Advancing functional dysconnectivity and atrophy in progressive supranuclear palsy

Allbwn ymchwil: Cyfraniad at gyfnodolynErthygladolygiad gan gymheiriaid

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Advancing functional dysconnectivity and atrophy in progressive supranuclear palsy. / Brown, Jesse A.; Hua, Alice Y.; Trujillo, Andrew et al.
Yn: NeuroImage: Clinical, Cyfrol 16, 2017, t. 564-574.

Allbwn ymchwil: Cyfraniad at gyfnodolynErthygladolygiad gan gymheiriaid

HarvardHarvard

Brown, JA, Hua, AY, Trujillo, A, Attygalle, S, Binney, RJ, Spina, S, Lee, SE, Kramer, JH, Miller, BL, Rosen, HJ, Boxer, AL & Seeley, WW 2017, 'Advancing functional dysconnectivity and atrophy in progressive supranuclear palsy', NeuroImage: Clinical, cyfrol. 16, tt. 564-574. https://doi.org/10.1016/j.nicl.2017.09.008

APA

Brown, J. A., Hua, A. Y., Trujillo, A., Attygalle, S., Binney, R. J., Spina, S., Lee, S. E., Kramer, J. H., Miller, B. L., Rosen, H. J., Boxer, A. L., & Seeley, W. W. (2017). Advancing functional dysconnectivity and atrophy in progressive supranuclear palsy. NeuroImage: Clinical, 16, 564-574. https://doi.org/10.1016/j.nicl.2017.09.008

CBE

Brown JA, Hua AY, Trujillo A, Attygalle S, Binney RJ, Spina S, Lee SE, Kramer JH, Miller BL, Rosen HJ, et al. 2017. Advancing functional dysconnectivity and atrophy in progressive supranuclear palsy. NeuroImage: Clinical. 16:564-574. https://doi.org/10.1016/j.nicl.2017.09.008

MLA

VancouverVancouver

Brown JA, Hua AY, Trujillo A, Attygalle S, Binney RJ, Spina S et al. Advancing functional dysconnectivity and atrophy in progressive supranuclear palsy. NeuroImage: Clinical. 2017;16:564-574. Epub 2017 Medi 12. doi: 10.1016/j.nicl.2017.09.008

Author

Brown, Jesse A. ; Hua, Alice Y. ; Trujillo, Andrew et al. / Advancing functional dysconnectivity and atrophy in progressive supranuclear palsy. Yn: NeuroImage: Clinical. 2017 ; Cyfrol 16. tt. 564-574.

RIS

TY - JOUR

T1 - Advancing functional dysconnectivity and atrophy in progressive supranuclear palsy

AU - Brown, Jesse A.

AU - Hua, Alice Y.

AU - Trujillo, Andrew

AU - Attygalle, Suneth

AU - Binney, Richard J.

AU - Spina, Salvatore

AU - Lee, Suzee E.

AU - Kramer, Joel H

AU - Miller, Bruce L.

AU - Rosen, Howard J

AU - Boxer, Adam L

AU - Seeley, William W

PY - 2017

Y1 - 2017

N2 - Progressive supranuclear palsy syndrome (PSP-S) results from neurodegeneration within a network of brainstem, subcortical, frontal and parietal cortical brain regions. It is unclear how network dysfunction progresses and relates to longitudinal atrophy and clinical decline. In this study, we evaluated patients with PSP-S (n=12) and healthy control subjects (n=20) at baseline and 6 months later. Subjects underwent structural MRI and task-free functional MRI (tf-fMRI) scans and clinical evaluations at both time points. At baseline, voxel based morphometry (VBM) revealed that patients with mild-to-moderate clinical symptoms showed structural atrophy in subcortex and brainstem, prefrontal cortex (PFC; supplementary motor area, paracingulate, dorsal and ventral medial PFC), and parietal cortex (precuneus). Tf-fMRI functional connectivity (FC) was examined in a rostral midbrain tegmentum (rMT)-anchored intrinsic connectivity network that is compromised in PSP-S. In healthy controls, this network contained a medial parietal module, a prefrontal-paralimbic module, and a subcortical-brainstem module. Baseline FC deficits in PSP-S were most severe in rMT network integrative hubs in the prefrontal-paralimbic and subcortical-brainstem modules. Longitudinally, patients with PSP-S had declining intermodular FC between the subcortical-brainstem and parietal modules, while progressive atrophy was observed in subcortical-brainstem regions (midbrain, pallidum) and posterior frontal (perirolandic) cortex. This suggested that later-stage subcortical-posterior cortical change may follow an earlier-stage subcortical-anterior cortical disease process. Clinically, patients with more severe baseline impairment showed greater subsequent prefrontal-parietal cortical FC declines and posterior frontal atrophy rates, while patients with more rapid longitudinal clinical decline showed coupled prefrontal-paralimbic FC decline. VBM and FC can augment disease monitoring in PSP-S by tracking the disease through stages while detecting changes that accompany heterogeneous clinical progression.

AB - Progressive supranuclear palsy syndrome (PSP-S) results from neurodegeneration within a network of brainstem, subcortical, frontal and parietal cortical brain regions. It is unclear how network dysfunction progresses and relates to longitudinal atrophy and clinical decline. In this study, we evaluated patients with PSP-S (n=12) and healthy control subjects (n=20) at baseline and 6 months later. Subjects underwent structural MRI and task-free functional MRI (tf-fMRI) scans and clinical evaluations at both time points. At baseline, voxel based morphometry (VBM) revealed that patients with mild-to-moderate clinical symptoms showed structural atrophy in subcortex and brainstem, prefrontal cortex (PFC; supplementary motor area, paracingulate, dorsal and ventral medial PFC), and parietal cortex (precuneus). Tf-fMRI functional connectivity (FC) was examined in a rostral midbrain tegmentum (rMT)-anchored intrinsic connectivity network that is compromised in PSP-S. In healthy controls, this network contained a medial parietal module, a prefrontal-paralimbic module, and a subcortical-brainstem module. Baseline FC deficits in PSP-S were most severe in rMT network integrative hubs in the prefrontal-paralimbic and subcortical-brainstem modules. Longitudinally, patients with PSP-S had declining intermodular FC between the subcortical-brainstem and parietal modules, while progressive atrophy was observed in subcortical-brainstem regions (midbrain, pallidum) and posterior frontal (perirolandic) cortex. This suggested that later-stage subcortical-posterior cortical change may follow an earlier-stage subcortical-anterior cortical disease process. Clinically, patients with more severe baseline impairment showed greater subsequent prefrontal-parietal cortical FC declines and posterior frontal atrophy rates, while patients with more rapid longitudinal clinical decline showed coupled prefrontal-paralimbic FC decline. VBM and FC can augment disease monitoring in PSP-S by tracking the disease through stages while detecting changes that accompany heterogeneous clinical progression.

KW - progressive supranuclear palsy

KW - Longitudinal

KW - Intrinsic connectivity network

KW - Modularity

U2 - 10.1016/j.nicl.2017.09.008

DO - 10.1016/j.nicl.2017.09.008

M3 - Article

VL - 16

SP - 564

EP - 574

JO - NeuroImage: Clinical

JF - NeuroImage: Clinical

SN - 2213-1582

ER -