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  • About
  • The Global ETD Search service is a free service for researchers to find electronic theses and dissertations. This service is provided by the Networked Digital Library of Theses and Dissertations.
    Our metadata is collected from universities around the world. If you manage a university/consortium/country archive and want to be added, details can be found on the NDLTD website.
141

Nanoparticle-Based Spintronic Computer Logic Switch

Luongo, Kevin 28 March 2019 (has links)
Spintronics is a rapidly growing research field due to scalability, integrablility within existing VLSI architecture, significantly reduced switching energy and latency while maintaining stable bit orientation (Spin-up, Spin-down). For the first time sub-5nm Spin Transfer Torque –Magnetic Tunneling Junctions (STT-MTJ) were investigated utilizing various Integrated Circuit (IC) fabrication techniques to evaluate novel concepts in logic switches. Tunneling Magnetoresistance (TMR) was measured in STT-MTJ stacks of Ta/CoFeB/MgO/CoFeB/Ta with differing diameter ferrimagnetic CoFe2O4 nanoparticles (10nm, 4nm and 2nm) embedded in the MgO layer. MR was detected in the 2nm and 4nm particle devices and demonstrated evidence of single electron transport. Tri-layer STT-MTJ devices were fabricated using a thin film stack of Ta/Ru/Ta/CoFeB(M1)/MgO/CoFeB(M2)/MgO/CoFeB(M3)/Ta. The overall diameter of the stack was reduced to sub-20nm using Focused Ion Beam (FIB) to mill away extra material. The coercivities of the ferrimagnetic CoFeB layers were modified during thin film deposition by altering sputter conditions. Field Applied- Magnetic Force Microscopy (FA-MFM) was used to detect four different magnetic intensities corresponding to three discreet resistances in the singly addressed device, making this architecture a candidate for neuromorphic computational applications. Lastly a lithographic-less architecture was developed to mass fabricate and electo-mechanically probe multi-layered, single point, sub-5nm particle based STT-MTJ devices using off-the-shelf anodized nanoporous alumina. Once fabricated, the devices were probed to measure their IV characteristics and magnetoresistance (MR). The unprecedented MR changes on the order of 50,000% at room temperature suggest quantum mechanical behavior.
142

Modular Nanoparticles for Selective Cell Targeting

Peuler, Kevin 05 1900 (has links)
Indiana University-Purdue University Indianapolis (IUPUI) / Nanoparticles (NPs) are an emerging technology in biomedical engineering with opportunities in diagnostics, imaging, and drug delivery. NPs can be prepared from a wide range of organic and/or inorganic materials. They can be fabricated to exhibit different characteristics for biomedical applications. The goal of this thesis was to develop NPs with tunable surface properties for selective cell targeting. Specifically, polyelectrolyte complexes composed of heparin (Hep, a growth factor binding glycosaminoglycan) and poly-L-lysine (PLL, a homopolymeric lysine) were prepared via a pulse sonication method. The Hep/PLL core NPs were further layered with additional Hep, tetrazine (Tz) modified Hep, or dextran sulfate (DS). The addition of Tz handle on Hep backbone permitted easy modification of NP surface with norbornene (NB) modified motifs/ligands, including inert poly(ethylene glycol) (PEG), cell adhesive peptides (e.g., RGD), and/or fluorescent marker. Both Hep and DS coated NPs could be readily internalized by J774A.1 monocytes/macrophages, whereas PEGylated NPs effectively reduced cellular uptake/recognition. The versatility of this NP system was further demonstrated by laying DS on the Hep/PLL NP surface. DS-coated NPs were recognized by J774A.1 cells more effectively. Furthermore, DS-layered NPs seemed to reduce IL-10 production on a per cell basis, suggesting that these NPs could be used to alter polarization of macrophages.
143

Augmented liver tageting of exosomes by surface modification with cationized pullulan / カチオン化プルランを用いたエクソソームの表面修飾はエクソソームの肝指向性を増強する

Tamura, Ryo 25 September 2017 (has links)
京都大学 / 0048 / 新制・課程博士 / 博士(医学) / 甲第20672号 / 医博第4282号 / 新制||医||1024(附属図書館) / 京都大学大学院医学研究科医学専攻 / (主査)教授 妹尾 浩, 教授 野田 亮, 教授 岩田 想 / 学位規則第4条第1項該当 / Doctor of Medical Science / Kyoto University / DFAM
144

Systematic Study on the Pd-H Interaction in the α-Phase PdHx / α相PdHxにおけるPd-H相互作用に関する系統的研究

Dekura, Shun 23 January 2019 (has links)
京都大学 / 0048 / 新制・課程博士 / 博士(理学) / 甲第21442号 / 理博第4435号 / 新制||理||1637(附属図書館) / 京都大学大学院理学研究科化学専攻 / (主査)教授 北川 宏, 教授 竹腰 清乃理, 教授 吉村 一良 / 学位規則第4条第1項該当 / Doctor of Science / Kyoto University / DGAM
145

Synthesis and Characterization of an Oligothiophene-Ruthenium Complex and Synthesis and Optical Properties of Oligothiophene-Ruthenium Complexes Bound to CdSe Nanoparticles

Bair, Nathan A. 12 August 2010 (has links) (PDF)
Oligothiophenes are of increasing interest in organic based electronic devices in part due to their high electron and hole mobilities. In an organic photovoltaic (OPV) device, the electronic properties of oligothiophenes make them advantageous as charge transfer junctions. To serve as charge transfer junctions, oligothiophenes must be functionalized to bind to the donor and acceptor parts of the device. The donor and acceptor parts are different materials and the synthesis of asymmetric oligothiophenes is of great interest. Previous researchers in our lab synthesized four asymmetric oligothiophenes, two with two thiophene subunits and two with four. Each set of oligothiophenes contained a pair of constitutional isomers. Here we report the synthesis of another asymmetric oligothiophene, one with three thiophene subunits. This compound is functionalized with bipyridine to bind Ru(bpy)22+ and with phosphonic acid moieties to bind CdSe nanoparticles. The synthesis was carried out by bonding a phosphonic acid moiety to bithiophene and bipyridine to thiophene and then coupling the phosphate-bithiophene and thiophene-bipyridine. Standard Stille couplings were used for carbon-carbon bond formation. The resulting compounds have complex NMR spectra and overlapping Ru MLCT and π-π* transitions at 450 nm with molar extinction coefficient on the order of 3 x 105 M-1 cm-1. The thiophene fluorescence is quenched by Ru(bpy)22+. These optical properties compare closely with the previous compounds synthesized. Solar cells occupy significant attention in the media, politics and science for their promise of continual pollution-free energy. Quantum dots, metal complexes and organic compounds are all under research as viable replacements for expensive silicon solar cells. To test the efficacy of a light harvesting compound before constructing a solar cell, a model system is constructed to show electron transfer from the light harvester into an electron acceptor. We synthesized oligothiophenes and oligothiophene-ruthenium complexes and tested their ability to act as sensitizers and charge transfer junctions. To do this, they were bonded to CdSe nanoparticles and their optical properties were measured. Steady-state photoluminescence and time correlated single photon counting were used to observe the effects on fluorescence and fluorescence lifetime of the CdSe-oligothiophene and CdSe-oligothiophene-ruthenium complexes before and after binding. It was found that CdSe fluorescence was quenched when bound to an oligothiophene ruthenium complex, and that the fluorescence of the oligothiophene was quenched when bound to CdSe in the absence of ruthenium. The fluorescence lifetimes of the quenched species were shortened.
146

Scalable Nano Particle Production of Low Bioavailability Pharmaceuticals for Augmented Aqueous Solubility

Madden, Aaron 01 May 2014 (has links)
The billion dollar pharmaceutical research and development pipeline suffers greatly from high attrition rates of novel therapeutic compounds within pre-clinical and clinical trials. Poor bioavailability in many new drugs, originating in the various methodologies of high throughput screening, may explain part of these growing failure rates. One interpretation of this phenomenon relies on bioavailability's correlation with aqueous solubility; much modern processing allows chemicals to fully develop without touching water, yielding upwards of 90% of new chemical entities practically insoluble in aqueous media. Thus, one approach to alleviating bioavailability and potentially clinical attrition rates necessitates augmented aqueous solubility. The amorphous nanoparticle presents the largest boost in aqueous solubility of a chemical through processing alone. In this contribution, we propose electrospray as a novel, competitive candidate to produce pharmaceutical amorphous nanoparticles with the intent of augmenting solubility. Electrospray represents an idyllic nominee for three reasons: repeatability, flexibility, and scalability. Electrospray offers low batch to batch variation with less than 30% relative standard deviation between various droplets. This triumphs over the several orders of magnitude in variation in pneumatic sprays. Electrospray's flexibility draws from its ability to attain diameters over several orders of magnitude, ranging from hundreds of microns to several nanometers; in this contribution droplets are produced between 500 nm and 1[micro]m. Finally, electrospray displays scalability to any industrial requirement; though a single nozzle operates at mere microliters per hour, a single multiplexed array of emitters may increase this throughput by several orders of magnitude. This exploration, utilizing Indomethacin as a model low solubility chemical, verifies electrospray as a compatible processing tool for the pharmaceutical industry. Scanning electron microscopy coupled with the image analysis software ImageJ gleans the size and shape of emitted (and dried) particles. Amorphicity verification of particles employs grazing angle x-ray diffraction. Finally, ultraviolet and visual spectrum spectroscopy evaluates the solubility advantage of particles.
147

Tools for modulating and measuring autophagy

Martin, Andrew J. 10 November 2023 (has links)
Autophagy is an essential quality control process in which proteins and organelles are degraded. In this work, we first extended our understanding of autophagic degradation in disease by investigating the use of acidic nanoparticles to restore autophagic flux in a neurotoxic model of Parkinson Disease (PD). Normal autophagic degradation follows two key steps. First, material is engulfed to form a double-membraned autophagosome. Next, autophagosomes fuse with an acidic lysosome to degrade the inner membrane contents. Insufficient lysosomal acidity results in autophagic flux arrest, and in PC-12 cells, we characterized the use of polymeric nanoparticles as a tool to restore lysosomal acidity and rescue autophagic flux in PC-12 cells. Specifically, in an MPP+ model of neurotoxicity, we demonstrated that formulations of poly(lactic-co-glycolic acid) nanoparticles (PLGA) improved lysosomal acidity, autophagic flux, and cell health significantly, but is likely limited in efficacy by polymer degradation rate. To improve upon this, we developed a new acidic nanoparticle formulated with a novel polymer backbone (termed acNPs), engineered to degrade within lysosomes and release tetrafluorosuccinic acid, a highly potent acid (pKa ~1.6). On the benchtop, these engineered nanoparticles demonstrated both colloidal instability and acid release within a weakly acidic environment (pH 6.0) similar to a diseased lysosome but not at a neutral pH of 7.4. In cells, acNPs effectively decreased lysosomal pH within disease lysosomes, thereby restoring autophagic flux and mitochondrial activity in PC-12 cells. Encouragingly, we also were able to show efficacy of acNPs in 2D and 3D models of the human midbrain. acNPs readily trafficked within the lysosomes of cells in 2D midbrain cultures and 3D midbrain organoids. Similar to PC-12 cells, when we challenged these cells in a model of neurotoxicity, we observed restoration of viability in human organoids following acNP treatment. Next, we addressed some current challenges regarding the quantification of autophagy within cells. We repurposed measures of economic income inequality to quantify the spatial dispersion of LC3 signal intensity in a starvation model of autophagy, and then compared these measures to other image-based measurements based on their ability to represent LC3-II levels, a robust protein marker of the autophagosome. Our analysis showed these indices outperformed all other generated measurements, including the current standard of autophagy research, LC3 puncta counting. Additionally, we also explored the linear decomposition properties of the generalized entropy index and found it a facile way to evaluate autophagic flux within 3D imaging datasets of multicellular systems. Specifically, we revealed a differential response to nutrient depravation between neurons and astrocytes. Finally, we translated this paradigm to a high throughput cell assay where we demonstrated EC50 and IC50 curves, produced from datasets acquired through both confocal and automated widefield fluorescence microscopy. Our results agree with standard cell assays.
148

Intermolecular Electron Transfer Reactivity and Dynamics of Cytochrome c – Nanoparticle Adducts

Carver, Adrienne M. 01 September 2009 (has links)
Interprotein electron transfer (ET) is crucial for natural energy conversion and a fundamental reaction in the pursuit of understanding the broader problem of proteinprotein interactions and reactivity. Simplifying the complicated nature of these natural systems has driven development of biomimetic approaches. Functionalized gold nanoparticles offer simplified, tunable surfaces that can serve as a proxy to study the reactivity and dynamics of proteins. Amino-acid functionalized gold nanoparticles (Au-TX) served as a complementary partner to cytochrome c (Cyt c) and catalyzed its ET reactivity without altering the native structure. Redox mediator and EPR experiments confirmed that the redox potential and coordination environment of the heme were unaltered. Varying the functionality of Au-TX under limiting redox reagent concentrations resulted in distinct ET reactivity. These conditions reflected the collision of a small redox reagent with the Cyt c/Au-TX adduct, introducing the possibility of Cyt c/Au-TX dynamics to modulate ET. Under high ionic strength conditions, the rate enhancement ranged from 0.0870 " 1011 for Cyt c/Au-TAsp to 1.95 " 1011 M-1 s-1 for Cyt c/Au-TPhe. Au-TAsp binds to a larger surface of the front face of Cyt c than Au-TPhe, likely reducing heme access and resulting in attenuated ET reactivity.Site-directed spin-labeling characterized the dynamic interactions and motion of Cyt c with Au-TX. Several mutants of Cyt c were utilized to extract information about the different dynamics of the Cyt c/Au-TPhe and Cyt c/Au-TAsp systems. Cyt c appeared to have a highly dynamic binding interaction with the surface of Au-TPhe while binding to Au-TAsp resulted in a more rigid interface, particularly at the heme crevice. The dynamic interaction of Cyt c/Au-TX at the heme crevice could promote a gated ET mechanism between Cyt c and its redox partner. Thus, the reduced reactivity of Cyt c/Au-TAsp is likely a result of both slower global dynamics and more rigid binding near the heme crevice.
149

Assembly Of Surface Engineered Nanoparticles For Functional Materials

Yu, Xi 01 February 2013 (has links)
Nanoparticles are regarded as exciting new building blocks for functional materials due to their fascinating physical properties because of the nano-confinement. Organizing nanoparticles into ordered hierarchical structures are highly desired for constructing novel optical and electrical artificial materials that are different from their isolated state or thermodynamics random ensembles. My research integrates the surface chemistry of nanoparticles, interfacial assembly and lithography techniques to construct nanoparticle based functional structures. We designed and synthesized tailor-made ligands for gold, semiconductor and magnetic nanoparticle, to modulate the assembly process and collective properties of the assembled structures, by controlling the key parameters such as particle-interface interaction, dielectric environments and inter-particle coupling etc. Top-down technologies such as micro contact printing, photolithography and nanoimprint lithography are used to guide the assembly into arbitrarily predesigned structures for potential device applications.
150

Design & Fabrication of Nanostructured Hydrogels From Biopolymer Nanoparticle Building Blocks for Biomedical and Environmental Applications

Majcher, Michael January 2021 (has links)
In recent years, there has been a growing interest within the field of soft materials engineering on the development of advanced hydrogel systems with well-defined chemistries and morphologies that can be customized to suit various applications ranging from biomedical to environmental to personal care. In any case, careful selection of the building block materials, crosslinking chemistry, degradation pathway, and overall hydrogel architecture is essential to ensure the final design (and the resulting degradation components if relevant) are safe/non-toxic, mechanically tunable, and overall translatable for their intended end use given industry safety/production standards. In this thesis, the utility of starch nanoparticles created by a reactive extrusion process was explored as one such building block for creating renewable hydrogels. Starch was reactively extruded by EcoSynthetix Inc. to create starch nanoparticles (SNPs) that are attractive as hydrogel building blocks due to their inherent small size (25-50 nm), generally safe degradation products, overall net neutral charge, high deformability/viscoelastic properties, stability in solution without collapsing or changing size (on the order of months), and the ability to be manufactured at a multiple kg/hr rate; in comparison, other manufacturing methods of SNPs suffer from a lack of scalability or require the use of potentially toxic solvents, making them less amenable to biological or environmental/agricultural applications. The amorphous nature of the starch also allows for facile functionalization to further chemically modify and/or crosslink the SNPs through surface functional group (i.e. hydroxyl) modification chemistries. The nanoparticle nature of the SNP building block, coupled with the facile functionalizability of the SNPs, also makes SNPs ideal building blocks for the design and fabrication of nanoparticle network hydrogels (NNHs) in which NPs create an interconnected network on their own on, in addition to, other polymeric networks at any desired length scale. There are a variety of NNH architectures that can be achieved through careful design considerations. More specifically, herein colloidal NNHs were created using UV photopolymerization post-functionalization with methacrylic anhydride, which leaves a vinyl group on the SNP surface. Alternately, plum pudding NNHs were created by mixing aldehyde-functionalized SNPs with amine-bearing O-carboxymethyl chitosan that were able to chemically react via hydrolytically labile imine bonds. The properties of various types of colloidal and plum-pudding hydrogels based on SNPs were tested and subsequently compared through a range of different performance tests such as rheological and micromechanical force testing, swelling/degradation kinetics, their potential for controlled bioactive release, and overall toxicity (cell and organ level). In addition to these macroscopic performance tests, the internal morphologies of both colloidal and plum pudding NNHs were assessed with small angle and very small angle neutron scattering experiments to glean insight into how these internal structures correlate to macroscopic properties. For all experiments, the effect of using SNPs versus typical cold water-soluble branched starch (SS) was assessed to further understand the impact of making hydrogels from nanoscale rather than soluble polymer building blocks, with the small size of SNPs compared to the large hydrodynamic radius of SS consistently allowing for greater control over the range of potential hydrogel properties. The results of these studies suggest that SNP-based NNHs are promising materials for studying the encapsulation and release of small molecules in both in vitro and in vivo settings. For example, the photopolymerization of methacrylated SNP-based NNH coatings can be fabricated at much higher concentrations than possible with conventional starch (35% for SNP, 10% for SS), leading to denser and stiffer gels compared to SS controls albeit with slightly longer gelation times due to the reduced conformational mobility of the polymerizable methacrylate groups on the SNPs. The addition of charge (cationic or anionic) to the SNP surface further increases the bulk gelation time while significantly reducing the observed changes in SNP deformation during photogelation as confirmed via very small angle neutron scattering experiments. Other functional groups were also demonstrated to be introduced to SNPs to enable different types of gelation for different applications. For example, in situ-gelling and degradable bulk nanoparticle network hydrogels consisting of oxidized starch nanoparticles (SNPs) and carboxymethyl chitosan (CMCh) were created for intranasal delivery that could be delivered into the nose via a commercial atomization device to enable high nasal mucosal retention and functional controlled release of the peptide drug PAOPA, a positive allosteric modulator of dopamine D2 receptor. Selected gels shown to alleviate negative behavioural abnormalities associated with for up to 72 hours in pre-clinical rat models of schizophrenia at a low drug dosage (0.5 mg/kg), compared to just a few hours with the drug alone. Finally, the functionalization of SNPs with hydrophobic groups (via grafting the starch with octenyl succinic acid (OSAn) or succinic anhydride (SAn)) was demonstrated as a promising delivery system for agricultural applications. Hydrophobization increased the contact angle of a sprayed watermelon and pumpkin leaves from <60˚ (unmodified) to ~80˚ when modified (DS 0.25), while confocal fluorescence microscopy confirmed that the hydrophobized SNPs can both adhere to the leaf surface as well as penetrate into the leaves when sprayed due to their small size (25-50 nm). Future work will look at other methods of crosslinking SNPs (i.e. Michael addition, hydrazone, and alkyne-azide “click” chemistry, amongst others) to see if there are beneficial differences compared to analogous hydrogels made from macroscopic alternatives (i.e. polymers alone) and to follow-up the findings already gleaned within this thesis. Further information on the impact and potential follow-up experiments for the work conducted in this thesis will be explained in Chapter 6 on final outlooks and conclusions of the following work. / Thesis / Doctor of Philosophy (PhD) / This thesis describes the chemical and physical modification of commercially-available starch nanoparticles (SNPs) to rationally create novel hydrogel systems. These gel-like networks are made by chemically connecting starch nanoparticles (with sizes on the 10-8 m length scale) by introducing various reactive chemical groups onto the surface of SNPs, enabling the creation of hydrogels with well-defined structures, features, and properties. Careful selection of the crosslinking chemistry made it possible to tune hydrogel properties to specific application requirements, such as the targeted delivery of pharmaceuticals (including the intranasal delivery of antipsychotic drugs to the brain, a key technical challenge to improve the quality of life of patients with mental health challenges) and agrochemical agents or as an anti-fouling coating. The hydrogels created herein are attractive since they directly incorporate nanoscale particles generated from a sustainable source and are generally regarded as safe (GRAS) in terms of their degradation products once they break down, a rare trait for nanoparticles of this size. The existing industrial-scale production of the SNPs also enables facile scaling of these strategies for ultimate commercial translation.

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