Clinico-demographics of people with younger-onset dementia and neuropsychiatric symptoms referred to an Australian dementia support service: A comparison study with older-onset dementia

Author:

Loi Samantha M12ORCID,Atee Mustafa3,Morris Thomas4,Whiting Daniel4,Macfarlane Stephen45,Cunningham Colm46,Velakoulis Dennis12

Affiliation:

1. Neuropsychiatry, The Royal Melbourne Hospital, Parkville, VIC, Australia

2. Melbourne Neuropsychiatry Centre, The University of Melbourne and The Royal Melbourne Hospital, Parkville, VIC, Australia

3. HammondCare, The Dementia Centre, Osborne Park, WA, Australia

4. HammondCare, The Dementia Centre, St Leonards, NSW, Australia

5. Faculty of Medicine, Nursing and Health Sciences, Monash University, Clayton, VIC, Australia

6. School of Public Health and Community Medicine, University of New South Wales, Sydney, NSW, Australia

Abstract

Objective: Younger-onset dementia accounts for about 5–10% of all dementias in Australia. Little data is available on neuropsychiatric symptoms in people with younger-onset dementia compared to those with older-onset dementia. This study aims to compare the types of neuropsychiatric symptoms and their clinico-demographic characteristics of people with younger-onset dementia and older-onset dementia who are referred to a specific dementia support service. Methods: A 2-year retrospective observational cross-sectional analysis was undertaken on referrals with neuropsychiatric symptoms from Dementia Support Australia programmes. Neuropsychiatric symptoms were measured using the Neuropsychiatric Inventory total severity scores and distress scores. Contributing factors to neuropsychiatric symptoms for dementia groups were examined. Logistic regression was used to examine the relationship between individual neuropsychiatric symptoms and having older-onset dementia vs younger-onset dementia. Results: Of the 15,952 referrals, about 5% ( n = 729, mean age: 60.7 years, standard deviation = 5.4) were individuals with younger-onset dementia. Referrals with older-onset dementia were more likely to be female (56%), whereas referrals with younger-onset dementia were more likely to be male (54%). There was a four times greater rate of frontotemporal dementia for those with younger-onset dementia (16.0%, n = 117) compared to those with older-onset dementia (2.8%, n = 427), χ2 (1)  = 366.2, p < 0.001. Referrals with younger-onset dementia were more likely to be referred from community settings and those with older-onset dementia were more likely to be from residential aged care. Overall, there was no difference in the severity and distress of neuropsychiatric symptoms between the two groups. Contributing factors to neuropsychiatric symptoms were different between the groups, with pain being more frequently endorsed for individuals with older-onset dementia whereas communication difficulties were more commonly identified for those with younger-onset dementia. Conclusion: Clinico-demographics of referrals with younger-onset dementia differ from those with older-onset dementia. There were some differences in the characteristics of neuropsychiatric symptoms between younger-onset dementia and older-onset dementia. Our findings have implications for service provision and support for people with dementia at different ages.

Funder

National Health and Medical Research Council

Publisher

SAGE Publications

Subject

Psychiatry and Mental health,General Medicine

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