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Dr. Müge Bıçakçıgil Kalaycı
ADULT ONSET STILL DISEASE
 Multi-system inflammatory disease
 begins with a sore throat
 may develop days to weeks before
 the typical quotidian fever
 Rash
 Joint pains
ETIOLOGY
 no etiologic factor has been identified
 Infectious??
 prodromal sore throat
 fever
 Possible mechanism;
- viral agent initiates a cascade of the immunological
events resulting in the characteristic clinical syndrome
of AOSD.
 Implicated organisms in AOSD
-Rubella
-Ebstein Barr
-Staphylococcus
-Parvovirus
-Yersinia enterocolitica
Brucela abortus
-Mycoplasma
-Borelia burgdoferi
-Cytomegalovirus
-Mumps
-Parainfluenza
Clinical Features
Common Clinical Features
*Fever of at least 39ºC lasting one week or longer
*Arthralgias or arthritis lasting two weeks or longer
*Characteristic rash which is a macular or
maculopapular, nonpruritic, salmon-pink
eruption usually apparent over the trunk or
extremities during febrile episodes
* Leukocytosis (10,000/µL or greater) with 80
percent or more granulocytes
* Sore throat
* Recent development of significant lymph node swelling
* Hepatomegaly or splenomegaly
*Abnormal liver function studies, particularly
aminotransferases and lactate dehydrogenase
*Negative tests for antinuclear antibody and rheumatoid
factor
FEVER
 Quotidian or "double-quotidian" with a brief peak
in the late afternoon or early evening.
 Temperature swings can be dramatic, with changes
of 4ºC occurring in four hours.
 Approximately 20 percent of cases, fever persists
between spikes.
 Over 99 % of patients manifest with fever > 39 0 C
FEVER
 The febrile paroxysms are cyclic and tend to recur every 24 or
sometimes every 12 hours. Characteristically very high in the
evening, returning to normal by morning.
 Paroxysms are heralded by shaking chills, followed by 2-4
hours of high fever (> 104°F), and ending with defervescence
and drenching sweats
 Still's rash is seen in 86% of patients
 Periodic appearance and location
 Appears during febrile attacks and may last for several
hours
 It is typically salmon-colored (infrequently
erythematous), maculopapular and may be confluent
or show areas of central clearing.
 Trunk, neck, extremity( extensor surface)
RASH
RASH
 Usually the face, palms, and soles are spared.
 Dermatographism: is an exaggerated cutaneous
urticarial response to cutaneous stimuli (ie, the
scratch test).
 Rash is typically nonpruritic.
Articular Manifestations
 Arthralgias dominate the early clinical picture
 During the first 6 mos. the onset of polyarthritis is
expected in > 90% of patients and may involve large and
small articulations
 Myalgias
 Affected joints: the knees, wrists, ankle, elbow, shoulder,
PlPs, DlPs, TMJ and cervical spine.
 Bony ankylosis of carpal, carpometacarpal. Intertarsal
joints
 Erosive and destructive polyarthritis, especially in those
with a chronic polyarticular course
Reticuloendothelial Disease
 Splenomegaly
 Very common early in the disease and reflects tissue infiltration with inflammatory
cells and heightened immunologic activity within the reticuloendothelial system (RES).
 Palpable or radiographic demonstration of splenomegaly is seen in 42% of individuals
 Hepatomegly
 40% of patients are found to have hepatomegaly
 70% demonstrate abnormalities of hepatic enzymes at some time during their illness
Lymphadenopathy
 65% of AOSD patients.
 Generalized mild to moderate nodal enlargement of
nontender lymph nodes located in the cervical, axillary,
epitrochlear, or inguinal regions.
 Mesenteric, para-aortic and hilar nodes may be discovered
during diagnostic imaging
 SEROSITIS

 Pleuritis (40%)
 Pleural effusions are usually bilateral, seldom large enough
to be symptomatic, and rarely produce pleural thickening.
 Thoracentesis often yields bloody, exudative effusions with
white blood cell counts ranging from 3-20 x 103/mm3 with a
polymorphonuclear predominance.
 Pneumonitis
 Pneumonitis is found in over 20% of patients
 These individuals often appear septic with complaints of
fever, dry cough, dyspnea and are found to have pulmonary
infiltrates that are unresponsive to anti-infective therapy
 Infiltrates tend to be bilateral more commonly than
unilateral, alveolar or interstitial in pattern and responds
well to anti-inflammatory therapy with steroids
Laboratory
Investigations
Absence of antinuclear antibodies
Absence of rheumatoid factor,
Elevated ESR and C-reactive protein
Neutrophilic leukocytosis
Elevated serum amyloid A
Thrombocytosis
Elevated serum ferritin and
glycosylated ferritin
Elevations the hepatic enzymes
Hypoalbuminemia
 Leukocytosis
 Leukocytes counts generally range between 12,500-40,000 cells/mm3,
with the highest recorded to be 69,000
 ESR
 90% of AOSD patients have an ESR > 50 mm/hr and 50% have and
ESR > 90 mm/hr.
 Hyperferritinemia
 It has been suggested that extreme elevations of the
acute phase reactant, ferritin, may be of diagnostic value
in assessing patients with AOSD
 Hyperferritinemia with values between 4000 30,000
mg/ml have often been reported in association with the
onset and/or flare of disease activity
 Levels as high as 250,000 mg/ml have been reported
AOSD.
Diagnosis
 Diagnosis
 Still disease lacks serologic test or histopathology and
thus, remains a clinical diagnosis of exclusion.
 AOSD is now being considered earlier in the course of
evaluation of patients with fever, dermatitis and
arthritis.
 Diagnostic steps should include a comprehensive,
noninvasive workup, documentation of fever pattern
 Yamaguchi et al 1992
 AOSD Total of > 5 criteria (including 2 major)
 Major Criteria Minor Criteria
Fever > 39°C Sore throat
Arthralgia > 2 wks. LN or splenomegaly
Still's rash Liver dysfunction
Neutrophilic leukocytosis Negative RF & ANA
 specificities greater than 92%, the sensitivity of Yamaguchi
(96%)
Treatment
Treatment
 NSAIDS or Aspirin
 Mild disease with no life- threatening visceral involvement
 20-25 % respond (good prognosis group with mild disease
activity)
 Aspirin or an NSAID should be continued for one to three
months following disease remission.
 GLUCOCORTICOSTEROIDS
 Patients with very high fever,
 Joint involvement that is disabling
 Potentially life-threatening visceral involvement
(myocarditis)
 Starting dose of 0.5 to 1.0 mg/kg per day PO
 Immunomodulating drugs
 There are no controlled trials assessing the efficacy of any
of the immunomodulating drugs in ASD
 * Intramuscular gold salts
 * Hydroxychloroquine,
 * Azathioprine,
 * Cyclophosphamide,
 * Cyclosporine,
 * Sulfasalazine,
 * Methotraxate
 * Intravenous immune globulin,
 * Anti-TNF-alpha agents

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Adult Onset Still Disease Symptoms & Treatment

  • 2. ADULT ONSET STILL DISEASE  Multi-system inflammatory disease  begins with a sore throat  may develop days to weeks before  the typical quotidian fever  Rash  Joint pains
  • 3. ETIOLOGY  no etiologic factor has been identified  Infectious??  prodromal sore throat  fever  Possible mechanism; - viral agent initiates a cascade of the immunological events resulting in the characteristic clinical syndrome of AOSD.
  • 4.  Implicated organisms in AOSD -Rubella -Ebstein Barr -Staphylococcus -Parvovirus -Yersinia enterocolitica Brucela abortus -Mycoplasma -Borelia burgdoferi -Cytomegalovirus -Mumps -Parainfluenza
  • 6. Common Clinical Features *Fever of at least 39ºC lasting one week or longer *Arthralgias or arthritis lasting two weeks or longer *Characteristic rash which is a macular or maculopapular, nonpruritic, salmon-pink eruption usually apparent over the trunk or extremities during febrile episodes * Leukocytosis (10,000/µL or greater) with 80 percent or more granulocytes
  • 7. * Sore throat * Recent development of significant lymph node swelling * Hepatomegaly or splenomegaly *Abnormal liver function studies, particularly aminotransferases and lactate dehydrogenase *Negative tests for antinuclear antibody and rheumatoid factor
  • 8. FEVER  Quotidian or "double-quotidian" with a brief peak in the late afternoon or early evening.  Temperature swings can be dramatic, with changes of 4ºC occurring in four hours.  Approximately 20 percent of cases, fever persists between spikes.  Over 99 % of patients manifest with fever > 39 0 C
  • 9. FEVER  The febrile paroxysms are cyclic and tend to recur every 24 or sometimes every 12 hours. Characteristically very high in the evening, returning to normal by morning.  Paroxysms are heralded by shaking chills, followed by 2-4 hours of high fever (> 104°F), and ending with defervescence and drenching sweats
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  • 11.  Still's rash is seen in 86% of patients  Periodic appearance and location  Appears during febrile attacks and may last for several hours  It is typically salmon-colored (infrequently erythematous), maculopapular and may be confluent or show areas of central clearing.  Trunk, neck, extremity( extensor surface) RASH
  • 12. RASH  Usually the face, palms, and soles are spared.  Dermatographism: is an exaggerated cutaneous urticarial response to cutaneous stimuli (ie, the scratch test).  Rash is typically nonpruritic.
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  • 16. Articular Manifestations  Arthralgias dominate the early clinical picture  During the first 6 mos. the onset of polyarthritis is expected in > 90% of patients and may involve large and small articulations  Myalgias
  • 17.  Affected joints: the knees, wrists, ankle, elbow, shoulder, PlPs, DlPs, TMJ and cervical spine.  Bony ankylosis of carpal, carpometacarpal. Intertarsal joints  Erosive and destructive polyarthritis, especially in those with a chronic polyarticular course
  • 18.
  • 19. Reticuloendothelial Disease  Splenomegaly  Very common early in the disease and reflects tissue infiltration with inflammatory cells and heightened immunologic activity within the reticuloendothelial system (RES).  Palpable or radiographic demonstration of splenomegaly is seen in 42% of individuals  Hepatomegly  40% of patients are found to have hepatomegaly  70% demonstrate abnormalities of hepatic enzymes at some time during their illness
  • 20. Lymphadenopathy  65% of AOSD patients.  Generalized mild to moderate nodal enlargement of nontender lymph nodes located in the cervical, axillary, epitrochlear, or inguinal regions.  Mesenteric, para-aortic and hilar nodes may be discovered during diagnostic imaging
  • 21.  SEROSITIS   Pleuritis (40%)  Pleural effusions are usually bilateral, seldom large enough to be symptomatic, and rarely produce pleural thickening.  Thoracentesis often yields bloody, exudative effusions with white blood cell counts ranging from 3-20 x 103/mm3 with a polymorphonuclear predominance.
  • 22.  Pneumonitis  Pneumonitis is found in over 20% of patients  These individuals often appear septic with complaints of fever, dry cough, dyspnea and are found to have pulmonary infiltrates that are unresponsive to anti-infective therapy  Infiltrates tend to be bilateral more commonly than unilateral, alveolar or interstitial in pattern and responds well to anti-inflammatory therapy with steroids
  • 24. Absence of antinuclear antibodies Absence of rheumatoid factor, Elevated ESR and C-reactive protein Neutrophilic leukocytosis Elevated serum amyloid A Thrombocytosis Elevated serum ferritin and glycosylated ferritin Elevations the hepatic enzymes Hypoalbuminemia
  • 25.  Leukocytosis  Leukocytes counts generally range between 12,500-40,000 cells/mm3, with the highest recorded to be 69,000  ESR  90% of AOSD patients have an ESR > 50 mm/hr and 50% have and ESR > 90 mm/hr.
  • 26.  Hyperferritinemia  It has been suggested that extreme elevations of the acute phase reactant, ferritin, may be of diagnostic value in assessing patients with AOSD  Hyperferritinemia with values between 4000 30,000 mg/ml have often been reported in association with the onset and/or flare of disease activity  Levels as high as 250,000 mg/ml have been reported AOSD.
  • 28.  Diagnosis  Still disease lacks serologic test or histopathology and thus, remains a clinical diagnosis of exclusion.  AOSD is now being considered earlier in the course of evaluation of patients with fever, dermatitis and arthritis.  Diagnostic steps should include a comprehensive, noninvasive workup, documentation of fever pattern
  • 29.  Yamaguchi et al 1992  AOSD Total of > 5 criteria (including 2 major)  Major Criteria Minor Criteria Fever > 39°C Sore throat Arthralgia > 2 wks. LN or splenomegaly Still's rash Liver dysfunction Neutrophilic leukocytosis Negative RF & ANA  specificities greater than 92%, the sensitivity of Yamaguchi (96%)
  • 31. Treatment  NSAIDS or Aspirin  Mild disease with no life- threatening visceral involvement  20-25 % respond (good prognosis group with mild disease activity)  Aspirin or an NSAID should be continued for one to three months following disease remission.
  • 32.  GLUCOCORTICOSTEROIDS  Patients with very high fever,  Joint involvement that is disabling  Potentially life-threatening visceral involvement (myocarditis)  Starting dose of 0.5 to 1.0 mg/kg per day PO
  • 33.  Immunomodulating drugs  There are no controlled trials assessing the efficacy of any of the immunomodulating drugs in ASD  * Intramuscular gold salts  * Hydroxychloroquine,  * Azathioprine,  * Cyclophosphamide,  * Cyclosporine,  * Sulfasalazine,  * Methotraxate  * Intravenous immune globulin,  * Anti-TNF-alpha agents