Literature DB >> 17347250

Rates of cerebral atrophy differ in different degenerative pathologies.

Jennifer L Whitwell1, Clifford R Jack, Joseph E Parisi, David S Knopman, Bradley F Boeve, Ronald C Petersen, Tanis J Ferman, Dennis W Dickson, Keith A Josephs.   

Abstract

Neurodegenerative disorders are pathologically characterized by the deposition of abnormal proteins in the brain. It is likely that future treatment trials will target the underlying protein biochemistry and it is therefore increasingly important to be able to distinguish between different pathologies during life. The aim of this study was to determine whether rates of brain atrophy differ in neurodegenerative dementias that vary by pathological diagnoses and characteristic protein biochemistry. Fifty-six autopsied subjects were identified with a clinical diagnosis of dementia and two serial head MRI. Subjects were subdivided based on pathological diagnoses into Alzheimer's disease, dementia with Lewy bodies (DLB), mixed Alzheimer's disease/DLB, frontotemporal lobar degeneration with ubiquitin-only-immunoreactive changes (FTLD-U), corticobasal degeneration (CBD) and progressive supranuclear palsy (PSP). Twenty-five controls were matched by age, gender and scan interval, to the study cohort. The boundary-shift integral was used to calculate change over time in whole brain (BBSI) and ventricular volume (VBSI). All BSI results were annualized by adjusting for scan interval. The rates of whole brain atrophy and ventricular expansion were significantly increased compared to controls in the Alzheimer's disease, mixed Alzheimer's disease/DLB, FTLD-U, CBD and PSP groups. However, atrophy rates in the DLB group were not significantly different from control rates of atrophy. The largest rates of atrophy were observed in the CBD group which had a BBSI of 2.3% and VBSI of 16.2%. The CBD group had significantly greater rates of BBSI and VBSI than the DLB, mixed Alzheimer's disease/DLB, Alzheimer's disease and PSP groups, with a similar trend observed when compared to the FTLD-U group. The FTLD-U group showed the next largest rates with a BBSI of 1.7% and VBSI of 9.6% which were both significantly greater than the DLB group. There was no significant difference in the rates of atrophy between the Alzheimer's disease, mixed Alzheimer's disease/DLB and PSP groups, which all showed similar rates of atrophy; BBSI of 1.1, 1.3 and 1.0% and VBSI of 8.3, 7.2 and 10.9%, respectively. Rates of atrophy therefore differ according to the pathological diagnoses and underlying protein biochemistry. While rates are unlikely to be useful in differentiating Alzheimer's disease from cases with mixed Alzheimer's disease/DLB pathology, they demonstrate important pathophysiological differences between DLB and those with mixed Alzheimer's disease/DLB and Alzheimer's disease pathology, and between those with CBD and PSP pathology.

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Year:  2007        PMID: 17347250      PMCID: PMC2752409          DOI: 10.1093/brain/awm021

Source DB:  PubMed          Journal:  Brain        ISSN: 0006-8950            Impact factor:   13.501


  83 in total

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Journal:  Neuroradiology       Date:  1996-05       Impact factor: 2.804

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  70 in total

1.  Rates of brain atrophy and clinical decline over 6 and 12-month intervals in PSP: determining sample size for treatment trials.

Authors:  Jennifer L Whitwell; Jia Xu; Jay N Mandrekar; Jeffrey L Gunter; Clifford R Jack; Keith A Josephs
Journal:  Parkinsonism Relat Disord       Date:  2011-11-13       Impact factor: 4.891

2.  Some is not enough: quantifier comprehension in corticobasal syndrome and behavioral variant frontotemporal dementia.

Authors:  Brianna Morgan; Rachel G Gross; Robin Clark; Michael Dreyfuss; Ashley Boller; Emily Camp; Tsao-Wei Liang; Brian Avants; Corey T McMillan; Murray Grossman
Journal:  Neuropsychologia       Date:  2011-09-12       Impact factor: 3.139

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Journal:  Anesthesiology       Date:  2012-03       Impact factor: 7.892

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Authors:  E Gordon; J D Rohrer; L G Kim; R Omar; M N Rossor; N C Fox; J D Warren
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5.  Sparse unbiased analysis of anatomical variance in longitudinal imaging.

Authors:  Brian Avants; Philip A Cook; Corey McMillan; Murray Grossman; Nicholas J Tustison; Yuanjie Zheng; James C Gee
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Authors:  Florence F Roussotte; Boris A Gutman; Derrek P Hibar; Sarah K Madsen; Katherine L Narr; Paul M Thompson
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Authors:  Brian B Avants; David J Libon; Katya Rascovsky; Ashley Boller; Corey T McMillan; Lauren Massimo; H Branch Coslett; Anjan Chatterjee; Rachel G Gross; Murray Grossman
Journal:  Neuroimage       Date:  2013-10-02       Impact factor: 6.556

8.  Rates of brain atrophy over time in autopsy-proven frontotemporal dementia and Alzheimer disease.

Authors:  Jennifer L Whitwell; Clifford R Jack; V Shane Pankratz; Joseph E Parisi; David S Knopman; Bradley F Boeve; Ronald C Petersen; Dennis W Dickson; Keith A Josephs
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