R arthiritis

Question 1

what is Inflammatory arthritis
symptoms

Answer 1

Group of diseases characterised by inflammation of the joints and often other tissues. Include (but are not limited to):
RA, psoriatic arthritis, ankylosing spondylitis, juvenile idiopathic arthritis.

Symptoms: typically characterised by joint pain (and joint swelling) and joint stiffness in the morning and also after inactivity, lasting more than 30 min.

Synovial inflammation i.e. synovitis is a predominant feature
Note: non-joint structures can also be affected (e.g. skin, eyes, lungs, heart).

Patients also often have:
Normochromic and normocytic anaemia: reduced numbers of normal-sized erythrocytes (red blood cells) with normal haemoglobin content which is associated with chronic disease.
Raised inflammatory markers: erythrocyte sedimentation rate (ESR) and also C reactive protein (CRP).

Question 2

what is rheumatoid arthritis (RA

Answer 2

RA is a chronic, disabling autoimmune disorder affecting 1% of UK population (0.5%-3% worldwide): 15% have severe disease.

Characterised by synovitis (synovial inflammation) of small and large joints, destruction of cartilage and bone.

Chronic symmetrical polyarthritis (unknown cause).

Pre-menopause, affects roughly 3x as many women as men (1:1 after menopause).

Can present at any age, but peak prevalence is seen between 40-60 years of age.

Gradual onset of symptoms most common; people usually present with joint pain and swelling:

Symptoms vary in severity and may ‘come and go’: periods of increased disease activity, i.e. flares, may alternate with periods of remission (i.e. when swelling and pain fade/disappear).

Question 3

causes of RA

Answer 3

We understand what causes inflammation in RA, but what exactly causes RA itself is unknown.
Proposed mechanism is:
Generalised, non-specific inflammatory response, localised tissue damage and release of neo-autoantigens leading to T cell activation (initiating event).
B cells activated and produce autoantibodies (e.g. rheumatoid factor and anti-cyclic citrullinated peptide (anti-CCP)) which form immune complexes, bind to complement, stimulating neutrophils to produce pro-inflammatory cytokines (e.g. IL-1, TNF-alpha) and chemokines.
Chronic inflammation seen in RA is maintained by e.g. rheumatoid factor and by continuous stimulation of macrophages which release pro-inflammatory cytokines and chemokines.

RA is a multifactorial disease: both genetic (accounts for ~60%!) and environmental factors play an important role.

Question 4

RA: pathology

Answer 4

RA is characterised by chronic synovitis (inflammation of synovial lining of joints, tendon sheaths or bursae): this is due to migration and retention of inflammatory cells at the site of inflammation.

In response to proinflammatory mediators, leukocytes and vascular cells are activated; T cells and other immune cells eventually extravasate from blood vessels into the synovium (the ‘inflammation zone’), where they are retained. New blood vessels formed.

Synovial hyperplasia, tissue grows out over cartilage surface, and forms a pannus.

Pannus destroys articular cartilage and subchondral bone, producing bony erosions.

Subcutaneous rheumatoid nodules may form

Question 5

RA: clinical features

Answer 5

Insidious (gradual) onset of pain.

Early-morning stiffness (lasting more than 30 minutes).

Swelling in small joints of hands and feet (symmetrical).

Joint capsules are weakened leading to instability, subluxation (partial dislocation) and deformity.

Multiple joints may become involved:
Wrists, elbows, shoulders, cervical spine, knees, ankles, feet.

Joint effusions (increased fluid in tissue surrounding the joint) and muscle wasting.

Question 6

RA: other manifestations

Answer 6

Non-articular features (tendons, ligaments, fascia):
Bursitis (inflammation/swelling of bursa).
Tenosynovitis (inflammation of the lining
of the tendon sheath around a tendon).

Extra-articular features (beyond joints):
Fever.
Fatigue.
Anaemia.
Nodules (present in <30% of cases).
Muscle wasting.
Sjögren’s syndrome (dry eyes and mouth due to destruction of epithelial exocrine glands; can also affect joints – autoimmune disease).
Carpal tunnel syndrome (median nerve compression: wrist).

People with RA have an increased risk of CVD (atherosclerosis), infection (commonly pulmonary) and osteoporosis.

Question 7

RA: initial investigations

Answer 7

suspected
refer to specialist opinion - (rheumatologist)
investigations
info and support after diagnosis
management

Refer urgently (even if normal acute-phase response, negative anti-CCP antibodies or rheumatoid factor, RF) if:
Small joints of hands or feet are affected.
> one joint is affected.
Been a delay of > 3 months between onset of symptoms and seeking medical advice.

Investigations for diagnosis of RA:
Offer blood test for RF in adults with suspected RA: have synovitis on clinical examination.
Consider anti-cyclic citrullinated peptide (CCP) antibody measurement in adults with suspected RA, if negative for RF.
X-ray the hands and feet (early in disease course) in adults with suspected RA and persistent synovitis: look for reduced joint space, erosion, deformities.

Question 8

RA: investigationsfollowing diagnosis

Answer 8

If anti-CCP antibodies present, or bone erosions are seen on X-ray  emphasise the importance for individual to monitor their condition, and seek quick access to specialist care, if:
Disease worsens.
They have a flare (review slide 4).

Question 9

what is treat-treat strategy

Answer 9

Disease activity scores (DAS): a measure used to assess response to treatment in RA: value is based on clinical assessment (e.g. number of swollen joints) and inflammation biomarkers (e.g. ESR, CRP). DAS28, remission: score of <2.6; low disease activity: score of ≤3.2.
Treat active RA in adults (or those at risk of developing RA) with the aim of achieving a target of remission, or low disease activity if remission is not achieved.

Question 10

what is Disease activity Score 28 (DAS28)

Answer 10

Mathematical formula calculates score based on:
Number of swollen joints (out of the 28),
Number of tender joints (out of the 28),
C reactive protein (CRP) and/or erythrocyte sedimentation rate (ESR) test results
Patient health assessment questionnaire

Generally, a DAS28 score of:
DAS28 > 5.1 indicates high disease activity
DAS28 of 3.2 to 5.1 indicates moderate disease activity
DAS28 of 2.6 to <3.2 indicates low disease activity
DAS28 < 2.6 indicates disease remission

Question 11

RA: non-pharmacologicalmanagement

Answer 11

Adults with RA should have access to:
Specialist physiotherapy:
Improve general fitness, encourage regular exercise.
Learn exercises to enhance joint flexibility, muscle strength.
Learn about short-term pain relief methods: transcutaneous electrical nerve stimulators (TENS) and wax baths.

Specialist Occupational therapy, if:
Have issues with everyday activities or hand function.

Hand exercise programmes (delivered by practitioner), if:
Not on a drug regimen.
Have been on stable RA drug regimen for >3 months.

Podiatrist, if have foot problems (discuss e.g. insoles).

Psychological interventions, i.e. stress management.

Question 12

Pharmacological options

Answer 12

Pharmacological treatments available for RA, which include:
Analgesics: non-steroidal anti-inflammatory drugs (NSAIDs).
Glucocorticoids (corticosteroids): e.g. prednisolone.
Disease-modifying anti-rheumatic drugs (DMARDs):
‘Traditional’ conventional synthetic DMARDs (cDMARDs): methotrexate, sulfasalazine, leflunomide, gold salts, antimalarials (hydroxychloroquine), D-penicillamine, etc.
Biological DMARDs (bDMARDs): sarilumab, adalimumab, etanercept, infliximab, certolizumab pegol, golimumab, tocilizumab, abatacept, etc.
Targeted synthetic DMARDs (tsDMARDs): tofacitinib (first Janus Kinase [JAK] inhibitor, ‘jakinibs’, approved for treatment of RA), fostamatinib, baricitinib, apremilast, etc.

Question 13

RA: initial treatment

Answer 13

Adult with newly diagnosed RA

First line - cDMARD monotherapy: (oral) methotrexate, leflunomide or sulfasalazine (within 3 months of persistent symptom presentation (Consider hydroxychloroquine as 1st line as an alternative to these cDMARDs for mild or palindromic disease*)

Not effective, even after dose escalation

STEP up stratergy
Offer additional cDMARD (combination): (oral) methotrexate, leflunomide, sulfasalazine or hydroxychloroquine if target treatment not achieved
(Consider short-term bridging treatment with glucocorticoids (oral, intramuscular or intra-articular) when starting a new cDMARD.)
-> Step-down strategy: adults who have maintained treatment target for 1 year+ without glucocorticoids, consider cautiously reducing drug doses, or stopping drugs

Inadequate response to cDMARDs

Combine sarilumab (bDMARD) with methotrexate to treat active RA in adults if: (a) disease is severe (DAS28 >5.1), (b) company provides sarilumab with discount.
->
Consider sarilumab as monotherapy for people who cannot take methotrexate (contraindicated or intolerance)

or
DMARD naive - Adalimumab, etanercept, infliximab, certolizumab pegol, golimumab, tocilizumab and abatacept (bDMARDs)
all in combination with methotrexate to treat active RA in adults if: (a) disease is severe (DAS28 >5.1), (b) disease not responded to intensive therapy with combination of cDMARDs, (c) companies provide.
->
Adalimumab, etanercept, certolizumab pegol or tocilizumab as monotherapy for people who cannot take methotrexate (contraindicated or intolerance)

Continue treatment only if there is a moderate response at 6 months after starting therapy.

MODERATE TO SEVERE RA:
Tofacitinib (tsDMARD) with methotrexate (or as monotherapy if methotrexate issues as above); same for baricitinib (tsDMARD).

If inadequate response or intolerance to bDMARDs, and
rituximab is suitable, then combine with methotrexate…

Question 14

NSAIDs/COX-2 inhibitors
example
use

Answer 14

Relieve pain and stiffness (i.e. used only for symptom control); they do not slow RA disease progression (i.e. are not DMARDs).

NSAIDs should be used at the lowest dose and for the shortest time possible (e.g. ibuprofen 200-400mg tbs).

Gastric protection is recommended: proton pump inhibitors e.g. lansoprazole.

Pain relief is rapid (full effect obtained within 1 week) but anti-inflammatory effect of NSAID(s) may take up to 3 weeks.

Individual response to different NSAIDs varies considerably despite their similarity:
60% of patients will respond to any NSAID.
Those that do not respond to one NSAID will respond to another.

Slow-release preparation at night can help morning symptoms (stiffness).

Question 15

corticosteroids
use
caution

Answer 15

Bridging treatment: glucocorticoids are used for a short period of time when a person is starting a new DMARD:
Intention is to improve symptoms while waiting for the new DMARD to take effect (as it can take 2-3 months).

Managing flares:
Offer short-term treatment in adults with recent or established disease to rapidly decrease inflammation.

Long-term use of glucocorticoids:
Only for those with established RA when long-term complications have been discussed, and when all other treatment options have been offered.

Concerns over long-term safety: infections, diabetes, osteoporosis, gastrointestinal and cardiovascular events.

Question 16

Methotrexate (MTX)
use
monitoring
route of admin

Answer 16

A cDMARD, methotrexate is commonly used for treatment in RA, others forms of inflammatory arthritis, autoimmune diseases (Crohn’s disease) and in cancer.

A folic acid analogue, it inhibits dihydrofolate reductase, the rate-limiting enzyme in tetrahydrofolate production, which is required for DNA synthesis, it reduces cell division in immune cells, suppressing cell-mediated immunity.

Response often seen in 4-6 weeks.

MTX is commonly used but is associated with a high risk of adverse effects:
RA: 50% stop treatment <2 years due to adverse effects, or lack of efficacy.

Careful monitoring is required to detect/prevent occurrence of serious adverse effects such as, bone marrow suppression, renal impairment, liver fibrosis or cirrhosis, pulmonary fibrosis

Route of administration: can be given by oral, subcutaneous (SC), and intramuscular (IM) routes. Low dose, oral MTX, is commonly used to treat RA
Adults with moderate to severe RA: 7.5mg (oral) once weekly, adjusted according to response; max. weekly dose of 20mg.
Adults with severe active RA: SC or IM injection: 7.5mg once weekly, 2.5mg incremental steps according to response; max. weekly dose of 25mg.

MTX: its inhibition of cellular turnover often leads to associated side effects (e.g. bone marrow suppression, stomatitis, etc):
reduce risk of some adverse effects (especially mucosal or GI side effects) with a once weekly folic acid supplement (oral: 5 mg, dose to be taken on a different day to MTX dose).

Question 17

Sulfasalazine
side effect
dose

Answer 17

cDMARD: exact mechanism of action in treatment of RA is not known:
Immunosuppressant actions (possibly by scavenging toxic oxygen metabolites produced by neutrophils).

Effective in 70% of patients after 1 year.

Initially 500mg daily (oral), increased in 500mg intervals weekly; max of 2-3g daily in divided doses.

Common side effects: GI disturbances, fever, headache, rashes, blood disorders; frequency not known: yellow discolouration of body fluids (tears).

Blood counts and liver function tests required monthly for first 3-6 months.

Folic acid supplements (same as for methotrexate) may be required to counteract impaired folic acid absorption.

Question 18

Leflunomide

Answer 18

cDMARD with immunosuppressant effects: potent inhibitor of pyrimidine synthesis which affects T cell proliferation and, thus, is immunomodulatory.

Licensed for moderate to severe active RA; therapeutic effect after 4-6 weeks.

Active metabolite of leflunomide persists for a long time (long half-life) which can be a concern if serious adverse effects are experienced.

Severe adverse effects include bone marrow toxicity, hepatotoxicity, increased risk of infection and malignancy.

Patients must be monitored; Blood counts and liver function.

Common side effects: GI disturbance, decreased appetite, hypertension, headache, dizziness, accelerated hair loss.

Question 19

Antimalarials

Answer 19

Exact mechanism of action in treatment of RA is poorly understood:
Direct anti-inflammatory effect by stabilising lysosomes, inhibiting the release of lysosomal enzymes, hence, inhibiting their inflammatory effects.

Hydroxychloroquine is used to treat RA of moderate inflammatory activity:
Well tolerated with effect observed within 1-3 months.
200-400mg daily (oral), max 6.5 mg/kg per day (very toxic in overdosage!)

Antimalarials (which includes chloroquine) may cause retinopathy: ocular toxicity (keep to recommended doses):
Adults who have taken hydroxychloroquine > 5 years are recommended to be annual screened for potential retinopathy.

Question 20

Cytokine modulators:‘Biologics’

Answer 20

bDMARDs only used under specialist supervision.

Used for highly active RA if patient has failed to respond to at least 2 cDMARDs (including methotrexate unless it is contraindicated): SC or IV injection.

Often given in combination with methotrexate (unless it is contraindicated).

Common side effects: increased risk of infections (caution in those exposed to tuberculosis; hepatitis B reactivation, septicaemia), dyslipidaemia, nausea, vomiting, abdominal pain, worsening heart failure, hypersensitivity, fever, headache, depression, injection site reactions, blood disorders (anaemia).

Continue treatment only if there is a moderate response at 6 months after starting therapy.

Question 21

Cytokine modulators:‘Biologics’
examples

Answer 21

Tumour necrosis factor alpha (TNF-α) inhibitors:
Infliximab (the first TNF inhibitor), adalimumab and golimumab are anti-TNF (human/mouse) monoclonal antibodies.
Etanercept is a recombinant fusion protein of TNF receptor fused to Fc region of human IgG.
Certolizumab pegol is a recombinant Fab antibody fragment.

Other bDMARDs may be considered if patient does not respond to above:
Rituximab is a chimeric anti-CD20 monoclonal antibody; depletes CD20+ve B cells.
Abatacept (the first co-stimulation blocker) is a recombinant fusion protein, CTLA-4 -immunoglobulin molecule that inhibits T cell stimulation.
Tocilizumab (the first IL-6 inhibitor), and sarilumab are humanised monoclonal antibodies to IL-6 receptor.

Question 22

Targeted synthetic DMARDS
side effects

Answer 22

Developed as up to 30% of RA patients still may not respond adequately.

tsDMARDs, ‘Jakinibs’: Tofacitinib was the first Janus Kinase (JAK) inhibitor was approved in the US in 2012 (Pfizer):
Oral, monotherapy (baricitinib, tofacitinib), or in combination with methotrexate for treatment of moderate to severe active RA in patients who had an inadequate response to, or who are intolerant to, one or more DMARDs.

Side effects: increased incidence of infection, hypercholesterolaemia (lipids), reduce lymphocyte numbers, lower haemoglobin levels.

Question 23

summary:
bDMARD treatments in RA targeting proinflammatory cells and cytokines to inhibit progression of joint inflammation and destruction. Abbreviations: DC, dendritic cell; IL, interleukin.

Overview of the inflammatory process in the synovium and mechanism of action of drugs (cDMARDs and bDMARDs) used to treat RA. Note: interaction between T and B cells often results in the production of rheumatoid factor (RF) and other autoantibodies. Abbreviations: HLA, human leukocyte antigen; NF-κB, nuclear factor κB.