applying unmixing to gene expression data for tumor phylogeny inference将分离应用于肿瘤基因表达数据发展史推理.pdfVIP
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applying unmixing to gene expression data for tumor phylogeny inference将分离应用于肿瘤基因表达数据发展史推理
Schwartz and Shackney BMC Bioinformatics 2010, 11:42
/1471-2105/11/42
METHODOLOGY ARTICLE Open Access
Applying unmixing to gene expression data for
tumor phylogeny inference
Russell Schwartz1*, Stanley E Shackney2
Abstract
Background: While in principle a seemingly infinite variety of combinations of mutations could result in tumor
development, in practice it appears that most human cancers fall into a relatively small number of “sub-types,”
each characterized a roughly equivalent sequence of mutations by which it progresses in different patients. There
is currently great interest in identifying the common sub-types and applying them to the development of
diagnostics or therapeutics. Phylogenetic methods have shown great promise for inferring common patterns of
tumor progression, but suffer from limits of the technologies available for assaying differences between and within
tumors. One approach to tumor phylogenetics uses differences between single cells within tumors, gaining
valuable information about intra-tumor heterogeneity but allowing only a few markers per cell. An alternative
approach uses tissue-wide measures of whole tumors to provide a detailed picture of averaged tumor state but at
the cost of losing information about intra-tumor heterogeneity.
Results: The present work applies “unmixing” methods, which separate complex data sets into combinations of
simpler components, to attempt to gain advantages of both tissue-wide and single-cell approaches to cancer
phylogenetics. We develop an unmixing method to infer recurring cell states from microarray measurements of
tumor populations and use the inferred mixtures of states in individual tumors to identify possible evolutionary
relationships among tumor cells. Validation on simulated data shows the method can accurately separate small
numbers of cell state
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