Patterns of cortical atrophy and cognitive decline associated with healthy aging: a structural magnetic resonance imaging study

A number of magnetic resonance imaging (MRI) studies have investigated the relationship between aging, reduced gray matter (GM) volumes in the brain and cognitive performance, using cross-sectional designs and correlation tests. However, very few VBM studies have documented GM decrements in healthy elderlies with repeated MRI measurements obtained in the same subjects, and none of these longitudinal studies investigated the relationship between GM deficits and changes in cognitive performance over time. Also, it is unclear the extent to which the APOE e4 allele influences on longitudinal findings of GM reductions in healthy elderlies. Were initially evaluated 187 elderly subjects (over 65 years); after 3 years, a sub-sample of 55 individuals underwent a second MRI examination in a 1.5 Tesla equipment, and a cognitive re-evaluation using a structured, transculturally validated neuropsychological battery. All subjects also underwent genotyping for ascertainment of the presence of the APOEe4 allele, as well as clinical assessment of cardiovascular risk according with Framingham scores (FRS). Using voxel-based morphometry (VBM), we will test the following hypotheses: the progression of cognitive decline will be associated with volumetric reductions of GM over three years, involving the hippocampal region and the temporal and frontal neocortices; cognitive decline associated with progressive GM volume reductions will be greater in individuals with higher cardiovascular risk and carriers of the APOE?4 allele. We found global GM reductions as well as regional GM decrements that were significant in the right thalamus and left parahippocampal gyrus (p < 0.05, family-wise error corrected for multiple comparisons over the whole brain). These findings were not affected by APOE e4. A trend correlation (p=0.093) was detected between the degree of cognitive decline over time and right thalamic volume shrinkage. This finding retained statistical significance when a partial coefficient of correlation was calculated taking into account variations in FRS scores. Irrespective of APOEe4, longitudinal VBM analyses show that the hippocampal region and thalamus are critical sites where GM shrinkage is significantly greater than the degree of global brain volume reduction in healthy elders. The trend towards an association between thalamic GM decrement and cognitive performance change over time supports the recently recognized role of the thalamus in the subtle cognitive decline associated with healthy human aging (AU)