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Development of a chemical biology toolbox for deciphering the ubiquitin code

Descripción del proyecto

Descifrar el código de la ubiquitina

Tras la síntesis, las proteínas experimentan modificaciones postraslacionales que desempeñan un papel fundamental en su función. La adición de fragmentos de ubiquitina a las proteínas (ubiquitinación) es una de las modificaciones implicadas en muchos aspectos de la biología eucariota. Los científicos del proyecto financiado con fondos europeos Ubl-tool se proponen estudiar la ubiquitinación a través de nuevos métodos químicos y de biología sintética. Generarán patrones complejos de ubiquitina en proteínas, investigarán su impacto, e identificarán proteínas novedosas que lean el código de la ubiquitina. Dada la intervención de la ubiquitinación en muchas enfermedades humanas, como el cáncer y la neurodegeneración, los resultados de Ubl-tool tienen el potencial de identificar nuevas dianas terapéuticas.

Objetivo

Cells respond to external and internal stimuli by dynamically altering the functional status of existing proteins via post-translational modifications (PTMs). One of the most common and versatile PTMs in eukaryotic cells is represented by the covalent attachment of the 76-amino acid protein ubiquitin (Ub) to substrate proteins (ubiquitylation). Substrate modifications range from a single Ub moiety being attached to a protein of interest to complex polymeric Ub chains that can also contain Ub-like proteins (Ubls). Ubiquitylation plays pivotal roles in nearly all aspects of eukaryotic biology and cells dedicate an orchestrated arsenal of enzymes to install (writer proteins), translate (reader proteins) and reverse (eraser proteins) these modifications. The entirety of this complex regulatory system has been coined the Ub code. As many different human diseases, including different types of cancer and neurodegenerative diseases are being linked to dysfunctions in Ubl-related pathways, it is of utmost importance to decipher the Ub code.
Within Ubl-tool we devise a modular and interdisciplinary chemical and synthetic biology platform for studying aspects of ubiquitylation that are challenging or impossible to be addressed by more traditional technologies. We will develop innovative toolkits for generating defined Ubl architectures, including mixed, branched and hybrid Ubl chains and we will apply these tools for identifying novel reader proteins as well as for studying the functional impact of these complex types of modifications on critical cellular processes. Given its fundamental importance in eukaryotic biology, the Ub system has attracted considerable interest and promise as therapeutic target. We aim at identifying new drug targets within the Ub system by developing in cellulo activity-based probes that allow profiling activities and specificities of Ub eraser enzymes, laying thereby the foundation for the discovery of next-generation therapeutics.

Régimen de financiación

ERC-COG - Consolidator Grant

Institución de acogida

EIDGENOESSISCHE TECHNISCHE HOCHSCHULE ZUERICH
Aportación neta de la UEn
€ 1 997 717,00
Dirección
Raemistrasse 101
8092 Zuerich
Suiza

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Región
Schweiz/Suisse/Svizzera Zürich Zürich
Tipo de actividad
Higher or Secondary Education Establishments
Enlaces
Coste total
€ 1 997 717,00

Beneficiarios (1)