Spondyloarthritis Clinical Trial
Official title:
Prospective, International, Multi-centre Study on ASAS Classification Criteria for SpA
Background:
Existing criteria for AS/SpA such as mod. New York, ESSG, or Amor criteria for
classification and/or diagnosis of spondyloarthritis have limitations when applied to early
disease. Moreover, MRI is not part of any of the established criteria and the precise role
of MRI in early axial disease has not been fully defined yet. Even less is known about
sacroiliac (SI) changes in SpA patients with peripheral symptoms. A pilot study using data
from 'paper patients' led to new candidate criteria for early spondyloarthritis.
Subsequently, the members of the ASAS International Working Group decided to conduct a
prospective multi-centre study to evaluate (validate) the new candidate criteria, and to
assess their performance as diagnostic criteria.
Aims of the study:
1. To evaluate the new candidate criteria for axial SpA in a multi-centre setting.
2. To assess the potential role of the new candidate criteria to be used as diagnostic
criteria. To accomplish this, inclusion of consecutive and undiagnosed patients is
mandatory as are longer periods of follow-up .
3. To compare criteria encompassing the whole group of SpA such as ESSG and Amor criteria
against criteria which are tailored to either predominant axial disease or predominant
peripheral disease. To accomplish this, both patients with predominant axial disease
(back pain) but also patient with predominant peripheral disease (arthritis/enthesitis)
will be included.
Background:
Existing criteria for AS/SpA such as mod. New York, ESSG, or Amor criteria for
classification and/or diagnosis of spondyloarthritis have limitations when applied to early
disease. Moreover, MRI is not part of any of the established criteria and the precise role
of MRI in early axial disease has not been fully defined yet. Even less is known about
sacroiliac (SI) changes in SpA patients with peripheral symptoms. A pilot study using data
from 'paper patients' led to new candidate criteria for early spondyloarthritis.
Subsequently, the members of the ASAS International Working Group decided to conduct a
prospective multi-centre study to evaluate (validate) the new candidate criteria, and to
assess their performance as diagnostic criteria.
Aims of the study:
1. To evaluate the new candidate criteria for axial SpA in a multi-centre setting.
2. To assess the potential role of the new candidate criteria to be used as diagnostic
criteria. To accomplish this, inclusion of consecutive and undiagnosed patients is
mandatory as are longer periods of follow-up .
3. To compare criteria encompassing the whole group of SpA such as ESSG and Amor criteria
against criteria which are tailored to either predominant axial disease or predominant
peripheral disease. To accomplish this, both patients with predominant axial disease
(back pain) but also patient with predominant peripheral disease (arthritis/enthesitis)
will be included.
Participating centres:
All ASAS members working in clinical practice are invited to participate in the study. More
than one ASAS member/ rheumatologist per centre may participate.
Inclusion criteria:
Include newly referred patients if
- onset of symptoms (back pain / arthritis / enthesitis) < 45 years and
- undiagnosed* disease with the following symptoms:
- chronic back pain (duration of back pain more than 3 months)
- or / and peripheral arthritis (asymmetric arthritis / predominantly of the lower
limbs)
- or / and enthesitis
- or / and dactylitis
- Definition of 'undiagnosed':
The patient is being referred to your department because of chronic back pain, arthritis,
enthesitis or dactylitis but has not been diagnosed confidently before by the referring
physician/rheumatologist as having SpA or as definitely not having SpA. If the referring
physician/GP/rheumatologist suspects SpA but is not certain about it, the patient is
considered as undiagnosed.
Endpoints of the study:
- Primary endpoint: the diagnosis made by the rheumatologist (ASAS member) after the
diagnostic work-up. This expert diagnosis serves as preliminary gold standard against
which the various criteria will be compared. Final gold standard will be the outcome
(diagnosis) after long-term follow up.
- Secondary endpoints: the diagnosis made by the rheumatologist at 2 and 5 years,
respectively, after the first assessment. Thus, all patients should be invited to
follow-up visits after 2 and 5 years, respectively.
Further study rules:
- Include all newly referred patients strictly consecutively as long as they meet the
inclusion criteria.
- The decision to include a patient should be based solely on the fulfilment of the
inclusion criteria, and should be made ideally before you make the final diagnosis
(prospective study design).
- Patients who have been diagnosed confidently and correctly by the referring physician
prior to being referred to your department cannot be included in the study.
- If you are unable to perform MRIs in your clinical setting you cannot include patients
with undiagnosed chronic back pain.
- If you want to include patients with undiagnosed chronic back pain, perform MRI of
sacroiliac (SI) joints in the first 10 patients with axial SpA and in the first 10
patients with non-SpA related (mechanical) back pain. In subsequent patients you may
perform MRIs as needed on clinical grounds. (Explanation: a minimum number of MRIs in
both SpA and non-SpA patients from several centres is necessary to obtain reliable
results on sensitivity and specificity of MRI in early axial SpA.)
- MRI of SI joints in patients with peripheral symptoms only will be performed in
selected centres (centres already indicated whether this will be possible).
- MRI results will be taken as provided by the local centre (either read by the
radiologist or rheumatologist, whoever has greater experience). Results will be
categorized into 'presence or absence of active inflammatory lesions compatible with
SpA', and 'presence or absence of chronic lesions compatible with
sacroiliitis/spondylitis'. (Selected centres will be invited to send us their MRIs for
validation of locally performed readings (the intention is to increase the quality of
data).
- Plain radiographs of the SI joints and lumbar spine are mandatory in all patients with
undiagnosed chronic back pain. Previously taken radiographs are acceptable if they are
not older than 6 months. Results are taken as provided locally either by the
radiologist or rheumatologist, whoever has greater experience.
- At the end of the diagnostic work up, a preliminary diagnosis must be made by the ASAS
rheumatologist as is done in usual daily clinics. It is not important to be absolutely
confident about the diagnosis at this stage since this i) reflects daily practice, and
ii) the level of confidence with the diagnosis will be assessed as well. (It is more
important to include all patients consecutively in your centre in order to avoid any
selection bias.) The senior ASAS member should supervise other physicians experienced
in SpA in her/his department who participate in the study.
- Patients with peripheral symptoms should be included if they meet the inclusion
criteria. Patients with peripheral symptoms and a history of chronic back pain or with
concomitant chronic back pain must undergo radiographic examination of the SI joints.
Patients with non-specific musculoskeletal pain or arthralgia (without arthritis) only
cannot be included.
Data documentation:
The results of the clinical history, physical examination, blood tests, radiographs, and
MRIs, and the diagnosis will be entered into the CRF locally by the ASAS member during/after
the diagnostic work-up. The diagnosis will be made by the local rheumatologist (ASAS member
or an experienced colleague at the centre). The completed CRF should be sent to the
coordinating centre (Berlin) for data check and data entry. A copy of the CRF should remain
locally at the study centre. The name, date of birth, address, and telephone number must
also be kept locally in the centre since follow-up assessments after 2 years and after 5
years are planned.
Sample size and inclusion period:
It is estimated that about 400-500 patients with SpA (ca 250-300 axial and 150-200
peripheral SpA) with complete data sets are needed to allow for a reliable comparison of new
candidate criteria with established criteria. Since the prevalence of SpA among newly
referred patients with unclear diagnoses varies from centre to centre any calculation of the
control group size (and thus total sample size) is bound to be inaccurate. Therefore, the
proposal is that each centre recruits as many consecutive patients as possible until
indicated by the study coordinators to stop inclusion. The study coordinators can adequately
terminate the inclusion period only if the completed CRFs are sent within a reasonably short
period of time (< 2 weeks) to the coordinating centre. Data entry and data analysis will be
done at the coordinating centre.
DNA/RNA-analysis and biomarker analysis:
In addition to the clinical study which aims to arrive at new classification and diagnostic
criteria, two groups of researches will perform laboratory experiments in patients from
selected centres: Genetic polymorphisms and gene products (RNA) which are potentially
associated with spondyloarthritis will be analysed by Prof. Matthew Brown in Brisbane,
Australia. A second group of researchers (Prof. Walter Maksymowych, Canada, Prof. Mikkel
Ostergaard, Denmark, Prof. Rob Inman, US, and Prof. David Yu, US) will analyse several
biomarkers such as cartilage break-down or bone formation proteins in serum and/or plasma.
Data from both experimental projects may be of potential diagnostic value in the future
and/or may reveal novel insights into pathophysiological mechanisms of spondyloarthritis.
Longterm follow-up:
A second follow-up visit of all patients 2 years after the first encounter and also 5 years
after the first encounter is highly warranted since diagnoses may change over time and the
final diagnosis after long-term follow up is the most important gold standard. Thus, a
record containing the names, addresses, and phone numbers of all patients included in the
study must be stored locally at the study site. The patient is best informed at the first
visit that a follow-up assessments 2 and 5 years later are envisaged.
;
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