Alzheimer's disease (AD) and frontotemporal dementia (FTD) are the most common neurodegenerative early-onset dementias. Despite the fact that both conditions have a very distinctive clinical pattern, they present with an overlap in their cognitive and behavioral features that may lead to misdiagnosis or delay in diagnosis. The current review intends to summarize briefly the main differences at the clinical, neuropsychological, and behavioral levels, in an attempt to suggest which aspects would facilitate an adequate diagnosis in a clinical setting, especially in Latin American and low-and middle-income countries, where the resources needed for a differential diagnosis (such as MRI or biomarkers) are not always available. A timely diagnosis of AD and FTD have significant implications for the medical management and quality of life of patients and careers.
The Neuropsychiatric Inventory Questionnaire (NPI-Q) is an informant-based
instrument that measures the presence and severity of 12 Neuropsychiatric
Symptoms (NPS) in patients with dementia, as well as informant distress.ObjectiveTo measure the psychometric properties of the NPI-Q and the prevalence of NPS
in patients with Alzheimer's disease (AD) in Chile.Methods53 patients with AD were assessed. Subjects were divided into two different
groups: mild AD (n=26) and moderate AD (n=27). Convergent validity was
estimated by correlating the outcomes of the NPI-Q with Neuropsychiatric
Inventory (NPI) scores and with a global cognitive efficiency test
(Addenbrooke's Cognitive Examination - Revised - ACE-R). Reliability of the
NPI-Q was analysed by calculating its internal consistency. Prevalence of
NPS was estimated with both the NPI and NPI-Q.ResultsPositive and significant correlations were observed between the NPI-Q, the
NPI, and the ACE-R (r=0.730; p<0.01 and 0.315; p<0.05 respectively).
The instrument displayed an adequate level of reliability (Cronbach's
alpha=0.783). The most prevalent NPS were apathy/indifference (62.3%) and
dysphoria/depression (58.5%).ConclusionThe NPI-Q exhibited acceptable validity and reliability indicators for
patients with AD in Chile, indicating that it is a suitable instrument for
the routine assessment of NPS in clinical practice.
Background: Memory impairment in behavioral variant frontotemporal dementia (bvFTD) is traditionally considered to be mild and attributed to prefrontal cortex dysfunction. Recent studies, however, indicated that some patients can present with a memory impairment of the hippocampal type, showing storage and consolidation deficits in addition to the more executive/prefrontal related encoding and strategic difficulties.
ObjectiveTo compare social cognition performance between patients with amyotrophic lateral sclerosis (ALS) and those patients with behavioural variant frontotemporal dementia (bvFTD).MethodsWe included 21 participants with ALS, 20 with bvFTD and 21 healthy controls who underwent a comprehensive cognitive battery, including the short version of the Social Cognition and Emotional Assessment (Mini-SEA), which comprises the faux pas test and Facial Emotion Recognition Test (FERT); Mini-Mental State Examination; Frontal Assessment Battery; lexical fluency (F-A-S), category fluency (animals/minute), digit span (direct and backwards) tests and the Hayling test. A post hoc analysis was conducted with the patients with ALS divided into two subgroups: patients without cognitive impairment (ALScn; n=13) and patients with cognitive impairment (ALSci; n=8).ResultsNo significant difference was noted between participant groups in terms of the age, sex and education. ALS-total group and patients with bvFTD had similar disease durations. Patients with ALSci performed poorly when compared with controls with regard to the FERT (p<0.001), the faux pas (p<0.004) and the Mini-SEA (p<0.002) total scores. Moreover, patients with bvFTD performed poorly in comparison with controls in executive and social cognition tests. The performance of patients with ALSci was similar to that of patients with bvFTD, while the performance of patients with ALScn was similar to that of controls.DiscussionOur findings support a cognitive continuum between ALS and bvFTD and shed light on the cognitive heterogeneity of ALS, expanding its possible neuropsychological profiles.
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