* Caseating granulomas containing Langhans giant cells, which have a "horseshoe" pattern of nuclei.
* Caseating granulomas containing Langhans giant cells, which have a "horseshoe" pattern of nuclei.
* Culture in Lowenstein-Jensen, and solid agar-based such as Middlebrook 7H11 or 7H10
* Culture in Lowenstein-Jensen, and solid agar-based such as Middlebrook 7H11 or 7H10
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* Tuberculosis can involve almost every organ in human body such as skin, renal, glands, eyes, neurons, etc.
|-
|-
| colspan="2" |Eosinophilic granulomatosis with polyangiitis (Churg-Strauss)
| colspan="2" |Eosinophilic granulomatosis with polyangiitis (Churg-Strauss)
Line 312:
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* Interstitial and perivascular necrotizing granulomas
* Interstitial and perivascular necrotizing granulomas
* Areas of necrosis
* Areas of necrosis
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* Skin, cardiovascular, gastrointestinal, renal, and neurologic systems may also be involved.
|-
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| colspan="2" |Drug- and toxin-induced eosinophilic lung diseases
| colspan="2" |Drug- and toxin-induced eosinophilic lung diseases
Line 361:
Line 363:
* ≥40 percent
* ≥40 percent
* Eosinophilia may be absent in 10-20% of patients
* Eosinophilia may be absent in 10-20% of patients
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* Bilateral peripheral or pleural-based infiltrates described as the "photographic negative" of pulmonary edema is virtually pathognomonic for the disease (in 33% of cases)
* Bilateral peripheral or pleural-based infiltrates described as the "photographic negative" of pulmonary edema is virtually pathognomonic for the disease (in 33% of cases)
| style="background: #F5F5F5; padding: 5px;" |Like tuberculosis, sarcoidosis can involve almost every organ in human body such as skin, renal, glands, eyes, neurons, etc.
* Peripheral ring shadows suggesting [[Cyst|cysts]] formation
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* '''Head CT''' scan may be helpful in the diagnosis of Langerhans cell histiocytosis.
* Findings on head CT scan suggestive of Langerhans cell histiocytosis include:
:* Multiple osteolytic lesions
:* Full thickness [[bone]] destruction
:* “Button sequestrum” sign
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* '''Light microscopy:'''
* Clusters of [[Dendritic cell|dendritic cells]]
* [[Kidney]]-shaped nucleus
* Abundant foamy [[cytoplasm]]
* Fine, granular [[chromatin]] pattern
* Prominent [[Eosinophil|eosinophils]]
* [[Fibrosis]]
* Other [[Inflammation|inflammatory cells]] may be present ([[Neutrophil|neutrophils]], [[Plasma cell|plasma cells]], and multinucleated giant cells)
* '''Electron microscopy''' Langerhans cell histiocytosis is characterized by Birbeck granules, which are electron dense, cytoplasmic, tennis racket-like bodies.
* '''Immunohistochemistry'''
* [[CD1a]] +ve
* S100 +ve
* CD207 (langerin) +ve
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* On [[Technetium|Tc 99m]] MDP whole body bone scintigraphy, Langerhans cell histiocytosis is characterized by an increased uptake of Tc 99m at hitiocytic lesion located around the [[Rib|ribs]], [[spine]], and [[pelvis]].
Loeffler syndrome must be differentiated from other diseases that cause pulmonary eosinophilia, such as Churg-Strauss, drug and toxin-induced eosinophilic lung diseases, other helminthic and fungal infection related eosinophilic lung diseases, and nonhelminthic infections such as Coccidioidomycosis, and Mycobacterium tuberculosis.
Differentiating Loeffler syndrome from other pulmonary eosinophilia syndromes on the basis of etiology.
Diseases
Clinical manifestations
Para-clinical findings
Additional findings
Symptoms
Physical examination
Lab Findings
Imaging
Histopathology
Increased Eosinophil
count
Other lab findings
CXR
CT Scan
Helminthic
and fungal infection-related
eosinophilic lung diseases
Transpulmonary
passage of larvae (Loffler's syndrome)
Cough
Sputum production
Wheezing
Fever
Crackles
Mild to moderate
Usually 5-20%
Stool exam
Parasites and ova can be found in the stool 6-12 weeks after the initial parasitic infection.
Immunoglobulin E (IgE) level
Might be elevated.
Round or oval opacities (several millimeters to several centimeters)
In both lungs
Generally present when blood eosinophilia exceeds 10%
Migratory
May become confluent in perihilar areas
Generally clear spontaneously
Areas of ground-glass opacity (halo) around consolidation
Nodules
Dilated airways within the lesion
Bronchoscopy and bronchoalveolar lavage
May show increased eosinophilic count.
Sputum analysis or gastric lavage
May occasionally show Larvae of Ascaris or the other parasites with pulmonary cycle.
Ascaris lumbricoides
Hookworms such as:
Ancylostoma duodenale
Necator americanus)
Strongyloides stercoralis
Tropical
pulmonary
eosinophilia
Cough
Breathlessness
Fatigue
Fever.
Wheezing
Crackles
40 to 70 percent (>3000/microL) plus elevated IgE levels ( >1000 units/mL)
Serum IgE levels
Antifilarial antibodies
Diffuse opacities
Around 20% of patients have a normal CXR
Reticular and small nodular opacities
Bronchiectasis
Air trapping
Calcification
Mediastinal adenopathy
Wuchereria bancrofti
Brugia malayi
The diagnostic criteria for tropical pulmonary eosinophilia include:
a history supportive of exposure to lymphatic filariasis;
a peripheral eosinophilia count greater than 3 × 109/L);
an elevated serum IgE levels (> 1000 kU/L);
increased titers of antifilarial antibodies;
peripheral blood negative for microfilariae; and
a clinical response to diethylcarbamazine.
Allergic bronchopulmonary aspergillosis
Repeated episodes of:
Bronchial obstruction, inflammation
Mucoid impaction
Can lead to:
Bronchiectasis
Fibrosis
Respiratory compromise
Clinical picture of ABPA is dominated by underlying asthma (or cystic fibrosis)
Bronchial obstruction
Fever
Malaise,
Expectoration of brownish mucous plugs
Peripheral blood eosinophilia
Hemoptysis
Wheezing
Fever
Crackles
Wheezing
Mild to moderate
Immunological tests for Aspergillus
Sputum staining and sputum cultures
Skin test for Aspergillus sp.
Early in the disease
Normal
Changes of asthma.
Transient patchy areas of consolidation may be evident representing eosinophilic pneumonia.
Late stage
Bronchiectasis may be evident.
Mucoid impaction in dilated bronchi can appear mass-like or sausage shaped or branching opacities (finger in glove sign).*
Pulmonary collapse may be seen as a consequence of endobronchial mucoid impaction.
Fleeting shadows over time can also be a characteristic feature of this disease.
These opacities usually appear and disappear in different areas of the lung over a period of time as transient pulmonary infiltrates.
HRCT:
Widespread proximal cylindrical bronchiectasis with upper lobe predominance and bronchial wall thickening.
Central bronchiectasis with normal tapering of distal bronchi (classic manifestation of ABPA, neither sensitive nor specific)
Asthmatic bronchiolitis, eosinophilic pneumonia, bronchocentric granulomatosis, and mucoid impaction of bronchi
+/- bronchocentric granulomatosis (pulmonary eosinophilia in the absence of endobronchial fungi)
Minimal criteria include:
The presence of asthma and/or cystic fibrosis,
A positive skin test to Aspergillus sp., an IgE > 417 IU/mL (or kU/L)
An increased specific IgE or IgG Aspergillus sp. antibodies
The presence of infiltrates on a chest X-ray
Heavy
hematogenous
seeding
with
helminths
Depends on the organism for example:
Periorbital edema, myositis, and eosinophilia (Trichinellosis)
Depends on the organism for example:
Periorbital edema
Tenderness in muscles
Fever
(Trichinellosis)
Mild to
moderate to
high
Trichinellosis: Ab will be positive 2-8 weeks after infection
Strongyloides: ELISA is generally positive while stool examination is often negative.
Strongyloides:
Diffuse ground glass opacities
Miliary nodules,
Reticular opacities
Airspace opacities ranging from multifocal to lobar distribution.
Adult respiratory distress syndrome :If widespread air space shadowing is seen on chest radiography
Rarely: granulomatous changes leading to pulmonary fibrosis.
Transient nodular or diffuse pulmonary infiltrates on the chest x-ray
Spontaneous pneumothoraces have been described infrequently.
Similar to Loeffler syndrome
Ascarids and hookworms
Trichinellosis
Disseminated strongyloidiasis
Cutaneous and visceral larva migrans
Schistosomiasis
Prior treatment with glucocorticoids may be a risk factor.
Pulmonary parenchymal invasion
Fever
Crackles
Wheezing
Eosinophilia is prominent in the early stages of disease but minimal with established disease
Ab testing Useful in later infection with Paragonimus
Nodular with surrounding areas of ground glass
Peripheral
Common in the mid- and lower lung zones
Nodular with surrounding areas of ground glass
Peripheral
Common in the mid- and lower lung zones
Finding eggs in the sputum or bronchoalveolar lavage fluid
Helminths such as paragonimiasis
Nonhelminthic infections
Coccidioidomycosis
Manifests as a community-acquired pneumonia (CAP) approximately 7 to 21 days after exposure
Fever
Crackles
Wheezing
Nail clubbing
Mild
Antibody testing may be negative early in the course of disease
Polymerase chain reaction (PCR)
Rarely demonstrate nodules or cavities in the lungs, but these images commonly demonstrate lung opacification, pleural effusions, or enlargement of lymph nodes associated with the lungs.
Computed tomography scans of the chest are better able to detect these changes than chest x-rays
Papanicolaou or Grocott's methenamine silver staining. These stains can demonstrate spherules and surrounding inflammation.
Types:
Acute coccidioidomycosis, sometimes described in literature as primary pulmonary coccidioidomycosis
Chronic coccidioidomycosis
Disseminated coccidioidomycosis, which includes primary cutaneous coccidioidomycosis
Mycobacterium tuberculosis
Cough
Weight loss
Fatigue
Night sweating
Sputum production
Fever
Chills
Mild
Quantiferon gold
Positive PPD
Elevated ESR
In active pulmonary TB, infiltrates or consolidations and/or cavities are often seen in the upper lungs with or without mediastinal or hilar lymphadenopathy.
Old healed tuberculosis usually presents as pulmonary nodules in the hilar area or upper lobes, with or without fibrotic scars and volume loss.
Bronchiectasis and pleural scarring may be present.
Ziehl-Neelsen stain, or fluorescent stains such as auramine
Caseating granulomas containing Langhans giant cells, which have a "horseshoe" pattern of nuclei.
Culture in Lowenstein-Jensen, and solid agar-based such as Middlebrook 7H11 or 7H10
Tuberculosis can involve almost every organ in human body such as skin, renal, glands, eyes, neurons, etc.
Eosinophilic granulomatosis with polyangiitis (Churg-Strauss)
Sinusitis
Asthma,
Skin, cardiovascular, gastrointestinal, renal, and neurologic systems may also be involved.
Aluminum silicate and particulate metals •Sulfite •Scorpion stings •Inhalation of o heroin, crack cocaine, or marijuana •Inhalation of organic chemicals, dust or smoke, during rubber manufacture, fireworks, firefighting, tobacco smoking •Abuse of 1,1,1-trichloroethane (Scotchgard)
Chronic eosinophilic pneumonia
Predominantly in women and nonsmokers
Following radiation therapy for breast cancer
Cough, fever, progressive breathlessness, weight loss, wheezing, and night sweats; asthma accompanies or precedes the illness in 50 percent of cases
Fever
Crackles
Wheezing
≥40 percent
Eosinophilia may be absent in 10-20% of patients
-
Bilateral peripheral or pleural-based infiltrates described as the "photographic negative" of pulmonary edema is virtually pathognomonic for the disease (in 33% of cases)
Pleural effusion
Cavitation
BAL eosinophilia ≥25 percent is suggestive of CEP.
Nodular bronchial mucosal lesions
Necrotizing eosinophilic inflammation
Lung biopsy:
Interstitial and alveolar eosinophils and histiocytes, including multinucleated giant cells
Fibrosis (minimal)
Organizing pneumonia (common)
-
Idiopathic acute eosinophilic pneumonia
Acute respiratory failure in a previously healthy patient
Acute febrile illness of less than seven days' duration, characterized by:
Nonproductive cough
Dyspnea,
Fever
Crackles
Wheezing
≥25 percent
-
Non specific but might reveal
Diffuse pulmonary opacities on imaging
Bronchoalveolar lavage that reveals ≥25 percent eosinophils
When the diagnosis is uncertain lung biopsy is recommended:
Histopathologic findings include:
Diffuse alveolar damage
Hyaline membranes
Marked numbers of interstitial and lesser numbers of alveolar eosinophils
Often associated with recent initiation or resumption of cigarette smoking
Less commonly with heavy inhalational exposure to smoke, fine sand, or dust
Electron microscopy Langerhans cell histiocytosis is characterized by Birbeck granules, which are electron dense, cytoplasmic, tennis racket-like bodies.
On Tc 99m MDP whole body bone scintigraphy, Langerhans cell histiocytosis is characterized by an increased uptake of Tc 99m at hitiocytic lesion located around the ribs, spine, and pelvis.
