Human LDL Structural Diversity Studied by IR Spectroscopy
View/ Open
Date
2014-03-18Author
Fernández Higuero, José Ángel
Salvador, Ana M.
Martín Plágaro, César Augusto
González Milicua, José Carlos
Rodríguez Arrondo, José Luis
Metadata
Show full item record
PLOS ONE 9(3) : (2014) // Article ID e92426
Abstract
Lipoproteins are responsible for cholesterol traffic in humans. Low density lipoprotein (LDL) delivers cholesterol from liver to peripheral tissues. A misleading delivery can lead to the formation of atherosclerotic plaques. LDL has a single protein, apoB-100, that binds to a specific receptor. It is known that the failure associated with a deficient protein-receptor binding leads to plaque formation. ApoB-100 is a large single lipid-associated polypeptide difficulting the study of its structure. IR spectroscopy is a technique suitable to follow the different conformational changes produced in apoB-100 because it is not affected by the size of the protein or the turbidity of the sample. We have analyzed LDL spectra of different individuals and shown that, even if there are not big structural changes, a different pattern in the intensity of the band located around 1617 cm 21 related with strands embedded in the lipid monolayer, can be associated with a different conformational rearrangement that could affect to a protein interacting region with the receptor.