Functional genomics of inborn errors and therapeutic interventions in high density lipoprotein metabolism

Objetivo

Despite considerable progress in prevention and therapy, coronary artery disease remains the most frequent cause of death. High- density lipoproteins (HDL) are promising targets to further reduce morbidity and mortality because low HDL cholesterol plasma concentrations increase cardiovascular risk and because HDL exerts many cardio- and vasoprotective functions. There is also great need in improving the diagnostic and prognostic value of the biomarker HDL cholesterol as HDL function is determined by the quality rather than by the quantity of HDL.

Therefore, this HDLomics project will apply functional genomics approaches including genomics, proteomics and lipidomics as well as new clinical diagnostic tools to study the effects of differential regulation of HDL metabolism on pathophysiological events relevant for atherosclerosis:
1) Using genome wide linkage analysis in families with Mendelian inheritance of low HDL cholesterol we will search new major genes regulating HDL cholesterol.
2) Using high throughput sequencing and allele specific genotyping technology we will elucidate the impact of mutations in candidate genes for the variation of HDL cholesterol as well as other lipid traits and the occurrence of cardiovascular events.
3) Using knock-out and transgenic mouse models we will study the metabolic and vascular impact of mutated candidate genes on HDL metabolism.
4) We will employ proteomic and lipidomic tools for the characterisation of HDL and finding specific effects of mutations or interventions on the structure and function of HDL as well as on lipid metabolism and atherosclerosis.
5. We will develop and evaluate new therapies including gene therapy protocols for the correction of inborn errors of HDL metabolism in humans.

The ultimate goals of HDLomics are hence the identification and validation of new targets, which can be used in differential diagnosis, prognosis, therapy, prevention, and therapy monitoring of low HDL cholesterol and atherosclerosis.

Ámbito científico (EuroSciVoc)

CORDIS clasifica los proyectos con EuroSciVoc, una taxonomía plurilingüe de ámbitos científicos, mediante un proceso semiautomático basado en técnicas de procesamiento del lenguaje natural. Véase: https://op.europa.eu/en/web/eu-vocabularies/euroscivoc.

• ciencias naturalesciencias biológicasbioquímicabiomoléculasproteínasproteómica
• ciencias socialessociologíademografíamortalidad
• ciencias médicas y de la saludbiotecnología médicaingeniería genéticaterapia génica
• ciencias médicas y de la saludmedicina clínicacardiologíaenfermedad cardiovasculararteriosclerosis
• ciencias naturalesciencias biológicasbioquímicabiomoléculaslípidos

Programa(s)

• FP6-LIFESCIHEALTH - Life sciences, genomics and biotechnology for health: Thematic Priority 1 under the Focusing and Integrating Community Research programme 2002-2006.

Tema(s)

• LSH-2005-2.1.1-4 - Functional genomics and regulatory networks in lipid metabolism and their effects on the development of atherogenic vascular disease
• LIFESCIHEALTH - Life sciences, genomics and biotechnology for health

Convocatoria de propuestas

FP6-2005-LIFESCIHEALTH-6
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Régimen de financiación

Coordinador

Participantes (6)