Décharge électrique à l'interface de deux liquides : application à la synthèse de nanoparticules

Mohammadi, Kyana

09 1900

Les procédés plasma-liquide sont considérablement étudiés en raison de leur potentiel élevé dans la production de divers nanomatériaux, parmi d’autres applications technologiques. En plus d'un rendement relativement élevé (mg/min) et d'une infrastructure simplifiée, les mécanismes de synthèse sont directs. Le fait que les produits restent confinés dans la solution, la manipulation de nanomatériaux ne présente un danger ni aux vivants ni à l’environnement. Dans ce mémoire de maitrise, les méthodes les plus courantes pour la synthèse de nanomatériaux, en particulier les systèmes plasma-liquide, sont discutées. La formation de différents régimes de plasma dans des liquides, dont chacun a des caractéristiques et des applications différentes, est présentée. Ensuite, le système multi-liquide et ses caractéristiques, telles que les caractéristiques électriques et la dynamique de l’émission des décharges dans différentes conditions, sont exposés. Pour la synthèse de nanoparticules, on traite les décharges Sparks (étincelles) avec une attention particulière. Au lieu de les produire entre deux électrodes immergées dans un liquide diélectrique, les décharges sont produites dans un hydrocarbure liquide entre une électrode et une solution conductrice. Cette dernière est produite via l’ajout de nitrate d’argent dans l’eau. Le plasma, via ses espèces réactives, réduit les ions Ag+ en Ag0 qui forment ensuite les nanoparticules. La décomposition de l’hydrocarbure produit aussi des espèces carbonées qui se recombinent sous forme d’une matrice hydrocarbonée. En se basant sur différentes méthodes de caractérisations (FTIR, MEB, MET, UV-vis, etc.), nous identifions deux zones de réactions : dans le plasma dans l’heptane et à l’interface plasma-solution. Les produits dans la première zone sont majoritairement des nanoparticules (< 10 nm) d’Ag enrobées dans une matrice de carbone hydrogénée. Cependant, les produits dans la solution sont des nanoparticules d’Ag (sans matrice) ayant une distribution de taille de quelques dizaines de nanomètres. / Plasma-liquid systems are significantly investigated due to their high potential in the production of various nanomaterials, among other technological applications. In addition to relatively high efficiency in production (mg/min) and simplified infrastructure, the mechanisms of synthesis are rather direct. Also, because the products are confined in solution, the handling of the nanomaterials do not present risks to the living or to the environment. In this master thesis, the most common methods for nanomaterial synthesis, in particular plasma-liquid systems, are discussed. Formation of different plasma regimes in liquids, which each of them has different features and application, are explained. Then, the multiple liquid system and their feature such as electrical characteristics and emission dynamic of the discharges at different conditions, are investigated. To produce nanoparticles, we present the Spark discharges with special attention. Instead of their production between two electrodes immersed in a liquid dielectric, the discharges are produced in a liquid hydrocarbon between one electrode and a conductive solution. This latter is prepared by adding silver nitrate to water. The plasma, through its reactive species, reduces the ions Ag+ to Ag0 that produces nanoparticles. The decomposition of the hydrocarbon produces carbonaceous species that recombine as hydrocarbon matrix. Based on the different characterisation techniques (FTIR, SEM. TEM. UV-vis, etc.), we identified two zones of reactions: in plasma in heptane and at the interface plasma-solution. The products in the former zone are majority 10 nm-particles of Ag embedded in a hydrocarbon matrix, while the products in solution are Ag nanoparticles (without matrix) with size of several tens of nanometers.

Plasma dans le liquide

Décharge par étincelle

Nanocomposite

Décharges nanosecondes

Nanoparticule d'argent

Réseau d'hydrocarbures

Plasma in-liquid

Spark discharge

Nanocomposites

Nanosecond discharges

Silver nanoparticle

Hydrocarbon network

Nanostructuration de films nanocomposites amidon / argent et amidon / argent / montmorillonites par procédé de « chimie verte » : influence des voies de génération des nanoparticules métalliques sur la structure et les propriétés de transport / Nanostructuration of starch/silver and starch/silver/montmorillonites nanocomposites films with green process : influence of the silver nanoparticles generation routes on structure and transport properties

Cheviron, Perrine

08 April 2015

Des films nanocomposites amidon / argent ont été préparés par deux voies de génération vertes de nanoparticules d'argent. La première voie, dite ex situ, consiste à préparer tout d'abord une solution colloïdale d'argent qui est ensuite redispersée dans une matrice amidon plastifiée glycérol. Les nanoparticules d'argent colloïdales sont synthétisées en solution aqueuse par réduction du nitrate d'argent par du glucose en présence d'amidon stabilisant. La seconde voie, dite in situ, consiste à disperser le nitrate d'argent dans le film amidon plastifié et le réduire directement dans le film par traitement thermique en présence ou non de réducteur. L'influence du taux de glucose réducteur, du temps de synthèse et de la température a été étudiée en termes de taille, distribution de taille et dispersion des nanoparticules d'argent dans les films nanocomposites ex situ et in situ. Tout en gardant des paramètres de procédé comparables, les deux voies de nanostructuration des films amidon/argent ont également été comparées en termes de structure, de propriétés thermiques et de transport. Enfin, l'incorporation de charges montmorillonites a également été étudiée dans les deux voies de génération des nanoparticules métalliques. L'ensemble des travaux a permis de valider les deux voies de génération vertes menant à des nanoparticules d'argent dispersées de manière homogène et de tailles moyennes inférieures à 30 nm. La voie in situ à 85°C se distingue par des nanoparticules d'argent cristallines et de très petites tailles (inférieures à 10 nm) avec une interface amidon/argent cohésive particulière qui permettent d'améliorer les propriétés barrières aux gaz et à l'eau avec une diminution de perméabilité observée jusqu'à 90% / The present work reports a strategy involving the preparation of silver nanoparticles in a biodegradable polymer stemming from either an ex situ or an in situ method, using in both cases a completely green chemistry process. The influence of the reducing agent concentration and the silver nanoparticles generation route is investigated on the structure, the morphology and the properties of the nanocomposite films. In both routes, silver nanoparticles with a diameter below 30 nm were highlighted in the nanocomposite films. For all nanocomposite films, no modification on the crystalline structure of the starch matrix is observed in the presence of silver. The in situ generation route allowed to obtain the smallest silver nanoparticles with a diameter below 10 nm. Crystalline silver nanoparticles were obtained only from the in situ generation route at the temperature of 85°C. The introduction of montmorillonites in both generation routes was also studied. The decrease of the water sorption and the improvement of water and oxygen barrier properties were found to be not dependent on the reducing agent concentration but mainly on the presence of the crystalline structure of the silver nanoparticles. Thus, significant enhancement of the barrier properties were finally obtained for the in situ nanocomposite films thanks to an efficient interaction between the crystalline silver nanoparticles and the starch matrix

Nanoparticules d’argent

Amidon

Films nanocomposites

Synthèse ex situ, in situ

Transport

Propriétés barrière

Sorption d’eau

Silver nanoparticle

Starch

Nanocomposite

In situ and ex situ syntheses

Transport

Barrier properties

Water sorption

Oxygen and water permeability

547.7

Novel Cationic Gemini Lipids, Click Chemistry Based Adducts And Amphiphile-Capped Silver Nanostructures : Synthesis, Aggregation And Biological Properties

Biswas, Joydeep

07 1900

The thesis entitled “Novel Cationic Gemini Lipids, Click Chemistry Based Adducts and Amphiphile-Capped Silver Nanostructures: Synthesis, Aggregation and Biological Properties” elucidates the design, synthesis, aggregation and gene transfection properties of novel gemini cationic lipids based on cholesterol and pseudoglyceryl backbone, and click chemistry based adducts. This thesis also elucidates the synthesis and aggregation properties of silver nanoparticles loaded cationic liposomes and silver nanorods stabilized by micellar solutions of gemini surfactants. The work has been divided into six chapters. Chapter 1: Introduction: Membrane Formation from Cholesterol-based Cationic Lipids and their use as Non-Viral Gene Delivery Agents This chapter describes the importance of cholesterol in biological membranes, the aggregation properties of cholesterol-based cationic lipids and their interactions with phospholipid membranes. This chapter also gives a comprehensive account of the research towards the development of novel cationic cholesterol-based monomeric and gemini lipids. It also reviews the utilization of cholesterol-based cationic monomeric and gemini lipids in gene transfection properties. Chapter 2A: Effect of Hydroxyl group on the Cationic Headgroups of Cholesterol-based Gemini Lipids on their Aggregation, DNA Binding Properties and Interaction with Phospholipid Membranes This chapter describes the syntheses and aggregation properties of two series of cholesterol-based monomeric and gemini cationic lipids with and without hydroxyl functionality (Figure 1). The gemini lipids of a given series differ in their spacer polymethylene -(CH2)n- chain lengths between the cationic headgroups. Figure 1. Molecular structures of non-hydroxylated and hydroxylated cationic cholesterol-based gemini lipids and their monomeric counterparts. All monomeric and gemini lipids were found to generate stable suspensions in aqueous media. Electron microscopic studies showed that all the lipids form vesicular aggregates in aqueous media. The structures seen under TEM for the non-hydroxylated series of monomeric (C-M) and gemini lipids are of variable sizes, they appeared like separated vesicular aggregates. For the hydroxylated series of lipids, however, both the monomeric lipid aggregates (CH-M) and aggregates of their gemini counterparts were found to be ‘connected’ with each other to form elongated chain of aggregates of different length scales. XRD studies with the cast films of lipids revealed that the monomeric lipids of either series have higher bilayer width than the corresponding gemini lipids. Incorporation of the -(CH2)n- spacer units at the head group level joining the two monomeric units lowered the bilayer thicknesses of both series of the lipid aggregates. Thus the monomeric lipids (C-M and CH-M) appear to form nearly regular bilayer type arrangements whereas gemini lipids form interdigited and tilted bilayer arrangements in their aggregates. Calorimetry studies of the coaggregates showed that ~10 mol-% of most of the cholesterol gemini lipids is enough to abolish the phase transition of DPPC membranes whereas more than 10 mol-% is required in case of their monomeric counterparts. Further these thermotropic properties depend upon the length of the spacer of the gemini lipid included in the mixture. We have observed greater quenching of the thermal phase transition of DPPC membranes with 10 mol-% of C-M as compared to CH-M doped liposomes. At 10 mol-% of all the cationic lipid doped DPPC covesicles, only CG-3 doped liposomes showed an observable transition temperature. Maximum broadening of the DPPC transition peak was observed in the case of the gemini lipids, CHG-6 and CHG-12. DNA binding and release studies show that the interactions between gemini lipids and DNA depend upon the nature of the head group as well as the length of the spacer between the cationic head groups. For the non-hydroxylated cholesterol-based cationic lipid series, the monomeric liposomes of C-M facilitates the dissociation of EB from the EB-DNA complex to an extent of 93% at a maximum lipid:DNA ratio of 3.0 whereas the liposomes of CG-4 and CG-12 showed the lowest extent of maximum EB exclusion (~74%) from the EB-DNA complex at lipid:DNA ratio of 3.0. For hydroxylated cholesterol-based cationic lipid series, the monomeric liposomes of CH-M facilitate the dissociation of EB from the intercalated EB-DNA complex to an extent of 81 % whereas the liposomes of CHG-3 showed the minimum binding to DNA. Thus the two monomeric liposomes C-M and CH-M were the more efficient formulations that allow dissociation of DNA from the corresponding lipoplexes. These findings have important being in their gene transfection activity compared their respective gemini lipid counterparts. Chapter 2B: Novel Cholesterol-based Cationic Gemini Lipids possessing Hydroxyethyl group on the Headgroup: Transfection Efficacy and Cell Toxicity Properties This chapter describes the transfection efficacy and cell toxicity properties of five cholesterol based gemini cationic lipids possessing hydroxyethyl functionality on each head group, which differ in the length of the polymethylene spacer [-(CH2)n-] chain (Figure 2). These gemini lipids are important to gene delivery processes as they possess pre-optimized molecular features, e.g., cholesterol backbone, ether linkage and a variable spacer chain between both the headgroups of the gemini lipids. Cationic liposomes were prepared from each of these lipids individually and as a mixture of individual cationic gemini lipid and 1,2-dioleoylphosphatidylethanolamine (DOPE). The gemini lipid with a hydroxyethylated headgroup and a -(CH2)5- spacer, CHG-5 showed the highest transfection activity at N/P (lipid/DNA) ratio of 0.5 and lipid:DOPE molar ratio of 2. Upon comparison of the relevant parameters, e.g., % transfected cells, the amount of DNA transfected to each cell and % cell viability all together against LipofectAMINE 2000, one of the most potent commercially available transfecting agents, the optimized lipid formulation based on CHG-5/DOPE was found to be comparable. In terms of its ability to induce gene-transfer in presence of serum and shelf-life CHG-5/DOPE liposome was found to be better than its commercial counterpart. Recording of confocal images confirmed that in presence of 10% serum using 1.2 µg DNA per well and lipid:DOPE ratio of 1:4 and N/P charge ratio of 0.75, CHG-5 is better than LipofectAMINE 2000. These properties render them to be reagents of practical value for various gene delivery applications. Figure 2. Molecular structures of cholesterol-based cationic monomeric lipid and gemini lipids possessing hydroxyethyl group on the headgroup synthesized. Chapter 3: Bilayer Membrane and Stable Monolayer Forming Properties of Cationic Pseudoglyceryl Gemini Lipids having Polymethylene Spacers and Oxyethylene Linkages This chapter describes the synthesis of five new cationic pseudoglyceryl gemini lipid versions of their monomeric counterpart (Figure 3). Each cationic lipid aggregate in aqueous media was found to form vesicular structures as evidenced from the negatively stained TEM experiments and DLS measurements. XRD experiments with their cast films of aqueous dispersions revealed that introduction of the polymethylene -(CH2)n-spacer chain joining the two monomers decreased the bilayer widths of the gemini lipid aggregates. The inter-lipidic packing and the hydration of the lipid vesicles were examined using fluorescence anisotropy and generalized polarization measurements using membrane-soluble probes, DPH and Paldan respectively. Fluorescence anisotropy measurements showed that the aggregates of lipid 2c with -(CH2)5- spacer chain were highly packed and ordered in the vesicular aggregates than that of the other cationic lipid aggregates in the series. Paldan hydration studies showed that incorporation of the polymethylene -(CH2)n- spacer chains joining two monomeric units lowered the hydration of the gemini lipid aggregates in the solid gel state. Each of these cationic lipid aggregates showed sharp transition temperatures (Tm) as observed from differential scanning calorimetric studies. DSC studies further revealed that the incorporation of oxyethylene group at the linker region of cationic pseudoglyceryl gemini lipid 2a with (CH2)3- spacer chain length lowered the thermotropic phase transition temperature (Tm) of the aggregates in aqueous media when compared with the corresponding gemini analogue without oxyethylene linkages. Langmuir film balance studies showed that each cationic gemini lipid and their monomeric counterpart were able to form stable monolayers at the air-water interphase. We observed that the mean molecular area (collapse area) of each of the cationic lipid obtained from the Langmuir monolayer studies increased with increase in the spacer chain lengths. Figure 3. Molecular structures of the cationic pseudoglyceryl gemini lipids and their monomeric counterpart. Chapter 4: Vesicle and Stable Monolayer Formation from Simple ‘Click’ Chemistry Adducts in Water This chapter describes successful use of Cu(I) catalyzed “Click Chemistry” for the syntheses of a series of hitherto unknown amphiphilic adducts (M1, M2, D1 and T1) which on dispersal in water afforded vesicular aggregates as evidenced from dye entrapment, TEM, SEM, AFM and DLS studies (Figure 4). Figure 4. Molecular structures of triazole based adducts. XRD experiments with their cast films of aqueous suspensions indicate the formation of a tilted bilayer arrangement for the aggregates of M1 whereas regular bilayer structures are predominant for the aggregates derived from M2, D1 and T1. Measurement of pKa values using UV-Vis spectroscopy showed that the aggregates of monomeric click adducts (M1 and M2) possess less pKa value than that of the aggregates of dimeric (D1) and tetrameric (T1) analogues and the values lie within the range of 2.8-3.2. The hydrodynamic diameter of the aggregates of each click adduct increased with decrease in the pH of the media. Thus, the protonation of the triazole groups in the aggregates of each click adduct increased the hydrodynamic diameter. Dye entrapment studies showed that each click chemistry based adduct formed closed vesicular aggregates with inner aqueous compartment in aqueous media. The temperature induced order-to-disorder transitions of the aggregates and the accompanying changes in hydration were examined using high sensitive DSC, fluorescence anisotropy and generalized polarization measurements using a membranesoluble probe, DPH and Paldan respectively. In the solid state, M1 remains as the most hydrated species whereas in the fluidized phase, D1 maintains as the most hydrated aggregate. Clearly simple variation in the adduct molecular architecture bring about significant changes in their packing in aggregates and also the hydration of the resulting vesicles. Langmuir monolayer studies confirmed that these click adducts do form stable monolayers as well on water subphase at the air-water interface. We also calculated the mean molecular areas from the Langmuir monolayer studies and as perhaps expected the adduct T1 has the highest head group area. Thus click chemistry based simple triazole adducts, which can be very easily prepared, are good candidates for further investigations involving syntheses of novel self-assembling structures. Chapter 5: Lipid Mediated Synthesis of Silver Nanoparticles, their Physical Characterizations and DNA Binding Abilities In this chapter, work on the Ag-NP (silver nanoparticle) loaded liposomes preparation using four cationic lipids (1-4) in which the Ag-NPs were entrapped within lipid bilayer has been described. A novel method was developed to synthesize the Ag-NPs where the lipid itself capped and stabilized the Ag-NPs. Consequently there was no need of inclusion of any other capping agents like citrate. Confocal microscopy confirmed that these Ag-nanoparticles are fluorescent in character. It was also demonstrated that silver nanoparticles are indeed entrapped in lipid bilayer with transmission electron microscopy (TEM). DLS experiments provided information about the hydrodynamic diameter of the lipid vesicles which increased with the increase in Ag concentrations. This could be due to the ‘loosening’ of the lipid packing in vesicles. Zeta potential measurements showed that the zeta potential value decreased with the increase in the concentration of Ag-NPs in the cationic lipid vesicles. XRD studies with the cast films of the lipid or Ag-NP loaded lipid suspensions revealed that when the Ag-NPs get entrapped into the bilayer of the multilamellar vesicles of the lipid in the aqueous media, the unit bilayer thickness of the aggregates increased. Paldan experiments showed that with the incorporation of Ag-NPs in the lipid vesicles, the hydration of the lipid vesicles increased to a significant extent but the phase transition temperatures remained practically unaltered for all the lipids. Fluorescence anisotropy experiments revealed that the hydrocarbon chain packing of the lipid vesicles ‘loosens’ with the incorporation of Ag-NPs. Ag-NP loaded liposomes showed enhanced DNA binding ability and also the presence of Ag-NPs in cationic liposomes induced the release of DNA from silver nanoparticle-loaded lipoplexes more effectively. Figure 5. Molecular structures of the cationic lipids mentioned in the present chapter. Chapter 6: Dependence of Spacer Chain Lengths in the Synthesis of Ag-Nanorods in Gemini Cationic Surfactant Micelles Figure 6. Chemical structures of cationic gemini surfactants. This chapter describes the synthesis of Ag-nanospecies by seed-mediated wet synthesis method using four gemini surfactants (16-2-16, 16-4-16, 16-5-16 and 16-1216) as the capping agents (Figure 6). For this, we first synthesized Ag-nanoseeds of diameter ~7 nm stabilized by trisodium citrate (as capping agent). Then the solution containing Ag-nanoseeds was used to synthesize Ag-nanorods of different aspect ratios. It was that with decreasing Ag-nanoseed concentration, the aspect ratios of Agnanorods stabilized by gemini surfactants (16-2-16 and 16-4-16) increased gradually as evidenced from TEM images. These Ag-nanoseeds and Ag-nanorods were further characterized using UV-Vis spectroscopy (to know the surface plasmon bands), transmission electron microscopy (TEM), energy-dispersive X-ray spectroscopy (EDAX) and X-ray diffraction (XRD). It was observed that when gemini surfactant 164-16 was used to stabilize Ag-nanorods, the λmax of the longitudinal band shifted more towards the red region (red-shift) as observed by UV-Vis spectroscopy when compared to that of gemini surfactant with shortest spacer, 16-2-16. Thus the gemini surfactants with shorter -(CH2)2- and -(CH2)4- spacer chains promoted the growth of Ag-nanorods in their micellar solutions whereas -(CH2)5- and -(CH2)12- spacer chains of gemini surfactants did not. So, the growth of Ag-nanorods in micellar solutions is found to be highly spacer-chain length specific. TEM micrographs revealed that the aspect ratios of Ag-nanorods stabilized by gemini surfactants 16-4-16 are larger than those compared to the Ag-nanorods stabilized by gemini surfactants 16-2-16 at a particular amount of Agnanoseed solution. TEM images of the samples containing micellar solutions of gemini surfactants 16-5-16 and 16-12-16 showed that the formation of only Ag-nanoparticles of larger sizes (compared to Ag-nanoseeds stabilized by trisodium citrate) and Agnanoprisms irrespective of the amount of Ag-nanoseed solution added. No Ag-nanorod formation in the micellar solutions of gemini surfactants 16-5-16 and 16-12-16 was observed. Gemini surfactants (16-2-16 and 16-4-16) formed bilayer arrangements to facilitate the growth and stabilization of Ag-nanorods in aqueous media where the inner layer is attached to the Ag-nanorod surface through the gemini surfactant ammonium headgroups. X-ray diffraction (XRD) studies showed that these Ag-nanorods stabilized by gemini surfactants 16-2-16 and 16-4-16 crystallized in the aqueous media via (111), (220) and (222) lattice faces. Thus this study demonstrated the way one can control structures and shapes of the silver nanoobjects using gemini surfactant micelles. (For structural formula pl refer the thesis)

Gemini Lipids

Amphiphile Silver Nanostructures

Gemini Cationic Lipids - Synthesis

Cationic Liposomes - Synthesis

Cholesterol-Based Cationic Lipids

Cholesterol-Based Gemini Lipids

Cationic Pseudoglyceryl Gemini Lipids

Click Chemistry

Silver Nanoparticle Loaded Liposomes

Gemini Cationic Surfactants

Ag-Nanorods

Cholesterol Based System

Ag-Nanoparticles

Biochemistry