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• W2071676680 endingPage "e56653" @default.
• W2071676680 startingPage "e56653" @default.
• W2071676680 abstract "The molecular complexity of genetic diseases requires novel approaches to break it down into coherent biological modules. For this purpose, many disease network models have been created and analyzed. We highlight two of them, “the human diseases networks” (HDN) and “the orphan disease networks” (ODN). However, in these models, each single node represents one disease or an ambiguous group of diseases. In these cases, the notion of diseases as unique entities reduces the usefulness of network-based methods. We hypothesize that using the clinical features (pathophenotypes) to define pathophenotypic connections between disease-causing genes improve our understanding of the molecular events originated by genetic disturbances. For this, we have built a pathophenotypic similarity gene network (PSGN) and compared it with the unipartite projections (based on gene-to-gene edges) similar to those used in previous network models (HDN and ODN). Unlike these disease network models, the PSGN uses semantic similarities. This pathophenotypic similarity has been calculated by comparing pathophenotypic annotations of genes (human abnormalities of HPO terms) in the “Human Phenotype Ontology”. The resulting network contains 1075 genes (nodes) and 26197 significant pathophenotypic similarities (edges). A global analysis of this network reveals: unnoticed pairs of genes showing significant pathophenotypic similarity, a biological meaningful re-arrangement of the pathological relationships between genes, correlations of biochemical interactions with higher similarity scores and functional biases in metabolic and essential genes toward the pathophenotypic specificity and the pleiotropy, respectively. Additionally, pathophenotypic similarities and metabolic interactions of genes associated with maple syrup urine disease (MSUD) have been used to merge into a coherent pathological module. Our results indicate that pathophenotypes contribute to identify underlying co-dependencies among disease-causing genes that are useful to describe disease modularity." @default.
• W2071676680 created "2016-06-24" @default.
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• W2071676680 date "2013-02-21" @default.
• W2071676680 modified "2023-10-18" @default.
• W2071676680 title "Global Analysis of the Human Pathophenotypic Similarity Gene Network Merges Disease Module Components" @default.
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• W2071676680 doi "https://doi.org/10.1371/journal.pone.0056653" @default.
• W2071676680 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/3692732" @default.
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• W2071676680 hasPublicationYear "2013" @default.
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