The fornix provides multiple biomarkers to characterize circuit disruption in a mouse model of Alzheimer's disease

Badea, Alexandra; Kane, Lauren P.; Qi, Yi; Foster, Mark P.; Cofer, Gary P.; Medvitz, Neil; Buckley, Anne F.; Badea, Andreas K.; Wetsel, William C.; Colton, Carol A.

doi:10.1016/j.neuroimage.2016.08.014

Cited by 32 publications

(36 citation statements)

References 104 publications

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“…This allows to model the human innate immune response, in particular with respect to the redox microenvironment, and NO production (Hoos et al, 2014). Mouse models on this genetic background expressing APP mutations present multiple AD like phenotypes (Wilcock et al, 2008;Colton et al, 2014;Kan et al, 2015;Badea et al, 2016). Here we assessed the differential effects of the interaction of the humanized NOS background with APOE3 and APOE4 alleles.…”

Section: Discussionmentioning

confidence: 99%

Identifying Vulnerable Brain Networks in Mouse Models of Genetic Risk Factors for Late Onset Alzheimer’s Disease

Badea

Shuff

et al. 2019

Front. Neuroinform.

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The major genetic risk for late onset Alzheimer's disease has been associated with the presence of APOE4 alleles. However, the impact of different APOE alleles on the brain aging trajectory, and how they interact with the brain local environment in a sex specific manner is not entirely clear. We sought to identify vulnerable brain circuits in novel mouse models with homozygous targeted replacement of the mouse ApoE gene with either human APOE3 or APOE4 gene alleles. These genes are expressed in mice that also model the human immune response to age and disease-associated challenges by expressing the human NOS2 gene in place of the mouse mNos2 gene. These mice had impaired learning and memory when assessed with the Morris water maze (MWM) and novel object recognition (NOR) tests. Ex vivo MRI-DTI analyses revealed global and local atrophy, and areas of reduced fractional anisotropy (FA). Using tensor network principal component analyses for structural connectomes, we inferred the pairwise connections which best separate APOE4 from APOE3 carriers. These involved primarily interhemispheric connections among regions of olfactory areas, the hippocampus, and the cerebellum. Our results also suggest that pairwise connections may be subdivided and clustered spatially to reveal local changes on a finer scale. These analyses revealed not just genotype, but also sex specific differences. Identifying vulnerable networks may provide targets for interventions, and a means to stratify patients.

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Section: Discussionmentioning

confidence: 99%

Identifying Vulnerable Brain Networks in Mouse Models of Genetic Risk Factors for Late Onset Alzheimer’s Disease

Badea

Shuff

et al. 2019

Front. Neuroinform.

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“…Evidence indicates the APPSwDI/Nos2−/− ( CVN-AD) mouse model replicates multiple AD pathologies [ 31 ] , Badea et al (2016) identified multivariate biomarkers that appear to predict cognitive decline. One of these biomarkers is the fornix.…”

Section: G Enetic and B Iological mentioning

confidence: 99%

Synaptic Pruning in Alzheimer’s Disease: Role of the Complement System

Brucato¹,

Benjamin²

2020

GJMR

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“…Further reductions in acquisition times come from compressed sensing [28], which several groups have implemented for mouse MRI [29][30][31]. Such advances can help translate diffusion protocols into population studies [32] incorporating multiple biomarkers from morphometry [33], microstructural properties based on diffusion [13] or magnetic susceptibility [34], or network properties [35]. Such integrative studies may better predict changes in behaviors, modeling those observed in humans with neurodegenerative conditions [34].…”

Section: Discussionmentioning

confidence: 99%

“…We need to compare 2-mm linear dimension voxel sizes in humans (corresponding to 8-mm 3 voxel volumes), vs. 0.2-0.043-mm linear dimension voxel sizes (corresponding to ∼8 × 10 −2 -8 × 10 −5 -mm 3 voxel volumes) required to distinguish similar levels of anatomical detail in mouse brains [6][7][8][9][10][11]. This increased resolution enables the observation of brain architecture at the level of cellular layers, which, therefore, can help us gain insight into the mechanistic drivers behind the etiology and progression of disease, using animal models where axonal dimensions are relatively similar to humans [12,13].…”

Section: Introductionmentioning

confidence: 99%

Optimizing Diffusion Imaging Protocols for Structural Connectomics in Mouse Models of Neurological Conditions

et al. 2020

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Network approaches provide sensitive biomarkers for neurological conditions, such as Alzheimer's disease (AD). Mouse models can help advance our understanding of underlying pathologies, by dissecting vulnerable circuits. While the mouse brain contains less white matter compared to the human brain, axonal diameters compare relatively well (e.g., ∼0.6 µm in the mouse and ∼0.65-1.05 µm in the human corpus callosum). This makes the mouse an attractive test bed for novel diffusion models and imaging protocols. Remaining questions on the accuracy and uncertainty of connectomes have prompted us to evaluate diffusion imaging protocols with various spatial and angular resolutions. We have derived structural connectomes by extracting gradient subsets from a high-spatial, high-angular resolution diffusion acquisition (120 directions, 43-µm-size voxels). We have simulated protocols with 12, 15, 20, 30, 45, 60, 80, 100, and 120 angles and at 43, 86, or 172-µm voxel sizes. The rotational stability of these schemes increased with angular resolution. The minimum condition number was achieved for 120 directions, followed by 60 and 45 directions. The percentage of voxels containing one dyad was exceeded by those with two dyads after 45 directions, and for the highest spatial resolution protocols. For the 86-or 172-µm resolutions, these ratios converged toward 55% for one and 39% for two dyads, respectively, with <7% from voxels with three dyads. Tractography errors, estimated through dyad dispersion, decreased most with angular resolution. Spatial resolution effects became noticeable at 172 µm. Smaller tracts, e.g., the fornix, were affected more than larger ones, e.g., the fimbria. We observed an inflection point for 45 directions, and an asymptotic behavior after 60 directions, corresponding to similar projection density maps. Spatially downsampling to 86 µm, while maintaining the angular resolution, achieved a subgraph similarity of 96% relative to the reference. Using 60 directions with 86-or 172-µm voxels resulted in 94% similarity. Node similarity metrics indicated that major white matter tracts were more robust to downsampling relative to cortical regions. Our study provides guidelines for new protocols in mouse models of neurological conditions, so as to achieve similar connectomes, while increasing efficiency.

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The fornix provides multiple biomarkers to characterize circuit disruption in a mouse model of Alzheimer's disease

Cited by 32 publications

References 104 publications

Identifying Vulnerable Brain Networks in Mouse Models of Genetic Risk Factors for Late Onset Alzheimer’s Disease

Identifying Vulnerable Brain Networks in Mouse Models of Genetic Risk Factors for Late Onset Alzheimer’s Disease

Synaptic Pruning in Alzheimer’s Disease: Role of the Complement System

Optimizing Diffusion Imaging Protocols for Structural Connectomics in Mouse Models of Neurological Conditions

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