CHANGES IN THE COORDINATION OF WALKING MOVEMENTS UNDER CONDITIONS OF CONSTANT AND VARIABLE SPEED

INTRODUCTION: A great number of scientific studies on the biomechanics of walking are available. In addition to the analysis of the time course of kinematic and dynamic quantities, increased efforts were made for the estimation of the muscle activities. It is common to use an average of the muscle activity patterns of several steps (Zwick (1993); Konrad/Tyry (1996)). This procedure presupposes constant external constraints, similar biomechanical curves and equal muscle activity patterns. Here arises the problem: How stable or variable is the movement coordination of single steps if a) the walking speed is constant and b) the walking speed is changed? METHODS: The investigations were carried out with three male sports students on a treadmill. As an example, the results of one subject (SR) will be represented in this presentation. Three walking speeds were selected which the subjects could realize as comfortable and below the point where running begins. The speeds for SR were 1.0 m/s (SR1), 2.0 m/s (SR2) and 2.2 m/s (SR3). The subjects walked for four minutes at each speed level. The breaks between the speed levels were used for relaxation. Muscle fatigue was thus minimized. By means of the SIMI-Motion movement analysis system and EMG-Telemetry system of Noraxon-Neurodata, two dimensional video analysis (50 s-1 and 200 s- 1) of the left side was carried out and the EMG signals of five muscles (m. biceps femoris, m. vastus medialis, m. rectus femoris, m. gastrocnemius, m. tibialis) were recorded synchronously. The cycles were divided in two phases (support and swing) on the basis of characteristics of the time courses of relative ankle velocity in relation to the hip. Due to high-speed video limitations, five cycles for SR1 and eight cycles for SR2 and SR3 could be analyzed. We applied the adaptive estimation of the momentary power of the EMG-signals for timedependent analysis of muscle activities (Grießbach, Schack et al., 1994)

Incentives of using the hydrodynamic invariant and sedimentation parameter for the study of naturally- and synthetically-based macromolecules in solution

The interrelation of experimental rotational and translational hydrodynamic friction data as a basis for the study of macromolecules in solution represents a useful attempt for the verification of hydrodynamic information. Such interrelation originates from the basic development of colloid and macromolecular science and has proven to be a powerful tool for the study of naturally- and synthetically-based, i.e., artificial, macromolecules. In this tutorial review, we introduce this very basic concept with a brief historical background, the governing physical principles, and guidelines for anyone making use of it. This is because very often data to determine such an interrelation are available and it only takes a set of simple equations for it to be established. We exemplify this with data collected over recent years, focused primarily on water-based macromolecular systems and with relevance for pharmaceutical applications. We conclude with future incentives and opportunities for verifying an advanced design and tailored properties of natural/synthetic macromolecular materials in a dispersed or dissolved manner, i.e., in solution. Particular importance for the here outlined concept emanates from the situation that the classical scaling relationships of Kuhn–Mark–Houwink–Sakurada, most frequently applied in macromolecular science, are fulfilled, once the hydrodynamic invariant and/or sedimentation parameter are established. However, the hydrodynamic invariant and sedimentation parameter concept do not require a series of molar masses for their establishment and can help in the verification of a sound estimation of molar mass values of macromolecules

Aqueous Redox Flow Battery Suitable for High Temperature Applications Based on a Tailor‐Made Ferrocene Copolymer

Abstract Water‐soluble, and ferrocene‐containing methacrylamide copolymers with different comonomer ratios of the solubility‐promoting comonomer [2‐(methacryloyloxy)‐ethyl]‐trimethylammonium chloride (METAC) are synthesized in order to obtain a novel, temperature‐stable electrolyte for aqueous redox flow batteries. The electrochemical properties of one chosen polymer are studied in detail by cyclic voltammetry and rotating disc electrode (RDE) investigations. Additionally, the diffusion coefficient and the charge transfer rate are obtained from these measurements. The diffusion coefficient from RDE is compared to the value from synthetic boundary experiments at battery concentrations, using an analytical ultracentrifuge, yielding diffusion coefficients of a similar order of magnitude. The polymer is further tested in a redox flow battery setup. While performing charge and discharge experiments against the well‐established bis ‐(trimethylammoniumpropyl)‐viologen, the polymer reveals high columbic efficiencies of >99.8% and desirable apparent capacity retention, both at room temperature as well as at 60 °C. Further experiments are conducted to verify the stability of the active compounds under these conditions in both charge states. Lastly, the electrochemical behavior is linked to the characteristics of the polymers concerning absolute values of the molar mass and diffusion coefficients.A new ferrocene containing monomer is synthesized and its copolymerization with a water‐solubility promoting comonomer is investigated. The electrochemical and solution characteristics of a corresponding polymer are studied in detail. With a coulombic efficiency of >99.8% in an aqueous redox flow battery setup at 60 °C, a cheap, robust system for use at elevated temperatures is presented. imag

A viologen polymer and a compact ferrocene: Comparison of solution viscosities and their performance in a redox flow battery with a size exclusion membrane

In this work, the synthesis and characterization of a compact, ferrocene tetramer and a linear viologen polymer is reported. The latter material is a new, 4,4′‐bipyridine containing, organo‐soluble polymer. As aimed for solubility in nonpolar solvents, a 2‐ethylhexyl‐moiety to promote organosolubility and 4‐vinylbenzyl serving as a polymerizable group are introduced to a 4,4′‐bipyridine. The halide anions of the monomer cation are exchanged to bis(trifluoromethansulfon)imide, which further enhances organosolubility. The monomer is subsequently copolymerized with styrene by free radical polymerization. In addition, a four‐ferrocene‐containing compact structure, based on pentaerythritol, is synthesized via the straightforward radical thiol‐ene reaction. The polymer solutions are thoroughly characterized hydrodynamically. Subsequently, propylene carbonate‐based solutions of both materials are prepared to allow an assessment for future energy storage applications. This is done by testing battery characteristics in a custom‐made flow‐cell with a simple dialysis membrane for physical separation of the active materials. The capability of energy storage is verified by leaving the charged materials in solution in an open circuit for 24 h. Here, more than 99% of the stored charges can be recovered. Cycling the battery for 100 times reveals the remarkable stability of the materials of only 0.2% capacity loss per day in the battery setup

Inadequate Clearance of Translocated Bacterial Products in HIV-Infected Humanized Mice

Bacterial translocation from the gut and subsequent immune activation are hallmarks of HIV infection and are thought to determine disease progression. Intestinal barrier integrity is impaired early in acute retroviral infection, but levels of plasma lipopolysaccharide (LPS), a marker of bacterial translocation, increase only later. We examined humanized mice infected with HIV to determine if disruption of the intestinal barrier alone is responsible for elevated levels of LPS and if bacterial translocation increases immune activation. Treating uninfected mice with dextran sodium sulfate (DSS) induced bacterial translocation, but did not result in elevated plasma LPS levels. DSS-induced translocation provoked LPS elevation only when phagocytic cells were depleted with clodronate liposomes (clodrolip). Macrophages of DSS-treated, HIV-negative mice phagocytosed more LPS ex vivo than those of control mice. In HIV-infected mice, however, LPS phagocytosis was insufficient to clear the translocated LPS. These conditions allowed higher levels of plasma LPS and CD8+ cell activation, which were associated with lower CD4+/CD8+ cell ratios and higher viral loads. LPS levels reflect both intestinal barrier and LPS clearance. Macrophages are essential in controlling systemic bacterial translocation, and this function might be hindered in chronic HIV infection

Stealth Effect of Short Polyoxazolines in Graft Copolymers: Minor Changes of Backbone End Group Determine Liver Cell-Type Specificity

Dye-loaded micelles of 10 nm diameter formed from amphiphilic graft copolymers composed of a hydrophobic poly(methyl methacrylate) backbone and hydrophilic poly(2-ethyl-2-oxazoline) side chains with a degree of polymerization of 15 were investigated concerning their cellular interaction and uptake in vitro as well as their interaction with local and circulating cells of the reticuloendothelial system in the liver by intravital microscopy. Despite the high molar mass of the individual macromolecules (Mn ≈ 20 kg mol-1), backbone end group modification by attachment of a hydrophilic anionic fluorescent probe strongly affected the in vivo performance. To understand these effects, the end group was additionally modified by the attachment of four methacrylic acid repeating units. Although various micelles appeared similar in dynamic light scattering and cryo-transmission electron microscopy, changes in the micelles were evident from principal component analysis of the Raman spectra. Whereas an efficient stealth effect was found for micelles formed from polymers with anionically charged or thiol end groups, a hydrophobic end group altered the micelles' structure sufficiently to adapt cell-type specificity and stealth properties in the liver. © 2021 The Authors. Published by American Chemical Society

Controlled ultraviolet (UV) photoinitiated fabrication of monolithic porous layer open tubular (monoPLOT) capillary columns for chromatographic applications

An automated column fabrication technique that is based on a ultraviolet (UV) light-emitting diode (LED) array oven, and provides precisely controlled "in-capillary" ultraviolet (UV) initiated polymerization at 365 nm, is presented for the production of open tubular monolithic porous polymer layer capillary (monoPLOT) columns of varying length, inner diameter (ID), and porous layer thickness. The developed approach allows the preparation of columns of varying length, because of an automated capillary delivery approach, with precisely controlled and uniform layer thickness and monolith morphology, from controlled UV power and exposure time. The relationships between direct exposure times, intensity, and layer thickness were determined, as were the effects of capillary delivery rate (indirect exposure rate), and multiple exposures on the layer thickness and axial distribution. Layer thickness measurements were taken by scanning electron microscopy (SEM), with the longitudinal homogeneity of the stationary phase confirmed using scanning capacitively coupled contactless conductivity detection (sC(4)D). The new automated UV polymerization technique presented in this work allows the fabrication of monoPLOT columns with a very high column-to-column production reproducibility, displaying a longitudinal phase thickness variation within ±0.8% RSD (relative standard deviation)

Targeted delivery of a phosphoinositide 3-kinase γ inhibitor to restore organ function in sepsis

Jaundice, the clinical hallmark of infection-associated liver dysfunction, reflects altered membrane organization of the canalicular pole of hepatocytes and portends poor outcomes. Mice lacking phosphoinositide 3-kinase-γ (PI3Kγ) are protected against membrane disintegration and hepatic excretory dysfunction. However, they exhibit a severe immune defect that hinders neutrophil recruitment to sites of infection. To exploit the therapeutic potential of PI3Kγ inhibition in sepsis, a targeted approach to deliver drugs to hepatic parenchymal cells without compromising other cells, in particular immune cells, seems warranted. Here, we demonstrate that nanocarriers functionalized through DY-635, a fluorescent polymethine dye, and a ligand of organic anion transporters can selectively deliver therapeutics to hepatic parenchymal cells. Applying this strategy to a murine model of sepsis, we observed the PI3Kγ-dependent restoration of biliary canalicular architecture, maintained excretory liver function, and improved survival without impairing host defense mechanisms. This strategy carries the potential to expand targeted nanomedicines to disease entities with systemic inflammation and concomitantly impaired barrier functionality