Your search keyword '"Dounavi, Maria Eleni"' showing total 5 results

1. Modifiable and non-modifiable risk factors of dementia on midlife cerebral small vessel disease in cognitively healthy middle-aged adults: the PREVENT-Dementia study

Author

Low, Audrey, Prats-Sedano, Maria A., McKiernan, Elizabeth, Carter, Stephen F., Stefaniak, James D., Nannoni, Stefania, Su, Li, Dounavi, Maria-Eleni, Muniz-Terrera, Graciela, Ritchie, Karen, Lawlor, Brian, Naci, Lorina, Malhotra, Paresh, Mackay, Clare, Koychev, Ivan, Ritchie, Craig W., Markus, Hugh S., and O’Brien, John T.

Published

2022

2. Texture‐based morphometry in relation to apolipoprotein ε4 genotype, ageing and sex in a midlife population.

Author

Dounavi, Maria‐Eleni, Mak, Elijah, Operto, Gregory, Muniz‐Terrera, Graciela, Bridgeman, Katie, Koychev, Ivan, Malhotra, Paresh, Naci, Lorina, Lawlor, Brian, Su, Li, Falcon, Carles, Ritchie, Karen, Ritchie, Craig W., Gispert, Juan Domingo, and O'Brien, John T.

Subjects

*OLDER people, *ALZHEIMER'S disease, *APOLIPOPROTEIN E4, *CEREBRAL cortical thinning, *DISEASE risk factors

Abstract

Brain atrophy and cortical thinning are typically observed in people with Alzheimer's disease (AD) and, to a lesser extent, in those with mild cognitive impairment. In asymptomatic middle‐aged apolipoprotein ε4 (ΑPOE4) carriers, who are at higher risk of future AD, study reports are discordant with limited evidence of brain structural differences between carriers and non‐carriers of the ε4 allele. Alternative imaging markers with higher sensitivity at the presymptomatic stage, ideally quantified using typically acquired structural MRI scans, would thus be of great benefit for the detection of early disease, disease monitoring and subject stratification. In the present cross‐sectional study, we investigated textural properties of T1‐weighted 3T MRI scans in relation to APOE4 genotype, age and sex. We pooled together data from the PREVENT‐Dementia and ALFA studies focused on midlife healthy populations with dementia risk factors (analysable cohort: 1585 participants; mean age 56.2 ± 7.4 years). Voxel‐based and texture (examined features: contrast, entropy, energy, homogeneity) based morphometry was used to identify areas of volumetric and textural differences between APOE4 carriers and non‐carriers. Textural maps were generated and were subsequently harmonised using voxel‐wise COMBAT. For all analyses, APOE4, sex, age and years of education were used as model predictors. Interactions between APOE4 and age were further examined. There were no group differences in regional brain volume or texture based on APOE4 carriership or when age × APOE4 interactions were examined. Older people tended to have a less homogeneous textural profile in grey and white matter and a more homogeneous profile in the ventricles. A more heterogeneous textural profile was observed for females in areas such as the ventricles, frontal and parietal lobes and for males in the brainstem, cerebellum, precuneus and cingulate. Overall, we have shown the absence of volumetric and textural differences between APOE4 carriers and non‐carriers at midlife and have established associations of textural features with ageing and sex. [ABSTRACT FROM AUTHOR]

Published

2024

3. Differential association of cerebral blood flow and anisocytosis in APOE ε4 carriers at midlife.

Author

Dounavi, Maria-Eleni, Mak, Elijah, Swann, Peter, Low, Audrey, Muniz-Terrera, Graciela, McKeever, Anna, Pope, Marianna, Williams, Guy B, Wells, Katie, Lawlor, Brian, Naci, Lorina, Malhotra, Paresh, Mackay, Clare, Koychev, Ivan, Ritchie, Karen, Su, Li, Ritchie, Craig W, and O'Brien, John T

Abstract

Cerebral hemodynamic alterations have been observed in apolipoprotein ε4 (APOE4) carriers at midlife, however the physiological underpinnings of this observation are poorly understood. Our goal was to investigate cerebral blood flow (CBF) and its spatial coefficient of variation (CoV) in relation to APOE4 and a measure of erythrocyte anisocytosis (red blood cell distribution width – RDW) in a middle-aged cohort. Data from 563 participants in the PREVENT-Dementia study scanned with 3 T MRI cross-sectionally were analysed. Voxel-wise and region-of-interest analyses within nine vascular regions were run to detect areas of altered perfusion. Within the vascular regions, interaction terms between APOE4 and RDW in predicting CBF were examined. Areas of hyperperfusion in APOE4 carriers were detected mainly in frontotemporal regions. The APOE4 allele differentially moderated the association between RDW and CBF, an association which was more prominent in the distal vascular territories (p – [0.01, 0.05]). The CoV was not different between the considered groups. We provide novel evidence that in midlife, RDW and CBF are differentially associated in APOE4 carriers and non-carriers. This association is consistent with a differential hemodynamic response to hematological alterations in APOE4 carriers. [ABSTRACT FROM AUTHOR]

Published

2023

4. Proximity to dementia onset and multi-modal neuroimaging changes: The prevent-dementia study.

Author

Mak, Elijah, Dounavi, Maria-Eleni, Low, Audrey, Carter, Stephen F., McKiernan, Elizabeth, Williams, Guy B, Jones, P Simon, Carriere, Isabelle, Muniz, Graciela Terrera, Ritchie, Karen, Ritchie, Craig, Su, Li, and O'Brien, John T

Subjects

*DEMENTIA, *MIDDLE-aged persons, *ALZHEIMER'S disease, *WHITE matter (Nerve tissue), *CORPUS callosum, *HYPERPERFUSION, *SENILE dementia

Abstract

First-degree relatives of people with dementia (FH+) are at increased risk of developing Alzheimer's disease (AD). Here, we investigate "estimated years to onset of dementia" (EYO) as a surrogate marker of preclinical disease progression and assess its associations with multi-modal neuroimaging biomarkers. 89 FH+ participants in the PREVENT-Dementia study underwent longitudinal MR imaging over 2 years. EYO was calculated as the difference between the parental age of dementia diagnosis and the current age of the participant (mean EYO = 23.9 years). MPRAGE, ASL and DWI data were processed using Freesurfer, FSL-BASIL and DTI-TK. White matter lesion maps were segmented from FLAIR scans. The SPM Sandwich Estimator Toolbox was used to test for the main effects of EYO and interactions between EYO, Time, and APOE-ε4+. Threshold free cluster enhancement and family wise error rate correction (TFCE FWER) was performed on voxelwise statistical maps. There were no significant effects of EYO on regional grey matter atrophy or white matter hyperintensities. However, a shorter EYO was associated with lower white matter Fractional Anisotropy and elevated Mean/Radial Diffusivity, particularly in the corpus callosum (TFCE FWER p < 0.05). The influence of EYO on white matter deficits were significantly stronger compared to that of normal ageing. APOE-ε4 carriers exhibited hyperperfusion with nearer proximity to estimated onset in temporo-parietal regions. There were no interactions between EYO and time, suggesting that EYO was not associated with accelerated imaging changes in this sample. Amongst cognitively normal midlife adults with a family history of dementia, a shorter hypothetical proximity to dementia onset may be associated with incipient brain abnormalities, characterised by white matter disruptions and perfusion abnormalities, particularly amongst APOE-ε4 carriers. Our findings also confer biological validity to the construct of EYO as a potential stage marker of preclinical progression in the context of sporadic dementia. Further clinical follow-up of our longitudinal sample would provide critical validation of these findings. [ABSTRACT FROM AUTHOR]

Published

2021

5. Inherited risk of dementia and the progression of cerebral small vessel disease and inflammatory markers in cognitively healthy midlife adults: the PREVENT-Dementia study.

Author

Low, Audrey, Su, Li, Stefaniak, James D., Mak, Elijah, Dounavi, Maria-Eleni, Muniz-Terrera, Graciela, Ritchie, Karen, Ritchie, Craig W., Markus, Hugh S., and O'Brien, John T.

Subjects

*CEREBRAL small vessel diseases, *MIDDLE-aged persons, *DEMENTIA, *ALZHEIMER'S disease

Abstract

Cerebral small vessel disease (SVD) and inflammation are increasingly recognized as key contributors to Alzheimer's disease (AD), although the timing, trajectory, and relation between them early in the disease process is unclear. Therefore, to investigate very early-stage changes, we compared 158 healthy midlife adults with and without inherited AD predisposition (APOE4 carriership (38% positive), parental family history (FH) of dementia (54% positive)) on markers of SVD (white matter hyperintensities (WMH), cerebral microbleeds), and inflammation (C-reactive protein (CRP), fibrinogen), cross-sectionally and longitudinally over two years. While WMH severity was comparable between groups at baseline, longitudinal progression of WMH was greater in at-risk groups (APOE4+ and FH+). Topographically, APOE4 was associated exclusively with deep, but not periventricular, WMH progression after adjusting for FH. Conversely, APOE4 carriers displayed lower CRP levels than noncarriers, but not fibrinogen. Furthermore, interaction analysis showed that FH moderated the effect of SVD and inflammation on reaction time, an early feature of SVD, but not episodic memory or executive function. Findings suggest that vascular and inflammatory changes could occur decades before dementia onset, and may be of relevance in predicting incipient clinical progression. • Heritable risk factors related to SVD progression, despite lower levels of inflammation. • SVD progression had more pronounced adverse effects on reaction time in at-risk individuals. • Association between SVD and inflammation was stronger in those at-risk. [ABSTRACT FROM AUTHOR]

Published

2021