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Rheumatoid Arthritis

Rheumatoid Arthritis. Carole Callaghan Principal Pharmacist NHS Lothian. Aim. To update pharmacists on the current management of rheumatoid arthritis and explore ways to implement pharmaceutical care for this patient group as part of normal working practice. Objectives.

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Rheumatoid Arthritis

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  1. Rheumatoid Arthritis Carole Callaghan Principal Pharmacist NHS Lothian

  2. Aim • To update pharmacists on the current • management of rheumatoid arthritis and • explore ways to implement • pharmaceutical care for this patient group • as part of normal working practice.

  3. Objectives • Describe the common signs and symptoms associated with rheumatoid arthritis. • Define the current therapeutic management for both the alleviation of symptoms and for modifying disease progression in rheumatoid arthritis. • Identify pharmaceutical care issues and appropriate management solutions when responding to symptoms in patient scenarios. • Explore how to implement the principles of a pharmaceutical care needs assessment tool in practice.

  4. Rheumatoid Arthritis • A chronic systemic inflammatory disease, characterised by potentially deforming symmetrical polyarthritis and extra-articular features.

  5. Epidemiology • prevalence approx. 1% in UK • 3:1 ratio of females:males affected • peak onset 40 and 50 years of age • genetic, environmental and infective factors involved in disease development

  6. Pathogenesis • cause remains unknown • toxic substances found in synovium • destruction of joints • immunological disturbances identified • RA is an autoimmune disease

  7. Pathology • disease of the synovium • inflammation due to infiltration of lymphocytes, macrophages etc • proliferation of cells results in ”pannus” formation

  8. Pathology

  9. Pathology

  10. Symptoms • joint pain (usually worse on waking) • morning stiffness (can vary in duration) • general symptoms e.g. fatigue, malaise, bone ‘ache’

  11. Signs • swelling • tenderness • reduced range of movement • deformities (if untreated over long-term) • extra-articular features e.g. nodules, anaemia of chronic disease, pleural effusion

  12. Signs

  13. Joint involvement • hands/wrists • elbows/shoulders • cervical spine • knees • ankles/feet • unpredictable pattern

  14. Investigation • Imaging e.g. x-ray, ultrasound, MRI • FBC and ESR • Other tests e.g RhF, anti-CCP (antibodies)

  15. Management (1st stage) • lifestyle – maintain where possible • multidisciplinary e.g. • physiotherapy • occupational therapy • podiatry

  16. Management (2nd stage) • relief of symptoms

  17. NSAIDs • more effective than simple analgesics • variation in response • balance efficacy • and toxicity

  18. NSAID toxicity • related to dose and duration of therapy • GI • renal and cardiovascular • elderly more at risk

  19. GI toxicity • well documented in literature • identifiable risk factors e.g. age, previous history, other medication (steroids, warfarin), alcohol • improved use secondary to identifying those at risk and using gastroprotection

  20. NSAID summary • use lowest dose compatible with symptom relief • use gastroprotection in “at risk” patient • reduce and, if possible, withdraw when good response from DMARD

  21. COX-2 Inhibitors • selectively block COX-2 isoenzyme • provide pain relief (as efficacious as NSAIDs) • less GI bleeding than NSAIDs (less significant GI symptoms remain e.g. dyspepsia) • CV risk??

  22. Management (3rd stage) • long-term suppressive drug therapy with disease modifying anti-rheumatic drugs (DMARDs)

  23. Early DMARD • stabilise joint function as early as possible = better outcome • greater awareness of NSAID toxicity • DMARDs slow disease progression

  24. DMARDs • efficacy .vs. toxicity • methotrexate and sulfasalazine have the best efficacy:toxicity ratio in meta-analyses • Increased use of combination therapy – TICORA, COBRA, BeST. • better than sequential monotherapy

  25. DMARDs (cont) • DAS28 (Disease Activity Score) • -swollen joints • -tender joints • -ESR • -patient’s general health score • Monitoring • -FBC • -LFTs • -U&Es • -BP • -urinalysis

  26. Systemic corticosteroids • not recommended for routine use • if necessary, use lowest dose, shortest time • monitor due to side effect profile

  27. Intra-articular corticosteroids • “target” joint i.e. one or two large joints affected, can avoid systemic steroid • maximum number per joint/time – but no evidence for this theory • evidence lacking for this practice, • but patients report benefit

  28. Activated Macrophage Target Cell sTNFR Signal TNF TNF a -Mode of Action

  29. Activated Macrophage Activated Target Target Cell Cell TNFR TNFR Signal Signal sTNFR sTNFR TNF TNF Anti-TNF Biologics - Mode of Action

  30. TNF a • Three agents currently licensed in UK and • SMC approved: • infliximab (human antichimeric antibody) • etanercept (fusion protein) • adalimumab (fully humanised monocloncal antibody)

  31. Effects of Blocking TNFa • Immunology •  RF, T cell function restored • Inflammation •  Cytokine production in joints (IL1, IL6, TNF) • Angiogenesis •  levels of angiogenesis • Joint destruction •  damage to bone and cartilage • Haematology •  platelets, fibrinogen, restoration of Hb

  32. B Cell Involvement in the Pathogenesis of RA

  33. Biologic Pathways

  34. Nomenclature • -ximab Chimeric antibody • -zumab Humanised antibody • -umab Human antibody • -cept Fusion protein

  35. Immunogenecity

  36. Eligibility Criteria for Biologic Therapy (BSR) • DAS28 >5.1 • At least 2 previous DMARDs • Adequate response at 3 months • 3-monthly monitoring

  37. Infection • Do not initiate in presence of serious • active infection or in patients at high risk • Discontinue in presence of serious • infection

  38. Tuberculosis • Screen for TB • Active TB needs to adequately treated • Prophylactic anti-TB therapy for potential latent • disease • Monitor during/after biologic; treat if required

  39. Other Infections • Listeria/salmonella • Varicella • HBV/HCV • HIV

  40. Vaccination • Data limited • Influenza and pnuemococcal • recommended (many also on MTX) • Hep B

  41. Malignancy • No increased risk of solid tumours or • lymphoproliferative disease • Investigate/stop therapy • Caution in pre-malignant conditions • Preventative skin care/ongoing surveillance

  42. Rituximab • With MTX only (SMC restricted use) • Inadequate response or intolerant of other • DMARDs, including at least one anti-TNF • By specialists in accordance with criteria

  43. Safety with Rituximab • Delay post-anti-TNF • Check immunoglobulins • Re-treat on clinical signs • Active infection, severe immunocompromised • Screen for hepatitis (B & C)

  44. Abatacept

  45. Abatacept (contd) • Selective T cell co-stimulation modulator – • blocks the co-stimulatory signal required for full • T cell activation • Not recommended by SMC and reserved for • refractory disease • Increase in efficacy after first year of treatment

  46. Tocilizumab

  47. Tocilizumab (contd) • Recommended by SMC for combination • therapy only i.e. with MTX • ADRs e.g. liver enzymes, neutropenia, • lipids etc . . . • Place in therapy?

  48. Certolizumab • Nanomolecule comprising a humanised • antibody fragment against TNF alpha with • a polyethylene glycol tail - designed • to increase bioavailability • RCTs show rapid improvement in disease • activity (ACR20) compared with placebo • and methotrexate • SMC outcome due May 2010

  49. Summary • RA = inflammatory & destructive • symptomatic relief • early disease modification

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