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Rheumatoid Arthritis

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Characterised by inflammation of the synovial tissue in joints, causing pain, ... Rheumatology referral is strongly recommended if symptoms persist for more than ... – PowerPoint PPT presentation

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Title: Rheumatoid Arthritis


1
Rheumatoid Arthritis
2
BackgroundNICE T.A. No 72, NICE draft scope for
RA, Nov 2006ODell JR. N Eng J Med 2004 350
2591602
  • RA is the most common inflammatory
    polyarthropathy in the UK
  • Affects between 0.5 and 1 of the population
  • Characterised by inflammation of the synovial
    tissue in joints, causing pain, swelling and
    stiffness and can lead to joint destruction
  • Life expectancy reduced by 510 years compared
    with that of people without the condition, and
    3550 of this excess risk is accounted for by
    cardiovascular mortality
  • Long-term prognosis for patients with RA depends
    not only on their joint disease but also on their
    co-existing illnesses

3
Diagnosis of early RASIGN 2000
  • Examination will usually show symmetrical
    swelling and tenderness of the small joints of
    the hands and feet (and to a variable extent the
    larger joints) and the presence of synovitis
    (i.e. soft tissue swelling in relation to the
    joint). Systemic 'flu-like' symptoms are not
    uncommon.
  • Essential aspects of the consultation
  • History
  • Pain
  • Stiffness after inactivity
  • Joint swelling
  • Fatigue
  • Examination
  • Affected joints
  • Synovitis vs. bony swelling/deformity
  • Range of movement
  • Extra-articular features

4
Therapeutic approaches the old and the newLee
DM, et al. Lancet 2001 358 90311PRODIGY 2005
SIGN 2000 NPC New Medicines Overview 2002
  • Pyramid approach
  • No longer recommended
  • Initial conservative management with NSAIDs for
    several years
  • DMARDs were withheld until clear evidence of
    erosions was seen
  • DMARDs then added individually in slow succession
    as the disease progressed
  • Oral corticosteroids, cytotoxics (e.g.
    cyclophosphomide)
  • Current approach
  • Early referral for diagnosis
  • Early treatment of diagnosed RA with DMARDs to
    control symptoms and delay disease progression

5
Early referral for specialist assessmentPRODIGY
2004 Emery P, et al. Ann Rheum Dis 2002 61
2907
  • Rheumatology referral is strongly recommended if
    symptoms persist for more than 6 weeks, even if
    there is a response to NSAIDs. Ideally, the
    person should be seen within 12 weeks of the
    onset of symptoms
  • Early referral from primary care to a
    rheumatologist is recommended in the event of
    clinical suspicion of RA, which may be supported
    by the presence of any of the following
  • Swelling of three or more joints
  • Involvement of the metacarpophalangeal or
    metatarsophalangeal joints or
  • Early morning stiffness of at least 30 min
    duration

6
3 steps to NSAID HeavenNational Prescribing
Centre
  • Dont use them unless you have to.
  • If you have to use them, use them wisely.
  • Use a safer drug (ibuprofen, then naproxen) in
    lowest effective dose for shortest period.
  • NSAID users should be a high priority for
    medication reviews.
  • Think about heart failure, hypertension and renal
    issues routinely.
  • Consider gastroprotection in those at high risk
    (NICE definition).
  • Options are misoprostol, PPIs, double dose H2RAs,
    and Cox-2s.
  • Cox-2s are not a panacea and the balance of
    benefits and risks (GI, CV, skin, renal, etc.)
    needs to be carefully assessed.
  • All of this particularly applies to those aged
    over 65

7
Steroids and DMARDsBSR guidelines 2006 Emery P,
et al. Clinical Evidence 2003 SIGN 2000 ODell
JR, et al. Ann Intern Med 2007 146 45960
  • Systemic steroid therapy beneficial in managing
    synovitis in early RA/flare or in bridging
    disease control between different DMARD therapies
    but long-term use is not justified
  • Conflicting evidence for a disease-modifying
    effect
  • Osteoporosis prevention should always be
    considered
  • Sulphasalazine, and methotrexate (MTX) are the
    current DMARDs of choice due to their more
    favourable efficacy/toxicity profiles
  • Leflunomide likely to be beneficial but can cause
    serious hepatic reactions and long-term safety is
    unclear
  • Patients with RA should be established on DMARDs
    as soon as possible after RA is diagnosed
  • But requires close monitoring under shared care
    arrangement
  • Best to start with a single DMARD /- steroids
    and escalate through dose increases and
    combination therapy as required

8
Biologic agents NICE TA 126 130 2007 BSR
guidelines April 2001 (updated 2005)
  • Adalimumab, etanercept and infliximab are
    recommended as options for the treatment of
    adults who have both the following
    characteristics
  • Active RA disease activity score (DAS28) gt 5.1
    on at least 2 occasions, one month apart
  • Have undergone trials of two DMARDs, including
    MTX (unless contraindicated)
  • TNF-alpha inhibitors should normally be used in
    combination with MTX. Where a patient is
    intolerant of MTX, or if MTX inappropriate,
    adalimumab and etanercept may be given as
    monotherapy
  • Continue treatment only if adequate response
    (improvement in DAS28 1.2 points) at 6 months
  • An alternative TNF-alpha inhibitor is recommended
    only where treatment is withdrawn due to ADRs
    before the initial 6 month assessment

9
Biologic agents (cont) NICE TA 126 and 130 2007
BSR guidelines April 2001 (updated 2005)
  • Escalation of doses above the licensed starting
    doses is not recommended
  • Normally initiate treatment with least expensive
    drug
  • Rituximab MTX is recommended as an option for
    the treatment of adults with severe active
    rheumatoid arthritis with inadequate response
    to/intolerance of other DMARDs, including at
    least TNF-alpha inhibitor
  • All patients need to be screened and closely
    monitored for TBcontinue for 6 months after
    discontinuing infliximab
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