brochado Kith

Investigador Predoctoral “PFIS”

ORCID code: 0000-0001-8372-2604

List of staff

Additional Information

El grupo está interesado en el estudio de la respuesta inmune desde una perspectiva multidisciplinar que incluye aproximaciones genómicas, bioquímicas, proteómicas, modelos in vivo y biotecnológicas encaminadas al diseño de estrategias terapéuticas frente a diversas enfermedades crónicas, infecciosas y raras que poseen un claro componente inmunológico en su etiología. Los objetivos concretos actuales se centran en: Presentación antigénica: Identificación de las reglas de presentación antigénica para su aplicación en el diseño tratamientos terapéuticos incluyendo vacunas. Estudio de la función CD69 y su regulación; su uso como diana terapéutica en la movilización de precursores hematopoyéticos y en la potenciación de la respuesta inmune mediada por CD69 con en la potenciación de vacunas utilizando como vector el virus vaccinia.

The group is interested in the study of the immune response from a multidisciplinary perspective that includes genomic, biochemical, proteomic, in vivo and biotechnological models aimed at the design of therapeutic strategies against various chronic, infectious and rare diseases that have a clear immunological component in their etiology.

The current specific objectives focus on:

Antigenic presentation: Identification of antigenic presentation rules for their application in the design of therapeutic treatments including vaccines.
Study of CD69 function and its regulation; its use as a therapeutic target in the mobilization of hematopoietic precursors and in the potentiation of the immune response mediated by CD69 with the potentiation of vaccines using the vaccinia virus as a vector.

The current specific objectives focus on:

Antigenic presentation: Identification of antigenic presentation rules for their application in the design of therapeutic treatments including vaccines.
Study of CD69 function and its regulation; its use as a therapeutic target in the mobilization of hematopoietic precursors and in the potentiation of the immune response mediated by CD69 with the potentiation of vaccines using the vaccinia virus as a vector.

Investigation