In contrast, vection occurred in only one direction (opposite to background motion) and developed later than VEPRs. The different time course and in-congruency between direction of VEPRs and direction of vection suggests that perceptual and postural responses H 89 solubility dmso are not causally related. However, since vection did increase VEPR magnitude in the direction of background motion, we postulate that VEPRs might be mediated by two different mechanisms: (1) a
short latency system, driven by transient visual stimuli and sensitive to visual geometry (parallax-no parallax), responsible for automatic postural sway adjustments and (2) a longer latency, vection-enhanced postural mechanism, related to the conscious perception of self-motion during longer duration (locomotor, vehicular) body displacements. (C) 2008 Published by Elsevier Ireland Ltd.”
“In previous work, we developed an 8-state nonlinear
dynamic model of the acute inflammatory response, including activated phagocytic cells, pro- and anti-inflammatory cytokines, and tissue damage, and calibrated it to data on cytokines from endotoxemic rats. In the interest of parsimony, the present work employed parametric sensitivity and local identifiability, analysis to establish a core set of parameters predominantly responsible for variability in model solutions. Parameter optimization, facilitated by varying only those parameters belonging to this core set, was used to identify NSC23766 an ensemble of parameter vectors, each representing an acceptable local optimum in terms of fit to experimental data. Individual models within this ensemble, characterized by their different parameter values, showed similar cytokine but diverse tissue damage behavior. A cluster analysis of the ensemble of models Masitinib (AB1010) showed the existence of a continuum of acceptable models, characterized by compensatory mechanisms and parameter changes. We calculated the direct correlations between the core set of model parameters and identified three mechanisms responsible for the conversion
of the diverse damage time courses to similar cytokine behavior in these models. Given that tissue damage level could be an indicator of the likelihood of mortality, our findings suggest that similar cytokine dynamics could be associated with very different mortality outcomes, depending on the balance of certain inflammatory elements. Published by Elsevier Ltd.”
“We examined the involvement of oxidative stress in neuronal cell death induced by taxol, a microtubule-stabilizing anti-cancer drug and investigated whether NADPH oxidase plays a role in taxol-induced neuronal cell death in mouse cortical cultures. Cell death was assessed by measuring lactate dehydrogenase in the bathing media after 24-h exposure to taxol. Taxol (30-1000 nM) induced the concentration-dependent neuronal death with apoptotic features.