2,495 research outputs found

    VMXR: a EUD Environment for Virtual Merchandizing in XR

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    This paper presents the current development state of VMXR, a Proof of Concept (PoC) environment allowing people without programming experience to create and configure product showcases in a Virtual and eXtended reality setting. The aim of the PoC is to identify proper metaphors and workflows for supporting showcase designers in creating interactions with the virtual product representation or enhancing the physical environment through additional information and media

    Drastic effects of damping mechanisms on the third-order optical nonlinearity

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    We have investigated the optical response of superradiant atoms, which undergoes three different damping mechanisms: radiative dissipation (γr\gamma_r), dephasing (γd\gamma_d), and nonradiative dissipation (γn\gamma_n). Whereas the roles of γd\gamma_d and γn\gamma_n are equivalent in the linear susceptibility, the third-order nonlinear susceptibility drastically depends on the ratio of γd\gamma_d and γn\gamma_n: When γd≪γn\gamma_d \ll \gamma_n, the third-order susceptibility is essentially that of a single atom. Contrarily, in the opposite case of γd≫γn\gamma_d \gg \gamma_n, the third-order susceptibility suffers the size-enhancement effect and becomes proportional to the system size.Comment: 5pages, 2figure

    Beyond-CMOS Artificial Neuron: A simulation-based exploration of the molecular-FET

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    The recent growth of Artificial Neural Networks fueled the design of numerous Artificial Intelligence (AI) dedicated hardware implementations. High power dissipation, computational complexity, and large area footprints currently limit CMOS based real-time embedded AI applications. In this work, we design and simulate through SPICE, for the first time, an artificial analog neuron based on the molecular Field-Effect Transistor (molFET) technology. MolFETs are described by a circuital model whose physical characteristics are extracted from atomistic simulations. The designed neuron is a single column of a crossbar-like circuit representing a layer of seven parallel neurons. The drain currents sum up in a soma-like circuit - modelled through a comparator - and trigger the output pulses. We demonstrate the advantages of the molFET in terms of area, power, and speed by comparing it with a conventional MOSFET implementation. The results confirm the molecular technology is a promising candidate for accomplishing high neuron throughput capability and massive redundancy, still providing high energy efficiency. The obtained results foster further investigation of molFET technology both at the device and circuit level

    Statistics of low-energy levels of a one-dimensional weakly localized Frenkel exciton: A numerical study

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    Numerical study of the one-dimensional Frenkel Hamiltonian with on-site randomness is carried out. We focus on the statistics of the energy levels near the lower exciton band edge, i. e. those determining optical response. We found that the distribution of the energy spacing between the states that are well localized at the same segment is characterized by non-zero mean, i.e. these states undergo repulsion. This repulsion results in a local discrete energy structure of a localized Frenkel exciton. On the contrary, the energy spacing distribution for weakly overlapping local ground states (the states with no nodes within their localization segments) that are localized at different segments has zero mean and shows almost no repulsion. The typical width of the latter distribution is of the same order as the typical spacing in the local discrete energy structure, so that this local structure is hidden; it does not reveal itself neither in the density of states nor in the linear absorption spectra. However, this structure affects the two-exciton transitions involving the states of the same segment and can be observed by the pump-probe spectroscopy. We analyze also the disorder degree scaling of the first and second momenta of the distributions.Comment: 10 pages, 6 figure

    Glutamatergic neurons induce expression of functional glutamatergic synapses in primary myotubes.

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    The functioning of the nervous system depends upon the specificity of its synaptic contacts. The mechanisms triggering the expression of the appropriate receptors on postsynaptic membrane and the role of the presynaptic partner in the differentiation of postsynaptic structures are little known.To address these questions we cocultured murine primary muscle cells with several glutamatergic neurons, either cortical, cerebellar or hippocampal. Immunofluorescence and electrophysiology analyses revealed that functional excitatory synaptic contacts were formed between glutamatergic neurons and muscle cells. Moreover, immunoprecipitation and immunofluorescence experiments showed that typical anchoring proteins of central excitatory synapses coimmunoprecipitate and colocalize with rapsyn, the acetylcholine receptor anchoring protein at the neuromuscular junction.These results support an important role of the presynaptic partner in the induction and differentiation of the postsynaptic structures

    Ab initio calculations of structural and electronic properties of CdTe clusters

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    We present results of a study of small stoichiometric CdnTenCd_{n}Te_{n} (1≤n≤61{\leq}n{\leq}6) clusters and few medium sized non-stoichiometric CdmTenCd_{m}Te_{n} [(m,n=13,16,19m,n= 13, 16, 19); (m≠nm{\neq}n)] clusters using the Density Functional formalism and projector augmented wave method within the generalized gradient approximation. Structural properties {\it viz.} geometry, bond length, symmetry and electronic properties like HOMO-LUMO gap, binding energy, ionization potential and nature of bonding {\it etc.} have been analyzed. Medium sized non-stoichiometric clusters were considered as fragments of the bulk with T{d_{d}} symmetry. It was observed that upon relaxation, the symmetry changes for the Cd rich clusters whereas the Te rich clusters retain their symmetry. The Cd rich clusters develop a HOMO-LUMO gap due to relaxation whereas there is no change in the HOMO-LUMO gap of the Te rich clusters. Thus, the symmetry of a cluster seems to be an important factor in determining the HOMO-LUMO gap.Comment: 8 pages 16 figure

    Excitonic Strings in one dimensional organic compounds

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    Important questions concern the existence of excitonic strings in organic compounds and their signatures in the photophysics of these systems. A model in terms of Hard Core Bosons is proposed to study this problem in one dimension. Mainly the cases with two and three particles are studied for finite and infinite lattices, where analytical results are accessible. It is shown that if bi-excitonic states exist, three-excitonic and even, n-excitonic strings, at least in a certain range of parameters, will exist. Moreover, the behaviour of the transitions from one exciton to the biexciton is fully clarified. The results are in agreement with exact finite cluster diagonalizations of several model Hamiltonians.Comment: 36 pages, 4 eps figs. to appear in Phys. Rev.

    Redistribution of DAT/α-synuclein complexes visualized by “in situ” proximity ligation assay in transgenic mice modelling early Parkinson’s disease

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    Alpha-synuclein, the major component of Lewy bodies, is thought to play a central role in the onset of synaptic dysfunctions in Parkinson's disease (PD). In particular, α-synuclein may affect dopaminergic neuron function as it interacts with a key protein modulating dopamine (DA) content at the synapse: the DA transporter (DAT). Indeed, recent evidence from our "in vitro" studies showed that α-synuclein aggregation decreases the expression and membrane trafficking of the DAT as the DAT is retained into α-synuclein-immunopositive inclusions. This notwithstanding, "in vivo" studies on PD animal models investigating whether DAT distribution is altered by the pathological overexpression and aggregation of α-synuclein are missing. By using the proximity ligation assay, a technique which allows the "in situ" visualization of protein-protein interactions, we studied the occurrence of alterations in the distribution of DAT/α-synuclein complexes in the SYN120 transgenic mouse model, showing insoluble α-synuclein aggregates into dopaminergic neurons of the nigrostriatal system, reduced striatal DA levels and an altered distribution of synaptic proteins in the striatum. We found that DAT/α-synuclein complexes were markedly redistributed in the striatum and substantia nigra of SYN120 mice. These alterations were accompanied by a significant increase of DAT striatal levels in transgenic animals when compared to wild type littermates. Our data indicate that, in the early pathogenesis of PD, α-synuclein acts as a fine modulator of the dopaminergic synapse by regulating the subcellular distribution of key proteins such as the DAT
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