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type=\u0022text\/css\u0022 rel=\u0022stylesheet\u0022 href=\u0022\/\/d282kpwvnogo5m.cloudfront.net\/sites\/default\/files\/advagg_css\/css__ce2QY63WIanKyr8eSq7eavr1XQRRmFD6ZSmwpyJi8lM__zXwFqpqmxrZOXXcd_TpBQpjuELbmIP9wBR5UuTDWAO4__YJWWMMdfCJuAFm5cUEp88OsodhO3ZA-2lzRfoBsSlk4.css\u0022 media=\u0022all\u0022 \/\u003E\n\u003Clink rel=\u0027stylesheet\u0027 type=\u0027text\/css\u0027 href=\u0027\/sites\/all\/modules\/contrib\/panels\/plugins\/layouts\/onecol\/onecol.css\u0027 \/\u003E\u003C\/head\u003E\u003Cbody\u003E\u003Cdiv class=\u0022panels-ajax-tab-panel panels-ajax-tab-panel-sageoa-tab-art\u0022\u003E\u003Cdiv class=\u0022panel-display panel-1col clearfix\u0022 \u003E\n  \u003Cdiv class=\u0022panel-panel panel-col\u0022\u003E\n    \u003Cdiv\u003E\u003Cdiv class=\u0022panel-pane pane-highwire-markup\u0022 \u003E\n  \n      \n  \n  \u003Cdiv class=\u0022pane-content\u0022\u003E\n    \u003Cdiv class=\u0022highwire-markup\u0022\u003E\u003Cdiv xmlns=\u0022http:\/\/www.w3.org\/1999\/xhtml\u0022 id=\u0022content-block-markup\u0022 xmlns:xhtml=\u0022http:\/\/www.w3.org\/1999\/xhtml\u0022\u003E\u003Cdiv class=\u0022article fulltext-view \u0022\u003E\u003Cspan class=\u0022highwire-journal-article-marker-start\u0022\u003E\u003C\/span\u003E\u003Cdiv class=\u0022section abstract\u0022 id=\u0022abstract-1\u0022\u003E\u003Ch2\u003ESummary\u003C\/h2\u003E\n            \u003Cp id=\u0022p-1\u0022\u003EThe spondyloarthritides (SpA) represent a combination of pathogenically related diseases that share many clinical manifestations. As a group, the prevalence of SpA is 0.5% to 1.9%, and the most common subgroups are ankylosing spondylitis (AS) and undifferentiated spondyloarthritis (uSpA). The typical age of onset of AS is between 20 and 30 years of age. Several studies have shown that there may be a delay of 5 to 10 years before diagnosis [Khan MA. \u003Cem\u003EAnn Rheum Dis\u003C\/em\u003E 2002; Mau W et al. \u003Cem\u003EJ Rheumatol\u003C\/em\u003E 1988; Feldtkeller E et al. \u003Cem\u003ERheumatol Int\u003C\/em\u003E 2003].\u003C\/p\u003E\n         \u003C\/div\u003E\u003Cul class=\u0022kwd-group\u0022\u003E\u003Cli class=\u0022kwd\u0022\u003Einflammatory disorders\u003C\/li\u003E\u003C\/ul\u003E\u003Cdiv class=\u0022section\u0022 id=\u0022sec-1\u0022\u003E\n         \n         \u003Cp id=\u0022p-2\u0022\u003EThe spondyloarthritides (SpA) represent a combination of pathogenically related diseases that share many clinical manifestations. As a group, the prevalence of SpA is 0.5% to 1.9%, and the most common subgroups are ankylosing spondylitis (AS) and undifferentiated spondyloarthritis (uSpA). The typical age of onset of AS is between 20 and 30 years of age. Several studies have shown that there may be a delay of 5 to 10 years before diagnosis [Khan MA. \u003Cem\u003EAnn Rheum Dis\u003C\/em\u003E 2002; Mau W et al. \u003Cem\u003EJ Rheumatol\u003C\/em\u003E 1988; Feldtkeller E et al. \u003Cem\u003ERheumatol Int\u003C\/em\u003E 2003].\u003C\/p\u003E\n         \u003Cp id=\u0022p-3\u0022\u003EMartin Rudwaleit, MD, University Hospital Charit\u00e9 Berlin, Berlin, Germany, offered 2 possible reasons for this delay in diagnosis: the relatively late appearance of radiographic sacroiliitis (a definitive diagnosis criterion for AS) in one subgroup of patients with SpA and the low degree of awareness of SpA among non-rheumatologists. Early diagnosis is important, however, because very effective new treatments have become available for this group of disabling diseases.\u003C\/p\u003E\n         \u003Cp id=\u0022p-4\u0022\u003EIt is important to realize that the disease does not start when radiographic changes occur. Inflammatory back pain (IBP), the leading symptom of AS and uSpA, precedes the development of radiographic changes in the sacroiliac joints, sometimes by many years [Rudwaleit M et al. \u003Cem\u003EAnn Rheum\u003C\/em\u003E Dis 2004]. It is during this stage that MRI is a particularly important diagnostic tool to possibly visualize sacroiliitis.\u003C\/p\u003E\n         \u003Cp id=\u0022p-5\u0022\u003EThe lesions that can be seen on MRI mainly are active (acute) inflammatory lesions (eg, bone marrow edema [BME; osteitis], capsulitis, synovitis, enthesitis), but structural damage (sclerosis, erosions, fat deposition, bony bridges\/ankylosis) also may be detected. However, conventional X-rays are superior in the detection of structural changes.\u003C\/p\u003E\n         \u003Cp id=\u0022p-6\u0022\u003EBased on interviews with AS patients (n=101) and patients with mechanical back pain (n=112), Dr. Rudwaleit and colleagues identified 4 items that differentiated the 2 groups: morning stiffness \u0026gt;30 minutes, pain that improves with exercise but not with rest, awakening in the early morning hours because of pain, and alternating buttock pain. Based on this study, the investigators determined that IBP is present if at least 2 of the 4 conditions are met (Sensitivity 70%; Specificity 81%) [Rudwaleit M et al. \u003Cem\u003EArthritis Rheum\u003C\/em\u003E 2006].\u003C\/p\u003E\n         \u003Cp id=\u0022p-7\u0022\u003EDr. Rudwaleit concluded by telling the audience that making an early diagnosis of SpA without definite radiographic changes in the sacroiliac joints is feasible in daily practice. The presence of IBP as such is not sufficient for diagnosis, a combination of several SpA features are necessary, including the presence of IBP, MRI results, and the human leukocyte antigen (HLA)-B27.\u003C\/p\u003E\n      \u003C\/div\u003E\u003Cdiv class=\u0022section\u0022 id=\u0022sec-2\u0022\u003E\n         \u003Ch2 class=\u0022\u0022\u003EMonitoring Patients in Clinical Practice\u003C\/h2\u003E\n         \u003Cp id=\u0022p-8\u0022\u003EAS is a multifaceted disease that affects multiple outcome domains. To assist rheumatologists in monitoring their patients, the Assessment in AS (ASAS) working group has established a core set of domains for clinical record keeping as well as specific assessment methods for each domain [van der Heijde et al. \u003Cem\u003EJ Rheumatol\u003C\/em\u003E 1999; ASAS workshop Ghent, Oct 2002; Bath 2007]. Two types of assessments are provided: patient self-assessments and measurements that are performed by health care providers. Robert B.M. Landew\u00e9, MD, University Hospital Maastricht, Maastricht, The Netherlands, reviewed the most recent set of recommendations that were considered appropriate for individual patients (\u003Ca id=\u0022xref-table-wrap-1-1\u0022 class=\u0022xref-table\u0022 href=\u0022#T1\u0022\u003ETable 1\u003C\/a\u003E).\u003C\/p\u003E\n         \u003Cdiv id=\u0022T1\u0022 class=\u0022table pos-float\u0022\u003E\u003Cdiv class=\u0022table-inline\u0022\u003E\u003Cdiv class=\u0022callout\u0022\u003E\u003Cspan\u003EView this table:\u003C\/span\u003E\u003Cul class=\u0022callout-links\u0022\u003E\u003Cli class=\u00220 first\u0022\u003E\u003Ca href=\u0022\/\u0022 class=\u0022table-expand-inline\u0022 data-table-url=\u0022\/highwire\/markup\/11046\/expansion?postprocessors=highwire_figures%2Chighwire_math%2Chighwire_inline_linked_media%2Chighwire_embed\u0026amp;table-expand-inline=1\u0022 html=\u00221\u0022 fragment=\u0022#\u0022 external=\u00221\u0022 data-icon-position=\u0022\u0022 data-hide-link-title=\u00220\u0022\u003EView inline\u003C\/a\u003E\u003C\/li\u003E\u003Cli class=\u00221\u0022\u003E\u003Ca href=\u0022\/highwire\/markup\/11046\/expansion?width=1000\u0026amp;height=500\u0026amp;iframe=true\u0026amp;postprocessors=highwire_figures%2Chighwire_math%2Chighwire_inline_linked_media\u0022 class=\u0022colorbox colorbox-load table-expand-popup\u0022 rel=\u0022gallery-fragment-tables\u0022 data-icon-position=\u0022\u0022 data-hide-link-title=\u00220\u0022\u003EView popup\u003C\/a\u003E\u003C\/li\u003E\u003Cli class=\u00222 last\u0022\u003E\u003Ca href=\u0022\/highwire\/powerpoint\/11046\u0022 class=\u0022highwire-figure-link highwire-figure-link-ppt\u0022 data-icon-position=\u0022\u0022 data-hide-link-title=\u00220\u0022\u003EDownload powerpoint\u003C\/a\u003E\u003C\/li\u003E\u003C\/ul\u003E\u003C\/div\u003E\u003C\/div\u003E\u003Cdiv class=\u0022table-caption\u0022\u003E\u003Cspan class=\u0022table-label\u0022\u003ETable 1.\u003C\/span\u003E \n               \u003Cp id=\u0022p-9\u0022 class=\u0022first-child\u0022\u003EASAS Core Set for Clinical Record Keeping.\u003C\/p\u003E\n            \u003Cdiv class=\u0022sb-div caption-clear\u0022\u003E\u003C\/div\u003E\u003C\/div\u003E\u003C\/div\u003E\n         \u003Cp id=\u0022p-11\u0022\u003EProf. Landew\u00e9 reminded the audience that improvement criteria such as the ASAS20 and 40, while validated for use in clinical trials, are not considered appropriate for use in individual patients. Although the BASDAI contains only patient-reported outcomes, it frequently is used in clinical practice because of its feasibility. However, the rheumatologist always needs to consider that there are many potential reasons for back pain, also in SpA patients. The ASAS working group has initiated a new project to develop a disease activity score for AS (the ASDAS) that includes both patient-reported outcomes as well as acute phase reactants. It is expected to be published later this year. In the meantime, Prof. Landew\u00e9 urged the members of the audience to monitor their patients with AS using the existing guidelines.\u003C\/p\u003E\n      \u003C\/div\u003E\u003Cdiv class=\u0022section\u0022 id=\u0022sec-3\u0022\u003E\n         \u003Ch2 class=\u0022\u0022\u003EHow to Use Biologics\u003C\/h2\u003E\n         \u003Cp id=\u0022p-12\u0022\u003ESeveral anti-TNF-\u03b1 agents (infliximab, etanercept, adalimumab) are now approved for the treatment of rheumatoid arthritis, AS, and psoriatic arthritis (PsA) in the United States and in Europe. In patients with active AS and PsA whose condition is not sufficiently controlled with NSAIDs (for axial disease) or sulfasalazine or methotrexate (for peripheral arthritis), anti-TNF-\u03b1 agents may be considered as first-line treatment.\u003C\/p\u003E\n         \u003Cp id=\u0022p-13\u0022\u003EJ\u00fcrgen Braun, MD, Ruhr-Universit\u00e4t Bochum, Bochum, Germany, discussed the use of TNF inhibitors in the treatment of SpA.\u003C\/p\u003E\n         \u003Cp id=\u0022p-14\u0022\u003EFor infliximab, a dose between 3 to 5 mg\/kg is required at intervals of 6 to 8 weeks to provide constant suppression of disease activity. The efficacy of infliximab can persist for over 3 years [Baraliakos \u00d7 et al. \u003Cem\u003EArthritis Res Ther\u003C\/em\u003E 2005; \u003Cem\u003EJ Rheumatol\u003C\/em\u003E 2007]. Now, data for up to 7 years are available [Baraliakos X et al. EULAR 2008], and although almost all patients relapse after withdrawal, readministration is safe and efficacious [Baraliakos X et al. \u003Cem\u003EArthritis Res Ther\u003C\/em\u003E 2005]. The standard dosage of etanercept is 2 \u00d7 25 mg subcutaneously per week. For adalimumab, the standard dose is 40 mg subcutaneously every 2 weeks. Although most controlled studies of the anti-TNF therapies have permitted concomitant therapy with methotrexate, there is no evidence that concomitant therapy provides significant additional effect on either axial symptoms [Breban M et al. \u003Cem\u003EArthritis Rheum\u003C\/em\u003E 2007] or MRI lesions for patients with AS [Li et al. \u003Cem\u003ERheumatology\u003C\/em\u003E 2008, in press].\u003C\/p\u003E\n         \u003Cp id=\u0022p-15\u0022\u003EAll SpA-related symptoms seem to respond to anti-TNF therapy; swollen joints [van den Bosch et al. \u003Cem\u003EArthritis Rheum\u003C\/em\u003E 2002], enthesitis [D\u0027Agostino MA et al. \u003Cem\u003EArthritis Rheum\u003C\/em\u003E 2002 and 2003], flares of anterior uveitis [Braun J et al. \u003Cem\u003EArthritis Rheum\u003C\/em\u003E 2005], and acute inflammatory bowel disease [Braun J et al. 2007 \u003Cem\u003EArthritis Rheum\u003C\/em\u003E] do not occur or occur less frequently. Adalimumab has been shown to work in subgroups of SpA patients, such as those with total spinal ankylosis [van der Heijde et al. \u003Cem\u003EArthritis Rheum\u003C\/em\u003E 2006], and in patients with early axial uSpA [Haibel et al. \u003Cem\u003EArthritis Rheum\u003C\/em\u003E 2008].\u003C\/p\u003E\n         \u003Cp id=\u0022p-16\u0022\u003EAdditional studies are needed to document the long-term efficacy of anti-TNF treatment. Limited evidence suggests that the efficacy may last for 7 years in about 50% of the initially treated patients. Importantly, function and spinal mobility are preserved and even improve over time.\u003C\/p\u003E\n         \u003Cp id=\u0022p-17\u0022\u003EThere is evidence that anti-TNF therapy has an effect on structural damage in PsA that relates to osteodestructive changes, but the osteoproliferative changes of AS, such as syndesmophytes and ankylosis, do not seem to be prevented. More studies are needed to clarify this issue.\u003C\/p\u003E\n         \u003Cp id=\u0022p-18\u0022\u003ESevere adverse events are rare, although complicated infections including tuberculosis have been reported. These can largely be prevented by appropriate screening. Autoantibodies have been reported to occur, especially with infliximab therapy, but associated clinical symptoms are rare. No increase in malignancies has been observed so far.\u003C\/p\u003E\n         \u003Cp id=\u0022p-19\u0022\u003EIn Prof. Braun\u0027s view, \u201cAs it stands now, the benefits of anti-TNF therapy in AS seem to clearly outweigh the few shortcomings.\u201d Given the lack of efficacy of conventional DMARDs to treat axial symptoms of SpA, anti-TNF therapy becomes more and more a standard of care.\u003C\/p\u003E\n      \u003C\/div\u003E\u003Cul class=\u0022copyright-statement\u0022\u003E\u003Cli class=\u0022fn\u0022 id=\u0022copyright-statement-1\u0022\u003E\u00a9 2008 MD Conference Express\u003C\/li\u003E\u003C\/ul\u003E\u003Cspan class=\u0022highwire-journal-article-marker-end\u0022\u003E\u003C\/span\u003E\u003C\/div\u003E\u003Cspan id=\u0022related-urls\u0022\u003E\u003C\/span\u003E\u003C\/div\u003E\u003Ca href=\u0022http:\/\/mdc.sagepub.com\/content\/8\/5\/28.abstract\u0022 class=\u0022hw-link hw-link-article-abstract\u0022 data-icon-position=\u0022\u0022 data-hide-link-title=\u00220\u0022\u003EView Summary\u003C\/a\u003E\u003C\/div\u003E  \u003C\/div\u003E\n\n  \n  \u003C\/div\u003E\n\u003C\/div\u003E\n  \u003C\/div\u003E\n\u003C\/div\u003E\n\u003C\/div\u003E\u003Cscript type=\u0022text\/javascript\u0022 src=\u0022http:\/\/mdc.sagepub.com\/sites\/all\/modules\/highwire\/highwire\/plugins\/highwire_markup_process\/js\/highwire_openurl.js?nzmf3e\u0022\u003E\u003C\/script\u003E\n\u003Cscript type=\u0022text\/javascript\u0022 src=\u0022http:\/\/mdc.sagepub.com\/sites\/all\/modules\/highwire\/highwire\/plugins\/highwire_markup_process\/js\/highwire_tables.js?nzmf3e\u0022\u003E\u003C\/script\u003E\n\u003C\/body\u003E\u003C\/html\u003E"}