Development of methoxy poly(ethylene glycol)-block-poly(caprolactone) amphiphilic diblock copolymer nanoparticulate formulations for the delivery of paclitaxel

Letchford, Kevin John

11 1900

The goal of this project was to develop a non-toxic amphiphilic diblock copolymer nanoparticulate drug delivery system that will solubilize paclitaxel (PTX) and retain the drug in plasma. Methoxy poly(ethylene glycol)-block-poly(ε-caprolactone) (MePEG-b-PCL) diblock copolymers loaded with PTX were characterized and their physicochemical properties were correlated with their performance as nanoparticulate drug delivery systems. A series of MePEG-b-PCL was synthesized with PCL blocks ranging from 2-104 repeat units and MePEG blocks of 17, 44 or 114 repeat units. All copolymers were water soluble and formed micelles except MePEG₁₁₄-b-PCL₁₀₄, which was water insoluble and formed nanospheres. Investigation of the effects of block length on the physicochemical properties of the nanoparticles was used to select appropriate copolymers for development as PTX nanoparticles. The critical micelle concentration, pyrene partition coefficient and diameter of nanoparticles were found to be dependent on the PCL block length. Copolymers based on a MePEG molecular weight of 750 g/mol were found to have temperature dependent phase behavior. Relationships between the concentration of micellized drug and the compatibility between the drug and core-forming block, as determined by the Flory-Huggins interaction parameter, and PCL block length were developed. Increases in the compatibility between PCL and the drug, as well as longer PCL block lengths resulted in increased drug solubilization. The physicochemical properties and drug delivery performance characteristics of MePEG₁₁₄-b-PCL₁₉ micelles and MePEG₁₁₄-b-PCL₁₀₄ nanospheres were compared. Nanospheres were larger, had a more viscous core, solubilized more PTX and released it slower, compared to micelles. No difference was seen in the hemocompatibility of the nanoparticles as assessed by plasma coagulation time and erythrocyte hemolysis. Micellar PTX had an in vitro plasma distribution similar to free drug. The majority of micellar PTX associated with the lipoprotein deficient plasma fraction (LPDP). In contrast, nanospheres were capable of retaining more of the encapsulated drug with significantly less PTX partitioning into the LPDP fraction. In conclusion, although both micelles and nanospheres were capable of solubilizing PTX and were hemocompatible, PTX nanospheres may offer the advantage of prolonged blood circulation, based on the in vitro plasma distribution data, which showed that nanospheres retained PTX more effectively.

Paclitaxel

Micelle

Nanosphere

Nanoparticle

Hemocompatibility

Solubilization

Plasma distribution

Flory Huggins interaction parameter

Biodegradable polymer

Block copolymer

Development of methoxy poly(ethylene glycol)-block-poly(caprolactone) amphiphilic diblock copolymer nanoparticulate formulations for the delivery of paclitaxel

Letchford, Kevin John

11 1900

The goal of this project was to develop a non-toxic amphiphilic diblock copolymer nanoparticulate drug delivery system that will solubilize paclitaxel (PTX) and retain the drug in plasma. Methoxy poly(ethylene glycol)-block-poly(ε-caprolactone) (MePEG-b-PCL) diblock copolymers loaded with PTX were characterized and their physicochemical properties were correlated with their performance as nanoparticulate drug delivery systems. A series of MePEG-b-PCL was synthesized with PCL blocks ranging from 2-104 repeat units and MePEG blocks of 17, 44 or 114 repeat units. All copolymers were water soluble and formed micelles except MePEG₁₁₄-b-PCL₁₀₄, which was water insoluble and formed nanospheres. Investigation of the effects of block length on the physicochemical properties of the nanoparticles was used to select appropriate copolymers for development as PTX nanoparticles. The critical micelle concentration, pyrene partition coefficient and diameter of nanoparticles were found to be dependent on the PCL block length. Copolymers based on a MePEG molecular weight of 750 g/mol were found to have temperature dependent phase behavior. Relationships between the concentration of micellized drug and the compatibility between the drug and core-forming block, as determined by the Flory-Huggins interaction parameter, and PCL block length were developed. Increases in the compatibility between PCL and the drug, as well as longer PCL block lengths resulted in increased drug solubilization. The physicochemical properties and drug delivery performance characteristics of MePEG₁₁₄-b-PCL₁₉ micelles and MePEG₁₁₄-b-PCL₁₀₄ nanospheres were compared. Nanospheres were larger, had a more viscous core, solubilized more PTX and released it slower, compared to micelles. No difference was seen in the hemocompatibility of the nanoparticles as assessed by plasma coagulation time and erythrocyte hemolysis. Micellar PTX had an in vitro plasma distribution similar to free drug. The majority of micellar PTX associated with the lipoprotein deficient plasma fraction (LPDP). In contrast, nanospheres were capable of retaining more of the encapsulated drug with significantly less PTX partitioning into the LPDP fraction. In conclusion, although both micelles and nanospheres were capable of solubilizing PTX and were hemocompatible, PTX nanospheres may offer the advantage of prolonged blood circulation, based on the in vitro plasma distribution data, which showed that nanospheres retained PTX more effectively.

Paclitaxel

Micelle

Nanosphere

Nanoparticle

Hemocompatibility

Solubilization

Plasma distribution

Flory Huggins interaction parameter

Biodegradable polymer

Block copolymer

Development of methoxy poly(ethylene glycol)-block-poly(caprolactone) amphiphilic diblock copolymer nanoparticulate formulations for the delivery of paclitaxel

Letchford, Kevin John

11 1900

The goal of this project was to develop a non-toxic amphiphilic diblock copolymer nanoparticulate drug delivery system that will solubilize paclitaxel (PTX) and retain the drug in plasma. Methoxy poly(ethylene glycol)-block-poly(ε-caprolactone) (MePEG-b-PCL) diblock copolymers loaded with PTX were characterized and their physicochemical properties were correlated with their performance as nanoparticulate drug delivery systems. A series of MePEG-b-PCL was synthesized with PCL blocks ranging from 2-104 repeat units and MePEG blocks of 17, 44 or 114 repeat units. All copolymers were water soluble and formed micelles except MePEG₁₁₄-b-PCL₁₀₄, which was water insoluble and formed nanospheres. Investigation of the effects of block length on the physicochemical properties of the nanoparticles was used to select appropriate copolymers for development as PTX nanoparticles. The critical micelle concentration, pyrene partition coefficient and diameter of nanoparticles were found to be dependent on the PCL block length. Copolymers based on a MePEG molecular weight of 750 g/mol were found to have temperature dependent phase behavior. Relationships between the concentration of micellized drug and the compatibility between the drug and core-forming block, as determined by the Flory-Huggins interaction parameter, and PCL block length were developed. Increases in the compatibility between PCL and the drug, as well as longer PCL block lengths resulted in increased drug solubilization. The physicochemical properties and drug delivery performance characteristics of MePEG₁₁₄-b-PCL₁₉ micelles and MePEG₁₁₄-b-PCL₁₀₄ nanospheres were compared. Nanospheres were larger, had a more viscous core, solubilized more PTX and released it slower, compared to micelles. No difference was seen in the hemocompatibility of the nanoparticles as assessed by plasma coagulation time and erythrocyte hemolysis. Micellar PTX had an in vitro plasma distribution similar to free drug. The majority of micellar PTX associated with the lipoprotein deficient plasma fraction (LPDP). In contrast, nanospheres were capable of retaining more of the encapsulated drug with significantly less PTX partitioning into the LPDP fraction. In conclusion, although both micelles and nanospheres were capable of solubilizing PTX and were hemocompatible, PTX nanospheres may offer the advantage of prolonged blood circulation, based on the in vitro plasma distribution data, which showed that nanospheres retained PTX more effectively. / Pharmaceutical Sciences, Faculty of / Graduate

Paclitaxel

Micelle

Nanosphere

Nanoparticle

Hemocompatibility

Solubilization

Plasma distribution

Flory Huggins interaction parameter

Biodegradable polymer

Block copolymer

Physico-chimie de méso-tétraphénylporphyrines glycoconjuguées pour la photothérapie dynamique : vers une meilleure compréhension de la distribution plasmatique et de la localisation subcellulaire ? / Physicochemistry of glycoconjugated meso-tetraphenylporphyrins in photodynamic therapy : towards a better understanding of plasma distribution and of subcellular localization ?

Chauvin, Benoît

19 October 2011

La photothérapie dynamique (PDT) consiste en la destruction d’une tumeur par l’association de l’administration d’un photosensibilisateur et de l’exposition à la lumière visible. Ce travail comporte : i) une étude de l’ionisation et de la lipophilie d’une série de photosensibilisateurs, des méso-tétraphénylporphyrines (TPP) glycoconjuguées, ii) une évaluation de l’impact de ces deux propriétés sur la distribution plasmatique et la localisation subcellulaire du photosensibilisateur.La protonation des azotes tétrapyrroliques a été étudiée par spectroscopie électronique, combinéeà une analyse chimiométrique, tandis que la lipophilie a été évaluée par chromatographie liquide haute performance. L’impact de différents effets de substitution (position, nombre ou nature du substituant) sur ces deux propriétés physico-chimiques a été mis en évidence.Dans le plasma, les TPP glycoconjuguées se lient principalement aux lipoprotéines de haute densité. La lipophilie de ces dérivés permet d'expliquer leur affinité pour les lipoprotéines, mais pas pour l'albumine. L’étude de localisation subcellulaire, combinant approche expérimentale et modélisation, a conduit à proposer une hypothèse expliquant la localisation de la TPP(pODEGOαManOH)3 au niveau du réticulum endoplasmique, hypothèse accordant un rôle central à la lipophilie de la TPP . A l'issue de ce travail, avant d'appliquer nos hypothèses à la synthèse de nouvelles molécules, il apparaît nécessaire de mieux explorer l'impact de la distribution plasmatique et de la localisation subcellulaire sur l'efficacité PDT. / Photodynamic Therapy (PDT) is based on the destruction of a tumor tissue through a combinationof administration of a photosensitizer and exposure to visible light. This work includes : i) a study of ionization and hydrophobicity of a series of candidate sensitizers, glycoconjugated mesotetraphenylporphyrins (TPP), ii) an evaluation of the impact of those two physico-chemicalproperties on sensitizer's plasma distribution and subcellular localization. Protonation of tetrapyrrolic nitrogens has been studied by electronic spectroscopy combined with chemometric analysis whereas hydrophobicity has been evaluated by high-performance liquid chromatography. The effect of substitution modalities (position, number and nature of pendantgroups) on both physico-chemical properties has been evidenced.In human plasma, glycoconjugated TPPs mainly bind to high density lipoproteins. Hydrophobicity accounts for differences in affinities towards lipoproteins, but not towards albumin. Subcellular localization studies, combining computational and experimental approaches, led to formulate some assumptions explaining localization of TPP(pODEGOαManOH)3 in endoplasmic reticulum,assumptions centered on a major role of sensitizer's hydrophobicity. At the end of this work, before trying to use our conclusions for the design of new sensitizers, it remains necessary to better explore the effect of plasma distribution and subcellular localization on sensitizer's photo-efficiency.

Photothérapie Dynamique

Méso-tétraphénylporphyrine

Distribution plasmatique

Localisation subcellulaire

Photodynamic therapy

Meso-tetraphenylporphyrin

Ionization

Hydrophobicity

Plasma distribution

Subcellular localization

Chemometrics

Modelling