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Identification of earlier biomarkers for Alzheimer’s disease: a neuroimaging study of individuals with subjective cognitive declineParker, Ashleigh 04 September 2019 (has links)
Background: Given that individuals with subjective cognitive decline (SCD) report a change that is not yet measurable with standard neuropsychological assessment measures, they are thought to be the earliest along the cognitive continuum between healthy aging and Alzheimer’s disease (AD). The current study used a neuroimaging approach to examine differences in brain function and structure between individuals with SCD and healthy controls (HC).
Method: 3T resting state functional MRI and high resolution anatomical images were retrieved from 23 individuals with SCD (mean age = 72.9 years, SD = 5.4, 12 females) and 23 HC (mean age = 74.3 years, SD = 5.0, 12 females) from the screening time point from the AD Neuroimaging Initiative database. All data were processed using the FMRIB Software Library. Seed-based analyses of the default mode network (DMN) were used to compare differences in brain function between SCD and HC groups (Z > 2.3; cluster significance: p < 0.05, corrected). Voxel-based morphometry (VBM) was used to examine differences in grey matter volume between the SCD and HC groups.
Results: The SCD and HC groups were not significantly different in age or education level. Results revealed significantly greater activity in the DMN including the bilateral precuneus cortex, bilateral thalamus, and right hippocampal regions in individuals with SCD relative to controls. Conversely, those with SCD showed decreased activation in the bilateral frontal pole, caudate, angular gyrus, lingual gyrus, right superior frontal gyrus, right occipital pole, right superior temporal gyrus, left superior temporal gyrus in the posterior division, left precuneus cortex, left precentral gyrus, left occipital fusiform gyrus, left temporal pole, and left cerebellum compared to HC. Finally, VBM results did not show significant differences in grey matter volume between the groups.
Conclusion: Findings revealed changes in brain function but not structure between individuals with SCD and HC. Overall, this study represents a crucial step in characterizing individuals with SCD, a group recognized to be at increased risk for AD. It is imperative to identify biomarkers prior to significant decline on clinical assessment, so that disease-delaying interventions may be delivered at the earliest possible time point. / Graduate / 2020-08-15
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Understanding subjective measures of olfaction and cognition : A study on the occurrence of subjective olfactory and/or cognitive decline and their effect on future behavioral performanceAejmelaeus-Lindström, Andrea January 2022 (has links)
Dementia is a growing burden for society, and it is of interest to discover it at an early stage. Both subjective cognitive decline (SCD) and subjective olfactory decline (SOD) has been associated with future cognitive decline and dementia. However, subjective measures have often been criticized and are still not fully understood. I aimed to examinate the frequency of SCD and SOD and whether they are likely to measure different things and what their longitudinal effects are. The baseline sample (N=784, 35-90 years, 51% female) were split into reported SCD, SOD, combined subjective olfactory and cognitive decline, and controls. Between-subjects and within-subjects statistical tests were conducted on a subset of participants (N=307, 45 to 90 years, 52% female) comparing SCD and SOD and their olfactory ability, cognitive performance, and demographics. In the baseline sample, a total of 21.1% reported a SOD whereas only 9.9% reported a SCD, only 2.7% reported both. SOD individuals had an emerged olfactory decline at follow up, their olfactory performance was associated with performance in several cognitive tests, this was not the case for the SCD individuals. The SOD and the SCD groups differ from each other, and they appear to be rather independent from each other. They might be complementary in understanding the aging brain.
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Kognition im Alter: Zusammenhänge von Parametern des peripheren Lipidstoffwechsels mit dem Hippocampus anhand multimodaler 7 Tesla MagnetresonanztomografieSchurig, Jana 15 January 2024 (has links)
In der vorliegenden Arbeit wurden Zusammenhänge zwischen Parametern des peripheren Cholesterolstoffwechsels mit Makrostruktur und Mikrostruktur des Hippocampus anhand multimodaler 7 Tesla Magnetresonanztomografie bei älteren, kognitiv gesunden Menschen untersucht. Dabei wurden Unterschiede zwischen den biologischen Geschlechtern der Teilnehmenden sowie Unterschiede zwischen Teilnehmenden mit und ohne subjektive kognitive Beeinträchtigungen betrachtet. Als zentrales Ergebnis zeigte sich ein Zusammenhang zwischen hohen HDL-Werten und niedrigem Hippocampusvolumen bei Frauen.:Inhaltsverzeichnis II
Abkürzungsverzeichnis V
Abbildungsverzeichnis VII
Tabellenverzeichnis IX
1 Einführung 1
1.1 Hintergrund 1
1.2 Demenzielle Erkrankungen 2
1.3 Subjective Cognitive Decline (SCD) in präklinischer Alzheimer-Demenz 4
1.4 Ätiopathogenese der Alzheimer-Demenz 6
1.4.1 Cholesterolstoffwechsel 7
1.4.2 Rolle des Cholesterolstoffwechsels in der Pathogenese der Alzheimer-Demenz 9
1.5 Hippocampus 14
1.5.1 Struktur und Funktionen 14
1.5.2 Physiologische und pathologische Veränderungen des Hippocampus 16
1.6 Die Verbindung zwischen Hyperlipidämie, Hippocampusstruktur und Kognition 20
2 Aufgabenstellung 23
3 Materialien und Methoden 25
3.1 Studienpopulation 26
3.1.1 Ein- und Ausschlusskriterien 26
3.1.2 Rekrutierung 26
3.1.3 Einteilung in Gruppen 27
3.2 Untersuchungen 27
3.2.1 Medizinische körperliche Untersuchung 29
3.2.2 Neuropsychologische Tests und Fragebögen 30
III
3.2.3 Magnetresonanztomografie (MRT) 31
3.3 Statistische Analyse 33
4 Ergebnisse 34
4.1 Deskriptive Statistik 34
4.1.1 Demografie 34
4.1.2 Somatische Parameter 35
4.2 Periphere Parameter des Lipidstoffwechsels und Hippocampusstruktur 39
4.2.1 Gesamte Gruppe 39
4.2.2 Geschlechter 42
4.2.3 Kognitive Gruppen 45
5 Diskussion 49
5.1 Zentrale Ergebnisse 49
5.2 Cholesterol 50
5.2.1 Cholesterolstoffwechsel und Pathogenese der Alzheimer-Demenz 50
5.2.2 Der Mythos des HDL-Cholesterols 53
5.3 Hippocampus 55
5.3.1 Volumen 55
5.3.2 Subfieldvolumetrie 56
5.3.3 Mean Diffusivity (MD) 57
5.4 Unterschiede zwischen den Geschlechtern 59
5.5 Subjective Cognitive Decline (SCD) 60
5.6 Stärken und Limitationen der Studie 63
5.6.1 Studiendesign 63
5.6.2 Studienpopulation 65
5.7 Schlussfolgerungen und Ausblick 66
6 Zusammenfassung 69
7 Literatur 73
8 Erklärung über die eigenständige Abfassung der Arbeit 93
9 Lebenslauf 94
10 Publikation 95
11 Danksagung 96
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Estimating prevalence of subjective cognitive decline in and across international cohort studies of aging: a COSMIC studyRöhr, Susanne, Pabst, Alexander, Riedel-Heller, Steffi Gerlinde, Jessen, Frank, Turana, Yuda, Handajani, Yvonne S., Brayne, Carol, Matthews, Fiona E., Stephan, Blossom C. M., Lipton, Richard B., Katz, Mindy J., Wang, Cuiling, Guerchet, Maëlenn, Preux, Pierre-Marie, Mbelesso, Pascal, Ritchie, Karen, Ancelin, Marie-Laure, Carrière, Isabelle, Guaita, Antonio, Davin, Annalisa, Vaccaro, Roberta, Kim, Ki Woong, Han, Ji Won, Suh, Seung Wan, Shahar, Suzana, Din, Normah C., Vanoh, Divya, van Boxtel, Martin, Köhler, Sebastian, Ganguli, Mary, Jacobsen, Erin P., Snitz, Beth E., Anstey, Kaarin J., Cherbuin, Nicolas, Kumagai, Shuzo, Chen, Sanmei, Narazaki, Kenji, Ng, Tze Pin, Gao, Qi, Gwee, Xinyi, Brodaty, Herny, Kochan, Nicole A., Trollor, Julian, Lobo, Antonio, López-Antón, Raúl, Santabárbara, Javier, Crawford, John D., Lipnicki, Darren M., Sachdev, Perminder S. 08 March 2022 (has links)
Background: Subjective cognitive decline (SCD) is recognized as a risk stage for Alzheimer’s disease (AD) and other dementias, but its prevalence is not well known. We aimed to use uniform criteria to better estimate SCD prevalence across international cohorts.
Methods: We combined individual participant data for 16 cohorts from 15 countries (members of the COSMIC consortium) and used qualitative and quantitative (Item Response Theory/IRT) harmonization techniques to estimate SCD prevalence.
Results: The sample comprised 39,387 cognitively unimpaired individuals above age 60. The prevalence of SCD across studies was around one quarter with both qualitative harmonization/QH (23.8%, 95%CI = 23.3–24.4%) and IRT (25.6%, 95%CI = 25.1–26.1%); however, prevalence estimates varied largely between studies (QH 6.1%, 95%CI = 5.1–7.0%, to 52.7%, 95%CI = 47.4–58.0%; IRT: 7.8%, 95%CI = 6.8–8.9%, to 52.7%, 95%CI = 47.4–58.0%). Across studies, SCD prevalence was higher in men than women, in lower levels of education, in Asian and Black African people compared to White people, in lower- and middle-income countries compared to high-income countries, and in studies conducted in later decades.
Conclusions: SCD is frequent in old age. Having a quarter of older individuals with SCD warrants further investigation of its significance, as a risk stage for AD and other dementias, and of ways to help individuals with SCD who seek medical advice. Moreover, a standardized instrument to measure SCD is needed to overcome the measurement variability currently dominant in the field.
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Subjective Aging in Activities of Daily Living among Older Adults: Moderation by Healthcare Access and Mediation by Healthcare ResourcesUdoh, Idorenyin Imoh 07 1900 (has links)
This study examined the role of health care access and health care resources in the association between subjective aging and activities of daily living among older adults. We examined subjective aging in the context of subjective cognitive decline (SCD) relationships in three studies: (1) a scoping review of healthcare access (HCA) and resources (HCR) on dementia and COVID-19 among African American older adults; (2) subjective cognitive decline in basic activities of daily living (bADL) across age cohorts, older adults and (3) subjective cognitive decline in instrumental activities of daily living (IADL) across older adults' moderation by HCA and mediation by HCR. For the scoping review, we utilized the population, concept, and context inclusion and exclusion criteria for study admissibility for articles published on dementia and COVID-19 studies in English language journals that published from January 2019 to December 2022. The two empirical studies utilized the 2021 round 11 of the National Health and Aging Trends dataset of older adults aged 70 to above 90 funded by the National Institute for Aging. We employed multiple regression and the bias-corrected percentile Bootstrap with 5000 samples using standard path-analytic approaches for the moderated-mediation approach for the two empirical studies. Findings from the scoping review indicated racial and age disparities affected older African American adults with dementia and COVID-19, associated with lower HCA and marginal HCR. Results of mediation–moderation analysis showed SCD, lower HCR, and HCA predict a decline in bADL to be higher among the older-old age (80-89) compared to the middle-old age (70-79) or oldest-old (90 years +) cohorts. We observed similar effects for IADL. The findings from the two empirical studies suggest a "doughnut" effect by which the older-old age cohort of 80-89 may be coping less well with their bADL, as well as IADL, while the oldest-old may have adapted to functional loss in their everyday living and/or comprises adults who may have passed a mortality selection despite a more significant burden of comorbidity.
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Outcomes of stable and unstable patterns of subjective cognitive declineRöhr, Susanne, Villringer, Arno, Angermeyer, Matthias C., Luck, Tobias, Riedel-Heller, Steffi G. 07 December 2016 (has links) (PDF)
Background: Subjective cognitive decline (SCD), i.e., the self-perceived feeling of worsening cognitive function, may be the first notable syndrome of preclinical Alzheimer’s disease and other dementias. However, not all individuals with SCD progress. Stability of SCD, i.e., repeated reports of SCD, could contribute to identify individuals at risk, as stable SCD may more likely reflect the continuous neurodegenerative process of Alzheimer’s and other dementias. Methods: Cox regression analyses were used to assess the association between stability of SCD and progression to MCI and dementia in data derived from the population-based Leipzig Longitudinal Study of the Aged (LEILA75+). Results: Of 453 cognitively unimpaired individuals with a mean age of 80.5 years (SD = 4.2), 139 (30.7 %) reported SCD at baseline. Over the study period (M = 4.8 years, SD = 2.2), 84 (18.5 %) individuals had stable SCD, 195 (43.1 %) unstable SCD and 174 (38.4 %) never reported SCD. Stable SCD was associated with increased risk of progression to MCI and dementia (unadjusted HR = 1.8, 95 % CI = 1.2–2.6; p < .01), whereas unstable SCD yielded a decreased progression risk (unadjusted HR = 0.5, 95 % CI = 0.4–0.7; p < .001) compared to no SCD. When adjusted for baseline cognitive functioning, progression risk in individuals with stable SCD was significantly increased in comparison to individuals with unstable SCD, but not compared to individuals without SCD. Conclusions: Our results, though preliminary, suggest that stable SCD, i.e., repeated reports of SCD, may yield an increased risk of progression to MCI and dementia compared to unstable SCD. Baseline cognitive scores, though within a normal range, seem to be a driver of progression in stable SCD. Future research is warranted to investigate whether stability could hold as a SCD research feature.
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Approche multimodale du continuum de la maladie d'Alzheimer: investigation neuropsychologique, structurelle et fonctionnelle de la phase préclinique au stade démentiel.Puttaert, Delphine 22 October 2021 (has links) (PDF)
Cette thèse vise à tester l’hypothèse selon laquelle la maladie d’Alzheimer (MA), à ses différents stades, est responsable d’un dysfonctionnement synaptique. Ce dernier, conjointement avec d’autres processus pathologiques, pourrait mener à des modifications de l’excitabilité neuronale au sein de régions cérébrales spécifiques et, en conséquence, à des altérations de la connectivité fonctionnelle au sein des réseaux neuronaux auxquels contribuent ces régions cérébrales.Deux objectifs principaux ont été visés tout au long de ce projet. Le premier ambitionnait l’identification de nouveaux marqueurs électrophysiologiques du continuum de la MA. Le second aspirait à une meilleure compréhension de la relation entre les changements électrophysiologiques, les anomalies structurelles et métaboliques ainsi que les déficits cognitifs des patients souffrant d’une MA ou étant à risque de la développer. Afin de répondre à ces buts de recherche, une approche multimodale combinant l’exploration électrophysiologique via la magnétoencéphalographie (MEG), métabolique et structurelle via un appareil hybride associant la tomographie par émission de positons avec comme traceur le fluorodésoxyglucose (FDG) et l’imagerie par résonance magnétique structurelle (TEP-IRM), et enfin cognitive via un examen neuropsychologique a été mise en place pour tous les participants qu’ils soient dans le cadre d’un vieillissement normal ou pathologique.La première étude a investigué la manière dont le continuum de la MA altère la dynamique de l’activité cérébrale spontanée et comment cette dernière est reliée aux anomalies structurelles, métaboliques et cognitives associées à la MA. Les résultats ont principalement montré des altérations dans l’activation du réseau du mode par défaut chez les patients avec une MA constituant un corrélat électrophysiologique supplémentaire du dysfonctionnement synaptique de la MA.La deuxième étude a étudié la relation entre l'activité rythmique cérébrale en bande de fréquence alpha et les altérations en mémoire épisodique verbale en utilisant la tâche de rappel libre/rappel indicé-16 items. Nos résultats ont principalement mis en évidence un nouveau corrélat électrophysiologique du dysfonctionnement à court terme en mémoire épisodique qui peut accompagner le vieillissement pathologique.Enfin, notre dernière étude a visé à fournir une vue d'ensemble des changements électrophysiologiques associés au continuum de la MA. Nos résultats ont principalement montré une diminution globale de la connectivité fonctionnelle en bande de fréquence alpha chez les patients avec une MA soutenant la théorie selon laquelle l'hypoconnectivité apparait à un stade tardif de la démence. Ceci suggère la présence d'un syndrome de déconnexion sévère dans la MA.De manière générale, ce projet de recherche a permis l’identification de marqueurs électrophysiologiques supplémentaires de la MA ainsi qu’une meilleure compréhension du lien entre les modifications électrophysiologiques et le déficit cognitif, les anomalies structurelles ainsi qu’avec les changements métaboliques observés dans la MA. / Doctorat en Sciences psychologiques et de l'éducation / info:eu-repo/semantics/nonPublished
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Časná stádia neurodegenerativních onemocnění a jejich diagnostika metodami klinické a experimentální neuropsychologie / Early stages of neurodegenerative diseases and their diagnostics using methods of clinical and experimental neuropsychologyMarková, Hana January 2019 (has links)
The diagnosis of neurodegenerative diseases leading to dementia is increasingly moving to the earlier stages in an effort to find the disease-modifying treatment for these diseases. Prodromal and preclinical stages of the diseases have become the primary research interests. Neuropsychology is specifically focused on early cognitive markers and development of methods that would be able to reliably assess these markers and to evaluate the risk of progression of cognitive decline in individual cases. The theoretical part of the thesis presents the current knowledge in the field of neurodegenerative diseases, it is specifically focused on Alzheimer's disease (AD) as the most common cause of dementia. We also present the current trends in neuropsychological diagnostics of early AD and the approach to subjective and objective evaluation of cognitive functioning. Building on that, we present the rationale for the empirical part of the thesis. The empirical part of the thesis extends the existing knowledge in the field of AD. We present and discuss seven original publications that follow three basic objectives: first, to characterize subjective cognitive complaints of individuals at risk of AD, second, to evaluate the potential of selected standard and experimental neuropsychological methods to detect...
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Subjective Cognitive Decline in Activities of Daily Living among Older Adults with Depressive SymptomsKomalasari, Renata 05 1900 (has links)
This study aimed to understand subjective cognitive decline (SCD) and functional difficulties in older age cohorts with depressive symptoms, using one scoping review and two empirical studies. We implemented the six steps of Arksey and O'Malley's procedure for the scoping review. We used the population, concept, and context (PCC) inclusion and exclusion criteria in the literature search across MEDLINE via Ebscohost, PubMed, and PsycINFO for articles published on ADL/IADL indicators of SCD in older adults with depressive symptoms and that published in English language journals from January 2011 to November 2021. The two empirical studies used the 2019 wave of the Behavioral Risk Factor Surveillance Survey dataset of older adults aged 65 and ≥ 80 from the Centers for Disease Control and Prevention. We used multiple regression and the bias-corrected percentile bootstrap with 5000 samples using standard path-analytic approaches for the moderated mediation for the two empirical studies. Findings supported that instrumental activities of daily living (IADLs) presented more difficulties for older adults with SCD than the basic activities of daily living (B-ADLs), given that IADLs require more cognitive capabilities than B-ADLs. Environmental factors like healthcare access and subjective functional difficulties predicted SCD by mentally unhealthy day (MUD) mediation and age cohort moderation. The middle age cohort (70–74) had the most pronounced effects of the MUDs mediation in the relationship between healthcare access and IADLs in older adults with SCD. The younger-old (65–69) showed more substantial MUD mediation effects in the relationship between subjective functional difficulties and SCD. Worse SCD was associated with being Asians, female older adults, and at lower education years and income levels. Findings profiled SCD indicators in daily living activities across age cohorts and the mentally unhealthy days presentation. We extend the chronic stress theory predictions on accentuated emotional vulnerability from increased functional difficulties, compounding SCD.
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Outcomes of stable and unstable patterns of subjective cognitive decline: results from the Leipzig Longitudinal Study of the Aged (LEILA75+)Röhr, Susanne, Villringer, Arno, Angermeyer, Matthias C., Luck, Tobias, Riedel-Heller, Steffi G. January 2016 (has links)
Background: Subjective cognitive decline (SCD), i.e., the self-perceived feeling of worsening cognitive function, may be the first notable syndrome of preclinical Alzheimer’s disease and other dementias. However, not all individuals with SCD progress. Stability of SCD, i.e., repeated reports of SCD, could contribute to identify individuals at risk, as stable SCD may more likely reflect the continuous neurodegenerative process of Alzheimer’s and other dementias. Methods: Cox regression analyses were used to assess the association between stability of SCD and progression to MCI and dementia in data derived from the population-based Leipzig Longitudinal Study of the Aged (LEILA75+). Results: Of 453 cognitively unimpaired individuals with a mean age of 80.5 years (SD = 4.2), 139 (30.7 %) reported SCD at baseline. Over the study period (M = 4.8 years, SD = 2.2), 84 (18.5 %) individuals had stable SCD, 195 (43.1 %) unstable SCD and 174 (38.4 %) never reported SCD. Stable SCD was associated with increased risk of progression to MCI and dementia (unadjusted HR = 1.8, 95 % CI = 1.2–2.6; p < .01), whereas unstable SCD yielded a decreased progression risk (unadjusted HR = 0.5, 95 % CI = 0.4–0.7; p < .001) compared to no SCD. When adjusted for baseline cognitive functioning, progression risk in individuals with stable SCD was significantly increased in comparison to individuals with unstable SCD, but not compared to individuals without SCD. Conclusions: Our results, though preliminary, suggest that stable SCD, i.e., repeated reports of SCD, may yield an increased risk of progression to MCI and dementia compared to unstable SCD. Baseline cognitive scores, though within a normal range, seem to be a driver of progression in stable SCD. Future research is warranted to investigate whether stability could hold as a SCD research feature.
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