Use of casein micelles to improve the solubility of hydrophobic pea proteins in aqueous solutions via low-temperature homogenization

Krentz, Abigail L.

January 2021

No description available.

Food Science

casein micelle

pea protein

homogenization

colloidal dispersion

Rational and precise design of polymeric nanoparticles for tumor imaging and internal radiation therapy / 腫瘍イメージングと内部照射療法に向けたポリマーナノ粒子の最適化

Hara, Eri

23 March 2015

京都大学 / 0048 / 新制・論文博士 / 博士(工学) / 乙第12923号 / 論工博第4116号 / 新制||工||1625(附属図書館) / 32133 / (主査)教授 木村 俊作, 教授 跡見 晴幸, 教授 岩田 博夫 / 学位規則第4条第2項該当 / Doctor of Philosophy (Engineering) / Kyoto University / DFAM

nanoparticle

polymeric micelle

ABC phenomenon

immune response

radionuclide therapy

500

Aggregation behavior of Pluronic P123 in bulk solution and under confinement at elevated temperatures near its cloud point / Aggregationsverhalten von Pluronic P123 in Lösung und an Grenzflächen bei hohen Temperaturen nahe des Trübungspunktes

Sochor, Benedikt

January 2021

This thesis aims to investigate the form-phase diagram of aqueous solutions of the triblock copolymer Pluronic P123 focusing on its high-temperature phases. P123 is based on polyethylene as well as polypropylene oxide blocks and shows a variety of di erent temperaturedependent micelle morphologies or even lyotropic liquid crystal phases in aqueous solutions. Besides the already well-studied spherical aggregates at intermediate temperatures, the size and internal structure of both worm-like and lamellar micelles, which appear near the cloud point, is determined using light, neutron and X-ray scattering. By combining the results of time-resolved dynamic light as well as small-angle neutron and X-ray scattering experiments, the underlying structural changes and kinetics of the sphere-to-worm transition were studied supporting the random fusion process, which is proposed in literature. For temperatures near the cloud point, it was observed that aqueous P123 solutions below the critical crystallization concentration gelate after several hours, which is linked to the presence and structure of polymeric surface layers on the sample container walls as shown by neutron re ectometry measurements. Using a hierarchical model for the lamellar micelles including their periodicity as well as domain and overall size, it is possible to unify the existing results in literature and propose a direct connection between the near-surface and bulk properties of P123 solutions at temperatures near the cloud point. / Ziel dieser Dissertation ist die Untersuchung des Form-Phasendiagrams des Dreiblock-Co- polymers Pluronic P123 mit dem besonderen Fokus auf dessen Phasenverhalten bei hohen Temperaturen. P123 besteht aus Polyethylen- und Polypropylenoxid-Blöcken und zeigt in wässriger Lösung vielfältige, temperaturabhängige Mizellformen oder sogar Flüssigkristallphasen. Neben den bereits intensiv untersuchten sphärischen Aggregaten bei mittleren Temperaturen, werden die Größen und inneren Strukturen der wurmartigen und lamellearen Aggregate mittels Licht-, Neutronen- und Röntgenstreumethoden untersucht, welche nahe des Trübungspunktes der Lösungen auftreten. Durch die Kombination von zeitaufgelösten dynamischen Licht- und Kleinwinkelstreuung-Experimenten wurden die strukturellen Änderungen und kinetischen Prozesse während des Kugel-Wurm-Übergangs untersucht, welche den bereits in der Literatur vorgeschlagenen zufälligen Fusionsprozess weiter bestätigen. Es wurde beobachtet, dass wässrige P123-Lösungen unterhalb der kritischen Kristallisationskonzentration nach mehreren Stunden gelieren, was durch Neutronenreflektometrie mit dem Auftreten und der Struktur von oberflächennahen Monolagen auf den Messzellwänden in Verbindung gebracht wurde. Wenn ein hierarchisches Model für die lamellaren Mizellen verwendet wird, das deren Periodizität, Domänen- und Gesamtgröße berücksichtigt, ist es außerdem möglich, die bisherigen Ergebnisse in der Literatur zu vereinigen und eine direkte Verbindung zwischen dem Aggregationsverhalten von P123 auf Oberflächen und in Lösung bei Temperaturen nahe des Trübungspunktes zu ziehen.

Weiche Materie

Polymerlösung

Micelle

Röntgenstreuung

Neutronenstreuung

ddc:530

Construction of the Novel Core/interfacial Crosslinked Inorganic/organic Hybrid Micelle Based on Functionalized Polyhedral Oligomeric Silsesquioxane (POSS) via Thiol-ene "Click" Chemistry

Chen, Ziran

06 June 2013

No description available.

Polymer Chemistry

Polymers

Crosslinked Micelle

POSS

click chemistry

Stable Polymer Micelle Systems as Anti-cancer Drug Delivery Carriers

Zeng, Yi

01 June 2005

Several temporarily stable polymer micelle systems that might be used as ultrasonic-activated drug delivery carriers were synthesized and investigated. These polymeric micelle systems were Plurogel®, Tetronic®, poly(ethylene oxide)-b-poly(N-isopropylacrylamide) and poly(ethylene oxide)-b-poly(N-isopropylacrylamide-co-2-hydroxyethyl methacrylate-lactaten). In previous work in our lab, Pruitt et al. developed a stabilized drug carrier named Plurogel® [5, 6]. Unfortunately, the rate of the successful Plurogel® synthesis was only about 30% by simply following Pruitt's process. In this work, this rate was improved to 60% by combining the process of adding 0.15 M NaCl and/or 10 µl/ml n-butanol and by preheating the solution before polymerization. Tetronics® were proved not to be good candidates to form temporarily stable polymeric micelle system by polymerizing interpenetrating networks inside their micelle cores. Tetronic micelle systems treated by this process still were not stable at concentrations below their critical micelle concentration (CMC). Poly(ethylene oxide)-b-poly(N-isopropylacrylamide)-N,N-bis(acryloyl)cystamine micelle-like nanoparticles were developed and characterized. When the N,N-bis(acryloyl)cystamine (BAC) was from 0.2 wt% to 0.75 wt% of the mass of poly(N-isopropylacrylamide), diameters of the nanoparticles at 40ºC were less than 150 nm. The cores of the nanoparticles were hydrophobic enough to sequester 1,6-diphenylhexatriene (DPH) and the anti-cancer drug doxorubicin (DOX). Nanoparticles with 0.5 wt% BAC stored at room temperature in 0.002 mg/ml solutions were stable for up to two weeks. Poly(ethylene oxide)-b-poly(N-isopropylacrylamide-co-2-hydroxyethyl methacrylate-lactaten) micelle systems were synthesized and characterized. The degree of polymerization of lactate side group, n, was 3 or 5. The copolymers with N-isopropylacrylamide:2-hydroxyethyl methacrylate-lactate3: poly(ethylene oxide) (NIPAAm:HEMA-lactate3:PEO) ratios of 20.0:5.0:1 or 22.5:2.5:1 and with NIPAAm:HEMA-lactate5:PEO ratios of 17.5:7.5:1, 20.0:5.0:1 or 22.5:2.5:1 produced micelles stable about 2 days at 40°C. The cores of the micelles were hydrophobic enough to sequester DPH and DOX. The DOX release from the micelles having molar ratio of NIPAAm:HEMA-lactate3:PEO equal to 20.0:5.0:1 was about 2 % at room temperature and 4 % at body temperature. This system is a possible candidate for ultrasonically activated drug delivery.

polymer micelle

drug delivery

anti-cancer

Chemical Engineering

Investigating the Effect of a Micelle-Based Drug Delivery System in Reducing IOP and Glaucomatous Effects in a Partially Open Angle Mouse Model of Glaucoma

Shirazee, Fatima

January 2023

This project explores the use of a novel sustained release mucoadhesive micelle-based drug delivery system in combination with 0.005% latanoprost (LTP) on our partially open angle mouse model of glaucoma (AP-2β TMR-KO). We previously tested for LTP treatment in our model and found a reduction in intraocular pressure (IOP) 20 minutes following treatment. This information led us to investigate the long-term effect of LTP treatment and micelle loaded with LTP (MLTP) treatment in our model. We hypothesized that the MLTP treatment would be more effective in reducing IOP and preventing glaucomatous effects than LTP treatment alone in the AP-2β TMR-KO mice. The MLTP groups of animals (wildtype and mutant) were treated every 3 days, and this was compared with animals treated with LTP daily as well as animals treated every 3 days with LTP alone for comparison’s sake for 60 days. IOP measurements were taken every 3 days. Following long term LTP treatment alone, mutant mice showed a consistent decrease in their baseline IOPs with a significant reduction in baseline IOP at 35 days of treatment across all cohorts (P<0.0001). In comparison, mutants treated with MLTP exhibited an even greater reduction in baseline IOP following long term treatment. After the treatment period, mice were euthanized, and their eyes were enucleated, fixed, sectioned, and stained for retinal ganglion cells (RGCs) using Brn3a. Mutant mice exhibited a significant decrease in RGC cell number when compared to wildtype, and this loss was not rescued by treatment with LTP. However, mutants treated with MLTP demonstrated significant RGC cell protection compared to eyes of untreated mutants, as well as everyday LTP treated mutants. / Thesis / Master of Science (MSc) / An effective treatment strategy is required to prevent irreversible blindness caused from glaucoma. Unfortunately, compliance with current medications is extremely poor, as they require frequent administration due to their low ocular bioavailability and short-term effect. As such, this thesis aims to explore an alternative drug delivery approach in a partially open angle mouse model of glaucoma to prevent the worsening of glaucoma and ultimately improve patient compliance.

Drug Delivery

Glaucoma

Micelle

Intraocular Pressure

Latanoprost

Retinal Ganglion Cells

Synthesis, Characterization, and Micellar Properties of Dendritic Amphiphiles

Macri, Richard Vincent

15 June 2009

Two new homologous series of amphiphiles–five long-chain, three-headed amphiphiles [3CCb14, 3CCb16, 3CCb18, 3CCb20, 3CCb22; CH3(CH2)n-1OCONHC(CH2CH2COOH)3, n = 14, 16, 18, 20, 22], and six branched-chain, three-headed amphiphiles [3CCb1(7,7), 3CCb1(8,8), 3CCb1(9,9), 3CCb1(10,10), 3CCb1(11,11), 3CCb1(12,12); (CH3(CH2)n-1)2CHOCONHC(CH2CH2COOH)3, n = 7, 8, 9, 10, 11, 12]–were synthesized. The synthesis of the 3CCbn series was accomplished in two steps from Weisocyanate™ and the long chain alcohol in good yields of chromatographed products (65–81%). The 3CCb1(n,n) series was similarly synthesized from Weisocyanate™ and the two-tailed symmetric alcohol (produced from a reaction of alkyl magnesium bromide and ethyl formate) in good yields of chromatographed products (71–84%). CMC data were collected by pendent-drop technique for the 3CAmn, 3CCbn, 3CUrn, and 3CCb1(n,n) series of amphiphiles to establish the concentration required for detergency. The triethanolammonium salt provided better solubility and higher CMCs of these amphiphiles than the potassium salt. All amphiphilic series tested lowered the solution surface tension from ~ 72 mN/m to ~ 50–55 mN/m, indicating that these amphiphiles are less surface active than typical surfactants such as sodium dodecyl sulfate. The CMCs for the 3CAmn series were found to decrease in value from 2 × 10⁻² M (3CAm15) to 2 × 10⁻³ M (3CAm21) in a linear fashion. The CMCs for the 3CCbn series were found to decrease in value from 7 × 10⁻³ M (3CCb16) to 0.4 × 10⁻³ M (3CCb22) in a linear fashion. The CMCs for the 3CUrn series were found to decrease in value from 2 × 10⁻³ M (3CUr18) to 1 × 10⁻³ M (3CUr22) in a linear fashion. Due to discrepancies in several of the IFT vs. log concentration plots for the previous homologous series of amphiphiles, the CMC data was collected using a pyrene fluorescence measurement technique. The data from the pyrene fluorescence technique seems likely to be more accurate, indicating that surface tension may not be the most reliable method for determining the CMC of these amphiphiles. The CMCs (as determined by pyrene fluorescence) for the 3CAmn series were found to decrease in value from 2 × 10⁻² M (3CAm15) to 2 × 10⁻³ M (3CAm21) in a linear fashion. The CMCs for the 3CCbn series were found to decrease in value from 7 × 10⁻³ M (3CCb16) to 0.3 × 10⁻³ M (3CCb22) in a linear fashion. The CMCs for the 3CUrn series were found to decrease in value from 7 × 10⁻³ M (3CUr16) to 0.2 × 10⁻³ M (3CUr22) in a linear fashion. In both the surface tension and the pyrene fluorescence techniques, the shortest chain length homologues (3CAm13, 3CCb14, and 3CUr14) did not show a break up to the limits of solubility. The CMCs as determined by surface tension for the 3CCb1(n,n) series were found to decrease in value from 0.5 × 10⁻³ M (3CCb1(9,9)) to 0.02 × 10⁻³ M (3CCb1(12,12)) in a linear fashion. The 3CCb1(8,8) and 3CCb1(7,7) amphiphiles did not show a CMC break up to the limits of solubility. The 3CCb1(12,12) showed an unusually steep decrease in surface tension over a very narrow range of concentration. There is considerable doubt as to the accuracy of the 3CCb1(11,11) data, and the CMCs for these two-tailed amphiphiles needs to be measured by a second method as was done for the single-tail series to verify the CMCs of all the two-tail homologues. Activity (minimal inhibitory concentrations, MICs) for the 3CAmn, 3CCbn, 3CUrn, 3CCb1(n,n), 2CAmn, and 2CCbn series was measured against several different bacteria, mycobacteria, yeast, and fungi. Additionally, anti-HIV and cytotoxicity data was collected for the 3CAmn, 3CCbn, and 3CUrn series. Greatest inhibition was typically seen from the 18–20 carbon tail length homologues of each series (3CAm19–3CAm21, 3CCb18–3CCb20, 3CUr18–3CUr20, 2CAm19–2CAm21, and 2CCb18–2CCb20). Inoculum density affected the activity of our earlier studies, and selected organisms were retested to obtain the intrinsic activity. 3CUr18 and 3CAm19 proved most effective against Mycobacterium smegmatis, with MIC99 = 6.3 μM @ 10⁵ CFU/mL inoculum density. 3CCb20 was most effective against Mycobacterium marinum with MIC99 = 16 μM @ 10⁵ CFU/mL inoculum density. 3CAm19, 3CCb18, and 3CUr18 all showed equivalent activity against Mycobacterium chelonae with MIC99 = 17 μM @ 10⁵ CFU/mL inoculum density. Against Staphylococcus aureus, the 2CAm21 was most effective, with MIC90 = 2.0 μM @ 10⁵ CFU/mL inoculum density. 3CCb20 was most effective against MRSA with MIC90 = 2.9 μM @ 10⁵ CFU/mL inoculum density. The two-tailed analogs (3CCb1(n,n), 3CUr(n,n), and 3CUr1(n,n)) typically showed little to no activity against the tested microorganisms. Comparison of MIC to CMC is a relative measure of safety of a drug candidate. All single-tail amphiphiles showed ratios of MIC/CMC of 16–126, with a ratio of 100 or better being optimal. The ratios for the two-tail amphiphiles ranged from 0.39 to 2.9. / Ph. D.

CMC

critical micelle concentration

pendent drop

surfactant

amphiphile

Elaboration of micelle formation in aqueous and two phase solutions by surface active phosphines

Barnes, Jeffery G.

11 June 2009

The surface active phosphine ((C6H4))C3H6((C6H4)S03 N+)3,1, aggregates in aqueous solution to form micelles. Light scattering experiments were used to determine the hydrodynamic radius of the aggregates. Fluorescence, conductivity, and surface tension experiments were used to measure the critical micelle concentration of these aggregates. Fluorescence experiments, using a quencher and probe analysis, show the number of particles per aggregate. Nuclear Magnetic Resonance (NMR) shows that these micelles are able to incorporate olefin within the hydrophobic region and are acting as phase transfer agents. / Master of Science

micelle

phosphine

chemistry

catalysis

two phase

LD5655.V855 1995.B3683

Élaboration de copolymères amphiphiles à base de poly (3-hydroxyalcanoate)s / Design of poly (3-hydroxyalkanoates)-based amphiphilic copolymers

Babinot, Julien

12 December 2012

Les poly (3-hydroxyalcanoates) (PHAs) sont des polyesters aliphatiques produits et accumulés par des bactéries en tant que réserve de carbone et d'énergie. Ils sont constitués d'unités β-hydroxyesters et possèdent des chaînes latérales de longueur variable, pouvant être fonctionnalisées. Ils possèdent des propriétés de biodégradabilité et de biocompatibilité; ceci leur confère de vastes possibilités d'utilisation dans le domaine biomédical, notamment pour la mise au point de systèmes de libération contrôlée de principes actifs. Dans cette optique, nous nous sommes intéressés à la synthèse de copolymères amphiphiles de différentes architectures à base de PHAs, ainsi qu'à l'étude de leurs propriétés d'auto-association en milieu aqueux. Une méthode simple et efficace permettant le greffage d'oligomères de poly (éthylène glycol) (PEG) a tout d'abord été mise au point grâce à l'utilisation de la chimie « click ». Une série de copolymères diblocs bien définis PHA-b-PEG a ainsi pu être synthétisée par cycloaddition de Huisgen catalysée par le cuivre (CuAAC). Les copolymères diblocs à base de PHAs à moyennes chaînes latérales (PHA-mcl) ont montré leur capacité à s'auto-associer en milieu aqueux et à former des micelles monodisperses présentant une concentration micellaire critique très faible. Par la suite des copolymères de type greffés PHOU-g-PEG ont été synthétisés par addition thiol-ène. Les analyses par cryo microscopie électronique à transmission (cryo-TEM) ont montré que dans ce cas les copolymères s'auto-associaient en structures vésiculaires, ou polymersomes. Enfin, la synthèse de copolymères amphiphiles greffés porteurs de chaînes perfluorées PHOU-g-(F;PEG) a permis l'obtention de structures auto-associées plus complexes. Le cryo-TEM a en effet révélé la formation de micelles multicompartimentées, c'est à dire possédant un coeur présentant une séparation de phase entre les domaines hydrophobes et les domaines fluorés. Des tests biologiques préliminaires ont montré la cytocompatibilité de ces micelles / Poly (3-hydroxyalkanoates) are natural aliphatic polyesters produced and accumulated by many bacteria as carbon and energy supply. They consist of β-hydroxy ester units, with pendant side chains of different lengths that can be functionalized. Thanks to their biodegradability and biocompatibility, they are promising polymers for biomedical applications, especially for controlled drug delivery systems. In this context, we aimed to synthesize PHA-based amphiphilic copolymers with different molecular architectures, and to study their self-assembly in water. First, a simple and straightforward method using click chemistry has been used to graft poly(ethylene glycol) (PEG) oligomers. A series of well-defined diblock copolymers PHA-b-PEG has thus been synthesized using copper-catalyzed azide-alkyne cycloaddition (CuAAC). Medium chain length PHA-based diblock copolymers have shown their ability to self-assemble into stable micelles having very low critical micelle concentrations. Afterwards, amphiphilic graft copolymers PHOU-g-PEG have been synthesized using thiol-ene addition. In this case, cryo-electron microscopy (cryo-TEM) analysis revealed that graft copolymers self-assembled into vesicular morphologies, i.e. in polymersomes. Finally, the synthesis of amphiphilic graft copolymers bearing perfluorinated chains PHOU-g-(F;PEG) was performed. After aqueous self-assembly, cryo-TEM shown the formation of multicompartment micelles, i.e. with a core displaying segregated hydrophobic and fluorophilic domains. Moreover, these multicompartment micelles have shown their cytocompatibility

Poly (3-hydroxyalcanoate)

Copolymère amphiphile

Chimie

Micelle

Polymersome

Poly (3-hydroxyalkanoate)

Amphiphilic copolymer

Click chemistry

Micelle

Polymersome

Synthèse de composés antidépresseurs et anticancéreux - Contribution méthodologique à la réactivité des époxydes et des dérivés organiques du bismuth / Synthesis of biologically active compounds for the treatment of depressive desorder and cancer - Methodological contribution to epoxydes and organobismuth derivatives chemistry.

Nguyen, Dinh Vu

24 October 2016

Au cours de ce travail, nous nous sommes intéressés à la synthèse d'un analogue de Milnacipran, une molécule commercialisée sous le nom d'Ixel pour son activité anti-dépresseur. Il s'agit d'un cyclobutane trisubstitué portant deux centres stéréogènes contigus. L'objectif est de développer une voie de synthèse efficace et transposable à la version énantiosélective.Nous avons également travaillé sur la formulation nanométrique d'épiPodophyllotoxines, un produit naturel biologiquement active. Nous avons imaginé une architecture moléculaire permettant à la molécule de s'auto-assembler en micelle, ainsi elle peut être transportée de manière efficace au tumeur cancéreux. Les études in vitro et in vivo ont apporté des résultats prometteurs vis-à-vis du potentiel thérapeutique de notre nano-objet. Enfin nous avons étudié au cours de cette thèse deux méthodologies: la réactivité des époxydes en milieu alcalin fort et les dérivés d'organobismuth pour les réactions d'oxydation. Ces derniers ont été exploités afin d'oxyder des hydroxylamines en nitrone dans des conditions douces, permettant de réaliser le tandem oxydation/cycloaddition 1,3 dipolaire in situ avec des alcynes tendus. / My PhD thesis mainly involves the enantioselective synthesis of the Milnacipran's analog, a trisubstituted cyclobutane bearing two contiguous stereogenic centers. We have devised a conventional approach which consists of an intramolecular SN2 cyclization. After an acidic treatment, the key intermediate lactone was isolated with an ee > 99%, which was converted to the Milnacarre with no erosion of the ee value. We have also interested in the nanometric formulation of Podophyllotoxine derivatives. The natural product was designed to bear a hydrophilic and hydrophobic side chain. Its micellar solution was evaluated in vitro, in vivo and the obtained resuls were shown to be promising.We have also studied two methodologies: the reactivity of glycidyl ether toward alkyllithium reagents and oxydation of hydroxylamines to nitrone using triphenylbismuth carbonate. We observed in the former case an original rearrangement of the substrate to a vicinal diol, while in the latter case we have developped a mild condition to perform an tandem oxydation/1,3-dipolar cycloaddition in situ with a strained alkyne.

Cyclobutane

Synthèse multi-Étape

Époxydes

Micelle

Triphénylbismuth carbonate

Podophyllotoxine

Cyclobutane

Multistep synthesis

Epoxyde

Micelle

Triphenylbismuth carbonate

Podophyllotoxine