The Effect of Dextran Sulfate—as Model Glycosaminoglycan Analogue—on Membrane Lipids: DPPC, Cholesterol, and DPPC–Cholesterol Mixture. The Monolayer Study

Glycosaminoglycans (GAGs) are essential components of the extracellular matrices (ECMs) located on the outer surface of cellular membranes. They belong to the group of polysaccharides involved in diverse biological processes acting on the surface and across natural lipid membranes. Recently, particu...

Descripción completa

Detalles Bibliográficos
Autores principales: Makyła-Juzak, Katarzyna, Chachaj-Brekiesz, Anna, Dynarowicz-Latka, Patrycja, Dąbczyński, Paweł, Zemla, Joanna
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Springer US 2018
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6244761/
https://www.ncbi.nlm.nih.gov/pubmed/30030544
http://dx.doi.org/10.1007/s00232-018-0041-z
_version_ 1783372113597431808
author Makyła-Juzak, Katarzyna
Chachaj-Brekiesz, Anna
Dynarowicz-Latka, Patrycja
Dąbczyński, Paweł
Zemla, Joanna
author_facet Makyła-Juzak, Katarzyna
Chachaj-Brekiesz, Anna
Dynarowicz-Latka, Patrycja
Dąbczyński, Paweł
Zemla, Joanna
author_sort Makyła-Juzak, Katarzyna
collection PubMed
description Glycosaminoglycans (GAGs) are essential components of the extracellular matrices (ECMs) located on the outer surface of cellular membranes. They belong to the group of polysaccharides involved in diverse biological processes acting on the surface and across natural lipid membranes. Recently, particular attention has been focused on possible role of GAGs in the amyloid deposits. The amyloid formation is related to a disorder in protein folding, causing that soluble—in normal conditions—peptides become deposited extracellularly as insoluble fibrils, impairing tissue structure and its function. One of the hypothesis holds that GAGs may inhibit amyloid formation by interacting with the lipid membrane by blocking the accumulation of protein aggregates on the membrane surface. Although the biophysical properties of GAGs are described rather well, little is known about the nature of association between these polysaccharides and components of natural cell membranes. Therefore, a study of GAGs influence on membrane lipids is of particular importance. The aim of the present work is to get insight into the effect of hydrophilic dextran sulfate (DS)—that can be considered as GAG analogue—on membrane lipids organization. This study was based on examining interactions between DS sodium salt of molecular weight equal to about 40 kDa (DS40), dissolved in water subphase, and a model membrane, mimicked as Langmuir monolayer, formed by representative natural membrane lipids: cholesterol and 1,2-dipalmitoyl-sn-glycero-3-phosphocholine (DPPC) as well as their mixtures. Due to the fact that calcium ions in excess may accumulate in the lipid membrane, attracting high molecular weight molecules to their surface, the influence of calcium ions present in the subphase on the DS40 activity has also been examined. It has been found that negatively charged DS, forming a sublayer underneath the monolayer, barely interacts with membrane lipids; however, in the presence of calcium ions the electrostatic interactions between DS40 and lipid membrane are significantly enhanced, leading to the formation of network-like crystalline structures at the surface of model membrane, which can prevent incorporation and interaction with other extracellular molecules, e.g., proteins.
format Online
Article
Text
id pubmed-6244761
institution National Center for Biotechnology Information
language English
publishDate 2018
publisher Springer US
record_format MEDLINE/PubMed
spelling pubmed-62447612018-12-04 The Effect of Dextran Sulfate—as Model Glycosaminoglycan Analogue—on Membrane Lipids: DPPC, Cholesterol, and DPPC–Cholesterol Mixture. The Monolayer Study Makyła-Juzak, Katarzyna Chachaj-Brekiesz, Anna Dynarowicz-Latka, Patrycja Dąbczyński, Paweł Zemla, Joanna J Membr Biol Article Glycosaminoglycans (GAGs) are essential components of the extracellular matrices (ECMs) located on the outer surface of cellular membranes. They belong to the group of polysaccharides involved in diverse biological processes acting on the surface and across natural lipid membranes. Recently, particular attention has been focused on possible role of GAGs in the amyloid deposits. The amyloid formation is related to a disorder in protein folding, causing that soluble—in normal conditions—peptides become deposited extracellularly as insoluble fibrils, impairing tissue structure and its function. One of the hypothesis holds that GAGs may inhibit amyloid formation by interacting with the lipid membrane by blocking the accumulation of protein aggregates on the membrane surface. Although the biophysical properties of GAGs are described rather well, little is known about the nature of association between these polysaccharides and components of natural cell membranes. Therefore, a study of GAGs influence on membrane lipids is of particular importance. The aim of the present work is to get insight into the effect of hydrophilic dextran sulfate (DS)—that can be considered as GAG analogue—on membrane lipids organization. This study was based on examining interactions between DS sodium salt of molecular weight equal to about 40 kDa (DS40), dissolved in water subphase, and a model membrane, mimicked as Langmuir monolayer, formed by representative natural membrane lipids: cholesterol and 1,2-dipalmitoyl-sn-glycero-3-phosphocholine (DPPC) as well as their mixtures. Due to the fact that calcium ions in excess may accumulate in the lipid membrane, attracting high molecular weight molecules to their surface, the influence of calcium ions present in the subphase on the DS40 activity has also been examined. It has been found that negatively charged DS, forming a sublayer underneath the monolayer, barely interacts with membrane lipids; however, in the presence of calcium ions the electrostatic interactions between DS40 and lipid membrane are significantly enhanced, leading to the formation of network-like crystalline structures at the surface of model membrane, which can prevent incorporation and interaction with other extracellular molecules, e.g., proteins. Springer US 2018-07-20 2018 /pmc/articles/PMC6244761/ /pubmed/30030544 http://dx.doi.org/10.1007/s00232-018-0041-z Text en © The Author(s) 2018 Open AccessThis article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made.
spellingShingle Article
Makyła-Juzak, Katarzyna
Chachaj-Brekiesz, Anna
Dynarowicz-Latka, Patrycja
Dąbczyński, Paweł
Zemla, Joanna
The Effect of Dextran Sulfate—as Model Glycosaminoglycan Analogue—on Membrane Lipids: DPPC, Cholesterol, and DPPC–Cholesterol Mixture. The Monolayer Study
title The Effect of Dextran Sulfate—as Model Glycosaminoglycan Analogue—on Membrane Lipids: DPPC, Cholesterol, and DPPC–Cholesterol Mixture. The Monolayer Study
title_full The Effect of Dextran Sulfate—as Model Glycosaminoglycan Analogue—on Membrane Lipids: DPPC, Cholesterol, and DPPC–Cholesterol Mixture. The Monolayer Study
title_fullStr The Effect of Dextran Sulfate—as Model Glycosaminoglycan Analogue—on Membrane Lipids: DPPC, Cholesterol, and DPPC–Cholesterol Mixture. The Monolayer Study
title_full_unstemmed The Effect of Dextran Sulfate—as Model Glycosaminoglycan Analogue—on Membrane Lipids: DPPC, Cholesterol, and DPPC–Cholesterol Mixture. The Monolayer Study
title_short The Effect of Dextran Sulfate—as Model Glycosaminoglycan Analogue—on Membrane Lipids: DPPC, Cholesterol, and DPPC–Cholesterol Mixture. The Monolayer Study
title_sort effect of dextran sulfate—as model glycosaminoglycan analogue—on membrane lipids: dppc, cholesterol, and dppc–cholesterol mixture. the monolayer study
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6244761/
https://www.ncbi.nlm.nih.gov/pubmed/30030544
http://dx.doi.org/10.1007/s00232-018-0041-z
work_keys_str_mv AT makyłajuzakkatarzyna theeffectofdextransulfateasmodelglycosaminoglycananalogueonmembranelipidsdppccholesterolanddppccholesterolmixturethemonolayerstudy
AT chachajbrekieszanna theeffectofdextransulfateasmodelglycosaminoglycananalogueonmembranelipidsdppccholesterolanddppccholesterolmixturethemonolayerstudy
AT dynarowiczlatkapatrycja theeffectofdextransulfateasmodelglycosaminoglycananalogueonmembranelipidsdppccholesterolanddppccholesterolmixturethemonolayerstudy
AT dabczynskipaweł theeffectofdextransulfateasmodelglycosaminoglycananalogueonmembranelipidsdppccholesterolanddppccholesterolmixturethemonolayerstudy
AT zemlajoanna theeffectofdextransulfateasmodelglycosaminoglycananalogueonmembranelipidsdppccholesterolanddppccholesterolmixturethemonolayerstudy
AT makyłajuzakkatarzyna effectofdextransulfateasmodelglycosaminoglycananalogueonmembranelipidsdppccholesterolanddppccholesterolmixturethemonolayerstudy
AT chachajbrekieszanna effectofdextransulfateasmodelglycosaminoglycananalogueonmembranelipidsdppccholesterolanddppccholesterolmixturethemonolayerstudy
AT dynarowiczlatkapatrycja effectofdextransulfateasmodelglycosaminoglycananalogueonmembranelipidsdppccholesterolanddppccholesterolmixturethemonolayerstudy
AT dabczynskipaweł effectofdextransulfateasmodelglycosaminoglycananalogueonmembranelipidsdppccholesterolanddppccholesterolmixturethemonolayerstudy
AT zemlajoanna effectofdextransulfateasmodelglycosaminoglycananalogueonmembranelipidsdppccholesterolanddppccholesterolmixturethemonolayerstudy

Ejemplares similares