Spondiloartritis Diagnosis 2017 222234456
Spondiloartritis Diagnosis 2017 222234456
Spondiloartritis Diagnosis 2017 222234456
Spondyloarthritis:
Pathogenesis, clinical
aspects and diagnosis
LEARNING OUTCOMES
Discuss the concept of spondyloarthritis (SpA)
Describe the pathophysiology of these disorders and the role of genetic and environmental factors
Explain the different hypotheses for the role of HLA-B27 in the pathogenesis of these disorders
Explain the approach to the diagnosis of SpA
Improve assessment of patients with SpA, especially disease activity, severity and refractory
characteristics of the disease
Present treatment strategies for patients with ankylosing spondylitis
Describe the use of the different tools allowing better patient monitoring
Spondyloarthritis: Pathogenesis, clinical aspects and diagnosis Module 6
Disease subgroups
Axial SpA including AS
Peripheral SpA
PsA
Reactive arthritis
Inflammatory bowel disease-related arthritis
Juvenile spondyloarthritis
Clinical features
Rheumatological manifestations
o Axial involvement
o Peripheral arthritis
o Enthesopathy
Extra-articular features
o Acute anterior uveitis
o Cardiac involvement (eg, heart block, aortic insufficiency)
Genetic background
o Family history
o HLA-B27 antigen
Specific manifestations
o Psoriasis
o Inflammatory bowel disease, etc
AS, ankylosing spondylitis; PsA, psoriatic arthritis; SpA, spondyloarthritis.
Adapted from Dougados and Hochberg, Best Pract Res Clin Rheumatol 2002;16:495505.
SpA occurs primarily in genetically predisposed individuals, particularly those who are positive for the major
histocompatibility complex (MHC) class I molecule HLA-B27. However, additional environmental factors are
also thought to play a role in its pathogenesis. It can be difficult to differentiate these disorders because their
clinical features may overlap, which is why undifferentiated forms of SpA are also recognised.
The monitoring and treatment of these diseases is related more closely to the clinical presentation than to the
precise diagnosis. The rheumatic manifestations include inflammation of the spine and sacroiliac (SI) joints,
peripheral arthritis and enthesitis (inflammation at the entheses, the sites of attachment of tendons,
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ligaments, fasciae or joint capsules to bone). Enthesitis is the distinguishing pathological feature of SpA. The
extra-articular manifestations of the disease may be similar whatever the SpA subgroup or may be specific to a
SpA subgroup, such as skin lesions in PsA, gut involvement in inflammatory bowel disease-related arthritis and
the oculo-urethro-synovial triangle in classic ReA.
1.1 Subtypes
SpA can present with a wide spectrum of clinical features. Certain features occur more commonly in some
subtypes of SpA. Table 1 shows typical patterns of SpA subtypes. However, symptoms overlap and so it is
possible for any of the principal clinical features to be present in any of the distinct diseases.
AS is the prototype of axial SpA (axSpA). It is characterised by the presence of spinal pain, resulting in
limitation of spinal mobility and radiological evidence of structural changes in the SI joints and the spine.
Nevertheless, other manifestations can also be seen, such as enthesitis (4060%) and/or acute anterior uveitis
(3050%). The disease course of axSpA is highly variable and often characterised by ongoing axial
inflammation and radiographic progression associated with restricted mobility of the spine and decreased
function. Since axSpA usually starts in early adulthood, the lifetime impact of the disease can be considerable,
resulting in stiffness, fatigue, limitation of social activities and participation.
The modified New York criteria (see box 7, section 6.1 Plain radiographs) have been widely accepted in clinical
practice and in clinical trials to classify patients as AS. Although they work well in established disease, they are
limited for capturing the early disease stages. This was the reason why the Assessment of SpA international
Society (ASAS) developed new classification criteria for patients with axSpA and also for those with peripheral
SpA (for further details see boxes 8 and 9, section 7. Classification).
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Psoriasis is a common skin disease among Caucasian subjects (13% prevalence), but uncommon in some
other ethnic groups, such as Afro-Caribbean and Native American populations (00.3%). It affects men and
women equally. About 1020% of patients have associated PsA. Psoriasis usually antedates the appearance of
arthritis, but the onset is simultaneous in 20% of patients, and in up to 15% the arthritis may precede the
onset or diagnosis of psoriasis. The arthritis usually starts between 30 and 50 years of age, but may also begin
in childhood. In most patients, exacerbations and remissions of skin and joint involvement occur with little or
no apparent relationship. Peripheral joint involvement may be polyarticular or oligoarticular. The typical
pattern of joint disease is an asymmetrical distribution with distal interphalangeal involvement and dactylitis.
About 5% present with predominant spondylitis. A few patients present with a mutilating type of disease
affecting the distal interphalangeal joints, called arthritis mutilans. PsA is characterised radiologically by juxta-
articular new bone formation, absence of periarticular osteopenia and relative preservation of the joint space.
It is a chronic erosive disease and treatments are similar to those used in rheumatoid arthritis.
The CASPAR (Classification Criteria for Psoriatic Arthritis) criteria were developed by an international study
group and have a sensitivity of 91% and a specificity of 99% (box 2).
Current psoriasisscore 2
A history of psoriasis (in the absence of current psoriasis)score 1
A family history of psoriasis in a first- or second-degree relative (in the absence of current psoriasis
and history of psoriasis)score 1
Dactylitisscore 1
Juxta-articular new-bone formationscore 1
Rheumatoid factor negativityscore 1
Nail dystrophyscore 1
The patient is considered to have PsA if the sum of the points is 3.
Adapted from Taylor et al, Arthritis Rheum 2006;54:266573.
The SAPHO (Synovitis, Acne, Pustulosis, Hyperostosis, Osteitis) syndrome has been associated by some with
PsA. It is a specific dermatological entity (pustulosis, acneiform skin rash) associated with synovitis of the
anterior chest wall and SI joints, spondylodiscitis, enthesopathy, aseptic osteomyelitis and/or hyperostosis.
Enteropathic arthritis describes the occurrence of inflammatory arthritis in patients with ulcerative colitis or
Crohns disease. The prevalence of arthritis in inflammatory bowel disease (IBD) ranges from 17% to 20%, with
a higher prevalence in Crohns disease.
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The most common manifestation of enteropathic arthritis is inflammation of the knee and ankle joints. The
peripheral arthritis is usually transient, migratory and non-deforming. The inflammatory episodes are generally
self-limiting, often subsiding within 6 weeks, but recurrences are common. Axial involvement and enthesitis
may also be found. In some cases, the arthritis may become chronic and destructive. Intestinal symptoms
usually antedate or coincide with joint manifestations, but arthritis may precede the intestinal symptoms by
years.
ReA describes an episode of aseptic peripheral arthritis that occurs within 1 month of a primary infection
elsewhere in the body, usually a genitourinary infection with Chlamydia trachomatis or enteritis due to Gram-
negative enterobacteria such as Shigella, Salmonella, Yersinia or Campylobacter species. Genitourinary tract
infection with Chlamydia trachomatis is the most commonly recognised initiator of ReA in developed
countries, whereas infections with enterobacteria are the most common triggers in developing parts of the
world (box 3). In about 25% of cases, however, the triggering organism is unknown.
Chlamydia trachomatis
Shigella flexneri
Salmonella spp
Yersinia enterocolitica
Yersinia pseudotuberculosis
Campylobacter fetus jejuni
Clostridium difficile
Intravesical injection of bacilli CalmetteGurin (BCG) to treat bladder cancer
Chlamydia pneumoniae (unconfirmed)
Adapted from Smith et al, Best Pract Res Clin Rheumatol 2006;20:57192.
ReA is typically an acute, asymmetrical oligoarthritis and is often associated with one or more characteristic
extra-articular features, such as ocular inflammation (conjunctivitis or acute iritis), enthesitis, mucocutaneous
lesions, urethritis and, on rare occasions, carditis. Conjunctivitis occurs in one-third of patients, usually at the
same time as arthritis flares, and acute anterior uveitis may occur at some time in about 5% of patients. The
triad of arthritis, conjunctivitis and urethritis is called classic ReA. However, most patients with ReA do not
present with this triad. The average duration of arthritis is 45 months, but two-thirds of patients have mild
musculoskeletal symptoms that persist for more than 1 year. Recurrent attacks are more common in patients
with chlamydia-induced ReA. About 1530% of patients develop chronic or recurrent peripheral arthritis,
sacroiliitis or spondylitis. Most patients with chronic ReA have a positive family history of SpA or are HLA-B27
positive.
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Juvenile-onset SpA usually manifests initially as peripheral arthritis or enthesitis in children aged 812 years,
but onset at younger or older ages has been reported. There is a striking predominance of male subjects,
particularly in the prepubertal stage. Juvenile-onset SpA clinically resembles adult SpA. Nonetheless, there are
a few differences. Oligoarthritis affecting the knee, ankle and/or mid-foot is the typical initial presentation,
and dactylitis is commoner in children. Systemic manifestations such as fever and weight loss occur more often
in children, and enthesitis is prominent early on in the disease course.
The disease pattern often changes throughout childhood, adolescence and adulthood (eg, from monoarthritis
to a more complex form of disease, leading to axial, peripheral and extra-articular manifestations).
There are undifferentiated and differentiated forms of juvenile-onset SpA, which can be classified according to
the International Association for Rheumatology criteria in the enthesitis-related arthritis subgroup. The adult
Amor and European Spondyloarthropathy Study Group criteria have been validated in children and may also
be used. Prognosis seems to be less favourable in juvenile-onset SpA than in adults. Potentially structural
damage at some sites (particularly the feet, hips and spine) may lead to long-term functional impairment.
Nearly 60% of patients have moderate-to-severe limitations 10 years after disease onset. The probability of
remission is only 17% after a disease duration of 5 years.
2 Epidemiology
The estimated prevalence of AS in Caucasian subjects is between 0.5% and 2%. This varies among different
ethnic populations, being higher in white and certain Native American subjects and lower in African American
and Asian subjects. AS is the most prevalent disease of the axSpA. The prevalence of AS parallels that of the
HLA-B27 gene. Eight per cent of the healthy white population is HLA-B27 positive, while 4% of the healthy
African American population is HLA-B27 positive. Ninety-two per cent of the white AS population is HLA-B27
positive, while 50% of the African American AS population is HLA-B27 positive. Sixty per cent of patients with
ReA, PsA and enteropathic spondylitis are HLA-B27 positive, while 25% of patients with undifferentiated SpA
are HLA-B27 positive. The chance of developing AS if one is HLA-B27 positive is 15%, increasing to 1520% for
people with an affected first-degree relative.
AS is more common in male subjects, with the male:female ratio being 2:1 to 3:1. However, in recent cohort
studies, this ratio has been found to be rather equally distributed between genders. The reasons why male
patients seem to progress more frequently than female patients towards development of AS are still unclear.
The mean age of onset of symptoms is 26 years and it can present from late adolescence to 40 years of age.
There is often significant delay in diagnosis, especially in HLA-B27-negative patients. A shorter time to
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diagnosis was observed in patients with inflammatory back pain (IBP) or a positive family history because
clinical suspicion tended to be higher.
3 Pathogenesis
3.1 Genetics
The aetiology of SpA is still largely unknown but is thought to reflect a complex interplay of genetic and
environmental factors. The involvement of genetic factors in determining susceptibility to SpA has long been
suspected owing to frequent familial clustering of cases. The first genetic factor identified was the tissue
antigen HLA-B27. Further genetic studies have led to the discovery of other genes important in disease
susceptibility, including various B27 subtypes as well as non-B27 MHC and non-MHC genes, although it is not
clear how these cause the disease. Studies are still in the early phase but potentially might provide further
insight into disease pathogenesis and translate into future diagnostic and prognostic tools.
The genetic analysis of complex, multifactorial diseases such as SpA is difficult owing to numerous factors. The
model underlying the inheritance of the disease is unknown, although several genes are likely to be involved,
which may be different from patient to patient (genetic heterogeneity). Moreover, the molecular variants of a
gene (alleles) associated with disease susceptibility may be present in healthy subjects, suggesting that
exposure to specific environmental factors is probably required to cause the disease to develop (incomplete
penetrance). Discovering genes through family-based or candidate gene methods has not been successful.
Using high-throughput microarray-based single nucleotide polymorphism (SNP) genotyping techniques has
made it easier to identify genes associated with SpA more rapidly.
Twin studies in AS have shown a monozygotic concordance rate of around 70%. The genetic risk determines
the risk of developing the disease and also the age of onset, clinical disease severity and radiographic severity.
Such high heritability is usually associated with monogenic diseases. However, this is unlikely given the high
prevalence of AS. In addition, there is clear evidence that other genes are involved. Familial studies show that
<50% of the genetic risk is secondary to HLA-B27. First-degree relatives have a 516% risk of developing the
disease, while only 15% of HLA-B27 individuals develop AS, suggesting that other genes and environmental
factors are involved. HLA-B27-positive relatives of patients with AS have recurrence risks that are 5.616 times
greater than in HLA-B27 individuals in the normal population, suggesting that there must be other non-HLA-
B27 genes which are responsible. This is further supported by twin studies, which have shown greater
concordance in monozygotic twins than in HLA-B27 dizygotic twins.
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The hypothesis of genetic susceptibility factors involved in AS was first developed during the years 195060
based on familial aggregation studies. In 1973, the association of HLA-B27 with the development of AS was
reported. Nevertheless, the precise role of B27 in the pathophysiology of the disease remains unknown.
Several lines of evidence recently suggested that HLA-B27 may not behave like other class I molecules: HLA-
B27 heavy chains can form homodimers that do not contain the 2-microglobulin light chain (a phenomenon
also called HLA-B27 misfolding). Such homodimers could mediate, or be the target for a proinflammatory
response. These hypotheses are under investigation.
The MHC consists of about 220 genes, many of which have immunoregulatory functions. Several studies have
looked at non-B27 MHC genes, but to date none have been able to pinpoint specific genes or genetic variants
associated with AS. Studies in this area have been hampered by extensive linkage disequilibrium between loci,
lack of sufficient marker density and small sample sizes.
Recently, two key studies have identified non-MHC genes which are associated with AS. The first study was
carried out by the Wellcome Trust Case Consortium and the Australo-Anglo-American Spondyloarthritis
Consortium (TASC, 2010*). In the former study, 14 500 non-synonymous SNPs (ie, SNPs which change the
amino acid sequence) identified disease association with interleukin 23 receptor (IL-23R) and endoplasmic
reticulum aminopeptidase 1 (ERAP1). IL-23R has also been found to be linked with IBD and PsA. This partially
explains the frequent coexistence of these diseases.
The second study carried out by TASC is a complete genome-wide association study. In addition to confirming
the above, new associations with gene deserts (regions of the genome lacking protein-encoding genes) at
chromosomes 2p15 and 21q22 and genes IL-1R2 and ANTXR2 were discovered. Strong evidence to support
association with the disease has also been demonstrated for the TNFSF15 and TNFR1 genes and a region on
chromosome 16q including the TRADD gene.
3.2 Infections
B27-Tg rats, housed in a probiotic (non-germ free) environment, develop a SpA-like disease. In contrast, when
raised under entirely germ-free conditions, B27-Tg rats do not develop disease. Interestingly, colonisation of
the gastrointestinal tract with normal gut flora, in particular Bacteroides spp, is sufficient to trigger
inflammation.
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The severity of the SpA-like disease developed by B27-Tg rats correlates with HLA-B27 expression.
Several gastrointestinal or genitourinary pathogens have been strongly implicated as triggers of HLA-B27-
associated ReA in humans, including Campylobacter spp, Chlamydia spp, Salmonella spp and Shigella spp (box
2). DNA from these organisms has been found by polymerase chain reaction in synovial cell and fluid samples.
Salmonella, yersinia and shigella lipopolysaccharide have also been found in the joints of patients with ReA.
The presence of bacterial products in the joints provides a potential link between gut infection and joint
inflammation. However, despite being strongly implicated in ReA, the requirement for gut pathogens and gut
inflammation in AS is less clear.
3.3 Inammation
The most common sites of inflammation in AS include the SI joints, entheses, vertebral bodies adjacent to
intervertebral discs, peripheral joint synovium, gastrointestinal tract and the eye. As many of these lesions are
poorly accessible, information on histopathology is limited. In early sacroiliitis, synovitis with myxoid-
appearing bone marrow and subsequent formation of pannus and granulation tissue is seen. Destroyed bone
is eventually replaced and endochondral ossification results in bony ankylosis. Histologically, there is
infiltration of T cells (CD4+ and CD8+) and CD68+ macrophages, proliferation of fibroblasts, and
neovascularisation as well as tumour necrosis factor blocker (TNF) and transforming growth factor mRNA
overexpression.
The synovitis in SpA displays features of other types of inflammatory arthritis, such as increased vascularity
and endothelial cell activation, with increased expression of adhesion molecules and chemotactic factors.
Relevant differences include a tendency towards greater vascularity, greater CD4+ T cell and CD20+ B cell
infiltration and few lymphoid aggregates. While the total numbers of CD68+ macrophages appear to be similar
or slightly lower than the threshold in SpA, macrophages expressing CD163 are increasingly reported. CD163 is
the haemoglobin scavenger receptor and may define a population that produces more proinflammatory TNF
and less IL-10, which could promote a Th1 response. These macrophages can also release soluble CD163,
which may inhibit T cell proliferation and activation. A recent study in a TNF overexpressing mouse model
suggested that mesenchymal stromal cells are the main target activated by TNF signalling. These mice
spontaneously develop an inflammatory disease characterised by Crohn-like arthritis, sacroiliitis, peripheral
arthritis and enteritis (Armaka et al, 2008).
TNF, but also other proinflammatory cytokines, are directly connected with Dickkopf-1, which leads to an
upregulation of Dickkopf-1, a key target gene of TNF and an inhibitor of osteophyte regulators. This process
results in increased new bone formation, which is also the hallmark radiographic sign of AS. Inhibition of TNF
and Dickkopf-1, for example by therapeutic compounds such as TNF blockers, may result in a blockade on
syndesmophyte formation after sufficient suppression of inflammation (see chapter 12, Treatment).
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Enthesitis is a hallmark of SpA and cartilage is one of the major targets of inflammation. Inflammatory lesions
are characterised by soft tissue inflammation and bone marrow infiltration with CD8 and CD4 T cells, B cells,
macrophages and osteoclasts. This is more common at peripheral sites subject to biomechanical stresses and
rich in fibrocartilage containing type II collagen and aggrecan proteoglycan such as at the insertion of the
Achilles tendon into the calcaneum. In the early phase of enthesitis, CD68+ and macrophages (1 month to 1
year of disease) seem to predominate, while abundant lymphocytes tend to be found in established disease.
4 Clinical features
IBP is the first clinical manifestation in 75% of patients with axSpA. Classically, the pain starts in the lumbar
region or at the lumbosacral junction. It is typically a dull pain of insidious onset, becoming persistent after a
few months. The pain worsens with inactivity and improves with exercise and non-steroidal anti-inflammatory
drugs (NSAIDs). Morning stiffness is often prolonged (>30 min) and nocturnal pain may awaken patients from
sleep. With imaging, sacroiliitis or spondylitis is the dominant finding. If there is progression to ankylosis over
time, the inflammatory pain usually lessens but is replaced by relevant functional impairment. Symptoms may
be mild with intermittent flares and remission. An acute onset of pain, worsening symptoms with activity and
radicular pain are more suggestive of a mechanical or degenerative cause, but both pathologies may also occur
in the same patient. Three different sets of criteria with similar sensitivities and specificities have been
proposed (boxes 4, 5 and 6).
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IBP is the one of the main symptoms in SpA, but its value in diagnosis/classification and screening in primary
care has still not been validated. About 5% of patients presenting with chronic back pain have SpA, and IBP has
long been a central criterion in the classification of AS. The sensitivity and specificity of IBP criteria are directly
related to the pre-test probability of the patient having the disease and the stringency of the IBP criteria used.
This is important, since the prevalence of IBP is much higher in rheumatology practices (2550%) than in the
primary care setting (<5%), where the IBP criteria are probably less useful. Another important observation is
that not all patients with axial SpA have IBP. These observations have led to the removal of IBP as the first
entry criterion in the new classification criteria for axSpA.
4.1.2 Ankylosis
One of the major concerns of patients with spondylitis is progression towards ankylosis of the axial skeleton,
which results from ossification of the ligaments and of the costovertebral and sternocostal joints. The first sign
of an abnormal posture is loss of lumbar lordosis, followed by thoracic hyperkyphosis and, in severe cases,
forward stooping of the neck. Spinal movement is restricted in all planes. The restriction of motion may not be
proportionate to the degree of ankylosis because of secondary muscle spasms. It is important to detect these
abnormal features as early as possible, so that physiotherapy or other appropriate treatments can be initiated.
In patients with restricted chest wall motion, airflow measurements are normal, but vital capacity is decreased
and functional residual capacity is increased. Respiratory failure can occur in severe cases. However, ankylosis
in the thoracic and lumbar spine is not necessarily linked to severe physical limitations unless the hip is
affected, in which case bending forward is a major problem. Ankylosis at the cervical level has major physical
consequencesfor example, in driving, as patients cannot turn their head to view cars alongside them.
4.1.3 Fracture
Although SpA is associated with new bone formation at sites of inflammation, spinal osteoporosis is commonly
seen in longstanding SpA, resulting in increased fracture risk (OR = 3.26, 95% CI 1.51 to 7.02). This contributes
to the high prevalence of fractures, which may often occur after very minimal trauma to the rigid, ankylosed
spine (figure 1). The risk of any clinical fracture is increased especially in patients with a history of IBD. One
needs to have a high index of suspicion for the possibility of fracture in patients with SpA who present with
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acute onset of back or neck pain, especially if this follows trauma. Plain radiography is poorly sensitive and CT
or preferably magnetic resonance imaging (MRI) may be needed to make the diagnosis.
Figure 1 (A) Fracture of the lower part of the thoracic spine (12th thoracic vertebra) and also of the lumbar
spine (fourth lumbar vertebra), the latter with an additional aspect of spondylitis and fusion with the third
lumbar vertebra in a patient with longstanding ankylosing spondylitis and osteoporosis. (B) Fracture of the
middle part of the thoracic spine in a patient with ankylosing spondylitis, causing additional hyperkyphosis
to the patient.
A B
Spinal osteoporosis is partly due to the lack of mobility as a consequence of the disease, as well as a result of
proinflammatory cytokines. Assessment of biochemical markers of bone metabolism has shown diminished
bone formation and enhanced bone resorption. Osteoporotic fractures of the thoracic spine contribute to
thoracic kyphosis and increased occiput-to-wall distance. Neurological involvement may rarely result following
atlanto-axial subluxation.
Peripheral arthritis is typically asymmetrical, oligoarticular and involves the lower limbs. Upper limb
involvement is typically associated with PsA. A bilateral symmetrical polyarticular presentation is possible,
which differs from rheumatoid arthritis in that the distal interphalangeal joints are often affected.
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Dactylitis is characteristic of SpA, although not entirely specific. It is not as common in AS but is more typical of
ReA, PsA or undifferentiated SpA. Unlike synovitis, the swelling is not confined to a joint but involves the
whole digit (sausage digit). It is a combination of synovitis, enthesitis, tenosynovitis and soft tissue swelling
(figure 2).
Figure 2 Sausage-like digit (dactylitis). (Source: CRI (Club Rhumatismes et Inflammation, http://www.cri-
net.com).)
4.1.6 Anterior chest wall pain and axial joint involvement (hips and shoulders)
Anterior chest wall pain occurs in about 15% of patients and is usually the result of sternoclavicular,
manubriosternal or sternocostal arthritis. As stated above, this can lead to reduced chest expansion.
Arthritis of the hips and shoulders often occurs early in the first 10 years of the disease and affects a third of
patients. Hip involvement is commonly bilateral. It is important to check for hip and shoulder joint
involvement, as there may be limited range of movement and flexion deformities. Hip involvement often leads
to severe destruction and disability. Total hip replacement might be needed at an earlier stage in patients with
SpA who usually also have a reduced range of spinal movement resulting in a severe functional disability
(virtually complete loss of forward flexion).
4.1.7 Enthesitis
Painful inflammation of entheses (the sites of attachment of tendons, ligaments, fascia or joint capsules to
bone) is the distinguishing pathological feature of SpA. The most typical enthesitis is heel pain (posterior or
inferior) related to inflammation of the Achilles tendon or the plantar fascia insertion. Pain appears in the
morning as soon as the patient sets foot on the floor and improves with ambulation. Heel enthesitis is not
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painful during sleep but can be very disabling and resistant to standard antirheumatic treatment. Other clinical
signs are tenderness of the iliac crest, anterior tibial tuberosity or anterior chest wall. Enthesitis is best
visualised by MRI (figure 3) or ultrasonography. It is only detected by radiography after the ossification process
has occurred (figure 4). Achilles tendon swelling can be better observed in the standing position from behind.
Evaluation of an enthesopathy can be undertaken in various ways, traditionally using enthesitis scoring
systems such as the Mandel Enthesitis Index, Stoke Enthesitis Index, University of San Francisco Enthesitis
Score, Maastricht Ankylosing Spondylitis Enthesitis Score, the Spondyloarthritis Research Consortium of
Canada Enthesitis Index or the Berlin Enthesitis Score. However, these scoring systems have been criticised for
being time consuming and having poor interobserver reliability and face validity. Clinical suggestions for
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screening include MRI, an ultrasound enthesitis score or more conventional symptomatic outcome measures,
such as patient global assessment, pain and functional impairment.
Acute anterior uveitis is the most common extra-articular manifestation of AS, occurring in about 2030% of
patients, with 2540% of these patients experiencing more than one episode (figure 5). The incidence is higher
in HLA-B27-positive patients. It is important to detect and treat acute anterior uveitis rapidly as visual loss may
be irreversible. The condition typically presents with unilateral eye pain, redness, photophobia and increased
lachrymation (figure 5). Patients with these signs require urgent examination by an ophthalmologist, and may
need specialised treatment (eg, retro-orbital injections of glucocorticoids in severe cases). With treatment,
attacks usually resolve after 23 months. The main complication is the occurrence of synechiae. Uveitis that
develops with PsA or enteropathic SpA tends to be more chronic and bilateral and often involves posterior
elements.
Cardiac features are rare but may be severe. Heart block is the most frequent manifestation. Aortic
insufficiency secondary to an aseptic endocarditis can also be a severe cardiac manifestation of the disease.
Restrictive lung disease may occur in end-stage disease, as a result of costovertebral and costosternal fusion
and limited chest expansion. Apical fibrosis may occur in severe disease and this may become colonised with
bacteria or fungi such as Aspergillus.
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IgA nephropathy has been reported in AS. Amyloidosis is a very rare complication in severe longstanding
disease.
Inflammatory lesions in the gut are common and can cause diarrhoea, which is usually accompanied by blood
and mucus. Loss of weight is common. IBD may or may not have already been diagnosed in these patients.
Colonoscopic mucosal biopsy shows that subclinical inflammatory lesions are seen in 2070% of patients with
AS who have no gastrointestinal symptoms or clinically obvious IBD. Follow-up studies of such patients
indicate that 6% will develop IBD. About 2835% of patients with enteropathic arthritis have axial disease: 10
20% have sacroiliitis alone, 712% have spondylitis and 10% have the classic features of SpA. The axial
radiology is similar to that of AS, characterised by symmetrical bilateral sacroiliitis. The onset of axial
involvement often precedes that of bowel disease, and axial symptoms do not fluctuate with bowel disease
activity.
Dermatological manifestations are common but are usually related to a specific disorder such as psoriasis or
ReA. Psoriasis is seen in 2040% of patients with SpA. Nail lesions are a common feature in patients with
rheumatological manifestations.
4.3 Comorbidities
When talking about comorbidities one has to consider mainly cardiovascular (CV) disorders and osteoporosis
(see section 4.1.3 Fracture). The mortality rate in patients with AS is increased twofold in comparison with that
in the general population, mainly owing to an increased CV risk. Although specific CV disorders (valvular
disease and conduction disturbances) occur more frequently in AS, accelerated atherosclerosis disease due to
chronic systemic inflammation probably also contributes to the increased CV risk of these patients.
5 Laboratory features
No laboratory tests are diagnostic for SpA. Erythrocyte sedimentation rate and C-reactive protein (CRP) are
raised in 40% of patients. Increased CRP is one of the features of SpA used in the ASAS classification for axial
SpA, but must be present with other features. Patients with non-radiographic axSpA who have increased CRP
levels have an increased risk of further structural progression in the SI joints, and develop AS. On the other
hand, increased CRP levels are also used as predictors for a good response to treatment with TNF blockers
(OR = 2.8, 95% CI 1.3 to 5.7).
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A mild normochromic normocytic anaemia of chronic disease may be present in patients with axSpA. Alkaline
phosphatase may also be raised but this does not correlate with disease activity.
HLA-B27 is present in >90% of patients with AS. However, HLA-B27 by itself has no diagnostic value since it is
found in up to 8% of healthy individuals; it is therefore more helpful in populations with lower HLA-B27
prevalence. Determining HLA-B27 status is not mandatory in clinical assessment but is especially helpful for
classifying patients who have negative imaging. With the new ASAS classification criteria for axSpA, a patient
with a 3-month history of back pain that started before the age of 45 years can be classified as having SpA if
HLA-B27 is positive and two other SpA features are present. The diagnosis of SpA is unlikely when imaging and
HLA-B27 are both negative.
6 Imaging
Plain radiographs of the spine, SI joints and peripheral joints can show various structural changes. However,
they are unhelpful in the early, non-radiographic stage because structural changes reflect the consequences
of inflammation rather than inflammation itself (see section 6.2 MRI). Radiographic sacroiliitis is the hallmark
of AS and takes several years to become visible on plain radiographs. The earliest visible changes include
blurring of the cortical margins of the subchondral bone, erosions and sclerosis (figure 6). As erosion
progresses, the joint space appears wider and then fibrous, until bony ankylosing obliterates the joint. Joint
changes usually become symmetrical during the course of the disease. Radiographic sacroiliitis can be graded
according to the New York grading system as follows: grade I, suspicious; grade II, evidence of erosion and
sclerosis; grade III, erosions, sclerosis and early ankylosis; and, finally, grade IV, total ankylosis.
The modified New York criteria for classification as AS (box 7) combine different clinical criteria with definite
structural changes on conventional radiographs. However, these criteria focus mainly on the SI joints (both
clinically and on radiographs) and the spine (only clinically) and do not include any extra-articular
manifestations of the disease. The sensitivity of the modified New York criteria increases with disease duration
(sensitivity 0% for a disease duration of 2 years vs 60% for a disease duration of >10 years). The delay before
detecting radiological sacroiliitis might explain these results. As stated above, although the modified New York
criteria are sensitive, they cannot detect mild, undifferentiated or early forms of the disease.
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Spinal X-ray findings typically show squaring of the vertebrae secondary to erosions of the superior and
inferior margins of these bodies (figure 7). Vertebral enthesitis may cause sclerosis of the upper and lower
vertebral bodies, which appears as the formerly called shiny corners. Annulus fibrosus ossification leads to
syndesmophyte formation and over time bridging of these syndesmophytes results in a bamboo spine (figure
8). Structural damage of the spine can be scored using the modified Stoke Ankylosing Spondylitis Spine Score
(mSASSS) (figure 9).
Figure 7 (A) Radiological lumbar spinal ankylosis; (B) normal spine. (Source: Cofer, http://www.lecofer.org.)
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Figure 8 Syndesmophytes.
Figure 9 Radiological spinal scoring system in ankylosing spondylitis (AS) (modied Stoke AS Spine Score).
(Reproduced with permission from Wanders et al, Arthritis Rheum 2004;50:262232.) Based on the Outcome
Measures in Rheumatology Clinical Trials (OMERACT) (2004).
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AS and enteropathic arthritis typically exhibit bilateral symmetrical arthritis and continuous syndesmophytes,
while ReA and PsA characteristically exhibit asymmetrical sacroiliitis and discontinuous spondylitis.
Radiographs of other areas such as the heel or hip might show evidence of enthesitis.
6.2 MRI
MRI can detect inflammatory lesions long before definite lesions are visible on plain radiographs. The ASAS
criteria for axSpA include inflammation in the SI joints seen on MRI as one of the major entry criteria. When
clinical suspicion of early SpA is high but standard radiography of the SI joints is normal or shows only
equivocal changes, MRI can produce excellent evidence of sacroiliitis and enthesitis (figure 10). T2-weighted
fat-suppressed fast spin-echo and short-tau inversion recovery (STIR) sequences are the preferred imaging
sequences for assessment of bone marrow oedema (BMO), which represents a sign of inflammation.
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Figure 10B Spondylitis (left image, STIR MRI) and fatty degeneration (postinflammatory, right image, T1-
weighted MRI). STIR, short-tau inversion recovery.
Diagnosis
Clinical criteria
o Low back pain and stiffness for more than 3 months which improves with exercise but is not relieved
by rest
o Limitation of motion of the lumbar spine in both the sagittal and the frontal planes
o Limitation of chest expansion relative to normal value, corrected for age and sex
Radiological criterion
o Sacroiliitis grade >2 bilaterally or sacroiliitis grade 34 unilaterally
Grading
Definite AS if the radiological criterion is present with at least one clinical criterion
Probable AS if:
o Three clinical criteria are present
o The radiological criterion is present without any signs or symptoms fulfilling the clinical criteria
Adapted from van der Linden et al, Arthritis Rheum 1984;27:3618.
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Patients with back pain 3 months and age at onset <45 years
1 SpA feature* plus sacroiliitis** or HLA-B27 plus 2 other SpA features
*SpA features
Inflammatory spinal pain
Arthritis
Enthesitis (heel)
Uveitis
Dactylitis
Psoriasis
Crohns/colitis
Good response to NSAIDs
Family history of SpA
HLA-B27
Elevated CRP
* A patient is considered to have axial SpA if they have 1 SpA feature plus sacroiliitis** or HLA-B27 plus 2
other SpA features.
**Inammation highly compatible with sacroiliitis on MRI or denite radiographic sacroiliitis according to the
modied New York criteria.
ASAS, Assessment of SpondyloArthritis international Society; CRP, C-reactive protein; NSAIDs, non-steroidal
anti-inammatory drugs; SpA, spondyloarthritis.
Source: Sieper et al, Ann Rheum Dis 2009a;68(Suppl II):ii144.
The ASAS/OMERACT (Outcome Measures in Rheumatology Clinical Trials) MRI working group has proposed a
definition of a positive MRI (Rudwaleit et al, 2009a*). This definition should be applied for the imaging
feature sacroiliitis by MRI of the ASAS classification criteria for axSpA.
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Active inflammatory lesions of the SI joints, BMO (on STIR) or osteitis (on T1 after Gd) must be clearly
located in typical anatomical areas (subchondral or periarticular bone marrow).
When a solitary BMO lesion is seen, this should be present on at least two consecutive slices.
When more BMO lesions are seen on one slice, documentation of inflammation by using one single
slice only is enough.
The presence of synovitis, enthesitis or capsulitis without concomitant BMO/osteitis is not sufficient
for diagnosis.
However, since BMO can also be found in patients with mechanical low back pain, but moderate or severe
lesions are only found in patients with IBP, there is definite need for experience in interpreting MRI of the SI
joints. Also, further study is needed to specify the size and severity of the lesions in order to improve the
specificity of MRI.
Furthermore, a definition of a positive MRI of the spine, has been also recently proposed by ASAS (Hermann
et al, 2012*). According to this definition, evidence of spondylitis in three or more vertebral sites is highly
suggestive of inflammatory lesions related to axSpA, while evidence of fatty deposition in several vertebral
sites (at least 5) is highly suggestive of postinflammatory lesion-related axSpA. These lesions should preferably
be located at the edges of the vertebrae, independently of whether these edges are in the anterior or the
posterior part of the vertebral body.
Bone scintigraphy is not recommended for identification of sacroiliitis or spondylitis in the context of axSpA
owing to its low sensitivity (5055%) and specificity (<80%). Furthermore, ultrasound is also not frequently
used in daily practice owing to lack of standardisation of both its use and interpretation of findings, while
computed tomography (CT) seems to have only an additional value in detection of structural changes but is
also associated with higher radiation exposures, which is an important limiting factor for its use in daily
routine.
7 Classification criteria
The new validated ASAS classification criteria for axSpA (box 8) and for peripheral SpA and SpA in general (box
9) are a major step forward (Rudwaleit et al, 2009b*; Rudwaleit et al, 2011*). It is now possible to diagnose
axSpA earlier. The ASAS criteria for axSpA are applied in patients with predominantly axial symptoms with or
without peripheral manifestations, while the criteria for peripheral SpA and SpA in general have been
developed for patients who present with predominantly symptoms of arthritis, enthesitis or dactylitis. The
ASAS classification criteria for axSpA require a history of chronic back pain (pain duration 3 months) and an
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age of onset of <45 years as entry criteria. Next, either sacroiliitis on X-ray examination or MRI in addition to at
least one typical clinical SpA feature, or presence of HLA-B27 in addition to at least two typical clinical SpA
features needs to be present. With this set of criteria, patients can be still classified as AS when they present
with established radiographic changes in the SI joints, or as non-radiographic axSpA (nr-axSpA) when such
changes have not yet occurred but other entry criteria (see above and box 8) are clinically present. The
introduction of this new concept has led to an increasing interest in patients with nr-axSpA, which is also
considered to be the early form of axSpA. The ASAS classification criteria have a sensitivity of 82.9% and a
specificity of 84.4%.
The most significant change in the criteria, as compared with former sets of criteria, is the inclusion of
inflammatory activity detected by MRI as one main finding. On the other hand, normal MRI results do not
necessarily exclude a classification as SpA, which can still be made on the basis of clinical findings. In such a
case, and as mentioned above, the presence of HLA-B27 plus two other SpA features is useful for classification.
Another important difference of the new ASAS criteria is that IBP is no longer a compulsory criterion but is
being considered as one of the typical clinical SpA features, among all others.
Patients with peripheral symptoms without major axial involvement can be classified with the ASAS
classification criteria for peripheral SpA. These require a history of arthritis, enthesitis or dactylitis in addition
to SpA features.
It is important to point out that both axial and peripheral SpA criteria are still designed primarily for
classification and research purposes. There are no diagnostic criteria for SpA, which means that in daily clinical
practice one might have to adopt a more flexible approach. A proposed clinical diagnostic tree is shown in
figure 11.
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Figure 11 Diagnostic criteria for ankylosing spondylitis (tree decision). AS, ankylosing spondylitis; ASAS,
Assessment of SpA international Society; LR, likelihood ratio; SpA, spondyloarthritis. (Reproduced from van
den Berg et al, Ann Rheum Dis 2013;72:164653.)
8 Treatment
Treatment with NSAIDs and exercise is recommended as first-line therapies in patients with SpA. For those
patients who still have active disease the introduction of TNF inhibitors (TNFi) was a major advance in the
management of axial SpA. The main principles of the treatment of patients with SpA is published by ASAS in
the ASAS/EULAR recommendations for the management of AS (Braun et al, 2011*). One important principle in
the treatment of patients with SpA is the need for a combination therapy including pharmacological and non-
pharmacological treatment options. The treating physician should tailor the treatment of patients according to
prognostic factors (see section 9.3, Can we predict the further course of the disease?) and to the general
clinical status, including comorbidity.
8.1 NSAIDs
NSAIDs are recommended as first-line drugs for patients with axSpA. If taken in appropriate dosages, they are
efficacious for the relief of pain and stiffness in up to 6070% of the patients. There is no significant difference
in efficacy between short-acting and long-acting agents or between Cox-2-selective and non-selective agents.
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Up to 15% of patients with active AS treated with a full dose of an NSAID may even reach a status of partial
remission. The question of whether it is advisable to recommend continuous treatment with NSAIDs even in,
or after reaching, a status of low disease activity is still a matter of discussion. The effect of NSAIDs on
inflammatory activity (CRP, BMO) or on the radiographic progression of patients with axSpA is still not clear.
The cornerstone in the treatment of patients with AS was developed at the beginning of the century with the
approval of anti-TNF blockers. Anti-TNF blockers should be prescribed according to the international ASAS
recommendations (van der Heijde et al, 2011*) (table 2). These recommendations give detailed information
for patient selection, assessment of disease and assessment of response when using these compounds. It is
important to notice that these recommendations specifically relate to patients with axSpA. For treatment with
anti-TNF agents, patients need to have increased disease activity, which is defined as Bath Ankylosing
Spondylitis Disease Activity Index (BASDAI) 4 (on a 010 scale) despite previous treatment with at least two
NSAIDs over a period of 4 weeks. There is no evidence to support the obligatory use of disease-modifying
antirheumatic drugs (DMARDs) before starting anti-TNF therapy.
Table 2 2010 Update of the international ASAS recommendations for the use of anti-TNF agents in patients
with SpA
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AS, ankyosing spondylitis; ASAS, Assessment of SpA international Society; BASDAI, Bath Ankylosing Spondylitis
Disease Activity Index; DMARDs, disease-modifying antirheumatic drugs; NSAIDs, non-steroidal anti-
inflammatory drugs; SpA, spondyloarthritis; TNF, tumour necrosis factor.
It is recommended that the response to anti-TNF is assessed 3 months after starting treatment. A decrease of
disease activity (as measured by the BASDAI) of at least 50% as compared with previous treatment (BASDAI-50
response) or an absolute BASDAI change of 2 units (on a 010 scale) in addition to an expert opinion (based on
improvement in CRP, MRI inflammation or clinical examination) are considered parameters for continuing
treatment.
Patients with high disease activity, short disease duration, no structural lesions and increased CRP are more
likely to benefit from anti-TNF medication than patients with longstanding disease, extensive structural
changes and poor functioning before treatment initiation. Overall, the response to anti-TNF treatment in AS is
considered to be better than the response to this treatment of patients with rheumatoid arthritis. Even in
patients with complete ankylosis of the spine, this treatment has substantial clinical efficacy. There is no
evidence of differences in the efficacy of the various TNFi approved so far. Other biological agents have failed
to show at least similar clinical outcomes to those of the TNF blockers. In contrast to their promising clinical
efficacy, radiographic progression does not seem to be inhibited by anti-TNF therapy.
8.3 DMARDs
Data on the use of DMARDs in patients with AS did not show an effect on axial symptoms. The majority of the
studies suggest a limited efficacy of sulfasalazine in patients with peripheral SpA and in the prevention of
anterior uveitis. One head-to head trial comparing sulfasalazine with a TNF blocker showed that TNF blockade
is more efficacious in achieving an ASAS20 response at week 16 than sulfasalazine (75.9% vs 52.9%, p < 0.0001)
The cornerstone of non-pharmacological treatment is regular exercise and patient education. It has been
shown that regular exercises are effective in reducing pain and preserving functioning. Overall, supervised
exercises are more effective than home exercises.
8.5 Surgery
Surgery might be required in patients with AS with hip involvement, severe spinal deformity or vertebral
fracture. Around 5% of patients will undergo a total hip arthroplasty, while around 50% of them will need
bilateral hip replacement during the course of their disease. The restricted mobility and hyperkyphosis of the
spine may lead to loss of the ability to keep the eyes and head upwards, being able to look horizontally.
Patients with such severe deformities can benefit from a spinal corrective osteotomy. Such procedures are
only performed in experienced centres. As stated above, patients with AS have an increased risk of clinical
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vertebral fractures but not of non-vertebral fractures. In most cases the occurrence of a spinal fracture is an
acute clinical situation which may be associated with neurological symptoms. Although not all patients need to
be operated on, physicians have to consider consulting an experienced surgeon when even silent fractures
are suspected.
9 Assessment/monitoring
For both assessment and monitoring, one has to consider systematically the four potential clinical
presentations of axSpA: axial involvement, peripheral arthritis, enthesopathy and extra-articular features.
According to the variable disease course, the clinical presentation of the patient should be the key feature for
disease monitoring. Monitoring is based on the clinical presentation, and the tools used for evaluating the
severity of axial involvement are similar, and independent of the SpA subgroup. Principles for monitoring
patients with AS are defined in the ASAS core set (table 3). The ASAS recommendations for the management
of AS do not specify the time frame in which patients have to visit the treating physician. It is advisable that a
patient with a new diagnosis or with a high disease activity should be seen more often than a patient with a
low disease activity. In general, spinal X-ray examinations do not need be repeated more frequently than every
2 years unless clearly indicated in individual cases owing to symptoms. Each change in the disease course
should be evaluated carefully by the treating physician.
Table 3 ASAS core set (Adapted from van der Heijde D et al, J Rheumatol 1999;26:9514)
Domain Instrument
Physical function* BASFI or Dougados Functional Index
Pain* VAS/NRS past week in spine, at night, due to AS and VAS/NRS past
week, in spine due to AS
Spinal mobility* Chest expansion and modified Schober and occiput-to-wall distance
and lateral spinal flexion
Patient global assessment* VAS/NRS past week
Morning stiffness* Duration of morning stiffness in spine past week
Fatigue* VAS/NRS past week
Peripheral joints and entheses Number of swollen joints (44 joint count). Validated enthesis indexes
Acute phase reactants ESR
Spine radiographs Anteroposterior + lateral lumbar and lateral cervical spine and X-ray
examination of pelvis to visualise sacroiliac joint and hips)
Hip radiographs As above
*Included in core set for DC-ART, SMARDs/physical therapy and clinical record keeping.
Included in core set for DC-ART and clinical record keeping.
Included in core set for DC-ART.
AS, ankylosing spondylitis; ASAS, Assessment of SpondyloArthritis international Society; BASFI, Bath AS
Functional Index; DC-ART, disease-controlling antirheumatic therapy; ESR, erythrocyte sedimentation rate; NRS,
numerical rating scale; SMARDs, symptom-modifying antirheumatic drugs; VAS, Visual Analogue Scale.
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The ASAS has issued recommendations about the use of different assessment tools covering the various
domains of disease activity (table 3).
Appropriate assessment tools are needed, depending on the clinical pattern of the disease. Table 4
summarises the different clinical patterns in patients with SpA.
In patients with axial involvement, the degree of both night pain and spinal pain during the day is measured
using either a Visual Analogue Scale (VAS) or a Numerical Rating Scale. Morning stiffness in the lumbar spine
should be evaluated for both duration and severity. Functional impairment is evaluated using the Bath AS
Functional Index (box 10). The score ranges from 0 to 10, where higher values indicate worse functioning. All
the above tools are patient reported and considered subjective. When using the VAS, a value >4 on a scale
from 0 to 10 is usually considered as reflecting active disease.
Please indicate your level of ability with each of the following activities during the past week (difculty is
assessed on an 11-point scale, 010)
Putting on your socks or tights without help or aid (eg, sock aids)
Bending forward from the waist to pick up a pen from the floor without an aid
Reaching up to a high shelf without help or aids (eg, helping hand)
Getting up out of an armless dining room chair without using your hands or any other help
Getting up off the floor without help from lying on your back
Standing unsupported for 10 min without discomfort
Climbing 1215 steps without using a handrail or walking aid (one foot each step)
Looking over your shoulder without turning your body
Doing physically demanding activities (eg, physiotherapy exercises, gardening or sports)
Doing a full days activities whether it be at home or at work
The main question in daily practice is whether it is mandatory to employ objective methods to evaluate such
activity before considering a new treatment, such as an anti-TNF agent. The only non-subjective instruments
reflecting disease activity are serum CRP (raised in up to 40% of patients) and the presence of inflammatory
lesions on MRI at the spine and/or SI joints.
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In peripheral arthritis, disease activity evaluation is similar to that used in rheumatoid arthritisfor example,
number of tender joints, number of swollen joints, CRP, etc. There is no consensual definition of a peripheral
active disease. However, the presence of at least three swollen joints is usually considered to reflect active
disease, particularly when associated with an increased CRP.
Besides the different instruments facilitating activity assessment of the different clinical presentations,
instruments (eg, a composite index) have been proposed to allow a general evaluation.
The BASDAI (box 11) is simple to use since it comprises only six questions related to:
How would you describe the overall level of fatigue/tiredness you have experienced?
How would you describe the overall level of ankylosing spondylitis neck, back or hip pain you have
had?
How would you describe the overall level of pain/swelling in joints other than the neck, back or hips
you have had?
How would you describe the overall level of discomfort you have had from any areas tender to touch
or pressure?
How would you describe the overall level of morning stiffness you have had from the time you wake
up?
How long does your morning stiffness last from the time you wake up?
fatigue
axial involvement
peripheral articular involvement
enthesopathy
morning stiffness (two questions).
The BASDAI score ranges from 0 to 10, higher values indicating more active disease. A score >4 is considered as
the threshold above which a disease status can be considered as active. A change of at least 50% in the BASDAI
is usually considered as reflecting a clinically relevant improvement.
More recently, another composite index taking into account some questions in the BASDAI (Q 2 total back
pain, 3 peripheral pain and 6 morning stiffness) and also the biological markers of inflammation (either CRP or
erythrocyte sedimentation rate) has been proposed (box 12). The ASDAS has been extensively validated. It has
been shown to be reliable, discriminative and sensitive. The cut-off points between the disease activity states
are: inactive disease 1.3, moderate 1.32.0, high 2.13.5 and very high 3.5 The ASDAS cut-off point for
clinically important improvement is 1.1 and the cut-off point for a major improvement is 2.0. However, the
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ASDAS has still not been evaluated for use in daily practice, whereas the BASDAI is the standard measuring
instrument for disease activity in axSpA.
ASDAS-CRP*
0.21Total back pain + 0.110Patient global + 0.073Peripheral pain/swelling + 0.058Duration of morning
stiffness + 0.579Ln (CRP + 1)
ASDAS-ESR*
0.113Patient global + 0.293 ESR + 0.086 Peripheral pain/swelling + 0.069 Duration of morning stiffness
+ 0.079 Total back pain
CRP, C-reactive protein; ESR, erythrocyte sedimentation rate.
Source: Lukas et al, Ann Rheum Dis 2009;68:1824.
ASAS has proposed two composite indices for monitoring disease activity in clinical trials:
Improvement of at least 20% and absolute improvement of at least 10 on a 0100 scale in at least three of
the following domains:
Patient global (VAS (0100))
Pain (VAS global, past 2 days (0100))
Function (BASFI (0100))
Inflammation
o First choicetwo last questions of the BASDAI
o Second choicemorning stiffness duration with a maximum of 120 mm on a 0100 scale
Absence of deterioration (of at least 20% and absolute deterioration of at least 10 on a 0100 scale) in the
remaining domain.
ASAS, Assessment of SpondyloArthritis international Society; BASDAI, Bath AS Disease Activity Index; BASFI,
Bath AS Functional Index; VAS, Visual Analogue Scale.
Source: Anderson et al, Arthritis Rheum 2001;44:187686.
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The term severity is often used but not defined for patients with AS. Severity as understood by experts
contains all the different aspects of the disease (disease activity, damage, reduced mobility, reduced physical
function, reduced social participation). Such severity can be assessed using different approaches, such as,
functional impairment, limited range of motion, hip involvement, radiological damage and even job loss or
death. Here, we focus on the four measures that are mainly related to SpA.
Functional impairment can be related to both the activity and the severity of the disease. Several available
instruments (Bath AS Functional Index, Health Assessment Questionnaire, Western Ontario and McMaster
Universities osteoarthritis index, etc) can be used depending on the clinical presentation of SpA.
The most commonly used instrument in clinical trials is the Bath AS Metrology Index (BASMI), a composite
index combining information from five different tools: cervicalrotation (figure 12), tragus-to-wall distance
(figure 13), spinal lateral flexion (figure 14), lumbar flexion (modified Schobers test) (figure 15) and
intermalleolar distance (figure 16). Three different definitions have been published: the 2-step definition, the
10-step definition and the linear definition. ASAS recommends the 10-step definition or the linear definition.
Table 5 shows details of the BASMI.
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Table 5 Bath Ankylosing Spondylitis Mobility Index (BASMI): evaluation of spinal mobility (Adapted from
Jenkinson et al, J Rheumatol 1994;21:16948 and van der Heijde et al, Ann Rheum Dis 2008;67:48993)
Abnormal postures have to be carefully checked in order to provide the best physical therapy. Once the loss of
lumbar lordosis has appeared, thoracic kyphosis and a fixed flexed posture of the cervical spine may follow.
The most disabling abnormal posture is the loss of the horizontal view, for which a surgical spinal intervention
(vertebral osteotomy) can be considered (see also above).
Hip involvement is closely related to the severity of spinal ossification and is responsible for significant
functional impairment. The prevalence after 10 years of disease is around 1015% in Western European
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countries, but up to 4050% in other parts of the world, such as North Africa. It is typically bilateral. The
significance of hip involvement has been shown in a recent multinational study, in which 5% of the patients
underwent a total hip arthroplasty, The intermalleolar distance of the BASMI reflects the degree of hip
involvement.
The disease course of AS is highly variable and one-third of patients with AS will develop a severe disease,
accompanied by structural changes such as syndesmophytes and ankylosis in the spine. Information about the
future potential severity of the disease is therefore important. Similar to rheumatoid arthritis, there is a trend
towards treating patients efficiently as early as possible and before irreversible structural damage has
occurred.
This prognostic assessment is important to guide treatment strategies. Candidate predictors for potentially
severe disease are shown in box 15. In general, the negative predictive value is more reliable than the positive
predictive value. In other words, the absence of any of the variables listed in box 15 is highly predictive of a
good prognosis. Recent data from inception cohorts showed that patients with raised CRP, with extensive
inflammation in the SI joints, and patients who smoke are at higher risk of developing structural changes in the
SI joints than those patients who do not have these factors.
This question is of great importance when considering treatments such as anti-TNF blockers. The most
common situation is when a patient is described as refractory to NSAIDs. Because of patients variability in
their response to NSAIDs, the current recommendation is to define a patient as refractory to NSAIDs only
when active disease persists despite the intake of at least two courses of NSAIDs taken at an optimal dosage
for at least 23 weeks.
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ASAS together with EULAR published in 2006 and updated in 2010 the ASAS/EULAR recommendations for the
management of AS (Braun et al, 2011*). Since the evidence on the course and management of axial SpA is
limited and the literature is mainly based on data about AS it has been decided to restrict the
recommendations to AS, although the experts unanimously agreed that these recommendations can equally
be applied to patients with axSpA.
The updated management recommendation includes overarching principles which deal with specific
modalities important for each patient with AS. Eleven recommendations address several aspects of the
management of patients with AS. It has been stated that management requires a multidisciplinary treatment
coordinated by the rheumatologists since AS is a potentially severe disease with diverse manifestations as we
have shown in the review above. To prevent deteriorating functioning in patients with AS it is important that
the optimal management is based on a combination of non-pharmacological and pharmacological treatment
modalities (see chapter 12, Treatment) and that the decision about optimal management is based on a shared
decision between patients and rheumatologists. Discrepancies between patients and physicians perspectives
of the disease and its outcome are well known and should be taken into account in the daily routine for
treating patients with AS.
Patient education is crucial for the successful management of patients with SpA. Once the diagnosis is made,
the patient should be given a clear description of the nature of the disease, including an explanation of the
potential clinical symptoms and presentations and the possible progression of the target symptom.
The patient has to be informed clearly about the differences between back pain due to SpA and
mechanical back pain. The most common misconceptions are that (a) NSAIDs have a higher toxicity
than efficacy and (b) physiotherapy has no effect on the long-term outcome of back pain.
Information about the possible occurrence of spinal ankylosis and abnormal postures will lead to
better compliance with proposed treatments, such as NSAIDs and physiotherapy, and will give the
patient a better understanding of the benefits of regular follow-up.
The patient must be informed about the possibility of the occurrence of other clinical symptoms of
SpA. For example, the risk of developing acute anterior uveitis, in which case an early ophthalmic
review would be required, and this has to be clearly explained.
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Acknowledgement
Previous editions of this chapter were authored by Maxime Dougados, Robert Landew, Cecilia Mercieca,
Andrew A Borg.
Summary points
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Affiliations
Key references*
Braun J, van den Berg R, Baraliakos X, et al. 2010 update of the ASAS/EULAR recommendations for the
management of ankylosing spondylitis. Ann Rheum Dis 2011;70:896904.
Hermann KG, Baraliakos X, van der Heijde DM, et al. Descriptions of spinal MRI lesions and definition of a
positive MRI of the spine in axial spondyloarthritis: a consensual approach by the ASAS/OMERACT MRI study
group. Ann Rheum Dis 2012;71:127888.
Lukas C, Landew R, Sieper J, et al. Development of an ASAS-endorsed disease activity score (ASDAS) in
patients with ankylosing spondylitis. Ann Rheum Dis 2009;68:1824.
Rudwaleit M, Jurik AG, Hermann KG, et al. Defining active sacroiliitis on magnetic resonance imaging (MRI) for
classification of axial spondyloarthritis: a consensual approach by the ASAS/OMERACT MRI group. Ann Rheum
Dis 2009a;68:15207.
Rudwaleit M, van der Heijde D, Landew R, et al. The development of Assessment of SpondyloArthritis
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Rheum Dis 2009b;68:77783.
Rudwaleit M, van der Heijde D, Landew R, et al. The development of Assessment of SpondyloArthritis
International Society classification criteria for peripheral spondyloarthritis and spondyloarthritis in general.
Ann Rheum Dis 2011;70:2531.
Van der Heijde D, Sieper J, Maksymowych WP, et al. 2010 Update of the international ASAS recommendations
for the use of anti-TNF agents in patients with spondyloarthritis. Ann Rheum Dis 2011;70:9058.
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