Confocal Image-Based Computational Modeling of Nitric Oxide Transport in a Rat Mesenteric Lymphatic Vessel

Wilson, John 1988-

14 March 2013

The lymphatic system plays an important role in protein and solute transport as well as the immune system. Its functionality is vital to proper homeostasis and fluid balance. Lymphatic fluid (lymph) may be propelled by intrinsic (active) vessel pumping or passively. With regard to the former, nitric oxide (NO) is known to play an important role in lymphatic vessel contraction and vasodilation. Lymphatic endothelial cells (LECs) are sensitive to shear and increases in flow have been shown to cause enhanced production of NO by LECs. Additionally, high concentrations of NO have been experimentally observed in the sinus region of mesenteric lymphatic vessels. The goal of this work was to develop a computational flow and mass transfer model using physiologic geometries obtained from confocal images of a rat mesenteric lymphatic vessel to determine the characteristics of NO transport in the lymphatic flow regime. Both steady and unsteady analyses were performed. Steady models were simulated by prescribing fully developed velocity profiles ranging from 0.5 mm s^-1 to 7 mm s^-1 as the inlet boundary conditions. Unsteady simulations were generated using a velocity profile taken from experimental data from in situ experiments with rats. Production of NO was shear-dependent; basal cases using constant production were also generated. Simulations revealed areas of flow stagnation adjacent to the valve leaflets, suggesting the high concentrations observed here experimentally are due to lack of convection in this region. LEC sensitivity was found to alter the concentration of NO in the vessel, and the convective forces were found to profoundly affect the concentration of NO at a Peclet value greater than or equal to approximately 61. The quasi-steady analysis was able to resolve wall shear stress within 0.15% of the unsteady case. However, the percent error between unsteady and quasi-steady conditions was higher for NO concentration (approximately 6.7%).

mass transport

lymphatic

CFD

nitric oxide

Characterization of oxygen and carbon effects in silicon material and MOSFET devices

Haddad, Homayoon

20 February 1990

Graduation date: 1990

Silicon

Gene Therapy for Endothelial Progenitor Cell Dysfunction

Ward, Michael Robert

23 February 2010

Endothelial progenitor cells (EPCs) have reduced neovascularization capacity in the context of coronary artery disease (CAD) or cardiac risk factors (RFs). Since, endothelial NO synthase (eNOS) is critical to normal EPC function, we hypothesized that bone marrow cells (BMCs) from rats with RFs and EPCs from humans with CAD and/or RFs show dramatically reduced neovascularization capacity in vitro and in vivo, which can be reversed by eNOS overexpression. BMCs were isolated from rat models of type II diabetes and the metabolic syndrome, and we showed a significant reduction in their ability to stimulate neovascularization in vitro and in vivo. In humans, we isolated circulating ‘early EPCs’ from healthy subjects and patients with CAD and RFs, and transduced them using lentiviral vectors containing either eNOS or GFP (sham). EPCs from patients had reduced in vitro migration in response to SDF-1 or VEGF, which was reversed by eNOS-transduction. In co-culture with human umbilical vein endothelial cells (HUVECs) on Matrigel, eNOS-transduced EPCs contributed to increased and more complex angiogenic tube formation compared to sham-transduced cells. Human EPCs from patients were ineffective in enhancing ischemic hind limb neovascularization and perfusion in a nude mouse, whereas eNOS-transduced EPCs resulted in a significant improvement compared to sham-transduced cells. In a swine model of acute myocardial infarction (MI), eNOS- and non-transfected BMCs both increased left ventricular function compared to sham. However, there was no benefit to eNOS overexpression in this model. Various differences in the models and procedures may explain the incongruous results obtained. Taken together, these results show that eNOS overexpression significantly improves the neovascularization capacity of EPCs of human subjects with CAD and RFs and could represent an effective adjunctive approach for the improvement of autologous cell therapies for cardiovascular disease.

cardiovascular disease

cell therapy

nitric oxide

0564

Vasculoprotective Effects of Insulin and Resveratrol In Vivo

Breen, Danna

23 February 2011

Atherosclerosis is a leading cause of morbidity and mortality worldwide and type 2 diabetes and obesity-associated metabolic syndrome, both characterized by insulin resistance, are potent risk factors. These conditions also increase the risk for restenosis after revascularization procedures used for treatment of atherosclerosis. Studies have shown that insulin and resveratrol (RSV), a red wine polyphenol, decrease neointimal growth after vessel injury in models of restenosis, demonstrating a protective effect on the vasculature. However, oral glucose and sucrose were used in insulin studies to maintain normoglycemia, and their effect on neointimal formation was not assessed. Several studies have shown that nitric oxide (NO) production is stimulated by insulin and RSV, and since NO can decrease neointimal growth, the objective of this thesis was to address the mechanism of action of insulin or RSV to protect against restenosis, and determine whether NO production mediates these effects. To examine this, we treated rats with insulin or RSV and performed arterial balloon injury. In Study 1, insulin reduced neointimal area after injury in rats receiving oral glucose but not oral sucrose. Oral glucose alone had no effect on neointimal formation or insulin sensitivity whereas oral sucrose increased neointimal growth and induced insulin resistance. In Study 2, insulin decreased neointimal area and cell migration, and increased re-endothelialization. These effects were abolished by nitric oxide synthase (NOS) inhibition. In addition, insulin increased eNOS protein expression in the vessel. In Study 3, RSV reduced neointimal growth, cell proliferation, and migration after injury, without affecting re-endothelialization. Most of these effects were abolished by NOS inhibition, except for the decrease in cell migration. Insulin sensitivity and systolic blood pressure were not affected by RSV. Together, the results demonstrate that insulin, independent of glycemic effects, and RSV have a protective effect on the vessel against restenosis, which is mediated by NO. Since both insulin and RSV decrease neointimal formation without negatively impacting re-endothelialization, insulin or RSV treatment could provide some advantage over anti-mitogenic agents currently used in drug-eluting stents, which delay re-endothelialization. These studies suggest that insulin or RSV may have clinical potential in the prevention of restenosis after angioplasty.

insulin

resveratrol

nitric oxide

restenosis

0719

Graphite Oxide: Structure, Reduction and Applications

Gao, Wei

05 September 2012

This thesis proposes a modified structure model for graphite oxide (GO), an important precursor in graphene chemistry, develops a new strategy to convert GO back to graphene-like structure, and demonstrates its possible applications in both water purification and supercapacitor technologies. GO, a nontraditional compound first obtained from graphite oxidation over 150 years ago, is now becoming an important player in the production of graphene-based materials, which has high technological relevance. GO structure and reduction have been vigorously investigated, but its precise chemical structure still remains obscure, and the complete restoration of the sp2 carbon lattice has not yet been achieved. In our work, solid state 13C NMR (MAS) analysis offered a piece of evidence for five or six-membered ring lactol structure existing in GO that had never been assigned before, leading to a modified Lerf-Klinowski model for GO. A three-step reduction strategy, involving sodium borohydride (NaBH4), sulfuric acid, and high temperature thermal annealing, described in the thesis, successfully reduced GO back to chemically converted graphene (CCG) with the lowest heteroatom abundance among all those previously reported. In addition to the chemical significance of graphene/CCG production, GO and its derivatives were used as novel adsorbents in water purification. GO-coated sand showed higher retention than ordinary sand for both Rhodamine B and mercuric ion (Hg2+) contaminants in water. Further functionalization of GO with thiophenol resulted in better adsorption capacity toward Hg2+ than that of activated carbon. In addition, free-standing films of GO were treated and reduced with a CO2 laser beam into different conductive reduced GO (RGO) patterns, and directly used as supercapacitor devices which showed good cyclic stability and energy storage capacities comparable to that of existing thin film ultracapacitors. GO turned out to be a solid electrolyte with anisotropic proton conductivity similar to Nafion, while the large amount of trapped water in GO played an important role.

Graphite Oxide

water purification

reduction

supercapacitors.

Surface Functionalization of Graphene-based Materials

Mathkar, Akshay

16 September 2013

Graphene-based materials have generated tremendous interest in the past decade. Manipulating their characteristics using wet-chemistry methods holds distinctive value, as it provides a means towards scaling up, while not being limited by yield. The majority of this thesis focuses on the surface functionalization of graphene oxide (GO), which has drawn tremendous attention as a tunable precursor due to its readily chemically manipulable surface and richly functionalized basal plane. Firstly, a room-temperature based method is presented to reduce GO stepwise, with each organic moiety being removed sequentially. Characterization confirms the carbonyl group to be reduced first, while the tertiary alcohol is reduced last, as the optical gap decrease from 3.5 eV down to 1 eV. This provides greater control over GO, which is an inhomogeneous system, and is the first study to elucidate the order of removal of each functional group. In addition to organically manipulating GO, this thesis also reports a chemical methodology to inorganically functionalize GO and tune its wetting characteristics. A chemical method to covalently attach fluorine atoms in the form of tertiary alkyl fluorides is reported, and confirmed by MAS 13C NMR, as two forms of fluorinated graphene oxide (FGO) with varying C/F and C/O ratios are synthesized. Introducing C-F bonds decreases the overall surface free energy, which drastically reduces GO’s wetting behavior, especially in its highly fluorinated form. Ease of solution processing leads to development of sprayable inks that are deposited on a range of porous and non-porous surfaces to impart amphiphobicity. This is the first report that tunes the wetting characteristics of GO. Lastly as a part of a collaboration with ConocoPhillips, another class of carbon nanomaterials - carbon nanotubes (CNTs), have been inorganically functionalized to repel 30 wt% MEA, a critical solvent in CO2 recovery. In addition to improving the solution processability of CNTs, composite, homogeneous solutions are created with polysulfones and polyimides to fabricate CNT-polymer nanocomposites that display contact angles greater than 150o with 30 wt% MEA. This yields materials that are inherently supersolvophobic, instead of simply surface treating polymeric films, while the low density of fluorinated CNTs makes them a better alternative to superhydrophobic polymer materials.

graphene oxide

wetting

carbon nanotubes

functionalization

Electromechanical Coupling of Graphene With Cells

Kempaiah, Ravindra

04 August 2011

Nanomaterials have been studied extensively in the last decade in the context of many applications such as polymer composites, energy harvesting systems, sensors, ‘transparent’-like materials, field-effect transistors (FETs), spintronic devices, gas sensors and biomedical applications. Graphene, a recently discovered two-dimensional form of carbon has captured the interest of material scientists, and physicists alike due to its excellent electrical, mechanical and thermal properties. Graphene has also kindled a tremendous interest among chemists and cell biologists to create cellular-electronic interface in the context of bio-electronic devices as it can enable fabricating devices with enhanced potential as compared to conventional bio-electronics. Graphene’s unique electronic properties and sizes comparable with biological structures involved in cellular communication makes it a promising nanostructure for establishing active interfaces with biological systems. In the recent past Field effect transistors (FETs) have been successfully fabricated using carbon nanotubes (CNTs) and nanowires (NWs) and electrical characterization of these FETs were done by interfacing them with various cell cultures, tissues and muscle cells. In these cases, exceptionally high surface area to thickness ratio of FETs provides high percentage of collectible signals and the cells that are used for the study are typically placed on the FET. In this thesis, we examine a different approach towards forming bio-electronic interfaces by covering the graphene oxide (reduced) sheets on the yeast cells. Graphene oxide and reduced graphene oxide sheets as two-dimensional electronic materials have very high charge carrier mobility, extremely high surface area to thickness ratio, mechanical modulus and elasticity. We report the synthesis of graphene oxide using wet chemistry method, reduction of graphene oxide using different reducing agents and electrical characterization of graphene oxide’s conductivity. Micro-meter sized graphene sheets are used to encapsulate the yeast cells with the aid of calcium and gold nanoparticle chains. We also demonstrate that graphene sheets form electrically conductive layers on the yeast cells and developing an electromechanical coupling with the cell. The mechanical and electrical characteristics of graphene sheets are highly dependent on the cell volume and structure which are in turn related to the environment around the cell. Furthermore, using the same principle of electromechanical coupling we study the dynamics of cell surface stresses and cell volume modification, which are of importance in processes such as cell growth, division, and response to physiological factors such as osmotic stresses.

Graphene, cellular coupling

graphene oxide

Chemistry

Metal oxide-facilitated oxidation of antibacterial agents

Zhang, Huichun

08 July 2004

Metal oxide-facilitated transformation is likely an important degradation pathway of antibacterial agents at soil-water interfaces. Phenolic disinfectants (triclosan and chlorophene), fluoroquinolones (FQs), and aromatic N-oxides are of particular concern due to their widespread usage, potential toxicity and frequent detection in the environment. Results of the present study show that the above antibacterial agents are highly susceptible to metal oxide-facilitated oxidation. The interfacial reactions exhibit complex reaction kinetics, which are affected by solution pH, the presence of co-solutes, surface properties of metal oxides, and structural characteristics of antibacterial agents. Adsorption of the antibacterial agents to Mn and Fe oxide surfaces generally proceeds faster than oxidation reactions of these compounds by Mn and Fe oxides, especially in the case of Fe oxides. Reaction intermediates and end products are identified by GC/MS, LC/MS and/or FTIR. Structurally-related model compounds are examined to facilitate reaction site and mechanism elucidation. On the basis of experimental results and literature, reaction schemes are proposed. In general, the antibacterial agent is adsorbed to the oxide surface, forming a precursor complex. Electrons are transferred within the precursor complex from the antibacterial agent to the oxide, followed by releasing of the radical intermediates which undergo further reactions to generate oxidation products. The precursor complex formation and electron transfer are likely rate-limiting. For triclosan, phenoxy radicals are critical intermediates to form oxidation products through three pathways (i.e., radical coupling, further oxidation of the radical, and breakdown of an ether bond within the radical). The first two pathways are also operative in the oxidation of chlorophene. For FQs, oxidation generates radical intermediates that are most likely centered on the inner N in the piperazine ring. The radical intermediates then undergo three major pathways (i.e., radical coupling, N-dealkylation, and hydroxylation) to yield a variety of products. For aromatic N-oxides, a N-oxide radical intermediate is generated upon oxidation by MnO2, followed by the loss of oxygen from the N-oxide moiety and the formation of a hydroxyl group at the C-atom adjacent to the N-oxide moiety. Overall, a fundamental understanding of the reaction mechanisms between three classes of antibacterial agents and metal oxides has been obtained.

Reaction mechanisms

Kinetics

Oxidation

Antibacterial agents

Fe oxide

Mn oxide

Aromatic N-oxides

Fluoroquinolones

Chlorophene

Triclosan

Reaction mechanisms (Chemistry)

Antibacterial agents

Ferrous oxide

Manganese oxide

Metallic oxides

Oxidation

Tetrahydrobiopterin Oxidation and Reactive Oxygen Species Contribute to H2O2-Induced Endothelial Nitric Oxide Synthase Dysfunction

Boulden, Beth Michelle

17 May 2005

An oxidative stress in the form of H2O2 exposure previously has been shown to cause a transient increase in NO??oduction and a chronic increase in eNOS protein levels. Nevertheless, oxidative stress can cause an uncoupling of catalytic activity resulting in decreased NO??d increased O2??roduction from eNOS. This uncoupling seems to be mediated predominantly by oxidation of tetrahydrobiopterin (BH4), an eNOS required cofactor. To study how these phenomena regulate the physiological balance of reactive oxygen species (ROS), H2O2-induced NO??oduction was measured in bovine aortic endothelial cells (BAECs) using an NO??ecific electrode. Following H2O2 exposure, NO??ncentrations initially increased; however, if cells were challenged a second time with H2O2, the increase in NO??oduction was attenuated. We postulated that the decline in NO??oduction after H2O2 exposure resulted from BH4 oxidation and tested this by supplementing cells with BH4 prior to the second H2O2 exposure. This resulted in a recovery of NO??oduction. Since H2O2 also activates NADPH oxidase to produce superoxide (O2?? we tested whether the decrease in NO??oduction during the second H2O2 exposure could be explained by increased NADPH oxidase-dependent oxygen free radical production, including O2??peroxynitrite (ONOO-), and hydroxyl radicals (??. A reduction in H2O2-induced NO??lease was prevented in apocynin-and PEG-SOD-treated cells and in p47phox-knockout mouse aortic endothelial cells (MAECs), which lack a critical subunit of the NADPH oxidase. These results suggest that O2??roduced by NADPH oxidase leads to eNOS dysfunction. Scavenging ONOO- resulted in a full recovery of NO??oduction, and scavenging ??resulted in a partial recovery of NO??oduction. This implies roles for these O2??erivatives in the reduced NO??sponse to repeated H2O2 exposures.

Electrochemical nitric oxide detection

Cardiovascular disease

High frequency voltage controlled ring oscillators in standard CMOS

Eken, Yalcin Alper

07 June 2004

No description available.

Metal oxide semiconductors

Complementary

Oscillators

Crystal