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ApoA-I-Mediated Lipoprotein Remodeling Monitored with a Fluorescent Phospholipid

We describe simple, sensitive and robust methods to monitor lipoprotein remodeling and cholesterol and apolipoprotein exchange, using fluorescent Lissamine Rhodamine B head-group tagged phosphatidylethanolamine (*PE) as a lipoprotein reference marker. Fluorescent Bodipy cholesterol (*Chol) and *PE d...

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Autores principales: Neufeld, Edward B., Sato, Masaki, Gordon, Scott M., Durbhakula, Vinay, Francone, Nicolas, Aponte, Angel, Yilmaz, Gizem, Sviridov, Denis, Sampson, Maureen, Tang, Jingrong, Pryor, Milton, Remaley, Alan T.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2019
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6784057/
https://www.ncbi.nlm.nih.gov/pubmed/31336888
http://dx.doi.org/10.3390/biology8030053
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author Neufeld, Edward B.
Sato, Masaki
Gordon, Scott M.
Durbhakula, Vinay
Francone, Nicolas
Aponte, Angel
Yilmaz, Gizem
Sviridov, Denis
Sampson, Maureen
Tang, Jingrong
Pryor, Milton
Remaley, Alan T.
author_facet Neufeld, Edward B.
Sato, Masaki
Gordon, Scott M.
Durbhakula, Vinay
Francone, Nicolas
Aponte, Angel
Yilmaz, Gizem
Sviridov, Denis
Sampson, Maureen
Tang, Jingrong
Pryor, Milton
Remaley, Alan T.
author_sort Neufeld, Edward B.
collection PubMed
description We describe simple, sensitive and robust methods to monitor lipoprotein remodeling and cholesterol and apolipoprotein exchange, using fluorescent Lissamine Rhodamine B head-group tagged phosphatidylethanolamine (*PE) as a lipoprotein reference marker. Fluorescent Bodipy cholesterol (*Chol) and *PE directly incorporated into whole plasma lipoproteins in proportion to lipoprotein cholesterol and phospholipid mass, respectively. *Chol, but not *PE, passively exchanged between isolated plasma lipoproteins. Fluorescent apoA-I (*apoA-I) specifically bound to high-density lipoprotein (HDL) and remodeled *PE- and *Chol-labeled synthetic lipoprotein-X multilamellar vesicles (MLV) into a pre-β HDL-like particle containing *PE, *Chol, and *apoA-I. Fluorescent MLV-derived *PE specifically incorporated into plasma HDL, whereas MLV-derived *Chol incorporation into plasma lipoproteins was similar to direct *Chol incorporation, consistent with apoA-I-mediated remodeling of fluorescent MLV to HDL with concomitant exchange of *Chol between lipoproteins. Based on these findings, we developed a model system to study lipid transfer by depositing fluorescent *PE and *Chol-labeled on calcium silicate hydrate crystals, forming dense lipid-coated donor particles that are readily separated from acceptor lipoprotein particles by low-speed centrifugation. Transfer of *PE from donor particles to mouse plasma lipoproteins was shown to be HDL-specific and apoA-I-dependent. Transfer of donor particle *PE and *Chol to HDL in whole human plasma was highly correlated. Taken together, these studies suggest that cell-free *PE efflux monitors apoA-I functionality.
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spelling pubmed-67840572019-10-16 ApoA-I-Mediated Lipoprotein Remodeling Monitored with a Fluorescent Phospholipid Neufeld, Edward B. Sato, Masaki Gordon, Scott M. Durbhakula, Vinay Francone, Nicolas Aponte, Angel Yilmaz, Gizem Sviridov, Denis Sampson, Maureen Tang, Jingrong Pryor, Milton Remaley, Alan T. Biology (Basel) Article We describe simple, sensitive and robust methods to monitor lipoprotein remodeling and cholesterol and apolipoprotein exchange, using fluorescent Lissamine Rhodamine B head-group tagged phosphatidylethanolamine (*PE) as a lipoprotein reference marker. Fluorescent Bodipy cholesterol (*Chol) and *PE directly incorporated into whole plasma lipoproteins in proportion to lipoprotein cholesterol and phospholipid mass, respectively. *Chol, but not *PE, passively exchanged between isolated plasma lipoproteins. Fluorescent apoA-I (*apoA-I) specifically bound to high-density lipoprotein (HDL) and remodeled *PE- and *Chol-labeled synthetic lipoprotein-X multilamellar vesicles (MLV) into a pre-β HDL-like particle containing *PE, *Chol, and *apoA-I. Fluorescent MLV-derived *PE specifically incorporated into plasma HDL, whereas MLV-derived *Chol incorporation into plasma lipoproteins was similar to direct *Chol incorporation, consistent with apoA-I-mediated remodeling of fluorescent MLV to HDL with concomitant exchange of *Chol between lipoproteins. Based on these findings, we developed a model system to study lipid transfer by depositing fluorescent *PE and *Chol-labeled on calcium silicate hydrate crystals, forming dense lipid-coated donor particles that are readily separated from acceptor lipoprotein particles by low-speed centrifugation. Transfer of *PE from donor particles to mouse plasma lipoproteins was shown to be HDL-specific and apoA-I-dependent. Transfer of donor particle *PE and *Chol to HDL in whole human plasma was highly correlated. Taken together, these studies suggest that cell-free *PE efflux monitors apoA-I functionality. MDPI 2019-07-12 /pmc/articles/PMC6784057/ /pubmed/31336888 http://dx.doi.org/10.3390/biology8030053 Text en © 2019 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Neufeld, Edward B.
Sato, Masaki
Gordon, Scott M.
Durbhakula, Vinay
Francone, Nicolas
Aponte, Angel
Yilmaz, Gizem
Sviridov, Denis
Sampson, Maureen
Tang, Jingrong
Pryor, Milton
Remaley, Alan T.
ApoA-I-Mediated Lipoprotein Remodeling Monitored with a Fluorescent Phospholipid
title ApoA-I-Mediated Lipoprotein Remodeling Monitored with a Fluorescent Phospholipid
title_full ApoA-I-Mediated Lipoprotein Remodeling Monitored with a Fluorescent Phospholipid
title_fullStr ApoA-I-Mediated Lipoprotein Remodeling Monitored with a Fluorescent Phospholipid
title_full_unstemmed ApoA-I-Mediated Lipoprotein Remodeling Monitored with a Fluorescent Phospholipid
title_short ApoA-I-Mediated Lipoprotein Remodeling Monitored with a Fluorescent Phospholipid
title_sort apoa-i-mediated lipoprotein remodeling monitored with a fluorescent phospholipid
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6784057/
https://www.ncbi.nlm.nih.gov/pubmed/31336888
http://dx.doi.org/10.3390/biology8030053
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