Study on the analytical model of vibration source for metro train

A novel analytical model of vibration source for metro train based on “coupled vehicle and track basic unit” is established in this paper. The dynamic vehicle-track equations are completed with the displacement compatibility and the force equilibrium, and the model takes into account the infinite track structure, whole vehicle, track irregularity and wheel-rail Hertz contact. The special feature of track structure model is the periodical system of discrete supported sleepers, which converts the infinite integral equation into the combination in the wave number-frequency domain and simplifies the calculation progress. The rail dynamic responses and the wheel-rail contact force can be calculated easily. A complete software package TMCVT is programmed. A calculated example is achieved using the program. Compared the theoretical calculated results and the field tested results ,the coincidence with each other proved the analytical dynamic model for metro train coupled with vehicle and track is correct

Analytical solution for dynamic response of curved rail subjected to moving train

The objective of this paper is to present an analytical solution for the dynamic response of curved rail. The detailed solution was derived for the out-of-plane vibration response of periodically supported curved Timoshenko beam subjected to moving loads. The accuracy of the solution was validated based on the results from previous study. Furthermore, the train/track interaction model was introduced into this solution to calculate the rail dynamic response in Beijing metro. The results presented herein indicated that the solution provided accurate results in comparison with both the result from previous study and the measurement data collected from Beijing metro and it can be used to derive the dynamic response for similar situations

Authentication codes from ε-ASU hash functions with partially secret keys

An authentication code can be constructed with a family of e-Almost strong universal (e-ASU) hash functions, with the index of hash functions as the authentication key. This paper considers the performance of authentication codes from e-ASU, when the authentication key is only partially secret. We show how to apply the result to privacy amplification against active attacks in the scenario of two independent partially secret strings shared between a sender and a receiver. Keywords: Authentication code; Information theory; Privacy amplification; Unconditional securit

Identifying progressive imaging genetic patterns via multi-task sparse canonical correlation analysis: a longitudinal study of the ADNI cohort

Motivation Identifying the genetic basis of the brain structure, function and disorder by using the imaging quantitative traits (QTs) as endophenotypes is an important task in brain science. Brain QTs often change over time while the disorder progresses and thus understanding how the genetic factors play roles on the progressive brain QT changes is of great importance and meaning. Most existing imaging genetics methods only analyze the baseline neuroimaging data, and thus those longitudinal imaging data across multiple time points containing important disease progression information are omitted. Results We propose a novel temporal imaging genetic model which performs the multi-task sparse canonical correlation analysis (T-MTSCCA). Our model uses longitudinal neuroimaging data to uncover that how single nucleotide polymorphisms (SNPs) play roles on affecting brain QTs over the time. Incorporating the relationship of the longitudinal imaging data and that within SNPs, T-MTSCCA could identify a trajectory of progressive imaging genetic patterns over the time. We propose an efficient algorithm to solve the problem and show its convergence. We evaluate T-MTSCCA on 408 subjects from the Alzheimer’s Disease Neuroimaging Initiative database with longitudinal magnetic resonance imaging data and genetic data available. The experimental results show that T-MTSCCA performs either better than or equally to the state-of-the-art methods. In particular, T-MTSCCA could identify higher canonical correlation coefficients and capture clearer canonical weight patterns. This suggests that T-MTSCCA identifies time-consistent and time-dependent SNPs and imaging QTs, which further help understand the genetic basis of the brain QT changes over the time during the disease progression. Availability and implementation The software and simulation data are publicly available at https://github.com/dulei323/TMTSCCA. Supplementary information Supplementary data are available at Bioinformatics online

Fast Multi-Task SCCA Learning with Feature Selection for Multi-Modal Brain Imaging Genetics

Brain imaging genetics studies the genetic basis of brain structures and functions via integrating both genotypic data such as single nucleotide polymorphism (SNP) and imaging quantitative traits (QTs). In this area, both multi-task learning (MTL) and sparse canonical correlation analysis (SCCA) methods are widely used since they are superior to those independent and pairwise univariate analyses. MTL methods generally incorporate a few of QTs and are not designed for feature selection from a large number of QTs; while existing SCCA methods typically employ only one modality of QTs to study its association with SNPs. Both MTL and SCCA encounter computational challenges as the number of SNPs increases. In this paper, combining the merits of MTL and SCCA, we propose a novel multi-task SCCA (MTSCCA) learning framework to identify bi-multivariate associations between SNPs and multi-modal imaging QTs. MTSCCA could make use of the complementary information carried by different imaging modalities. Using the G2,1-norm regularization, MTSCCA treats all SNPs in the same group together to enforce sparsity at the group level. The l2,1-norm penalty is used to jointly select features across multiple tasks for SNPs, and across multiple modalities for QTs. A fast optimization algorithm is proposed using the grouping information of SNPs. Compared with conventional SCCA methods, MTSCCA obtains improved performance regarding both correlation coefficients and canonical weights patterns. In addition, our method runs very fast and is easy-to-implement, and thus could provide a powerful tool for genome-wide brain-wide imaging genetic studies

Tissue-specific network-based genome wide study of amygdala imaging phenotypes to identify functional interaction modules

Motivation: Network-based genome-wide association studies (GWAS) aim to identify functional modules from biological networks that are enriched by top GWAS findings. Although gene functions are relevant to tissue context, most existing methods analyze tissue-free networks without reflecting phenotypic specificity. Results: We propose a novel module identification framework for imaging genetic studies using the tissue-specific functional interaction network. Our method includes three steps: (i) re-prioritize imaging GWAS findings by applying machine learning methods to incorporate network topological information and enhance the connectivity among top genes; (ii) detect densely connected modules based on interactions among top re-prioritized genes; and (iii) identify phenotype-relevant modules enriched by top GWAS findings. We demonstrate our method on the GWAS of [18F]FDG-PET measures in the amygdala region using the imaging genetic data from the Alzheimer's Disease Neuroimaging Initiative, and map the GWAS results onto the amygdala-specific functional interaction network. The proposed network-based GWAS method can effectively detect densely connected modules enriched by top GWAS findings. Tissue-specific functional network can provide precise context to help explore the collective effects of genes with biologically meaningful interactions specific to the studied phenotype

Transcriptome-Guided Imaging Genetic Analysis via a Novel Sparse CCA Algorithm

Imaging genetics is an emerging field that studies the influence of genetic variation on brain structure and function. The major task is to examine the association between genetic markers such as single nucleotide polymorphisms (SNPs) and quantitative traits (QTs) extracted from neuroimaging data. Sparse canonical correlation analysis (SCCA) is a bi-multivariate technique used in imaging genetics to identify complex multi-SNP-multi-QT associations. In imaging genetics, genes associated with a phenotype should at least expressed in the phenotypical region. We study the association between the genotype and amyloid imaging data and propose a transcriptome-guided SCCA framework that incorporates the gene expression information into the SCCA criterion. An alternating optimization method is used to solve the formulated problem. Although the problem is not biconcave, a closed-form solution has been found for each subproblem. The results on real data show that using the gene expression data to guide the feature selection facilities the detection of genetic markers that are not only associated with the identified QTs, but also highly expressed there

Predicting Interrelated Alzheimer's Disease Outcomes via New Self-Learned Structured Low-Rank Model

Alzheimer's disease (AD) is a progressive neurodegenerative disorder. As the prodromal stage of AD, Mild Cognitive Impairment (MCI) maintains a good chance of converting to AD. How to efficaciously detect this conversion from MCI to AD is significant in AD diagnosis. Different from standard classification problems where the distributions of classes are independent, the AD outcomes are usually interrelated (their distributions have certain overlaps). Most of existing methods failed to examine the interrelations among different classes, such as AD, MCI conversion and MCI non-conversion. In this paper, we proposed a novel self-learned low-rank structured learning model to automatically uncover the interrelations among different classes and utilized such interrelated structures to enhance classification. We conducted experiments on the ADNI cohort data. Empirical results demonstrated advantages of our model