Enhancing the utility of Proteomics Signature Profiling (PSP) with Pathway Derived Subnets (PDSs) performance analysis and specialised ontologies

摘要

BackgroundProteomics Signature Profiling (PSP) is a novel hit-rate based method that proved useful in resolving consistency and coverage issues in proteomics. As a follow-up study, several points need to be addressed: 1/ PSP’s generalisability to pathways, 2/ understanding the biological interplay between significant complexes and pathway subnets co-located on the same pathways on our liver cancer dataset, 3/ understanding PSP’s false positive rate and 4/ demonstrating that PSP works on other suitable proteomics datasets as well as expanding PSP’s analytical resolution via the use of specialised ontologies.