Mechanical properties of drug loaded diblock copolymer bilayers: A molecular dynamics study

In this work, we present results of coarse-grained simulations to study the encapsulation of prilocaine (PLC), both neutral and protonated, on copolymer bilayers through molecular dynamics simulations. Using a previously validated membrane model, we have simulated loaded bilayers at different drug c...

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Veröffentlicht in:The Journal of chemical physics 2018-06, Vol.148 (21), p.214901-214901
Hauptverfasser: Grillo, Damián A., Albano, Juan M. R., Mocskos, Esteban E., Facelli, Julio C., Pickholz, Mónica, Ferraro, Marta B.
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Sprache:eng
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Zusammenfassung:In this work, we present results of coarse-grained simulations to study the encapsulation of prilocaine (PLC), both neutral and protonated, on copolymer bilayers through molecular dynamics simulations. Using a previously validated membrane model, we have simulated loaded bilayers at different drug concentrations and at low (protonated PLC) and high (neutral PLC) pH levels. We have characterized key structural parameters of the loaded bilayers in order to understand the effects of encapsulation of PLC on the bilayer structure and mechanical properties. Neutral PLC was encapsulated in the hydrophobic region leading to a thickness increase, while the protonated species partitioned between the water phase and the poly(ethylene oxide)-poly(butadiene) (PBD) interface, relaxing the PBD region and leading to a decrease in the thickness. The tangential pressures of the studied systems were calculated, and their components were decomposed in order to gain insights on their compensation. In all cases, it is observed that the loading of the membrane does not significantly decrease the stability of the bilayer, indicating that the system could be used for drug delivery.
ISSN:0021-9606
1089-7690
DOI:10.1063/1.5028377