In vitro model using biotinylated human HDL(2) and HDL(3), and wild-type human and mouse apolipoprotein A-I (apoA-I)
Surface plasmon resonance (SPR) analysis and fluorescence experiments with pyrene-labeled apoA-I
Mechanism and kinetics of apoA-I binding to HDL particles (association/dissociation rates, dissociation constants)surrogate
The study demonstrates that apoA-I binds to HDL via a two-step process involving the N-terminal helix bundle domain, with a low-affinity interaction for a labile pool of apoA-I molecules.
The partitioning of apolipoprotein A-I (apoA-I) molecules in plasma between HDL-bound and -unbound states is an integral part of HDL metabolism. We used the surface plasmon resonance (SPR) technique to monitor in real time the reversible binding of apoA-I to HDL. Biotinylated human HDL(2) and HDL(3) were immobilized on a streptavidin-coated SPR sensor chip, and apoA-I solutions at different concentrations were flowed across the surface. The wild-type (WT) human and mouse apoA-I/HDL interaction involves a two-step process; apoA-I initially binds to HDL with fast association and dissociation rates, followed by a step exhibiting slower kinetics. The isolated N-terminal helix bundle domains of human and mouse apoA-I also exhibit a two-step binding process, consistent with the second slower step involving opening of the helix bundle domain. The results of fluorescence experiments with pyrene-labeled apoA-I are consistent with the N-terminal helix bundle domain interacting with proteins resident on the HDL particle surface. Dissociation constants (K(d)) measured for WT human apoA-I interactions with HDL(2) and HDL(3) are about 10 microM, indicating that the binding is low affinity. This K(d) value does not apply to all of the apoA-I molecules on the HDL particle but only to a relatively small, labile pool.
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Sissel Lund‐Katz
David Nguyen
Padmaja Dhanasekaran
Journal of Lipid Research
SHILAP Revista de lepidopterología
University of Pennsylvania
Children's Hospital of Philadelphia
Kobe Pharmaceutical University
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Lund‐Katz et al. (Tue,) studied this question.
www.synapsesocial.com/papers/69e63ea47051b84d08e707ae — DOI: https://doi.org/10.1194/jlr.m002055