Fate of Liposomes in the Presence of Phospholipase C and D: From Atomic to Supramolecular Lipid Arrangement

[Image: see text] Understanding the origins of lipid membrane bilayer rearrangement in response to external stimuli is an essential component of cell biology and the bottom-up design of liposomes for biomedical applications. The enzymes phospholipase C and D (PLC and PLD) both cleave the phosphorus–...

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Autores principales: Holme, Margaret N., Rashid, M. Harunur, Thomas, Michael R., Barriga, Hanna M. G., Herpoldt, Karla−Luise, Heenan, Richard K., Dreiss, Cécile A., Bañuelos, José Leobardo, Xie, Hai-nan, Yarovsky, Irene, Stevens, Molly M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Chemical Society 2018
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6107861/
https://www.ncbi.nlm.nih.gov/pubmed/30159399
http://dx.doi.org/10.1021/acscentsci.8b00286
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author Holme, Margaret N.
Rashid, M. Harunur
Thomas, Michael R.
Barriga, Hanna M. G.
Herpoldt, Karla−Luise
Heenan, Richard K.
Dreiss, Cécile A.
Bañuelos, José Leobardo
Xie, Hai-nan
Yarovsky, Irene
Stevens, Molly M.
author_facet Holme, Margaret N.
Rashid, M. Harunur
Thomas, Michael R.
Barriga, Hanna M. G.
Herpoldt, Karla−Luise
Heenan, Richard K.
Dreiss, Cécile A.
Bañuelos, José Leobardo
Xie, Hai-nan
Yarovsky, Irene
Stevens, Molly M.
author_sort Holme, Margaret N.
collection PubMed
description [Image: see text] Understanding the origins of lipid membrane bilayer rearrangement in response to external stimuli is an essential component of cell biology and the bottom-up design of liposomes for biomedical applications. The enzymes phospholipase C and D (PLC and PLD) both cleave the phosphorus–oxygen bonds of phosphate esters in phosphatidylcholine (PC) lipids. The atomic position of this hydrolysis reaction has huge implications for the stability of PC-containing self-assembled structures, such as the cell wall and lipid-based vesicle drug delivery vectors. While PLC converts PC to diacylglycerol (DAG), the interaction of PC with PLD produces phosphatidic acid (PA). Here we present a combination of small-angle scattering data and all-atom molecular dynamics simulations, providing insights into the effects of atomic-scale reorganization on the supramolecular assembly of PC membrane bilayers upon enzyme-mediated incorporation of DAG or PA. We observed that PC liposomes completely disintegrate in the presence of PLC, as conversion of PC to DAG progresses. At lower concentrations, DAG molecules within fluid PC bilayers form hydrogen bonds with backbone carbonyl oxygens in neighboring PC molecules and burrow into the hydrophobic region. This leads initially to membrane thinning followed by a swelling of the lamellar phase with increased DAG. At higher DAG concentrations, localized membrane tension causes a change in lipid phase from lamellar to the hexagonal and micellar cubic phases. Molecular dynamics simulations show that this destabilization is also caused in part by the decreased ability of DAG-containing PC membranes to coordinate sodium ions. Conversely, PLD-treated PC liposomes remain stable up to extremely high conversions to PA. Here, the negatively charged PA headgroup attracts significant amounts of sodium ions from the bulk solution to the membrane surface, leading to a swelling of the coordinated water layer. These findings are a vital step toward a fundamental understanding of the degradation behavior of PC lipid membranes in the presence of these clinically relevant enzymes, and toward the rational design of diagnostic and drug delivery technologies for phospholipase-dysregulation-based diseases.
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spelling pubmed-61078612018-08-29 Fate of Liposomes in the Presence of Phospholipase C and D: From Atomic to Supramolecular Lipid Arrangement Holme, Margaret N. Rashid, M. Harunur Thomas, Michael R. Barriga, Hanna M. G. Herpoldt, Karla−Luise Heenan, Richard K. Dreiss, Cécile A. Bañuelos, José Leobardo Xie, Hai-nan Yarovsky, Irene Stevens, Molly M. ACS Cent Sci [Image: see text] Understanding the origins of lipid membrane bilayer rearrangement in response to external stimuli is an essential component of cell biology and the bottom-up design of liposomes for biomedical applications. The enzymes phospholipase C and D (PLC and PLD) both cleave the phosphorus–oxygen bonds of phosphate esters in phosphatidylcholine (PC) lipids. The atomic position of this hydrolysis reaction has huge implications for the stability of PC-containing self-assembled structures, such as the cell wall and lipid-based vesicle drug delivery vectors. While PLC converts PC to diacylglycerol (DAG), the interaction of PC with PLD produces phosphatidic acid (PA). Here we present a combination of small-angle scattering data and all-atom molecular dynamics simulations, providing insights into the effects of atomic-scale reorganization on the supramolecular assembly of PC membrane bilayers upon enzyme-mediated incorporation of DAG or PA. We observed that PC liposomes completely disintegrate in the presence of PLC, as conversion of PC to DAG progresses. At lower concentrations, DAG molecules within fluid PC bilayers form hydrogen bonds with backbone carbonyl oxygens in neighboring PC molecules and burrow into the hydrophobic region. This leads initially to membrane thinning followed by a swelling of the lamellar phase with increased DAG. At higher DAG concentrations, localized membrane tension causes a change in lipid phase from lamellar to the hexagonal and micellar cubic phases. Molecular dynamics simulations show that this destabilization is also caused in part by the decreased ability of DAG-containing PC membranes to coordinate sodium ions. Conversely, PLD-treated PC liposomes remain stable up to extremely high conversions to PA. Here, the negatively charged PA headgroup attracts significant amounts of sodium ions from the bulk solution to the membrane surface, leading to a swelling of the coordinated water layer. These findings are a vital step toward a fundamental understanding of the degradation behavior of PC lipid membranes in the presence of these clinically relevant enzymes, and toward the rational design of diagnostic and drug delivery technologies for phospholipase-dysregulation-based diseases. American Chemical Society 2018-08-06 2018-08-22 /pmc/articles/PMC6107861/ /pubmed/30159399 http://dx.doi.org/10.1021/acscentsci.8b00286 Text en Copyright © 2018 American Chemical Society This is an open access article published under a Creative Commons Attribution (CC-BY) License (http://pubs.acs.org/page/policy/authorchoice_ccby_termsofuse.html) , which permits unrestricted use, distribution and reproduction in any medium, provided the author and source are cited.
spellingShingle Holme, Margaret N.
Rashid, M. Harunur
Thomas, Michael R.
Barriga, Hanna M. G.
Herpoldt, Karla−Luise
Heenan, Richard K.
Dreiss, Cécile A.
Bañuelos, José Leobardo
Xie, Hai-nan
Yarovsky, Irene
Stevens, Molly M.
Fate of Liposomes in the Presence of Phospholipase C and D: From Atomic to Supramolecular Lipid Arrangement
title Fate of Liposomes in the Presence of Phospholipase C and D: From Atomic to Supramolecular Lipid Arrangement
title_full Fate of Liposomes in the Presence of Phospholipase C and D: From Atomic to Supramolecular Lipid Arrangement
title_fullStr Fate of Liposomes in the Presence of Phospholipase C and D: From Atomic to Supramolecular Lipid Arrangement
title_full_unstemmed Fate of Liposomes in the Presence of Phospholipase C and D: From Atomic to Supramolecular Lipid Arrangement
title_short Fate of Liposomes in the Presence of Phospholipase C and D: From Atomic to Supramolecular Lipid Arrangement
title_sort fate of liposomes in the presence of phospholipase c and d: from atomic to supramolecular lipid arrangement
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6107861/
https://www.ncbi.nlm.nih.gov/pubmed/30159399
http://dx.doi.org/10.1021/acscentsci.8b00286
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