Lec 44- RA

Question 1

What is it

Answer 1

• Most common autoimmune disease
• Chronic, progressive, system inflammatory disorder (including cardiovascular system)
• Affects synovial joints
• Many non-articular manifestations, some of which decrease life expectancy
• Causes significant disability

Question 2

Who is affected

Answer 2

• 1% of UK population
• Decrease in past few years
• 2-3 times more common in women
• Increased prevalence with age
• Peak incidence 30-50 years

Question 3

What causes RA

Answer 3

• Unknown
• Genetic
• Hormones
• Cigarettes
• Infection

Question 4

How does it present

Answer 4

• Typically- slowly progressive, symmetrical peripheral polyarthritis, evolving over few weeks or months
• Pain and stiffness of the small joints of hands and feet; patients fell tired and unwell
• Also writes, elbow, shoulders, knees and ankles
• Joints are warm and tender, with swelling; stiffness especially morning; limited moment and muscle wasting
• Occasionally mono arthritis
• Occasionally very sudden

Question 5

RA in hands

Answer 5

• Early disease- swelling and early joint damage

- Late disease- deformity and contractures

Question 6

Co-morbities

Answer 6

• MI, HF, CVA, CVD, HTN
• Lymphoma and lymphorproliferative diseases
• Lung cancer, skin cancer
• Infections (disease and treatment)
• Depression, GI disease, osteoporosis, psoriasis, renal disease (disease and treatment)

Question 7

Pathophysiology- much simplified

Answer 7

• Widespread inflammation of synovium- thickens
• Infiltration by inflammatory cells
• Synovium spreads onto the cartilage surface (pannus) damaging it
• Cartilage thins; underlying bone exposed -> damage (osteoclasts stimulated)
• Key inflammatory cells include T cells, B cells, macrophages and plasma cells.
• Key inflammatory mediators: Cytokines: IL-6, IL-1 and TNFa
• AutoAbs such as rheumatoid factor and citrullainated peptides activate the complement system –> stimulates macrophages

Question 8

How is RA diagnosed

Answer 8

-Patient history
-Presenting symptoms/clinical examination
-American college of Rheumatology classification criteria- poor sensitivity for early disease
CLINICAL TESTS
-increase ESR and CRP
-Increased platelet count
-Rheumatoid factor- IgM present in 75-80% of patients with RA (seropositive) and 5% of patient without RA
-Anti-cyclic citrullinated peptides (anti-CCP) Abs is more specific (90-96%
-Anaemia of chronic disease (norm chromic, normocytic)- will not respond to Fe treatment
-Radiology- X-ray, MRI, Ultrasound

Question 9

Monitoring disease

Answer 9

-Symptoms and clinical markers (CRP)
-NICE refers to DAS28- disease activity score which has 4 parameters
1) Number of swollen joints out fo a total of 28 specific joints
2)Number of tender joints out of total of 28 specified joints
3)Erythrocyte sedimentation rate
4)Patients interpretation of wellbeing
Disease activity
High= >5.1
Moderate= 3.2-5.1
LOW= 2.6-3.2
Remission <2.6

Question 10

Management

Answer 10

Multidisciplinary team

• Medical- shared care
• Specialist RA nurses
• Pharmacists
• Psychology
• Occupational therapy
• Physiotherapy
• Podiatry- patient education is very important

Question 11

Management

Answer 11

-Early diagnosis is important
-Analgesics and NSAID only useful for:
+Symptoms relief including pain control
-Corticosteroids, DMARDs and biologics
+Slowing or prevention of joint damage
+Preserving and improving functional ability
+Acheiving and maintaining remission

Question 12

Analgesics and NSAIDs

Answer 12

-Analgesics- adjunct for pain relief
+NSAIDs- analgesic and anti-inflammatory effect, but only provide symptomatic relief
-Use lowest dose possible and withdraw if possible once patient response to DMARD
-Side effects: GI (ulcers); Renal; CV (Na and water retention), increase risk of stroke and MI

Question 13

Corticosteroids

Answer 13

• Inhibit cytokine release
• Rapid relief of symptoms/ decrease inflammation
• Long term oral steroids associated with long term side effects
• Oral therapy- bridging therapy until respond to DMARD (withdraw slowly)
• Intra-articular injection into target joint

Question 14

Disease modifying anti-rheumatic drugs

Answer 14

• The sooner the better to prevent damage
• Ideally within 3 months of start of persistent symptoms
• NICE- first line treatment is a combination of DMARDs, unless inappropriate; if so mono therapy
• Regimen, unless C/I’d should contain- methotrexate

Question 15

Biological response modifiers

Answer 15

• Huge change in management of RA in past decade
• Currently only used if DMARDs fail- NICE
• Specialist supervision
• Expensive
• Balance cost of treatment Vs cost of disability

Question 16

Biological response modifiers (2)

Answer 16

-TNFa blocker (1st line)
+Adalimumab, certolizumab, etanercept, infliximab
-JAK inhibitor- baracitinib, tofacitinib
-IL-6 antagonist- Toclilizumab
-T cell co-stimulation modulator- abatacept
-B-cell depleting- rituximab

Question 17

Biologic response modifiers

Answer 17

• Given along with DMARD e.g. MTX
• Assessment using DAS28 at least every 6 months
• Continue if improvement in DAS28 of 1.2 points or more
• All given by injection- mostly s/c but some by infusion (big proteins), except JAK inhibitors
• Different regimens- daily twice weekly, weekly, 2 weekly, 4 weekly
• Not just licensed for RA, other inflammatory diseases including Chrons and UC

Question 18

Biological response modifier- problems

Answer 18

• Increased risk of infection , particularly TNF-a inhibitors
• Particularly reactivation latent TB (screen before commencing Tx)
• Rituximab associated with 3 cases of progressive multifocal leukoencephalopathy (damage to brain white matter)
• Injection site and infusion reactions
• TNF-a inhibitors C/Id in advanced HF