READ-OUT observational study will investigate blood-based biomarkers for dementia in real-world clinical settings. This 3-year observational study will include 3165 people, males or females aged 45 years or older, with cognitive impairment of any severity. Participants provide blood samples and complete questionnaires about quality of life and healthcare use, with some having additional follow-ups at 2 weeks and 1 year. The study will assess reliability and accuracy of blood tests in diagnosing dementia.
Dementia affects a growing number of people in the UK, with significant costs for individuals, families, and society. There is an urgent need for accurate diagnosis of dementia to allow early intervention and support when people can still make decisions about their care. Current dementia diagnosis in memory clinics relies on clinical assessment, cognitive testing, and brain scans (MRI or CT). Only a small proportion of UK patients have access to more specific tests like PET brain scans or spinal fluid analysis, which are expensive and not widely available. Recent developments have shown that blood tests can accurately detect the underlying brain changes of dementia, particularly Alzheimer's disease. In research studies, these blood-based biomarkers (ptau217, AB42/40 ratio, GFAP, NFL etc) have successfully identified people with Alzheimer's disease when compared to clinical diagnoses, gold standard brain scans, and post-mortem brain examination. These blood tests also show promise for predicting people with future dementia risk. However, most research has been conducted in younger, less diverse populations than those seen in real-world memory services. Blood-based biomarkers are not yet used in routine NHS practice, and more work is needed to test how well they perform in representative UK populations. We also need to understand whether people want to know their blood test results, what information they want, and how this is best communicated. The READ-OUT study will test blood-based biomarkers in people attending memory clinics across the UK (30 NHS sites), ensuring participants represent the full diversity of people with dementia or memory concerns (30% from underrepresented groups). Participants will provide a 40ml blood sample and complete questionnaires about quality of life, healthcare use, and attitudes toward blood testing for dementia. The accuracy of blood biomarkers will be compared against established diagnostic methods including expert clinical review, brain scans, spinal fluid tests, and long-term health record follow-up. The study includes three optional sub-studies: test-retest reliability of blood biomarkers (10% of participants returning after 1-2 weeks), investigating disease progression over one year (20% of participants), and evaluating whether people can collect blood samples at home using finger-prick cards (75 participants). The study will determine which blood biomarkers are most accurate for diagnosing different types of dementia, predict disease progression, and assess their cost-effectiveness in the healthcare system. Results will inform whether these tests should be integrated into NHS clinical pathways and will guide the design of READ-OUT Phase 2, a randomized trial testing whether providing blood biomarker results to patients and doctors improves clinical care and outcomes.
Diagnostic accuracy of blood-based biomarkers for dementia diagnosis
Accuracy, Positive and Negative predictive value in regard to diagnosis and, where available, gold standard biomarker measures (clinical consensus, cerebrospinal fluid, CSF, positron emission tomography, PET)
Time frame: baseline and at 52 weeks
Feasibility and acceptability of blood-based biomarkers for dementia diagnosis
Recruitment metrics at site level Acceptability patient questionnaires Patient and Public Involvement qualitative data around acceptability of BBM collection
Time frame: baseline, at 2 weeks and 52 weeks
Cost-effectiveness of blood biomarkers in a real-world cognitive disorders population
Health-related quality of life (HR-QoL) Healthcare utilisation
Time frame: baseline and at 52 weeks
Disease prediction utility of blood-based biomarkers in diverse cognitive disorders populations
Cognitive score progression, MCI to dementia conversion, Institutionalisation, or Death, ethnicity.
Time frame: baseline and at 52 weeks
Optimal individual or sets of biomarkers for separate dementia aetiologies
Accuracy, Positive and Negative predictive value in regard to subgroups of dementia diagnosis
Time frame: baseline, at 2 weeks and 52 weeks
Impact of sample processing delays on the accuracy of blood biomarkers
BBM levels obtained from samples of varying degrees of processing delays
Time frame: Baseline study visit
The test-retest reliability of blood biomarkers
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Study Type
OBSERVATIONAL
Enrollment
3,165
Betsi Cadwaladr University Health Board
Bangor, United Kingdom
ReMind UK
Bath, United Kingdom
Belfast Health & Social Care Trust
Belfast, United Kingdom
Dorset HealthCare University NHS Foundation Trust
Bournemouth, United Kingdom
Berkshire Healthcare NHS Foundation Trust
Bracknell, United Kingdom
Bradford District Care NHS Foundation Trust
Bradford, United Kingdom
North Bristol NHS Trust
Bristol, United Kingdom
Cambridgeshire and Peterborough NHS Foundation Trust
Cambridge, United Kingdom
Devon Partnership NHS Trust
Exeter, United Kingdom
Barts Health NHS Trust
London, United Kingdom
...and 17 more locations
BBM levels obtained from repeated sampling at baseline and after 1-2 week - a sub- study involving 10% of the participant sample. Whether samples taken at different time points are comparable will be assessed
Time frame: Baseline study visit, 1-2 week visit
The utility of remote blood test kits
Comparison of BBM levels obtained from phlebotomy and blood spot cards/Capillary Tubes involving 75 individuals within the sample; Accuracy, positive and negative predictive value for blood spot card/Capillary Tubes BBMs
Time frame: Baseline study visit
Understanding participant preferences on disclosure of biomarker status in dementia diagnosis
Evaluation of participants' views on what information they wish to receive about their biomarker status, the preferred timing of disclosure, and the most appropriate method of communication. Quantitative data will be collected via questionnaires completed by all participants at baseline. A qualitative sub-study involving 15-20 participants, supported by the trial PPIE group, will explore experiences and preferences in greater depth through interviews and/or focus groups.
Time frame: baseline and at 52 weeks