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- W2950704620 abstract "Target selection is the first and pivotal step in drug discovery. An incorrect choice may not manifest itself for many years after hundreds of millions of research dollars have been spent. We collected a set of 332 targets that succeeded or failed in phase III clinical trials, and explored whether Omic features describing the target genes could predict clinical success. We obtained features from the recently published comprehensive resource: Harmonizome. Nineteen features appeared to be significantly correlated with phase III clinical trial outcomes, but only 4 passed validation schemes that used bootstrapping or modified permutation tests to assess feature robustness and generalizability while accounting for target class selection bias. We also used classifiers to perform multivariate feature selection and found that classifiers with a single feature performed as well in cross-validation as classifiers with more features (AUROC = 0.57 and AUPR = 0.81). The two predominantly selected features were mean mRNA expression across tissues and standard deviation of expression across tissues, where successful targets tended to have lower mean expression and higher expression variance than failed targets. This finding supports the conventional wisdom that it is favorable for a target to be present in the tissue(s) affected by a disease and absent from other tissues. Overall, our results suggest that it is feasible to construct a model integrating interpretable target features to inform target selection. We anticipate deeper insights and better models in the future, as researchers can reuse the data we have provided to improve methods for handling sample biases and learn more informative features. Code, documentation, and data for this study have been deposited on GitHub at https://github.com/arouillard/omic-features-successful-targets." @default.
- W2950704620 created "2019-06-27" @default.
- W2950704620 creator A5007100650 @default.
- W2950704620 creator A5033246609 @default.
- W2950704620 creator A5040334133 @default.
- W2950704620 date "2018-05-21" @default.
- W2950704620 modified "2023-10-17" @default.
- W2950704620 title "Systematic interrogation of diverse Omic data reveals interpretable, robust, and generalizable transcriptomic features of clinically successful therapeutic targets" @default.
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- W2950704620 doi "https://doi.org/10.1371/journal.pcbi.1006142" @default.
- W2950704620 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/5983857" @default.
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- W2950704620 hasPublicationYear "2018" @default.
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