1,768 research outputs found
Secure Vehicular Communication Systems: Implementation, Performance, and Research Challenges
Vehicular Communication (VC) systems are on the verge of practical
deployment. Nonetheless, their security and privacy protection is one of the
problems that have been addressed only recently. In order to show the
feasibility of secure VC, certain implementations are required. In [1] we
discuss the design of a VC security system that has emerged as a result of the
European SeVeCom project. In this second paper, we discuss various issues
related to the implementation and deployment aspects of secure VC systems.
Moreover, we provide an outlook on open security research issues that will
arise as VC systems develop from today's simple prototypes to full-fledged
systems
The Gerasimov-Drell-Hearn Sum Rule and the Spin Structure of the Nucleon
The Gerasimov-Drell-Hearn sum rule is one of several dispersive sum rules
that connect the Compton scattering amplitudes to the inclusive photoproduction
cross sections of the target under investigation. Being based on such universal
principles as causality, unitarity, and gauge invariance, these sum rules
provide a unique testing ground to study the internal degrees of freedom that
hold the system together. The present article reviews these sum rules for the
spin-dependent cross sections of the nucleon by presenting an overview of
recent experiments and theoretical approaches. The generalization from real to
virtual photons provides a microscope of variable resolution: At small
virtuality of the photon, the data sample information about the long range
phenomena, which are described by effective degrees of freedom (Goldstone
bosons and collective resonances), whereas the primary degrees of freedom
(quarks and gluons) become visible at the larger virtualities. Through a rich
body of new data and several theoretical developments, a unified picture of
virtual Compton scattering emerges, which ranges from coherent to incoherent
processes, and from the generalized spin polarizabilities on the low-energy
side to higher twist effects in deep inelastic lepton scattering.Comment: 32 pages, 19 figures, review articl
PHOTOCHEMICAL RING-OPENING IN meso-CHLORINATED CHLOROPHYLLS
Irradiation of 20-chloro-chlorophylls of the a-type with visible light produces long-wavelength shifted photoproducts, which transform in the dark to linear tetrapyrroles (bile pigments). The possible significance for chlorophyll degradation is discussed
REACTIVITY OF CHLOROPHYLL a/b-PROTEINS AND MICELLAR TRITON X-100 COMPLEXES OF CHLOROPHYLLS a OR b WITH BOROHYDRIDE
The reaction of several plant chlorophyll-protein complexes with NaBH4 has been studied by absorption spectroscopy. In all the complexes studied, chlorophyll b is more reactive than Chi a, due to preferential reaction of its formyl substituent at C-7. The complexes also show large variations in reactivity towards NaBH4 and the order of reactivity is: LHCI > PSII complex > LHCII > PSI > P700 (investigated as a component of PSI). Differential pools of the same type of chlorophyll have been observed in several complexes.
Parallel work was undertaken on the reactivity of micellar complexes of chlorophyll a and of chlorophyll b with NaBH4 to study the effect of aggregation state on this reactivity. In these complexes, both chlorophyll a and b show large variations in reactivity in the order monomer > oligomer > polymer with chlorophyll b generally being more reactive than chlorophyll a. It is concluded that aggregation decreases the reactivity of chlorophylls towards NaBH4 in vitro, and may similarly decrease reactivity in naturally-occurring chlorophyll-protein complexes
Loss of AP-3 function affects spontaneous and evoked release at hippocampal mossy fiber synapses
Synaptic vesicle (SV) exocytosis mediating neurotransmitter release occurs
spontaneously at low intraterminal calcium concentrations and is stimulated by
a rise in intracellular calcium. Exocytosis is compensated for by the
reformation of vesicles at plasma membrane and endosomes. Although the adaptor
complex AP-3 was proposed to be involved in the formation of SVs from
endosomes, whether its function has an indirect effect on exocytosis remains
unknown. Using mocha mice, which are deficient in functional AP-3, we identify
an AP-3-dependent tetanus neurotoxin-resistant asynchronous release that can be
evoked at hippocampal mossy fiber (MF) synapses. Presynaptic targeting of the
tetanus neurotoxin-resistant vesicle soluble N-ethylmaleimide-sensitive factor
attachment protein receptor (SNARE) tetanus neurotoxin-insensitive
vesicle-associated membrane protein (TI-VAMP) is lost in mocha hippocampal MF
terminals, whereas the localization of synaptobrevin 2 is unaffected. In
addition, quantal release in mocha cultures is more frequent and more sensitive
to sucrose. We conclude that lack of AP-3 results in more constitutive
secretion and loss of an asynchronous evoked release component, suggesting an
important function of AP-3 in regulating SV exocytosis at MF terminals
Analysis of resonance multipoles from polarization observables in eta photoproduction
A combined analysis of new eta photoproduction data for total and
differential cross sections, target asymmetry and photon asymmetry is
presented. Using a few reasonable assumptions we perform the first
model-independent analysis of the E0+, E2- and M2- eta photoproduction
multipoles. Making use of the well-known A3/2 helicity amplitude of the
D13(1520) state we extract its branching ratio to the eta-N channel,
Gamma(eta,N)/Gamma = (0.08 +- 0.01)%. At higher energies, we show that the
photon asymmetry is extremely sensitive to small multipoles that are excited by
photons in the helicity 3/2 state. The new GRAAL photon asymmetry data at
higher energy show a clear signal of the F15(1680) excitation which permits
extracting an F15(1680)->eta,N branching ratio of (0.15 +0.35 -0.10)%.Comment: 14 pages of LATEX including 7 postscript figure
An active vesicle priming machinery suppresses axon regeneration upon adult CNS injury
Axons in the adult mammalian central nervous system fail to regenerate after spinal cord injury. Neurons lose their capacity to regenerate during development, but the intracellular processes underlying this loss are unclear. We found that critical components of the presynaptic active zone prevent axon regeneration in adult mice. Transcriptomic analysis combined with live-cell imaging revealed that adult primary sensory neurons downregulate molecular constituents of the synapse as they acquire the ability to rapidly grow their axons. Pharmacogenetic reduction of neuronal excitability stimulated axon regeneration after adult spinal cord injury. Genetic gain- and loss-of-function experiments uncovered that essential synaptic vesicle priming proteins of the presynaptic active zone, but not clostridial-toxin-sensitive VAMP-family SNARE proteins, inhibit axon regeneration. Systemic administration of Baclofen reduced voltage-dependent Ca2+ influx in primary sensory neurons and promoted their regeneration after spinal cord injury. These findings indicate that functional presynaptic active zones constitute a major barrier to axon regeneration
Circuit-selective cell-autonomous regulation of inhibition in pyramidal neurons by Ste20-like kinase
Maintaining an appropriate balance between excitation and inhibition is critical for neuronal information processing. Cortical neurons can cell-autonomously adjust the inhibition they receive to individual levels of excitatory input, but the underlying mechanisms are unclear. We describe that Ste20-like kinase (SLK) mediates cell-autonomous regulation of excitation-inhibition balance in the thalamocortical feedforward circuit, but not in the feedback circuit. This effect is due to regulation of inhibition originating from parvalbumin-expressing interneurons, while inhibition via somatostatin-expressing interneurons is unaffected. Computational modeling shows that this mechanism promotes stable excitatory-inhibitory ratios across pyramidal cells and ensures robust and sparse coding. Patch-clamp RNA sequencing yields genes differentially regulated by SLK knockdown, as well as genes associated with excitation-inhibition balance participating in transsynaptic communication and cytoskeletal dynamics. These data identify a mechanism for cell-autonomous regulation of a specific inhibitory circuit that is critical to ensure that a majority of cortical pyramidal cells participate in information coding
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