The Influence of Co-Morbidity and Frailty on the Clinical Manifestation of Patients with Alzheimer's Disease

Oosterveld, Saskia M.; Kessels, Roy P. C.; Hamel, Renske; Ramakers, Inez H.G.B.; Aalten, Pauline; Verhey, Frans R.J.; Sistermans, Nicole; Smits, Lieke; Pijnenburg, Yolande A.L.; Flier, Wiesje M. van der; Rikkert, Marcel G M Olde; Melis, René J. F.

doi:10.3233/jad-140138

Cited by 35 publications

(38 citation statements)

References 38 publications

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“…Studies of imaging and pathology in AD show faster evolving brain atrophy in early-onset than in late-onset AD [28], which is in contrast to our study where some of the younger patients with mild or very mild AD showed little progression. The heterogeneity of our sample regarding age and disease severity indicates that age-related comorbidities may be of importance for disease progression although this could not be shown by the analyses in the present study [29].…”

Section: Discussioncontrasting

confidence: 53%

Progression of Alzheimer’s Disease: A Longitudinal Study in Norwegian Memory Clinics

Eldholm

Barca

Persson

et al. 2018

JAD

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Abstract.Background: The course of Alzheimer's disease (AD) varies considerably between individuals. There is limited evidence on factors important for disease progression. Objective: The primary aim was to study the progression of AD, as measured by the Clinical Dementia Rating Scale Sum of Boxes (CDR-SB). Secondary aims were to investigate whether baseline characteristics are important for differences in progression, and to examine the correlation between progression assessed using three different instruments: CDR-SB (0-18), the cognitive test Mini-Mental State Examination (MMSE, 0-30), and the functional measure Instrumental Activities of Daily Living (IADL, 0-1). Methods: The Progression of AD and Resource use (PADR) study is a longitudinal observational study in three Norwegian memory clinics. Results: In total, 282 AD patients (mean age 73.3 years, 54% female) were followed for mean 24 (16-37) months. The mean annual increase in CDR-SB was 1.6 (SD 1.8), the mean decrease in MMSE score 1.9 (SD 2.6), and the mean decrease in IADL score 0.13 (SD 0.14). Of the 282 patients, 132 (46.8%) progressed slowly, with less than 1 point yearly increase in CDR-SB. Cognitive test results at baseline predicted progression rate, and together with age, ApoE, history of hypertension, and drug use could explain 17% of the variance in progression rate. The strongest correlation of change was found between CDR-SB and IADL scores, the weakest between MMSE and IADL scores.

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Section: Discussioncontrasting

confidence: 53%

Progression of Alzheimer’s Disease: A Longitudinal Study in Norwegian Memory Clinics

Eldholm

Barca

Persson

et al. 2018

JAD

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“…Adjustment for baseline age was unclear in two studies [15, 19]. Adjustment for education was lacking or unclear in five studies examining cognition [16, 17, 19–21]. Adjustment for baseline symptoms of interest was unclear in one out of six longitudinal studies [19].…”

Section: Resultsmentioning

confidence: 99%

“…An overview of these studies, including their measurement scales and results is provided in Table 2. Eight studies used the Mini-Mental State Examination (MMSE) [27] to measure cognition, one used the Global Deterioration Scale (GDS) [28] and one used a composite score of neuropsychological tests [16]. The presence of comorbidities was related to decreased cognitive abilities in seven out of the ten studies examining cognition.…”

Section: Resultsmentioning

confidence: 99%

Comorbidity and progression of late onset Alzheimer’s disease: A systematic review

et al. 2017

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BackgroundAlzheimer’s disease is a neurodegenerative syndrome characterized by multiple dimensions including cognitive decline, decreased daily functioning and psychiatric symptoms. This systematic review aims to investigate the relation between somatic comorbidity burden and progression in late-onset Alzheimer’s disease (LOAD).MethodsWe searched four databases for observational studies that examined cross-sectional or longitudinal associations of cognitive or functional or neuropsychiatric outcomes with comorbidity in individuals with LOAD. From the 7966 articles identified originally, 11 studies were included in this review. The Newcastle-Ottawa quality assessment was used. The large variation in progression measures, comorbidity indexes and study designs hampered the ability to perform a meta-analysis. This review was registered with PROSPERO under DIO: 10.15124/CRD42015027046.ResultsNine studies indicated that comorbidity burden was associated with deterioration in at least one of the three dimensions of LOAD examined. Seven out of ten studies investigating cognition found comorbidities to be related to decreased cognitive performance. Five out of the seven studies investigating daily functioning showed an association between comorbidity burden and decreased daily functioning. Neuropsychiatric symptoms (NPS) increased with increasing comorbidity burden in two out of three studies investigating NPS. Associations were predominantly found in studies analyzing the association cross-sectionally, in a time-varying manner or across short follow-up (≤2 years). Rarely baseline comorbidity burden appeared to be associated with outcomes in studies analyzing progression over longer follow-up periods (>2 years).ConclusionThis review provides evidence of an association between somatic comorbidities and multifaceted LOAD progression. Given that time-varying comorbidity burden, but much less so baseline comorbidity burden, was associated with the three dimensions prospectively, this relationship cannot be reduced to a simple cause-effect relation and is more likely to be dynamic. Therefore, both future studies and clinical practice may benefit from regarding comorbidity as a modifiable factor with a possibly fluctuating influence on LOAD.

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“…The total CIRS-G score leaving out the category of psychiatric illness was higher in the dementia than in the MCI cohort. For the AD patients in the dementia cohort, it was found that comorbidities were associated with cognitive performance; frailty was associated with functional abilities at baseline [25]. Comparing older and younger persons with dementia contrasting persons from the 4c Dementia cohort data with persons from the NeedYD cohort [26], showed that younger persons had less comorbidity and may more often have neurological comorbidities than older persons with dementia [27].…”

Section: Resultsmentioning

confidence: 99%

A profile of The Clinical Course of Cognition and Comorbidity in Mild Cognitive Impairment and Dementia Study (The 4C study): two complementary longitudinal, clinical cohorts in the Netherlands

et al. 2016

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BackgroundHeterogeneous disease trajectories of mild cognitive impairment (MCI) and dementia are frequently encountered in clinical practice, but there is still insufficient knowledge to understand the reasons and mechanisms causing this heterogeneity. In addition to correlates of the disorder, patient characteristics such as their health status, social environment, comorbidities and frailty may contribute to variability in trajectories over time. The current paper outlines the study design and the study population of and provides an overview of the data collected in the Clinical Course of Cognition and Comorbidity in Mild Cognitive Impairment (4C-MCI cohort, n = 315) and Dementia (4C-Dementia cohort, n = 331) Study. MethodsThe two complementary longitudinal cohorts part of the 4C study began enrolment in March 2010. Participants were prospectively recruited from three collaborating Dutch Alzheimer Centers, with three annual follow-up assessments after baseline. Extensive neuropsychological assessments, and detailed profiling of comorbidities, health and frailty at each follow up were the key features of the 4C study. As such, the 4C study was designed to study if and how patients’ comorbidities and frailty are associated with the course of MCI and dementia measured with a comprehensive and multidimensional set of outcomes including cognition, daily functioning, quality of life, behavioral disturbances, caregiver burden, institutionalization and death and whether the effects of medical health and frailty differ between MCI and dementia stages of cognitive disorders.ConclusionSampled in a clinical setting, the 4C study complements population-based studies on neurodegenerative disorders in terms of the type of assessment (e.g. comorbidity, frailty, and functional status were repeatedly assessed). The 4C study complements available clinical cohorts of MCI and dementia patients, because the exclusion criteria were kept to a minimum, to obtain a sample that is representative for the average patient visiting a memory clinic.

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The Influence of Co-Morbidity and Frailty on the Clinical Manifestation of Patients with Alzheimer's Disease

Cited by 35 publications

References 38 publications

Progression of Alzheimer’s Disease: A Longitudinal Study in Norwegian Memory Clinics

Progression of Alzheimer’s Disease: A Longitudinal Study in Norwegian Memory Clinics

Comorbidity and progression of late onset Alzheimer’s disease: A systematic review

A profile of The Clinical Course of Cognition and Comorbidity in Mild Cognitive Impairment and Dementia Study (The 4C study): two complementary longitudinal, clinical cohorts in the Netherlands

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