Pattern of brain destruction in Parkinson's and Alzheimer's diseases

Braak, Heiko; Braak, Eva; Yilmazer, D.; Vos, Rob A. I. de; Jansen, E. N. H.; Böhl, Jürgen

doi:10.1007/bf01276421

Cited by 306 publications

(184 citation statements)

References 108 publications

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“…The Hip region has been shown to have elevated iron levels in AD (Deibel et al, 1996;Good et al, 1992;Smith et al, 1997;Thompson et al, 1988) (Bartzokis et al, unpublished data), and is affected early and severely in age-related proteinopathies such as AD and DLB (Braak et al, 1996;Kotzbauer et al, 2001) that cause the vast majority (over 70%) of dementia (Barker et al, 2002;Fratiglioni et al, 2000;Lobo et al, 2000). The observation that increased hippocampal iron is associated with poorer memory function even in healthy older individuals supports the suggestion that the 'normal' trajectory of age-related increases in brain ferritin iron may represent an underlying risk factor for age-related degenerative brain diseases ) (reviewed in Bartzokis, 2009).…”

Section: Discussionmentioning

confidence: 99%

“…We hypothesized that even in healthy individuals, agerelated increases in ferritin iron levels in the Hip, which is damaged early and severely in dementia-causing diseases such as AD and DLB (Braak et al, 1996;Kotzbauer et al, 2001), will negatively impact memory function (Bartzokis et al, 2007a;Bartzokis et al, 2007c;Bartzokis et al, 2004). Based on data that men may develop neurodegenerative diseases at younger ages (Barker et al, 2002;Friedman, 1994;Miech et al, 2002;Pantelatos and Fornadi, 1993;Raber et al, 2004) (reviewed in Bartzokis et al, 2004), we also hypothesized that healthy older men may be at increased risk for such iron-associated declines in memory function compared to women (Bartzokis et al, 2007c;Bartzokis et al, 2004).…”

Section: Introductionmentioning

confidence: 99%

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Gender and Iron Genes May Modify Associations Between Brain Iron and Memory in Healthy Aging

Bartzokis

Tingus

et al. 2011

Neuropsychopharmacol

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Brain iron increases with age and is abnormally elevated early in the disease process in several neurodegenerative disorders that impact memory including Alzheimer's disease (AD). Higher brain iron levels are associated with male gender and presence of highly prevalent allelic variants in genes encoding for iron metabolism proteins (hemochromatosis H63D (HFE H63D) and transferrin C2 (TfC2)). In this study, we examined whether in healthy older individuals memory performance is associated with increased brain iron, and whether gender and gene variant carrier (IRON + ) vs noncarrier (IRONÀ) status (for HFE H63D/TfC2) modify the associations. Tissue iron deposited in ferritin molecules can be measured in vivo with magnetic resonance imaging utilizing the field-dependent relaxation rate increase (FDRI) method. FDRI was assessed in hippocampus, basal ganglia, and white matter, and IRON + vs IRONÀ status was determined in a cohort of 63 healthy older individuals. Three cognitive domains were assessed: verbal memory (delayed recall), working memory/attention, and processing speed. Independent of gene status, worse verbal-memory performance was associated with higher hippocampal iron in men (r ¼ À0.50, p ¼ 0.003) but not in women. Independent of gender, worse verbal working memory performance was associated with higher basal ganglia iron in IRONÀ group (r ¼ À0.49, p ¼ 0.005) but not in the IRON + group. Between-group interactions (p ¼ 0.006) were noted for both of these associations. No significant associations with white matter or processing speed were observed. The results suggest that in specific subgroups of healthy older individuals, higher accumulations of iron in vulnerable gray matter regions may adversely impact memory functions and could represent a risk factor for accelerated cognitive decline. Combining genetic and MRI biomarkers may provide opportunities to design primary prevention clinical trials that target high-risk groups.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Gender and Iron Genes May Modify Associations Between Brain Iron and Memory in Healthy Aging

Bartzokis

Tingus

et al. 2011

Neuropsychopharmacol

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“…29 Very few studies have investigated the potential effects of the APOE genotype on white matter (WM) structure. This is surprising considering that the major role of apoE in the brain is the transport of lipid components which contribute to building up the myelin sheath.…”

Section: Introductionmentioning

confidence: 99%

The APOE ɛ4 allele modulates brain white matter integrity in healthy adults

et al. 2010

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The Apolipoprotein E (APOE) ε4 allele is the best-established genetic risk factor for sporadic Alzheimer's disease (AD) and is also associated with structural gray matter (GM) and functional brain changes in healthy young, middle-aged and elderly subjects. Because APOE is implicated in brain mechanisms associated with white matter (WM) development and repair, we investigated the potential role played by the APOE polymorphism on WM structure in healthy younger (age range: 20-35 years) and older (aged 50-78 years) adults using diffusion tensor imaging (DTI). General reduction of fractional anisotropy (FA) and increase in mean diffusivity (MD) values was found in carriers of the APOE ε4 allele relative to non-carriers. No significant interactions between genotype and age were observed, suggesting that differences in WM structure between APOE ε4-carriers and non-carriers do not undergo significant differential changes with age. This result was not explained by differences in brain morphology or cognitive measures. The APOE ε4 allele modulates brain WM structure before any clinical or neurophysiological expression of impending disease.

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“…Neuropathologically, AD is characterized by the presence of amyloid plaques, neurofibrillary tangles and cell atrophy in susceptible brain regions. These cytoskeletal abnormalities develop initially in brain regions of the medial temporal lobe that are involved in processing olfactory information such as the entorhinal and transentorhinal cortex (Braak et al, 1996). The brain degeneration proceeds from these initial areas to other temporal lobe structures and eventually reaches association areas (Braak et al, 1996).…”

Section: Introductionmentioning

confidence: 99%

“…These cytoskeletal abnormalities develop initially in brain regions of the medial temporal lobe that are involved in processing olfactory information such as the entorhinal and transentorhinal cortex (Braak et al, 1996). The brain degeneration proceeds from these initial areas to other temporal lobe structures and eventually reaches association areas (Braak et al, 1996). This pattern of brain degeneration suggests that AD patients may show impairments in olfactorymediated tasks in the early stages of the disease.…”

Section: Introductionmentioning

confidence: 99%

The effect of hormone therapy on olfactory sensitivity is dependent on apolipoprotein E genotype

Sundermann

Gilbert

Murphy

2008

Hormones and Behavior

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Patients with Alzheimer's disease (AD) show a deficit in olfactory threshold sensitivity. The Apolipoprotein E (ApoE) ε4 allele is associated with increased risk of AD and earlier symptom onset. Hormone therapy (HT) may exert neuroprotective effects on brain areas affected by AD. The current study investigated the effect of HT on performance on an olfactory threshold test in ε4 positive and ε4 negative non-hysterectomized, non-demented, elderly females and AD patients. Among the non-demented participants, ε4 positive females who had received HT performed 1) significantly better than those without HT, and 2) at levels similar to those of ε4 negative females. In contrast, those without HT who were ε4 positive performed significantly worse than those who were ε4 negative. HT had no effect on performance in AD patients regardless of ε4 status. These results suggest that HT may offer protection against loss of olfactory function in ε4 positive individuals in preclinical stages of AD. Future research is warranted in order to investigate further the neuroprotective role of HT on sensory and cognitive functions in non-demented aging individuals.

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Pattern of brain destruction in Parkinson's and Alzheimer's diseases

Cited by 306 publications

References 108 publications

Gender and Iron Genes May Modify Associations Between Brain Iron and Memory in Healthy Aging

Gender and Iron Genes May Modify Associations Between Brain Iron and Memory in Healthy Aging

The APOE ɛ4 allele modulates brain white matter integrity in healthy adults

The effect of hormone therapy on olfactory sensitivity is dependent on apolipoprotein E genotype

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