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- W3080644311 abstract "ABSTRACT Understanding the functional impact of cancer somatic mutations represents a critical knowledge gap for implementing precision oncology. It has been increasingly appreciated that the ‘edgotype’ of a genomic mutation provides a fundamental link between genotype and phenotype. However, specific effects on biological signaling networks for the majority of mutations are largely unknown by experimental approaches. To resolve this challenge, we developed e-MutPath, a network-based computational method to identify candidate ‘edgetic’ mutations that perturb functional pathways. e-MutPath identifies informative paths that could be used to distinguish disease risk factors from neutral elements and to stratify disease subtypes with clinical relevance. The predicted targets are enriched in cancer vulnerability genes, known drug targets but depleted for proteins associated with side effects, demonstrating the power of network-based strategies to investigate the functional impact and perturbation profiles of genomic mutations. Together, e-MutPath represents a robust computational tool to systematically assign functions to genetic mutations, especially in the context of their specific pathway perturbation effect. The code for e-MutPath is available as a user-friendly R package at the GitHub website ( https://github.com/lyshaerbin/eMutPath )." @default.
- W3080644311 created "2020-09-01" @default.
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- W3080644311 date "2020-08-24" @default.
- W3080644311 modified "2023-09-24" @default.
- W3080644311 title "e-MutPath: Computational modelling reveals the functional landscape of genetic mutations rewiring interactome networks" @default.
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- W3080644311 doi "https://doi.org/10.1101/2020.08.22.262386" @default.
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