Efficient and generalizable prediction of molecular alterations in multiple cancer cohorts using H&E whole slide images
This work addresses the need for efficient and generalizable prediction of molecular alterations in cancer diagnostics, offering a promising incremental improvement for prioritizing samples in clinical workflows.
The authors tackled the problem of predicting multiple DNA alterations from H&E whole slide images in cancer cohorts, using a multi-task approach that outperformed biomarker-specific models, especially for rare mutations, and demonstrated generalization across independent test sets.
Molecular testing of tumor samples for targetable biomarkers is restricted by a lack of standardization, turnaround-time, cost, and tissue availability across cancer types. Additionally, targetable alterations of low prevalence may not be tested in routine workflows. Algorithms that predict DNA alterations from routinely generated hematoxylin and eosin (H&E)-stained images could prioritize samples for confirmatory molecular testing. Costs and the necessity of a large number of samples containing mutations limit approaches that train individual algorithms for each alteration. In this work, models were trained for simultaneous prediction of multiple DNA alterations from H&E images using a multi-task approach. Compared to biomarker-specific models, this approach performed better on average, with pronounced gains for rare mutations. The models reasonably generalized to independent temporal-holdout, externally-stained, and multi-site TCGA test sets. Additionally, whole slide image embeddings derived using multi-task models demonstrated strong performance in downstream tasks that were not a part of training. Overall, this is a promising approach to develop clinically useful algorithms that provide multiple actionable predictions from a single slide.