Rheumatoid Arthritis - PowerPoint PPT Presentation

1 / 49
About This Presentation
Title:

Rheumatoid Arthritis

Description:

Rheumatoid Arthritis Carole Callaghan Principal Pharmacist NHS Lothian Aim To update pharmacists on the current management of rheumatoid arthritis and explore ways to ... – PowerPoint PPT presentation

Number of Views:123
Avg rating:3.0/5.0
Slides: 50
Provided by: anne195
Category:

less

Transcript and Presenter's Notes

Title: Rheumatoid Arthritis


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
  • 31 ratio of femalesmales 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
    efficacytoxicity 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
  • -patients general health score
  • Monitoring
  • -FBC
  • -LFTs
  • -UEs
  • -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
TNF a - Mode of Action
29
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 gt5.1
  • 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
Write a Comment
User Comments (0)
About PowerShow.com