Author
Listed:
- Aditya Rao
- Thomas Joseph
- Vangala G Saipradeep
- Sujatha Kotte
- Naveen Sivadasan
- Rajgopal Srinivasan
Abstract
Introduction: Phenotype-driven rare disease gene prioritization relies on high quality curated resources containing disease, gene and phenotype annotations. However, the effectiveness of gene prioritization tools is constrained by the incomplete coverage of rare disease, phenotype and gene annotations in such curated resources. Methods: We extracted rare disease correlation pairs involving diseases, phenotypes and genes from MEDLINE abstracts and used the information propagation algorithm GCAS to build an association network. We built a tool called PRIORI-T for rare disease gene prioritization that uses this network for phenotype-driven rare disease gene prioritization. The quality of disease-gene associations in PRIORI-T was compared with resources such as DisGeNET and Open Targets in the context of rare diseases. The gene prioritization performance of PRIORI-T was evaluated using phenotype descriptions of 230 real-world rare disease clinical cases collated from recent publications, as well as compared to other gene prioritization tools such as HANRD and Orphamizer. Results: PRIORI-T contains qualitatively better associations than DisGeNET and Open Targets. Furthermore, the causal genes were captured within Top-50 for more than 40% of the real-world clinical cases and within Top-300 for more than 72% of the cases when PRIORI-T was used for gene prioritization. It outperformed other gene prioritization tools such as HANRD and Orphamizer that primarily rely on curated resources. Conclusions: PRIORI-T exhibited improved gene prioritization performance without requiring high quality curated data. Thus, it holds great promise in phenotype-driven gene prioritization for rare disease studies.
Suggested Citation
Aditya Rao & Thomas Joseph & Vangala G Saipradeep & Sujatha Kotte & Naveen Sivadasan & Rajgopal Srinivasan, 2020.
"PRIORI-T: A tool for rare disease gene prioritization using MEDLINE,"
PLOS ONE, Public Library of Science, vol. 15(4), pages 1-12, April.
Handle:
RePEc:plo:pone00:0231728
DOI: 10.1371/journal.pone.0231728
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