Anhörigas upplevelser av att vårda en familjemedlem som insjuknat i demens : en analys av självbiografier

Bengtsson, Margareta, Gosende, Martina

January 2008

När en familjemedlem drabbas av demens förändras hela livssituationen för den anhörige. För att sjuksköterskan ska kunna stödja de anhöriga krävs det kunskap och ökad förståelse om de anhörigas vårdarroll i hemmet. Syftet med studien var att beskriva anhörigas upplevelser av att vårda en familjemedlem i hemmet som insjuknat i demens. Sex självbiografier analyserades för att ta del av anhörigas egna upplevelser av att vårda en demenssjuk familjemedlem. Till grund för analys av data låg Burnards (1991) innehållsanalys och Graneheims & Lundmans (2004) kvalitativa innehållsanalys. Resultatet utgörs av tre huvudkategorier och 10 kategorier. Huvudkategorierna var: Lidande, desperation och isolering. Det mest utmärkande hos anhörigvårdarna är den känslomässiga upplevelsen som beskrivs som mer betungande än vad det fysiska vårdandet gör. Det som även kännetecknar anhörigas upplevelser är att de blir mer och mer isolerade allt eftersom sjukdomen fortskrider. / Being the relative of a person with dementia is a life changing experience. The relatives often find themselves in a complex situation, which requires that the nurse, can identify needs among the relatives. It‘s also important that the nurse has a broad knowledge about the role of the relative as a caregiver, to be able to give support to them in this situation. The purpose of this study was to describe the relative’s experiences of taking care of a familymember with dementia in the home. Six autobiographies were studied to emerge in the experiences of the family caregivers. Burnards (1991) content analysis and Graneheims & Lundmans (2004) qualitative content analysis was used to analyze the data and the result reveals 3 main categories and 10 categories. The main categories were: Suffering, desperation and isolation. The situation of the caregiving relatives involves experiences of mental distress as well as having to cope with several difficulties. Their new role as a family caregiver is characterized by feelings of isolation which increases as the sickness proceeds.

Dementia

Alzheimer’s

relatives

experience

Demens

Alzheimers

anhöriga

upplevelse

Nursing

Omvårdnad

Alzheimer's Disease Classification using K-OPLS and MRI

Falahati Asrami, Farshad

January 2012

In this thesis, we have used the kernel based orthogonal projection to latent structures (K-OPLS) method to discriminate between Alzheimer's Disease patients (AD) and healthy control subjects (CTL), and to predict conversion from mild cognitive impairment (MCI) to AD. In this regard three cohorts were used to create two different datasets; a small dataset including 63 subjects based on the Alzheimer’s Research Trust (ART) cohort and a large dataset including 1074 subjects combining the AddNeuroMed (ANM) and the Alzheimer’s Disease Neuroimaging Initiative (ADNI) cohorts. In the ART dataset, 34 regional cortical thickness measures and 21 volumetric measures from MRI in addition to 3 metabolite ratios from MRS, altogether 58 variables obtained for 28 AD and 35 CTL subjects. Three different K-OPLS models were created based on MRI and MRS measures and their combination. Combining the MRI and the MRS measures significantly improved the discriminant power resulting in a sensitivity of 96.4% and a specificity of 97.1%. In the combined dataset (ADNI and AddNeuroMed), the Freesurfer pipeline was utilized to extract 34 regional cortical thickness measures and 23 volumetric measures from MRI scans of 295 AD, 335 CTL and 444 MCI subjects. The classification of AD and CTL subjects using the K-OPLS model resulted in a high sensitivity of 85.8% and a specificity of 91.3%. Subsequently, the K-OPLS model was used to prospectively predict conversion from MCI to AD, according to the one year follow up diagnosis. As a result, 78.3% of the MCI converters were classified as AD-like and 57.5% of the MCI non-converters were classified as control-like. Furthermore, an age correction method was proposed to remove the effect of age as a confounding factor. The age correction method successfully removed the age-related changes of the data. Also, the age correction method slightly improved the performance regarding to classification and prediction. This resulted in that 82.1% of the MCI converters were correctly classified. All analyses were performed using 7-fold cross validation. The K-OPLS method shows strong potential for classification of AD and CTL, and for prediction of MCI conversion.

Studies of unspecific interaction between the Aβ antibody 6E10 and blood coagulation protein factor X

Karlsson, Cecilia

January 2012

Alzheimer’s disease is neurodegenerative with amyloid plaque and neurofibrillary tangles as pathological hallmarks. The most abundant component in the amyloid plaque is the amyloid-β (Aβ) peptide, with presence of both isoform Aβ40 and Aβ42. In immunological methods studying the Aβ peptide a specific monoclonal antibody, 6E10, is routinly being used. In this master thesis work unspecific binding of 6E10 antibody to the blood coagulating protein factor X has been investigated. Factor X is a protein in the blood coagulation cascade where it forms protein complex that activates thrombin. Non-hemostatic functions with connections to nerves and Aβ peptide are also known. Studies with Western blot show clear binding of 6E10 to denatured factor X. Interaction studies with ELISA gives uncertain results, where binding is found but no clear binding curve is obtained. Studies with native factor X in real time measurements with SPR gave no binding at all. These results suggest binding to denatured factor X. Immunohistochemistry studies of colocalisation of factor X and Aβ peptide gave clear evidence that factor X and Aβ are found near each other in mouse brain tissue. Factor X is located outside the blood vessels and Aβ is located at the inside.

Alzheimer’s disease

6E10

Aβ

Factor X

SPR

ELISA

Kronisk behandling med allopregnanolon påverkar inte mängden beta-amyloida plack i AβPPSwePSEN1∆E9 AD-möss / Chronic treatment with allopregnanolone does not affect beta-amyloid plaques in AβPPSwePSEN1∆E9 AD-mice

Öystilä Sjödin, Madelen

January 2012

No description available.

Alzheimer’s sjukdom

allopregnanolon

stress

beta-amyloid

plack

GABA-A.

Design and Characterisation of Multifunctional Tools for the Elucidation of the Cu+ Chemistry in Alzheimer`s Disease

Rittmeier, Markus

05 February 2013

No description available.

540

Alzheimer’s Disease

Copper

Chelating

Amyloid plaques

Chemie  (PPN62138352X)

Assessing Olfactory Learning and Memory in the 5XFAD Mouse Model of Alzheimer’s Disease

Roddick, Kyle

24 July 2012

Using an operant-olfactometer, the long term learning and memory, executive function, olfactory sensitivity, and working memory of the 5XFAD mouse model of Alzheimer’s disease was assessed. Six month old male and female 5XFAD and wildtype mice were tested. No deficits were found on an olfactory discrimination task or a reversal learning task. Female and transgenic mice performed better than male and wildtype mice on the higher odour concentrations, but not the lower concentrations, of the sensitivity task, suggesting differences in learning rate or maximum performance on the task, but not olfactory detection. This study demonstrated for the first time that mice are able to learn an olfactory delayed matching to sample task with delays up to 30 seconds long. Female mice showed higher levels of performance on the matching to sample task than male mice, indicative of better working memory.

5XFAD

Alzheimer’s Disease

Learning and Memory

Olfaction

Mice

Working Memory

Cellular level/distribution of γ-secretase subunit nicastrin and its modulator p23 in the brain

Kodam, Anitha

Unknown Date

No description available.

Nicastrin

p23/TMP21

Gamma secretase

Gamma secretase modulator

Alzheimer’s disease

Characterisation of a mouse model of chronic cerebral hypoperfusion and its application to investigating the impact of hypoperfusion on the development of Alzheimer's disease

Coltman, Robin Bruce

January 2012

The integrity of brain white matter is vital for the interneuronal signalling between distinct brain regions required for normal cognitive function. White matter integrity is compromised with ageing and could contribute to age-related cognitive decline. Chronic cerebral hypoperfusion is thought to underlie the development of white matter pathology and cognitive changes, often seen in the elderly. Additionally, the development of regional hypoperfusion and white matter damage are thought to be early events in Alzheimer’s disease (AD) pathogenesis. This thesis set out to test the hypothesis that chronic cerebral hypoperfusion underlies the development of white matter pathology and cognitive decline and also that chronic cerebral hypoperfusion causes the development of Ab pathology in AD. The first aim was to investigate the impact of hypoperfusion on the development of white matter damage and different aspects of cognition in a mouse model of chronic cerebral hypoperfusion. Two studies were undertaken to address this. The first study examined the temporal development of pathology following hypoperfusion induced by bilateral carotid artery stenosis (BCAS) using microcoils Hypoperfusion was induced in wild type (WT) mice and the pathological changes examined at one week, two weeks, one month and two months. Hypoperfused animals developed a diffuse and widespread white matter pathology, present from one week, which occurred predominantly in the myelin component of white matter; this was accompanied by minimal axonal damage. A second study examined the impact of hypoperfusion on different aspects of spatial memory and further investigated pathological changes in the model at one and two months. Behavioural testing revealed a significant impairment in spatial working memory but not episodic memory or spatial reference memory in hypoperfused animals. In the same mice, pathological assessment indicated that there was a significant increase in levels of myelin damage and elevated levels of microglial activation as compared to shams. These results demonstrate that modest reductions in cerebral blood flow are sufficient to cause the development of white matter damage and the development of cognitive deficits. The second aim was to investigate the impact of hypoperfusion on the development of white matter and amyloid pathology in a mouse model (3xTg-AD) of AD. To address this, using 2 different sizes of microcoils (0.18mm and 0.16mm internal diameter) BCAS of varying severities was induced in 3xTg-AD mice and white matter and Ab pathology were assessed at one month. Circle of Willis (CoW) architecture was also compared between WT and 3xTg-AD mice. Overall white matter pathology was not exacerbated in experimental 3xTg-AD mice with BCAS induced by 0.18mm coils. However with a greater level of stenosis (0.16mm coil) ischaemic damage to neuronal perikarya was present in most experimental animals. In addition to ischaemic damage, localised areas of severe white matter pathology were also observed in conjunction with subtle changes to white matter Ab levels. Hypoperfusion did not impact on the development of intraneuronal Ab pathology, other than in the presence of ischaemic damage when levels were reduced. Comparison of CoW architecture between WT and 3xTg-AD mice revealed strain specific differences in the presence and morphology of the posterior communicating artery which may explain the lack of pathology in 3xTg-AD mice as compared to WT following BCAS induced using 0.18mm dia. microcoils. The third aim was to investigate whether white matter protein composition changed with age and also whether ageing conferred increased vulnerability to hypoperfusion. To address this, white matter protein levels were compared between young (3-4 months) and old (12-13 months) 3xTg-AD mice. White matter pathology was compared between sham and hypoperfused animals in the aged cohort. Levels of myelin basic protein and 2', 3'-cyclic nucleotide 3'- phosphodiesterase were found to be significantly increased whilst levels of myelin associated glycoprotein were significantly reduced with ageing. These results suggest that changes in myelin protein composition may contribute to the development of age related white matter pathology. White matter pathology was not exacerbated in aged hypoperfused animals following one month of hypoperfusion as compared to shams. The results presented within the thesis demonstrate that chronic cerebral hypoperfusion precipitates the development of selective white matter damage and impacts on cognition. Also it has been shown that where hypoperfusion is severe enough to cause ischaemic damage to neuronal perikarya and localised areas of severe white matter pathology, alterations in white matter Ab levels can occur. Hypoperfusion does not impact on APP processing or on intraneuronal levels of APP or Ab, other than in the presence of ischaemic damage to neuronal perikarya, when levels are reduced. These findings highlight the importance of early intervention strategies in the treatment of vascular risk factors which can lead to hypoperfusion and the development of white matter damage and a decline in cognitive function in later life. These findings also suggest that repair or prevention of white matter damage may be an appropriate strategy for the attenuation of cognitive decline following onset of hypoperfusion. This thesis also highlights some of the limitations of animal models of human disease.

616.831

A LIFE SPAN APPROACH TO THE RELATIONSHIP BETWEEN CHOLESTEROL, LATE ONSET ALZHEIMER’S DISEASE, AND COGNITIVE FUNCTIONING AMONG OLDER ADULTS

Downer, Brian

01 January 2014

There is evidence that cholesterol presents an important risk factor for Alzheimer’s disease (AD), but the direction of this relationship is modified by age. High cholesterol during midlife and low cholesterol during late life are both associated with an increased risk for AD. This dissertation research engaged a life span approach to study the relationship between cholesterol, AD and cognitive functioning among older adults. The purpose of this research was to determine if trajectories of cholesterol from midlife through late life differ according to AD status and if these trajectories are associated with cognitive functioning during old age. This research employed a secondary analysis of cognitive, phenotypic and genetic data collected from subjects of the Framingham Heart Study (FHS) Original and Offspring Cohorts. Aim One involved creating three summary scores of the FHS neuropsychological battery. ROC analysis was used to determine which score best differentiated between cognitively normal, impaired and dementia subjects. Aim Two used generalized additive mixed models to examine trajectories of total, HDL and total/HDL cholesterol ratio according to AD status in the Original Cohort. Aim Three used mixed-effects models to examine the relationship between subject-specific trajectories of total cholesterol and cognition during old age. Aim One determined that a summary score that provided equal weight to each assessment in the FHS neuropsychological battery best differentiates between subjects classified as cognitively normal, cognitively impaired and dementia. The findings from Aim Two indicated that there are subtle differences in the longitudinal trajectories of total, HDL and total/HDL ratio according to AD status. The findings from Aim Three provide limited evidence for a relationship between subject-specific trajectories of total cholesterol and cognitive functioning later in life. Older adults in the highest quartile for cognitive functioning had lower total cholesterol at approximately 55 years of age, but there were no differences in the mean trajectories of total cholesterol according to cognitive functioning later in life. The findings from this research suggest that older adults with high cognitive functioning have lower total cholesterol during midlife, but life span cholesterol trajectories do not appear to be associated with AD status or cognitive function.

Life span

Cholesterol

Alzheimer’s Disease

Cognition

Older Adults

Epidemiology

Gerontology

Neuroinflammation in Alzheimer's disease : Focus on NF-κB and C/EBP transcription factors

Ramberg, Veronica

January 2011

Alzheimer's disease (AD) is the most common form of dementia among elderly. The disease is characterized by amyloid-β (Aβ) plaques, neurofibrillary tangles, loss of synapses and neurons and chronic neuroinflammation. The significance of neuroinflammatory processes in disease on-set and progression has been debated since activated microglia and reactive astrocytes have been attributed both protective and damaging properties. However, patients systematically treated with anti-inflammatory drugs have been shown to develop AD to a lesser extent than average. This indicates an important role of neuroinflammation in AD. This thesis focuses on two inflammatory related transcription factors, nuclear factor κB (NF-κB) and CCAAT/enhancer binding protein (C/EBP). Both NF-κB and C/EBP are known regulators of many pro-inflammatory genes and may during certain circumstances dimerize with each other. In paper I we use a new strategy to inhibit NF-κB DNA binding activity in primary astro-microglial cell cultures treated with Aβ and IL-1β. By coupling the NF-κB decoy to a transport peptide both concentration and incubation time can be shortened in comparison to previous studies. Moreover, using the same in vitro model in paper II and III, we show members of the C/EBP family to be dysregulated during AD mimicking conditions. Additional focus was directed towards C/EBPδ, which was shown to respond differently to oligomeric and fibrillar forms of Aβ. Results were also confirmed in vivo using an AD mouse model characterized by high levels of fibrillar Aβ deposits. Finally, in order to get further insight in neurodegenerative processes, induced by Aβ or microglial activation, we present in paper IV a new set of anchored sensors for detection of locally activated caspases in neuronal cells. By anchoring the sensors to tau they become less dynamic and caspase activation can be detected early on in the apoptotic process, in a spatio-temporal and reproducible manner.

Alzheimer’s disease

neuroinflammation

NF-κB

C/EBP

apoptosis

caspases

FRET