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dc.contributor.authorBanerjee, S
dc.contributor.authorFarina, N
dc.contributor.authorHenderson, C
dc.contributor.authorHigh, J
dc.contributor.authorStirling, S
dc.contributor.authorShepstone, L
dc.contributor.authorFountain, J
dc.contributor.authorBallard, C
dc.contributor.authorBentham, P
dc.contributor.authorBurns, A
dc.contributor.authorFox, C
dc.contributor.authorFrancis, P
dc.contributor.authorHoward, R
dc.contributor.authorKnapp, M
dc.contributor.authorLeroi, I
dc.contributor.authorLivingston, G
dc.contributor.authorNilforooshan, R
dc.contributor.authorNurock, S
dc.contributor.authorO’Brien, J
dc.contributor.authorPrice, A
dc.contributor.authorThomas, AJ
dc.contributor.authorSwart, AM
dc.contributor.authorTelling, T
dc.contributor.authorTabet, N
dc.contributor.otherHealth Technology Assessment programme
dc.date.accessioned2024-05-08T06:59:25Z
dc.date.available2024-05-08T06:59:25Z
dc.date.issued2023-10
dc.identifier.issn1366-5278
dc.identifier.issn2046-4924
dc.identifier.urihttps://pearl.plymouth.ac.uk/handle/10026.1/22469
dc.description.abstract

Background: Agitation is common and impacts negatively on people with dementia and carers. Non-drug patient-centred care is first-line treatment, but we need other treatment when this fails. Current evidence is sparse on safer and effective alternatives to antipsychotics.

Objectives: To assess clinical and cost-effectiveness and safety of mirtazapine and carbamazepine in treating agitation in dementia.

Design: Pragmatic, phase III, multicentre, double-blind, superiority, randomised, placebo-controlled trial of the clinical effectiveness of mirtazapine over 12 weeks (carbamazepine arm discontinued).

Setting: Twenty-six UK secondary care centres.

Participants: Eligibility: probable or possible Alzheimer’s disease, agitation unresponsive to non-drug treatment, Cohen-Mansfield Agitation Inventory score ≥ 45.

Interventions: Mirtazapine (target 45 mg), carbamazepine (target 300 mg) and placebo.

Outcome measures: Primary: Cohen-Mansfield Agitation Inventory score 12 weeks post randomisation. Main economic outcome evaluation: incremental cost per six-point difference in Cohen-Mansfield Agitation Inventory score at 12 weeks, from health and social care system perspective. Data from participants and informants at baseline, 6 and 12 weeks. Long-term follow-up Cohen-Mansfield Agitation Inventory data collected by telephone from informants at 6 and 12 months.

Randomisation and blinding: Participants allocated 1 : 1 : 1 ratio (to discontinuation of the carbamazepine arm, 1 : 1 thereafter) to receive placebo or carbamazepine or mirtazapine, with treatment as usual. Random allocation was block stratified by centre and residence type with random block lengths of three or six (after discontinuation of carbamazepine, two or four). Double-blind, with drug and placebo identically encapsulated. Referring clinicians, participants, trial management team and research workers who did assessments were masked to group allocation.

Results: Two hundred and forty-four participants recruited and randomised (102 mirtazapine, 102 placebo, 40 carbamazepine). The carbamazepine arm was discontinued due to slow overall recruitment; carbamazepine/placebo analyses are therefore statistically underpowered and not detailed in the abstract. Mean difference placebo-mirtazapine (−1.74, 95% confidence interval −7.17 to 3.69; p = 0.53). Harms: The number of controls with adverse events (65/102, 64%) was similar to the mirtazapine group (67/102, 66%). However, there were more deaths in the mirtazapine group (n = 7) by week 16 than in the control group (n = 1). Post hoc analysis suggests this was of marginal statistical significance (p = 0.065); this difference did not persist at 6- and 12-month assessments. At 12 weeks, the costs of unpaid care by the dyadic carer were significantly higher in the mirtazapine than placebo group [difference: £1120 (95% confidence interval £56 to £2184)]. In the cost-effectiveness analyses, mean raw and adjusted outcome scores and costs of the complete cases samples showed no differences between groups.

Limitations: Our study has four important potential limitations: (1) we dropped the proposed carbamazepine group; (2) the trial was not powered to investigate a mortality difference between the groups; (3) recruitment beyond February 2020, was constrained by the COVID-19 pandemic; and (4) generalisability is limited by recruitment of participants from old-age psychiatry services and care homes.

Conclusions: The data suggest mirtazapine is not clinically or cost-effective (compared to placebo) for agitation in dementia. There is little reason to recommend mirtazapine for people with dementia with agitation.

Future work: Effective and cost-effective management strategies for agitation in dementia are needed where non-pharmacological approaches are unsuccessful.

Study registration: This trial is registered as ISRCTN17411897/NCT03031184.

Funding: This project was funded by the National Institute for Health and Care Research (NIHR) Health Technology Assessment programme and will be published in full in Health Technology Assessment; Vol. 27, No. 23. See the NIHR Journals Library website for further project information.

dc.format.extent1-108
dc.format.mediumPrint
dc.languageen
dc.publisherNational Institute for Health and Care Research
dc.subjectAGITATION
dc.subjectALZHEIMER’S DISEASE
dc.subjectCARBAMAZEPINE
dc.subjectDEMENTIA
dc.subjectMIRTAZAPINE
dc.subjectRCT
dc.subjectHumans
dc.subjectAlzheimer Disease
dc.subjectCarbamazepine
dc.subjectCost-Benefit Analysis
dc.subjectMirtazapine
dc.subjectPandemics
dc.subjectQuality of Life
dc.subjectTechnology Assessment, Biomedical
dc.titleA pragmatic, multicentre, double-blind, placebo-controlled randomised trial to assess the safety, clinical and cost-effectiveness of mirtazapine and carbamazepine in people with Alzheimer’s disease and agitated behaviours: the HTA-SYMBAD trial
dc.typereport
plymouth.author-urlhttps://www.ncbi.nlm.nih.gov/pubmed/37929672
plymouth.confidentialfalse
plymouth.issue23
plymouth.volume27
plymouth.publisher-urlhttp://dx.doi.org/10.3310/vpdt7105
plymouth.publication-statusPublished online
plymouth.journalHealth Technology Assessment
dc.identifier.doi10.3310/vpdt7105
plymouth.organisational-group|Plymouth
plymouth.organisational-group|Plymouth|PS - Office of Vice Chancellor
plymouth.organisational-group|Plymouth|Faculty of Health
plymouth.organisational-group|Plymouth|REF 2021 Researchers by UoA
plymouth.organisational-group|Plymouth|Users by role
plymouth.organisational-group|Plymouth|Users by role|Current Academic staff
plymouth.organisational-group|Plymouth|REF 2021 Researchers by UoA|UoA04 Psychology, Psychiatry and Neuroscience
plymouth.organisational-group|Plymouth|Faculty of Health|Peninsula Medical School
plymouth.organisational-group|Plymouth|Users by role|Researchers in ResearchFish submission
plymouth.organisational-group|Plymouth|Faculty of Health|Peninsula Medical School|PMS - Manual
plymouth.organisational-group|Plymouth|REF 2029 Researchers by UoA
plymouth.organisational-group|Plymouth|REF 2029 Researchers by UoA|UoA04 Psychology, Psychiatry and Neuroscience
dc.publisher.placeEngland
dc.date.updated2024-05-08T06:59:25Z
dc.rights.embargodate2024-5-9
dc.identifier.eissn2046-4924
dc.rights.embargoperiod
rioxxterms.versionofrecord10.3310/vpdt7105


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