A clinicopathological study of selected cognitive impairment cases in Lothian, Scotland: enhanced CJD surveillance in the 65 + population group

Lovney Kanguru; Gemma Logan; Briony Waddel; Colin Smith; Anna Molesworth; Richard Knight

doi:10.1186/s12877-022-03280-4

BMC Geriatrics (Jul 2022)

A clinicopathological study of selected cognitive impairment cases in Lothian, Scotland: enhanced CJD surveillance in the 65 + population group

Lovney Kanguru,
Gemma Logan,
Briony Waddel,
Colin Smith,
Anna Molesworth,
Richard Knight

Affiliations

Lovney Kanguru: National CJD Research & Surveillance Unit (NCJDRSU), University of Edinburgh, Western General Hospital
Gemma Logan: NHS Lothian and Queen Margaret University
Briony Waddel: Department of Neurology, Ninewells Hospital
Colin Smith: National CJD Research & Surveillance Unit (NCJDRSU), University of Edinburgh, Western General Hospital
Anna Molesworth: Public Health Scotland (PHS)
Richard Knight: National CJD Research & Surveillance Unit (NCJDRSU), University of Edinburgh, Western General Hospital

DOI: https://doi.org/10.1186/s12877-022-03280-4
Journal volume & issue: Vol. 22, no. 1
pp. 1 – 13

Abstract

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Abstract Background Variant Creutzfeldt-Jakob Disease (vCJD) is primarily associated with dietary exposure to bovine-spongiform-encephalopathy. Cases may be missed in the elderly population where dementia is common with less frequent referral to specialist neurological services. This study’s twin aims were to determine the feasibility of a method to detect possible missed cases in the elderly population and to identify any such cases. Methods A multi-site study was set-up in Lothian in 2016, to determine the feasibility of enhanced CJD-surveillance in the 65 + population-group, and undertake a clinicopathological investigation of patients with features of ‘atypical’ dementia. Results Thirty patients are included; 63% male, 37% female. They were referred because of at least one neurological feature regarded as ‘atypical’ (for the common dementing illnesses): cerebellar ataxia, rapid progression, or somato-sensory features. Mean-age at symptom-onset (66 years, range 53–82 years), the time between onset-of-symptoms and referral to the study (7 years, range 1–13 years), and duration-of-illness from onset-of-symptoms until death or the censor-date (9.5 years, range 1.1–17.4 years) were determined. By the censor-date, 9 cases were alive and 21 had died. Neuropathological investigations were performed on 10 cases, confirming: Alzheimer’s disease only (2 cases), mixed Alzheimer’s disease with Lewy bodies (2 cases), mixed Alzheimer’s disease with amyloid angiopathy (1 case), moderate non-amyloid small vessel angiopathy (1 case), a non-specific neurodegenerative disorder (1 case), Parkinson's disease with Lewy body dementia (1 case), and Lewy body dementia (2 cases). No prion disease cases of any type were detected. Conclusion The surveillance approach used was well received by the local clinicians and patients, though there were challenges in recruiting sufficient cases; far fewer than expected were identified, referred, and recruited. Further research is required to determine how such difficulties might be overcome. No missed cases of vCJD were found. However, there remains uncertainty whether this is because missed cases are very uncommon or because the study had insufficient power to detect them.

Published in BMC Geriatrics

ISSN: 1471-2318 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine: Special situations and conditions: Geriatrics
Website: https://bmcgeriatr.biomedcentral.com

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