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From a deep learning model back to the brain-Identifying regional predictors and their relation to aging. | LitMetric

AI Article Synopsis

  • A new Deep Learning framework predicts chronological age using structural MRI scans and demonstrates strong correlations with actual age and neurodegenerative indicators.
  • Previous approaches yielded unreliable pixel-wise explanation maps, but the new method combines maps across subjects to create more consistent, population-based results.
  • Analysis revealed that cerebrospinal fluid cavities are significant for age prediction, enhancing the understanding of brain aging and offering improved replicability compared to traditional methods.

Article Abstract

We present a Deep Learning framework for the prediction of chronological age from structural magnetic resonance imaging scans. Previous findings associate increased brain age with neurodegenerative diseases and higher mortality rates. However, the importance of brain age prediction goes beyond serving as biomarkers for neurological disorders. Specifically, utilizing convolutional neural network (CNN) analysis to identify brain regions contributing to the prediction can shed light on the complex multivariate process of brain aging. Previous work examined methods to attribute pixel/voxel-wise contributions to the prediction in a single image, resulting in "explanation maps" that were found noisy and unreliable. To address this problem, we developed an inference scheme for combining these maps across subjects, thus creating a population-based, rather than a subject-specific map. We applied this method to a CNN ensemble trained on predicting subjects' age from raw T1 brain images in a lifespan sample of 10,176 subjects. Evaluating the model on an untouched test set resulted in mean absolute error of 3.07 years and a correlation between chronological and predicted age of r = 0.98. Using the inference method, we revealed that cavities containing cerebrospinal fluid, previously found as general atrophy markers, had the highest contribution for age prediction. Comparing maps derived from different models within the ensemble allowed to assess differences and similarities in brain regions utilized by the model. We showed that this method substantially increased the replicability of explanation maps, converged with results from voxel-based morphometry age studies and highlighted brain regions whose volumetric variability correlated the most with the prediction error.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7426775PMC
http://dx.doi.org/10.1002/hbm.25011DOI Listing

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