Influence of Solvent Evaporation Technique Parameters on Diameter of Submicron Lamivudine-Poly-ε-Caprolactone Conjugate Particles

The size of active pharmaceutical ingredient carrier is one of the key properties considered during design of submicron drug delivery systems. Particle diameter may determine drug biodistribution, cellular uptake, and elimination path. Solvent evaporation technique is a flexible method of particle p...

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Main Authors: Tomasz Urbaniak, Witold Musiał
Format: Article
Language:English
Published: MDPI AG 2019-08-01
Series:Nanomaterials
Subjects:
Online Access:https://www.mdpi.com/2079-4991/9/9/1240
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spelling doaj-40256cd52f354ce19c4c6498656a286a2020-11-25T02:47:44ZengMDPI AGNanomaterials2079-49912019-08-0199124010.3390/nano9091240nano9091240Influence of Solvent Evaporation Technique Parameters on Diameter of Submicron Lamivudine-Poly-ε-Caprolactone Conjugate ParticlesTomasz Urbaniak0Witold Musiał1Department of Physical Chemistry and Biophysics, Pharmaceutical Faculty, Wroclaw Medical University, Borowska 211, 50-556 Wroclaw, PolandDepartment of Physical Chemistry and Biophysics, Pharmaceutical Faculty, Wroclaw Medical University, Borowska 211, 50-556 Wroclaw, PolandThe size of active pharmaceutical ingredient carrier is one of the key properties considered during design of submicron drug delivery systems. Particle diameter may determine drug biodistribution, cellular uptake, and elimination path. Solvent evaporation technique is a flexible method of particle preparation, in which various macromolecules and drugs may be employed. Parameters of emulsion obtained as first step of particle preparation are crucial in terms of particle size, drug loading, and morphology. The aim of the study was to investigate the influence of emulsion preparation parameters on diameter of resulting particles. Impact of surfactant type and concentration, homogenization time, homogenization rate, phase ratio, and conjugate concentration were evaluated. Model drug lamivudine was covalently bound to polymer and applied in solvent evaporation method in order to overcome issues related to drug loading and provide method-independent incorporation. Synthesized drug−polymer conjugate and obtained particles were evaluated via dynamic light scattering, chromatography, scanning electron microscopy, and spectroscopic methods. Covalent bonding between drug and polymeric chain was confirmed, estimated drug content per milligram of conjugate was 19 μg. Among employed colloid stabilizer, poly(vinyl alcohol) was proven to be most effective. Homogenization rate and surfactant concentration were identified as crucial parameters in terms of particle diameter control.https://www.mdpi.com/2079-4991/9/9/1240drug deliverybiodegradable polymersdrug-polymer conjugatessubmicron particle preparationsolvent evaporation technique
collection DOAJ
language English
format Article
sources DOAJ
author Tomasz Urbaniak
Witold Musiał
spellingShingle Tomasz Urbaniak
Witold Musiał
Influence of Solvent Evaporation Technique Parameters on Diameter of Submicron Lamivudine-Poly-ε-Caprolactone Conjugate Particles
Nanomaterials
drug delivery
biodegradable polymers
drug-polymer conjugates
submicron particle preparation
solvent evaporation technique
author_facet Tomasz Urbaniak
Witold Musiał
author_sort Tomasz Urbaniak
title Influence of Solvent Evaporation Technique Parameters on Diameter of Submicron Lamivudine-Poly-ε-Caprolactone Conjugate Particles
title_short Influence of Solvent Evaporation Technique Parameters on Diameter of Submicron Lamivudine-Poly-ε-Caprolactone Conjugate Particles
title_full Influence of Solvent Evaporation Technique Parameters on Diameter of Submicron Lamivudine-Poly-ε-Caprolactone Conjugate Particles
title_fullStr Influence of Solvent Evaporation Technique Parameters on Diameter of Submicron Lamivudine-Poly-ε-Caprolactone Conjugate Particles
title_full_unstemmed Influence of Solvent Evaporation Technique Parameters on Diameter of Submicron Lamivudine-Poly-ε-Caprolactone Conjugate Particles
title_sort influence of solvent evaporation technique parameters on diameter of submicron lamivudine-poly-ε-caprolactone conjugate particles
publisher MDPI AG
series Nanomaterials
issn 2079-4991
publishDate 2019-08-01
description The size of active pharmaceutical ingredient carrier is one of the key properties considered during design of submicron drug delivery systems. Particle diameter may determine drug biodistribution, cellular uptake, and elimination path. Solvent evaporation technique is a flexible method of particle preparation, in which various macromolecules and drugs may be employed. Parameters of emulsion obtained as first step of particle preparation are crucial in terms of particle size, drug loading, and morphology. The aim of the study was to investigate the influence of emulsion preparation parameters on diameter of resulting particles. Impact of surfactant type and concentration, homogenization time, homogenization rate, phase ratio, and conjugate concentration were evaluated. Model drug lamivudine was covalently bound to polymer and applied in solvent evaporation method in order to overcome issues related to drug loading and provide method-independent incorporation. Synthesized drug−polymer conjugate and obtained particles were evaluated via dynamic light scattering, chromatography, scanning electron microscopy, and spectroscopic methods. Covalent bonding between drug and polymeric chain was confirmed, estimated drug content per milligram of conjugate was 19 μg. Among employed colloid stabilizer, poly(vinyl alcohol) was proven to be most effective. Homogenization rate and surfactant concentration were identified as crucial parameters in terms of particle diameter control.
topic drug delivery
biodegradable polymers
drug-polymer conjugates
submicron particle preparation
solvent evaporation technique
url https://www.mdpi.com/2079-4991/9/9/1240
work_keys_str_mv AT tomaszurbaniak influenceofsolventevaporationtechniqueparametersondiameterofsubmicronlamivudinepolyecaprolactoneconjugateparticles
AT witoldmusiał influenceofsolventevaporationtechniqueparametersondiameterofsubmicronlamivudinepolyecaprolactoneconjugateparticles
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