Atherosclerosis Clinical Trial
Official title:
Vascular Effects of Achieving Minimal Disease Activity in Psoriatic Arthritis - a 2 Year Prospective Cohort Study
Objectives To investigate the effect of achieving minimal disease activity (MDA) using a
protocolized treatment strategy on the progression of subclinical atherosclerosis and
arterial stiffness in psoriatic arthritis (PsA) patients.
Hypothesis Effective suppression of inflammation in patients who can achieve MDA will have
less progression of subclinical atherosclerosis and arterial stiffness then patients who
cannot achieve MDA by means of a standardized treatment algorithm aiming at MDA.
Design and subjects One hundred consecutive PsA patients will participate in this 2-year
prospective, hospital-based, cohort study.
Interventions All participants will receive 2-year tight-control treatment. Treatment will be
adjusted according to a standardized protocol based on the European League Against Rheumatism
(EULAR) recommendation and the Hong Kong guideline on the use of biologics every 4-monthly
aiming at MDA.
Study instruments Carotid intima-media thickness (IMT) will be measured using high-resolution
ultrasound. Arterial stiffness is measured using pulse wave velocity (PWV) by a dedicated
tonometry system and augmentation index (AIx) by the SphygmoCor device.
Main outcome measures and analysis The main outcome measure is the change in IMT over a
period of 2 years comparing between patients who achieve MDA at 12 months (MDA group) to
those who cannot achieve MDA (non-MDA group). Secondary outcomes include differences in the
changes in AIx and PWV over 2 years between the 2 groups. Comparisons of the changes in IMT,
AIx and PWV over 2 years between the MDA and non-MDA groups will be performed.
Background:
Patients with psoriatic arthritis (PsA) experience substantial morbidity and unfavorable
outcomes at referral centers. Although studies on all-cause mortality have yielded mixed
results, increased cardiovascular (CV) mortality and morbidity in PsA have been consistently
reported. Data from our group and others have shown that underlying these higher CV disease
(CVD) rates is a greater burden of subclinical carotid atherosclerosis. Increased
intima-media thickness (IMT) significantly correlates with traditional risk factors and
disease-related parameters. An increased prevalence of arterial stiffness has also been
demonstrated in patients with psoriasis and PsA compared with controls. In PsA, criteria for
minimal disease activity (MDA) have been developed and validated. These criteria use 7
measurements including entheseal and skin assessments. Achieving MDA by these criteria
results in less radiographic damage in the long term. The development of this instrument is a
step toward 'treatment to target' in PsA. MDA is achieved in 48-60% of patients at ≥ 1 visit,
and is sustained for ≥ 12 months (sustained MDA) in at least one third of PsA patients in a
large observational cohort.
While achieving MDA may result in significant benefits in articular disease, little is known
about its effect on extra-articular disease, including CVD risk. The use of surrogate end
points instead of actual CV events may provide more evidence on whether PsA patients may
benefit from potent anti-inflammatory treatment on the prevention of premature
atherosclerosis. Data from our group and others linked the suppression of inflammation using
anti-tumour necrosis factor (anti-TNF) with a favourable effect on CV surrogate makers,
including carotid IMT and arterial stiffness. More recently, a tight-control treatment
strategy aiming at remission was effective in improving arterial stiffness in our early
rheumatoid arthritis (RA) cohort. There is an imperative need for interventional trials with
CV end points to investigate whether achievement of MDA by a protocolized treatment strategy
could reduce CVD risk in PsA. To fill in these gaps of knowledge, we propose a prospective
cohort study to ascertain whether achieving MDA through a protocolized treatment strategy may
prevent long term progression of IMT and arterial stiffness to a greater extent than those
who cannot achieve MDA in patients with PsA.
Aim of the study:
Primary outcome:
1. Effect of achieving MDA (MDA group) at 12 months on the progression of subclinical
atherosclerosis over a period of 24 months as evaluated by IMT compared to those who cannot
achieve MDA (non-MDA group)
Secondary outcomes:
1. Changes in arterial stiffness over a period of 24 months as evaluated by pulse wave
velocity (PWV) and augmentation Index (AIx) between the MDA group and non-MDA group.
2. The proportion of patients achieving sustained MDA (from 12 to 24 months)
3. Changes in IMT and arterial stiffness over a period of 24 months as evaluated by IMT,
PWV and AIx between patients who can achieve sustained MDA and those who cannot achieve
sustained MDA.
4. Correlations between the changes in IMT, PWV, and AIX and the changes in markers of
disease activity
Hypothesis:
Effective suppression of inflammation in PsA patients who can achieve MDA will have less
progression of subclinical atherosclerosis and arterial stiffness than patients who cannot
achieve MDA by means of a protocolized treatment algorithm
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