This title appears in the Scientific Report :
2020
Please use the identifier:
http://dx.doi.org/10.1016/j.nicl.2020.102287 in citations.
Please use the identifier: http://hdl.handle.net/2128/25128 in citations.
Role of the default mode resting-state network for cognitive functioning in malignant glioma patients following multimodal treatment
Role of the default mode resting-state network for cognitive functioning in malignant glioma patients following multimodal treatment
Progressive cognitive decline following multimodal neurooncological treatment is a common observation in patients suffering from malignant glioma. Alterations of the default-mode network (DMN) represent a possible source of impaired neurocognitive functioning and were analyzed in these patients.Eigh...
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Personal Name(s): | Kocher, Martin (Corresponding author) |
---|---|
Jockwitz, Christiane / Caspers, Svenja / Schreiber, Jan / Farrher, Ezequiel / Stoffels, Gabriele / Filss, Christian / Lohmann, Philipp / Tscherpel, Caroline / Ruge, Maximilian I. / Fink, Gereon R. / Shah, Nadim J. / Galldiks, Norbert / Langen, Karl-Josef | |
Contributing Institute: |
Kognitive Neurowissenschaften; INM-3 Strukturelle und funktionelle Organisation des Gehirns; INM-1 Physik der Medizinischen Bildgebung; INM-4 |
Published in: | NeuroImage: Clinical, 27 (2020) S. 102287 - |
Imprint: |
[Amsterdam u.a.]
Elsevier
2020
|
DOI: |
10.1016/j.nicl.2020.102287 |
PubMed ID: |
32540630 |
Document Type: |
Journal Article |
Research Program: |
Connectivity and Activity (Dys-)function and Plasticity |
Link: |
Get full text Get full text OpenAccess OpenAccess |
Publikationsportal JuSER |
Please use the identifier: http://hdl.handle.net/2128/25128 in citations.
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520 | |a Progressive cognitive decline following multimodal neurooncological treatment is a common observation in patients suffering from malignant glioma. Alterations of the default-mode network (DMN) represent a possible source of impaired neurocognitive functioning and were analyzed in these patients.Eighty patients (median age, 51 years) with glioma (WHO grade IV glioblastoma, n=57; WHO grade III anaplastic astrocytoma, n=13; WHO grade III anaplastic oligodendroglioma, n=10) and ECOG performance score 0-1 underwent resting-state functional MRI (rs-fMRI) and neuropsychological testing at a median interval of 13 months (range, 1-114 months) after initiation of therapy. For evaluation of structural and metabolic changes after treatment, anatomical MRI and amino acid PET using O-(2-[18F]fluoroethyl)-L-tyrosine (FET) were simultaneously acquired to rs-fMRI on a hybrid MR/PET scanner. A cohort of 80 healthy subjects matched for gender, age, and educational status served as controls.The connectivity pattern within the DMN (12 nodes) of the glioma patients differed significantly from that of the healthy subjects but did not depend on age, tumor grade, time since treatment initiation, presence of residual/recurrent tumor, number of chemotherapy cycles received, or anticonvulsive medication. Small changes in the connectivity pattern were observed in patients who had more than one series of radiotherapy. In contrast, structural tissue changes located at or near the tumor site (including resection cavities, white matter lesions, edema, and tumor tissue) had a strong negative impact on the functional connectivity of the adjacent DMN nodes, resulting in a marked dependence of the connectivity pattern on tumor location. In the majority of neurocognitive domains, glioma patients performed significantly worse than healthy subjects. Correlation analysis revealed that reduced connectivity in the left temporal and parietal DMN nodes was associated with low performance in language processing and verbal working memory. Furthermore, connectivity of the left parietal DMN node also correlated with processing speed, executive function, and verbal as well as visual working memory. Overall DMN connectivity loss and cognitive decline were less pronounced in patients with higher education.Personalized treatment strategies for malignant glioma patients should consider the left parietal and temporal DMN nodes as vulnerable regions concerning neurocognitive outcome. | ||
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