Accounting for digestion enzyme bias in Casanovo

Abstract

AbstractA key parameter of any proteomics mass spectrometry experiment is the identity of the enzyme that is used to digest proteins in the sample into peptides. The Casanovode novosequencing model was trained using data that was generated with trypsin digestion; consequently, the model prefers to predict peptides that end with the amino acids “K” or “R.” This bias is desirable when the Casanovo is used to analyze data that was also generated using trypsin but can be problematic if the data was generated using some other digestion enzyme. In this work, we modify Casanovo to take as input the identify of the digestion enzyme, alongside each observed spectrum. We then train Casanovo with data generated using several different restriction enzymes, and we demonstrate that the resulting model successfully learns to capture enzyme-specific behavior. However, we find, surprisingly, that this new model does not yield a significant improvement in sequencing accuracy relative to a model trained without the enzyme information but using the same training set. This observation may have important implications for future attempts to make use of experimental metadata inde novosequencing models.