Anticipatory care planning intervention for older adults at risk of functional decline: study protocol for a primary care cluster feasibility randomised trial

As a first step, the trial administrator will order the GP practices alphabetically and use this order to code the four practices in Northern Ireland and the four practices in the RoI. The trial administrator will inform the co-applicant methodologist when all four practices in Northern Ireland or the RoI are ready for randomisation and send him their codes, along with an indication of whether the practice is urban or rural. The methodologist, who will be blind to the identity of the practice, will then use the random number function in Microsoft Excel to assign a random number for each code. In each jurisdiction, the urban and the rural practice with the lowest number will be allocated to the intervention group and the other two practices will be allocated to the control group. The methodologist will send the allocations to the trial administrator, who, by linking the alphabetic code to the relevant practice, will know to which group each practice has been allocated. The trial administrator will inform the research nurse of the allocations and will then inform each practice of their allocation.

The project will be implemented across two healthcare systems: Northern Ireland and the RoI. Northern Ireland is a region within the United Kingdom that provides an integrated health and social services model of care, under the NHS, which is free to the user at the point of delivery. The RoI has a mixed public-private healthcare system with all persons resident in the country entitled to receive hospital care through the publicly funded healthcare system. In addition, the General Medical Services (GMS) card, which is available to all persons aged ≥ 70 years and those under 70 years who meet a certain income threshold, facilitates the use of the majority of health services free of charge, including GP practice visits as well as inpatient, emergency and outpatient services in public hospitals. In this group, medication charges incur a small co-payment (€2.50 per item) to a maximum of €25 per family per month [9]. Those not eligible to receive a medical card must pay for primary care following each visit. In addition, the two jurisdictions differ in their stage of adopting a national ageing strategy and implementation of integrated health and social care [6, 7].

The GP practice manager will conduct a search employing the study eligibility criteria on the practice’s electronic health record system to identify potential study participants. Eligible patients will be sent a letter from their GP informing them about the project and inviting them to complete the PRISMA 7 questionnaire. This is a seven-item screening questionnaire that includes items related to age, gender, mobility, need for assistance in activities of daily living and the availability of informal support [10]. It identifies frailty, is suitable for postal completion and is considered a best-practice tool recommended by NHS England to case find at-risk patients for frailty in general practice. Individuals who obtain a score of > 3 are identified as being at risk of functional decline [11, 12]. If patients do not respond to an initial invitation letter, one follow-up reminder will be mailed 7 to 10 days later.

The study methodology is designed to identify individuals who will screen as at risk of functional decline. Initially, patients who screen as ‘at risk’ would receive a letter from their GP inviting them to participate in the study. Patients who reply that they agree to be contacted will be telephoned by a research assistant, who would seek their consent by telephone. Allocation to the intervention versus the usual care group will be communicated to the study participant by a member of the research team after consent has been obtained and the baseline-standardised interview completed. If more than one eligible participants is identified in any one household, all will be eligible for enrolment into the study and, if enrolled, would receive the same study allocation. Following consent, study nurses will commence arrangements to visit the study participants in the intervention group. Changes to enrolment procedures in the RoI were made in response to ethical review in that jurisdiction. These changes related to patient screening and require patients who meet the study inclusion criteria to be assessed for risk of functional decline through a three-step process: (1) GP staff generate a pseudonymised list of potential participants via the GP electronic health record system search, identifying candidates who have two or more chronic medical conditions; four or more regular prescribed medications and, the availability of an informal caregiver if recorded; (2) identified candidates will be reviewed by their own GP to confirm suitability for inclusion in the study; and, (3) eligible patients will then be sent a letter from their GP providing information about the study and inviting them to complete the PRISMA 7 questionnaire that will also include a ‘consent to be contacted’ statement. Patients who do not respond to the initial GP’s letter may be contacted using the same methodology on one additional occasion. If there is no response at this stage, they will not be contacted again. Patients return the completed pseudonymised PRISMA 7 to the research team which will then score it. The research team will then send the GP practice staff the unique code assigned to the completed PRISMA 7 questionnaire. These staff members will link the patient’s name, telephone number and address to the assigned code. Patients who do not screen as ‘at risk’ on the basis of their answers on the PRISMA 7 questionnaire will receive a letter from the GP explaining that they do not meet the criteria to participate in the study and thanking them for their time. The GP practice manager will provide the research team with the name and telephone number of patients who do screen as at risk and have consented to be contacted by them. A member of the research team will then telephone the patient to discuss the study and answer any questions that they have. If a patient is interested in participating in the study, the researcher will arrange to meet with them to complete the written informed consent process and administer baseline questionnaires.

A total of 64 patients (32 per randomised group) will be enrolled into the study. This will comprise eight patients per GP practice, and random selection will be used if more than eight patients are available in a practice. This size of sample is recommended to allow the standard deviation (SD) of the continuous outcome EuroQol 5-dimension, 5-level health survey (EQ-5D-5 L) [13] to be determined at a sufficient level of accuracy while minimising the number of patients required in the pilot [14, 15].

The framework for this intervention comprises personalised care and support planning. To ensure a personalised care approach in the ACP intervention, registered nurses from both jurisdictions complete a training programme that was designed to orientate the nurses to the intervention and study procedures. This training lasts for 3 days and is facilitated by a clinician who is acknowledged as an expert in the field. It covered a range of topics including: an overview of the study; principles and practice of personalised care; shared-decision-making; conducting a holistic assessment using the Easy-Care Assessment instrument [16]; and, completing a medication review facilitated by a clinical pharmacist.

Patients in the usual care group will not receive the ACP intervention but will receive usual care from their GP. The PRISMA 7 score and the explanation of this score will not be shared with the GP in this group. Usual care comprises the following: patients seeking appointments with their GPs to discuss presenting complaints as these arise, if any. Given the range and complexity of potential presenting issues, an exhaustive account is not provided here. This comparator is, therefore, usually reactive, rather than anticipatory. However, some care episodes will be initiated by the GP, e.g. a reminder for the influenza vaccine, chronic care delivery for certain chronic conditions such as diabetes, reminders regarding need for monitoring bloods for certain medical conditions/medications. GPs fulfil a gatekeeper role to secondary care, and access to care is free for older patients who have a medical card in the RoI. Similar to participants in the intervention group, usual care participants will complete study questionnaires with the help of a research assistant at baseline, 10 weeks and 6 months following enrolment.

There is no anticipated harm or compensation for trial participation.

Data will be expressed as a mean, SD or median and for continuous variables and count (percent) for categorical variables. The analysis of indicators will be based on descriptive statistics reported as estimates with confidence intervals. Outcome analyses will be conducted to compare the intervention and control groups, recognising that this analysis will be underpowered for a robust statistical analysis. Means and SD will be reported for each combination of baseline and final data. Frequency and percentage will be reported in the same manner for categorical variables. The SD of the difference in primary outcome (EuroQol EQ-5D-5 L at 6 months) will be determined and the intra-cluster correlation of this difference will be estimated to inform the sample size required for the definitive trial. Recruitment and retention rates at 6 months will also be used to inform the sample size calculation. We will also consider acceptability of the mode and timing of the administration of impact measures. Incremental cost-effectiveness and cost-utility analyses will be conducted for the purposes of the economic evaluation. All quantitative analysis will be conducted in a manner consistent with guidelines for the analysis of data from cRCTs. The data analyst will be blinded for all primary and secondary quantitative outcome analysis, with the exception of the health economics analysis. All participants will be analysed according to the intention-to-treat (ITT) principle. The primary analysis will be a complete case analysis and a sensitivity analysis will be conducted using multiple imputation to impute missing values. A Data Monitoring Committee was not considered as this was a low-risk intervention. There are no stopping guidelines as there are no anticipated problems that are detrimental to the participants.

The software package NVivo 10.0 [31] will be used to help organise and analyse the qualitative data. We will analyse interview data following the template analysis style outlined by Miles and Huberman [32] and will develop an open-ended and modifiable codebook. We will use this tool to generate themes, patterns and interrelationships in an interpretive fashion, drawing on the expertise of our research team and our Personal and Public Involvement (PPI) advisors. No blinding for qualitative analysis is possible.