Project description:Identification of novel molecular subtypes of disease using multi-source 'omics data is an active area of on-going research. Integrative clustering is a powerful approach to identify latent subtype structure inherent in the data sets accounting for both between and within data correlations. We propose a new integrative network-based clustering method using the non-negative matrix factorization, nNMF, for clustering multiple types of interrelated datasets assayed on same tumor-samples. nNMF utilizes the consensus matrices generated using the non-negative matrix factorization (NMF) algorithm on each type of data as networks among the patient samples. The multiple networks are then combined, and a comprehensive network structure is created optimizing the strengths of the relationships. A spectral clustering algorithm is then used on the final network data to determine the cluster groups. nNMF is a non-parametric method and therefore prior assumptions on the statistical distribution of data is not required. The application of the proposed nNMF method has been provided with simulated and the real-life datasets obtained from The Cancer Genome Atlas studies on glioblastoma, lower grade glioma and head and neck cancer. nNMF was found to be working competitively with previous methods and sometimes better as compared to previous NMF or model-based method especially when the signal to noise ratio is small. The novel nNMF method allows researchers to utilize such relationships to identify the latent subtype structure inherent in the data so that further association studies can be carried out. The R program for the nNMF will be available upon request.

Project description:Identification of clinically relevant tumor subtypes and omics signatures is an important task in cancer translational research for precision medicine. Large-scale genomic profiling studies such as The Cancer Genome Atlas (TCGA) Research Network have generated vast amounts of genomic, transcriptomic, epigenomic, and proteomic data. While these studies have provided great resources for researchers to discover clinically relevant tumor subtypes and driver molecular alterations, there are few computationally efficient methods and tools for integrative clustering analysis of these multi-type omics data. Therefore, the aim of this article is to develop a fully Bayesian latent variable method (called iClusterBayes) that can jointly model omics data of continuous and discrete data types for identification of tumor subtypes and relevant omics features. Specifically, the proposed method uses a few latent variables to capture the inherent structure of multiple omics data sets to achieve joint dimension reduction. As a result, the tumor samples can be clustered in the latent variable space and relevant omics features that drive the sample clustering are identified through Bayesian variable selection. This method significantly improve on the existing integrative clustering method iClusterPlus in terms of statistical inference and computational speed. By analyzing TCGA and simulated data sets, we demonstrate the excellent performance of the proposed method in revealing clinically meaningful tumor subtypes and driver omics features.

Project description:We consider the problem of model-based clustering in the presence of many correlated, mixed continuous, and discrete variables, some of which may have missing values. Discrete variables are treated with a latent continuous variable approach, and the Dirichlet process is used to construct a mixture model with an unknown number of components. Variable selection is also performed to identify the variables that are most influential for determining cluster membership. The work is motivated by the need to cluster patients thought to potentially have autism spectrum disorder on the basis of many cognitive and/or behavioral test scores. There are a modest number of patients (486) in the data set along with many (55) test score variables (many of which are discrete valued and/or missing). The goal of the work is to (1) cluster these patients into similar groups to help identify those with similar clinical presentation and (2) identify a sparse subset of tests that inform the clusters in order to eliminate unnecessary testing. The proposed approach compares very favorably with other methods via simulation of problems of this type. The results of the autism spectrum disorder analysis suggested 3 clusters to be most likely, while only 4 test scores had high (>0.5) posterior probability of being informative. This will result in much more efficient and informative testing. The need to cluster observations on the basis of many correlated, continuous/discrete variables with missing values is a common problem in the health sciences as well as in many other disciplines.

Project description:Many applications of biomedical science involve unobservable constructs, from measurement of health states to severity of complex diseases. The primary aim of measurement is to identify relevant pieces of observable information that thoroughly describe the construct of interest. Validation of the construct is often performed separately. Noting the increasing popularity of latent variable methods in biomedical research, we propose a Multiple Indicator Multiple Cause (MIMIC) latent variable model that combines item reduction and validation. Our joint latent variable model accounts for the bias that occurs in the traditional 2-stage process. The methods are motivated by an example from the Physical Activity and Lymphedema clinical trial in which the objectives were to describe lymphedema severity through self-reported Likert scale symptoms and to determine the relationship between symptom severity and a "gold standard" diagnostic measure of lymphedema. The MIMIC model identified 1 symptom as a potential candidate for removal. We present this paper as an illustration of the advantages of joint latent variable models and as an example of the applicability of these models for biomedical research.

Project description:Next-generation sequencing (NGS) technology has become a trend in the genomics research area. There are many software programs and automated pipelines to analyze NGS data, which can ease the pain for traditional scientists who are not familiar with computer programming. However, downstream analyses, such as finding differentially expressed genes or visualizing linkage disequilibrium maps and genome-wide association study (GWAS) data, still remain a challenge. Here, we introduce a dockerized web application written in R using the Shiny platform to visualize pre-analyzed RNA sequencing and GWAS data. In addition, we have integrated a genome browser based on the JBrowse platform and an automated intermediate parsing process required for custom track construction, so that users can easily build and navigate their personal genome tracks with in-house datasets. This application will help scientists perform series of downstream analyses and obtain a more integrative understanding about various types of genomic data by interactively visualizing them with customizable options.

Project description:The Agincourt Health and Demographic Surveillance System has since 2001 conducted a biannual household asset survey in order to quantify household socio-economic status (SES) in a rural population living in northeast South Africa. The survey contains binary, ordinal and nominal items. In the absence of income or expenditure data, the SES landscape in the study population is explored and described by clustering the households into homogeneous groups based on their asset status. A model-based approach to clustering the Agincourt households, based on latent variable models, is proposed. In the case of modeling binary or ordinal items, item response theory models are employed. For nominal survey items, a factor analysis model, similar in nature to a multinomial probit model, is used. Both model types have an underlying latent variable structure-this similarity is exploited and the models are combined to produce a hybrid model capable of handling mixed data types. Further, a mixture of the hybrid models is considered to provide clustering capabilities within the context of mixed binary, ordinal and nominal response data. The proposed model is termed a mixture of factor analyzers for mixed data (MFA-MD). The MFA-MD model is applied to the survey data to cluster the Agincourt households into homogeneous groups. The model is estimated within the Bayesian paradigm, using a Markov chain Monte Carlo algorithm. Intuitive groupings result, providing insight to the different socio-economic strata within the Agincourt region.

Project description:Background:Soft tissue sarcomas (STSs) are heterogeneous at the clinical and molecular level and need to be further sub-clustered for treatment and prognosis. Materials And Methods:STSs were sub-clustered based on RNAseq and miRNAseq data extracted from The Cancer Genome Atlas (TCGA) through the combined process of similarity network fusion (SNF) and consensus clustering (CC). The expression and clinical characteristics of each sub-cluster were analyzed. The genes differentially expressed (lncRNAs, miRNAs, and mRNAs) between the poor prognosis and good prognosis clusters were used to construct a competing endogenous RNA (ceRNA) network. Functional enrichment analysis was conducted and a hub network was extracted from the constructed ceRNA network. Results:A total of 247 STSs were classified into three optimal sub-clusters, and patients in cluster 2 (C2) had a significantly lower rate of survival. A ceRNA network with 91 nodes and 167 edges was constructed according to the hypothesis of ceRNA. Functional enrichment analysis revealed that the network was mainly associated with organism development functions. Moreover, LncRNA (KCNQ1OT1)-miRNA (has-miR-29c-3p)-mRNA (JARID2, CDK8, DNMT3A, TET1)-competing endogenous gene pairs were identified as hub networks of the ceRNA network, in which each component showed survival significance. Conclusion:Integrative clustering analysis revealed that the STSs could be clustered into three sub-clusters. The ceRNA network, especially the subnetwork LncRNA (KCNQ1OT1)-miRNA (has-miR-29c-3p)-mRNA (JARID2, CDK8, DNMT3A, TET1) was a promising therapeutic target for the STS sub-cluster associated with a poor prognosis.

Project description:MotivationDiverse applications-particularly in tumour subtyping-have demonstrated the importance of integrative clustering techniques for combining information from multiple data sources. Cluster Of Clusters Analysis (COCA) is one such approach that has been widely applied in the context of tumour subtyping. However, the properties of COCA have never been systematically explored, and its robustness to the inclusion of noisy datasets is unclear.ResultsWe rigorously benchmark COCA, and present Kernel Learning Integrative Clustering (KLIC) as an alternative strategy. KLIC frames the challenge of combining clustering structures as a multiple kernel learning problem, in which different datasets each provide a weighted contribution to the final clustering. This allows the contribution of noisy datasets to be down-weighted relative to more informative datasets. We compare the performances of KLIC and COCA in a variety of situations through simulation studies. We also present the output of KLIC and COCA in real data applications to cancer subtyping and transcriptional module discovery.Availability and implementationR packages klic and coca are available on the Comprehensive R Archive Network.Supplementary informationSupplementary data are available at Bioinformatics online.

Project description:Emerging evidence suggests that a genetic variant can affect multiple phenotypes, especially in complex human diseases. Therefore, joint analysis of multiple phenotypes may offer new insights into disease etiology. Recently, many statistical methods have been developed for joint analysis of multiple phenotypes, including the clustering linear combination (CLC) method. Due to the unknown number of clusters for a given data, a simulation procedure must be used to evaluate the p-value of the final test statistic of CLC. This makes the CLC method computationally demanding. In this paper, we use a stopping criterion to determine the number of clusters in the CLC method. We have named our method, hierarchical clustering CLC (HCLC). HCLC has an asymptotic distribution, which is very computationally efficient and makes it applicable for genome-wide association studies. Extensive simulations together with the COPDGene data analysis have been used to assess the type I error rates and power of our proposed method. Our simulation results demonstrate that the type I error rates of HCLC are effectively controlled in different realistic settings. HCLC either outperforms all other methods or has statistical power that is very close to the most powerful method with which it has been compared.

Project description:BACKGROUND:The increased multi-omics information on carefully phenotyped patients in studies of complex diseases requires novel methods for data integration. Unlike continuous intensity measurements from most omics data sets, phenome data contain clinical variables that are binary, ordinal and categorical. RESULTS:In this paper we introduce an integrative phenotyping framework (iPF) for disease subtype discovery. A feature topology plot was developed for effective dimension reduction and visualization of multi-omics data. The approach is free of model assumption and robust to data noises or missingness. We developed a workflow to integrate homogeneous patient clustering from different omics data in an agglomerative manner and then visualized heterogeneous clustering of pairwise omics sources. We applied the framework to two batches of lung samples obtained from patients diagnosed with chronic obstructive lung disease (COPD) or interstitial lung disease (ILD) with well-characterized clinical (phenomic) data, mRNA and microRNA expression profiles. Application of iPF to the first training batch identified clusters of patients consisting of homogenous disease phenotypes as well as clusters with intermediate disease characteristics. Analysis of the second batch revealed a similar data structure, confirming the presence of intermediate clusters. Genes in the intermediate clusters were enriched with inflammatory and immune functional annotations, suggesting that they represent mechanistically distinct disease subphenotypes that may response to immunomodulatory therapies. The iPF software package and all source codes are publicly available. CONCLUSIONS:Identification of subclusters with distinct clinical and biomolecular characteristics suggests that integration of phenomic and other omics information could lead to identification of novel mechanism-based disease sub-phenotypes.