Joint Modeling and Registration of Cell Populations in Cohorts of High-Dimensional Flow Cytometric Data
Identifieur interne : 001B78 ( Ncbi/Curation ); précédent : 001B77; suivant : 001B79Joint Modeling and Registration of Cell Populations in Cohorts of High-Dimensional Flow Cytometric Data
Auteurs : Saumyadipta Pyne [Inde] ; Sharon X. Lee [Australie] ; Kui Wang [Australie] ; Jonathan Irish [États-Unis] ; Pablo Tamayo [États-Unis] ; Marc-Danie Nazaire [États-Unis] ; Tarn Duong [France] ; Shu-Kay Ng [Australie] ; David Hafler [États-Unis] ; Ronald Levy [États-Unis] ; Garry P. Nolan [États-Unis] ; Jill Mesirov [États-Unis] ; Geoffrey J. Mclachlan [Australie]Source :
- PLoS ONE [ 1932-6203 ] ; 2014.
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- KwdFr :
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English descriptors
- KwdEn :
- MESH :
Abstract
In biomedical applications, an experimenter encounters different potential sources of variation in data such as individual samples, multiple experimental conditions, and multivariate responses of a panel of markers such as from a signaling network. In multiparametric cytometry, which is often used for analyzing patient samples, such issues are critical. While computational methods can identify cell populations in individual samples, without the ability to automatically match them across samples, it is difficult to compare and characterize the populations in typical experiments, such as those responding to various stimulations or distinctive of particular patients or time-points, especially when there are many samples. Joint Clustering and Matching (JCM) is a multi-level framework for simultaneous modeling and registration of populations across a cohort. JCM models every population with a robust multivariate probability distribution. Simultaneously, JCM fits a random-effects model to construct an overall batch template – used for registering populations across samples, and classifying new samples. By tackling systems-level variation, JCM supports practical biomedical applications involving large cohorts. Software for fitting the JCM models have been implemented in an R package EMMIX-JCM, available from
Url:
DOI: 10.1371/journal.pone.0100334
PubMed: 24983991
PubMed Central: 4077578
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PMC:4077578Le document en format XML
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<front><div type="abstract" xml:lang="en"><p>In biomedical applications, an experimenter encounters different potential sources of variation in data such as individual samples, multiple experimental conditions, and multivariate responses of a panel of markers such as from a signaling network. In multiparametric cytometry, which is often used for analyzing patient samples, such issues are critical. While computational methods can identify cell populations in individual samples, without the ability to automatically match them across samples, it is difficult to compare and characterize the populations in typical experiments, such as those responding to various stimulations or distinctive of particular patients or time-points, especially when there are many samples. Joint Clustering and Matching (JCM) is a multi-level framework for simultaneous modeling and registration of populations across a cohort. JCM models every population with a robust multivariate probability distribution. Simultaneously, JCM fits a random-effects model to construct an overall batch template – used for registering populations across samples, and classifying new samples. By tackling systems-level variation, JCM supports practical biomedical applications involving large cohorts. Software for fitting the JCM models have been implemented in an R package EMMIX-JCM, available from <ext-link ext-link-type="uri" xlink:href="http://www.maths.uq.edu.au/~gjm/mix_soft/EMMIX-JCM/">http://www.maths.uq.edu.au/~gjm/mix_soft/EMMIX-JCM/</ext-link>
.</p>
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<back><div1 type="bibliography"><listBibl><biblStruct><analytic><author><name sortKey="Irish, Jm" uniqKey="Irish J">JM Irish</name>
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<author><name sortKey="Kotecha, N" uniqKey="Kotecha N">N Kotecha</name>
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<author><name sortKey="Nolan, Gp" uniqKey="Nolan G">GP Nolan</name>
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<author><name sortKey="Chattopadhyay, Pk" uniqKey="Chattopadhyay P">PK Chattopadhyay</name>
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<author><name sortKey="Roederer, M" uniqKey="Roederer M">M Roederer</name>
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