Literature DB >> 33894945

SIGNAL: A web-based iterative analysis platform integrating pathway and network approaches optimizes hit selection from genome-scale assays.

Samuel Katz1, Jian Song2, Kyle P Webb2, Nicolas W Lounsbury2, Clare E Bryant3, Iain D C Fraser4.   

Abstract

Hit selection from high-throughput assays remains a critical bottleneck in realizing the potential of omic-scale studies in biology. Widely used methods such as setting of cutoffs, prioritizing pathway enrichments, or incorporating predicted network interactions offer divergent solutions yet are associated with critical analytical trade-offs. The specific limitations of these individual approaches and the lack of a systematic way by which to integrate their rankings have contributed to limited overlap in the reported results from comparable genome-wide studies and costly inefficiencies in secondary validation efforts. Using comparative analysis of parallel independent studies as a benchmark, we characterize the specific complementary contributions of each approach and demonstrate an optimal framework to integrate these methods. We describe selection by iterative pathway group and network analysis looping (SIGNAL), an integrated, iterative approach that uses both pathway and network methods to optimize gene prioritization. SIGNAL is accessible as a rapid user-friendly web-based application (https://signal.niaid.nih.gov). A record of this paper's transparent peer review is included in the Supplemental information.
Copyright © 2021. Published by Elsevier Inc.

Entities:  

Keywords:  bioinformatics; enrichment; genome-wide studies; genomics; high-throughput hit selection; network analysis; pathway analysis; prioritization; software

Mesh:

Year:  2021        PMID: 33894945      PMCID: PMC7613048          DOI: 10.1016/j.cels.2021.03.001

Source DB:  PubMed          Journal:  Cell Syst        ISSN: 2405-4712            Impact factor:   11.091


  66 in total

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