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Featured researches published by Sj Schreiner.


Scientific Reports | 2016

Colocalization of cerebral iron with amyloid beta in mild cognitive impairment

J.M.G. van Bergen; Xu Li; Jun Hua; Sj Schreiner; Sc Steininger; Frances C. Quevenco; Matthias T. Wyss; Anton Gietl; Valerie Treyer; Sandra E. Leh; F. Buck; Roger M. Nitsch; Klaas P. Pruessmann; P. C. M. van Zijl; Christoph Hock; Paul G. Unschuld

Quantitative Susceptibility Mapping (QSM) MRI at 7 Tesla and 11-Carbon Pittsburgh-Compound-B PET were used for investigating the relationship between brain iron and Amyloid beta (Aβ) plaque-load in a context of increased risk for Alzheimers disease (AD), as reflected by the Apolipoprotein E ε4 (APOE-e4) allele and mild cognitive impairment (MCI) in elderly subjects. Carriers of APOE-e4 with normal cognition had higher cortical Aβ-plaque-load than non-carriers. In MCI an association between APOE-e4 and higher Aβ-plaque-load was observable both for cortical and subcortical brain-regions. APOE-e4 and MCI was also associated with higher cortical iron. Moreover, cerebral iron significantly affected functional coupling, and was furthermore associated with increased Aβ-plaque-load (R2-adjusted = 0.80, p < 0.001) and APOE-e4 carrier status (p < 0.001) in MCI. This study confirms earlier reports on an association between increased brain iron-burden and risk for neurocognitive dysfunction due to AD, and indicates that disease-progression is conferred by spatial colocalization of brain iron deposits with Aβ-plaques.


Frontiers in Aging Neuroscience | 2014

Cortical Amyloid Beta in Cognitively Normal Elderly Adults is Associated with Decreased Network Efficiency within the Cerebro-Cerebellar System

Sc Steininger; Xinyang Liu; Anton Gietl; Michael Wyss; Sj Schreiner; Esmeralda Gruber; Valerie Treyer; Andrea M. Kälin; Sandra E. Leh; Alfred Buck; Roger M. Nitsch; Kp Prüssmann; Christoph Hock; Paul G. Unschuld

Background: Deposition of cortical amyloid beta (Aβ) is a correlate of aging and a risk factor for Alzheimer disease (AD). While several higher order cognitive processes involve functional interactions between cortex and cerebellum, this study aims to investigate effects of cortical Aβ deposition on coupling within the cerebro-cerebellar system. Methods: We included 15 healthy elderly subjects with normal cognitive performance as assessed by neuropsychological testing. Cortical Aβ was quantified using (11)carbon-labeled Pittsburgh compound B positron-emission-tomography late frame signals. Volumes of brain structures were assessed by applying an automated parcelation algorithm to three dimensional magnetization-prepared rapid gradient-echo T1-weighted images. Basal functional network activity within the cerebro-cerebellar system was assessed using blood-oxygen-level dependent resting state functional magnetic resonance imaging at the high field strength of 7 T for measuring coupling between cerebellar seeds and cerebral gray matter. A bivariate regression approach was applied for identification of brain regions with significant effects of individual cortical Aβ load on coupling. Results: Consistent with earlier reports, a significant degree of positive and negative coupling could be observed between cerebellar seeds and cerebral voxels. Significant positive effects of cortical Aβ load on cerebro-cerebellar coupling resulted for cerebral brain regions located in inferior temporal lobe, prefrontal cortex, hippocampus, parahippocampal gyrus, and thalamus. Conclusion: Our findings indicate that brain amyloidosis in cognitively normal elderly subjects is associated with decreased network efficiency within the cerebro-cerebellar system. While the identified cerebral regions are consistent with established patterns of increased sensitivity for Aβ-associated neurodegeneration, additional studies are needed to elucidate the relationship between dysfunction of the cerebro-cerebellar system and risk for AD.


Frontiers in Aging Neuroscience | 2014

Regional Fluid-Attenuated Inversion Recovery (FLAIR) at 7 Tesla correlates with amyloid beta in hippocampus and brainstem of cognitively normal elderly subjects

Sj Schreiner; Xinyang Liu; Anton Gietl; Michael Wyss; Sc Steininger; Esmeralda Gruber; Valerie Treyer; Irene B. Meier; Andrea M. Kälin; Sandra E. Leh; Alfred Buck; Roger M. Nitsch; Klaas P. Pruessmann; Christoph Hock; Paul G. Unschuld

Background: Accumulation of amyloid beta (Aβ) may occur during healthy aging and is a risk factor for Alzheimer Disease (AD). While individual Aβ-accumulation can be measured non-invasively using Pittsburgh Compund-B positron emission tomography (PiB-PET), Fluid-attenuated inversion recovery (FLAIR) is a Magnetic Resonance Imaging (MRI) sequence, capable of indicating heterogeneous age-related brain pathologies associated with tissue-edema. In the current study cognitively normal elderly subjects were investigated for regional correlation of PiB- and FLAIR intensity. Methods: Fourteen healthy elderly subjects without known history of cognitive impairment received 11C-PiB-PET for estimation of regional Aβ-load. In addition, whole brain T1-MPRAGE and FLAIR-MRI sequences were acquired at high field strength of 7 Tesla (7T). Volume-normalized intensities of brain regions were assessed by applying an automated subcortical segmentation algorithm for spatial definition of brain structures. Statistical dependence between FLAIR- and PiB-PET intensities was tested using Spearmans rank correlation coefficient (rho), followed by Holm–Bonferroni correction for multiple testing. Results: Neuropsychological testing revealed normal cognitive performance levels in all participants. Mean regional PiB-PET and FLAIR intensities were normally distributed and independent. Significant correlation between volume-normalized PiB-PET signals and FLAIR intensities resulted for Hippocampus (right: rho = 0.86; left: rho = 0.84), Brainstem (rho = 0.85) and left Basal Ganglia vessel region (rho = 0.82). Conclusions: Our finding of a significant relationship between PiB- and FLAIR intensity mainly observable in the Hippocampus and Brainstem, indicates regional Aβ associated tissue-edema in cognitively normal elderly subjects. Further studies including clinical populations are necessary to clarify the relevance of our findings for estimating individual risk for age-related neurodegenerative processes such as AD.


Alzheimer's Research & Therapy | 2017

Memory performance-related dynamic brain connectivity indicates pathological burden and genetic risk for Alzheimer’s disease

Frances C. Quevenco; Maria Giulia Preti; Jiri M.G. Van Bergen; Jun Hua; Michael Wyss; Xu Li; Sj Schreiner; Sc Steininger; Rafael Meyer; Irene Meier; Adam M. Brickman; Sandra E. Leh; Anton Gietl; Alfred Buck; Roger M. Nitsch; Klaas P. Pruessmann; Peter C. M. van Zijl; Christoph Hock; Dimitri Van De Ville; Paul G. Unschuld


Neurobiology of Aging | 2016

Low episodic memory performance in cognitively normal elderly subjects is associated with increased posterior cingulate gray matter N-acetylaspartate: a (1)H MRSI study at 7 Tesla.

Sj Schreiner; T Kirchner; Michael Wyss; Jiri M.G. Van Bergen; Frances C. Quevenco; Sc Steininger; Erica Y. Griffith; Irene B. Meier; Lars Michels; Anton Gietl; Sandra E. Leh; Adam M. Brickman; Christoph Hock; Roger M. Nitsch; Klaas P. Pruessmann; A Henning; Paul G. Unschuld


Neurobiology of Aging | 2017

Brain amyloid burden and cerebrovascular disease are synergistically associated with neurometabolism in cognitively unimpaired older adults

Sj Schreiner; T Kirchner; Atul Narkhede; Michael Wyss; Jiri M.G. Van Bergen; Stephanie C. Steininger; Anton Gietl; Sandra E. Leh; Valerie Treyer; Alfred Buck; Klaas P. Pruessmann; Roger M. Nitsch; Christoph Hock; A Henning; Adam M. Brickman; Paul G. Unschuld


International Geneva Springfield Symposium on Advances in Alzheimer Therapy (ALZHEIMER 2014) | 2014

Investigating the metabolic signature of aging-related brain amyloidosis using 7 Tesla Magnetic resonance spectroscopic imaging

Sj Schreiner; T Kirchner; Anton Gietl; Sc Steininger; Matthias T. Wyss; F Buck; Sandra E. Leh; Roger Nitsch; Klaas P. Pruessmann; Christoph Hock; A Henning; Paul G. Unschuld


Clinical Nuclear Medicine | 2018

Value of 18F-FET PET in Patients With Suspected Tumefactive Demyelinating Disease—Preliminary Experience From a Retrospective Analysis

Massimo Barbagallo; Abdulrahman A. Albatly; Sj Schreiner; Helen K. Hayward-Könnecke; Alfred Buck; Spyros Kollias; Martin W. Huellner


Archive | 2017

GABA promotes beta-Amyloid related changes in dynamic network expression of elderly subjects at risk for Alzheimer's disease

F-C Quevenco; Sj Schreiner; Maria Giulia Preti; J van Bergen; T Kirchner; Matthias T. Wyss; Sc Steininger; Anton Gietl; Sandra E. Leh; Alfred Buck; K Pruessman; Christoph Hock; Roger Nitsch; A Henning; D Van de Ville; Paul G. Unschuld


DGPPN Kongress 2013: Kongress der Deutschen Gesellschaft für Psychiatrie und Psychotherapie, Psychosomatik und Nervenheilkunde | 2017

7 Tesla magnetic resonance imaging (MRSI) of Aβ related brain metabolism in cognitively normal elderly adults

Sj Schreiner; T Kirchner; Anton Gietl; Sc Steininger; Michael Wyss; Esmeralda Gruber; Alfred Buck; Sandra Leh-Seal; Roger Nitsch; Kp Prüssmann; Christoph Hock; A Henning; Paul G. Unschuld

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