Dementia Clinical Trial
Official title:
A Longitudinal Assessment of Cognitive Impairment in Advanced CKD Transitioning Into Renal Replacement Therapy
Patients with failed kidneys need Renal Replacement Therapy (RRT) to remove fluid and toxins
from the body. The 3 types of RRT are kidney transplant or removal of waste by dialysis,
either via the blood (haemodialysis) or via the stomach area (peritoneal dialysis). 27,000
patients currently receive dialysis in the UK and some endure reduced quality-of-life,
depression, and thinking and memory difficulties. Some of these symptoms reflect undiagnosed
dementia. Indeed up to 7/10 dialysis patients suffer moderate to severe brain impairment or
dementia - much more frequently than in the general population.
This study will assess brain function just before starting dialysis/transplant and at 3 and
12 months afterwards with face to face assessments and with brain scans in some patients.
Changes in brain function will be compared between people treated with the different forms of
dialysis and transplant.
The Investigators hope to evaluate whether these tests are acceptable to patients, whether
affected sub-groups with cognitive impairment can be identified early, and if certain
dialysis methods are better for patients with cognitive impairment/dementia, so that a larger
study to try to improve brain function after RRT can be developed.
Aims of the proposed research
Primary Objective:
To test the feasibility of performing serial detailed neurocognitive assessments in patients
before during and after the period of commencing RRT for End-Stage Kidney Disease
Secondary Objectives:
1. Estimate cross-sectional and longitudinal variability in a novel battery of
neurocognitive assessments amongst participants in transition to all 3 modalities of
RRT.
2. Assess the administration, suitability and adherence of the chosen cognitive and quality
of life measures in participants.
3. Test the feasibility of recruitment to a longitudinal brain magnetic resonance imaging
(MRI) study in a randomly selected proportion of participants.
4. Estimate the cross-sectional and longitudinal variability in multiparametric brain MRI
parameters and their interaction with cognitive functional change in this transitional
population.
5. To describe resource implications including patients referred to specialist services due
to new diagnoses of cognitive impairment, dementia and/or depression
Study Design
This is a prospective study of 96 patients who are about to commence renal replacement
therapy (RRT). Patients will undergo a neurocognitive, depression and quality of life
assessments at baseline, 3 months after commencing RRT and 12 months after commencing RRT. A
nested cohort of 25% will undergo MR brain scans at baseline and at 12 months.
Detailed Plan of Investigation
Recruitment procedure The target population is clinic based patients with advanced CKD who
are due to commence RRT in the next 1-2 months as determined by the treating clinician.
Patient screening, information giving and consenting for this feasibility study will be
performed in the low clearance clinic at Salford (held twice per week). Enrolment of willing
and eligible patients who are admitted into hospital to start RRT in the absence of infection
and delirium may also be assessed.
Study Protocol Overall feasibility of the study will be assessed based on recruitment rates
of eligible patients as well as consent rates, withdrawal rates, missing data and study
costs. This data is also relevant to assess the feasibility of performing brain MR scans in
this cohort. In addition, factors which may impact on cognitive function, such as age,
gender, education, ethnicity and socioeconomic status, will be assessed at baseline to better
inform future trial design.
Participants will undergo testing of all measures (except imaging) at baseline, 3 months
after starting renal replacement therapy (RRT+3) and after 12 months (RRT+12). Baseline is
defined as any participant whose eGFR is <15mls/min/1.73m2 and is expected to need to start
renal replacement therapy within 2 months. An opportunistic sampling technique will be used.
The research fellow will engage in multidisciplinary meetings that follow the low clearance
clinics and will use these to identify potential participants, participants will then be
contacted and if they demonstrate potential willingness to participate then will be sent the
participant information sheet. Consent will then be taken and if the participant is expected
to start RRT within 2 months then baseline assessments will occur at next clinic appointment.
Where participants transfer from one modality of dialysis to another the participants will be
assigned to the modality of dialysis most frequently undertaken in the 3 months prior to
testing. Assessment will be delayed when there has been a modality switch within the last 1
month of assessment date. Where a participant has received a renal transplant after
commencing dialysis cognitive assessment will occur as near to the 3 and 12-month time point
as possible. Where a participant receives a pre-emptive transplant (prior to any dialysis)
then cognitive assessments will occur at 3 and 12 months post-transplant date.
Cognition Cognitive assessments will be performed by the research fellow in a quiet clinical
room with refreshments made available to the participants. This methodology has been used
previously. Family members or carers will not be present. The assessments may last up to 2
hours. The assessments will usually follow clinic appointments to minimise participant
inconvenience. Due to fluctuations in cognition in the weekly haemodialysis cycle. Cognitive
assessments will occur on non-dialysis days in participants undergoing haemodialysis. There
are no known treatment related fluctuations in cognition in peritoneal dialysis and these
participants will be assessed before or after routine clinic appointments. The neurocognitive
tests will be a combination of previously used and validated tests (below) and specifically
designed assessments by Professor Montaldi at University of Manchester. They will be designed
to detect the expected defects in cognitive domains that are known to be present in CKD and
dialysis patients. It will be probe into these defects with more thoroughness and sensitivity
than has been undertaken in previous studies.
The MoCA is a one-page 30-point screening test of global cognitive function taking
approximately 10 minutes to administer. There are 3 alternate forms in English designed to
minimize practice effects in longitudinal studies. The MoCA will be used in this study
primarily to allow comparison with the results of other studies in RRT. It will also permit
the first longitudinal validation of the MoCA in the target group against our detailed
neurocognitive battery.
The main standardised neurocognitive tests will include:
- IQ (WASI);
- Memory (Weschler Memory Scale, Doors and People, Rey Figure) subtests;
- Speed of processing, attention (TEA) and executive function subtests (Hayling and
Brixton).
Detection of more subtle memory changes over time will be explored using a similar foils test
designed by Montaldi and colleagues and used in an older population The neurocognitive
battery will be especially optimised to avoid potential practice effects.
Anxiety and Depression There are complex interactions between anxiety, depression and
cognition. This has also been demonstrated in a cohort of haemodialysis patients. The
hospital anxiety and depression scale will be used to measure this confounding variable. It
has been used in a similar fashion in other studies of similar patient populations. It takes
the form of a questionnaire and takes 2-5 minutes to complete. A systematic review of this
tool identified that a score of 8/21 was optimal for the balancing sensitivity and
specificity of an accurate depression and anxiety diagnosis. Participants with newly
diagnosed severe anxiety or depression will be referred onwards to our renal psychology teams
and local mental health care providers as appropriate.
Quality of life Quality of life (QOL) is an important output of healthcare analyses with
quality of life factoring into patient decisions on RRT modality choices. A meta analyses of
healthcare related quality of life demonstrated that in-centre haemodialysis patients
suffered most. However most studies are cross sectional and subject to ascertainment bias.
This study will use KDQOL-36TM questionnaire. This is a purposely designed QOL instrument for
patients on dialysis. Relevant questions will be used at month 0 and the whole instrument
will be applied at month RRT+3 and RRT+12.
Magnetic Resonance brain imaging Clinicians need to identify which patients are susceptible
to cognitive changes in the future. Similarly, our renal service user group identified
dementia risk as a key patient concern. Neuroimaging at baseline will identify those with
changes indicative of vulnerability to cognitive decline. Longitudinal MR changes will
provide insight into mechanistic aetiology and will help clarify the link between brain
structure and function.
The Investigators will use a state-of the art dementia imaging protocol in a randomly
selected group of 25% participants. This protocol has been developed by Dr Parkes and others
as part of the Dementia Platforms UK Imaging network. This includes measures of gross
morphological structure from high resolution T1-weighted images, microstructural change from
diffusion-weighted imaging and markers of microvascular disease from T2-weighted FLAIR
imaging (to quantify white matter lesion volume), susceptibility-weighted imaging (to
visualise microbleeds) and arterial spin labelling (ASL) (for cerebral blood flow images).
These quantitative imaging measurements will provide insight into the mechanisms by which
kidney disease impacts cognition, and may allow prediction of the progression of such
impairment. In particular, ASL (a technique in which Dr Parkes is internationally renowned),
will provide information on the metabolic state of the brain which may be altered in kidney
disease. Advanced diffusion-weighted imaging will also provide a sensitive indicator of loss
of neural density/structure. The imaging protocol will last for 45 minutes and studies will
be carried out in the MR imaging facilities at Central Manchester University Hospital, using
exactly the same protocol. MR imaging will be performed twice in each of these participants -
first prior to commencement of RRT and within 1 month of the baseline cognitive assessment
and then within1 month of the RRT +12 assessment
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