MLLGBIO-PHBMOct 14, 2021

Deep learning models for predicting RNA degradation via dual crowdsourcing

arXiv:2110.07531v232 citations
Originality Incremental advance
AI Analysis

This work addresses the thermostability issue in mRNA-based medicines, which is crucial for global distribution, though it is incremental as it builds on existing methods with new data and integration.

The researchers tackled the problem of predicting RNA degradation to design more stable mRNA therapeutics by using a dual crowdsourcing approach to generate data and develop models, achieving 41% of nucleotide-level predictions within experimental error and improved accuracy on longer mRNA molecules.

Messenger RNA-based medicines hold immense potential, as evidenced by their rapid deployment as COVID-19 vaccines. However, worldwide distribution of mRNA molecules has been limited by their thermostability, which is fundamentally limited by the intrinsic instability of RNA molecules to a chemical degradation reaction called in-line hydrolysis. Predicting the degradation of an RNA molecule is a key task in designing more stable RNA-based therapeutics. Here, we describe a crowdsourced machine learning competition ("Stanford OpenVaccine") on Kaggle, involving single-nucleotide resolution measurements on 6043 102-130-nucleotide diverse RNA constructs that were themselves solicited through crowdsourcing on the RNA design platform Eterna. The entire experiment was completed in less than 6 months, and 41% of nucleotide-level predictions from the winning model were within experimental error of the ground truth measurement. Furthermore, these models generalized to blindly predicting orthogonal degradation data on much longer mRNA molecules (504-1588 nucleotides) with improved accuracy compared to previously published models. Top teams integrated natural language processing architectures and data augmentation techniques with predictions from previous dynamic programming models for RNA secondary structure. These results indicate that such models are capable of representing in-line hydrolysis with excellent accuracy, supporting their use for designing stabilized messenger RNAs. The integration of two crowdsourcing platforms, one for data set creation and another for machine learning, may be fruitful for other urgent problems that demand scientific discovery on rapid timescales.

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