hanna przepiera-będzak klinika reumatologii pam, szczecin
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Hanna Przepiera-Będzak
Klinika Reumatologii PAM, Szczecin
LUPUS ERYTHEMATOSUSLUPUS ERYTHEMATOSUS
• autoimmune disease expressed in both localized cutaneous and systemic multiorgan forms
• characterized by humoral and cellular immunologic abnormalities that lead to tissue destruction through the deposition of immune complexes and autoantibodies
ETIOLOGYETIOLOGY
The exact etiology of LE remains unknown Factors contributing to the development of disease exposure to ultraviolet ancillary viral infections psychological stress Certain medications: procainamide, hydralazine (can lead to a drug-induced lupuslike
syndrome) women are much more likely to have lupus than men (in adults- ratio 10:1; in both
prepubertal and postmenopausal - ratio 2:1 or 3:1.) black, Asian, and Native American groups have a higher prevalence of lupus than
do whites. genetic markers that are associated with SLE
the class I major histocompatibility complex (MHC) molecule HLA-B8 the class II MHC molecules HLA-DR2 and HLA-DR3deficiencies of complement components (class III MHC molecules), specially
the absence of C2 or C4 or the presence of the C4A null allele
LUPUS ERYTHEMATOSUSLUPUS ERYTHEMATOSUSINCIDENCE AND EPIDEMIOLOGYINCIDENCE AND EPIDEMIOLOGY
• incidence
among white females two to three per 100,000
and among black females seven to eight per 100,000. • prevalence
vary between one and ten per 10,000 in the general population
one per 100 among family members of patients
LUPUS ERYTHEMATOSUSLUPUS ERYTHEMATOSUS CLINICAL FEATURES
Systemic lupus is a multisystemic disease for which the diagnosis rests on the identification of a constellation of clinical findings with supportive laboratory tests.
No single finding or test result confirms the diagnosis. However, some findings, such as a characteristic malar rash or discoid lesions or high titers of antibodies to double-stranded DNA or antibodies to the Sm antigen, in the context of a systemic illness are more suggestive than others.
Criteria for the identification and classification of patients as having SLE suitable for clinical studies have been formulated by the American Rheumatism Association
LUPUS ERYTHEMATOSUSLUPUS ERYTHEMATOSUS CONSTITUTIONAL FINDINGS
fever (fever due to infection must be differentiated from fever due to SLE. Acute severe LE may be accompanied by fever above 40 °C, but sustained fever above 39.5 °C is not common)
fatigue
anorexia,
nausea,
weight loss
LUPUS ERYTHEMATOSUSLUPUS ERYTHEMATOSUS CUTANEOUS FINDINGS Acute cutaneous lupus: facial (malar or butterfly) erythema involving the bridge of the nose and the
cheeks, often with extension to the chin and ears. It heals without scarring, although telangiectasia may occur. More extensive erythema, either palpable or nonpalpable, may involve the arms and trunk, predominantly in sun-exposed areas (exacerbated by exposure to ultraviolet light) Widespread morbilliform or bullous eruption.
Subacute cutaneous lupus: superficial, nonscarring papulosquamous or annular lesions of the trunk with a
widespread and symmetrical distribution (exacerbated by exposure to the sun) The involved skin may become hypopigmented and telangiectatic.
Chronic cutaneous lupus: discoid skin lesions, which are erythematous, raised, scaling patches most
commonly found on the head and scalp. They are characterized by follicular plugging, atrophic central scarring, depigmentation, and telangiectasia
LUPUS ERYTHEMATOSUSLUPUS ERYTHEMATOSUS MUSCULOSKELETAL FINDINGS
• arthralgia (arthritis presents classically as nonerosive, nondeforming polyarthritis with symmetrical involvement of the proximal interphalangeal joints, metacar-pophalangeal joints, wrists, and knees)
• myalgia. Muscle weakness may reflect general malaise, (sub)clinical myopathy, or overt inflammatory myositis. Electromyographic abnormalities are more common than elevations in the creatine kinase value; muscle biopsy may show myositis with fiber damage and inflammatory cells or a vacuolar myopathy. Muscle weakness may also reflect a corticosteroid-induced myopathy, a chloroquine-in duced myopathy, or a myasthenia gravis-like syndrome in addition to direct involvement of muscle by LE.
LUPUS ERYTHEMATOSUSLUPUS ERYTHEMATOSUS CARDIOVASCULAR FINDINGSCARDIOVASCULAR FINDINGS • Pericarditis is the most common manifestation. Effusions demonstrable by
echocardiography are present in more than half of patients, whereas symptomatic disease occurs in one fourth to one third of patients. Tam-ponade rarely occurs.
• Myocardial disease secondary to muscle inflammation or small vessel involvement can cause conduction defects and myocardial dysfunction leading to congestive heart failure.
• Verrucous endocarditis (Libman-Sacks syndrome) rarely leads to clinically important valvular lesions or embolic complications.
• Peripheral vascular manifestations include small vessel vasculitis, phlebothrombosis with or without thrombophlebitis, thrombosis without vasculitis, and, rarely, gangrene.
• Raynaud's phenomenon occurs in one fourth of patients. • Accelerated atherosclerosis with early myocardial infarction and
myocardiopathy is increasingly recognized as a cause of significant morbidity in LE patients, especially in those treated with glucocorticoids for long periods.
PULMONARY FINDINGSPULMONARY FINDINGS Pleuritis is the most common pulmonary finding of LE. Pleural
effusions occur in up to half the patients, whereas pleuritic pain is reported by at least two thirds.
Abnormal results of pulmonary functions tests with both restrictive and obstructive deficits occur more frequently than radiologi-cally overt interstitial fibrosis.
• Acute "lupus pneumonitis" may be extensive or more limited with only patchy infiltrates and platelike atelectasis on the chest film. Progression to acute pulmonary insufficiency with intrapulmonary hemorrhage is infrequent. Lupus pneumonitis is a diagnosis of exclusion; as with many other manifestations of LE, infection must be rigorously excluded.
RENAL FINDINGS
deposition of immunoglobulin in glomeruli is probably very common, but only about half of SLE patients have clinically evident nephritis with proteinuria, hematuria, and/or cylindruria.
In lupus nephritis the entire range of glomerular pathologic lesions (mesangial, membranous, proliferative, and membranoproliferative) as well as interstitial abnormalities have been reported.
NEUROLOGIC FINDINGSNEUROLOGIC FINDINGS seizures and psychiatric dysfunction, which may
range to overt psychosis. · organic brain syndrome, both extrapyramidal and
cerebellar dysfunction, optic neuritis, and aseptic meningitis as well as tissue infarcts and subarachnoid hemorrhage.
· headaches, which may resemble migraine · peripheral nervous system involvement cranial
nerve palsies, transverse myeitis with paraparesis or quadriparesis, and sensory or sensorimotor neuropathies.
· depression and anxiety
HEMATOLOGIC FINDINGSHEMATOLOGIC FINDINGS the lupus anticoagulant, leads to a mild prolongation of
the prothrombin time and a more significant prolongation of the partial thromboplastin time. The lupus anticoagulant is also associated with a false-positive serologic test for syphilis (VDRL)
autoimmune hemolytic anemia occurs in about 10% of patients, although a much higher percentage may have a positive Coombs' test.
leukopenia is found is about half of patients and usually reflects a lympho-penia. Granulocytopenia may also occur. The leukopenia in SLE results from both antileukocyte antibodies and other mechanisms.
thrombocytopenia is usually mild, with platelet counts remaining above 80,000 to 100,000 cells per milliliter, but severe thrombocytopenia with bleeding or risk of bleeding may occur and require corticosteroid treatment
SYSTEMIC LUPUSSYSTEMIC LUPUS ERYTHEMATOSUSERYTHEMATOSUSDRUG TREATMENTDRUG TREATMENT
CORTICOSTEROIDS
- oral 60-80 mg/day
- pulse i.v. methylprednisolone 500-1000 mg /day 2-3 days
CYCLOPHOSPHAMIDE
- - pulse i.v. 500 mg-1 g /weekly for 3 weeks followed by monthly pulses for 3-12 months (+ MESNA to eliminate cystitis)
- oral 100-200 mg/day 10-days/20 day
ANTIPHOSPHOLIPID ANTIBODY (APL) SYNDROME
the clinical constellation of:
venous and arterial thrombosis
recurrent fetal loss
thrombocytopenia
associated with the occurrence of autoantibodies with an apparent specificity for anionic phospholipids
Clinical manifestation
Venous thrombosis: Most common: deep or superficial veins of the legs
Less common: inferior vena cava, iliofemoral, axillary, renal, portal, hepatic, or retinal veins.
Clinical manifestation
Arterial thrombosis: Most common: Cerebral infarct, some strokes may be caused by cardiogenic emboli.
Less common: Coronary, retinal, and visceral artery
Clinical manifestation Other symptoms Cutaneous: livedo reticularis, splinter hemorrhages, leg ulcer, skin insarcts, blue toe syndrome
Neuro: multi-infarct dementia, chorea, transverse myelopathy, Pseudotumor cerebri, cerebral venous thrombosis
Cardiac: Coronary artery disease, valve vegetations, intracardiac thrombus
Hematologic: Thrmobocytopenia (40% of patients), hemolytic anemia
Obstetric: Late term pregnancy loss, intrauterine growth retardation.
Clinical manifestation Hypertension, coronary artery disease, hyperlipidemia, cigarette smoking, and a positive ANA are associated with an increased risk of stroke or TIA, whereas those on aspirin plus dipyridamole were at a decreased risk.
Stroke recurrence rate may be as high as 10% per year. Usually large or median branch artery infarcts and rarely causes lacunar infarcts.
Clinical manifestation
The best independent predictor of a thrombotic event is a history of thrombosis.
Cardiac valve thickening or vegetative lesions: may occur in > 30% of patients with primary Antiphospholipid antibody syndrome.
Recurrent spontaneous fetal loss: more common in the second or third trimester. Observed in 15% to 75% of Antiphospholipid antibody-positive women.
Clinical manifestation
Livedo reticularis, a lattice-like pattern of skin discoloration: most common cutaneous finding, seen in up to 80% of patients with Antiphospholipid antibodies.
Cutaneous ulcers, which may be refractory to treatment.
ANTIPHOSPHOLIPID ANTIBODY (APL) SYNDROMELABORATORY
anticardiolipin antibody: IgG, IgM
B2GP1
lupus anticoagulant
prolongation of aPTT
SCLERODERMA
Systemic sclerosis (SScI, scleroderma) is characterized by thickening and fibrosis of the skin (scleroderma) and by distinctive forms of internal organ involvement.
INCIDENCE AND EPIDEMIOLOGY
• SScI is believed to occur in four to 12 persons per million population per year
• SScI is four times more common in women than in men and is found in all racial groups and geographic areas
• disease onset is highest between ages 25 and 50. • detailed study of HLA phenotypes has failed to
reveal any consistent associations with SScI.
SCLERODERMAMUSCULOSKELETAL FEATURES
• The edema of the fingers and other locations is typically painless but may be accompanied by symptoms of morning stiffness, arthralgia, and carpal tunnel syndrome;. As skin thickening worsens, the underlying joints become tethered and restricted in motion.
• Arthritic complaints are common, and erosive arthropathy occurs in a minority. Restricted motion leads to disuse atrophy of muscles, and weakness may be worsened by accompanying skeletal muscle inflammation
• Ischemic ulcerations of the fingertips occur in 10% to 20% of patients per year, and the fingers themselves may shorten and atrophy from both disuse and ischemic re-sorption of the phalanges.
• Skin tightening on the face may restrict the ability to open the mouth and impair adequate dental hygiene.
SCLERODERMAGASTROINTESTINAL INVOLVEMENT
• Weakness of the lower esophageal sphincter is associated with chronic reflux esophagitis.
• Hypomotility of the lower esophagus causes symptoms of dysphagia for solid foods, which may be significantly worsened by lower esophageal stricture secondary to chronic reflux.
• Small bowel involvement presents as intermittent abdominal cramping and diarrhea. Malabsorption may occur and weight loss
• Colon involvement is typified by complaints of constipation. Gastrointestinal bleeding is most frequently due to erosive esophagitis, although bowel telangiectasia must also be considered.
• Hepatic involvement is uncommon, although patients with limited scleroderma may develop the complication of primary biliary cirrhosis.
SCLERODERMACARDIAC INVOLVEMENT
– Patchy fibrosis of the myocardium occurs in as many as 80% of patients with SScI.
– Contraction band necrosis has been reported, suggesting intermittent myocardial ischemia
– Raynaud-like reactivity of the coronary microvasculature is suspected.
– Symptoms of exertional dyspnea and palpitations are common, whereas chest pain and clinical congestive heart failure are not.
– Supraventricular and ventricular arrhythmias are seen in many patients, and the latter are strongly associated with mortality, including sudden death.
– Involvement of the conduction system and bradyarrhythmias are less frequently encountered.
SCLERODERMAPULMONARY INVOLVEMENT
• pulmonary involvement is a major cause of morbidity and mortality in SScl. Dyspnea on exertion is present in 50% to 60% of all patients. No organ illustrates the diversity of pathologic processes operative in SScl as well as the lung, where any combination of interstitial inflammation, fibrosis, and pulmonary vascular injury may be present.
• interstitial lung disease typified by basilar rales, abnormal chest radiographs, and loss of lung volume on pulmonary function testing.
DIAGNOSTIC TESTS• Gallium scanning is relatively insensitive in recognizing
pulmonary inflammation in SScl• bronchoalveolar lavage reveals increased numbers of
neutrophils, lymphocytes, and occasionally eosinophils in 40% to 60% of patients
SCLERODERMARENAL INVOLVEMENT
• The sudden onset of accelerated to malignant hypertension and progressive renal insufficiency usually accompanied by microangiopathic hemolytic anemia constitutes the syndrome of scleroderma renal crisis.
• Obliterative vasculopathy with cortical infarction is present and marked hyperren-inemia the principal mechanism of hypertension. Peak onset occurs during cold weather months.
• A Raynaud-like mechanism overlying renal intimal fibrotic arteriosclerosis
SCLERODERMAENDOCRINE AND EXOCRINE FEATURES
• Hypothyroidism occurs in as many as 50% of patients with SScl and is frequently occult.
• Vaginal dryness and dyspa-reunia are common. • Impotence is recognized as a presenting feature in
males • Fertility is lowered in female patients
SCLERODERMALABORATORY FINDINGS
• Nonspecific sero-logic abnormalities • antinuclear antibodies in around 90%, most typically
nucleolar in pattern; rheumatoid factor in 30%; • polyclonal hypergammaglobulinemia and
cryoglobulinemia in 20% to 40%. • moderate elevations of ESR anemia of chronic disease, • Anticentromere antibody • Anti-Scl 70 antibody is of low sensitivity, being present
in only 30% to 40% of generalized scleroderma, but is highly specific for this diagnosis.
SJÖGREN’S SYNDROME
chronic autoimmune rheumatic and lymphoproliferative disease characterized by a progressive lymphocytic and plasma cell infiltration of the salivary and lacrimal glands leading to xerostomia (dry mouth), salivary gland swelling and xerophtalmia (dry eyes)
Primarily affects women 40-50 years (F:M ratio 9:1)
PRIMARY SJÖGREN’S SYNDROME
SECONDARY SJÖGREN’S SYNDROME:accompanying RA or other connective tissue disease
SJÖGREN’S SYNDROME• Sicca syndromeo Keratoconjunctivitis - Dry eyes with reduced tear production
with gritty or sandy sensation under the lids; red eyes; photosensitivity
o Xerostomia - Decreased saliva production leading to difficulties with chewing, swallowing, and even speech; abnormality in taste and smell; dental caries; mucosal burning sensation; sensitivity to spicy and acidic foods and beverages; increased risk for oral candidiasis; hoarseness of voice
• Musculoskeletal symptomso Arthralgia, morning stiffness, nonerosive arthritiso Myalgia, muscle weakness
• Cutaneous findingso Raynaud phenomenono Nonthrombocytopenic purpura, especially of lower extremitieso Nasal, vaginal, and cutaneous dryness
SJÖGREN’S SYNDROME
•Gastrointestinal symptomsoDysphagia, nausea, epigastric painoAchalasia (in children)oAchlorhydria, chronic atrophic gastritisoPrimary biliary cirrhosis
•Pulmonary findingsoDyspnea due to mild interstitial diseaseoDry cough
•Renal findings - Interstitial nephritis•Other symptoms - Fatigue, depression
SJÖGREN’S SYNDROMEPhysical examination
•Parotid gland enlargement•Corneal ulceration, vascularization•Vasculitic lesions - Purpura•Lymphadenopathy•Autoimmune thyroiditis•Neuromuscular manifestationsoPeripheral sensorimotor neuropathyoCNS disorders, such as movement disorder, transverse myelopathy, encephalopathy, aseptic meningitis, and dementia, have been described in some studies.
SJÖGREN’S SYNDROME Physical examination
•ArthritisoIntermittent synovitisoChronic nonerosive polyarthritis: Jaccoud arthropathy is observed in adults.•Oral cavityoMild erythema and thinning of the mucosaoErythema, fissuring, coating, and depapillation of the dorsal tongueoTraumatic erosions and ulcers, angular cheilitis, and chapped lipsoFrothy, ropey, and thickened saliva
SJÖGREN’S SYNDROMELABORATORY
•CBC count with differential: Mild anemia and leukopenia are present.•Erythrocyte sedimentation rate (ESR): Elevated ESR is observed in 80-90% of patients; however, C-reactive protein (CRP) usually is within the reference range.•Immunoglobulin levels: Hypergammaglobulinemia, up to several grams of immunoglobulin G (IgG), is observed in 80% of patients.•Autoantibodies
oAntinuclear antibody (ANA) and rheumatoid factor (RF) - Usually elevatedoAnti-Ro (SS-A), anti-La (SS-B)oOther autoantibodies to thyroglobulin, thyroid microsomal, mitochondrial, smooth muscle, and salivary duct
•Rose Bengal staining: The dye stains the damaged corneal epithelium and indicates keratoconjunctivitis.
SJÖGREN’S SYNDROMEImaging Studies
•Sialography - A sensitive and specific radiographic technique to find evidence of sialectasis
•Technetium Tc 99 pertechnetate scintigraphy - Delayed uptake in Sjögren syndrome, and correlates with pathological changes
•Magnetic resonance imaging (MRI) - Visualization of the glandular parenchyma, in particular for the evaluation of cystic or solid masses (In addition, the volumetric estimate of the gland size can be determined.)
SJÖGREN’S SYNDROMEOther Tests
•In the questionnaire for salivary hypofunction, positive responses to all 4 of the following questions indicate major salivary gland hypofunction (adapted from Fox and others, 1998).
oDo you sip liquids to aid in swallowing dry foods? oDoes your mouth feel dry when eating a meal? oDo you have difficulties swallowing any foods? oDoes the amount of saliva in your mouth seem to be too little?
•Schirmer tear test: This test is used to evaluate tear production by lacrimal glands. A strip of filter paper is placed beneath the lower lid, and wetting of the paper is measured at 5 minutes. Less than 5 mm of wetting suggests decreased tear production.
SJÖGREN’S SYNDROMEOther Tests
•Salivary gland biopsyoThe pathological findings are very useful in diagnosis.
oBecause of the relative ease and lack of complications, labial minor salivary gland biopsy is preferred over parotid gland biopsy, which can result in facial nerve damage.
oIn order to ensure that a representative sample has been obtained for histopathologic examination, harvesting 5-10 lobules of minor salivary glands is important.
SJÖGREN’S SYNDROMEMedical Care
•Xerostomia - Stimulation of salivary flow with sialagogues, such as pilocarpine or cevimeline; mechanical stimulation through the use of sugarless chewing gum or lozenges; topical tissue hydration or lubrication from drinking water or the use of artificial saliva
•Oral hygiene
•Keratoconjunctivitis - Artificial tears
POLYMYOSITIS
chronic inflammatory disease of skeletal muscle characterised by symmetrical weakness of proximal limb girdle muscles as well as of the trunk, neck, and pharyngeal musculature.
When a rash is also present, the term DERMATOMYOSITIS is used
POLYMYOSITISETIOLOGY AND PATHOGENESIS
•the cause - unknown. •serum antibodies directed against certain nuclear and cytoplasmic proteins : anti-Jo 1, anti-PM-Scl, and anti-RNP, •polymyositis has occurred in several patients with hypogammaglobulinemia, •the relationship to malignancy should be considered •infectious agents Influenza B1 virus infection echovirus, coxsackievirus B1 antigens Toxoplasma gondii •there is a 2:1 female predominance
POLYMYOSITISCLINICAL FEATURES
• Proximal muscle - the onset of weakness is usually insidious, and it primarily affects the hip and/ or shoulder girdle and neck flexors. Inability to rise from a squatting or kneeling position or from a low chair, to climb stairs, and to raise arms above one's head are common early complaints that progress over a period of weeks or months
• Pharyngeal muscles: dysphagia, difficulty swallowing liquids with nasal regurgi-tation, aspiration into the tracheobronchial tree, and dysphonia.
• Weakness in the distal extremities (forearm, hand, leg, foot) is less common (25%),
• Muscle pain, aching, or tenderness on palpation may be present in up to half of patients but is usually mild.
• Late findings include atrophy with wasting, joint contractures
POLYMYOSITIS
chronic inflammatory disease of skeletal muscle characterised by symmetrical weakness of proximal limb girdle muscles as well as of the trunk, neck, and pharyngeal musculature.
When a rash is also present, the term DERMATOMYOSITIS is used
POLYMYOSITIS / DERMATOMYOSITIS ETIOLOGY AND PATHOGENESIS
•the cause - unknown. •serum antibodies directed against certain nuclear and cytoplasmic proteins : anti-Jo 1, anti-PM-Scl, and anti-RNP, •polymyositis has occurred in several patients with hypogammaglobulinemia, •the relationship to malignancy should be considered •infectious agents Influenza B1 virus infection echovirus, coxsackievirus B1 antigens Toxoplasma gondii •there is a 2:1 female predominance
POLYMYOSITIS / DERMATOMYOSITIS CLINICAL FEATURES
• Proximal muscle - the onset of weakness is usually insidious, and it primarily affects the hip and/ or shoulder girdle and neck flexors. Inability to rise from a squatting or kneeling position or from a low chair, to climb stairs, and to raise arms above one's head are common early complaints that progress over a period of weeks or months
• Pharyngeal muscles: dysphagia, difficulty swallowing liquids with nasal regurgi-tation, aspiration into the tracheobronchial tree, and dysphonia.
• Weakness in the distal extremities (forearm, hand, leg, foot) is less common (25%),
• Muscle pain, aching, or tenderness on palpation may be present in up to half of patients but is usually mild.
• Late findings include atrophy with wasting, joint contractures
POLYMYOSITIS / DERMATOMYOSITIS CLINICAL FEATURES
• Cutaneous involvement may precede, accompany, or follow muscle weakness. classic facial rash (10%-15% of patients) - affects the upper eyelids and face with edema and has a lilac or heliotrope color
• Red, scaly patches (Gottron's papules) are found over the extensor surfaces of the elbows, knees, and small joints of the hands and may be pruritic.
• Nailfolds show periungual erythema, thickening, and gross telangiectatic changes
POLYMYOSITIS / DERMATOMYOSITIS CLINICAL FEATURES
• Diffuse erythematous rash involving the forehead, neck, anterior chest, shoulders, and arms
• Pulmonary interstitial disease (pneumonitis and/or fibrosis) occurs in 10% to 20% Dyspnea, a nonproductive cough, and bibasilar interstitial roentgenographic changes are found. Pulmonary function tests reveal restrictive disease, including a reduced diffusing capacity for carbon monoxide.
• Asymptomatic electrocardiographic abnormalities
POLYMYOSITIS / DERMATOMYOSITIS LABORATORY FINDINGS
• Anemia • ESR -elevated in only one half of patients and does not appear to be
a useful guide to disease activity.• RF and antinuclear antibody are not usually present. • serum autoantibodies - Jo-1 antibody• elevated serum levels of enzymes that diffuse from damaged
muscle (95% patients) • creatine kinase - most sensitive and specific of these enzymes• aldolase• transaminases• lactate dehydrogenase • EMG - extremely sensitive but nonspecific tool; • muscle biopsy - the most conclusive evidence of myositis
WEGENER'S GRANULOMATOSIS
• a systemic vasculitis of unknown cause associated with sinopulmonary and renal system involvement and characterized by granulomatous arteritis of medium-sized vessels
• incidence is unknown - much less common than giant
cell arteritis.
• no familial tendency
• sinusitis - often relatively severe but may vary anywhere
from rhinorrhea to nasal perforation to bony dissolution
WEGENER'S GRANULOMATOSIS-CLINICAL FEATURES
• lung > 90% of patients chest x-ray - multiple pulmonary infiltrates - often
cavitary, pulmonary function tests - obstructive changes, restrictive disease atelectasis and small pleural effusions occur in less than 20% of patients.
• joint involvement in half of the patients mild and nondeforming and strikes the large joints,
polyarticular symmetrical • eyes - in half the cases
anterior chamber inflammatory changes; uveitis; optic neuropathies (III, IV, VI cranial nerves; proptosis
• cough • renal disease
urine sediment abnormal, containing red blood cells, casts, and protein
• central nervous system 20% to 50% of patients.
WEGENER'S GRANULOMATOSISLABORATORY FINDINGS
• ESR elevated • autoantibody to certain neutrophil cytoplasmic antigens (ANCA)• white blood count - increased • anemia of a normocytic normochromic type • platelets may be increased • complement levels in the serum are usually normal• mild eosinophilia
• in patients with renal disease- urinalysis abnormal