Improving diagnosis and care in people affected by ... · Care: the right interventions, to the...

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Improving diagnosis and care in people affected by progressive supranuclear palsy (PSP) and corticobasal degeneration (CBD) CSO/PSP Association Clinical Research Fellowship Dr Diane Swallow NHS Research Scotland Annual Conference, 26 th October 2016

Transcript of Improving diagnosis and care in people affected by ... · Care: the right interventions, to the...

Page 1: Improving diagnosis and care in people affected by ... · Care: the right interventions, to the right patients, at the right time Prognosis: improved communication, care planning

Improving diagnosis and care in people affected by progressive supranuclear palsy (PSP) and

corticobasal degeneration (CBD)

CSO/PSP Association Clinical Research Fellowship

Dr Diane Swallow

NHS Research Scotland Annual Conference, 26th October 2016

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Overview

“…to improve the evidence base on routes to diagnosis and care of people living with progressive supranuclear palsy (PSP) and

corticobasal degeneration (CBD)…”

• Background

• Study aims and overview

• Relevance to the NHS and future directions

• Benefits of the fellowship

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Background PSP and CBD

• Progressive neurodegenerative diseases causing physical and dementia-like symptoms

• Significant disability with an average life expectancy of 5 – 8 years

• Misdiagnosis and delayed diagnosis common- Reasons for misdiagnosis and delayed diagnosis?- Screening tools to improve diagnosis?

• Prognosis and care- Implementation and access to multidisciplinary care?- Prognosis other than survival?- Impact on carers?

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Study aims

1 Describe & improve diagnostic pathways in PSP/CBD

2 Validate & develop new diagnostic tools in PSP/CBD

- Edinburgh Cognitive and Edinburgh Motor Assessment Scales

- MRI (3T structural)

3 Describe & improve the quality of care of PSP/CBD patients from diagnosis to end-of-life

4 Evaluate activity limitations as a measure of disease progression, and assess carer outcomes

5 Establish the prevalence of PSP/CBD in Scotland using new diagnostic criteria

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Study population and setting

• Existing cohorts of PSP/CBD patients and carers• PINE study

• Tracking Parkinson’s study

• New national cohort of PSP/CBD patients and carers

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The PINE Study (Parkinsonism in the North East of Scotland)

PSP/CBD patients and their carers recruited from 2002-09 (n=30)

PSP/CBD patients initially thought to have Parkinson’s (n~5)

Annual assessments: motor and cognitive function, activity limitation, mood, quality of life and carer mood and care burden

6 monthly assessments: diagnostic features, risk factors, motor and non-motor features, cognition, quality of life, olfaction testing

Tracking Parkinson’s (PRoBaND)

Existing cohorts

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New cohort: case finding

Existing patients with PSP/CBD over 2 to 2.5 year recruitment period:

• National- ICD-10 diagnostic coding from Scottish Morbidity Record

- Referrals from hospital specialists

- Patient self-referral

• Grampian (to determine true prevalence rate)- Referrals from GP’s

- Search of outpatient referral letters: neurology, medicine for the elderly and old age psychiatry

Inclusion criteria

Fulfil diagnostic criteria for possible or probable PSP, or

CBD

Subtypes considered to be possible allied syndromes (e.g.

PSP-parkinsonism)

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New cohort: staged consent

Patients invited to consent (or assent sought) to any/all of:

I. access to medical records and linkage to health and social care registers

II. a one-off assessment visit

III. a six month postal follow-up

IV. inclusion in a new Scottish PSP/CBD register

V. 3T MR brain imaging

VI. DNA/serum for the PROgressive Supranuclear Palsy CorTicoBasal Syndrome Multiple System Atrophy Longitudinal Study UK (PROSPECT-M-UK) biomarker study

Carers invited to return questionnaires about their health, carer burden, and a proxy assessment of patients capabilities

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Methods 1: Describe & improve diagnostic pathways in PSP/CBD

Using health records and interviews assess:

• Time delays (patient, primary, secondary care)

• Frequency and type of incorrect initial diagnoses

• Reasons for misdiagnosis

• Location of secondary care speciality referrals

• Potential missed diagnostic opportunities

Compare delays and error rates with age-sex matched Parkinson’s disease patients

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Methods 2: Validate & develop new diagnostic tools

Edinburgh Cognitive Assessment Scale (ECAS) and Edinburgh Motor

Assessment Scale (EMAS)

Compare with established cognitive (ACE-III) and motor assessments (UPDRS Part 3)

Compare scores of PSP/CBD cases with PD cases to determine their ability to discriminate between PSP/CBD and PD

Imaging 3T MRI

Imaging features which discriminate between PSP/CBD and other parkinsonian or dementia conditions (e.g. midbrain:pons ratio)

Additional MRI scans from PINE and local imaging studies.

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Methods 3: Describe & improve the quality of care from diagnosis to end-of-life

Using research records, clinical assessments and questionnaires:

• Describe clinical features (e.g. motor, cognitive, mood) at study onset and 6 months to define disease stage and care requirements

• Evaluate health service interventions and care pathway co-ordination to determine if these meet recommended standards

• Include patient/carer self report of interactions and their perceived effectiveness

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Aim 4 Patient and carer prognosis, and functional activity limitations

Evaluation of activity limitation/dependency

• Existing functional scales

• Extended list of basic and instrumental ADLs- Frequency of limitation- Order of loss of independence- Activities particularly affecting quality of life

Carer prognosis

• Matched to PSP/CBD patient’s symptoms and health needs

• Compared to carers of people with PD

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Future outcomes and benefits of the fellowship

Diagnosis: targeted education and adoption new tools

Care: the right interventions, to the right patients, at the right time

Prognosis: improved communication, care planning and provision, carer support

Prevalence: resource allocation for care planning

Future: earlier diagnosis, national register, well characterised clinical trial ready cohort, ongoing follow-up

Fellowship benefits: time, funding and opportunity to work in an area of clinical and academic interest, and to be equipped for a future independent academic career

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Acknowledgements

Funders: Chief Scientist Office and PSP Association

Supervisors: Dr Carl Counsell, Dr Donald Grosset, Dr Thomas Bak