Transcript Document
DIFFUSE ALVEOLAR
HEMORRHAGE SYNDROM
Katarina Osolnik
University Clinic of Respiratory and
Allergic Diseases, Golnik, Slovenia
Portorož, May 8th 2009
DIFFUSE ALVEOLAR
HEMORRHAGE
•
•
•
•
•
acute, life-threatening event
repeated episodes can lead to:
organizing pneumonia
collagen deposition in small airways
fibrosis
DIFFUSE ALVEOLAR
HEMORRHAGE
•
•
•
•
•
•
•
Wegener granulomatosis
microscopic polyangiitis
Goodpasture syndrome
connective tissue disorders
antiphospholipid antibody sy
infectious or toxic exposures
neoplastic conditions
CAUSES OF DIFFUSE
ALVEOLAR HEMORRHAGE
• vasculitis or capillaritis
• pulmonary haemorrhage without
capillaritis or vasculitis (»bland«
pulmonary haemorrhage)
• alveolar bleeding associated with another
process or condition
CLINICAL MANIFESTATIONS
Acute or subacute (present for less than a
week)
• dyspnea,
• cough,
• fever,
• haemoptysis are the most common clinical
manifestations of DAH.
*Haemoptysis may be absent at time of presentation in up to a third of patients.
DIAGNOSTIC EVALUATION
Chest X-ray
• diffuse, bilateral
consolidation or groundglass opacities due to
alveolar filling
• distributed in the perihilar
regions, sparing the
apices and costophrenic
angels
DIAGNOSTIC EVALUATION
HRCT
• better evaluate the
extent of disease
• more sensitive in
identifying groundglass opacities, but
not more specific
DIAGNOSTIC EVALUATION
Laboratory tests
• anemia, leukocytosis
• ESR, CRP
• blood urea and serum
creatinine, abnormal
findings of urin analysis in
pulmonary-renal sy
• anti-GBM, ANCA, C3 and
C4, anti-ds-DNA,
antiphospholipid Ab
Pulmonary function test
• increased diffusing
capacity
• restrictive changes
• obstructive changes
DIAGNOSTIC EVALUATION
Bronchoscopy
• to document alveolar hemorrhage by BAL
• to exclude airway sources of bleeding
• to exclude an associated infection
Within the first 48 hours of symptoms the diagnostic yield is higher!
BAL
• is the method of
choice
• by showing free red
blood cells and
hemosiderin-laden,
iron-positive
macrophages
BAL WITH IRON +AM
GOLNIK 2004-2009
(64+/84staining samples)
• vasculitis or capillaritis
29%
• pulmonary haemorrhage without
capillaritis or vasculitis (»bland«
pulmonary haemorrhage)
18%
• alveolar bleeding associated with another
process or condition
39%
...................................................................
• pneumoconiosis
14%
BAL WITH IRON +AM
GOLNIK 2004-2009
vasculitis or capillaritis:
• 58% sistemic
vasculitis
• 42% connective
tissue disorders
pulmonary
haemorrhage without
capillaritis or
vasculitis:
• 66% drugs
• 17% infective
endocarditis
BAL WITH IRON +AM
GOLNIK 2004-2009
alveolar bleeding associated with another
process or condition:
• 48% infections
• 32% sarcoidosis
• 20% malignant conditions
TREATMENT OF DAH
• combination of treatment autoimmune destruction of the
alveolare capillary membrane and the underlaying
condition
• immunosupresive agents are the mainstay of therapy,
especially if DAH is associated with systemic or
pulmonary vasculitis, Goodpasture syndrome or
conective tissue disorders
• treatment of small vessel vasculitis of the lung is largely
the same, regardless of aetiology or whether it is isolated
to the lung or a component of a systemic disease
TREATMENT OF DAH
Immunosupresive agents
• Methylprednisolone and
• Cyclophosphamide are the mainstay of therapy.
• Plasmapheresis - clinical benefit in Goodpasture
syndrome
• Recombinant activated human factor VIIsuccessful in several case reports of treating
alveolar hemorrhage due to allogenic hematopoietic
stem cell transplantation, ANCA associated
vascullitis, SLE or antiphospholipid syndrome.
TREATMENT OF DAH-other
possible management measures:
• supplemental oxygen,
• bronchodilators,
• reversal of any coagulopathy,
• intubation with bronchial tamponade,
• protective strategies for the less involved lung,
• mechanical ventilation
should be done in the course of the disease if they
are needed.
CONCLUSION
• DAH can be a catastrophic illness if recognition
and treatment are delayed.
• Diagnosis is often aided by other systemic
findings, associated illnes and serological
results.
• Patients with unexplained isolated DAH should
undergo a lung biopsy with immunofluorescent
studies and routine histological tests.
• During therapy close monitoring, due to potential
complications of treatment and the possibility to
relapses, is needed.