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Juvenile Idiopathic
Arthritis (JIA)
Dr Urmila Dhakad
Assistant professor
Dept of Rheumatology
KGMU, Lucknow
23-06-15
Definition - Juvenile Idiopathic Arthritis
• Arthritis of unknown aetiology that begins
before the 16th birthday and persists for at least
6 wks.
• Previously known as juvenile rheumatoid
arthritis (JRA) and juvenile chronic arthritis (JCA).
Criteria for the diagnosis of JIA
All three conditions must be met
 Arthritis persisting for longer than 6 weeks
 Arthritis beginning before 16 years of age
 Exclusion of other conditions associated with
or mimicking arthritis
Classification of JIA
Based on symptoms presented during 1st 6 months of ds -
1. Systemic onset JIA ( 10-15% )
2. Oligo-articular JIA ( 50 % )
a. Persistent oligo-articular JIA
b. Extended oligo-articular JIA
3. Polyarticular JIA (RF negative) ( 15-20% )
4. Polyarticular JIA (RF positive) ( ≤5% )
5. Psoriatic arthritis (5-10%)
6. Enthesitis related arthritis ( 5-10% )
7. Undifferentiated arthritis ( 10-15% )
Systemic onset JIA (SOJIA)
• Quotidian, high spiking fever(> 2 wk) associated
with systemic features
Evanescent, non-fixed, erythematous rash
Hepato-splenomegaly
Serositis
Generalized lymphadenopathy.
Systemic onset JIA (SOJIA)
• Boys > girls.
• Myalgias and abdominal pain during fever
peaks.
• Arthritis - symmetrical and polyarticular; it may
be absent at onset and develop during disease
course.
Erythematous & evanescent rash of SOJIA. Frequently, rash
is obvious only at height of fever and sometimes confined
to axillary region, ant chest wall and inside both thighs.
Systemic onset JIA (SOJIA)
• Lab test - inflammatory response characterized
by leukocytosis, hyperferritinemia, microcytic
anaemia, thrombocytosis, high ESR and CRP .
• Diagnosis of SOJIA can be difficult, especially at
presentation, and D/D includes bacterial or viral
infection, malignancy, and other rheumatic ds.
Oligoarticular JIA
• Oligoarthritis - arthritis that affects 4 or less joints, in
absence of other features ( psoriasis, RF positivity, high
spiking fever). Characterized by –
 Female predilection
 Early onset asymmetric arthritis (before 6 years of age)
 Positive ANA & HLA associations.
 High risk for developing chronic iridocyclitis
Categories of Oligoarticular JIA
Persistent oligoarthritis - disease remains
confined to 4 or less joints.
Extended oligoarthritis - arthritis extend to > 4
joints after first six months of ds.
• Involvement of UL joints & high ESR at onset have
been identified as predictors for evolution to
extended type.
Polyarticular JIA (RF negative)
• Arthritis that affects 5 or more joints during first
6 months of disease in absence of RF.
• Two clinical phenotypes can be identified:
(1)Form that is closely similar to adult-onset RF
negative RA. characterized by symmetric synovitis
of large & small joints, high ESR and negative ANA.
Polyarticular JIA (RF negative)
(2) second form that resembles ANA +ve early-
onset oligoarthritis in every aspect other then
number of joint involved during first 6 months of
disease. characterised by early age at onset, +ve
ANA, asymmetric arthritis, female predominance,
high incidence of chronic iridocyclitis.
Polyarticular JIA (RF positive)
• Similar to adult RA. RF is by definition positive.
• Accounts for a small (≤5%) percentage of pts with JIA.
• Primarily affects girls and usually presents in late
childhood or adolescence.
• It can be rapidly progressive and destructive.
• Rheumatoid nodules are common.
• failure to thrive more frequent than in RF –ve type.
• Only JIA category in which Anti CCP are found.
Psoriatic arthritis (PsA)
• Diagnosis of PsA requires simultaneous presence of
arthritis and a typical psoriatic rash
or
• If psoriasis is absent, presence of arthritis plus any 2 of
following:
A) Family history of psoriasis in a first-degree relative;
B) Dactylitis (swelling of one or more digits )
C) Nail pitting.
Enthesitis related arthritis
• An undifferentiated spondyloarthritis.
• Typically begins after age of 6 years, affects boys > girls.
• Characterised initially by LL arthritis & enthesitis
(inflammation at insertion of tendon/ligament/fascia ).
• Most common sites of enthesitis are at insertion of
achilles tendon to calcaneum and insertions of plantar
fascia (calcaneum, base of 5th metatarsal & metatarsal
heads), and around & below patella.
Enthesitis related arthritis
• Hip involvement is frequent at presentation.
• Symptoms of sacroilitis and spinal arthritis are
uncommon at presentation.
• Uveitis - red eyes, photophobia and pain.
• Family history of similar disease is often +ve.
• HLA-B27 found in 50% of pts, while ANA is -ve.
Undifferentiated arthritis
• A category that includes patients who do not
fulfill inclusion criteria for any category, or
fulfill the criteria for more than one category.
• About 10-15% of all JIA cases are included in
this category.
Clinical features of JIA
• Pain
• joint swelling
• limping
• Early morning stiffness
Investigations in children with arthritis
• No diagnostic tests exist. It is a clinical diagnosis.
• Investigations have important role in excluding a
wide range of differential diagnoses.
• RF & ANA - are of no use for diagnosis. should
only be used after diagnosis has been made.
RF - help sub-classify children with polyarthritis
ANA - determining risk of chronic ant uveitis.
• Full blood count
• Acute phase response (CRP and ESR)
• ASO titers and other serology for infection.
• Coagulation studies (haemophilia)
• Autoantibodies (CTDs are suspected)
• Biochemistry -for muscle enzymes, endocrinopathies.
• Urine analysis and uinary catecholamines: to exclude
renal involvement or neuroblastoma
• Imaging -including plain x-rays of affected jts
may be useful to exclude fracture, AVN,
osteomyelitis, neoplasm and bone dysplasia.
• USG of jts is useful to confirm effusion and USG
of abdomen may help to exclude neuroblastoma.
• Aspiration of jt for synovial fluid microscopy and
culture is must in suspected septic arthritis.
Differential diagnosis of JIA
Child presenting with a single inflammed joint -
Septic arthritis : Staph aureus, H influenzae (non-
immunised), M tuberculosis, Salmonella (sickle
cell ds), Pseudomonas (puncture wounds).
Reactive arthritis: secondary to extra-articular
bacterial / viral infections e.g. strep, enteric
bacteria, hepatitis B, parvovirus, EBV, varicella.
 Haemarthrosis: trauma or bleeding diathesis
Malignancy: leukaemia or lymphoma should
always be considered. Most common is ALL.
Solid tumour
A child presenting with > 1 inflamed joint
Connective ts diseases: SLE, Dermatomyositis,
Sarcoidosis, MCTD, HSP.
Reactive arthritis
Malignancy
Immunodeficiency associated arthritis
IBD associated arthritis
Other: chronic recurrent multifocal osteomyelitis,
cryopyrin-associated periodic syndromes.
Child presenting with prominent systemic features
 Connective tissue diseases, Neoplasia
Infection, Inflammatory bowel disease
Auto-inflammatory disorders:
o characterised by recurrent fever and arthritis
often accompanied by abdominal pain & rash.
o Results of gene mutations and so present from
birth or at a very early age.
o Familial Mediterranean fever, hyper-IgD
syndrome, cryopyrin associated periodic fever
syndromes, TNF receptor associated syndromes.
Treatment of JIA
Goals of Treatment of JIA
• Suppression of inflammation
• Pain management
• Preservation of muscle strength
• Prevention of jt destruction, muscle atrophy,
asymmetric growth and other long-term
sequelae.
Treatment of JIA
Non-steroidal anti-inflammatory drugs (NSAIDs)
Used in higher doses relative to body weight,
than in adults because children have increased
rates of metabolism and renal excretion.
Majority of early JIA patients respond partialy to
NSAIDs and need more aggressive treatment.
• Glucocorticoids
Intra-articular steroids - Single injection resolves
signs of inflammation for several months
Pulses of IV methylprednisolone - For control of
severe systemic arthritis. lifesaving in case of
pericarditis with tamponade or MAS.
Oral steroids - Chronic use can lead to adverse
effects: growth and immune suppression, cataract,
DM, AVN, vertebral collapse and Cushing syndrome.
Disease modifying anti-rheumatic drugs (DMARDs)
Methotrexate - effective in approximately 70% of
children with polyarthritis but much less so in
systemic arthritis
Sulfasalazine - particularly effective in ERA. Also
efficacious in oligoarthritis and polyarthritis.
Leflunomide
Biologicals –
• Whose ds is not controlled with NSAIDs, steroids
and DMARDs or who are intolerant of it.
• Significantly alter natural history and stopped
progression of ds in a substantial portion of pts.
• Adverse events: infections, neutropenia, and
increased aminotransferase levels
TNF alpha blockers – Etanercept, Infliximab.
polyarthritis/extended oligoarthritis. less
effective in patients with systemic JIA.
 Anti IL-1 drugs – Anakinra, Canakinumab.
effective in pts with SOJIA
Anti IL-6 drugs – Tocilizumab. efficacious in
severe, persistent SOJIA
Other drugs
• Hydroxychloroquine - RF positive polyarthritis.
• Cyclosporine A - efficacious in treating MAS
associated with SOJIA.
• Cyclophosphamide – severe recalcitrant SOJIA for
whom even biological therapies are not working.
• Autologous stem cell transplantation - recalcitrant
SOJIA unresponsive to all other therapies.
Complications of JIA
(1) Macrophage activation syndrome (MAS):
• Occur in aprox. 7% of pts with systemic JIA.
• Secondary haemophagocytic histiocytosis
occurring in active ds.
• Associated with high morbidity and mortality.
Characterised by –
Diffuse intravascular coagulation.
Hepatosplenomegaly
Pancytopenia
Abrupt decrease in ESR
 High serum levels of ferritin, liver enzymes and
triglycerides.
Bone marrow examination shows active
Phagocytosis by macrophages and histiocytes.
 Treatment - MP pulse therapy and cyclosporine.
(2) Chronic anterior uveitis:
Most important complication of oligoarthritis.
Often clinically silent and insidiously progressive.
It is especially associated with +ve ANA. Every 3
monthly eye check up is suggested.
(3) Growth disturbance, atrophy, contrature, and
mis-alignment
are major concerns in chronic arthritis.
Successful control of ds and decreased use of
steroids have reduced this complication
(4) Cardiac disease:
Pericardial involvement occurs almost exclusively
with systemic-onset disease.
Myocarditis and endocarditis are much rarer
(5) Osteoporosis –
JAO and growth arrest lines are common.
Generalised OP may be observed, especially in
patients with a polyarticular course.
Other complicationsof JIA
(6) Intercurrent infections
(7) Anaemia
(7) Secondary amyloidosis
Summary
• Diagnosis - typical clinical features, persistent
swelling of 1 or more jts, before 16th b’day,
without any clear cause.
• Mimickers of JIA-septic arthritis, osteomyelitis,
neoplasia ( ALL), neuroblastoma and lymphoma.
• Subtypes -oligoarthritis, extended oligoarthritis,
ERA, PsA, RF -ve & RF +ve polyarthritis and SOJIA.
• No pathognomonic investigations for diagnosis.
Laboratory investigations may be helpful-
To exclude differential diagnoses (mimickers)
To sub-classify JIA
To monitor disease
• Multidisciplinary treatment is required including
nursing staff, physiotherapists, occupational
therapists and psychologists.
• Treatment for JIA - usually proceeds in a step-
wise escalating approach, beginning with
NSAIDs and I/A steroids, early use of DMARDs
for higher risk JIA groups.
• Biologicals - Anti TNF, IL-1 and IL-6, for SOJIA
which cannot be treated effectively with
methotrexate.
• Complications of JIA - chronic ant. uveitis,
dental decay, anaemia, osteoporosis and
growth disturbance.
• Life threatening complications & adverse
effects of Tx include sepsis, MAS, Reye
syndrome and amyloidosis.
Multiple choice questions (MCQs)
MCQ - 1
Following is true about systemic onset JIA-
A. It usually occurs in children under 5 yrs of age
B. Fever lasts for more then two weeks
C. Only cervical lymphadenopthy is seen
D. ANA is always present
E. DIC is a recognized complication
MCQ - 2
Following are true about oligo-articular JIA
except–
A. More common in females
B. It is usually seen after the age of 8 years
C. High risk for developing chronic iridocyclitis
D. Associated with ANA positivity
MCQ-3
All are true for Enthesitis related arthritis except -
A. Typically begins after age of 6 years
B. It affects boys more than girls.
C. Characterised initially by upper limb arthritis
D. HLA-B27 found in 50% of patients
E. ANA is negative.
MCQ-4
All are complications of JIA except -
A. Intercurrent infections
B. Pulmonary embolism
C. Anaemia
D. Osteoporosis
E. Chronic anterior uveitis
MCQ - 5
All are feutures of Macrophase activating syndrome
except -
A. Hepatosplenomegaly
B. Pancytopenia
C. Abrupt decrease in ESR
D. Low serum level of ferritin
E. Elevated levels of liver enzymes and triglycerides.
Juvenile Idiopathic Arthritis Diagnosis and Treatment

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Juvenile Idiopathic Arthritis Diagnosis and Treatment

  • 1. Juvenile Idiopathic Arthritis (JIA) Dr Urmila Dhakad Assistant professor Dept of Rheumatology KGMU, Lucknow 23-06-15
  • 2. Definition - Juvenile Idiopathic Arthritis • Arthritis of unknown aetiology that begins before the 16th birthday and persists for at least 6 wks. • Previously known as juvenile rheumatoid arthritis (JRA) and juvenile chronic arthritis (JCA).
  • 3. Criteria for the diagnosis of JIA All three conditions must be met  Arthritis persisting for longer than 6 weeks  Arthritis beginning before 16 years of age  Exclusion of other conditions associated with or mimicking arthritis
  • 4. Classification of JIA Based on symptoms presented during 1st 6 months of ds - 1. Systemic onset JIA ( 10-15% ) 2. Oligo-articular JIA ( 50 % ) a. Persistent oligo-articular JIA b. Extended oligo-articular JIA 3. Polyarticular JIA (RF negative) ( 15-20% ) 4. Polyarticular JIA (RF positive) ( ≤5% ) 5. Psoriatic arthritis (5-10%) 6. Enthesitis related arthritis ( 5-10% ) 7. Undifferentiated arthritis ( 10-15% )
  • 5. Systemic onset JIA (SOJIA) • Quotidian, high spiking fever(> 2 wk) associated with systemic features Evanescent, non-fixed, erythematous rash Hepato-splenomegaly Serositis Generalized lymphadenopathy.
  • 6. Systemic onset JIA (SOJIA) • Boys > girls. • Myalgias and abdominal pain during fever peaks. • Arthritis - symmetrical and polyarticular; it may be absent at onset and develop during disease course.
  • 7. Erythematous & evanescent rash of SOJIA. Frequently, rash is obvious only at height of fever and sometimes confined to axillary region, ant chest wall and inside both thighs.
  • 8. Systemic onset JIA (SOJIA) • Lab test - inflammatory response characterized by leukocytosis, hyperferritinemia, microcytic anaemia, thrombocytosis, high ESR and CRP . • Diagnosis of SOJIA can be difficult, especially at presentation, and D/D includes bacterial or viral infection, malignancy, and other rheumatic ds.
  • 9. Oligoarticular JIA • Oligoarthritis - arthritis that affects 4 or less joints, in absence of other features ( psoriasis, RF positivity, high spiking fever). Characterized by –  Female predilection  Early onset asymmetric arthritis (before 6 years of age)  Positive ANA & HLA associations.  High risk for developing chronic iridocyclitis
  • 10. Categories of Oligoarticular JIA Persistent oligoarthritis - disease remains confined to 4 or less joints. Extended oligoarthritis - arthritis extend to > 4 joints after first six months of ds. • Involvement of UL joints & high ESR at onset have been identified as predictors for evolution to extended type.
  • 11. Polyarticular JIA (RF negative) • Arthritis that affects 5 or more joints during first 6 months of disease in absence of RF. • Two clinical phenotypes can be identified: (1)Form that is closely similar to adult-onset RF negative RA. characterized by symmetric synovitis of large & small joints, high ESR and negative ANA.
  • 12. Polyarticular JIA (RF negative) (2) second form that resembles ANA +ve early- onset oligoarthritis in every aspect other then number of joint involved during first 6 months of disease. characterised by early age at onset, +ve ANA, asymmetric arthritis, female predominance, high incidence of chronic iridocyclitis.
  • 13. Polyarticular JIA (RF positive) • Similar to adult RA. RF is by definition positive. • Accounts for a small (≤5%) percentage of pts with JIA. • Primarily affects girls and usually presents in late childhood or adolescence. • It can be rapidly progressive and destructive. • Rheumatoid nodules are common. • failure to thrive more frequent than in RF –ve type. • Only JIA category in which Anti CCP are found.
  • 14. Psoriatic arthritis (PsA) • Diagnosis of PsA requires simultaneous presence of arthritis and a typical psoriatic rash or • If psoriasis is absent, presence of arthritis plus any 2 of following: A) Family history of psoriasis in a first-degree relative; B) Dactylitis (swelling of one or more digits ) C) Nail pitting.
  • 15. Enthesitis related arthritis • An undifferentiated spondyloarthritis. • Typically begins after age of 6 years, affects boys > girls. • Characterised initially by LL arthritis & enthesitis (inflammation at insertion of tendon/ligament/fascia ). • Most common sites of enthesitis are at insertion of achilles tendon to calcaneum and insertions of plantar fascia (calcaneum, base of 5th metatarsal & metatarsal heads), and around & below patella.
  • 16. Enthesitis related arthritis • Hip involvement is frequent at presentation. • Symptoms of sacroilitis and spinal arthritis are uncommon at presentation. • Uveitis - red eyes, photophobia and pain. • Family history of similar disease is often +ve. • HLA-B27 found in 50% of pts, while ANA is -ve.
  • 17. Undifferentiated arthritis • A category that includes patients who do not fulfill inclusion criteria for any category, or fulfill the criteria for more than one category. • About 10-15% of all JIA cases are included in this category.
  • 18. Clinical features of JIA • Pain • joint swelling • limping • Early morning stiffness
  • 19.
  • 20. Investigations in children with arthritis
  • 21. • No diagnostic tests exist. It is a clinical diagnosis. • Investigations have important role in excluding a wide range of differential diagnoses. • RF & ANA - are of no use for diagnosis. should only be used after diagnosis has been made. RF - help sub-classify children with polyarthritis ANA - determining risk of chronic ant uveitis.
  • 22. • Full blood count • Acute phase response (CRP and ESR) • ASO titers and other serology for infection. • Coagulation studies (haemophilia) • Autoantibodies (CTDs are suspected) • Biochemistry -for muscle enzymes, endocrinopathies. • Urine analysis and uinary catecholamines: to exclude renal involvement or neuroblastoma
  • 23. • Imaging -including plain x-rays of affected jts may be useful to exclude fracture, AVN, osteomyelitis, neoplasm and bone dysplasia. • USG of jts is useful to confirm effusion and USG of abdomen may help to exclude neuroblastoma. • Aspiration of jt for synovial fluid microscopy and culture is must in suspected septic arthritis.
  • 25. Child presenting with a single inflammed joint - Septic arthritis : Staph aureus, H influenzae (non- immunised), M tuberculosis, Salmonella (sickle cell ds), Pseudomonas (puncture wounds). Reactive arthritis: secondary to extra-articular bacterial / viral infections e.g. strep, enteric bacteria, hepatitis B, parvovirus, EBV, varicella.  Haemarthrosis: trauma or bleeding diathesis
  • 26. Malignancy: leukaemia or lymphoma should always be considered. Most common is ALL. Solid tumour A child presenting with > 1 inflamed joint Connective ts diseases: SLE, Dermatomyositis, Sarcoidosis, MCTD, HSP. Reactive arthritis
  • 27. Malignancy Immunodeficiency associated arthritis IBD associated arthritis Other: chronic recurrent multifocal osteomyelitis, cryopyrin-associated periodic syndromes. Child presenting with prominent systemic features  Connective tissue diseases, Neoplasia Infection, Inflammatory bowel disease
  • 28. Auto-inflammatory disorders: o characterised by recurrent fever and arthritis often accompanied by abdominal pain & rash. o Results of gene mutations and so present from birth or at a very early age. o Familial Mediterranean fever, hyper-IgD syndrome, cryopyrin associated periodic fever syndromes, TNF receptor associated syndromes.
  • 30. Goals of Treatment of JIA • Suppression of inflammation • Pain management • Preservation of muscle strength • Prevention of jt destruction, muscle atrophy, asymmetric growth and other long-term sequelae.
  • 31. Treatment of JIA Non-steroidal anti-inflammatory drugs (NSAIDs) Used in higher doses relative to body weight, than in adults because children have increased rates of metabolism and renal excretion. Majority of early JIA patients respond partialy to NSAIDs and need more aggressive treatment.
  • 32. • Glucocorticoids Intra-articular steroids - Single injection resolves signs of inflammation for several months Pulses of IV methylprednisolone - For control of severe systemic arthritis. lifesaving in case of pericarditis with tamponade or MAS. Oral steroids - Chronic use can lead to adverse effects: growth and immune suppression, cataract, DM, AVN, vertebral collapse and Cushing syndrome.
  • 33. Disease modifying anti-rheumatic drugs (DMARDs) Methotrexate - effective in approximately 70% of children with polyarthritis but much less so in systemic arthritis Sulfasalazine - particularly effective in ERA. Also efficacious in oligoarthritis and polyarthritis. Leflunomide
  • 34. Biologicals – • Whose ds is not controlled with NSAIDs, steroids and DMARDs or who are intolerant of it. • Significantly alter natural history and stopped progression of ds in a substantial portion of pts. • Adverse events: infections, neutropenia, and increased aminotransferase levels
  • 35. TNF alpha blockers – Etanercept, Infliximab. polyarthritis/extended oligoarthritis. less effective in patients with systemic JIA.  Anti IL-1 drugs – Anakinra, Canakinumab. effective in pts with SOJIA Anti IL-6 drugs – Tocilizumab. efficacious in severe, persistent SOJIA
  • 36. Other drugs • Hydroxychloroquine - RF positive polyarthritis. • Cyclosporine A - efficacious in treating MAS associated with SOJIA. • Cyclophosphamide – severe recalcitrant SOJIA for whom even biological therapies are not working. • Autologous stem cell transplantation - recalcitrant SOJIA unresponsive to all other therapies.
  • 37. Complications of JIA (1) Macrophage activation syndrome (MAS): • Occur in aprox. 7% of pts with systemic JIA. • Secondary haemophagocytic histiocytosis occurring in active ds. • Associated with high morbidity and mortality. Characterised by – Diffuse intravascular coagulation.
  • 38. Hepatosplenomegaly Pancytopenia Abrupt decrease in ESR  High serum levels of ferritin, liver enzymes and triglycerides. Bone marrow examination shows active Phagocytosis by macrophages and histiocytes.  Treatment - MP pulse therapy and cyclosporine.
  • 39. (2) Chronic anterior uveitis: Most important complication of oligoarthritis. Often clinically silent and insidiously progressive. It is especially associated with +ve ANA. Every 3 monthly eye check up is suggested. (3) Growth disturbance, atrophy, contrature, and mis-alignment are major concerns in chronic arthritis. Successful control of ds and decreased use of steroids have reduced this complication
  • 40. (4) Cardiac disease: Pericardial involvement occurs almost exclusively with systemic-onset disease. Myocarditis and endocarditis are much rarer (5) Osteoporosis – JAO and growth arrest lines are common. Generalised OP may be observed, especially in patients with a polyarticular course.
  • 41. Other complicationsof JIA (6) Intercurrent infections (7) Anaemia (7) Secondary amyloidosis
  • 42. Summary • Diagnosis - typical clinical features, persistent swelling of 1 or more jts, before 16th b’day, without any clear cause. • Mimickers of JIA-septic arthritis, osteomyelitis, neoplasia ( ALL), neuroblastoma and lymphoma. • Subtypes -oligoarthritis, extended oligoarthritis, ERA, PsA, RF -ve & RF +ve polyarthritis and SOJIA.
  • 43. • No pathognomonic investigations for diagnosis. Laboratory investigations may be helpful- To exclude differential diagnoses (mimickers) To sub-classify JIA To monitor disease • Multidisciplinary treatment is required including nursing staff, physiotherapists, occupational therapists and psychologists.
  • 44. • Treatment for JIA - usually proceeds in a step- wise escalating approach, beginning with NSAIDs and I/A steroids, early use of DMARDs for higher risk JIA groups. • Biologicals - Anti TNF, IL-1 and IL-6, for SOJIA which cannot be treated effectively with methotrexate.
  • 45. • Complications of JIA - chronic ant. uveitis, dental decay, anaemia, osteoporosis and growth disturbance. • Life threatening complications & adverse effects of Tx include sepsis, MAS, Reye syndrome and amyloidosis.
  • 47. MCQ - 1 Following is true about systemic onset JIA- A. It usually occurs in children under 5 yrs of age B. Fever lasts for more then two weeks C. Only cervical lymphadenopthy is seen D. ANA is always present E. DIC is a recognized complication
  • 48. MCQ - 2 Following are true about oligo-articular JIA except– A. More common in females B. It is usually seen after the age of 8 years C. High risk for developing chronic iridocyclitis D. Associated with ANA positivity
  • 49. MCQ-3 All are true for Enthesitis related arthritis except - A. Typically begins after age of 6 years B. It affects boys more than girls. C. Characterised initially by upper limb arthritis D. HLA-B27 found in 50% of patients E. ANA is negative.
  • 50. MCQ-4 All are complications of JIA except - A. Intercurrent infections B. Pulmonary embolism C. Anaemia D. Osteoporosis E. Chronic anterior uveitis
  • 51. MCQ - 5 All are feutures of Macrophase activating syndrome except - A. Hepatosplenomegaly B. Pancytopenia C. Abrupt decrease in ESR D. Low serum level of ferritin E. Elevated levels of liver enzymes and triglycerides.