Diagnostic Tests in Rheumatic Disease: What s Old, What s New & What s Useful? COPYRIGHT

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Diagnostic Tests in Rheumatic Disease: What s Old, What s New & What s Useful? Robert H. Shmerling, M.D. Beth Israel Deaconess Medical Center Boston, MA

Diagnostic Tests in Rheumatic Disease: What's Old, What's New & What's Useful 1. Introduction 4. ANA 2. ESR & CRP 5. ANCA 3. RF & anti-ccp 6. Imaging Studies

DIAGNOSTIC TESTS: INTRODUCTION Diagnostic tests rarely establish a diagnosis in rheumatic disease and frequently provide more prognostic than diagnostic information. Sensitivity and specificity are a good start: they are available for many tests and are not dependent on prevalence of disease. Predictive value is the most useful characteristic of a test but varies with disease prevalence (or pre-test probability) it is highly dependent on judgment. The rheumatic disease criteria help standardize studies but have limitations - milder disease may be excluded.

ERYTHROCYTE SEDIMENTATION RATE (ESR) Highly sensitive, but not specific ØThat includes the ESR > 100 Rises with age (normal = age/2; see Ann Intern Med 1986;104:515), pregnancy, infection, malignancy Be prepared to deal with the results (SUO* versus false negative) *Sed rate of unknown origin

The ESR: How it s done

ERYTHROCYTE SEDIMENTATION RATE (ESR) Rheumatic Disease Giant Cell Arteritis, Polymyalgia Rheumatica (PMR) - high sensitivity, useful as adjunct to monitor course Other diseases variable, somewhat unreliable Non-rheumatic Disease Subacute Bacterial Endocarditis - high sensitivity Other diseases - may be helpful in monitoring treatment of osteomyelitis, inflammatory bowel disease, abscess

C-REACTIVE PROTEIN (CRP) Discovered in human serum, able to precipitate with c-polysaccharide of the pneumococcus Conserved in evolution (chickens,horseshoe crab, etc.) helpful to monitor inflammation/disease activity; less sluggish in its response (vs. ESR) - may change over hours range of abnormal values for CRP is greater than for ESR CRP tends not to rise much in lupus unless infection present - CRP > 10 mg/dl, 80+% have bacterial infections minor elevations in CRP may identify cardiac risk unknown: Is CRP better for assessing disease severity or predicting prognosis than ESR? What if they are discordant?

ESR vs. CRP ESR CRP Gender (Female) Age Pregnancy Drugs (e.g., steroids, NSAIDs) Smoking X X X X X Adapted from: Best Practice Advocacy Centre New Zealand http://www.bpac.org.nz/resources/campaign/crp_esr/crp_esr_rem.asp

CRP more sensitive (98.9% vs. 91.5%) and predicted relapse better than ESR ESR reflected response to treatment better (ESR high in 13%, CRP in 42% after 4 weeks of treatment) IL-6 was even better: persistent elevation predicted relapse

ESR vs. CRP for Temporal Arteritis 764 patients with ESR, CRP & temporal artery biopsy (23% of which were positive) Sensitivity of CRP = 87% Sensitivity of ESR = 84% Only 7 patients (4%) with a positive TAB for GCA CRP had a normal ESR and Kermaniet al. SeminArthritis Rheum. 2012; 41: 866

Symmetric, persistent polyarthritis in rheumatoid distribution

RHEUMATOID FACTOR Considered helpful: sensitive and However, specific, reliable, inexpensive, included among criteria for RA, present in other rheumatic disease. Sensitivity & specificity in RA are modest False positive test results are common & may outnumber true positive test results in many primary care settings. Prognostic information likely outweighs diagnostic information and results do not affect management.

Rheumatic diseases associated with a positive rheumatoid factor Disease Sensitivity Rheumatoid arthritis 50-90% SLE 15-35% Sjogren's syndrome 75-95% Systemic sclerosis 20-30% Polymyositis/ dermatomyositis 5-10% Cryoglobulinemia 40-100% Mixed connective 50-60% tissue disease

Non-rheumatic conditions associated with a positive rheumatoid factor Aging (>age 70) 10-25% Infection Bacterial endocarditis 25-50% Liver disease 15-40% Tuberculosis 10% Syphilis Parasitic disease up to 10% up to 90% Leprosy up to 60% Viral infection up to 60% Pulmonary Disease Sarcoidosis 3-33% Interstitial pulm. fibrosis 10-50% Silicosis 30-50% Asbestosis 30% Miscellaneous Diseases Primary biliary cirrhosis 45-70% Malignancy 5-25%

Pre-test probability makes all the difference Based on Sens = 0.7 & Spec = 0.85 for RF in RA:

Rheumatoid Factor Summary Moderately sensitive and specific Higher titers have higher specificity and positive predictive value Positive predictive value is low in most nonspecialty settings A negative test does not rule out disease (20-50% of RA patients are seronegative) High titer RF without rheumatic disease: think of cryoglobulinemia and SBE

Anti-cyclic citrullinated protein (anti-ccp) Anti-CCP antibodies - target citrulline, a modified form of arginine Sensitivity = 50-70% Specificity = 95-98%, correlates with erosive disease, can be present before symptoms May identify some RF-negative RA patients May identify some false+ RF patients (e.g., negative in patients with Hep. C)?Pathogenic - modest sensitivity argues against The bottom line: anti-ccp useful given its higher specificity but RA still cannot be diagnosed by a blood test.

Meta-analysis of 86 studies: Ann Intern Med. 2007;146:797-808. Sensitivity was similar for the 2 tests (67% vs. 69%) Specificity of anti-ccp was higher than RF (95% vs. 85%) anti-ccp antibody positivity is more specific than IgM RF positivity for diagnosing rheumatoid arthritis and early rheumatoid arthritis.

Criteria for RA The 2010 American College of Rheumatology/European League Against Rheumatism classification criteria for RA Criteria to apply to those who: have at least 1 joint with definite clinical synovitis synovitis not better explained by another disease A score of 6 out of 10 is needed for classification of a patient as having definite RA A. Joint involvement - 1 large joint: 0 2-10 large joints: 1 1-3 small joints: 2 4-10 small joints: 3 >10 joints (at least 1 small joint): 5

Criteria for RA (continued) B. Serology RF and anti-ccp both negative: 0 Low titer positive RF or anti-ccp: 2 High titer RF or anti-ccp: 3 C. Acute-phase reactants CRP and ESR both normal: 0 Either CRP or ESR elevated: 1 D. Duration of symptoms <6 weeks: 0 > 6 weeks: 1

Something new: multiple biomarker testing

Vectra testing: disease activity measure 12 biomarkers, including CRP, IL-6, serum amyloid A (largest contributors to score) Vectra scores correlate with clinical measures of disease activity (e.g., DAS28), x-ray changes Not for diagnosis, only for disease activity Marginal benefit uncertain

Photosensitive, malar rash sparing nasolabial fold, alopecia

An Emailed case... I sent an ANA on a young female patient with unexplained weight loss but not much else. Her ANA was 1:80, speckled. Would you make much of this in the absence of other symptoms?

ANA SENSITIVITY IN SELECTED DISORDERS DISEASE Systemic lupus erythematosus 95-99% Drug-induced lupus 100% Sjogren s Syndrome 75% Scleroderma 50-90% ANA sensitivity MCTD 99-100% RA 20-40% Other: autoimmune thyroid disease, hepatitis, PBC, infections

ANTINUCLEARANTIBODIES Useful to know: The ANA is highly sensitive (95-99%) in SLE, low specificity, lab variability; also sensitive for Sjogren s Syndrome, Scleroderma, Drug-Induced Lupus Maybe helpful to know: The higher the ANA titer, the more likely the result is a true positive Probably useless: The ANA pattern (diffuse, speckled, peripheral, nucleolar)

ANA SUBTYPES Also called specific autoantibodies, extractable nuclear antigens (ENAs), ANA panel Anti-ds-DNA (peripheral) and anti-sm (speckled) are highly specific, but not sensitive, for SLE Anti-Ro crosses placenta and mediates congenital CHB, neonatal lupus Any pattern/specificity may be noted in SLE - anti-ro (speckled) also common in Sjogren s, Scleroderma - anti-histone (diffuse) common in RA, aging, DILE - RNA staining (nucleolar) found in Scleroderma, RA, Sjogren s

Antinuclear antibody (ANA) Patterns Peripheral or Rim: anti-dsdna Diffuse: nonspecific Speckled: anti-ro or anti-sm Nucleolar: anti-rna

Antineutrophilic cytoplasmic antibody (ANCA) c-anca (cytoplasmic) Usually antiproteinase-3 (PR-3) p-anca (peri-nuclear) Often antimyeloperoxidase (MPO)

ANTI-NEUTROPHIL CYTOPLASMIC ANTIBODIES (ANCA) Rheumatic Disease: c-anca/pr3 p-anca/mpo Granulomatosis with polyangiitis 80% 10% Microscopic polyangiitis 20% 50% Eosinophilic Granulomatosis with polyangiitis (Churg-Strauss) 10% 40% Other vasculitides generally ANCA-negative: hypersensitivity, Henoch- Schönlein purpura (HSP), polyarteritis nodosa, GCA, Takayasu s Note: drug-induced vasculitis (especially PTU, hydralazine, minocycline) also associated with +p-anca/mpo; tainted cocaine may have both anti-mpo and anti-pr3 RA, SLE, Sjogren s, other rheumatic disease may be associated with nonspecific p-ancas (not directed against MPO)

ANTI-NEUTROPHIL CYTOPLASMIC ANTIBODIES (ANCA) ANCA in non-rheumatic disease: canca/ panca/ PR-3 MPO Idiopathic crescentic glomerulonephritis 10-20% 65-75% Anti-GBM Disease 10% 30-40% Nonspecific pancas (that is, not directed against MPO) also observed in: Ulcerative colitis Primary sclerosing cholangitis Cystic Fibrosis Autoimmune hepatitis Infection: leprosy, malaria, SBE (Pre)eclampsia, diffuse alveolar hemorrhage, graft-versus-host disease

ANCA to predict relapse? The correlation between ANCA level and disease activity is variable Ability of ANCA level & relapse depends in part on: - Disease phenotype, e.g., renal involvement or alveolar hemorrhage - Treatment, e.g., rituximab vs. cyclophosphamide Fussner LA, et al. Factors Determining the Clinical Utility of Serial Measurements of Antineutrophil Cytoplasmic Antibodies Targeting Proteinase 3. Arthritis Rheumatol. 2016;68:1700

ANCA: Summary It is not enough to know that the ANCA is positive Anti-PR3 and Anti-MPO are highly specific for crescentic GN, GPA (WG), related vasculitides Monitoring ANCA results in known ANCA-associated disease is of limited value In the proper clinical setting, ANCA results may be enough to warrant treatment without biopsy (but such settings are probably rare) A negative ANCA is the rule in largest and smallest vessel vasculitides Sensitivity and specificity are good but not perfect

The expanding role of ultrasound and MRI in Rheumatic Disease Ultrasound examples: MRI temporal arteritis - halo surrounding inflamed artery tendinitis - thickening of tendon with peritendinous fluid rotator cuff disease, including rupture erosions in rheumatoid arthritis early erosions in RA myositis

Ultrasound in joint and tendon disease Tendonitis Fluid Thickening Normal

Ultrasound and MRI: Sensitive for early erosions in inflammatory joint disease X-ray Erosion by MRI & US, missed by radiograph MRI Ultrasound

Ultrasound findings in gout & CPPD (pseudogout)

Ultrasound-guided joint aspiration

MRI inflammatory muscle disease (myositis)

Dual energy CT for diagnosis of gout http://therheumatologypodcast.com/podcast/dual-energy-ct-for-diagnosis-of-gout

DIAGNOSTIC TESTS IN RHEUMATIC DISEASE Most diagnostic tests in rheumatic disease are not diagnostic and have significant limitations Selective testing, rather than ordering panels, tends to provide more useful information Avoid the temptation to check ANA, RF, ESR in every patient with arthralgia, or ANCA for every patient with possible vasculitis Testing to rule-out disease in settings of low likelihood is often unhelpful - a negative test often does not exclude disease and a positive test may be confusing Anti-CCP is the first highly specific biomarker for RA Don t avoid checking non-exotic labs, e.g., urinalysis, CBC renal function Consider time as a diagnostic test of choice

DIAGNOSTIC TESTS IN RHEUMATIC DISEASE (2) What s old? ESR, RF, ANA, ANCA, radiographs What s new(er)? CRP, anti-ccp, MSK US, MRI Anti-CCP is the first highly specific biomarker for RA What s useful? Each one of the above when ordered selectively and interpreted in light of known limitations Stand by: CRP vs. ESR? How best to assess RA disease activity? Routine office use of musculoskeletal US? Dual energy CT for gout?

Thanks for your attention!