Knowing your boundaries: no effect of tool-use on body representation following a gather-and-sort task.

Internal representations of the body have received considerable attention in recent years, particularly in the context of tool-use. Results have supported the notion that these representations are plastic and tool-use engenders an extension of the internal representation of the arm. However, the limitations of the literature underlying this tool embodiment process have not been adequately considered or tested. For example, there is some evidence that tool-use effects do not extend beyond simplistic tool-use tasks. To further clarify this issue, 66 participants engaged in a period of tool-augmented reaches in a speeded gather-and-sort task. If task characteristics inherent to simplistic tasks are relevant to putative embodiment effects, it was predicted that there would be no effect of tool-use on tactile distance judgments or forearm bisections. A Bayesian analysis found considerable support for the null hypothesis in both outcome measures, suggesting that some of the evidence for tool embodiment may be based in task characteristics inherent in the narrow range of tool-use tasks used to study them, rather than a tool incorporation process. Potential sources of influence stemming from these characteristics are discussed.

Are tools truly incorporated as an extension of the body representation?: Assessing the evidence for tool embodiment.

The predominant view on human tool-use suggests that an action-oriented body representation, the body schema, is altered to fit the tool being wielded, a phenomenon termed tool embodiment. While observations of perceptual change after tool-use purport to support this hypothesis, several issues undermine their validity in this context, discussed at length in this critical review. The primary measures used as indicators of tool embodiment each face unique challenges to their construct validity. Further, the perceptual changes taken as indicating extension of the body representation only appear to account for a fraction of the tool's size in any given experiment, and do not demonstrate the covariance with tool length that the embodiment hypothesis would predict. The expression of tool embodiment also appears limited to a narrow range of tool-use tasks, as deviations from a simple reaching paradigm can mollify or eliminate embodiment effects altogether. The shortcomings identified here generate important avenues for future research. Until the source of the kinematic and perceptual effects that have substantiated tool embodiment is disambiguated, the hypothesis that the body representation changes to fit tools during tool-use should not be favored over other possibilities such as the formation of separable internal tool models, which seem to offer a more complete account of human tool-use behaviors. Indeed, studies of motor learning have observed analogous perceptual changes as aftereffects to adaptation despite the absence of handheld tool-use, offering a compelling alternative explanation, though more work is needed to confirm this possibility.

Goal-directed aiming under restricted viewing conditions with confirmatory sensory feedback.

A substantial body of research has examined the speed-accuracy tradeoff captured by Fitts' law, demonstrating increases in movement time that occur as aiming tasks are made more difficult by decreasing target width and/or increasing the distance between targets. Yet, serial aiming movements guided by internal spatial representations, rather than by visual views of targets have not been examined in this manner, and the value of confirmatory feedback via different sensory modalities within this paradigm is unknown. Here we examined goal-directed serial aiming movements (tapping back and forth between two targets), wherein targets were visually unavailable during the task. However, confirmatory feedback (auditory, haptic, visual, and bimodal combinations of each) was delivered upon each target acquisition, in a counterbalanced, within-subjects design. Each participant performed the aiming task with their pointer finger, represented within an immersive virtual environment as a 1 cm white sphere, while wearing a head-mounted display. Despite visual target occlusion, movement times increased in accordance with Fitts' law. Though Fitts' law captured performance for each of the sensory feedback conditions, the slopes differed. The effect of increasing difficulty on movement times was least influential in the haptic condition, suggesting more efficient processing of confirmatory haptic feedback during aiming movements guided by internal spatial representations.

Analytical calculation of two-dimensional spectra.

We demonstrate an analytical calculation of two-dimensional (2D) coherent spectra of electronic or vibrational resonances. Starting with the solution to the optical Bloch equations for a two-level system in the 2D time domain, we show that a fully analytical 2D Fourier transform can be performed if the projection-slice and Fourier-shift theorems of Fourier transforms are applied. Results can be fit to experimental 2D coherent spectra of resonances with arbitrary inhomogeneity.

Platelet-mediated changes to neuronal glutamate receptor expression at sites of microthrombosis following experimental subarachnoid hemorrhage.

OBJECT: Glutamate is important in the pathogenesis of brain damage after cerebral ischemia and traumatic brain injury. Notably, brain extracellular and cerebrospinal fluid as well as blood glutamate concentrations increase after experimental and clinical trauma. While neurons are one potential source of glutamate, platelets also release glutamate as part of their recruitment and might mediate neuronal damage. This study investigates the hypothesis that platelet microthrombi release glutamate that mediates excitotoxic brain injury and neuron dysfunction after subarachnoid hemorrhage (SAH). METHODS: The authors used two models, primary neuronal cultures exposed to activated platelets, as well as a whole-animal SAH preparation. Propidium iodide was used to evaluate neuronal viability, and surface glutamate receptor staining was used to evaluate the phenotype of platelet-exposed neurons. RESULTS: The authors demonstrate that thrombin-activated platelet-rich plasma releases glutamate, at concentrations that can exceed 300 µM. When applied to neuronal cultures, this activated plasma is neurotoxic, and the toxicity is attenuated in part by glutamate receptor antagonists. The authors also demonstrate that exposure to thrombin-activated platelets induces marked downregulation of the surface glutamate receptor glutamate receptor 2, a marker of excitotoxicity exposure and a possible mechanism of neuronal dysfunction. Linear regression demonstrated that 7 days after SAH in rats there was a strong correlation between proximity to microthrombi and reduction of surface glutamate receptors. CONCLUSIONS: The authors conclude that platelet-mediated microthrombosis contributes to neuronal glutamate receptor dysfunction and might mediate brain injury after SAH.

Pressure-induced transition from an antiferromagnet to a ferrimagnet for Mn(II)(TCNE)[C4(CN)8]1/2 (TCNE = tetracyanoethylene).

Mn(II)(TCNE)[C(4)(CN)(8)](1/2) (TCNE = tetracyanoethylene) exhibits a reversible pressure-induced piezomagnetic transition from a low magnetization antiferromagnetic state to a high magnetization ferrimagnetic state above 0.50 ± 0.15 kbar. In the ferrimagnetic state, the critical temperature, T(c), increases with increasing hydrostatic pressure and is ~97 K at 12.6 kbar, the magnetization increases by 3 orders of magnitude (1000-fold), and the material becomes a hard magnet with a significant remnant magnetization.

Unusually long, multicenter, cation(δ+)···anion(δ-) bonding observed for several polymorphs of [TTF][TCNE].

The α, ß, and δ polymorphs of [TTF][TCNE] (TTF=tetrathiafulvalene; TCNE=tetracyanoethylene) exhibit a new type of long, multicenter bonding between the [TTF](δ+) and [TCNE](δ-) moieties, demonstrating the existence of long, hetero-multicenter bonding with a cationic(δ+)···anionic(δ-) zwitterionic-like structure. These diamagnetic π-[TTF](δ+) [TCNE](δ-) heterodimers exhibit a transfer of about 0.5 e(-) from the TTF to the TCNE fragments, as observed from experimental studies, in accord with theoretical predictions, that is, [TTF(δ+)···TCNE(δ-)] (δ≅0.5). They have several interfragment distances <3.4 Å, and a computed interaction energy of -21.2 kcal mol(-1), which is typical of long, multicenter bonds. The lower stability of [TTF](δ+) [TCNE](δ-) with respect to typical ionic bonds is due, in part, to the partial electron transfer that reduces the electrostatic bonding component. This reduced electrostatic interaction, and the large interfragment dispersion stabilize the long, heterocationic/anionic multicenter interaction, which in [TTF(δ+)···TCNE(δ-)] always involves two electrons, but have ten, eight, and eight bond critical points (bcps) involving C-C, N-S, and sometimes C-S and C-N components for the α, ß, and δ polymorphs, respectively. In contrast, γ-[TTF][TCNE] possesses [TTF](2)(2+) and [TCNE](2)(2-) dimers, each with long, homo-multicenter 2e(-)/12c (c=center, 2 C+4 S) [TTF](2)(2+) cationic(+)···cationic(+) bonds, as well as long, homo-multicenter 2e(-)/4c [TCNE](2)(2-) anionic(-)···anionic(-) bonding. The MO diagrams for the α, ß, and δ polymorphs have all of the features found for conventional covalent C-C bonds, and for all of the previously studied multicenter long bonds, for example, π-[TTF](2)(2+) and π-[TCNE](2)(2-). The HOMOs for α-, ß-, and δ-[TTF][TCNE] have 2c C-S and 3c C-C-C orbital-overlap contributions between the [TTF](δ+-) and [TCNE](δ-) moieties; these are the shortest intra [TTF···TCNE] separations. Thus, from an orbital-overlap perspective, the bonding has 2c and 3c components residing over one S and four C atoms.

Solid-State NMR spectra and long, intra-dimer bonding in the pi-[TTF](2)(2+) (TTF = tetrathiafulvalene) dication.

The (13)C chemical-shift tensor principal values for TTF and pi-[TTF](2)(2+) (TTF = tetrathiafulvalene) dimer dications have been measured in order to better understand the electronic structure and long intradimer bonding of these TTF-based dimer structures. The structure of pi-[TTF](2)(2+) is abnormal due to its two C-C and four S-S ca. 3.4 A intradimer separations, which is less than the sum of the sulfur van der Waals radii, and has a singlet (1)A(1g) electronic ground state. This study of TTF and [TTF](2)(2+) was conducted to determine how the NMR chemical-shift tensor principal values change as a function of electronic structure. This study also establishes a better understanding of the interactions that lead to spin-pairing of the monomeric radical units. The density functional theory (DFT) calculated nuclear shielding tensors are correlated with the experimentally determined principal chemical-shift values. The embedded ion method (EIM) was used to investigate the electrostatic lattice potential in [TTF](2)(2+). These theoretical methods provide information on the tensor magnitudes and orientations of their tensor principal values with respect to the molecular frame. The experimental chemical-shift principal values agree with the calculated quantum mechanical chemical-shielding principal values, within typical errors commonly seen for this class of molecular system. Relatively weak Wiberg bond orders between the two [TTF](+) components of the dimer dication correlate with the long bonds linking the two [TTF](+) monomers and substantiate the claim that there is weak multicenter bonding present.

An analysis of regional microvascular loss and recovery following two grades of fluid percussion trauma: a role for hypoxia-inducible factors in traumatic brain injury.

Secondary hypoxic/ischemic injuries, stemming from reductions in cerebral blood flow are important contributing factors in progressive neuronal dysfunction after brain trauma. A greater preclinical understanding of how brain trauma leads to secondary hypoxia/ischemia is necessary in the development of posttraumatic brain injury (TBI) therapeutics. To this end, we examined the density of microvascular coverage in the injured and contralateral cortical hemispheres using two intensities of fluid percussion trauma in rats. A silicone microangiography technique showed a significant loss in microvascular density in 2 atmosphere (atm) (16.9+/-3.8%) and 3 atm (15.7+/-1.3%) injured animals relative to sham animals (29.9+/-2.5%; P<0.01). RECA-1 immunohistochemistry indicated that capillary changes involved a reduction in capillary number and diameter. Reduction in microvascular density was shown to be a diffuse phenomenon occurring up to 4 mm rostral and caudal to the injury epicenter. Recovery of microvasculature occurred by 2 weeks after injury only in the 2 atm injury group. Expression of HIF1alpha and increased vascular endothelial growth factor expression were observed in the ipsilateral hippocampus suggesting sufficiently impaired microcirculation resulting in the expression of hypoxic-response proteins. Collectively, the results indicate diffuse and heterogeneous microvascular alterations as well as endogenous expression of neuroprotective and neovascularization pathways after TBI.

Traumatic brain injury: can the consequences be stopped?

Traumatic brain injury is a leading cause of morbidity and death in both industrialized and developing countries. To date, there is no targeted pharmacological treatment that effectively limits the progression of secondary injury. The delayed progression of deterioration of grey and white matter gives hope that a meaningful intervention can be applied in a realistic timeframe following initial trauma. In this review we discuss new insights into the subcellular mechanisms of secondary injury that have highlighted numerous potential targets for intervention.

Mild in vitro trauma induces rapid Glur2 endocytosis, robustly augments calcium permeability and enhances susceptibility to secondary excitotoxic insult in cultured Purkinje cells.

Mild brain trauma results in a wide range of neurological symptoms that are not easily explained by the primary pathology. Purkinje neurons of the cerebellum are selectively vulnerable to brain trauma, including indirect remote trauma to the forebrain. This vulnerability manifests itself as a selective and delayed cell loss, for which the underlying mechanisms are poorly understood. Alterations to the surface expression of calcium impermeable AMPA receptors (GluR2-containing) may mediate post-traumatic calcium overload, and initiate biochemical cascades that ultimately cause progressive cell death. Our current study examined this hypothesis using an in vitro model of mild Purkinje trauma, delivered by an elastic stretch at 2.5-2.9 pounds per square inch (psi). This mild trauma alone did not increase cell loss as measured by propidium iodide (PI) uptake (at 20 h) compared to uninjured controls. However, there was a marked increase in cell loss, when cells following mild trauma, were exposed to 10 microM AMPA for 1 h compared to either mild trauma or AMPA exposure alone. Mild injury rendered Purkinje neurons significantly more permeable to AMPA-stimulated (4 microM) calcium influx at 15 min post-injury, including a sustained calcium plateau. This effect was eliminated by inhibiting protein kinase C-dependent GluR2 endocytosis with 2 microM Go6976 or blocking the calcium pore of GluR1/3 containing AMPARs with 500 nM 1-naphthylacetyl spermine (Naspm). Nifedipine (2 microM) eliminated the calcium plateau following mild injury but not the initial spike of Ca2+ increase. These results suggest that mild injuries resulted in a rapid AMPA receptor subtype switch (GluR2 was replaced by GluR1/3), which in turn resulted in an enhanced Ca2+ permeability. We further confirmed this by immunocytochemistry. Dendritic GluR2 co-localization with the pre-synaptic marker synaptophysin was markedly down-regulated at 15 min following mild stretch (P < 0.01), indicative of a rapid decrease in the synaptic expression of receptors containing this subunit. Carboxyfluorescence (CBF) assays revealed that mild stretch did not alter membrane integrity. Finally, we demonstrated that the combination of 500 nM Naspm and 5 nM Go6976 conferred a powerful neuroprotective effect on Purkinje cells by effectively eliminating the effects of mild stretch combined with AMPA in 95% of cells. These results represent a newly described mechanism rendering neurons susceptible to secondary injuries following trauma. Prevention of GluR2 endocytosis may be critical in the development of pharmacotherapies aimed at mild, seemingly inconsequential trauma, to avoid ensuing secondary damage.