295 research outputs found

    On "Ergodicity and Central Limit Theorem in Systems with Long-Range Interactions" by Figueiredo et al

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    In the present paper we refute the criticism advanced in a recent preprint by Figueiredo et al [1] about the possible application of the qq-generalized Central Limit Theorem (CLT) to a paradigmatic long-range-interacting many-body classical Hamiltonian system, the so-called Hamiltonian Mean Field (HMF) model. We exhibit that, contrary to what is claimed by these authors and in accordance with our previous results, qq-Gaussian-like curves are possible and real attractors for a certain class of initial conditions, namely the one which produces nontrivial longstanding quasi-stationary states before the arrival, only for finite size, to the thermal equilibrium.Comment: 2 pages, 2 figures. Short version of the paper, accepted for publication in Europhysics Letters, (2009) in pres

    Inclusion of new 5-fluorouracil amphiphilic derivatives in liposome formulation for cancer treatment

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    Correction for 'Inclusion of new 5-fluorouracil amphiphilic derivatives in liposome formulation for cancer treatment' by M. Petaccia et al., Med. Chem. Commun., 2015, 6, 1639–1642

    Lyapunov exponent of many-particle systems: testing the stochastic approach

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    The stochastic approach to the determination of the largest Lyapunov exponent of a many-particle system is tested in the so-called mean-field XY-Hamiltonians. In weakly chaotic regimes, the stochastic approach relates the Lyapunov exponent to a few statistical properties of the Hessian matrix of the interaction, which can be calculated as suitable thermal averages. We have verified that there is a satisfactory quantitative agreement between theory and simulations in the disordered phases of the XY models, either with attractive or repulsive interactions. Part of the success of the theory is due to the possibility of predicting the shape of the required correlation functions, because this permits the calculation of correlation times as thermal averages.Comment: 11 pages including 6 figure

    Canonical Solution of Classical Magnetic Models with Long-Range Couplings

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    We study the canonical solution of a family of classical nvectorn-vector spin models on a generic dd-dimensional lattice; the couplings between two spins decay as the inverse of their distance raised to the power α\alpha, with α<d\alpha<d. The control of the thermodynamic limit requires the introduction of a rescaling factor in the potential energy, which makes the model extensive but not additive. A detailed analysis of the asymptotic spectral properties of the matrix of couplings was necessary to justify the saddle point method applied to the integration of functions depending on a diverging number of variables. The properties of a class of functions related to the modified Bessel functions had to be investigated. For given nn, and for any α\alpha, dd and lattice geometry, the solution is equivalent to that of the α=0\alpha=0 model, where the dimensionality dd and the geometry of the lattice are irrelevant.Comment: Submitted for publication in Journal of Statistical Physic

    Identification of Drosophila Mitotic Genes by Combining Co-Expression Analysis and RNA Interference

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    RNAi screens have, to date, identified many genes required for mitotic divisions of Drosophila tissue culture cells. However, the inventory of such genes remains incomplete. We have combined the powers of bioinformatics and RNAi technology to detect novel mitotic genes. We found that Drosophila genes involved in mitosis tend to be transcriptionally co-expressed. We thus constructed a co-expression–based list of 1,000 genes that are highly enriched in mitotic functions, and we performed RNAi for each of these genes. By limiting the number of genes to be examined, we were able to perform a very detailed phenotypic analysis of RNAi cells. We examined dsRNA-treated cells for possible abnormalities in both chromosome structure and spindle organization. This analysis allowed the identification of 142 mitotic genes, which were subdivided into 18 phenoclusters. Seventy of these genes have not previously been associated with mitotic defects; 30 of them are required for spindle assembly and/or chromosome segregation, and 40 are required to prevent spontaneous chromosome breakage. We note that the latter type of genes has never been detected in previous RNAi screens in any system. Finally, we found that RNAi against genes encoding kinetochore components or highly conserved splicing factors results in identical defects in chromosome segregation, highlighting an unanticipated role of splicing factors in centromere function. These findings indicate that our co-expression–based method for the detection of mitotic functions works remarkably well. We can foresee that elaboration of co-expression lists using genes in the same phenocluster will provide many candidate genes for small-scale RNAi screens aimed at completing the inventory of mitotic proteins

    Combined inhibition of Aurora-A and ATR kinase results in regression of MYCN-amplified neuroblastoma

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    Amplification of MYCN is the driving oncogene in a subset of high-risk neuroblastoma. The MYCN protein and the Aurora-A kinase form a complex during S phase that stabilizes MYCN. Here we show that MYCN activates Aurora-A on chromatin, which phosphorylates histone H3 at serine 10 in S phase, promotes the deposition of histone H3.3 and suppresses R-loop formation. Inhibition of Aurora-A induces transcription-replication conflicts and activates the Ataxia telangiectasia and Rad3 related (ATR) kinase, which limits double-strand break accumulation upon Aurora-A inhibition. Combined inhibition of Aurora-A and ATR induces rampant tumor-specific apoptosis and tumor regression in mouse models of neuroblastoma, leading to permanent eradication in a subset of mice. The therapeutic efficacy is due to both tumor cell-intrinsic and immune cell-mediated mechanisms. We propose that targeting the ability of Aurora-A to resolve transcription-replication conflicts is an effective therapy for MYCN-driven neuroblastoma (141 words)

    A Fall and Near-Fall Assessment and Evaluation System

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    The FANFARE (Falls And Near Falls Assessment Research and Evaluation) project has developed a system to fulfill the need for a wearable device to collect data for fall and near-falls analysis. The system consists of a computer and a wireless sensor network to measure, display, and store fall related parameters such as postural activities and heart rate variability. Ease of use and low power are considered in the design. The system was built and tested successfully. Different machine learning algorithms were applied to the stored data for fall and near-fall evaluation. Results indicate that the Naïve Bayes algorithm is the best choice, due to its fast model building and high accuracy in fall detection
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