eNOS Activation by HDL Is Impaired in Genetic CETP Deficiency.

6533b7d2fe1ef96bd125f648

RESEARCH PRODUCT

eNOS Activation by HDL Is Impaired in Genetic CETP Deficiency.

Alice Ossoli Peter M. Nilsson G. Kees Hovingh Monica Gomaraschi Angelo B. Cefalù Fabrizio Veglia Guido Franceschini Jan Albert Kuivenhoven Laura Calabresi Silvia Pozzi Maurizio Averna

subject

Settore MED/09 - Medicina Interna CHOLESTEROL EFFLUX Apolipoprotein B Epidemiology lcsh:Medicine ANTIINFLAMMATORY PROPERTIES medicine.disease_cause Biochemistry Vascular Medicine chemistry.chemical_compound High-density lipoprotein Enos Medicine and Health Sciences Endothelial dysfunction lcsh:Science Mutation Multidisciplinary biology Homozygote CETP; eNOS; HDL;Neurochemistry Lipids Genetic Epidemiology eNOS lipids (amino acids peptides and proteins)Anatomy Neurochemicals Lipoproteins HDL Research Article medicine.medical_specialty Drug Research and Development HDL Nitric Oxide Synthase Type III Lipoproteins ENDOTHELIAL FUNCTION INHIBITION Cardiology Down-Regulation Vascular Cell Adhesion Molecule-1 Nitric Oxide CELL-ADHESION MOLECULE-1 Lipid Metabolism Inborn Errors ESTER TRANSFER PROTEIN Internal medicine CETP Cholesterylester transfer protein Human Umbilical Vein Endothelial Cells medicine Humans NITRIC-OXIDE SYNTHASE Inflammation Clinical Genetics Pharmacology Cholesterol lcsh:R Torcetrapib Endothelial Cells Biology and Life Sciences Proteins nutritional and metabolic diseases Lipid Metabolism Atherosclerosis medicine.disease biology.organism_classification Cholesterol Ester Transfer Proteins carbohydrates (lipids)Metabolism Endocrinology chemistry Other Clinical Medicine Mutation Immunology Cardiovascular Anatomy biology.protein lcsh:Q TORCETRAPIB Clinical Medicine HIGH-DENSITY-LIPOPROTEIN SCAVENGER RECEPTOR BI

description

Mutations in the CETP gene resulting in defective CETP activity have been shown to cause remarkable elevations of plasma HDL-C levels, with the accumulation in plasma of large, buoyant HDL particles enriched in apolipoprotein E. Genetic CETP deficiency thus represents a unique tool to evaluate how structural alterations of HDL impact on HDL atheroprotective functions. Aim of the present study was to assess the ability of HDL obtained from CETP-deficient subjects to protect endothelial cells from the development of endothelial dysfunction. HDL isolated from one homozygous and seven heterozygous carriers of CETP null mutations were evaluated for their ability to down-regulate cytokine-induced cell adhesion molecule expression and to promote NO production in cultured endothelial cells. When compared at the same protein concentration, HDL and HDL3 from carriers proved to be as effective as control HDL and HDL3 in down-regulating cytokine-induced VCAM-1, while carrier HDL2 were more effective than control HDL2 in inhibiting VCAM-1 expression. On the other hand, HDL and HDL fractions from carriers of CETP deficiency were significantly less effective than control HDL and HDL fractions in stimulating NO production, due to a reduced eNOS activating capacity, likely because of a reduced S1P content. In conclusion, the present findings support the notion that genetic CETP deficiency, by affecting HDL particle structure, impacts on HDL vasculoprotective functions. Understanding of these effects might be important for predicting the outcomes of pharmacological CETP inhibition.

year	journal	country	edition	language
2014-05-15

http://lup.lub.lu.se/record/4455124/file/5045851.pdf