Your search keyword '"Brain-age"' showing total 3 results

1. Brain age and cognitive functioning in first-episode bipolar disorder.

Author

Chakrabarty, Trisha, Frangou, Sophia, Torres, Ivan J., Ge, Ruiyang, and Yatham, Lakshmi N.

Subjects

*BRAIN anatomy, *BRAIN, *MEMORY, *EXECUTIVE function, *COGNITION, *MAGNETIC resonance imaging, *MACHINE learning, *AGING, *ANALYSIS of covariance, *DESCRIPTIVE statistics, *RESEARCH funding, *BIPOLAR disorder, *NEURORADIOLOGY

Abstract

Background: There is significant heterogeneity in cognitive function in patients with bipolar I disorder (BDI); however, there is a dearth of research into biological mechanisms that might underlie cognitive heterogeneity, especially at disease onset. To this end, this study investigated the association between accelerated or delayed age-related brain structural changes and cognition in early-stage BDI. Methods: First episode patients with BDI (n = 80) underwent cognitive assessment to yield demographically normed composite global and domain-specific scores in verbal memory, non-verbal memory, working memory, processing speed, attention, and executive functioning. Structural magnetic resonance imaging data were also collected from all participants and subjected to machine learning to compute the brain-predicted age difference (brainPAD), calculated by subtracting chronological age from age predicted by neuroimaging data (positive brainPAD values indicating age-related acceleration in brain structural changes and negative values indicating delay). Patients were divided into tertiles based on brainPAD values, and cognitive performance compared amongst tertiles with ANCOVA. Results: Patients in the lowest (delayed) tertile of brainPAD values (brainPAD range −17.9 to −6.5 years) had significantly lower global cognitive scores (p = 0.025) compared to patients in the age-congruent tertile (brainPAD range −5.3 to 2.4 yrs), and significantly lower verbal memory scores (p = 0.001) compared to the age-congruent and accelerated (brainPAD range 2.8 to 16.1 yrs) tertiles. Conclusion: These results provide evidence linking cognitive dysfunction in the early stage of BDI to apparent delay in typical age-related brain changes. Further studies are required to assess how age-related brain changes and cognitive functioning evolve over time. [ABSTRACT FROM AUTHOR]

Published

2023

2. Advanced Brain-Age in Psychotic Psychopathology: Evidence for Transdiagnostic Neurodevelopmental Origins.

Author

Demro, Caroline, Shen, Chen, Hendrickson, Timothy J., Arend, Jessica L., Disner, Seth G., and Sponheim, Scott R.

Subjects

BRAIN, SCHIZOPHRENIA, PSYCHOSES, SCHIZOAFFECTIVE disorders, PATHOLOGICAL psychology, RESEARCH funding, AGING, QUESTIONNAIRES, PREDICTION models, BIPOLAR disorder

Abstract

Schizophrenia is characterized by abnormal brain structure such as global reductions in gray matter volume. Machine learning models trained to estimate the age of brains from structural neuroimaging data consistently show advanced brain-age to be associated with schizophrenia. Yet, it is unclear whether advanced brain-age is specific to schizophrenia compared to other psychotic disorders, and whether evidence that brain structure is "older" than chronological age actually reflects neurodevelopmental rather than atrophic processes. It is also unknown whether advanced brain-age is associated with genetic liability for psychosis carried by biological relatives of people with schizophrenia. We used the Brain-Age Regression Analysis and Computation Utility Software (BARACUS) prediction model and calculated the residualized brain-age gap of 332 adults (163 individuals with psychotic disorders: 105 schizophrenia, 17 schizoaffective disorder, 41 bipolar I disorder with psychotic features; 103 first-degree biological relatives; 66 controls). The model estimated advanced brain-ages for people with psychosis in comparison to controls and relatives, with no differences among psychotic disorders or between relatives and controls. Specifically, the model revealed an enlarged brain-age gap for schizophrenia and bipolar disorder with psychotic features. Advanced brain-age was associated with lower cognitive and general functioning in the full sample. Among relatives, cognitive performance and schizotypal symptoms were related to brain-age gap, suggesting that advanced brain-age is associated with the subtle expressions associated with psychosis. Exploratory longitudinal analyses suggested that brain aging was not accelerated in individuals with a psychotic disorder. In sum, we found that people with psychotic disorders, irrespective of specific diagnosis or illness severity, show indications of non-progressive, advanced brain-age. These findings support a transdiagnostic, neurodevelopmental formulation of structural brain abnormalities in psychotic psychopathology. [ABSTRACT FROM AUTHOR]

Published

2022

3. Towards the interpretability of deep learning models for multi-modal neuroimaging: Finding structural changes of the ageing brain

Author

Simon M. Hofmann, Frauke Beyer, Sebastian Lapuschkin, Ole Goltermann, Markus Loeffler, Klaus-Robert Müller, Arno Villringer, Wojciech Samek, A. Veronica Witte, and Publica

Subjects

Adult, Aging, Cognitive Neuroscience, Population, Neuroimaging, Biology, Convolutional neural network, Structural mri, medicine, Humans, education, Cardiovascular risk factors, Interpretability, education.field_of_study, medicine.diagnostic_test, business.industry, Deep learning, Brain, deep learning, Magnetic resonance imaging, Explainable a.i, Magnetic Resonance Imaging, Ageing, Neurology, Frontal lobe, Brain-age, Child, Preschool, Biomarker (medicine), Artificial intelligence, business, Neuroscience

Abstract

Brain-age (BA) estimates based on deep learning are increasingly used as neuroimaging biomarker for brain health; however, the underlying neural features have remained unclear. We combined ensembles of convolutional neural networks with Layer-wise Relevance Propagation (LRP) to detect which brain features contribute to BA. Trained on magnetic resonance imaging (MRI) data of a population-based study (n=2637, 18-82 years), our models estimated age accurately based on single and multiple modalities, regionally restricted and whole-brain images (mean absolute errors 3.37-3.86 years). We find that BA estimates capture aging at both small and large-scale changes, revealing gross enlargements of ventricles and subarachnoid spaces, as well as white matter lesions, and atrophies that appear throughout the brain. Divergence from expected aging reflected cardiovascular risk factors and accelerated aging was more pronounced in the frontal lobe. Applying LRP, our study demonstrates how superior deep learning models detect brain-aging in healthy and at-risk individuals throughout adulthood.

Published

2022