The rationale for this study is to use immune molecule-specific drug treatment to leverage a mechanistic understanding of the brain changes that drive sickness behaviour. This will combine current therapy with innovative neuroimaging technologies to obtain data in humans that has hitherto only been available in animal studies. Data supporting the role of inflammatory molecules in sickness behaviours and other cognitive disorders are increasingly compelling. A putative mechanism linking inflammatory proteins to sickness behaviour is Tumour Necrosis Factor (TNF)-driven increases in extracellular glutamate leading to changes in neural function and brain network integrity and ultimately to sickness behaviour. Investigators hypothesise that TNF antagonism will effect changes in brain network connectivity and sickness behaviour score, that Rheumatoid Arthritis (RA) patients will show changes in brain network connectivity and glutamate quantification in the brain and that RA patients will show changes in monocyte infiltration into the brain that are correlated with changes in sickness behaviours. This is a randomised, placebo-controlled waiting list study. All patients will be eligible for anti-TNF treatment i.e. moderate to severe active disease as defined by Physician. Participants will be randomised to immediate (fast tracked) treatment or to treatment after 6-8 weeks (the routine waiting time). The latter group will receive placebo during the treatment phase.
The study will involve participants aged over 18 years with RA and are scheduled to start outpatient anti-TNF treatment (with Adalimumab) as part of standard clinical care, who meet the inclusion criteria and none of the specified exclusion criteria. All will give full informed consent. This is a single-blind, randomised placebo-controlled waiting list study and after screening and consent, eligible participants will be randomised (1:1) to receive either adalimumab or placebo. The study comprises standard care screening for anti-TNF therapy (incorporated into the study to allow us to fast track screening), a total of 7 research visits and one remote visit via telephone. At Visit 1 (Day 0) and Visit 4 ((14 ± 2 days from Visit 3), participants will undergo 7T MRI and MRS Neuroimaging protocols that incorporate resting-state and task-based fMRI and glutamate MRS measures. At Visit 1A (1 - 7 days from Visit 1) and Visit 4A (1 - 7 days from Visit 4), participants will undergo an optional SPECT scanning protocol. This visit will involve a 160ml blood draw, from which monocytes will be isolated and radiolabelled before being reinjected prior to SPECT scanning.
Study Type
INTERVENTIONAL
Allocation
RANDOMIZED
Purpose
BASIC_SCIENCE
Masking
SINGLE
Enrollment
46
Adalimumab 40mg, will be administered as a subcutaneous injection once fortnightly on four occasions. The actual Adalimumab product selected at site will be dictated by what is used in standard care.
Sodium chloride 0.9% for injection will be used as a placebo. An equal volume will be drawn up into a suitable sized syringe and labelled in accordance with standard practice at site. The dose will be administered as a subcutaneous injection once fortnightly on four occasions.
Addenbrooks Hopsital
Cambridge, United Kingdom
Neil Basu
Glasgow, United Kingdom
Change in sickness score as measured using the sickness questionnaire
The sickness questionnaire is a 10-item instrument used to capture perceived sickness behaviour. It was developed to display sensitivity to an inflammatory challenge and have adequate psychometric properties.
Time frame: Visit 1 (Baseline, Day 0), Visit 2 (14 ± 2 days from Visit 1 or Visit 1A), Visit 3 (14 ± 2 days from Visit 2), and Visit 4 (14 ± 2 days from Visit 3).
Change in brain connectivity as measured by 7T MRI
Changes in dorsal attention network (DAN) - left inferior parietal lobule (LIPL) brain connectivity as measured by 7T MRI
Time frame: Visit 1 (Baseline, Day 0) and Visit 4 (14 ± 2 days from Visit 3).
Changes in fatigue from Baseline to Visit 4 via BRAF Severity
Fatigue, measured by BRAF severity
Time frame: Visit 1 (Baseline, Day 0), Visit 2 (14 ± 2 days from Visit 1 or Visit 1A), Visit 3 (14 ± 2 days from Visit 2), and Visit 4 (14 ± 2 days from Visit 3).
Changes in fatigue from Baseline to Visit 4 via PROMIS Fatigue
Fatigue, measured by PROMIS-Fatigue.
Time frame: Visit 1 (Baseline, Day 0), Visit 2 (14 ± 2 days from Visit 1 or Visit 1A), Visit 3 (14 ± 2 days from Visit 2), and Visit 4 (14 ± 2 days from Visit 3).
Changes in Hyperalgesia from Baseline to Visit 4 via ACR-FM Scale
Hyperalgesia, measured by the ACR-FM Scale (American College of Rheumatology Fibromyalgia Scale).
Time frame: Visit 1 (Baseline, Day 0), Visit 2 (14 ± 2 days from Visit 1 or Visit 1A), Visit 3 (14 ± 2 days from Visit 2), and Visit 4 (14 ± 2 days from Visit 3).
Changes in pain from Baseline to Visit 4 via McGill Pain Questionnaire
Pain, measured by McGill Pain Questionnaire
Time frame: Visit 1 (Baseline, Day 0), Visit 2 (14 ± 2 days from Visit 1 or Visit 1A), Visit 3 (14 ± 2 days from Visit 2), and Visit 4 (14 ± 2 days from Visit 3).
Changes in pain from Baseline to Visit 4 via Michigan Body Map Regional Pain Intensity
Pain, measured by Michigan Body Map Regional Pain Intensity.
Time frame: Visit 1 (Baseline, Day 0), Visit 2 (14 ± 2 days from Visit 1 or Visit 1A), Visit 3 (14 ± 2 days from Visit 2), and Visit 4 (14 ± 2 days from Visit 3).
Changes in pain from Baseline to Visit 4 via Finger Perception Task
Pain, measured by Finger Perception Task.
Time frame: Visit 1 (Baseline, Day 0), Visit 2 (14 ± 2 days from Visit 1 or Visit 1A), Visit 3 (14 ± 2 days from Visit 2), and Visit 4 (14 ± 2 days from Visit 3).
Changes in pain from Baseline to Visit 4 via Neglect-like Symptoms Questionnaire.
Pain, measured by Neglect-like Symptoms Questionnaire.
Time frame: Visit 1 (Baseline, Day 0), Visit 2 (14 ± 2 days from Visit 1 or Visit 1A), Visit 3 (14 ± 2 days from Visit 2), and Visit 4 (14 ± 2 days from Visit 3).
Changes in pain from Baseline to Visit 4 via Number Rating Scale - Pain
Pain, measured by Number Rating Scale - Pain.
Time frame: Visit 1 (Baseline, Day 0), Visit 2 (14 ± 2 days from Visit 1 or Visit 1A), Visit 3 (14 ± 2 days from Visit 2), and Visit 4 (14 ± 2 days from Visit 3).
Changes in sleep disturbance from Baseline to Visit 4
Sleep disturbance, measured by PROMIS-Sleep related impairment.
Time frame: Visit 1 (Baseline, Day 0), Visit 2 (14 ± 2 days from Visit 1 or Visit 1A), Visit 3 (14 ± 2 days from Visit 2), and Visit 4 (14 ± 2 days from Visit 3).
Changes in mood from Baseline to Visit 4 via HADS
Mood, measured by HADS (Hospital Anxiety Depression Scale).
Time frame: Visit 1 (Baseline, Day 0), Visit 2 (14 ± 2 days from Visit 1 or Visit 1A), Visit 3 (14 ± 2 days from Visit 2), and Visit 4 (14 ± 2 days from Visit 3).
Changes in mood from Baseline to Visit 4 via PROMIS-Depression
Mood, measured by PROMIS-Depression
Time frame: Visit 1 (Baseline, Day 0), Visit 2 (14 ± 2 days from Visit 1 or Visit 1A), Visit 3 (14 ± 2 days from Visit 2), and Visit 4 (14 ± 2 days from Visit 3).
Changes in mood from Baseline to Visit 4 via PROMIS-Anxiety
Mood, measured by PROMIS-Anxiety.
Time frame: Visit 1 (Baseline, Day 0), Visit 2 (14 ± 2 days from Visit 1 or Visit 1A), Visit 3 (14 ± 2 days from Visit 2), and Visit 4 (14 ± 2 days from Visit 3).
Changes in cognition from Baseline to Visit 4
Cognition, measured by Cognitive failures questionnaire.
Time frame: Visit 1 (Baseline, Day 0), Visit 2 (14 ± 2 days from Visit 1 or Visit 1A), Visit 3 (14 ± 2 days from Visit 2), and Visit 4 (14 ± 2 days from Visit 3).
Changes in processing speed from Baseline to Visit 4
Processing Speed, measured by Symbol Digit Modalities Test.
Time frame: Visit 1 (Baseline, Day 0), Visit 2 (14 ± 2 days from Visit 1 or Visit 1A), Visit 3 (14 ± 2 days from Visit 2), and Visit 4 (14 ± 2 days from Visit 3).
Changes in memory from Baseline to Visit 4
Memory, measured by Auditory Verbal Learning Test.
Time frame: Visit 1 (Baseline, Day 0), Visit 2 (14 ± 2 days from Visit 1 or Visit 1A), Visit 3 (14 ± 2 days from Visit 2), and Visit 4 (14 ± 2 days from Visit 3).
Changes in verbal fluency from Baseline to Visit 4
Memory, measured by Auditory Verbal Learning Test.
Time frame: Visit 1 (Baseline, Day 0), Visit 2 (14 ± 2 days from Visit 1 or Visit 1A), Visit 3 (14 ± 2 days from Visit 2), and Visit 4 (14 ± 2 days from Visit 3).
Change in brain network connectivity at Baseline and Visit 4
Change in brain network connectivity as measured by 7T Magnetic Resonance Imaging (MRI).
Time frame: Visit 1 (Baseline, Day 0) and Visit 4 (14 ± 2 days from Visit 3).
Change in brain glutamate quantification at Baseline and Visit 4
Change in brain glutamate quantification as measured by 7T Magnetic Resonance Spectroscopy (MRS).
Time frame: Visit 1 (Baseline, Day 0) and Visit 4 (14 ± 2 days from Visit 3).
Measures of RA disease activity from Baseline to Visit 4 via DAS28
Indices of of disease activity for Rheumatoid Arthritis as measured by DAS28 (Disease Activity Score-28).
Time frame: Visit 1 (Baseline, Day 0), Visit 2 (14 ± 2 days from Visit 1 or Visit 1A), Visit 3 (14 ± 2 days from Visit 2), and Visit 4 (14 ± 2 days from Visit 3).
Measures of RA disease activity from Baseline to Visit 4 via CDAI
Indices of of disease activity for Rheumatoid Arthritis as measured by CDAI (Clinical Disease Activity Index).
Time frame: Visit 1 (Baseline, Day 0), Visit 2 (14 ± 2 days from Visit 1 or Visit 1A), Visit 3 (14 ± 2 days from Visit 2), and Visit 4 (14 ± 2 days from Visit 3).
Measures of RA disease activity from Baseline to Visit 4 via SDAI
Indices of of disease activity for Rheumatoid Arthritis as measured by SDAI (Simple Disease Activity Index).
Time frame: Visit 1 (Baseline, Day 0), Visit 2 (14 ± 2 days from Visit 1 or Visit 1A), Visit 3 (14 ± 2 days from Visit 2), and Visit 4 (14 ± 2 days from Visit 3).
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