Towards a potential pan-cancer prognostic signature for gene expression based on probesets and ensemble machine learning.
Davide ChiccoAbbas AlameerSara RahmatiGiuseppe JurmanPublished in: BioData mining (2022)
Cancer is one of the leading causes of death worldwide and can be caused by environmental aspects (for example, exposure to asbestos), by human behavior (such as smoking), or by genetic factors. To understand which genes might be involved in patients' survival, researchers have invented prognostic genetic signatures: lists of genes that can be used in scientific analyses to predict if a patient will survive or not. In this study, we joined together five different prognostic signatures, each of them related to a specific cancer type, to generate a unique pan-cancer prognostic signature, that contains 207 unique probesets related to 187 unique gene symbols, with one particular probeset present in two cancer type-specific signatures (203072_at related to the MYO1E gene). We applied our proposed pan-cancer signature with the Random Forests machine learning method to 57 microarray gene expression datasets of 12 different cancer types, and analyzed the results. We also compared the performance of our pan-cancer signature with the performances of two alternative prognostic signatures, and with the performances of each cancer type-specific signature on their corresponding cancer type-specific datasets. Our results confirmed the effectiveness of our prognostic pan-cancer signature. Moreover, we performed a pathway enrichment analysis, which indicated an association between the signature genes and a protein-protein interaction analysis, that highlighted PIK3R2 and FN1 as key genes having a fundamental relevance in our signature, suggesting an important role in pan-cancer prognosis for both of them.
Keyphrases
- papillary thyroid
- gene expression
- squamous cell
- machine learning
- genome wide
- randomized controlled trial
- dna methylation
- chronic kidney disease
- protein protein
- young adults
- squamous cell carcinoma
- end stage renal disease
- childhood cancer
- small molecule
- systematic review
- endothelial cells
- climate change
- transcription factor
- copy number
- ejection fraction
- convolutional neural network
- patient reported outcomes
- peritoneal dialysis
- single cell