Limin Jiang scite author profile

Between 1996 and 1998, two clades (B and C; genotype I) of dengue virus type 1 (DENV-1) appeared in Myanmar (Burma) that were new to that location. Between 1998 and 2000, a third clade (A; genotype III) of DENV-1, which had been circulating at that locality for at least 25 years, became extinct. These changes preceded the largest outbreak of dengue recorded in Myanmar, in 2001, in which more than 95% of viruses recovered from patients were DENV-1, but where the incidence of severe disease was much less than in previous years. Phylogenetic analyses of viral genomes indicated that the two new clades of DENV-1 did not arise from the, now extinct, clade A viruses nor was the extinction of this clade due to differences in the fitness of the viral populations. Since the extinction occurred during an inter-epidemic period, we suggest that it was due to a stochastic event attributable to the low rate of virus transmission in this interval.

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BP Neural Network Could Help Improve Pre-miRNA Identification in Various Species

Jiang

Zhang

Xuan

et al. 2016

BioMed Research International

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MicroRNAs (miRNAs) are a set of short (21–24 nt) noncoding RNAs that play significant regulatory roles in cells. In the past few years, research on miRNA-related problems has become a hot field of bioinformatics because of miRNAs' essential biological function. miRNA-related bioinformatics analysis is beneficial in several aspects, including the functions of miRNAs and other genes, the regulatory network between miRNAs and their target mRNAs, and even biological evolution. Distinguishing miRNA precursors from other hairpin-like sequences is important and is an essential procedure in detecting novel microRNAs. In this study, we employed backpropagation (BP) neural network together with 98-dimensional novel features for microRNA precursor identification. Results show that the precision and recall of our method are 95.53% and 96.67%, respectively. Results further demonstrate that the total prediction accuracy of our method is nearly 13.17% greater than the state-of-the-art microRNA precursor prediction software tools.

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MDA-SKF: Similarity Kernel Fusion for Accurately Discovering miRNA-Disease Association

et al. 2018

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Identifying accurate associations between miRNAs and diseases is beneficial for diagnosis and treatment of human diseases. It is especially important to develop an efficient method to detect the association between miRNA and disease. Traditional experimental method has high precision, but its process is complicated and time-consuming. Various computational methods have been developed to uncover potential associations based on an assumption that similar miRNAs are always related to similar diseases. In this paper, we propose an accurate method, MDA-SKF, to uncover potential miRNA-disease associations. We first extract three miRNA similarity kernels (miRNA functional similarity, miRNA sequence similarity, Hamming profile similarity for miRNA) and three disease similarity kernels (disease semantic similarity, disease functional similarity, Hamming profile similarity for disease) in two subspaces, respectively. Then, due to limitations that some initial information may be lost in the process and some noises may be exist in integrated similarity kernel, we propose a novel Similarity Kernel Fusion (SKF) method to integrate multiple similarity kernels. Finally, we utilize the Laplacian Regularized Least Squares (LapRLS) method on the integrated kernel to find potential associations. MDA-SKF is evaluated by three evaluation methods, including global leave-one-out cross validation (LOOCV) and local LOOCV and 5-fold cross validation (CV), and achieves AUCs of 0.9576, 0.8356, and 0.9557, respectively. Compared with existing seven methods, MDA-SKF has outstanding performance on global LOOCV and 5-fold. We also test case studies to further analyze the performance of MDA-SKF on 32 diseases. Furthermore, 3200 candidate associations are obtained and a majority of them can be confirmed. It demonstrates that MDA-SKF is an accurate and efficient computational tool for guiding traditional experiments.

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Discovering Cancer Subtypes via an Accurate Fusion Strategy on Multiple Profile Data

et al. 2019

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Discovering cancer subtypes is useful for guiding clinical treatment of multiple cancers. Progressive profile technologies for tissue have accumulated diverse types of data. Based on these types of expression data, various computational methods have been proposed to predict cancer subtypes. It is crucial to study how to better integrate these multiple profiles of data. In this paper, we collect multiple profiles of data for five cancers on The Cancer Genome Atlas (TCGA). Then, we construct three similarity kernels for all patients of the same cancer by gene expression, miRNA expression and isoform expression data. We also propose a novel unsupervised multiple kernel fusion method, Similarity Kernel Fusion (SKF), in order to integrate three similarity kernels into one combined kernel. Finally, we make use of spectral clustering on the integrated kernel to predict cancer subtypes. In the experimental results, the P-values from the Cox regression model and survival curve analysis can be used to evaluate the performance of predicted subtypes on three datasets. Our kernel fusion method, SKF, has outstanding performance compared with single kernel and other multiple kernel fusion strategies. It demonstrates that our method can accurately identify more accurate subtypes on various kinds of cancers. Our cancer subtype prediction method can identify essential genes and biomarkers for disease diagnosis and prognosis, and we also discuss the possible side effects of therapies and treatment.

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Limin Jiang

Lineage extinction and replacement in dengue type 1 virus populations are due to stochastic events rather than to natural selection

BP Neural Network Could Help Improve Pre-miRNA Identification in Various Species

MDA-SKF: Similarity Kernel Fusion for Accurately Discovering miRNA-Disease Association

Discovering Cancer Subtypes via an Accurate Fusion Strategy on Multiple Profile Data

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