Multi-Structure Turbulence in a Boundary Layer with a Uniformly Sheared Free Stream

Livingston, Curtis

02 September 2020

A turbulent boundary layer (TBL), generated in a water tunnel, extended to a highly turbulent and anisotropic “free stream” that consisted of a uniformly sheared flow (USF) with a mean shear that was in the opposite direction to that in the TBL. Extensive measurements of the fluctuating velocity were taken with the use of hot-film anemometry, laser Doppler velocimetry and particle image velocimetry. On either side of the TBL edge, defined as the location of maximum velocity, the turbulence relaxed to its canonical structures in TBL and USF, respectively, but, in the vicinity of the edge, the turbulence was multi-structure and exhibited strong departures from canonical behaviour. Of particular interest was the variation of the dissipation parameter, which, in contrast to its near-constancy in well-developed canonical flows, varied inversely proportionally to the turbulence Reynolds number. The entire flow contained horseshoe-shaped coherent structures, whose properties, however, varied from the TBL, across the multi-structure region and into the USF.

Turbulence

Turbulent Boundary Layer

Uniformly sheared flow

Multi-structure

Méthodes numériques pour problèmes d'interaction fluide-structure avec valves

Diniz Dos Santos, Nuno

11 December 2007

Cette thèse est motivée par la modélisation et la simulation numérique des phénomènes d'interaction fluide-structure autour de valves cardiaques. L'interaction avec la paroi des vaisseaux est traitée avec une formulation Arbitraire Lagrange Euler (ALE), tandis que l'interaction avec les valves est traitée à l'aide de multiplicateurs de Lagrange, dans une formulation de type Domaines Fictifs (FD). Après une présentation de synthèse des diverses méthodes utilisées en interaction fluide-structure dans les écoulements sanguins, nous décrivons une méthode permettant de simuler la dynamique d'une valve immergée dans un écoulement visqueux incompressible. L'algorithme de couplage est partionné, ce qui permet de conserver des solveurs fluides et structures indépendants. Le maillage du fluide est mobile pour suivre la paroi des vaisseaux, mais indépendant du maillage des valves. Ceci autorise des très grands déplacements sans nécessiter de remaillage. Nous proposons une stratégie pour gérer le contact entre plusieurs valves. L'algorithme est totalement indépendant des solveurs de structures et est bien adapté au couplage fluide-structure partionné. Enfin, nous proposons un schéma de couplage semi-implicite permettant de mêler efficacement les formulations ALE et FD. Toutes les méthodes considérées sont accompagnées de nombreux tests numériques en 2D et 3D.

[MATH] Mathematics

Valves

interaction fluide structure

Arbitraire Lagrange Euler

Domaines Fictifs

multiplicateurs de Lagrange

algorithme de couplage partitionné

contact multi-structure

couplage semi-implicite

Méthodes numériques pour problèmes d'interaction fluide structure avec valves

Diniz Dos Santos, Nuno

11 December 2007

Cette thèse est motivée par la modélisation et la simulation numérique des phénomènes d'interaction fluide-structure autour de valves cardiaques. L'interaction avec la paroi des vaisseaux est traitée avec une formulation Arbitraire Lagrange Euler (ALE), tandis que l'interaction avec les valves est traitée à l'aide de multiplicateurs de Lagrange, dans une formulation de type Domaines Fictifs (FD). Après une présentation de synthèse des diverses méthodes utilisées en interaction fluide-structure dans les écoulements sanguins, nous décrivons une méthode permettant de simuler la dynamique d'une valve immergée dans un écoulement visqueux incompressible. L'algorithme de couplage est partitionné, ce qui permet de conserver des solveurs fluides et structures indépendants. Le maillage du fluide est mobile pour suivre la paroi des vaisseaux, mais indépendant du maillage des valves. Ceci autorise des très grands déplacements sans nécessiter de remaillage. Nous proposons une stratégie pour gérer le contact entre plusieurs valves. L'algorithme est totalement indépendant des solveurs de structures et est bien adapté au couplage fluide-structure partitionné. Enfin, nous proposons un schéma de couplage semi-implicite permettant de mêler efficacement les formulations ALE et FD. Toutes les méthodes considérées sont accompagnées de nombreux tests numériques en 2D et 3D.

Valves

interaction fluide structure

Arbitraire Lagrange Euler

Domaines Fictifs

multiplicateurs de Lagrange

algorithme de couplage partitionné

contact multi-structure

couplage semi-implicite

Step-growth thiol-ene photopolymerization to form degradable, cytocompatible and multi-structural hydrogels

Shih, Han

17 January 2014

Indiana University-Purdue University Indianapolis (IUPUI) / Hydrogels prepared from photopolymerization have been used for a variety of tissue engineering and controlled release applications. Polymeric biomaterials with high cytocompatibility, versatile degradation behaviors, and diverse material properties are particularly useful in studying cell fate processes. In recent years, step-growth thiol-ene photochemistry has been utilized to form cytocompatible hydrogels for tissue engineering applications. This radical-mediated gelation scheme utilizes norbornene functionalized multi-arm poly(ethylene glycol) (PEGNB) as the macromer and di-thiol containing molecules as the crosslinkers to form chemically crosslinked hydrogels. While the gelation mechanism was well-described in the literature, the network properties and degradation behaviors of these hydrogels have not been fully characterized. In addition, existing thiol-ene photopolymerizations often used type I photoinitiators in conjunction with an ultraviolet (UV) light source to initiate gelation. The use of cleavage type initiators and UV light often raises biosafety concerns. The first objective of this thesis was to understand the gelation and degradation properties of thiol-ene hydrogels. In this regard, two types of step-growth hydrogels were compared, namely thiol-ene hydrogels and Michael-type addition hydrogels. Between these two step-growth gel systems, it was found that thiol-ene click reactions formed hydrogels with higher crosslinking efficiency. However, thiol-ene hydrogels still contained significant network non-ideality, demonstrated by a high dependency of hydrogel swelling on macromer contents. In addition, the presence of ester bonds within the PEGNB macromer rendered thiol-ene hydrogels hydrolytically degradable. Through validating model predictions with experimental results, it was found that the hydrolytic degradation of thiol-ene hydrogels was not only governed by ester bond hydrolysis, but also affected by the degree of network crosslinking. In an attempt to manipulate network crosslinking and degradation rate of thiol-ene hydrogels, different macromer contents and peptide crosslinkers with different amino acid sequences were used. A chymotrypsin-sensitive peptide was also used as part of the hydrogel crosslinkers to render thiol-ene hydrogels enzymatically degradable. The second objective of this thesis was to develop a visible light-mediated thiol-ene hydrogelation scheme using a type II photoinitiator, eosin-Y, as the only photoinitiator. This approach eliminates the incorporation of potentially cytotoxic co-initiator and co-monomer that are typically used with a type II initiator. In addition to investigating the gelation kinetics and properties of thiol-ene hydrogels formed by this new gelation scheme, it was found that the visible light-mediated thiol-ene hydrogels were highly cytocompatible for human mesenchymal stem cells (hMSCs) and pancreatic MIN6 beta-cells. It was also found that eosin-Y could be repeatedly excited for preparing step-growth hydrogels with multilayer structures. This new gelation chemistry may have great utilities in controlled release of multiple sensitive growth factors and encapsulation of multiple cell types for tissue regeneration.

hydrogel

biomaterial

degradation

multi-structure

photopolymerization

thiol-ene chemistry

Glycoconjugates -- Research

Polyethylene glycol -- Biotechnology

Photopolymerization -- Analysis

Biodegradation

Ultraviolet radiation

Polymers -- Effect of radiation on

Biotechnology -- Safety measures

Hydrolases

Peptides -- Synthesis

Eosin -- Research

Mesenchymal stem cells

Pancreatic beta cells

Biomimetic materials