182 research outputs found
A semantic web approach for built heritage representation
In a built heritage process, meant as a structured system of activities
aimed at the investigation, preservation, and management of architectural
heritage, any task accomplished by the several actors involved in it is deeply
influenced by the way the knowledge is represented and shared. In the current
heritage practice, knowledge representation and management have shown several
limitations due to the difficulty of dealing with large amount of extremely heterogeneous
data. On this basis, this research aims at extending semantic web
approaches and technologies to architectural heritage knowledge management in
order to provide an integrated and multidisciplinary representation of the artifact
and of the knowledge necessary to support any decision or any intervention and
management activity. To this purpose, an ontology-based system, representing
the knowledge related to the artifact and its contexts, has been developed through
the formalization of domain-specific entities and relationships between them
The three-body recombination of a condensed Bose gas near a Feshbach resonance
In this paper, we study the three-body recombination rate of a homogeneous
dilute Bose gas with a Feshbach resonance at zero temperature. The ground state
and excitations of this system are obtained. The three-body recombination in
the ground state is due to the break-up of an atom pair in the quantum
depletion and the formation of a molecule by an atom from the broken pair and
an atom from the condensate. The rate of this process is in good agreement with
the experiment on Na in a wide range of magnetic fields.Comment: 10 pages, 2 figures, to be published in Phys. Rev.
Resilience of Historic Residential Areas Subjected to Natural Disasters
The paper presents decision support tools developed for municipalities and historic city managers. These exploit the categorization of cultural heritage assets according to their vulnerability in disaster situations. A manual guiding individual cultural heritage owners, users and other citizens of historic areas provides advices on how to prevent or reduce damage and loss to cultural heritage. The recommendations cover pre-disaster, during as well as post-disaster situations and concern both built and moveable heritage. All measures are illustrated with examples taken during real disaster situations. The methodology has been tested during the international research project “ProteCHt2save”
supported under the Interreg CE program
Climate change-induced disasters and cultural heritage: Optimizing management strategies in Central Europe
Due to climate change, it is foreseen that the frequency and magnitude of extreme climate events such as heavy precipitation, flooding and drought will increase throughout Europe. In recent times, numerous areas suffered from disasters that produced significant damage to cultural heritage. Although different risk management strategies are currently enforced in Central Europe, there still exist many challenges that undermine their effectiveness. This study reviews the necessary points to be addressed for strengthening existing management strategies within the region and the characteristics of potential resilience building measures. It presents feasible and tailored ICT solutions (e.g. a web GIS platform) and decision support tools (e.g. a manual for cultural heritage resilience and a handbook on transnational rescue procedures) for the protection of cultural heritage against floods, heavy rain and fire. These tools result from the Interreg Central Europe project ProteCHt2save, concentrating on risk assessment and sustainable protection of cultural heritage in changing environments. The proposed measures are tested at pilot sites and successfully integrated in local risk management plans. Future work is also proposed for further implementation of the results
Usefulness of Low-Dose Statin Plus Ezetimibe and/or Nutraceuticals in Patients With Coronary Artery Disease Intolerant to High-Dose Statin Treatment.
High-dose statin (HDS) therapy is recommended to reduce low-density lipoprotein cholesterol (LDL-C); however, some patients are unable to tolerate the associated side effects. Nutraceuticals have shown efficacy in lowering LDL-C. The aim of this study was to evaluate whether the combination of low-dose statin (LDS) plus ezetimibe (EZE) or LDS plus nutraceutical (Armolipid Plus [ALP] containing red yeast rice, policosanol, and berberine) can lead to a higher proportion of high-risk patients achieving target LDL-C. A secondary objective was to assess the efficacy of triple combination LDS + EZE + ALP in resistant patients (LDL-C >70 mg/dl). A randomized, prospective, parallel-group, single-blind study was conducted in patients with coronary artery disease (n = 100) who had undergone percutaneous coronary intervention in the preceding 12 months, were HDS-intolerant, and were not at LDL-C target (<70 mg/dl) with LDS alone. Patients received either LDS + EZE or LDS + ALP. Of the 100 patients, 33 patients (66%) treated with LDS + EZE and 31 patients (62%) treated with LDS + ALP achieved target LDL-C after 3 months, which was maintained at 6 months. Patients who did not achieve the therapeutic goal received a triple combination of LDS + EZE + ALP for a further 3 months. At 6 months, 28 of 36 patients (78%) achieved LDL-C target. Overall, 92% of patients enrolled in this study were at target LDL-C at 6 months. No patients in any group experienced major side effects. In conclusion, in HDS-intolerant coronary artery disease patients, the combination of LDS plus EZE and/or ALP represents a valuable therapeutic option allowing most patients to reach target LDL-C within 3 to 6 months
Multi-GeV Electron Spectrometer
The advance in laser plasma acceleration techniques pushes the regime of the
resulting accelerated particles to higher energies and intensities. In
particular the upcoming experiments with the FLAME laser at LNF will enter the
GeV regime with almost 1pC of electrons. From the current status of
understanding of the acceleration mechanism, relatively large angular and
energy spreads are expected. There is therefore the need to develop a device
capable to measure the energy of electrons over three orders of magnitude (few
MeV to few GeV) under still unknown angular divergences. Within the PlasmonX
experiment at LNF a spectrometer is being constructed to perform these
measurements. It is made of an electro-magnet and a screen made of
scintillating fibers for the measurement of the trajectories of the particles.
The large range of operation, the huge number of particles and the need to
focus the divergence present unprecedented challenges in the design and
construction of such a device. We will present the design considerations for
this spectrometer and the first results from a prototype.Comment: 7 pages, 6 figures, submitted to NIM
Perifosine as a Potential Novel Anti-Cancer Agent Inhibits EGFR/MET-AKT Axis in Malignant Pleural Mesothelioma
PI3K/AKT signalling pathway is aberrantly active and plays a critical role for cell cycle progression of human malignant pleural mesothelioma (MMe) cells. AKT is one of the important cellular targets of perifosine, a novel bio-available alkylphospholipid that has displayed significant anti-proliferative activity in vitro and in vivo in several human tumour model systems and is currently being tested in clinical trials.We tested Perifosine activity on human mesothelial cells and different mesothelioma cell lines, in order to provide evidence of its efficacy as single agent and combined therapy.We demonstrate here that perifosine, currently being evaluated as an anti-cancer agent in phase 1 and 2 clinical trials, caused a dose-dependent reduction of AKT activation, at concentrations causing MMe cell growth arrest. In this study we firstly describe that MMe cells express aside from AKT1 also AKT3 and that either the myristoylated, constitutively active, forms of the two proteins, abrogated perifosine-mediated cell growth inhibition. Moreover, we describe here a novel mechanism of perifosine that interferes, upstream of AKT, affecting EGFR and MET phosphorylation. Finally, we demonstrate a significant increase in cell toxicity when MMe cells were treated with perifosine in combination with cisplatin.This study provides a novel mechanism of action of perifosine, directly inhibiting EGFR/MET-AKT1/3 axis, providing a rationale for a novel translational approach to the treatment of MMe
Frequency-modulated electromagnetic neural stimulation (FREMS) as a treatment for symptomatic diabetic neuropathy: results from a double-blind, randomised, multicentre, long-term, placebo-controlled clinical trial
AIMS/HYPOTHESIS: The aim was to evaluate the efficacy and safety of
transcutaneous frequency-modulated electromagnetic neural stimulation (frequency
rhythmic electrical modulation system, FREMS) as a treatment for symptomatic
peripheral neuropathy in patients with diabetes mellitus.
METHODS: This was a double-blind, randomised, multicentre, parallel-group study
of three series, each of ten treatment sessions of FREMS or placebo administered
within 3 weeks, 3 months apart, with an overall follow-up of about 51 weeks. The
primary endpoint was the change in nerve conduction velocity (NCV) of deep
peroneal, tibial and sural nerves. Secondary endpoints included the effects of
treatment on pain, tactile, thermal and vibration sensations. Patients eligible
to participate were aged 18-75 years with diabetes for ≥ 1 year, HbA(1c) <11.0%
(97 mmol/mol), with symptomatic diabetic polyneuropathy at the lower extremities
(i.e. abnormal amplitude, latency or NCV of either tibial, deep peroneal or sural
nerve, but with an evocable potential and measurable NCV of the sural nerve), a
Michigan Diabetes Neuropathy Score ≥ 7 and on a stable dose of medications for
diabetic neuropathy in the month prior to enrolment. Data were collected in an
outpatient setting. Participants were allocated to the FREMS or placebo arm (1:1
ratio) according to a sequence generated by a computer random number generator,
without block or stratification factors. Investigators digitised patients' date
of birth and site number into an interactive voice recording system to obtain the
assigned treatment. Participants, investigators conducting the trial, or people
assessing the outcomes were blinded to group assignment.
RESULTS: Patients (n = 110) with symptomatic neuropathy were randomised to FREMS
(n = 54) or placebo (n = 56). In the intention-to-treat population (50 FREMS, 51
placebo), changes in NCV of the three examined nerves were not different between
FREMS and placebo (deep peroneal [means ± SE]: 0.74 ± 0.71 vs 0.06 ± 1.38 m/s;
tibial: 2.08 ± 0.84 vs 0.61 ± 0.43 m/s; and sural: 0.80 ± 1.08 vs -0.91 ± 1.13
m/s; FREMS vs placebo, respectively). FREMS induced a significant reduction in
day and night pain as measured by a visual analogue scale immediately after each
treatment session, although this beneficial effect was no longer measurable 3
months after treatment. Compared with the placebo group, in the FREMS group the
cold sensation threshold was significantly improved, while non-significant
differences were observed in the vibration and warm sensation thresholds. No
relevant side effects were recorded during the study.
CONCLUSIONS/INTERPRETATION: FREMS proved to be a safe treatment for symptomatic
diabetic neuropathy, with immediate, although transient, reduction in pain, and
no effect on NCV.
TRIAL REGISTRATION: ClinicalTrials.gov NCT01628627.
FUNDING: The clinical trial was sponsored by Lorenz Biotech (Medolla, Italy),
lately Lorenz Lifetech (Ozzano dell'Emilia, Italy)
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