| Literature DB >> 25385447 |
Johannes Attems1, Kurt A Jellinger.
Abstract
Recent epidemiological and clinico-pathological data indicate considerable overlap between cerebrovascular disease (CVD) and Alzheimer's disease (AD) and suggest additive or synergistic effects of both pathologies on cognitive decline. The most frequent vascular pathologies in the aging brain and in AD are cerebral amyloid angiopathy and small vessel disease. Up to 84% of aged subjects show morphological substrates of CVD in addition to AD pathology. AD brains with minor CVD, similar to pure vascular dementia, show subcortical vascular lesions in about two-thirds, while in mixed type dementia (AD plus vascular dementia), multiple larger infarcts are more frequent. Small infarcts in patients with full-blown AD have no impact on cognitive decline but are overwhelmed by the severity of Alzheimer pathology, while in early stages of AD, cerebrovascular lesions may influence and promote cognitive impairment, lowering the threshold for clinically overt dementia. Further studies are warranted to elucidate the many hitherto unanswered questions regarding the overlap between CVD and AD as well as the impact of both CVD and AD pathologies on the development and progression of dementia.Entities:
Mesh:
Year: 2014 PMID: 25385447 PMCID: PMC4226890 DOI: 10.1186/s12916-014-0206-2
Source DB: PubMed Journal: BMC Med ISSN: 1741-7015 Impact factor: 8.775
Types and location of cerebrovascular lesions in vascular dementia (total 188)
|
| |
| MCA bilateral | 4 |
| MCA left/right | 9 |
| MCA bilat. + PCAS/PCAD | 2/1 |
| MCA bilat. + PCA bilat. | 2 |
| MCAS + PCAS | 4 |
| MCAD + PCAD | 4 |
| PCA bilateral | 3 |
| PCA left/right | 5/7 |
| ACAS + MCAS | 2 |
| ACAD | 1 |
| Multiple cortico-subcortico bilateral | 12 |
| Multiple cortico-subcortico left hem. | 2 |
|
| |
| Basal ganglia | 21 |
| Basal ganglia + white matter | 31 |
| Basal ganglia + thalamus (+white matter) | 33 |
| Basal ganglia brainstem (+thalamus) | 23 |
|
| |
| Thalamus bilateral | 9 |
| Thalamus left | 2 |
| Thalamus + hippocampus | 8 |
Types and location of cerebrovascular lesions in mixed dementia (n = 83)
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| |
| MCA bilateral | 7 |
| MCA left | 6 |
| MCA right (+ lacunes basal ganglia) | 3/1 |
| MCA + ACA bilat. | 1 |
| MCA + PCA left | 2 |
| MCA + PCA right | 1 |
| MCA + PCA left/right | 3/3 |
| MCA bilat. +PCAD | 1 |
| PCA bilateral | 2 |
| Multiple cort. and subcort. bilateral | 13 |
| Multiple left hemisphere | 4 |
|
| |
| Lacunes basal ganglia | 15 |
| Lacunes basal ganglia + white matter | 8 |
| Lacunes basal ganglia + thalamus | 10 |
|
| |
| Thalamus bilateral | 2 |
| Thalamus + hippocampus | 1 |
Common lesions in AD, VaD, MIX, and aged controls (from[130])
| Pathological feature | AD [%] | VaD [%] | MIX [%] | Aged controls [%] |
|---|---|---|---|---|
| Cerebral amyloid angiopathy | 98 | 30 | ~90 | 23-45 |
| Small vessel disease/MVD | ~50 | >50 | >50 | ~20 |
| Total infarctions | 10-20 | 100 | 30-40 | >10 |
| Microinfarcts/lacunes | 30-46 | 70 | 60-70 | 17-21 |
| Intracerebral hemorrhage | 10-15 | 15 | 10 | 1-2 |
| White matter pathology | 40 | 80 | 70-80 | <20 |
| Loss of cholinergic markers | 75 | 40 | ~70 | |
| CVD/atherosclerosis | 45-60 | 60 | ~60 | 30-53 |
Abbreviations: AD, Alzheimer’s disease; CVD, Cerebrovascular disease; MIX, mixed type dementia (AD plus vascular dementia); MVD, Microvascular disease; VaD, Vascular dementia.
Figure 1Pathogenic factors for the development of mixed dementia. Modified from [147].